Download PDF

Clinical Trial Results:
A Randomized, Multicenter, Open-Label Cross-Over Study to Evaluate Patient Preference and Satisfaction of Subcutaneous Administration of the Fixed-Dose Combination of Pertuzumab and Trastuzumab in Patients with HER2-Positive Early Breast Cancer

Summary
EudraCT number	2018-002153-30
Trial protocol	ES PT SE FI
Global end of trial date

Results information
Results version number	v1
This version publication date	04 Mar 2021
First version publication date	04 Mar 2021
Other versions	v2 , v3

Trial Information
Subject Disposition
Baseline Characteristics
End Points
Adverse Events
More Information

Collapse all Expand all

Trial information

Top of page

Sponsor protocol code

MO40628

ISRCTN number

US NCT number

NCT03674112

WHO universal trial number (UTN)

Sponsor organisation name

F. Hoffmann-La Roche, Ltd.

Sponsor organisation address

Grenzacherstrasse 124, Basel, Switzerland, CH-4070

Public contact

F. Hoffmann-La Roche, Ltd., F. Hoffmann-La Roche, Ltd., +41 616878333, global.trial_information@roche.com

Scientific contact

F. Hoffmann-La Roche, Ltd., F. Hoffmann-La Roche, Ltd., +41 616878333, global.trial_information@roche.com

Is trial part of an agreed paediatric investigation plan (PIP)

Does article 45 of REGULATION (EC) No 1901/2006 apply to this trial?

Does article 46 of REGULATION (EC) No 1901/2006 apply to this trial?

Analysis stage

Interim

Date of interim/final analysis

24 Feb 2020

Is this the analysis of the primary completion data?

Yes

Primary completion date

24 Feb 2020

Global end of trial reached?

Main objective of the trial

The primary objective for this study is to evaluate patient preference for pertuzumab and trastuzumab FDC SC.

Protection of trial subjects

This study is conducted in full conformance with the ICH E6 guideline for Good Clinical Practice and the principles of the Declaration of Helsinki, or the laws and regulations of the country in which the research is conducted, whichever affords the greater protection to the individual. All participants are required to read and sign an informed consent form prior to participation in the study.

Background therapy

Evidence for comparator

Actual start date of recruitment

19 Dec 2018

Long term follow-up planned

Yes

Long term follow-up rationale

Safety, Efficacy

Long term follow-up duration

3 Years

Independent data monitoring committee (IDMC) involvement?

Yes

Number of subjects enrolled per country

Country: Number of subjects enrolled

Argentina: 8

Country: Number of subjects enrolled

Brazil: 10

Country: Number of subjects enrolled

Chile: 8

Country: Number of subjects enrolled

Finland: 10

Country: Number of subjects enrolled

Hong Kong: 8

Country: Number of subjects enrolled

Jordan: 5

Country: Number of subjects enrolled

Lebanon: 3

Country: Number of subjects enrolled

Mexico: 4

Country: Number of subjects enrolled

Panama: 7

Country: Number of subjects enrolled

Portugal: 24

Country: Number of subjects enrolled

Qatar: 2

Country: Number of subjects enrolled

Saudi Arabia: 2

Country: Number of subjects enrolled

Serbia: 22

Country: Number of subjects enrolled

Spain: 18

Country: Number of subjects enrolled

Sweden: 6

Country: Number of subjects enrolled

United States: 23

Worldwide total number of subjects

160

EEA total number of subjects

Number of subjects enrolled per age group

In utero

Preterm newborn - gestational age < 37 wk

Newborns (0-27 days)

Infants and toddlers (28 days-23 months)

Children (2-11 years)

Adolescents (12-17 years)

Adults (18-64 years)

140

From 65 to 84 years

85 years and over

Subject disposition

Top of page

Recruitment details

Screening details

A total of 183 patients were screened and 160 participants were enrolled.

Period 1 title

Overall Study (overall period)

Is this the baseline period?

Yes

Allocation method

Randomised - controlled

Blinding used

Not blinded

Are arms mutually exclusive

Yes

A: P+H IV Followed by PH FDC SC

Arm description

In the Treatment Cross-Over Period of the study, participants randomized to Arm A first received pertuzumab IV and trastuzumab IV (P+H IV) administration for 3 treatment cycles followed by the pertuzumab and trastuzumab fixed-dose combination subcutaneous (PH FDC SC) administration for 3 treatment cycles (1 cycle = 21 days). Following completion of this study period, participants chose one of the two study treatments to receive in the Treatment Continuation Period for the remaining anti-HER2 treatment cycles (18 planned cycles in total, including pre-study neoadjuvant treatment). After completing study treatment, participants entered the Follow-up Period wherein they were to be followed for 3 years from the date the last participant was randomized.

Arm type

Experimental

Investigational medicinal product name

Pertuzumab

Investigational medicinal product code

RO4368451

Other name

Perjeta

Pharmaceutical forms

Concentrate for solution for infusion

Routes of administration

Intravenous use

Dosage and administration details

Pertuzumab was non-weight based and was administered as an intravenous (IV) infusion once every 3 weeks (Q3W) in 2 dose configurations as follows: Loading dose of 840 milligrams (mg) IV, and maintenance dose of 420 mg IV. The dose and schedule were consistent with the prescribing information. Loading doses of pertuzumab and trastuzumab (P+H) IV were only required for subjects who had ≥6 weeks since their last neoadjuvant dose of P+H at study entry or ≥6 weeks since their last study treatment during the study. Maintenance doses were used for subsequent administrations or dose delays <6 weeks between doses.

Investigational medicinal product name

Trastuzumab

Investigational medicinal product code

Ro 45-2317

Other name

Herceptin

Pharmaceutical forms

Powder for concentrate for solution for infusion

Routes of administration

Intravenous use

Dosage and administration details

Trastuzumab was weight based and was administered as an intravenous (IV) infusion Q3W after completion of the pertuzumab infusion and observation period in 2 dose configurations as follows: Loading dose of 8 milligrams per kilogram (mg/kg) IV, and maintenance dose of 6 mg/kg IV. The dose and schedule were consistent with the prescribing information. Loading doses of pertuzumab and trastuzumab (P+H) IV were only required for subjects who had ≥6 weeks since their last neoadjuvant dose of P+H at study entry or ≥6 weeks since their last study treatment during the study. Maintenance doses were used for subsequent administrations or dose delays <6 weeks between doses.

Investigational medicinal product name

Pertuzumab and trastuzumab FDC SC

Investigational medicinal product code

RO7198574

Other name

Phesgo

Pharmaceutical forms

Solution for injection

Routes of administration

Subcutaneous use

Dosage and administration details

The pertuzumab and trastuzumab fixed-dose combination subcutaneous (FDC SC) administration was non-weight based and was administered as an SC injection to the thigh Q3W in 2 dose configurations as follows: Loading dose of 1200 milligrams (mg) pertuzumab and 600 mg trastuzumab SC; and maintenance dose of 600 mg pertuzumab and 600 mg trastuzumab SC. Loading doses of pertuzumab and trastuzumab (PH) FDC SC were only required for subjects who had ≥6 weeks since their last neoadjuvant dose of P+H at study entry or ≥6 weeks since their last study treatment during the study. Maintenance doses were used for subsequent administrations or dose delays <6 weeks between doses.

B: PH FDC SC Followed by P+H IV

Arm description

In the Treatment Cross-Over Period of the study, participants randomized to Arm B first received the pertuzumab and trastuzumab fixed-dose combination subcutaneous (PH FDC SC) administration for 3 treatment cycles followed by pertuzumab intravenous (IV) and trastuzumab IV (P+H IV) administration for 3 treatment cycles (1 cycle = 21 days). Following completion of this study period, participants chose one of the two study treatments to receive in the Treatment Continuation Period for the remaining anti-HER2 treatment cycles (18 planned cycles in total, including pre-study neoadjuvant treatment). After completing study treatment, participants entered the Follow-up Period wherein they were to be followed for 3 years from the date the last participant was randomized.

Arm type

Experimental

Investigational medicinal product name

Pertuzumab and trastuzumab FDC SC

Investigational medicinal product code

RO7198574

Other name

Phesgo

Pharmaceutical forms

Solution for injection

Routes of administration

Subcutaneous use

Dosage and administration details

Investigational medicinal product name

Pertuzumab

Investigational medicinal product code

RO4368451

Other name

Perjeta

Pharmaceutical forms

Concentrate for solution for infusion

Routes of administration

Intravenous use

Dosage and administration details

Investigational medicinal product name

Trastuzumab

Investigational medicinal product code

Ro 45-2317

Other name

Herceptin

Pharmaceutical forms

Powder for concentrate for solution for infusion

Routes of administration

Intravenous use

Dosage and administration details

Number of subjects in period 1	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Started	80	80
Completed Cross-Over (Cycles 1 to 6)	80	80
Completed Continuation (Cycles 7 to 18)	34	36
Completed Follow-Up (Up to 3 Years)	0	0
Completed	0	0
Not completed	80	80
Adverse event, non-fatal	1	-
Ongoing in the Study	79	80

Baseline characteristics

Top of page

Reporting group title

A: P+H IV Followed by PH FDC SC

Reporting group description

Reporting group title

B: PH FDC SC Followed by P+H IV

Reporting group description

Reporting group values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV	Total
Number of subjects	80	80	160
Age categorical
Units: Subjects
In utero	0	0	0
Preterm newborn infants (gestational age < 37 wks)	0	0	0
Newborns (0-27 days)	0	0	0
Infants and toddlers (28 days-23 months)	0	0	0
Children (2-11 years)	0	0	0
Adolescents (12-17 years)	0	0	0
Adults (18-64 years)	68	72	140
From 65-84 years	12	8	20
85 years and over	0	0	0
Age Continuous
Units: Years
arithmetic mean (standard deviation)	49.4 ( 11.6 )	48.2 ( 12.1 )	-
Sex: Female, Male
Units: Participants
Female	80	80	160
Male	0	0	0
Ethnicity (NIH/OMB)
Units: Subjects
Hispanic or Latino	17	21	38
Not Hispanic or Latino	59	54	113
Unknown or Not Reported	4	5	9
Race (NIH/OMB)
Units: Subjects
American Indian or Alaska Native	5	3	8
Asian	8	4	12
Native Hawaiian or Other Pacific Islander	0	0	0
Black or African American	2	2	4
White	62	67	129
More than one race	0	0	0
Unknown or Not Reported	3	4	7
Eastern Cooperative Oncology Group (ECOG) Performance Status at Baseline
ECOG Performance Status: 0 = Fully active, able to carry on all pre-disease performance without restriction; 1 = Restricted in physically strenuous activity but ambulatory and able to carry out work of a light or sedentary nature, e.g., light housework or office work.
Units: Subjects
ECOG Peformance Status 0	70	70	140
ECOG Peformance Status 1	10	10	20
Number of Cycles of Prior Neoadjuvant Pertuzumab IV and Trastuzumab IV
Units: Subjects
<4 Cycles	5	10	15
≥4 Cycles	75	70	145
Prior Neoadjuvant Chemotherapy Regimen
Participants were stratified at randomization according to prior neoadjuvant chemotherapy regimen, pathological complete response to prior neoadjuvant treatment, and hormone receptor status.
Units: Subjects
Anthracyclines + Taxanes	55	53	108
Carboplatin + Taxanes	22	23	45
Taxanes Only	3	4	7
Pathological Complete Response (pCR) to Prior Neoadjuvant Treatment
Participants were stratified at randomization according to prior neoadjuvant chemotherapy regimen, pathological complete response to prior neoadjuvant treatment, and hormone receptor status.
Units: Subjects
pCR	52	50	102
Non-pCR	28	30	58
Hormone Receptor Status
Participants were stratified at randomization according to prior neoadjuvant chemotherapy regimen, pathological complete response to prior neoadjuvant treatment, and hormone receptor status (estrogen receptor [ER] and progesterone receptor [PgR]).
Units: Subjects
ER-Positive and/or PgR-Positive	53	51	104
ER-Negative and PgR-Negative	27	29	56
Baseline Weight
Units: kilograms (kg)
arithmetic mean (standard deviation)	67.36 ( 12.08 )	70.21 ( 14.15 )	-

End points

Top of page

Reporting group title

A: P+H IV Followed by PH FDC SC

Reporting group description

Reporting group title

B: PH FDC SC Followed by P+H IV

Reporting group description

Subject analysis set title

All Participants

Subject analysis set type

Modified intention-to-treat

Subject analysis set description

In the Treatment Cross-Over Period of the study, all participants received their first 6 cycles of treatment in accordance with the study arm to which they were randomized: Arm A) pertuzumab IV and trastuzumab IV (P+H IV) for 3 treatment cycles followed by the pertuzumab and trastuzumab fixed-dose combination for subcutaneous administration (PH FDC SC) for 3 treatment cycles (1 cycle = 21 days); or Arm B) PH FDC SC for 3 treatment cycles followed by P+H IV for 3 treatment cycles (1 cycle = 21 days). Following completion of this study period, participants chose one of the two study treatments to receive in the Treatment Continuation Period for the remaining anti-HER2 treatment cycles (18 planned cycles in total, including pre-study neoadjuvant treatment). After completing study treatment, participants entered the Follow-up Period wherein they were to be followed for 3 years from the date the last participant was randomized.

Subject analysis set title

All Participants: TASQ-IV Completers

Subject analysis set type

Modified intention-to-treat

Subject analysis set description

This analysis set includes all participants from Arms A and B who completed the TASQ-IV questionnaire, which was administered at the last IV treatment cycle in the Treatment Cross-Over Period of the study. During the Treatment Cross-Over Period, all participants received their first 6 cycles of treatment in accordance with the study arm to which they were randomized: Arm A) pertuzumab IV and trastuzumab IV (P+H IV) for 3 treatment cycles followed by the pertuzumab and trastuzumab fixed-dose combination for subcutaneous administration (PH FDC SC) for 3 treatment cycles (1 cycle = 21 days); or Arm B) PH FDC SC for 3 treatment cycles followed by P+H IV for 3 treatment cycles (1 cycle = 21 days).

Subject analysis set title

All Participants: TASQ-SC Completers

Subject analysis set type

Modified intention-to-treat

Subject analysis set description

This analysis set includes all participants from Arms A and B who completed the TASQ-SC questionnaire, which was administered at the last SC treatment cycle in the Treatment Cross-Over Period of the study. During the Treatment Cross-Over Period, all participants received their first 6 cycles of treatment in accordance with the study arm to which they were randomized: Arm A) pertuzumab IV and trastuzumab IV (P+H IV) for 3 treatment cycles followed by the pertuzumab and trastuzumab fixed-dose combination for subcutaneous administration (PH FDC SC) for 3 treatment cycles (1 cycle = 21 days); or Arm B) PH FDC SC for 3 treatment cycles followed by P+H IV for 3 treatment cycles (1 cycle = 21 days).

Subject analysis set title

All Healthcare Professionals

Subject analysis set type

Intention-to-treat

Subject analysis set description

This analysis set includes all healthcare professionals who treated participants from Arms A and B and completed the HCPQ questionnaire, which was administered at the last treatment cycle in the Treatment Cross-Over Period of the study. During the Treatment Cross-Over Period, all participants received their first 6 cycles of treatment in accordance with the study arm to which they were randomized: Arm A) pertuzumab IV and trastuzumab IV (P+H IV) for 3 treatment cycles followed by the pertuzumab and trastuzumab fixed-dose combination for subcutaneous administration (PH FDC SC) for 3 treatment cycles (1 cycle = 21 days); or Arm B) PH FDC SC for 3 treatment cycles followed by P+H IV for 3 treatment cycles (1 cycle = 21 days).

Subject analysis set title

Arm A: Treatment With P+H IV (Cycles 1–3)

Subject analysis set type

Safety analysis

Subject analysis set description

This safety analysis population only includes the adverse events that occurred in Arm A participants during treatment Cycles 1 to 3 when all Arm A participants were treated with P+H IV. In the Treatment Cross-Over Period of the study, participants randomized to Arm A first received treatment with pertuzumab IV and trastuzumab IV (P+H IV) for 3 treatment cycles and that was followed by treatment with pertuzumab and trastuzumab FDC SC (PH FDC SC) for 3 treatment cycles (1 cycle = 21 days).

Subject analysis set title

Arm A: Treatment With PH FDC SC (Cycles 4–6)

Subject analysis set type

Safety analysis

Subject analysis set description

This safety analysis population only includes adverse events that occurred in Arm A participants during treatment Cycles 4 to 6 when all Arm A participants were treated with PH FDC SC. In the Treatment Cross-Over Period of the study, participants randomized to Arm A first received treatment with pertuzumab IV and trastuzumab IV (P+H IV) for 3 treatment cycles and that was followed by treatment with pertuzumab and trastuzumab FDC SC (PH FDC SC) for 3 treatment cycles (1 cycle = 21 days).

Subject analysis set title

Arm B: Treatment With PH FDC SC (Cycles 1–3)

Subject analysis set type

Safety analysis

Subject analysis set description

This safety analysis population only includes adverse events that occurred in Arm B participants during treatment Cycles 1 to 3 when all Arm B participants were treated with PH FDC SC. In the Treatment Cross-Over Period of the study, participants randomized to Arm B first received treatment with pertuzumab and trastuzumab FDC SC (PH FDC SC) for 3 treatment cycles and that was followed by treatment with pertuzumab IV and trastuzumab IV (P+H IV) for 3 treatment cycles (1 cycle = 21 days).

Subject analysis set title

Arm B: Treatment With P+H IV (Cycles 4–6)

Subject analysis set type

Safety analysis

Subject analysis set description

This safety analysis population only includes adverse events that occurred in Arm B participants during treatment Cycles 4 to 6 when all Arm B participants were treated with P+H IV. In the Treatment Cross-Over Period of the study, participants randomized to Arm B first received treatment with pertuzumab and trastuzumab FDC SC (PH FDC SC) for 3 treatment cycles and that was followed by treatment with pertuzumab IV and trastuzumab IV (P+H IV) for 3 treatment cycles (1 cycle = 21 days).

Subject analysis set title

P+H IV: Treatment Cross-Over Period

Subject analysis set type

Safety analysis

Subject analysis set description

This safety analysis population includes all participants from Arms A and B who received up to 3 cycles (1 cycle = 21 days) of treatment with pertuzumab IV and trastuzumab IV (P+H IV) during the Treatment Cross-Over Period of the study.

Subject analysis set title

PH FDC SC: Treatment Cross-Over Period

Subject analysis set type

Safety analysis

Subject analysis set description

This safety analysis population includes all participants from Arms A and B who received up to 3 cycles (1 cycle = 21 days) of treatment with the pertuzumab and trastuzumab fixed-dose combination administered subcutaneously (PH FDC SC) during the Treatment Cross-Over Period of the study.

Subject analysis set title

P+H IV: Treatment Continuation Period

Subject analysis set type

Safety analysis

Subject analysis set description

This safety analysis population includes all participants from Arms A and B who, following completion of the Treatment Cross-Over Period, chose to receive pertuzumab IV and trastuzumab IV (P+H IV) during the Treatment Continuation Period for the remaining anti-HER2 treatment cycles (18 planned cycles in total, including pre-study neoadjuvant treatment).

Subject analysis set title

PH FDC SC: Treatment Continuation Period

Subject analysis set type

Safety analysis

Subject analysis set description

This safety analysis population includes all participants from Arms A and B who, following completion of the Treatment Cross-Over Period, chose to receive the pertuzumab and trastuzumab fixed-dose combination administered subcutaneously (PH FDC SC) during the Treatment Continuation Period for the remaining anti-HER2 treatment cycles (18 planned cycles in total, including pre-study neoadjuvant treatment).

Primary: Percentage of Participants by Their Preferred Method of Pertuzumab and Trastuzumab Administration, as Assessed in Question 1 of the Patient Preference Questionnaire (PPQ)

Top of page

End point title

Percentage of Participants by Their Preferred Method of Pertuzumab and Trastuzumab Administration, as Assessed in Question 1 of the Patient Preference Questionnaire (PPQ) ^[1]

End point description

Question 1 of the Patient Preference Questionnaire (PPQ) asked participants the following question: “All things considered, which method of administration did you prefer?" The three available options for a participant's response were: IV, SC, or No preference. A point estimate with associated exact Clopper-Pearson binomial 95% confidence interval (CI) was calculated only for the percentage of participants who preferred PH FDC SC (i.e., 95% CI values of 0.000000 to 999999 for IV and No Preference only indicate that they were not calculated). The modified Intent-to-Treat (mITT) population was analyzed, which included all randomized participants allocated to their randomized treatment arm, who received at least one dose by both SC and IV routes of administration during the Treatment Cross-over Period and subsequently answered at least Question 1 of the PPQ.

End point type

Primary

End point timeframe

Cycle 6 Day 1 (each cycle is 21 days)

Notes
[1] - No statistical analyses have been specified for this primary end point. It is expected there is at least one statistical analysis for each primary end point.
Justification: No formal hypothesis testing was planned for this study. The results are presented using descriptive statistics.

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV	All Participants
Number of subjects analysed	80	80	160
Units: Percentage of participants
number (confidence interval 95%)
SC Preference	87.50 (78.21 to 93.84)	82.50 (72.38 to 90.09)	85.00 (78.51 to 90.15)
IV Preference	12.5 (0.000000 to 999999)	15.0 (0.000000 to 999999)	13.8 (0.000000 to 999999)
No Preference	0.0 (0.000000 to 999999)	2.5 (0.000000 to 999999)	1.3 (0.000000 to 999999)

No statistical analyses for this end point

Secondary: Percentage of Participants by Responses to the Strength of Their Preferred Method of Pertuzumab and Trastuzumab Administration, as Assessed in Question 2 of the Patient Preference Questionnaire (PPQ)

Top of page

End point title

Percentage of Participants by Responses to the Strength of Their Preferred Method of Pertuzumab and Trastuzumab Administration, as Assessed in Question 2 of the Patient Preference Questionnaire (PPQ)

End point description

Question 1 of the Patient Preference Questionnaire (PPQ) was as follows: “All things considered, which method of administration did you prefer?" The available options for a participant's response were IV, SC, or No preference. In Question 2 of the PPQ, participants who reported a preference for one of the two administration routes in Question 1 of the PPQ were asked to rate the strength of their preference (very strong, fairly strong, not very strong). The modified ITT (mITT) Population was analyzed; for Question 2 of the PPQ, the number analyzed for the strength of SC or IV preference represents the participants who indicated in their responses to Question 1 of the PPQ that they preferred the SC or IV route of administration, respectively.

End point type

Secondary

End point timeframe

Cycle 6 Day 1 (each cycle is 21 days)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV	All Participants
Number of subjects analysed	80	78	158
Units: Percentage of participants
number (not applicable)
SC Preference: Very Strong (n=70,66,136)	68.6	66.7	67.6
SC Preference: Fairly Strong (n=70,66,136)	24.3	25.8	25.0
SC Preference: Not Very Strong (n=70,66,136)	7.1	7.6	7.4
IV Preference: Very Strong (n=10,12,22)	40.0	66.7	54.5
IV Preference: Fairly Strong (n=10,12,22)	10.0	8.3	9.1
IV Preference: Not Very Strong (n=10,12,22)	50.0	25.0	36.4

No statistical analyses for this end point

Secondary: Percentage of Responses from Participants to the Two Main Reasons for Their Preferred Method of Pertuzumab and Trastuzumab Administration, as Assessed in Question 3 of the Patient Preference Questionnaire (PPQ)

Top of page

End point title

Percentage of Responses from Participants to the Two Main Reasons for Their Preferred Method of Pertuzumab and Trastuzumab Administration, as Assessed in Question 3 of the Patient Preference Questionnaire (PPQ)

End point description

In Question 3 of the PPQ, participants who reported a preference for one of the two administration routes in Question 1 of the PPQ were asked to provide the two main reasons for their preference. The five available options for a participant's response were: Feels less emotionally distressing; Requires less time in the clinic; Lower level of injection-site pain; Feels more comfortable during administration; and Other reason. The modified ITT (mITT) population was analyzed; for Question 3, the number analyzed for the two main reasons for SC or IV preference represents the participants who indicated in their responses to Question 1 of the PPQ that they preferred the SC or IV route of administration, respectively.

End point type

Secondary

End point timeframe

Cycle 6 Day 1 (each cycle is 21 days)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV	All Participants
Number of subjects analysed	80	78	158
Units: Percentage of responses
number (not applicable)
SC: Feels Less Emotionally Distressing	14.7	18.0	16.3
SC: Requires Less Time in the Clinic	42.0	42.4	42.2
SC: Lower Level of Injection-Site Pain	9.8	12.9	11.3
SC: Feels More Comfortable During Administration	28.7	23.0	25.9
SC: Other Reason	4.9	3.6	4.3
IV: Feels Less Emotionally Distressing	17.6	16.0	16.7
IV: Requires Less Time in the Clinic	5.9	4.0	4.8
IV: Lower Level of Injection-Site Pain	23.5	28.0	26.2
IV: Feels More Comfortable During Administration	47.1	24.0	33.3
IV: Other Reason	5.9	28.0	19.0

No statistical analyses for this end point

Secondary: Percentage of Participants by Their Level of Satisfaction with the Respective Methods of Administration (IV and SC), Question 1 of the Therapy Administration Satisfaction Questionnaire –Intravenous (TASQ-IV) and –Subcutaneous (TASQ-SC)

Top of page

End point title

Percentage of Participants by Their Level of Satisfaction with the Respective Methods of Administration (IV and SC), Question 1 of the Therapy Administration Satisfaction Questionnaire –Intravenous (TASQ-IV) and –Subcutaneous (TASQ-SC)

End point description

The Therapy Administration Satisfaction Questionnaire (TASQ) is a 12-item, patient-reported questionnaire measuring the impact of the mode of treatment administration (TASQ-IV for IV treatment and TASQ-SC for SC treatment) on five domains: Physical Impact, Psychological Impact, Impact on Activities of Daily Living, Convenience, and Satisfaction. The TASQ-IV/-SC was administered at treatment Cycles 3 and 6 according to the order of treatment received per arm during the Cross-Over Period. Question 1 of the TASQ-IV/TASQ-SC is one of two items in the Satisfaction domain, with participants providing their answers to the following question: "How satisfied or dissatisfied were you with the IV infusion/SC injection?" The five available options for a participant's response were: very satisfied, satisfied, neither satisfied nor dissatisfied, dissatisfied, and very dissatisfied. The modified Intent-to-Treat (mITT) population was analyzed.

End point type

Secondary

End point timeframe

Cycle 3 Day 1, Cycle 6 Day 1 (each cycle is 21 days)

End point values	All Participants: TASQ-IV Completers	All Participants: TASQ-SC Completers
Number of subjects analysed	160	160
Units: Participants
number (not applicable)
Very Satisfied	25.6	57.5
Satisfied	41.9	30.6
Neither Satisfied nor Dissatisfied	25.6	4.4
Dissatisfied	5.6	1.9
Very Dissatisfied	1.3	4.4
Did Not Answer Question	0.0	1.3

No statistical analyses for this end point

Secondary: Mean Scores of the Five Domains of the TASQ-IV and TASQ-SC (Satisfaction, Physical Impact, Psychological Impact, Impact on Activities of Daily Living, and Convenience) to Assess the Impact of IV and SC Routes of Administration

Top of page

End point title

Mean Scores of the Five Domains of the TASQ-IV and TASQ-SC (Satisfaction, Physical Impact, Psychological Impact, Impact on Activities of Daily Living, and Convenience) to Assess the Impact of IV and SC Routes of Administration

End point description

The TASQ is a 12-item, patient-reported questionnaire measuring the impact of the mode of treatment administration (TASQ-IV for IV treatment and TASQ-SC for SC treatment) on 5 domains: Physical Impact (3 items: Question [Q]2. Pain, Q3. Swelling, Q4. Redness), Psychological Impact (1 item: Q5. Feeling restricted), Impact on Activities of Daily Living (1 item: Q8. Lost/gained time), Convenience (2 items: Q6. Is it convenient?, Q7. Bothered by the amount of time?), and Satisfaction (2 items: Q1. How satisfied or dissatisfied are you with treatment?, Q12: Would you recommend the way you received the treatment?). In addition, 3 questions in the TASQ (Q9, Q10, Q11) are not part of the domains. Responses for the 3 domains that contain more than 1 item were scored from 0 to 100, with a higher score indicating a better outcome. Responses for the 2 domains with 1 item were scored from 1 to 5, with a higher score indicating a better outcome.

End point type

Secondary

End point timeframe

Cycle 3 Day 1, Cycle 6 Day 1 (each cycle is 21 days)

End point values	All Participants: TASQ-IV Completers	All Participants: TASQ-SC Completers
Number of subjects analysed	160	160
Units: Score on a scale
arithmetic mean (standard deviation)
Satisfaction Domain	64.3 ( 23.6 )	87.7 ( 17.5 )
Physical Impact Domain	86.5 ( 14.8 )	81.3 ( 15.4 )
Psychological Impact Domain	3.8 ( 1.2 )	4.6 ( 0.7 )
Impact on Activities Daily Living Domain	2.3 ( 0.9 )	3.9 ( 1.0 )
Convenience Domain	56.8 ( 26.0 )	90.0 ( 13.8 )

No statistical analyses for this end point

Secondary: Percentage of Participants by Their Responses to Question 9 of the TASQ-IV and TASQ-SC, Assessing Whether Participants Receiving IV and SC Administration Have as Much Time as They Would Like to Talk to Their Nurse and/or Doctor About Their Illness

Top of page

End point title

Percentage of Participants by Their Responses to Question 9 of the TASQ-IV and TASQ-SC, Assessing Whether Participants Receiving IV and SC Administration Have as Much Time as They Would Like to Talk to Their Nurse and/or Doctor About Their Illness

End point description

The TASQ is a 12-item, patient-reported questionnaire measuring the impact of the mode of treatment administration (TASQ-IV for IV treatment and TASQ-SC for SC treatment) on 5 domains. In addition, 3 questions (Q.9-11) are not part of the domains. The TASQ-IV/-SC was administered at treatment Cycles 3 and 6 according to the order of treatment received per arm during the Cross-Over Period. Question 9 asked the participant, "When you receive the IV infusion/SC injection treatment, are you able to talk to your nurse and/or doctor as much as you would like about your illness?" There were five available response options: a) Yes, I had more than enough time to talk to my nurse and/or doctor; b) Yes, but I would have liked more time to talk to my nurse and/or doctor; c) It does not matter to me if I have time to talk to my nurse and/or doctor during my treatment; d) No, I did not have enough time to talk to my nurse and/or doctor; and e) No, I did not talk to my nurse and/or doctor at all.

End point type

Secondary

End point timeframe

Cycle 3 Day 1 and Cycle 6 Day 1 (each cycle is 21 days)

End point values	All Participants: TASQ-IV Completers	All Participants: TASQ-SC Completers
Number of subjects analysed	160	160
Units: Percentage of participants
number (not applicable)
a) Yes, I had enough time to talk	82.5	90.0
b) Yes, but I would have liked more time to talk	9.4	5.0
c) It does not matter to me if I have time to talk	5.0	3.1
d) No, I did not have enough time to talk	0.6	0.6
e) No, I did not talk to my nurse/doctor	2.5	0.0
Patient did not answer question	0.0	1.3

No statistical analyses for this end point

Secondary: Percentage of Participants by Their Responses to Question 10 of the TASQ-IV and TASQ-SC, Assessing Whether IV and SC Administration Have an Impact on the Amount of Time Participants Have to Talk to Their Nurse and/or Doctor About Their Illness

Top of page

End point title

Percentage of Participants by Their Responses to Question 10 of the TASQ-IV and TASQ-SC, Assessing Whether IV and SC Administration Have an Impact on the Amount of Time Participants Have to Talk to Their Nurse and/or Doctor About Their Illness

End point description

The Therapy Administration Satisfaction Questionnaire (TASQ) is a 12-item, patient-reported questionnaire measuring the impact of the mode of treatment administration (TASQ-IV for IV treatment and TASQ-SC for SC treatment) on 5 domains (questions [Q] 1 to 8 and Q12): Physical Impact, Psychological Impact, Impact on Activities of Daily Living, Convenience, and Satisfaction. In addition, 3 questions in the TASQ-IV/-SC (Q 9-11) are not part of the domains. The TASQ-IV/-SC were administered at treatment Cycles 3 and 6 according to the order of treatment received in each study arm during the Cross-Over Period. Question 10 of the TASQ-IV/-SC asked the participant "Does the IV infusion/SC injection impact the amount of time you have to talk to your nurse and/or doctor about your illness and other concerns?" There were two available options for the participant's response: Yes or No.

End point type

Secondary

End point timeframe

Cycle 3 Day 1 and Cycle 6 Day 1 (each cycle is 21 days)

End point values	All Participants: TASQ-IV Completers	All Participants: TASQ-SC Completers
Number of subjects analysed	160	160
Units: Percentage of participants
number (not applicable)
Yes	20.0	13.1
No	79.4	85.0
Patient Did Not Answer Question	0.6	1.9

No statistical analyses for this end point

Secondary: Percentage of Participants by Their Responses to Question 11 of the TASQ-IV and TASQ-SC, Assessing the Participants' Preferred Method for Receiving Cancer Treatment

Top of page

End point title

Percentage of Participants by Their Responses to Question 11 of the TASQ-IV and TASQ-SC, Assessing the Participants' Preferred Method for Receiving Cancer Treatment

End point description

The Therapy Administration Satisfaction Questionnaire (TASQ) is a 12-item, patient-reported questionnaire measuring the impact of the mode of treatment administration (TASQ-IV for IV treatment and TASQ-SC for SC treatment) on 5 domains (questions [Q] 1 to 8 and Q12): Physical Impact, Psychological Impact, Impact on Activities of Daily Living, Convenience, and Satisfaction. In addition, 3 questions in the TASQ-IV/-SC (Q 9-11) are not part of the domains. The TASQ-IV/-SC was administered at treatment Cycles 3 and 6 according to the order of treatment received during the Cross-Over Period. Question 11 of the TASQ-IV/-SC asked the participant, "There are two ways to get cancer treatment: a) IV infusion given through a port or small tube; b) SC (subcutaneous) injection in your thigh. Which would you prefer?" There were three available options for the participant's response: IV, SC, or No Preference.

End point type

Secondary

End point timeframe

Cycle 3 Day 1 and Cycle 6 Day 1 (each cycle is 21 days)

End point values	All Participants: TASQ-IV Completers	All Participants: TASQ-SC Completers
Number of subjects analysed	160	160
Units: Percentage of participants
number (not applicable)
Prefer IV Method	11.9	9.4
Prefer SC Method	70.6	82.5
No Preference	11.9	5.6
Patient Did Not Answer Question	5.6	2.5

No statistical analyses for this end point

Secondary: Percentage of Participants by Their Choice of Treatment in the Treatment Continuation Period (PH FDC SC or P+H IV) and by Consistency of This Choice with Their Preferred Method of Administration Reported in Question 1 of the PPQ

Top of page

End point title

Percentage of Participants by Their Choice of Treatment in the Treatment Continuation Period (PH FDC SC or P+H IV) and by Consistency of This Choice with Their Preferred Method of Administration Reported in Question 1 of the PPQ

End point description

At treatment Cycle 7, participants were expected to select the study treatment formulation (PH FDC SC or P+H IV) to complete their 18 cycles of neo/adjuvant HER2-targeted treatment after completion of the Treatment Cross-over Period. Additionally, for each participant’s preference category (SC, IV, and No preference) as per the question 1 of the patient preference questionnaire (PPQ), the percentage of participants who selected each treatment administration route for the Treatment Continuation Period (PH FDC SC or P+H IV) was summarized.

End point type

Secondary

End point timeframe

Cycle 7 Day 1 (each cycle is 21 days)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV	All Participants
Number of subjects analysed	80	80	160
Units: Percentage of participants
number (not applicable)
Chose SC for Treatment Continuation	88.8	85.0	86.9
Chose IV for Treatment Continuation	11.3	15.0	13.1
Preferred SC per PPQ & Chose SC for Continuation	87.5	82.5	85.0
Preferred SC per PPQ & Chose IV for Continuation	0.0	0.0	0.0
Preferred IV per PPQ & Chose SC for Continuation	1.3	0.0	0.6
Preferred IV per PPQ & Chose IV for Continuation	11.3	15.0	13.1
No Preference per PPQ & Chose SC for Continuation	0.0	2.5	1.3
No Preference per PPQ & Chose IV for Continuation	0.0	0.0	0.0

No statistical analyses for this end point

Secondary: Duration of Treatment Administration Activities According to Healthcare Professionals' Responses on Perception of Time by Treatment Cycle, Question 1 of the Healthcare Professional Questionnaire (HCPQ) - Treatment Room

Top of page

End point title

Duration of Treatment Administration Activities According to Healthcare Professionals' Responses on Perception of Time by Treatment Cycle, Question 1 of the Healthcare Professional Questionnaire (HCPQ) - Treatment Room

End point description

The Healthcare Professional Questionnaire (HCPQ)-Treatment Room Question 1 was completed at each treatment cycle of the Treatment Cross-Over Period by the healthcare professionals (HCPs) who administered treatment to the study's participants. HCPs responded to the following parts of Question 1 that sought to evaluate the amount of time it took to complete activities related to treatment administration: "If new IV access was needed for this cycle of treatment, please indicate what type of IV access was provided (central venous catheter [CVC], peripherally inserted central catheter [PICC], or peripheral vein cannulation [PVC]) and how long (in minutes) this took to set up (only for participants receiving IV treatment)? How long (in minutes) did it take to administer the treatment, i.e. total infusion duration? How long (in minutes) was the patient in the Treatment Room for in total?" The value '999999' indicates 0 participants were analyzed.

End point type

Secondary

End point timeframe

Day 1 of Cycles (Cyc) 1-6 (each cycle is 21 days)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	80	80
Units: minutes
median (full range (min-max))
Cyc 1. Time for CVC Set Up (IV Only; n=4,0)	5.0 (4 to 6)	999999 (999999 to 999999)
Cyc 1. Time for PICC Set Up (IV Only; n=1,0)	5.0 (5 to 5)	999999 (999999 to 999999)
Cyc 1. Time for PVC Set Up (IV Only; n=50,0)	5.0 (1 to 40)	999999 (999999 to 999999)
Cyc 1. Time Taken to Administer Treatment(n=79,79)	150.0 (60 to 396)	8.0 (2 to 17)
Cyc 1. Time Patient Was in Treatment Room(n=79,79)	300.0 (90 to 450)	50.0 (8 to 240)
Cyc 2. Time for CVC Set Up (IV Only; n=4,0)	5.0 (3 to 5)	999999 (999999 to 999999)
Cyc 2. Time for PICC Set Up (IV Only; n=1,0)	3.0 (3 to 3)	999999 (999999 to 999999)
Cyc 2. Time for PVC Set Up (IV Only; n=48,0)	5.0 (1 to 20)	999999 (999999 to 999999)
Cyc 2. Time Taken to Administer Treatment(n=77,80)	90.0 (8 to 260)	8.0 (5 to 20)
Cyc 2. Time Patient Was in Treatment Room(n=77,78)	153.0 (30 to 342)	40.0 (8 to 225)
Cyc 3. Time for CVC Set Up (IV Only; n=5,0)	5.0 (3 to 10)	999999 (999999 to 999999)
Cyc 3. Time for PICC Set Up (IV Only; n=1,0)	3.0 (3 to 3)	999999 (999999 to 999999)
Cyc 3. Time for PVC Set Up (IV Only; n=48,0)	5.0 (1 to 30)	999999 (999999 to 999999)
Cyc 3. Time Taken to Administer Treatment(n=79,80)	70.0 (30 to 240)	7.5 (4 to 16)
Cyc 3. Time Patient Was in Treatment Room(n=79,79)	150.0 (105 to 330)	36.0 (5 to 327)
Cyc 4. Time for CVC Set Up (IV Only; n=0,7)	999999 (999999 to 999999)	5.0 (2 to 10)
Cyc 4. Time for PICC Set Up (IV Only; n=0,1)	999999 (999999 to 999999)	42.0 (42 to 42)
Cyc 4. Time for PVC Set Up (IV Only; n=0,36)	999999 (999999 to 999999)	5.0 (1 to 20)
Cyc 4. Time Taken to Administer Treatment(n=80,77)	8.0 (4 to 12)	60.0 (30 to 210)
Cyc 4. Time Patient Was in Treatment Room(n=78,77)	45.0 (1 to 185)	150.0 (80 to 480)
Cyc 5. Time for CVC Set Up (IV Only; n=0,5)	999999 (999999 to 999999)	3.0 (2 to 10)
Cyc 5. Time for PICC Set Up (IV Only; n=0,1)	999999 (999999 to 999999)	10.0 (10 to 10)
Cyc 5. Time for PVC Set Up (IV Only; n=0,38)	999999 (999999 to 999999)	5.0 (1 to 20)
Cyc 5. Time Taken to Administer Treatment(n=79,77)	8.0 (3 to 14)	83.0 (30 to 200)
Cyc 5. Time Patient Was in Treatment Room(n=79,77)	33.0 (8 to 135)	150.0 (95 to 343)
Cyc 6. Time for CVC Set Up (IV Only; n=0,6)	999999 (999999 to 999999)	10.0 (1 to 91)
Cyc 6. Time for PICC Set Up (IV Only; n=0,0)	999999 (999999 to 999999)	999999 (999999 to 999999)
Cyc 6. Time for PVC Set Up (IV Only; n=0,43)	999999 (999999 to 999999)	5.0 (1 to 60)
Cyc 6. Time Taken to Administer Treatment(n=79,80)	7.0 (3 to 11)	60.0 (5 to 275)
Cyc 6. Time Patient Was in Treatment Room(n=79,80)	35.0 (10 to 150)	130.0 (45 to 330)

No statistical analyses for this end point

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Impact of PH FDC SC on Clinical Management and Clinical Efficiency, Question 2 of the HCPQ - Treatment Room

Top of page

End point title

Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Impact of PH FDC SC on Clinical Management and Clinical Efficiency, Question 2 of the HCPQ - Treatment Room

End point description

HCPs who administered study treatment responded at Cycle 6 of the Treatment Cross-Over Period to the following HCPQ-Treatment Room Question 2: "If all P+H IV infusions are switched to FDC SC injections, please indicate how strongly you agree or disagree with each of the following statements: a) Patients will be moved outside of infusion unit to receive FDC SC; b) FDC SC route will allow more flexible scheduling; c) More patients will be treated in the infusion unit; d) Waiting list for any P+H IV treatment at the infusion unit will be reduced; e) Staff resources will be redistributed to other departments of the hospital; f) There will still be sufficient interaction time between HCPs and patients; g) Staff will spend more time for further education/development; h) Staff will dedicate more time attending to administrative tasks for Perjeta-Herceptin patients; i) Patients will spend less time in the care unit; j) Administration by FDC SC injection is preferred by patients."

End point type

Secondary

End point timeframe

Day 1 of Cycle 6 (each cycle is 21 days)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV	All Healthcare Professionals
Number of subjects analysed	79	80	159
Units: Percentage of HCPs
number (not applicable)
Statement a): Strongly Disagree	11.4	21.3	16.4
Statement a): Disagree	12.7	17.5	15.1
Statement a): Neutral	8.9	3.8	6.3
Statement a): Agree	26.6	16.3	21.4
Statement a): Strongly Agree	22.8	22.5	22.6
Statement a): Not Applicable	13.9	11.3	12.6
Statement a): Answer Missing	3.8	7.5	5.7
Statement b): Strongly Disagree	0.0	6.3	3.1
Statement b): Disagree	7.6	10.0	8.8
Statement b): Neutral	10.1	7.5	8.8
Statement b): Agree	29.1	27.5	28.3
Statement b): Strongly Agree	49.4	41.3	45.3
Statement b): Not Applicable	0.0	0.0	0.0
Statement b): Answer Missing	3.8	7.5	5.7
Statement c): Strongly Disagree	1.3	3.8	2.5
Statement c): Disagree	7.6	7.5	7.5
Statement c): Neutral	17.7	12.5	15.1
Statement c): Agree	29.1	31.3	30.2
Statement c): Strongly Agree	36.7	37.5	37.1
Statement c): Not Applicable	3.8	0.0	1.9
Statement c): Answer Missing	3.8	7.5	5.7
Statement d): Strongly Disagree	1.3	7.5	4.4
Statement d): Disagree	8.9	7.5	8.2
Statement d): Neutral	17.7	11.3	14.5
Statement d): Agree	29.1	26.3	27.7
Statement d): Strongly Agree	36.7	33.8	35.2
Statement d): Not Applicable	2.5	5.0	3.8
Statement d): Answer Missing	3.8	8.8	6.3
Statement e): Strongly Disagree	15.2	10.0	12.6
Statement e): Disagree	16.5	22.5	19.5
Statement e): Neutral	17.7	22.5	20.1
Statement e): Agree	19.0	11.3	15.1
Statement e): Strongly Agree	20.3	18.8	19.5
Statement e): Not Applicable	7.6	6.3	6.9
Statement e): Answer Missing	3.8	8.8	6.3
Statement f): Strongly Disagree	0.0	3.8	1.9
Statement f): Disagree	6.3	3.8	5.0
Statement f): Neutral	15.2	16.3	15.7
Statement f): Agree	31.6	32.5	32.1
Statement f): Strongly Agree	43.0	35.0	39.0
Statement f): Not Applicable	0.0	0.0	0.0
Statement f): Answer Missing	3.8	8.8	6.3
Statement g): Strongly Disagree	0.0	5.0	2.5
Statement g): Disagree	7.6	11.3	9.4
Statement g): Neutral	31.6	23.8	27.7
Statement g): Agree	20.3	22.5	21.4
Statement g): Strongly Agree	35.4	27.5	31.4
Statement g): Not Applicable	1.3	2.5	1.9
Statement g): Answer Missing	3.8	7.5	5.7
Statement h): Strongly Disagree	1.3	5.0	3.1
Statement h): Disagree	11.4	16.3	13.8
Statement h): Neutral	25.3	23.8	24.5
Statement h): Agree	24.1	16.3	20.1
Statement h): Strongly Agree	32.9	27.5	30.2
Statement h): Not Applicable	1.3	3.8	2.5
Statement h): Answer Missing	3.8	7.5	5.7
Statement i): Strongly Disagree	0.0	0.0	0.0
Statement i): Disagree	6.3	3.8	5.0
Statement i): Neutral	1.3	5.0	3.1
Statement i): Agree	27.8	22.5	25.2
Statement i): Strongly Agree	60.8	60.0	60.4
Statement i): Not Applicable	0.0	0.0	0.0
Statement i): Answer Missing	3.8	8.8	6.3
Statement j): Strongly Disagree	0.0	0.0	0.0
Statement j): Disagree	8.9	1.3	5.0
Statement j): Neutral	10.1	15.0	12.6
Statement j): Agree	22.8	26.3	24.5
Statement j): Strongly Agree	53.2	47.5	50.3
Statement j): Not Applicable	1.3	1.3	1.3
Statement j): Answer Missing	3.8	8.8	6.3

No statistical analyses for this end point

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Time/Resource Use and Convenience of Each Study Regimen, Questions 3 to 7 of the HCPQ - Treatment Room

Top of page

End point title

Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Time/Resource Use and Convenience of Each Study Regimen, Questions 3 to 7 of the HCPQ - Treatment Room

End point description

Healthcare professionals (HCPs) who administered study treatment responded at Cycle 6 of the Treatment Cross-Over Period to the following HCPQ-Treatment Room Questions (Q) 3 to 7: "Looking back over the Perjeta-Herceptin treatment sessions, please indicate based on your opinion which administration method: Q3. Which Method Was Most Convenient for the Patient? Q4. Which Method Was Best for Optimizing Patient Care in Your Centre? Q5. Which Method Took the Least Time from Start to Finish of Administration? Q6. Which Method Required the Least Resource Use for Administration? Q7. Which Method Was Preferred by Patients?" The four available response options were: P+H IV, FDC SC, No Difference, and Unsure.

End point type

Secondary

End point timeframe

Day 1 of Cycle 6 (each cycle is 21 days)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV	All Healthcare Professionals
Number of subjects analysed	79	80	159
Units: Percentage of HCPs
number (not applicable)
Q3. Answer: FDC SC	88.6	85.0	86.8
Q3. Answer: P+H IV	6.3	1.3	3.8
Q3. Answer: No Difference	2.5	5.0	3.8
Q3. Answer: Unsure	0.0	7.5	3.8
Q3. Answer: Missing	2.5	1.3	1.9
Q4. Answer: FDC SC	79.7	78.8	79.2
Q4. Answer: P+H IV	3.8	1.3	2.5
Q4. Answer: No Difference	12.7	12.5	12.6
Q4. Answer: Unsure	1.3	6.3	3.8
Q4. Answer: Missing	2.5	1.3	1.9
Q5. Answer: FDC SC	94.9	96.3	95.6
Q5. Answer: P+H IV	0.0	0.0	0.0
Q5. Answer: No Difference	2.5	2.5	2.5
Q5. Answer: Unsure	0.0	0.0	0.0
Q5. Answer: Missing	2.5	1.3	1.9
Q6. Answer: FDC SC	83.5	88.8	86.2
Q6. Answer: P+H IV	0.0	1.3	0.6
Q6. Answer: No Difference	13.9	8.8	11.3
Q6. Answer: Unsure	0.0	0.0	0.0
Q6. Answer: Missing	2.5	1.3	1.9
Q7. Answer: FDC SC	77.2	77.5	77.4
Q7. Answer: P+H IV	7.6	5.0	6.3
Q7. Answer: No Difference	2.5	2.5	2.5
Q7. Answer: Unsure	10.1	13.8	11.9
Q7. Answer: Missing	2.5	1.3	1.9

No statistical analyses for this end point

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses to Question 8 of the HCPQ - Treatment Room

Top of page

End point title

Percentage of Healthcare Professionals (HCPs) by Their Responses to Question 8 of the HCPQ - Treatment Room

End point description

Healthcare professionals (HCPs) who administered study treatment responded at Cycle 6 of the Treatment Cross-Over Period to the following HCPQ-Treatment Room Question 8: "How frequently would you offer or recommend FDC SC administration to your patients in the future?" The three available response options were: Always, Sometimes, and Never.

End point type

Secondary

End point timeframe

Day 1 of Cycle 6 (each cycle is 21 days)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV	All Healthcare Professionals
Number of subjects analysed	79	80	159
Units: Percentage of HCPs
number (not applicable)
Always	69.6	65.0	67.3
Sometimes	26.6	33.8	30.2
Never	1.3	0.0	0.6
Missing	2.5	1.3	1.9

No statistical analyses for this end point

Secondary: Duration of Treatment Preparation According to Healthcare Professionals' Responses on Perception of Time by Treatment Cycle, Question 1 of the HCPQ - Drug Preparation Room

Top of page

End point title

Duration of Treatment Preparation According to Healthcare Professionals' Responses on Perception of Time by Treatment Cycle, Question 1 of the HCPQ - Drug Preparation Room

End point description

The Healthcare Professional Questionnaire (HCPQ)-Drug Preparation Room Question 1 was completed at each treatment cycle of the Treatment Cross-Over Period by the healthcare professionals (HCPs) within the pharmacy/drug preparation area where pertuzumab IV and trastuzumab IV and pertuzumab and trastuzumab FDC SC were prepared and dispensed for treating the study's participants. HCPs responded to the following question: "How long (in minutes) did it take to prepare the treatment for use?"

End point type

Secondary

End point timeframe

Day 1 of Cycles 1-6 (each cycle is 21 days)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	80	80
Units: minutes
median (full range (min-max))
Cycle 1 (n = 80, 79)	20.0 (3 to 60)	5.0 (1 to 50)
Cycle 2 (n = 79, 80)	20.0 (3 to 60)	5.0 (1 to 30)
Cycle 3 (n = 80, 79)	17.5 (3 to 90)	5.0 (1 to 40)
Cycle 4 (n = 80, 80)	5.0 (1 to 30)	15.0 (3 to 49)
Cycle 5 (n = 80, 79)	5.0 (1 to 35)	15.0 (3 to 50)
Cycle 6 (n = 80, 78)	5.0 (1 to 40)	15.0 (3 to 50)

No statistical analyses for this end point

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Impact of PH FDC SC on Clinical Management and Clinical Efficiency, Question 2 of the HCPQ - Drug Preparation Room

Top of page

End point title

Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Impact of PH FDC SC on Clinical Management and Clinical Efficiency, Question 2 of the HCPQ - Drug Preparation Room

End point description

Healthcare professionals (HCPs) who prepared study treatment within the pharmacy/drug preparation area responded at Cycle 6 of the Treatment Cross-Over Period to the following HCPQ-Drug Preparation Room Question 2: "If all P+H IV infusions are switched to FDC SC injections, please indicate how strongly you agree or disagree with each of the following statements: a) Staff will have increased availability for other tasks in the pharmacy; b) Administrative procedures around FDC SC will require less time; c) FDC SC formulations will provide more flexibility for staff in managing their workload; d) Due to ready-to-use FDC SC formulations, potential dosing errors will be avoided; e) Due to ready-to-use FDC SC formulations, there will be less drug wastage; f) Without having to reconstitute the drug, less storage space for FDC SC related supplies will be required in the pharmacy; g) Preparation procedures and associated time staff time commitment will be reduced."

End point type

Secondary

End point timeframe

Day 1 of Cycle 6 (each cycle is 21 days)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV	All Healthcare Professionals
Number of subjects analysed	80	80	160
Units: Percentage of HCPs
number (not applicable)
Statement a): Strongly Disagree	1.3	1.3	1.3
Statement a): Disagree	1.3	0.0	0.6
Statement a): Neutral	8.8	6.3	7.5
Statement a): Agree	28.8	28.8	28.8
Statement a): Strongly Agree	52.5	48.8	50.6
Statement a): Not Applicable	3.8	1.3	2.5
Statement a): Answer Missing	3.8	13.8	8.8
Statement b): Strongly Disagree	8.8	2.5	5.6
Statement b): Disagree	3.8	3.8	3.8
Statement b): Neutral	16.3	12.5	14.4
Statement b): Agree	17.5	18.8	18.1
Statement b): Strongly Agree	46.3	46.3	46.3
Statement b): Not Applicable	2.5	2.5	2.5
Statement b): Answer Missing	5.0	13.8	9.4
Statement c): Strongly Disagree	0.0	1.3	0.6
Statement c): Disagree	0.0	1.3	0.6
Statement c): Neutral	15.0	11.3	13.1
Statement c): Agree	28.8	23.8	26.3
Statement c): Strongly Agree	50.0	47.5	48.8
Statement c): Not Applicable	1.3	1.3	1.3
Statement c): Answer Missing	5.0	6.3	9.4
Statement d): Strongly Disagree	1.3	1.3	1.3
Statement d): Disagree	1.3	6.3	3.8
Statement d): Neutral	5.0	6.3	5.6
Statement d): Agree	26.3	20.0	23.1
Statement d): Strongly Agree	60.0	52.5	56.3
Statement d): Not Applicable	1.3	1.3	1.3
Statement d): Answer Missing	5.0	12.5	8.8
Statement e): Strongly Disagree	1.3	1.3	1.3
Statement e): Disagree	1.3	2.5	1.9
Statement e): Neutral	11.3	6.3	8.8
Statement e): Agree	21.3	22.5	21.9
Statement e): Strongly Agree	58.8	51.3	55.0
Statement e): Not Applicable	1.3	2.5	1.9
Statement e): Answer Missing	5.0	13.8	9.4
Statement f): Strongly Disagree	0.0	1.3	0.6
Statement f): Disagree	3.8	5.0	4.4
Statement f): Neutral	16.3	7.5	11.9
Statement f): Agree	20.0	28.8	24.4
Statement f): Strongly Agree	53.8	42.5	48.1
Statement f): Not Applicable	1.3	1.3	1.3
Statement f): Answer Missing	5.0	13.8	9.4
Statement g): Strongly Disagree	0.0	1.3	0.6
Statement g): Disagree	0.0	0.0	0.0
Statement g): Neutral	8.8	5.0	6.9
Statement g): Agree	30.0	32.5	31.3
Statement g): Strongly Agree	52.5	45.0	48.8
Statement g): Not Applicable	3.8	2.5	3.1
Statement g): Answer Missing	5.0	13.8	9.4

No statistical analyses for this end point

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Time/Resource Use of Each Study Regimen, Questions 3 and 4 of the HCPQ - Drug Preparation Room

Top of page

End point title

Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Time/Resource Use of Each Study Regimen, Questions 3 and 4 of the HCPQ - Drug Preparation Room

End point description

Healthcare professionals (HCPs) who prepared study treatment within the pharmacy/drug preparation area responded at Cycle 6 of the Treatment Cross-Over Period to the following HCPQ-Drug Preparation Room Questions 3 and 4: "Looking back over the Perjeta-Herceptin treatment sessions, please indicate based on your opinion which administration method: Q3. Was quickest from start to end of preparation to finish of administration (excluding observation period)?; Q4. Required less resource use for preparation and administration, for example nursing time, facility costs, equipment etc?" The three available response options were: P+H IV, FDC SC, and No Difference.

End point type

Secondary

End point timeframe

Day 1 of Cycle 6 (each cycle is 21 days)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV	All Healthcare Professionals
Number of subjects analysed	80	80	160
Units: Percentage of HCPs
number (not applicable)
Q3. Answer: FDC SC	92.5	82.5	87.5
Q3. Answer: P+H IV	0.0	1.3	0.6
Q3. Answer: No Difference	1.3	1.3	1.3
Q3. Answer: Missing	6.3	15.0	10.6
Q4. Answer: FDC SC	93.8	80.0	86.9
Q4. Answer: P+H IV	0.0	0.0	0.0
Q4. Answer: No Difference	0.0	5.0	2.5
Q4. Answer: Missing	6.3	15.0	10.6

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in Health-Related Quality of Life (HRQoL) as Assessed by the Global Health Status/QoL Scale Score of the the European Organization for Research and Treatment of Cancer Quality of Life Questionnaire 30 (EORTC QLQ-C30)

Top of page

End point title

Change From Baseline Over Time in Health-Related Quality of Life (HRQoL) as Assessed by the Global Health Status/QoL Scale Score of the the European Organization for Research and Treatment of Cancer Quality of Life Questionnaire 30 (EORTC QLQ-C30)

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[2]	0 ^[3]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[2] - Results are not reported at this time because data collection is ongoing.
[3] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Physical Functioning Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Physical Functioning Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[4]	0 ^[5]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[4] - Results are not reported at this time because data collection is ongoing.
[5] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Role Functioning Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Role Functioning Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[6]	0 ^[7]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[6] - Results are not reported at this time because data collection is ongoing.
[7] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Emotional Functioning Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Emotional Functioning Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[8]	0 ^[9]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[8] - Results are not reported at this time because data collection is ongoing.
[9] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Cognitive Functioning Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Cognitive Functioning Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[10]	0 ^[11]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[10] - Results are not reported at this time because data collection is ongoing.
[11] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Social Functioning Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Social Functioning Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[12]	0 ^[13]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[12] - Results are not reported at this time because data collection is ongoing.
[13] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Fatigue Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Fatigue Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[14]	0 ^[15]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[14] - Results are not reported at this time because data collection is ongoing.
[15] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Nausea and Vomiting Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Nausea and Vomiting Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[16]	0 ^[17]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[16] - Results are not reported at this time because data collection is ongoing.
[17] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Pain Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Pain Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[18]	0 ^[19]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[18] - Results are not reported at this time because data collection is ongoing.
[19] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Dyspnoea Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Dyspnoea Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[20]	0 ^[21]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[20] - Results are not reported at this time because data collection is ongoing.
[21] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Insomnia Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Insomnia Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[22]	0 ^[23]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[22] - Results are not reported at this time because data collection is ongoing.
[23] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Appetite Loss Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Appetite Loss Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[24]	0 ^[25]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[24] - Results are not reported at this time because data collection is ongoing.
[25] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Constipation Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Constipation Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[26]	0 ^[27]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[26] - Results are not reported at this time because data collection is ongoing.
[27] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Diarrhoea Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Diarrhoea Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[28]	0 ^[29]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[28] - Results are not reported at this time because data collection is ongoing.
[29] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Change From Baseline Over Time in the Financial Difficulties Scale Score of the EORTC QLQ-C30

Top of page

End point title

Change From Baseline Over Time in the Financial Difficulties Scale Score of the EORTC QLQ-C30

End point description

End point type

Secondary

End point timeframe

Baseline (Day 1 of Cycle 1); Day 1 of Cycles 3, 6, and 15 (or last treatment cycle; each cycle is 21 days); 1.5, 2, and 3 years (up to 3 years)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[30]	0 ^[31]
Units: Score on a scale
arithmetic mean (standard deviation)	( )	( )

Notes
[30] - Results are not reported at this time because data collection is ongoing.
[31] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Safety Summary for Assessment of Switching Between the FDC SC and IV Formulations: Number of Participants with at Least One Adverse Event During the Treatment Cross-Over Period by Treatment Arm and Treatment Received

Top of page

End point title

Safety Summary for Assessment of Switching Between the FDC SC and IV Formulations: Number of Participants with at Least One Adverse Event During the Treatment Cross-Over Period by Treatment Arm and Treatment Received

End point description

Investigators used the NCI CTCAE v4.0 grading scale for assessing adverse event (AE) severity; if not listed, AE severity was graded as follows: Grade 1 = mild; Grade 2 = moderate; Grade 3 = severe or medically significant; Grade 4 = life-threatening; Grade 5 = death related to AE. Severity and seriousness are not synonymous and investigators independently assessed these criteria for each AE. Investigators also determined whether an AE was considered to be related to the study drug. Adverse events to monitor were defined based on known risks associated with the study drugs and included: hypersensitivity reactions, administration-related reactions (ARRs), cardiac dysfunction, diarrhea grade ≥3, rash/skin reactions, mucositis, interstitial lung disease (ILD), (febrile) neutropenia, pulmonary events that may occur as a result of an ARR, and pregnancy/neonatal related. Multiple occurrences of AEs were counted only once per participant. LVEF = left ventricular ejection fraction

End point type

Secondary

End point timeframe

From Day 1 of Cycle 1 to the end of Cycle 3 of Cross-Over Period; from Day 1 of Cycle 4 to the end of Cycle 6 of Cross-Over Period (1 cycle is 21 days)

End point values	Arm A: Treatment With P+H IV (Cycles 1–3)	Arm A: Treatment With PH FDC SC (Cycles 4–6)	Arm B: Treatment With PH FDC SC (Cycles 1–3)	Arm B: Treatment With P+H IV (Cycles 4–6)
Number of subjects analysed	80	80	80	80
Units: Participants
Any Adverse Event (AE)	62	58	62	51
AE with Fatal Outcome	0	0	0	0
Related AE with Fatal Outcome	0	0	0	0
Grade 3 to 5 AE	2	1	3	4
Related Grade 3 to 5 AE	1	0	1	0
Cardiac AE (Including LVEF Events)	1	2	3	2
Serious AE	1	1	1	5
Anaphylaxis and Hypersensitivity AE, All Grades	0	2	1	0
Anaphylaxis and Hypersensitivity AE, Grade ≥3	0	0	0	0
Administration Related Reaction (ARR), All Grades	7	14	23	2
Administration Related Reaction (ARR), Grade ≥3	0	0	0	0
Cardiac Dysfunction AE, All Grades	2	1	3	3
Cardiac Dysfunction AE, Grade ≥3	1	0	0	0
Diarrhea Grade ≥3	0	0	1	0
Rash/Skin Reactions	0	0	0	0
Mucositis	0	0	0	0
Pulmonary Events (ARR), All Grades	18	7	4	7
Pulmonary Events (ARR), Grade ≥3	0	0	1	0
Pregnancy and Neonatal Related AEs, All Grades	0	0	1	0
Pregnancy and Neonatal Related AEs, Grade ≥3	0	0	0	0
Interstitial Lung Disease (ILD)	0	0	0	0
Neutropenia/Febrile Neutropenia, All Grades	4	1	2	4
Neutropenia/Febrile Neutropenia, Grade ≥3	1	0	0	0
Local Infusion Site Reaction	1	0	0	0
Systemic Infusion Site Reaction	5	0	0	1
Local Injection Site Reaction	0	12	24	0
Systemic Injection Site Reaction	0	2	1	0
AE Leading to Any Study Treatment Discontinuation	0	1	0	0
AE Leading to PH FDC SC Discontinuation	0	1	0	0
AE Leading to Pertuzumab IV Discontinuation	0	0	0	0
AE Leading to Trastuzumab IV Discontinuation	0	0	0	0
AE Leading to Any Study Trx Interrupt./Dose Reduc.	1	0	2	2

No statistical analyses for this end point

Secondary: Safety Summary of the FDC SC and IV Formulations: Number of Participants with at Least One Adverse Event During the Cross-Over and Continuation Treatment Periods

Top of page

End point title

Safety Summary of the FDC SC and IV Formulations: Number of Participants with at Least One Adverse Event During the Cross-Over and Continuation Treatment Periods

End point description

End point type

Secondary

End point timeframe

From Day 1 of Cycle 1 of the Cross-Over Period up to the completion of 18 cycles of neo/adjuvant anti-HER2 treatment in the Continuation Period (1 cycle is 21 days)

End point values	P+H IV: Treatment Cross-Over Period	PH FDC SC: Treatment Cross-Over Period	P+H IV: Treatment Continuation Period	PH FDC SC: Treatment Continuation Period
Number of subjects analysed	160	160	21	137
Units: Participants
Any Adverse Event (AE)	113	120	13	70
AE with Fatal Outcome	0	0	0	0
Related AE with Fatal Outcome	0	0	0	0
Grade 3 to 5 AE	6	4	2	4
Related Grade 3 to 5 AE	1	1	0	0
Cardiac AE (Including LVEF Events)	3	5	0	1
Serious AE	6	2	0	3
Anaphylaxis and Hypersensitivity AE, All Grades	0	3	0	2
Anaphylaxis and Hypersensitivity AE, Grade ≥3	0	0	0	0
Administration Related Reaction (ARR), All Grades	9	38	0	13
Administration Related Reaction (ARR), Grade ≥3	0	0	0	0
Cardiac Dysfunction AE, All Grades	5	4	0	3
Cardiac Dysfunction AE, Grade ≥3	1	0	0	0
Diarrhea Grade ≥3	0	1	0	0
Rash/Skin Reactions	0	0	0	0
Mucositis	0	0	0	0
Pulmonary Events (ARR), All Grades	25	11	3	11
Pulmonary Events (ARR), Grade ≥3	0	1	0	0
Pregnancy and Neonatal Related AEs, All Grades	0	1	0	0
Pregnancy and Neonatal Related AEs, Grade ≥3	0	0	0	0
Interstitial Lung Disease (ILD), All Grades	0	0	0	1
Interstitial Lung Disease (ILD), Grade ≥3	0	0	0	0
Neutropenia/Febrile Neutropenia, All Grades	8	3	0	3
Neutropenia/Febrile Neutropenia, Grade ≥3	1	0	0	1
Local Infusion Site Reaction	1	0	0	0
Systemic Infusion Site Reaction	6	0	0	0
Local Injection Site Reaction	0	36	0	10
Systemic Injection Site Reaction	0	3	0	2
AE Leading to Any Study Treatment Discontinuation	0	1	1	0
AE Leading to PH FDC SC Discontinuation	0	1	0	0
AE Leading to Pertuzumab IV Discontinuation	0	0	1	0
AE Leading to Trastuzumab IV Discontinuation	0	0	1	0
AE Leading to Any Study Trx Interrupt./Dose Reduc.	3	2	1	3

No statistical analyses for this end point

Secondary: Number of Participants with at Least One Event of Heart Failure with the FDC SC and IV Formulations During the Cross-Over and Continuation Treatment Periods

Top of page

End point title

Number of Participants with at Least One Event of Heart Failure with the FDC SC and IV Formulations During the Cross-Over and Continuation Treatment Periods

End point description

Heart failure is defined as a disorder characterized by the inability of the heart to pump blood at an adequate volume to meet tissue metabolic requirements, or, the ability to do only at an elevation in the filling pressure. Any adverse event of symptomatic left ventricular systolic dysfunction (LVSD; also referred to as heart failure) occurring during the study was to be reported as a serious adverse event.

End point type

Secondary

End point timeframe

From Day 1 of Cycle 1 of the Cross-Over Period up to the completion of 18 cycles of neo/adjuvant anti-HER2 treatment in the Continuation Period (1 cycle is 21 days)

End point values	P+H IV: Treatment Cross-Over Period	PH FDC SC: Treatment Cross-Over Period	P+H IV: Treatment Continuation Period	PH FDC SC: Treatment Continuation Period
Number of subjects analysed	160	160	21	137
Units: Participants	0	0	0	0

No statistical analyses for this end point

Secondary: Number of Participants with at Least One Event of Ejection Fraction Decreased with the FDC SC and IV Formulations During the Cross-Over and Continuation Treatment Periods

Top of page

End point title

Number of Participants with at Least One Event of Ejection Fraction Decreased with the FDC SC and IV Formulations During the Cross-Over and Continuation Treatment Periods

End point description

Left ventricular ejection fraction (LVEF) is the measurement of how much blood is being pumped out of the left ventricle of the heart (the main pumping chamber) with each contraction. All participants who enrolled in this study must have had a baseline LVEF ≥55%. Verbatim description of adverse events was mapped to Medical Dictionary for Regulatory Activities (MedDRA) version 22.1. The MedDRA preferred term of 'ejection fraction decreased' is defined as an LVEF decrease of at least 10 percentage points from baseline and to below 50%.

End point type

Secondary

End point timeframe

Baseline; Day 1 of Cycles 4, 7, and 11 (each cycle is 21 days); End of Treatment and Follow-Up visits (up to 3 years)

End point values	P+H IV: Treatment Cross-Over Period	PH FDC SC: Treatment Cross-Over Period	P+H IV: Treatment Continuation Period	PH FDC SC: Treatment Continuation Period
Number of subjects analysed	160	160	21	137
Units: Participants	3	4	0	0

No statistical analyses for this end point

Secondary: Number of Participants with Targeted Vital Signs Outside the Normal Limits Among Those Without an Abnormality at Baseline

Top of page

End point title

Number of Participants with Targeted Vital Signs Outside the Normal Limits Among Those Without an Abnormality at Baseline

End point description

The number of participants at any post-baseline timepoint with abnormal readings outside the normal range for vital signs of diastolic and systolic blood pressure, pulse rate, respiratory rate, and body temperature were summarized according the specified direction of the abnormal reading (high or low). The number analyzed (denominator) in the results table represents participants without the specified abnormal vital sign at baseline.

End point type

Secondary

End point timeframe

Pre-dose at Day 1 of Cycles 1 (baseline), 4, and 7, and end of treatment (up to 18 cycles; 1 cycle is 21 days)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	80	80
Units: Participants
Diastolic Blood Pressure - Low (n=80,80)	0	0
Diastolic Blood Pressure - High (n=80,78)	4	0
Systolic Blood Pressure - Low (n=80,80)	0	0
Systolic Blood Pressure - High (n=77,75)	14	9
Pulse Rate - Low (n=80,80)	0	0
Pulse Rate - High (n=75,75)	1	1
Respiratory Rate - Low (n=80,80)	0	0
Respiratory Rate - High (n=80,79)	1	5
Temperature - Low (n=53,39)	27	19
Temperature - High (n=80,80)	0	1

No statistical analyses for this end point

Secondary: Number of Participants with Chemistry and Hematology Laboratory Test Result Shifts from NCI-CTCAE Grade 0–2 at Baseline to Grade 3–4 Post-Baseline

Top of page

End point title

Number of Participants with Chemistry and Hematology Laboratory Test Result Shifts from NCI-CTCAE Grade 0–2 at Baseline to Grade 3–4 Post-Baseline

End point description

Laboratory data for targeted chemistry and hematology parameters were classified according to the National Cancer Institute Common Terminology Criteria for Adverse Events version 4.0 (NCI CTCAE v4.0); Grade 0 is normal and Grades 1 to 4 represent worsening levels of the laboratory parameter outside of the normal range in the specified direction of the abnormality (e.g., high is an increase, low is a decrease). The results table presents the shifts in the number of participants with NCI-CTCAE Grade 0–2 at baseline to Grade 3–4 post-baseline for the targeted parameters according to the specified direction of the abnormality outside of the normal range (high or low). Participants with missing baseline values were counted as Grade 0–2 at baseline. SGOT/AST = aspartate aminotransferase; SGPT/ALT = alanine aminotransferase

End point type

Secondary

End point timeframe

Pre-dose at Day 1 of Cycles 1 (baseline), 4, 7, 11, 15, and end of treatment (up to 18 cycles; 1 cycle is 21 days)

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	80	80
Units: Participants
Alkaline Phosphatase - High (n=80,80)	0	0
SGPT/ALT - High (n=80,80)	0	0
SGOT/AST - High (n=80,80)	0	0
Creatinine - High (n=80,80)	0	0
Bilirubin, Total - High (n=80,80)	0	0
Hemoglobin - Low (n=80,80)	0	0
Hemoglobin - High (n=80,80)	0	0
Neutrophils, Total, Abs - Low (n=80,79)	0	1
Platelet - Low (n=80,80)	0	0
Total Leukocyte Count - Low (n=80,80)	1	1
Total Leukocyte Count - High (n=80,80)	0	0

No statistical analyses for this end point

Secondary: Kaplan-Meier Estimate of the Percentage of Participants in Overall Survival

Top of page

End point title

Kaplan-Meier Estimate of the Percentage of Participants in Overall Survival

End point description

End point type

Secondary

End point timeframe

Up to 3 years

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[32]	0 ^[33]
Units: Percentage of participants
number (not applicable)

Notes
[32] - Results are not reported at this time because data collection is ongoing.
[33] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Kaplan-Meier Estimate of the Percentage of Participants in Invasive Disease-Free Survival Including Second Primary Non-Breast Cancer

Top of page

End point title

Kaplan-Meier Estimate of the Percentage of Participants in Invasive Disease-Free Survival Including Second Primary Non-Breast Cancer

End point description

End point type

Secondary

End point timeframe

Up to 3 years

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[34]	0 ^[35]
Units: Percentage of participants
number (not applicable)

Notes
[34] - Results are not reported at this time because data collection is ongoing.
[35] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Kaplan-Meier Estimate of the Percentage of Participants in Invasive Disease-Free Survival

Top of page

End point title

Kaplan-Meier Estimate of the Percentage of Participants in Invasive Disease-Free Survival

End point description

End point type

Secondary

End point timeframe

Up to 3 years

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[36]	0 ^[37]
Units: Percentage of participants
number (not applicable)

Notes
[36] - Results are not reported at this time because data collection is ongoing.
[37] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Secondary: Kaplan-Meier Estimate of the Percentage of Participants in Distant Disease-Free Survival

Top of page

End point title

Kaplan-Meier Estimate of the Percentage of Participants in Distant Disease-Free Survival

End point description

End point type

Secondary

End point timeframe

Up to 3 years

End point values	A: P+H IV Followed by PH FDC SC	B: PH FDC SC Followed by P+H IV
Number of subjects analysed	0 ^[38]	0 ^[39]
Units: Percentage of participants
number (not applicable)

Notes
[38] - Results are not reported at this time because data collection is ongoing.
[39] - Results are not reported at this time because data collection is ongoing.

No statistical analyses for this end point

Adverse events

Top of page

Timeframe for reporting adverse events

From Baseline until the primary completion date (up to 1 year, 2 months)

Assessment type

Systematic

Dictionary name

MedDRA

Dictionary version

22.1

Reporting group title

Pertuzumab IV and Trastuzumab IV: Cross-Over Period

Reporting group description

This safety analysis population includes all participants from arms A and B who received up to 3 cycles (1 cycle = 21 days) of treatment with pertuzumab IV and trastuzumab IV during the Treatment Cross-Over Period of the study.

Reporting group title

Pertuzumab and Trastuzumab FDC SC: Cross-Over Period

Reporting group description

This safety analysis population includes all participants from arms A and B who received up to 3 cycles (1 cycle = 21 days) of treatment with the pertuzumab and trastuzumab fixed dose combination administered subcutaneously (FDC SC) during the Treatment Cross-Over Period of the study.

Reporting group title

Pertuzumab IV and Trastuzumab IV: Continuation Period

Reporting group description

This safety analysis population includes all participants from arms A and B who, following completion of the Treatment Cross-Over Period, chose to receive pertuzumab IV and trastuzumab IV during the Treatment Continuation Period for the remaining anti-HER2 treatment cycles (18 planned cycles in total, including pre-study neoadjuvant treatment).

Reporting group title

Pertuzumab and Trastuzumab FDC SC: Continuation Period

Reporting group description

This safety analysis population includes all participants from arms A and B who, following completion of the Treatment Cross-Over Period, chose to receive the pertuzumab and trastuzumab fixed dose combination administered subcutaneously (FDC SC) during the Treatment Continuation Period for the remaining anti-HER2 treatment cycles (18 planned cycles in total, including pre-study neoadjuvant treatment).

Serious adverse events	Pertuzumab IV and Trastuzumab IV: Cross-Over Period	Pertuzumab and Trastuzumab FDC SC: Cross-Over Period	Pertuzumab IV and Trastuzumab IV: Continuation Period	Pertuzumab and Trastuzumab FDC SC: Continuation Period
Total subjects affected by serious adverse events
subjects affected / exposed	6 / 160 (3.75%)	2 / 160 (1.25%)	0 / 21 (0.00%)	3 / 137 (2.19%)
number of deaths (all causes)	0	0	0	0
number of deaths resulting from adverse events
Investigations
Ejection fraction decreased
subjects affected / exposed	1 / 160 (0.63%)	1 / 160 (0.63%)	0 / 21 (0.00%)	0 / 137 (0.00%)
occurrences causally related to treatment / all	1 / 1	1 / 1	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0
Respiratory, thoracic and mediastinal disorders
Asthma
subjects affected / exposed	0 / 160 (0.00%)	1 / 160 (0.63%)	0 / 21 (0.00%)	0 / 137 (0.00%)
occurrences causally related to treatment / all	0 / 0	0 / 1	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0
Infections and infestations
Device related infection
subjects affected / exposed	1 / 160 (0.63%)	0 / 160 (0.00%)	0 / 21 (0.00%)	1 / 137 (0.73%)
occurrences causally related to treatment / all	0 / 1	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0
Erysipelas
subjects affected / exposed	1 / 160 (0.63%)	0 / 160 (0.00%)	0 / 21 (0.00%)	1 / 137 (0.73%)
occurrences causally related to treatment / all	0 / 1	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0
Breast cellulitis
subjects affected / exposed	1 / 160 (0.63%)	0 / 160 (0.00%)	0 / 21 (0.00%)	0 / 137 (0.00%)
occurrences causally related to treatment / all	0 / 1	0 / 0	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0
Bronchopulmonary aspergillosis
subjects affected / exposed	0 / 160 (0.00%)	0 / 160 (0.00%)	0 / 21 (0.00%)	1 / 137 (0.73%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0
Pneumonia
subjects affected / exposed	1 / 160 (0.63%)	0 / 160 (0.00%)	0 / 21 (0.00%)	0 / 137 (0.00%)
occurrences causally related to treatment / all	0 / 1	0 / 0	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0
Upper respiratory tract infection
subjects affected / exposed	1 / 160 (0.63%)	0 / 160 (0.00%)	0 / 21 (0.00%)	0 / 137 (0.00%)
occurrences causally related to treatment / all	0 / 1	0 / 0	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0

Frequency threshold for reporting non-serious adverse events: 5%

Non-serious adverse events	Pertuzumab IV and Trastuzumab IV: Cross-Over Period	Pertuzumab and Trastuzumab FDC SC: Cross-Over Period	Pertuzumab IV and Trastuzumab IV: Continuation Period	Pertuzumab and Trastuzumab FDC SC: Continuation Period
Total subjects affected by non serious adverse events
subjects affected / exposed	57 / 160 (35.63%)	77 / 160 (48.13%)	8 / 21 (38.10%)	29 / 137 (21.17%)
Injury, poisoning and procedural complications
Radiation skin injury
subjects affected / exposed	27 / 160 (16.88%)	17 / 160 (10.63%)	0 / 21 (0.00%)	1 / 137 (0.73%)
occurrences all number	28	17	0	1
Vascular disorders
Hot flush
subjects affected / exposed	6 / 160 (3.75%)	9 / 160 (5.63%)	0 / 21 (0.00%)	3 / 137 (2.19%)
occurrences all number	6	10	0	3
Nervous system disorders
Headache
subjects affected / exposed	3 / 160 (1.88%)	5 / 160 (3.13%)	2 / 21 (9.52%)	1 / 137 (0.73%)
occurrences all number	3	6	3	1
General disorders and administration site conditions
Fatigue
subjects affected / exposed	9 / 160 (5.63%)	9 / 160 (5.63%)	1 / 21 (4.76%)	4 / 137 (2.92%)
occurrences all number	9	9	2	4
Injection site reaction
subjects affected / exposed	0 / 160 (0.00%)	36 / 160 (22.50%)	0 / 21 (0.00%)	10 / 137 (7.30%)
occurrences all number	0	50	0	25
Gastrointestinal disorders
Diarrhoea
subjects affected / exposed	16 / 160 (10.00%)	13 / 160 (8.13%)	4 / 21 (19.05%)	14 / 137 (10.22%)
occurrences all number	19	17	4	20
Skin and subcutaneous tissue disorders
Rash
subjects affected / exposed	2 / 160 (1.25%)	2 / 160 (1.25%)	2 / 21 (9.52%)	2 / 137 (1.46%)
occurrences all number	3	2	2	3
Musculoskeletal and connective tissue disorders
Arthralgia
subjects affected / exposed	6 / 160 (3.75%)	8 / 160 (5.00%)	2 / 21 (9.52%)	1 / 137 (0.73%)
occurrences all number	8	8	2	1
Bone pain
subjects affected / exposed	0 / 160 (0.00%)	0 / 160 (0.00%)	2 / 21 (9.52%)	0 / 137 (0.00%)
occurrences all number	0	0	2	0
Myalgia
subjects affected / exposed	5 / 160 (3.13%)	3 / 160 (1.88%)	2 / 21 (9.52%)	0 / 137 (0.00%)
occurrences all number	5	3	2	0

More information

Top of page

Were there any global substantial amendments to the protocol? No

Were there any global interruptions to the trial? No

Limitations of the trial such as small numbers of subjects analysed or technical problems leading to unreliable data.

None reported

Select Country:	Select Age Range:
Select Trial Status:	Select Trial Phase:
Select Gender:
Select Date Range: to
Select Rare Disease:
IMP with orphan designation in the indication
Orphan Designation Number:
Results Status:
Clear advanced search filters

Austria
Belgium
Bulgaria
Croatia
Cyprus
Czechia
Denmark
Estonia
Finland
France
Germany
Greece
Hungary
Iceland
Ireland
Italy
Latvia
Liechtenstein
Lithuania
Luxembourg
Malta
Netherlands
Norway
Poland
Portugal
Romania
Slovakia
Slovenia
Spain
Sweden
United Kingdom
Outside EU/EEA

Clinical trials

Clinical Trial Results: A Randomized, Multicenter, Open-Label Cross-Over Study to Evaluate Patient Preference and Satisfaction of Subcutaneous Administration of the Fixed-Dose Combination of Pertuzumab and Trastuzumab in Patients with HER2-Positive Early Breast Cancer

Trial information

Trial information

Subject disposition

Subject disposition

Baseline characteristics

Baseline characteristics

End points

End points

Primary: Percentage of Participants by Their Preferred Method of Pertuzumab and Trastuzumab Administration, as Assessed in Question 1 of the Patient Preference Questionnaire (PPQ)

Primary: Percentage of Participants by Their Preferred Method of Pertuzumab and Trastuzumab Administration, as Assessed in Question 1 of the Patient Preference Questionnaire (PPQ)

Secondary: Percentage of Participants by Responses to the Strength of Their Preferred Method of Pertuzumab and Trastuzumab Administration, as Assessed in Question 2 of the Patient Preference Questionnaire (PPQ)

Secondary: Percentage of Participants by Responses to the Strength of Their Preferred Method of Pertuzumab and Trastuzumab Administration, as Assessed in Question 2 of the Patient Preference Questionnaire (PPQ)

Secondary: Percentage of Responses from Participants to the Two Main Reasons for Their Preferred Method of Pertuzumab and Trastuzumab Administration, as Assessed in Question 3 of the Patient Preference Questionnaire (PPQ)

Secondary: Percentage of Responses from Participants to the Two Main Reasons for Their Preferred Method of Pertuzumab and Trastuzumab Administration, as Assessed in Question 3 of the Patient Preference Questionnaire (PPQ)

Secondary: Percentage of Participants by Their Level of Satisfaction with the Respective Methods of Administration (IV and SC), Question 1 of the Therapy Administration Satisfaction Questionnaire –Intravenous (TASQ-IV) and –Subcutaneous (TASQ-SC)

Secondary: Percentage of Participants by Their Level of Satisfaction with the Respective Methods of Administration (IV and SC), Question 1 of the Therapy Administration Satisfaction Questionnaire –Intravenous (TASQ-IV) and –Subcutaneous (TASQ-SC)

Secondary: Mean Scores of the Five Domains of the TASQ-IV and TASQ-SC (Satisfaction, Physical Impact, Psychological Impact, Impact on Activities of Daily Living, and Convenience) to Assess the Impact of IV and SC Routes of Administration

Secondary: Mean Scores of the Five Domains of the TASQ-IV and TASQ-SC (Satisfaction, Physical Impact, Psychological Impact, Impact on Activities of Daily Living, and Convenience) to Assess the Impact of IV and SC Routes of Administration

Secondary: Percentage of Participants by Their Responses to Question 9 of the TASQ-IV and TASQ-SC, Assessing Whether Participants Receiving IV and SC Administration Have as Much Time as They Would Like to Talk to Their Nurse and/or Doctor About Their Illness

Secondary: Percentage of Participants by Their Responses to Question 9 of the TASQ-IV and TASQ-SC, Assessing Whether Participants Receiving IV and SC Administration Have as Much Time as They Would Like to Talk to Their Nurse and/or Doctor About Their Illness

Secondary: Percentage of Participants by Their Responses to Question 10 of the TASQ-IV and TASQ-SC, Assessing Whether IV and SC Administration Have an Impact on the Amount of Time Participants Have to Talk to Their Nurse and/or Doctor About Their Illness

Secondary: Percentage of Participants by Their Responses to Question 10 of the TASQ-IV and TASQ-SC, Assessing Whether IV and SC Administration Have an Impact on the Amount of Time Participants Have to Talk to Their Nurse and/or Doctor About Their Illness

Secondary: Percentage of Participants by Their Responses to Question 11 of the TASQ-IV and TASQ-SC, Assessing the Participants' Preferred Method for Receiving Cancer Treatment

Secondary: Percentage of Participants by Their Responses to Question 11 of the TASQ-IV and TASQ-SC, Assessing the Participants' Preferred Method for Receiving Cancer Treatment

Secondary: Percentage of Participants by Their Choice of Treatment in the Treatment Continuation Period (PH FDC SC or P+H IV) and by Consistency of This Choice with Their Preferred Method of Administration Reported in Question 1 of the PPQ

Secondary: Percentage of Participants by Their Choice of Treatment in the Treatment Continuation Period (PH FDC SC or P+H IV) and by Consistency of This Choice with Their Preferred Method of Administration Reported in Question 1 of the PPQ

Secondary: Duration of Treatment Administration Activities According to Healthcare Professionals' Responses on Perception of Time by Treatment Cycle, Question 1 of the Healthcare Professional Questionnaire (HCPQ) - Treatment Room

Secondary: Duration of Treatment Administration Activities According to Healthcare Professionals' Responses on Perception of Time by Treatment Cycle, Question 1 of the Healthcare Professional Questionnaire (HCPQ) - Treatment Room

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Impact of PH FDC SC on Clinical Management and Clinical Efficiency, Question 2 of the HCPQ - Treatment Room

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Impact of PH FDC SC on Clinical Management and Clinical Efficiency, Question 2 of the HCPQ - Treatment Room

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Time/Resource Use and Convenience of Each Study Regimen, Questions 3 to 7 of the HCPQ - Treatment Room

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Time/Resource Use and Convenience of Each Study Regimen, Questions 3 to 7 of the HCPQ - Treatment Room

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses to Question 8 of the HCPQ - Treatment Room

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses to Question 8 of the HCPQ - Treatment Room

Secondary: Duration of Treatment Preparation According to Healthcare Professionals' Responses on Perception of Time by Treatment Cycle, Question 1 of the HCPQ - Drug Preparation Room

Secondary: Duration of Treatment Preparation According to Healthcare Professionals' Responses on Perception of Time by Treatment Cycle, Question 1 of the HCPQ - Drug Preparation Room

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Impact of PH FDC SC on Clinical Management and Clinical Efficiency, Question 2 of the HCPQ - Drug Preparation Room

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Impact of PH FDC SC on Clinical Management and Clinical Efficiency, Question 2 of the HCPQ - Drug Preparation Room

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Time/Resource Use of Each Study Regimen, Questions 3 and 4 of the HCPQ - Drug Preparation Room

Secondary: Percentage of Healthcare Professionals (HCPs) by Their Responses on Perception of Time/Resource Use of Each Study Regimen, Questions 3 and 4 of the HCPQ - Drug Preparation Room

Secondary: Change From Baseline Over Time in Health-Related Quality of Life (HRQoL) as Assessed by the Global Health Status/QoL Scale Score of the the European Organization for Research and Treatment of Cancer Quality of Life Questionnaire 30 (EORTC QLQ-C30)

Secondary: Change From Baseline Over Time in Health-Related Quality of Life (HRQoL) as Assessed by the Global Health Status/QoL Scale Score of the the European Organization for Research and Treatment of Cancer Quality of Life Questionnaire 30 (EORTC QLQ-C30)

Secondary: Change From Baseline Over Time in the Physical Functioning Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Physical Functioning Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Role Functioning Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Role Functioning Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Emotional Functioning Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Emotional Functioning Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Cognitive Functioning Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Cognitive Functioning Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Social Functioning Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Social Functioning Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Fatigue Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Fatigue Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Nausea and Vomiting Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Nausea and Vomiting Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Pain Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Pain Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Dyspnoea Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Dyspnoea Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Insomnia Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Insomnia Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Appetite Loss Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Appetite Loss Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Constipation Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Constipation Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Diarrhoea Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Diarrhoea Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Financial Difficulties Scale Score of the EORTC QLQ-C30

Secondary: Change From Baseline Over Time in the Financial Difficulties Scale Score of the EORTC QLQ-C30

Secondary: Safety Summary for Assessment of Switching Between the FDC SC and IV Formulations: Number of Participants with at Least One Adverse Event During the Treatment Cross-Over Period by Treatment Arm and Treatment Received

Secondary: Safety Summary for Assessment of Switching Between the FDC SC and IV Formulations: Number of Participants with at Least One Adverse Event During the Treatment Cross-Over Period by Treatment Arm and Treatment Received

Secondary: Safety Summary of the FDC SC and IV Formulations: Number of Participants with at Least One Adverse Event During the Cross-Over and Continuation Treatment Periods

Secondary: Safety Summary of the FDC SC and IV Formulations: Number of Participants with at Least One Adverse Event During the Cross-Over and Continuation Treatment Periods

Secondary: Number of Participants with at Least One Event of Heart Failure with the FDC SC and IV Formulations During the Cross-Over and Continuation Treatment Periods

Secondary: Number of Participants with at Least One Event of Heart Failure with the FDC SC and IV Formulations During the Cross-Over and Continuation Treatment Periods

Secondary: Number of Participants with at Least One Event of Ejection Fraction Decreased with the FDC SC and IV Formulations During the Cross-Over and Continuation Treatment Periods

Secondary: Number of Participants with at Least One Event of Ejection Fraction Decreased with the FDC SC and IV Formulations During the Cross-Over and Continuation Treatment Periods

Clinical Trial Results:
A Randomized, Multicenter, Open-Label Cross-Over Study to Evaluate Patient Preference and Satisfaction of Subcutaneous Administration of the Fixed-Dose Combination of Pertuzumab and Trastuzumab in Patients with HER2-Positive Early Breast Cancer