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Clinical Trial Results:
A Multicenter, Open-Label, Uncontrolled, Extension Study of RA101495 in Subjects with Paroxysmal Nocturnal Hemoglobinuria who have Completed a RA101495 Clinical Study

Summary
EudraCT number	2016-003523-34
Trial protocol	FI HU DK GB
Global end of trial date	26 Oct 2021

Results information
Results version number	v2(current)
This version publication date	15 Dec 2022
First version publication date	23 Sep 2022
Other versions	v1
Version creation reason	Correction of full data set Alignment with final posting on ClinicalTrials.gov after NIH review.

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

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Trial information

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Sponsor protocol code

RA101495-01.202

ISRCTN number

US NCT number

NCT03225287

WHO universal trial number (UTN)

Other trial identifiers

UCB Study Id: PNH001

Sponsor organisation name

Ra Pharmaceuticals, Inc.

Sponsor organisation address

87 Cambridge Park Drive, Cambridge, Massachusetts, United States, 02140

Public contact

Clin Trial Reg & Results Disclosure, UCB BIOSCIENCES GmbH, clinicaltrials@ucb.com

Scientific contact

Clin Trial Reg & Results Disclosure, UCB BIOSCIENCES GmbH, clinicaltrials@ucb.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

Final

Date of interim/final analysis

21 Oct 2021

Is this the analysis of the primary completion data?

Yes

Primary completion date

07 Sep 2021

Global end of trial reached?

Yes

Global end of trial date

26 Oct 2021

Was the trial ended prematurely?

Yes

Main objective of the trial

• To provide access to RA101495 for participants with PNH who have completed a Ra Pharmaceuticals sponsored study, have demonstrated clinical benefit, and who wish to continue receiving RA101495 for treatment of PNH • To evaluate the long-term safety and tolerability of RA101495 administered to participants with PNH who have completed a Ra Pharmaceuticals sponsored RA101495 clinical study • To evaluate the long-term preliminary efficacy of RA101495 administered to participants with PNH who have completed a Ra Pharmaceuticals sponsored RA101495 clinical study • To obtain periodic PK and PD data to confirm long-term maintenance of steady-state RA101495 plasma levels and sustained inhibition of hemolysis and complement

Protection of trial subjects

During the conduct of the study all participants were monitored for safety.

Background therapy

Background therapy as permitted in the protocol at the discretion of each treating physician.

Evidence for comparator

Not applicable

Actual start date of recruitment

17 Jul 2017

Long term follow-up planned

Independent data monitoring committee (IDMC) involvement?

Number of subjects enrolled per country

Country: Number of subjects enrolled

Australia: 3

Country: Number of subjects enrolled

Canada: 1

Country: Number of subjects enrolled

Germany: 2

Country: Number of subjects enrolled

Finland: 1

Country: Number of subjects enrolled

United Kingdom: 3

Country: Number of subjects enrolled

Hungary: 2

Country: Number of subjects enrolled

New Zealand: 4

Country: Number of subjects enrolled

United States: 3

Worldwide total number of subjects

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)

From 65 to 84 years

85 years and over

Subject disposition

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Recruitment details

The study started to enroll participants in July 2017 and concluded in October 2021.

Screening details

The Participant Flow refers to the All Enrolled Subjects.

Period 1 title

Overall Study (overall period)

Is this the baseline period?

Yes

Allocation method

Not applicable

Blinding used

Not blinded

Are arms mutually exclusive

Yes

Zilucoplan-Cohort A (Eculizumab Naïve)

Arm description

Cohort A (Eculizumab Naive) included all participants from study RA101495-01.201 (NCT03078582) who had not received eculizumab for treatment of paroxysmal nocturnal hemoglobinuria (PNH). Participants received a loading dose of 0.3 milligram/kilogram (mg/kg) zilucoplan administered by subcutaneous (SC) injection at Day 1 of this study. Following in-clinic education and training, all participants self-injected 0.1 mg/kg of zilucoplan by SC injection once daily for 12 months. From Week 2 onwards, if a participant had not achieved an adequate response, the zilucoplan dose was escalated to 0.3 mg/kg daily.

Arm type

Experimental

Investigational medicinal product name

Zilucoplan

Investigational medicinal product code

RA101495

Other name

Pharmaceutical forms

Solution for injection in pre-filled syringe

Routes of administration

Subcutaneous use

Dosage and administration details

Participants received zilucoplan administered by SC injection at pre-defined timepoints.

Zilucoplan-Cohort B (Eculizumab Switch)

Arm description

Cohort B (Eculizumab Switch) included all participants from study RA101495-01.201 (NCT03078582) who had received eculizumab for treatment of PNH. Participants received a loading dose of 0.3 mg/kg zilucoplan administered by SC injection at Day 1 of this study. Following in-clinic education and training, all participants self-injected 0.1 mg/kg of zilucoplan by SC injection once daily for 12 months. From Week 2 onwards, if a participant had not achieved an adequate response, the zilucoplan dose was escalated to 0.3 mg/kg daily.

Arm type

Experimental

Investigational medicinal product name

Zilucoplan

Investigational medicinal product code

RA101495

Other name

Pharmaceutical forms

Solution for injection in pre-filled syringe

Routes of administration

Subcutaneous use

Dosage and administration details

Participants received zilucoplan administered by SC injection at pre-defined timepoints.

Zilucoplan (Inadequate Responder to Eculizumab)

Arm description

Inadequate Responder cohort included participants from qualifying study RA101495-01.203 (NCT03030183) who had an inadequate response to eculizumab treatment for PNH. Participants received a loading dose of 0.3 mg/kg zilucoplan administered by SC injection at Day 1 of this study. Following in-clinic education and training, all participants self-injected 0.1 mg/kg of zilucoplan by SC injection once daily for 12 months. From Week 2 onwards, if a participant had not achieved an adequate response, the zilucoplan dose was escalated to 0.3 mg/kg daily.

Arm type

Experimental

Investigational medicinal product name

Zilucoplan

Investigational medicinal product code

RA101495

Other name

Pharmaceutical forms

Solution for injection in pre-filled syringe

Routes of administration

Subcutaneous use

Dosage and administration details

Participants received zilucoplan administered by SC injection at pre-defined timepoints.

Number of subjects in period 1	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Started	10	6	3
Completed	0	0	0
Not completed	10	6	3
Stem cell transplantation	-	1	-
Protocol non-compliance	-	-	1
Adverse event, non-fatal	-	-	1
Trial drug not effective	-	1	-
Sponsor, regulatory, or EC/IRB request	7	3	1
Subject withdraws consent	3	-	-
Need of transfusions and signs of hemolysis	-	1	-

Baseline characteristics

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Reporting group title

Zilucoplan-Cohort A (Eculizumab Naïve)

Reporting group description

Reporting group title

Zilucoplan-Cohort B (Eculizumab Switch)

Reporting group description

Reporting group title

Zilucoplan (Inadequate Responder to Eculizumab)

Reporting group description

Reporting group values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)	Total
Number of subjects	10	6	3	19
Age Categorical
Units: participants
<=18 years	0	0	0	0
Between 18 and 65 years	6	4	3	13
>=65 years	4	2	0	6
Age Continuous
Units: years
arithmetic mean (standard deviation)	59.6 ( 14.5 )	45.0 ( 23.0 )	35.3 ( 16.3 )	-
Sex: Female, Male
Units: participants
Female	6	1	1	8
Male	4	5	2	11

End points

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Reporting group title

Zilucoplan-Cohort A (Eculizumab Naïve)

Reporting group description

Reporting group title

Zilucoplan-Cohort B (Eculizumab Switch)

Reporting group description

Reporting group title

Zilucoplan (Inadequate Responder to Eculizumab)

Reporting group description

Primary: Percentage of participants with Treatment Emergent Adverse events (TEAEs)

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End point title

Percentage of participants with Treatment Emergent Adverse events (TEAEs) ^[1]

End point description

TEAEs were defined as an AE that occurs after a participant's initial treatment zilucoplan start for this study (RA101495-01.202) that was not present at the time of treatment start, or an AE that increases in severity after treatment start in this study, if the event was present at the time of treatment start. Safety population included all participants who received at least 1 injection of zilucoplan on or after Day 1 of this extension study.

End point type

Primary

End point timeframe

From Day 1 until the Final Study Visit (up to Month 49)

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 statistical hypothesis testing was planned for this study. Results were summarized in tables as descriptive statistics only.

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	10	6	3
Units: percentage of participants
number (not applicable)	90.0	100	66.7

No statistical analyses for this end point

Primary: Percentage of participants with Serious TEAEs

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End point title

Percentage of participants with Serious TEAEs ^[2]

End point description

Serious Adverse event (SAE) was defined as any untoward medical occurrence that:• results in death, • is life-threatening threatening (note that this refers to an event in which the participant was at risk of death at the time of the event; it does not refer to an event that hypothetically might have caused death if it were more severe), • requires hospitalization or prolongation of existing hospitalization, • results in persistent or significant disability/incapacity, and • results in a congenital anomaly/birth defect. Safety population included all participants who received at least 1 injection of zilucoplan on or after Day 1 of this extension study.

End point type

Primary

End point timeframe

From Day 1 until the Final Study Visit (up to Month 49)

Notes
[2] - 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 statistical hypothesis testing was planned for this study. Results were summarized in tables as descriptive statistics only.

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	10	6	3
Units: percentage of participants
number (not applicable)	10.0	50.0	66.7

No statistical analyses for this end point

Secondary: Number of participants with anti-drug antibodies (ADA)

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End point title

Number of participants with anti-drug antibodies (ADA)

End point description

Blood samples collection were planned to analyze for the presence/absence of ADAs to zilucoplan for immunogenicity assessments. Safety population included all participants who received at least 1 injection of zilucoplan on or after Day 1 of this extension study. The planned analysis of immunogenicity (ADA) was not performed as the assay was considered not fit for purpose due to an insufficient level of drug tolerance; therefore, no samples were processed.

End point type

Secondary

End point timeframe

At Day 1, Month 1, 2, 3, 6, 9, and 12

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	0 ^[3]	0 ^[4]	0 ^[5]
Units: participants

Notes
[3] - Due to insufficient level of drug tolerance samples were not processed.
[4] - Due to insufficient level of drug tolerance samples were not processed.
[5] - Due to insufficient level of drug tolerance samples were not processed.

No statistical analyses for this end point

Secondary: Change from Baseline in Serum Lactate Dehydrogenase (LDH) Levels at each time point

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End point title

Change from Baseline in Serum Lactate Dehydrogenase (LDH) Levels at each time point

End point description

Serum LDH levels were measure of intravascular hemolysis. As high level of LDH in the blood was indicative of hemolysis in participants with PNH. Safety population included all participants who received at least 1 injection of zilucoplan on or after Day 1 of this extension study. Baseline was generally the final visit of the qualifying study (RA101495-01.201 or RA101495-01.203). Here, Number of participants analyzed included those participants who were evaluable for the assessment and 'n' signifies participants who were evaluable at specified time points. '99999' (n=0) signifies that the Mean and Standard Deviation (SD) was not calculated due to 0 participants and ‘99999’ (n=1) signifies that SD could not be calculated for a single participant.

End point type

Secondary

End point timeframe

Baseline, Month 1, 2, 3, 6, 9, 12, 15, 18, 21, 24, 27, 30, 33, 36, 39, 42, 45, and Final Study Visit (Month 49)

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	9	6	3
Units: Units per litre (U/L)
arithmetic mean (standard deviation)
Month 1 (n= 9, 6, 3)	-3.7 ( 71.5 )	10.0 ( 16.4 )	336.7 ( 636.9 )
Month 2 (n= 9, 5, 2)	50.3 ( 156.2 )	-2.4 ( 22.2 )	676.5 ( 970.9 )
Month 3 (n= 8, 5, 2)	-6.5 ( 58.2 )	-1.6 ( 40.5 )	39.5 ( 40.3 )
Month 6 (n=8, 5, 2)	32.4 ( 142.5 )	-28.4 ( 127.3 )	-3.5 ( 12.0 )
Month 9 (n=8, 3, 2 )	-18.1 ( 59.7 )	22.7 ( 23.6 )	-5.0 ( 35.4 )
Month 12 (n= 7, 3, 2)	-39.7 ( 54.9 )	8.7 ( 10.1 )	456.0 ( 640.6 )
Month 15 (n= 6, 3, 2)	-24.5 ( 70.8 )	4.0 ( 30.4 )	174.5 ( 215.7 )
Month 18 (n=7, 3, 1)	-27.9 ( 54.8 )	5.7 ( 56.8 )	-56.0 ( 99999 )
Month 21 (n= 7, 3, 1)	-12.0 ( 93.9 )	-7.3 ( 33.5 )	73.0 ( 99999 )
Month 24 (n= 7, 3, 1)	-18.7 ( 53.9 )	-27.0 ( 64.1 )	-29.0 ( 99999 )
Month 27 (n= 5, 2, 0)	-14.0 ( 99.3 )	58.0 ( 8.5 )	99999 ( 99999 )
Month 30 (n= 5, 2, 1)	-28.0 ( 36.1 )	59.0 ( 140.0 )	1817.0 ( 99999 )
Month 33 (n= 5, 3, 0)	-39.0 ( 65.9 )	-16.3 ( 66.7 )	99999 ( 99999 )
Month 36 (n= 5, 2, 0)	-61.6 ( 47.1 )	0.5 ( 4.9 )	99999 ( 99999 )
Month 39 (n= 5, 3, 0)	-78.4 ( 80.9 )	-29.7 ( 83.5 )	99999 ( 99999 )
Month 42 (n= 4, 2, 0)	-42.3 ( 78.3 )	35.5 ( 75.7 )	99999 ( 99999 )
Month 45 (n= 1, 1, 0)	27.0 ( 99999 )	53.0 ( 99999 )	99999 ( 99999 )
Final Study Visit (Month 49) (n= 9, 5, 2)	41.6 ( 303.1 )	-93.2 ( 139.8 )	682.0 ( 548.7 )

No statistical analyses for this end point

Secondary: Change from Baseline in Total Bilirubin Values at each time point

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End point title

Change from Baseline in Total Bilirubin Values at each time point

End point description

Total Bilirubin was monitored for signs and symptoms of hepatic or biliary dysfunction. Safety population included all participants who received at least 1 injection of zilucoplan on or after Day 1 of the extension study. Baseline was generally the final visit of the qualifying study (RA101495-01.201 or RA101495-01.203). Here, Number of participants analyzed included those participants who were evaluable for the assessment and 'n' (Number analyzed) signifies participants who were evaluable at specified time points. '99999' (n=0) signifies that the Mean and Standard Deviation (SD) was not calculated due to 0 participants and ‘99999’ (n=1) signifies that SD could not be calculated for a single participant.

End point type

Secondary

End point timeframe

Baseline, Month 1, 2, 3, 6, 9, 12, 15, 18, 21, 24, 27, 30, 33, 36, 39, 42, 45, and Final Study Visit (Month 49)

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	9	6	3
Units: micromole per litre (umol/L)
arithmetic mean (standard deviation)
Month 1 (n= 9, 6, 3)	-2.1 ( 7.7 )	1.7 ( 6.2 )	-0.3 ( 4.5 )
Month 2 (n= 9, 5, 2)	0.1 ( 10.7 )	2.0 ( 7.2 )	6.0 ( 2.8 )
Month 3 (n= 8, 5, 2)	1.4 ( 13.7 )	8.2 ( 13.1 )	3.5 ( 2.1 )
Month 6 (n= 8, 5, 2)	4.6 ( 14.8 )	3.2 ( 7.2 )	2.5 ( 0.7 )
Month 9 (n= 8, 3, 2)	-0.3 ( 7.4 )	6.0 ( 3.0 )	-1.0 ( 1.4 )
Month 12 (n= 8, 3, 2)	3.9 ( 8.4 )	3.0 ( 2.0 )	2.5 ( 3.5 )
Month 15 (n= 7, 3, 2)	-0.4 ( 6.4 )	6.0 ( 9.5 )	8.5 ( 9.2 )
Month 18 (n= 6, 3, 1)	2.8 ( 9.5 )	2.0 ( 6.2 )	3.0 ( 99999 )
Month 21 (n= 7, 3, 1)	3.9 ( 8.3 )	2.0 ( 7.8 )	7.0 ( 99999 )
Month 24 (n= 7, 3, 1)	5.1 ( 16.0 )	-1.3 ( 3.1 )	8.0 ( 99999 )
Month 27 (n= 7, 2, 0)	4.3 ( 12.2 )	-2.0 ( 5.7 )	99999 ( 99999 )
Month 30 (n= 5, 2, 1)	5.8 ( 14.6 )	3.0 ( 7.1 )	13.0 ( 99999 )
Month 33 (n= 5, 3, 0)	2.6 ( 5.7 )	3.0 ( 2.6 )	99999 ( 99999 )
Month 36 (n= 5, 2, 0)	-3.8 ( 6.8 )	3.0 ( 0.0 )	99999 ( 99999 )
Month 39 (n= 5, 3, 0)	0.2 ( 3.1 )	0.7 ( 4.6 )	99999 ( 99999 )
Month 42 (n= 5, 2, 0)	4.8 ( 15.5 )	4.0 ( 15.6 )	99999 ( 99999 )
Month 45 (n= 2, 1, 0)	5.0 ( 17.0 )	-2.0 ( 99999 )	99999 ( 99999 )
Final Study Visit (Month 49) (n= 9, 5, 2)	8.0 ( 17.3 )	0.4 ( 3.9 )	0.0 ( 9.9 )

No statistical analyses for this end point

Secondary: Change from Baseline in Total Hemoglobin Values at each time point

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End point title

Change from Baseline in Total Hemoglobin Values at each time point

End point description

Total Hemoglobin Values were analyzed for hematology assessments. Safety population included all participants who received at least 1 injection of zilucoplan on or after Day 1 of the extension study. Baseline was generally the final visit of the qualifying study (RA101495-01.201 or RA101495-01.203). Here, Number of participants analyzed included those participants who were evaluable for the assessment and 'n' (Number analyzed) signifies participants who were evaluable at specified time points. '99999' (n=0) signifies that the Mean and Standard Deviation (SD) was not calculated due to 0 participants and ‘99999’ (n=1) signifies that SD could not be calculated for a single participant.

End point type

Secondary

End point timeframe

Baseline, Month 1, 2, 3, 6, 9, 12, 15, 18, 21, 24, 27, 30, 33, 36, 39, 42, 45, and Final Study Visit (Month 49)

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	9	6	3
Units: grams per litre (g/L)
arithmetic mean (standard deviation)
Month 1 (n= 8, 6, 3)	0.0 ( 11.4 )	0.0 ( 8.2 )	-5.7 ( 3.8 )
Month 2 (n= 9, 5, 2)	1.1 ( 8.3 )	-5.0 ( 9.9 )	-2.0 ( 11.3 )
Month 3 (n= 7, 5, 2)	6.4 ( 6.4 )	3.0 ( 9.1 )	-3.5 ( 6.4 )
Month 6 (n= 8, 5, 2)	1.1 ( 11.2 )	2.0 ( 17.9 )	-5.0 ( 17.0 )
Month 9 (n= 8, 3, 2)	2.9 ( 7.1 )	-1.3 ( 4.0 )	-9.0 ( 5.7 )
Month 12 (n= 8, 3, 2)	2.9 ( 6.1 )	-1.7 ( 6.8 )	-5.0 ( 17.0 )
Month 15 (n= 7, 3, 2)	3.9 ( 8.4 )	-5.0 ( 5.3 )	-9.0 ( 28.3 )
Month 18 (n= 7, 3, 1)	5.0 ( 4.9 )	1.7 ( 9.5 )	-2.0 ( 99999 )
Month 21 (n= 7, 3, 1)	6.4 ( 6.3 )	-6.7 ( 7.6 )	-1.0 ( 99999 )
Month 24 (n= 7, 3, 0)	7.9 ( 12.6 )	-5.0 ( 2.6 )	99999 ( 99999 )
Month 27 (n= 7, 2, 0)	7.0 ( 10.0 )	-5.0 ( 11.3 )	99999 ( 99999 )
Month 30 (n= 5, 2, 1)	10.8 ( 7.0 )	-4.5 ( 12.0 )	-8.0 ( 99999 )
Month 33 (n= 5, 3, 0)	10.0 ( 8.8 )	-3.0 ( 4.4 )	99999 ( 99999 )
Month 36 (n= 5, 2, 0)	8.4 ( 14.2 )	-2.0 ( 4.2 )	99999 ( 99999 )
Month 39 (n= 5, 3, 0)	7.6 ( 10.1 )	4.7 ( 2.9 )	99999 ( 99999 )
Month 42 (n= 5, 2, 0)	5.2 ( 11.2 )	5.5 ( 0.7 )	99999 ( 99999 )
Month 45 (n= 3, 1, 0)	-1.3 ( 23.3 )	-4.0 ( 99999 )	99999 ( 99999 )
Final Study Visit (Month 49) (n= 9, 4, 1)	1.8 ( 10.6 )	-2.0 ( 4.1 )	-7.0 ( 99999 )

No statistical analyses for this end point

Secondary: Change from Baseline in Free Hemoglobin Values at each time point

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End point title

Change from Baseline in Free Hemoglobin Values at each time point

End point description

Free Hemoglobin Values were analyzed for hematology assessments. Safety population included all participants who received at least 1 injection of zilucoplan on or after Day 1 of the extension study. Baseline was generally the final visit of the qualifying study (RA101495-01.201 or RA101495-01.203). Here, Number of participants analyzed included those participants who were evaluable for the assessment and 'n' (Number analyzed) signifies participants who were evaluable at specified time points. '99999' (n=0) signifies that the Mean and Standard Deviation (SD) was not calculated due to 0 participants and ‘99999’ (n=1) signifies that SD could not be calculated for a single participant.

End point type

Secondary

End point timeframe

Baseline, Month 1, 2, 3, 6, 9, 12, 15, 18, 21, 24, 27, 30, 33, 36, 39, 42, 45, and Final Study Visit (Month 49)

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	7	5	2
Units: milligrams per decilitre (mg/dL)
arithmetic mean (standard deviation)
Month 1 (n= 6, 5, 2)	-0.20 ( 2.78 )	2.86 ( 4.30 )	0.80 ( 4.38 )
Month 2 (n= 5, 5, 1)	-1.14 ( 3.04 )	0.48 ( 1.77 )	6.10 ( 99999 )
Month 3 (n= 5, 5, 1)	1.34 ( 0.48 )	-0.02 ( 0.95 )	0.80 ( 99999 )
Month 6 (n= 6, 4, 1)	-0.43 ( 1.24 )	0.55 ( 2.45 )	1.20 ( 99999 )
Month 9 (n= 6, 3, 1)	-1.10 ( 2.11 )	-1.50 ( 1.57 )	0.00 ( 99999 )
Month 12 (n= 7, 2, 1)	-0.56 ( 2.80 )	0.80 ( 0.28 )	2.10 ( 99999 )
Month 15 (n= 4, 2, 1)	3.93 ( 11.61 )	-1.35 ( 2.19 )	1.60 ( 99999 )
Month 18 (n= 4, 3, 0)	1.98 ( 3.05 )	0.77 ( 1.56 )	99999 ( 99999 )
Month 21 (n= 4, 2, 0)	3.15 ( 5.84 )	-1.30 ( 0.85 )	99999 ( 99999 )
Month 24 (n= 3, 2, 0)	0.27 ( 0.35 )	-0.50 ( 0.99 )	99999 ( 99999 )
Month 27 (n= 0, 0, 0)	99999 ( 99999 )	99999 ( 99999 )	99999 ( 99999 )
Month 30 (n= 3, 0, 0)	0.33 ( 2.37 )	99999 ( 99999 )	99999 ( 99999 )
Month 33 (n= 3, 1, 0)	0.17 ( 2.66 )	5.80 ( 99999 )	99999 ( 99999 )
Month 36 (n= 0, 0, 0)	99999 ( 99999 )	99999 ( 99999 )	99999 ( 99999 )
Month 39 (n= 1, 2, 0)	-0.60 ( 99999 )	-0.95 ( 0.64 )	99999 ( 99999 )
Month 42 (n= 1, 2, 0)	1.30 ( 99999 )	0.50 ( 3.68 )	99999 ( 99999 )
Month 45 (n= 0, 0, 0)	99999 ( 99999 )	99999 ( 99999 )	99999 ( 99999 )
Final Study Visit (Month 49) (n= 1, 2, 1)	-2.70 ( 99999 )	-0.60 ( 1.13 )	-3.10 ( 99999 )

No statistical analyses for this end point

Secondary: Change from Baseline in Haptoglobin Values at each time point

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End point title

Change from Baseline in Haptoglobin Values at each time point

End point description

Haptoglobin values were analyzed for hematology assessments. Safety population included all participants who received at least 1 injection of zilucoplan on or after Day 1 of the extension study. Baseline was generally the final visit of the qualifying study (RA101495-01.201 or RA101495-01.203). Here, Number of participants analyzed included those participants who were evaluable for the assessment and 'n' (Number analyzed) signifies participants who were evaluable at specified time points. '99999' (n=0) signifies that the Mean and Standard Deviation (SD) was not calculated due to 0 participants and ‘99999’ (n=1) signifies that SD could not be calculated for a single participant.

End point type

Secondary

End point timeframe

Baseline, Month 1, 2, 3, 6, 9, 12, 15, 18, 21, 24, 27, 30, 33, 36, 39, 42, 45, and Final Study Visit (Month 49)

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	9	6	3
Units: g/L
arithmetic mean (standard deviation)
Month 1 (n= 9, 6, 3)	0.032 ( 0.097 )	0.000 ( 0.000 )	0.000 ( 0.000 )
Month 2 (n= 9, 5, 2)	0.053 ( 0.160 )	0.000 ( 0.000 )	0.000 ( 0.000 )
Month 3 (n= 8, 5, 2)	0.021 ( 0.060 )	0.000 ( 0.000 )	0.000 ( 0.000 )
Month 6 (n= 8, 5, 2)	0.031 ( 0.088 )	0.036 ( 0.080 )	0.020 ( 0.028 )
Month 9 (n= 8, 3, 2)	0.008 ( 0.021 )	0.000 ( 0.000 )	0.000 ( 0.000 )
Month 12 (n= 8, 3, 2)	0.000 ( 0.000 )	0.000 ( 0.000 )	0.000 ( 0.000 )
Month 15 (n= 7, 3, 2)	0.000 ( 0.000 )	0.000 ( 0.000 )	0.000 ( 0.000 )
Month 18 (n= 7, 3, 1)	0.000 ( 0.000 )	0.000 ( 0.000 )	0.000 ( 99999 )
Month 21 (n= 7, 3, 1)	0.030 ( 0.079 )	0.000 ( 0.000 )	0.000 ( 99999 )
Month 24 (n= 7, 3, 1)	0.030 ( 0.079 )	0.000 ( 0.000 )	0.000 ( 99999 )
Month 27 (n= 7, 2, 0)	0.000 ( 0.000 )	0.000 ( 0.000 )	99999 ( 99999 )
Month 30 (n= 5, 2, 1)	0.004 ( 0.009 )	0.000 ( 0.000 )	0.000 ( 99999 )
Month 33 (n= 5, 3, 0)	0.002 ( 0.004 )	0.000 ( 0.000 )	99999 ( 99999 )
Month 36 (n= 5, 2, 0)	0.036 ( 0.080 )	0.000 ( 0.000 )	99999 ( 99999 )
Month 39 (n= 5, 3, 0)	0.020 ( 0.045 )	0.000 ( 0.000 )	99999 ( 99999 )
Month 42 (n= 5, 2, 0)	0.034 ( 0.076 )	0.000 ( 0.000 )	99999 ( 99999 )
Month 45 (n= 2, 1, 0)	0.080 ( 0.113 )	0.000 ( 99999 )	99999 ( 99999 )
Final Study Visit (Month 49) (n= 9, 5, 2)	0.042 ( 0.127 )	0.006 ( 0.013 )	0.000 ( 0.000 )

No statistical analyses for this end point

Secondary: Change from Baseline in Reticulocytes Values at each time point

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End point title

Change from Baseline in Reticulocytes Values at each time point

End point description

Reticulocytes values were analyzed for hematology assessments. Safety population included all participants who received at least 1 injection of zilucoplan on or after Day 1 of the extension study. Here, Number of participants analyzed included those participants who were evaluable for the assessment and 'n' (Number analyzed) signifies participants who were evaluable at specified time points. '99999' (n=0) signifies that the Mean and Standard Deviation (SD) was not calculated due to 0 participants and ‘99999’ (n=1) signifies that SD could not be calculated for a single participant.

End point type

Secondary

End point timeframe

Baseline, Month 1, 2, 3, 6, 9, 12, 15, 18, 21, 24, 27, 30, 33, 36, 39, 42, 45, and Final Study Visit (Month 49)

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	9	6	3
Units: 10^12 reticulocytes (cells)/L
arithmetic mean (standard deviation)
Month 1 (n= 8, 6, 3)	0.0104 ( 0.0484 )	0.0107 ( 0.0299 )	-0.0457 ( 0.0505 )
Month 2 (n= 9, 5, 2)	-0.0046 ( 0.0354 )	-0.0046 ( 0.0130 )	0.0115 ( 0.0049 )
Month 3 (n= 7, 5, 2)	-0.0249 ( 0.0310 )	-0.0112 ( 0.0251 )	0.0170 ( 0.0113 )
Month 6 (n= 8, 5, 2)	-0.0006 ( 0.0452 )	-0.0042 ( 0.0363 )	0.0200 ( 0.0382 )
Month 9 (n= 8, 3, 2)	0.0063 ( 0.0334 )	0.0070 ( 0.0171 )	0.0640 ( 0.0297 )
Month 12 (n= 8, 3, 2)	-0.0041 ( 0.0427 )	-0.0070 ( 0.0346 )	0.0240 ( 0.0113 )
Month 15 (n= 7, 3, 2)	-0.0264 ( 0.0601 )	-0.0343 ( 0.0191 )	0.0285 ( 0.0290 )
Month 18 (n= 7, 3, 1)	-0.0040 ( 0.0382 )	0.0027 ( 0.0380 )	0.0460 ( 99999 )
Month 21 (n= 7, 3, 0)	-0.0223 ( 0.0554 )	-0.0087 ( 0.0380 )	99999 ( 99999 )
Month 24 (n= 7, 3, 0)	-0.0123 ( 0.0711 )	-0.0093 ( 0.0186 )	99999 ( 99999 )
Month 27 (n= 7, 2, 0)	-0.0017 ( 0.0553 )	0.0150 ( 0.0127 )	99999 ( 99999 )
Month 30 (n= 5, 2, 1)	0.0016 ( 0.0524 )	0.0060 ( 0.0594 )	0.0300 ( 99999 )
Month 33 (n= 5, 3, 0)	-0.0302 ( 0.0446 )	-0.0093 ( 0.0234 )	99999 ( 99999 )
Month 36 (n= 5, 2, 0)	-0.0630 ( 0.0621 )	-0.0215 ( 0.0078 )	99999 ( 99999 )
Month 39 (n= 5, 3, 0)	-0.0340 ( 0.0860 )	-0.0133 ( 0.0291 )	99999 ( 99999 )
Month 42 (n= 5, 2, 0)	-0.0270 ( 0.0721 )	-0.0015 ( 0.0078 )	99999 ( 99999 )
Month 45 (n= 3, 1, 0)	-0.0423 ( 0.1189 )	-0.0050 ( 99999 )	99999 ( 99999 )
Final Study Visit (Month 49) (n= 8, 4, 1)	-0.0433 ( 0.0480 )	-0.0333 ( 0.0116 )	0.0100 ( 99999 )

No statistical analyses for this end point

Secondary: Change from Baseline in Hemoglobinuria Values at each time point

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End point title

Change from Baseline in Hemoglobinuria Values at each time point

End point description

Hemoglobinuria was assessed using a urine colorimetric scoring system with a score of 1 through 10 where 1 represents no hemoglobinuria and 10 represents maximum hemoglobinuria. Safety population included all participants who received at least 1 injection of zilucoplan on or after Day 1 of the extension study. Baseline was generally the final visit of the qualifying study (RA101495-01.201 or RA101495-01.203). Here, Number of participants analyzed included those participants who were evaluable for the assessment and 'n' (Number analyzed) signifies participants who were evaluable at specified time points. '99999' (n=0) signifies that the Mean and Standard Deviation (SD) was not calculated due to 0 participants and ‘99999’ (n=1) signifies that SD could not be calculated for a single participant.

End point type

Secondary

End point timeframe

Baseline, Month 1, 2, 3, 6, 9, 12, 15, 18, 21, 24, 27, 30, 33, 36, 39, 42, 45, 48 and Final Study Visit (Month 49)

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	9	6	3
Units: score on a scale
arithmetic mean (standard deviation)
Month 1 (n= 8, 6, 3)	0.1 ( 1.0 )	0.2 ( 1.5 )	1.7 ( 1.5 )
Month 2 (n= 9, 5, 2)	0.9 ( 1.4 )	0.8 ( 1.3 )	1.0 ( 1.4 )
Month 3 (n= 8, 5, 1)	0.4 ( 1.2 )	0.8 ( 1.3 )	0.0 ( 99999 )
Month 6 (n= 8, 5, 1)	0.4 ( 0.9 )	0.8 ( 1.3 )	0.0 ( 99999 )
Month 9 (n= 8, 2, 1)	0.4 ( 0.9 )	1.5 ( 2.1 )	0.0 ( 99999 )
Month 12 (n= 8, 3, 2)	0.9 ( 1.4 )	1.0 ( 1.7 )	1.0 ( 1.4 )
Month 15 (n= 7, 3, 2)	0.9 ( 1.1 )	1.0 ( 1.7 )	1.0 ( 1.4 )
Month 18 (n= 7, 3, 1)	0.1 ( 0.9 )	0.3 ( 0.6 )	0.0 ( 99999 )
Month 21 (n= 7, 3, 1)	0.7 ( 1.6 )	1.0 ( 1.7 )	0.0 ( 99999 )
Month 24 (n= 7, 3, 1)	0.6 ( 1.6 )	0.3 ( 0.6 )	0.0 ( 99999 )
Month 27 (n= 7, 2, 1)	0.7 ( 1.5 )	1.5 ( 2.1 )	0.0 ( 99999 )
Month 30 (n= 5, 2, 1)	0.6 ( 1.3 )	1.5 ( 2.1 )	0.0 ( 99999 )
Month 33 (n= 5, 3, 0)	1.4 ( 0.9 )	1.0 ( 1.7 )	99999 ( 99999 )
Month 36 (n= 5, 2, 0)	1.4 ( 1.9 )	1.5 ( 2.1 )	99999 ( 99999 )
Month 39 (n= 5, 3, 0)	0.4 ( 1.7 )	1.0 ( 1.7 )	99999 ( 99999 )
Month 42 (n= 5, 2, 0)	1.0 ( 1.2 )	1.5 ( 2.1 )	99999 ( 99999 )
Month 45 (n= 3, 1, 0)	1.0 ( 1.0 )	-1.0 ( 99999 )	99999 ( 99999 )
Month 48 (n= 0, 0, 0)	99999 ( 99999 )	99999 ( 99999 )	99999 ( 99999 )
Final Study Visit (Month 49) (n= 9, 5, 2)	0.4 ( 1.1 )	0.6 ( 0.9 )	2.5 ( 3.5 )

No statistical analyses for this end point

Secondary: Plasma concentrations of RA101495 and its major metabolite(s)

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End point title

Plasma concentrations of RA101495 and its major metabolite(s)

End point description

Blood samples of RA101495 (zilucoplan) and its metabolites (RA102758 and RA103488) were collected for Plasma concentration analysis. Pharmacokinetic (PK) population included all participants in the Safety population who had at least 1 plasma sample obtained for PK assessment. Here, 'n' signifies participants who were evaluable at specified time points. ‘99999’ (n=1) signifies that SD could not be calculated for a single participant.

End point type

Secondary

End point timeframe

Predose: At Day 1 (Screening), Month 1, 2, 3, 6, 9, 12, and Final Study Visit (Month 49)

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	9	6	3
Units: micrograms per litre (ug/L)
arithmetic mean (standard deviation)
RA101495- Day 1 (n= 9, 5, 3)	10999.99 ( 2698.29 )	13616.08 ( 1490.81 )	6976.50 ( 5663.23 )
RA101495- Month 1 (n= 9, 6, 3)	10879.13 ( 2405.19 )	12645.38 ( 1620.31 )	7630.03 ( 7060.56 )
RA101495- Month 2 (n= 9, 5, 2)	11276.17 ( 2896.98 )	12220.10 ( 2188.78 )	6865.45 ( 8108.18 )
RA101495- Month 3 (n= 8, 5, 2)	10806.17 ( 3418.92 )	12315.28 ( 2515.84 )	12430.00 ( 16.55 )
RA101495- Month 6 (n= 6, 5, 1)	9393.42 ( 2224.52 )	12218.72 ( 2166.05 )	12254.00 ( 99999 )
RA101495- Month 9 (n= 7, 3, 2)	11848.67 ( 2685.92 )	12282.83 ( 3064.42 )	15193.35 ( 2756.66 )
RA101495- Month 12 (n= 8, 3, 2)	11495.99 ( 2885.81 )	13279.97 ( 2148.60 )	12038.65 ( 7934.94 )
RA101495-Final Study Visit (Month 49) (n= 0, 0, 1)	99999 ( 99999 )	99999 ( 99999 )	7174.20 ( 99999 )
RA102758- Day 1 (n= 9, 5, 3)	1883.49 ( 593.93 )	2443.62 ( 560.97 )	1280.07 ( 1109.03 )
RA102758- Month 1 (n= 9, 6, 3)	1865.06 ( 594.31 )	2185.00 ( 631.37 )	757.30 ( 997.44 )
RA102758- Month 2 (n= 9, 5, 2)	1894.86 ( 608.46 )	2090.04 ( 831.80 )	757.85 ( 1018.59 )
RA102758- Month 3 (n= 8, 5, 2)	1758.55 ( 689.03 )	1990.54 ( 700.70 )	1954.05 ( 160.58 )
RA102758- Month 6 (n= 6, 5, 1)	1467.85 ( 563.68 )	1819.20 ( 613.14 )	1725.50 ( 99999 )
RA102758- Month 9 (n= 7, 3, 2)	1686.80 ( 554.87 )	1881.73 ( 583.87 )	1238.55 ( 166.24 )
RA102758- Month 12 (n= 8, 3, 1)	1646.99 ( 536.00 )	1954.23 ( 725.54 )	10.00 ( 99999 )
RA102758- Final Study Visit (Month 49) (n=0,0,1)	99999 ( 99999 )	99999 ( 99999 )	1094.60 ( 99999 )
RA103488- Day 1 (n= 9, 5, 3)	3587.68 ( 1747.12 )	4887.98 ( 1969.22 )	2084.83 ( 1791.35 )
RA103488- Month 1 (n= 9, 6, 3)	4344.99 ( 2319.10 )	4400.68 ( 1823.93 )	1703.73 ( 1605.96 )
RA103488- Month 2 (n= 9, 5, 2)	4799.29 ( 3113.57 )	4365.84 ( 1537.67 )	1591.35 ( 1552.03 )
RA103488- Month 3 (n= 8, 5, 2)	4191.36 ( 2347.65 )	4541.78 ( 1706.07 )	2715.60 ( 1345.48 )
RA103488- Month 6 (n= 6, 5, 1)	4027.53 ( 2730.92 )	4436.46 ( 2341.16 )	1929.60 ( 99999 )
RA103488- Month 9 (n= 7, 3, 2)	3132.54 ( 1320.61 )	4217.97 ( 2015.36 )	2954.85 ( 1754.97 )
RA103488- Month 12 (n= 8, 3, 2)	3903.41 ( 1960.30 )	4334.47 ( 1976.47 )	2319.20 ( 2534.84 )
RA103488- Final Study Visit (Month 49) (n=0,0,1)	99999 ( 99999 )	99999 ( 99999 )	2210.00 ( 99999 )

No statistical analyses for this end point

Secondary: Maximum plasma concentration (Cmax) of RA101495

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End point title

Maximum plasma concentration (Cmax) of RA101495

End point description

Cmax is the maximum plasma drug concentration. PK population included all participants in the Safety population who had at least 1 plasma sample obtained for PK assessment. Data was not collected and analyzed for this outcome measure due to change in planned analysis.

End point type

Secondary

End point timeframe

At Day 1, Month 1, 2, 3, 6, 9, and 12

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	0 ^[6]	0 ^[7]	0 ^[8]
Units: ug/L
geometric mean (geometric coefficient of variation)	( )	( )	( )

Notes
[6] - As per the change in planned analyses, maximum plasma concentration was not collected and analyzed.
[7] - As per the change in planned analyses, maximum plasma concentration was not collected and analyzed.
[8] - As per the change in planned analyses, maximum plasma concentration was not collected and analyzed.

No statistical analyses for this end point

Secondary: Time corresponding to Cmax (tmax) of RA101495

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End point title

Time corresponding to Cmax (tmax) of RA101495

End point description

tmax is the time to corresponding Cmax. PK population included all participants in the Safety population who had at least 1 plasma sample obtained for PK assessment. Data was not collected and analyzed for this outcome measure due to change in planned analysis.

End point type

Secondary

End point timeframe

At Day 1, Month 1, 2, 3, 6, 9, and 12

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	0 ^[9]	0 ^[10]	0 ^[11]
Units: hours (h)
median (full range (min-max))	( to )	( to )	( to )

Notes
[9] - As per the change in planned analyses, time corresponding to Cmax was not collected and analyzed.
[10] - As per the change in planned analyses, time corresponding to Cmax was not collected and analyzed.
[11] - As per the change in planned analyses, time corresponding to Cmax was not collected and analyzed.

No statistical analyses for this end point

Secondary: Area under the drug concentration-time curve (AUC0-t) of RA101495

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End point title

Area under the drug concentration-time curve (AUC0-t) of RA101495

End point description

AUC0-t is area under the drug concentration-time curves. PK population included all participants in the Safety population who had at least 1 plasma sample obtained for PK assessment. As per the change in planned analyses, samples/data were not collected, and AUC0-t not calculated.

End point type

Secondary

End point timeframe

At Day 1, Month 1, 2, 3, 6, 9, and 12

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	0 ^[12]	0 ^[13]	0 ^[14]
Units: hours*ug/L
geometric mean (geometric coefficient of variation)	( )	( )	( )

Notes
[12] - As per the change in planned analyses, samples/data were not collected, and AUC0-t not calculated.
[13] - As per the change in planned analyses, samples/data were not collected, and AUC0-t not calculated.
[14] - As per the change in planned analyses, samples/data were not collected, and AUC0-t not calculated.

No statistical analyses for this end point

Secondary: Total complement (CH50) Levels

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End point title

Total complement (CH50) Levels

End point description

Blood samples collection were planned to assess complement (CH50) levels. The planned analysis of CH50 was not performed because the CH50 assay was not able to be validated due to lack of reproducibility of the manufacturer’s kits. Pharmacodynamic (PD) population included all participants in the Safety population who had at least 1 plasma sample obtained for PD assessment. Data was not collected and analyzed for this outcome measure due to change in planned analysis.

End point type

Secondary

End point timeframe

At Day 1, Month 1, 2, 3, 6, 9, and 12

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	0 ^[15]	0 ^[16]	0 ^[17]
Units: ug/mL
arithmetic mean (standard deviation)	( )	( )	( )

Notes
[15] - As per the change in planned analyses, CH50 levels were not collected and analyzed.
[16] - As per the change in planned analyses, CH50 levels were not collected and analyzed.
[17] - As per the change in planned analyses, CH50 levels were not collected and analyzed.

No statistical analyses for this end point

Secondary: Change from Baseline in Sheep Red Blood Cell (sRBC) Values at each time point

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End point title

Change from Baseline in Sheep Red Blood Cell (sRBC) Values at each time point

End point description

Blood samples were collected for measurement of sRBC lysis for the Classical Complement Pathways. PD population included all participants in the Safety population who had at least 1 plasma sample obtained for PD assessment. Here, Number of participants analyzed included those participants who were evaluable for the assessment and 'n' signifies participants who were evaluable at specified time points. '99999' (n=0) signifies that the Mean and SD was not calculated due to 0 participants and ‘99999’ (n=1) signifies that SD could not be calculated for a single participant.

End point type

Secondary

End point timeframe

Baseline, Month 1, 2, 3, 6, 9, 12 and Final Study Visit (Month 49)

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	9	6	1
Units: percent lysis of sheep erythrocytes
arithmetic mean (standard deviation)
Month 1 (n= 9, 6,1)	1.378 ( 2.277 )	0.523 ( 0.772 )	93.870 ( 99999 )
Month 2 (n= 9, 5,1)	1.248 ( 1.789 )	-0.308 ( 0.452 )	93.870 ( 99999 )
Month 3 (n= 8, 5, 1)	1.256 ( 1.799 )	0.576 ( 0.972 )	-2.620 ( 99999 )
Month 6 (n= 6, 5, 1)	1.493 ( 2.838 )	0.458 ( 1.657 )	-2.300 ( 99999 )
Month 9 (n= 7, 3, 1)	0.683 ( 1.055 )	0.757 ( 0.673 )	-1.410 ( 99999 )
Month 12 (n= 8, 3, 1)	0.759 ( 0.557 )	0.773 ( 0.415 )	8.390 ( 99999 )
Final Study Visit (Month 49) (n= 0, 2, 0)	99999 ( 99999 )	25.230 ( 35.200 )	99999 ( 99999 )

No statistical analyses for this end point

Secondary: Change from Baseline in Wieslab enzyme-linked immunosorbent assay (ELISA) Values for alternative complement pathway at each time point

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End point title

Change from Baseline in Wieslab enzyme-linked immunosorbent assay (ELISA) Values for alternative complement pathway at each time point

End point description

Blood samples were collected for measurement of membrane attack complex (MAC) by Wieslab ELISA for alternative complement pathway. PD population included all participants in the Safety population who had at least 1 plasma sample obtained for PD assessment. Here, Number of participants analyzed included those participants who were evaluable for the assessment and 'n' signifies participants who were evaluable at specified time points. '99999' (n=0) signifies that the Mean and SD was not calculated due to 0 participants and ‘99999’ (n=1) signifies that SD could not be calculated for a single participant.

End point type

Secondary

End point timeframe

Baseline, Month 1, 2, 3, 6, 9, 12 and Final Study Visit (Month 49)

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	9	6	2
Units: percentage of activity
arithmetic mean (standard deviation)
Month 1 (n= 9, 6, 2)	1.7 ( 5.8 )	1.0 ( 1.7 )	48.0 ( 67.9 )
Month 2 (n= 9, 5, 2)	0.1 ( 1.9 )	-1.0 ( 1.0 )	51.5 ( 74.2 )
Month 3 (n= 8, 5, 2)	0.1 ( 2.0 )	0.0 ( 0.7 )	2.0 ( 1.4 )
Month 6 (n= 6, 5, 1)	1.0 ( 4.5 )	-0.2 ( 1.9 )	5.0 ( 99999 )
Month 9 (n= 8, 3, 1)	-0.9 ( 0.8 )	-0.7 ( 0.6 )	-2.0 ( 99999 )
Month 12 (n= 8, 3, 2)	-1.4 ( 1.4 )	-1.3 ( 0.6 )	4.5 ( 6.4 )
Final Study Visit (Month 49) (n= 0, 2, 0)	99999 ( 99999 )	1.0 ( 2.8 )	99999 ( 99999 )

No statistical analyses for this end point

Secondary: Change from Baseline in Complement Component 5 (C5) Values at each time point

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End point title

Change from Baseline in Complement Component 5 (C5) Values at each time point

End point description

Blood samples were collected for measurement of Complement component 5 (C5) levels. PD population included all participants in the Safety population who had at least 1 plasma sample obtained for PD assessment. Here, Number of participants analyzed included those participants who were evaluable for the assessment and 'n' signifies participants who were evaluable at specified time points. '99999' (n=0) signifies that the Mean and SD was not calculated due to 0 participants and ‘99999’ (n=1) signifies that SD could not be calculated for a single participant.

End point type

Secondary

End point timeframe

Baseline, Month 1, 2, 3, 6, 9, 12 and Final Study Visit (Month 49)

End point values	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan-Cohort B (Eculizumab Switch)	Zilucoplan (Inadequate Responder to Eculizumab)
Number of subjects analysed	9	6	2
Units: ug/mL
arithmetic mean (standard deviation)
Month 1 (n= 9, 6, 2)	-11.231 ( 24.960 )	20.488 ( 31.024 )	-27.505 ( 90.092 )
Month 2 (n= 9, 5, 2)	-15.914 ( 32.737 )	17.716 ( 33.125 )	16.310 ( 36.077 )
Month 3 (n= 8, 5, 2)	-24.404 ( 50.084 )	-2.898 ( 49.747 )	22.355 ( 19.764 )
Month 6 (n= 6, 5, 1)	-6.823 ( 44.787 )	9.572 ( 24.927 )	91.640 ( 99999 )
Month 9 (n= 8, 3, 1)	-0.019 ( 53.475 )	1.177 ( 27.654 )	89.670 ( 99999 )
Month 12 (n= 7, 3, 2)	-40.591 ( 34.977 )	-23.487 ( 30.911 )	-24.905 ( 17.685 )
Final Study Visit (Month 49) (n= 3, 3, 0)	-28.663 ( 46.526 )	-19.770 ( 74.604 )	99999 ( 99999 )

No statistical analyses for this end point

Adverse events

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Timeframe for reporting adverse events

From Day 1 until the Final Study Visit (up to Month 49)

Adverse event reporting additional description

TEAEs were reported for Safety population. Deaths and TEAEs were monitored together for each cohort regardless of dose administered.

Assessment type

Non-systematic

Dictionary name

MedDRA

Dictionary version

23.0

Reporting group title

Zilucoplan-Cohort A (Eculizumab Naïve)

Reporting group description

Reporting group title

Zilucoplan (Inadequate Responder to Eculizumab)

Reporting group description

Reporting group title

Zilucoplan-Cohort B (Eculizumab Switch)

Reporting group description

Serious adverse events	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan (Inadequate Responder to Eculizumab)	Zilucoplan-Cohort B (Eculizumab Switch)
Total subjects affected by serious adverse events
subjects affected / exposed	1 / 10 (10.00%)	2 / 3 (66.67%)	3 / 6 (50.00%)
number of deaths (all causes)	0	0	0
number of deaths resulting from adverse events	0	0	0
Vascular disorders
Deep vein thrombosis
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0
Nervous system disorders
Encephalopathy
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences causally related to treatment / all	0 / 0	0 / 1	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0
Headache
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences causally related to treatment / all	1 / 1	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0
Blood and lymphatic system disorders
Anaemia
subjects affected / exposed	1 / 10 (10.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences causally related to treatment / all	0 / 1	0 / 1	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0
Gastrointestinal disorders
Tongue haematoma
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0
Nausea
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences causally related to treatment / all	1 / 1	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0
Psychiatric disorders
Suicide attempt
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences causally related to treatment / all	0 / 0	0 / 1	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0
Musculoskeletal and connective tissue disorders
Osteoarthritis
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences causally related to treatment / all	0 / 1	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0
Rotator cuff syndrome
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences causally related to treatment / all	0 / 1	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0
Infections and infestations
Enterocolitis infectious
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0
Pneumonia pneumococcal
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences causally related to treatment / all	0 / 0	0 / 1	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0

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

Non-serious adverse events	Zilucoplan-Cohort A (Eculizumab Naïve)	Zilucoplan (Inadequate Responder to Eculizumab)	Zilucoplan-Cohort B (Eculizumab Switch)
Total subjects affected by non serious adverse events
subjects affected / exposed	9 / 10 (90.00%)	2 / 3 (66.67%)	6 / 6 (100.00%)
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
Basal cell carcinoma
subjects affected / exposed	2 / 10 (20.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	3	0	0
Vascular disorders
Hypertension
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Lymphoedema
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
General disorders and administration site conditions
Chest discomfort
subjects affected / exposed	2 / 10 (20.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	2	0	0
Pyrexia
subjects affected / exposed	3 / 10 (30.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	3	0	0
Injection site bruising
subjects affected / exposed	2 / 10 (20.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	2	0	1
Fatigue
subjects affected / exposed	4 / 10 (40.00%)	1 / 3 (33.33%)	2 / 6 (33.33%)
occurrences all number	9	1	3
Chest pain
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	0	1	0
Injection site haematoma
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Influenza like illness
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	0	1	0
Chills
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Immune system disorders
Seasonal allergy
subjects affected / exposed	2 / 10 (20.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	3	0	0
Alloimmunisation
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Drug hypersensitivity
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	0	0	1
Respiratory, thoracic and mediastinal disorders
Oropharyngeal pain
subjects affected / exposed	3 / 10 (30.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	4	0	0
Dyspnoea
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Cough
subjects affected / exposed	2 / 10 (20.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	2	1	0
Laryngospasm
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Pleural effusion
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Psychiatric disorders
Depression
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	1 / 6 (16.67%)
occurrences all number	0	2	1
Insomnia
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Investigations
Alanine aminotransferase increased
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	0	1	0
Aspartate aminotransferase increased
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	0	1	0
Weight decreased
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
International normalised ratio increased
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	0	1	0
Grip strength decreased
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Injury, poisoning and procedural complications
Contusion
subjects affected / exposed	2 / 10 (20.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	3	0	0
Post vaccination syndrome
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	2	0	0
Animal bite
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Bone contusion
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Eye contusion
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	0	0	1
Fall
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	0	0	1
Post-traumatic pain
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	0	0	1
Foot fracture
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Limb injury
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Tooth fracture
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Traumatic haematoma
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	0	0	1
Cardiac disorders
Bradycardia
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Nervous system disorders
Dizziness
subjects affected / exposed	2 / 10 (20.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	4	0	0
Headache
subjects affected / exposed	2 / 10 (20.00%)	1 / 3 (33.33%)	2 / 6 (33.33%)
occurrences all number	4	2	6
Sensory disturbance
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Amnesia
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	0	1	0
Blood and lymphatic system disorders
Anaemia
subjects affected / exposed	2 / 10 (20.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	4	0	0
Pancytopenia
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	0	0	1
Aplastic anaemia
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	0	0	2
Haemolysis
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	1	0	1
Ear and labyrinth disorders
Tinnitus
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Eye disorders
Lacrimation increased
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	0	0	1
Gastrointestinal disorders
Diarrhoea
subjects affected / exposed	5 / 10 (50.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	8	0	1
Abdominal pain
subjects affected / exposed	3 / 10 (30.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	7	0	0
Nausea
subjects affected / exposed	4 / 10 (40.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	5	0	0
Constipation
subjects affected / exposed	1 / 10 (10.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	1	1	0
Abdominal pain upper
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Abdominal discomfort
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Abdominal distension
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	2	0	0
Gastrooesophageal reflux disease
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Large intestine polyp
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Oral discomfort
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Rectal polyp
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Rectal haemorrhage
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Oral pain
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Retching
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Vomiting
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	0	1	0
Hepatobiliary disorders
Cholelithiasis
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Skin and subcutaneous tissue disorders
Psoriasis
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	0	0	1
Actinic keratosis
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Pruritus
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	2	0	0
Rash
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Rash pruritic
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Urticaria
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Renal and urinary disorders
Paroxysmal nocturnal haemoglobinuria
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	3	0	0
Chromaturia
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Musculoskeletal and connective tissue disorders
Back pain
subjects affected / exposed	3 / 10 (30.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	9	1	0
Muscle spasms
subjects affected / exposed	2 / 10 (20.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	6	0	0
Arthralgia
subjects affected / exposed	1 / 10 (10.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	1	1	0
Myalgia
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	1	0	1
Joint swelling
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	0	0	1
Arthritis
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Pain in extremity
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	2	0	0
Limb discomfort
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Musculoskeletal pain
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	0	0	1
Muscle tightness
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Plantar fasciitis
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Rotator cuff syndrome
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Infections and infestations
Nasopharyngitis
subjects affected / exposed	4 / 10 (40.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	10	0	2
Upper respiratory tract infection
subjects affected / exposed	4 / 10 (40.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	5	0	1
Bronchitis
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	2	0	0
Viral infection
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	1	0	1
Sinusitis
subjects affected / exposed	1 / 10 (10.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	1	1	0
Pharyngitis
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	1	0	1
Influenza
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	2	0	0
Rhinitis
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	2	0	0
Cystitis
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Ear infection
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Gastroenteritis
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Gastrointestinal infection
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Hordeolum
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Infection
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Oral candidiasis
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Oral herpes
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Respiratory tract infection
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	0	1	0
Skin bacterial infection
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Skin infection
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Tooth abscess
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Urinary tract infection
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Metabolism and nutrition disorders
Hyperkalaemia
subjects affected / exposed	1 / 10 (10.00%)	0 / 3 (0.00%)	0 / 6 (0.00%)
occurrences all number	1	0	0
Vitamin D deficiency
subjects affected / exposed	0 / 10 (0.00%)	0 / 3 (0.00%)	1 / 6 (16.67%)
occurrences all number	0	0	1
Hypokalaemia
subjects affected / exposed	0 / 10 (0.00%)	1 / 3 (33.33%)	0 / 6 (0.00%)
occurrences all number	0	1	0

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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

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Clinical trials

Clinical Trial Results: A Multicenter, Open-Label, Uncontrolled, Extension Study of RA101495 in Subjects with Paroxysmal Nocturnal Hemoglobinuria who have Completed a RA101495 Clinical Study

Trial information

Trial information

Subject disposition

Subject disposition

Baseline characteristics

Baseline characteristics

End points

End points

Primary: Percentage of participants with Treatment Emergent Adverse events (TEAEs)

Primary: Percentage of participants with Treatment Emergent Adverse events (TEAEs)

Primary: Percentage of participants with Serious TEAEs

Primary: Percentage of participants with Serious TEAEs

Secondary: Number of participants with anti-drug antibodies (ADA)

Secondary: Number of participants with anti-drug antibodies (ADA)

Secondary: Change from Baseline in Serum Lactate Dehydrogenase (LDH) Levels at each time point

Secondary: Change from Baseline in Serum Lactate Dehydrogenase (LDH) Levels at each time point

Secondary: Change from Baseline in Total Bilirubin Values at each time point

Secondary: Change from Baseline in Total Bilirubin Values at each time point

Secondary: Change from Baseline in Total Hemoglobin Values at each time point

Secondary: Change from Baseline in Total Hemoglobin Values at each time point

Secondary: Change from Baseline in Free Hemoglobin Values at each time point

Secondary: Change from Baseline in Free Hemoglobin Values at each time point

Secondary: Change from Baseline in Haptoglobin Values at each time point

Secondary: Change from Baseline in Haptoglobin Values at each time point

Secondary: Change from Baseline in Reticulocytes Values at each time point

Secondary: Change from Baseline in Reticulocytes Values at each time point

Secondary: Change from Baseline in Hemoglobinuria Values at each time point

Secondary: Change from Baseline in Hemoglobinuria Values at each time point

Secondary: Plasma concentrations of RA101495 and its major metabolite(s)

Secondary: Plasma concentrations of RA101495 and its major metabolite(s)

Secondary: Maximum plasma concentration (Cmax) of RA101495

Secondary: Maximum plasma concentration (Cmax) of RA101495

Secondary: Time corresponding to Cmax (tmax) of RA101495

Secondary: Time corresponding to Cmax (tmax) of RA101495

Secondary: Area under the drug concentration-time curve (AUC0-t) of RA101495

Secondary: Area under the drug concentration-time curve (AUC0-t) of RA101495

Secondary: Total complement (CH50) Levels

Secondary: Total complement (CH50) Levels

Secondary: Change from Baseline in Sheep Red Blood Cell (sRBC) Values at each time point

Secondary: Change from Baseline in Sheep Red Blood Cell (sRBC) Values at each time point

Secondary: Change from Baseline in Wieslab enzyme-linked immunosorbent assay (ELISA) Values for alternative complement pathway at each time point

Secondary: Change from Baseline in Wieslab enzyme-linked immunosorbent assay (ELISA) Values for alternative complement pathway at each time point

Secondary: Change from Baseline in Complement Component 5 (C5) Values at each time point

Secondary: Change from Baseline in Complement Component 5 (C5) Values at each time point

Adverse events

Adverse events

More information

Substantial protocol amendments (globally)

Interruptions (globally)

Limitations and caveats

More information

Clinical Trial Results:
A Multicenter, Open-Label, Uncontrolled, Extension Study of RA101495 in Subjects with Paroxysmal Nocturnal Hemoglobinuria who have Completed a RA101495 Clinical Study