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Clinical Trial Results:
Immunogenicity and safety study of GSK Biologicals’ meningococcal vaccine 134612 with or without co-administration of Cervarix and Boostrix in female adolescents and young adults at 9-25 years of age

Summary
EudraCT number	2012-001876-13
Trial protocol	EE
Global end of trial date	29 Apr 2014

Results information
Results version number	v2
This version publication date	15 Sep 2017
First version publication date	17 Jun 2017
Other versions	v1 , v3
Version creation reason	Correction of full data set Correction to Safety section

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

113823

ISRCTN number

US NCT number

NCT01755689

WHO universal trial number (UTN)

Sponsor organisation name

GlaxoSmithKline Biologicals

Sponsor organisation address

Rue de l’Institut 89, Rixensart, Belgium, B-1330

Public contact

Clinical Trials Call Center, GlaxoSmithKline Biologicals, 044 2089-904466, GSKClinicalSupportHD@gsk.com

Scientific contact

Clinical Trials Call Center, GlaxoSmithKline Biologicals, 044 2089-904466, GSKClinicalSupportHD@gsk.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?

Yes

Analysis stage

Final

Date of interim/final analysis

25 May 2017

Is this the analysis of the primary completion data?

Global end of trial reached?

Yes

Global end of trial date

29 Apr 2014

Was the trial ended prematurely?

Main objective of the trial

To demonstrate the non-inferiority of MenACWY-TT conjugate vaccine co-administered with HPV-16/18 L1 AS04 compared to MenACWY-TT alone with respect to Serum Bactericidal Assay using rabbit complement (rSBA) geometric mean titres (GMTs) for serogroups A, C, W-135 and Y one month after vaccination. To demonstrate the non-inferiority of HPV-16/18 L1 AS04 co-administered with MenACWY-TT compared to HPV-16/18 L1 AS04 alone in terms of HPV16 and HPV18 GMTs as measured by ELISA one month after the third dose of HPV-16/18 L1 AS04. To demonstrate the non-inferiority of MenACWY-TT co-administered with HPV-16/18 L1 AS04 and Tdap compared to MenACWY-TT alone with respect to rSBA GMTs for serogroups A, C, W-135 and Y one month after vaccination. To demonstrate the non-inferiority of HPV-16/18 L1 AS04 co-administered with MenACWY-TT and Tdap compared to HPV-16/18 L1 AS04 co-administered with Tdap in terms of HPV16 and HPV18 GMTs as measured by ELISA one month after the third dose of HPV-16

Protection of trial subjects

All subjects were supervised after vaccination/product administration with appropriate medical treatment readily available. Vaccines were administered by qualified and trained personnel. Vaccines were administered only to eligible subjects that had no contraindications to any components of the vaccines.

Background therapy

Evidence for comparator

Actual start date of recruitment

01 Nov 2013

Long term follow-up planned

Independent data monitoring committee (IDMC) involvement?

Number of subjects enrolled per country

Country: Number of subjects enrolled

Dominican Republic: 435

Country: Number of subjects enrolled

Estonia: 435

Country: Number of subjects enrolled

Thailand: 430

Worldwide total number of subjects

1300

EEA total number of subjects

435

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)

153

Adolescents (12-17 years)

606

Adults (18-64 years)

541

From 65 to 84 years

85 years and over

Subject disposition

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Recruitment details

Screening details

During the screening the following steps occurred: check for inclusion/exclusion criteria, contraindications/precautions, medical history of the subjects and signing informed consent forms.

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

Nimenrix+Cervarix (1,2,7-Month) Group

Arm description

Subjects in this group received 1 dose of Nimenrix vaccine at Month 0 and 3 doses of Cervarix vaccine at Month 1, Month 2 and Month 7. Both vaccines were administered intramuscularly (IM) in the deltoid region of the arm.

Arm type

Experimental

Investigational medicinal product name

Cervarix

Investigational medicinal product code

Other name

Pharmaceutical forms

Suspension for injection in pre-filled syringe

Routes of administration

Intramuscular use

Dosage and administration details

3 doses of Cervarix vaccine at Month 0, Month 1 and Month 6/7, administered intramuscularly (IM) in the deltoid region of the arm.

Investigational medicinal product name

Nimenrix

Investigational medicinal product code

Other name

Pharmaceutical forms

Powder and solvent for solution for injection

Routes of administration

Intramuscular use

Dosage and administration details

1 dose of Nimenrix vaccine at Month 0, administered intramuscularly (IM) in the deltoid region of the arm.

Nimenrix+Cervarix (0,1,6-Month) Group

Arm description

Subjects in this group received 1 dose of Nimenrix vaccine at Month 0 and 3 doses of Cervarix vaccine at Month 0, Month 1 and Month 6. Both vaccines were administered intramuscularly (IM) in the deltoid region of the arm.

Arm type

Experimental

Investigational medicinal product name

Cervarix

Investigational medicinal product code

Other name

Pharmaceutical forms

Suspension for injection in pre-filled syringe

Routes of administration

Intramuscular use

Dosage and administration details

3 doses of Cervarix vaccine at Month 0, Month 1 and Month 6/7, administered intramuscularly (IM) in the deltoid region of the arm.

Investigational medicinal product name

Nimenrix

Investigational medicinal product code

Other name

Pharmaceutical forms

Powder and solvent for solution for injection

Routes of administration

Intramuscular use

Dosage and administration details

1 dose of Nimenrix vaccine at Month 0, administered intramuscularly (IM) in the deltoid region of the arm.

Cervarix Group

Arm description

Subjects in this group received 3 doses of Cervarix vaccine at Month 0, Month 1 and Month 6, administered intramuscularly (IM) in the deltoid region of the arm.

Arm type

Active comparator

Investigational medicinal product name

Cervarix

Investigational medicinal product code

Other name

Pharmaceutical forms

Suspension for injection in pre-filled syringe

Routes of administration

Intramuscular use

Dosage and administration details

3 doses of Cervarix vaccine at Month 0, Month 1 and Month 6/7, administered intramuscularly (IM) in the deltoid region of the arm.

Nimenrix+Cervarix+Boostrix Group

Arm description

Subjects in this group received 1 dose each of Nimenrix and Boostrix vaccines at Month 0 and 3 doses of Cervarix vaccine at Month 0, Month 1 and Month 6. All vaccines were administered intramuscularly (IM) in the deltoid region of the arm.

Arm type

Experimental

Investigational medicinal product name

Nimenrix

Investigational medicinal product code

Other name

Pharmaceutical forms

Powder and solvent for solution for injection

Routes of administration

Intramuscular use

Dosage and administration details

1 dose of Nimenrix vaccine at Month 0, administered intramuscularly (IM) in the deltoid region of the arm.

Investigational medicinal product name

Cervarix

Investigational medicinal product code

Other name

Pharmaceutical forms

Suspension for injection in pre-filled syringe

Routes of administration

Intramuscular use

Dosage and administration details

3 doses of Cervarix vaccine at Month 0, Month 1 and Month 6/7, administered intramuscularly (IM) in the deltoid region of the arm.

Investigational medicinal product name

Boostrix

Investigational medicinal product code

Other name

Pharmaceutical forms

Suspension for injection

Routes of administration

Intramuscular use

Dosage and administration details

1 dose of Boostrix vaccine at Month 0, administered intramuscularly (IM) in the deltoid region of the arm.

Boostrix+Cervarix Group

Arm description

Subjects in this group received 1 dose of Boostrix vaccine at Month 0 and 3 doses of Cervarix vaccine at Month 0, Month 1 and Month 6. Both vaccines were administered intramuscularly (IM) in the deltoid region of the arm.

Arm type

Active comparator

Investigational medicinal product name

Boostrix

Investigational medicinal product code

Other name

Pharmaceutical forms

Suspension for injection

Routes of administration

Intramuscular use

Dosage and administration details

1 dose of Boostrix vaccine at Month 0, administered intramuscularly (IM) in the deltoid region of the arm.

Investigational medicinal product name

Cervarix

Investigational medicinal product code

Other name

Pharmaceutical forms

Suspension for injection in pre-filled syringe

Routes of administration

Intramuscular use

Dosage and administration details

3 doses of Cervarix vaccine at Month 0, Month 1 and Month 6/7, administered intramuscularly (IM) in the deltoid region of the arm.

Number of subjects in period 1	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Started	259	259	261	260	261
Completed	256	254	255	254	255
Not completed	3	5	6	6	6
Consent withdrawn by subject	1	3	2	1	1
Migrated/moved from study area	-	1	1	1	1
Unspecified	1	1	2	4	2
Lost to follow-up	1	-	1	-	2

Baseline characteristics

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Reporting group title

Nimenrix+Cervarix (1,2,7-Month) Group

Reporting group description

Reporting group title

Nimenrix+Cervarix (0,1,6-Month) Group

Reporting group description

Reporting group title

Cervarix Group

Reporting group description

Subjects in this group received 3 doses of Cervarix vaccine at Month 0, Month 1 and Month 6, administered intramuscularly (IM) in the deltoid region of the arm.

Reporting group title

Nimenrix+Cervarix+Boostrix Group

Reporting group description

Reporting group title

Boostrix+Cervarix Group

Reporting group description

Reporting group values	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group	Total
Number of subjects	259	259	261	260	261
Age categorical
Units: Subjects
Age continuous
Units: years
arithmetic mean (standard deviation)	16.3 ( 4.6 )	16.6 ( 4.4 )	16.6 ( 4.6 )	16.6 ( 4.6 )	16.6 ( 4.5 )	-
Gender categorical
Units:
Male	0	0	0	0	0	0
Female	259	259	261	260	261	1300
Race/Ethnicity, Customized
Units: Subjects
African Heritage / African American	0	0	0	1	0	1
Asian - South East Asian Heritage	86	86	86	86	86	430
Other	86	87	88	86	87	434
White - Caucasian / European Heritage	87	86	87	87	88	435

End points

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Reporting group title

Nimenrix+Cervarix (1,2,7-Month) Group

Reporting group description

Reporting group title

Nimenrix+Cervarix (0,1,6-Month) Group

Reporting group description

Reporting group title

Cervarix Group

Reporting group description

Subjects in this group received 3 doses of Cervarix vaccine at Month 0, Month 1 and Month 6, administered intramuscularly (IM) in the deltoid region of the arm.

Reporting group title

Nimenrix+Cervarix+Boostrix Group

Reporting group description

Reporting group title

Boostrix+Cervarix Group

Reporting group description

Primary: Anti-Meningitis antibody titers by serum bactericidal assay using rabbit complement (rSBA)

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End point title

Anti-Meningitis antibody titers by serum bactericidal assay using rabbit complement (rSBA) ^[1]

End point description

The analysis was performed for the serogroups -MenA, -MenC -MenW-135 and -MenY. Antibody titers, tabulated as geometric mean titers (GMTs), were obtained by serum bactericidal assay using rabbit complement. This analysis was only performed on groups receiving Nimenrix vaccine.

End point type

Primary

End point timeframe

At one month after vaccination with Nimenrix (Month 1)

Notes
[1] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Nimenrix vaccine.

End point values	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Nimenrix+Cervarix+Boostrix Group
Number of subjects analysed	256	255	257
Units: Titers
geometric mean (confidence interval 95%)
rSBA-MenA	5517.1 (4791.4 to 6352.6)	5523.5 (4913.2 to 6209.6)	4649.6 (4022.8 to 5374)
rSBA-MenC	4277.3 (3604.3 to 5076.1)	5091 (4338.6 to 5973.8)	3598.6 (3004.2 to 4310.7)
rSBA-MenW-135	14782.1 (12254.2 to 17831.5)	18068.3 (15381.6 to 21224.4)	11663.6 (9336.8 to 14570.2)
rSBA-MenY	11871 (10542.3 to 13367.2)	12758.9 (11569.6 to 14070.5)	11201.2 (9678.7 to 12963.1)

Statistical analysis 1

Statistical analysis description

Adjusted GMT ratio of the Nimenrix Group versus Nimenrix+Cervarix+Boostrix Group in terms of rSBA-MenA titers.

Comparison groups

Nimenrix+Cervarix+Boostrix Group v Nimenrix+Cervarix (1,2,7-Month) Group

Number of subjects included in analysis

513

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[2]

Method

ANCOVA

Parameter type

Adjusted GMT Ratio

Point estimate

1.19

Confidence interval

level

95%

sides

2-sided

lower limit

0.99

upper limit

1.43

Notes
[2] - The non-inferiority criteria: the UL of the 2-sided standardised asymptotic 95% CI for the ratio of rSBA GMTs had to be below the pre-defined limit of 2.

Statistical analysis 2

Statistical analysis description

Adjusted GMT ratio of the Nimenrix Group versus Nimenrix+Cervarix Group in terms of rSBA-MenA titers.

Comparison groups

Nimenrix+Cervarix (1,2,7-Month) Group v Nimenrix+Cervarix (0,1,6-Month) Group

Number of subjects included in analysis

511

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[3]

Method

ANCOVA

Parameter type

Adjusted GMT Ratio

Point estimate

1.01

Confidence interval

level

95%

sides

2-sided

lower limit

0.83

upper limit

1.21

Notes
[3] - The non-inferiority criteria: the UL of the 2-sided standardised asymptotic 95% CI for the ratio of rSBA GMTs had to be below the pre-defined limit of 2.

Statistical analysis 3

Statistical analysis description

Adjusted GMT ratio of the Nimenrix Group versus Nimenrix+Cervarix+Boostrix Group in terms of rSBA-MenC titers.

Comparison groups

Nimenrix+Cervarix+Boostrix Group v Nimenrix+Cervarix (1,2,7-Month) Group

Number of subjects included in analysis

513

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[4]

Method

ANCOVA

Parameter type

Adjusted GMT Ratio

Point estimate

1.19

Confidence interval

level

95%

sides

2-sided

lower limit

0.93

upper limit

1.51

Notes
[4] - The non-inferiority criteria: the UL of the 2-sided standardised asymptotic 95% CI for the ratio of rSBA GMTs had to be below the pre-defined limit of 2.

Statistical analysis 4

Statistical analysis description

Adjusted GMT ratio of the Nimenrix Group versus Nimenrix+Cervarix Group in terms of rSBA-MenC titers.

Comparison groups

Nimenrix+Cervarix (1,2,7-Month) Group v Nimenrix+Cervarix (0,1,6-Month) Group

Number of subjects included in analysis

511

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[5]

Method

ANCOVA

Parameter type

Adjusted GMT Ratio

Point estimate

0.83

Confidence interval

level

95%

sides

2-sided

lower limit

0.66

upper limit

1.06

Notes
[5] - The non-inferiority criteria: the UL of the 2-sided standardised asymptotic 95% CI for the ratio of rSBA GMTs had to be below the pre-defined limit of 2.

Statistical analysis 5

Statistical analysis description

Adjusted GMT ratio of the Nimenrix Group versus Nimenrix+Cervarix+Boostrix Group in terms of rSBA-MenW-135 titers.

Comparison groups

Nimenrix+Cervarix+Boostrix Group v Nimenrix+Cervarix (1,2,7-Month) Group

Number of subjects included in analysis

513

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[6]

Method

ANCOVA

Parameter type

Adjusted GMT Ratio

Point estimate

1.26

Confidence interval

level

95%

sides

2-sided

lower limit

0.97

upper limit

1.64

Notes
[6] - The non-inferiority criteria: the UL of the 2-sided standardised asymptotic 95% CI for the ratio of rSBA GMTs had to be below the pre-defined limit of 2.

Statistical analysis 6

Statistical analysis description

Adjusted GMT ratio of the Nimenrix Group versus Nimenrix+Cervarix Group in terms of rSBA-MenW-135 titers.

Comparison groups

Nimenrix+Cervarix (1,2,7-Month) Group v Nimenrix+Cervarix (0,1,6-Month) Group

Number of subjects included in analysis

511

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[7]

Method

ANCOVA

Parameter type

Adjusted GMT Ratio

Point estimate

0.82

Confidence interval

level

95%

sides

2-sided

lower limit

0.63

upper limit

1.07

Notes
[7] - The non-inferiority criteria: the UL of the 2-sided standardised asymptotic 95% CI for the ratio of rSBA GMTs had to be below the pre-defined limit of 2.

Statistical analysis 7

Statistical analysis description

Adjusted GMT ratio of the Nimenrix Group versus Nimenrix+Cervarix+Boostrix Group in terms of rSBA-MenY titers.

Comparison groups

Nimenrix+Cervarix+Boostrix Group v Nimenrix+Cervarix (1,2,7-Month) Group

Number of subjects included in analysis

513

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[8]

Method

ANCOVA

Parameter type

Adjusted GMT Ratio

Point estimate

1.05

Confidence interval

level

95%

sides

2-sided

lower limit

0.89

upper limit

1.25

Notes
[8] - The non-inferiority criteria: the UL of the 2-sided standardised asymptotic 95% CI for the ratio of rSBA GMTs had to be below the pre-defined limit of 2.

Statistical analysis 8

Statistical analysis description

Adjusted GMT ratio of the Nimenrix Group versus Nimenrix+Cervarix Group in terms of rSBA-MenY titers.

Comparison groups

Nimenrix+Cervarix (1,2,7-Month) Group v Nimenrix+Cervarix (0,1,6-Month) Group

Number of subjects included in analysis

511

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[9]

Method

ANCOVA

Parameter type

Adjusted GMT Ratio

Point estimate

0.95

Confidence interval

level

95%

sides

2-sided

lower limit

0.8

upper limit

1.12

Notes
[9] - The non-inferiority criteria: the UL of the 2-sided standardised asymptotic 95% CI for the ratio of rSBA GMTs had to be below the pre-defined limit of 2.

Primary: Anti-HPV-16 and anti-HPV-18 concentrations

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End point title

Anti-HPV-16 and anti-HPV-18 concentrations ^[10]

End point description

The antibody concentrations were calculated as geometric mean concentrations (GMCs) and expressed as ELISA units per milliliter (EU/mL).

End point type

Primary

End point timeframe

At one month after the third dose of Cervarix (Month 7)

Notes
[10] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Cervarix vaccine.

End point values	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	248	249	244	247
Units: EU/mL
geometric mean (confidence interval 95%)
Anti-HPV-16	12124.9 (10564.5 to 13915.7)	11672.1 (10173.5 to 13391.4)	9563.8 (8262 to 11070.7)	11470.7 (10018.5 to 13133.5)
Anti-HPV-18	5234.1 (4573.9 to 5989.6)	5655 (4978.5 to 6423.4)	4306.2 (3748.3 to 4947.1)	5110 (4487 to 5819.6)

Statistical analysis 1

Statistical analysis description

Adjusted GMT ratio of the Cervarix Group versus Nimenrix+Cervarix (0,1,6-Month) Group in terms of HPV-16 titers.

Comparison groups

Cervarix Group v Nimenrix+Cervarix (0,1,6-Month) Group

Number of subjects included in analysis

497

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[11]

Method

ANCOVA

Parameter type

Adjusted GMT

Point estimate

0.97

Confidence interval

level

95%

sides

2-sided

lower limit

0.81

upper limit

1.16

Notes
[11] - For HPV-16, one month after the third dose, the UL of the two-sided standardized asymptotic 95% CI on the group GMT ratiohad to be below the pre-defined limit of 2.

Statistical analysis 2

Statistical analysis description

Adjusted GMT ratio of the Cervarix Group versus Nimenrix+Cervarix (0,1,6-Month) Group in terms of HPV-18 titers.

Comparison groups

Cervarix Group v Nimenrix+Cervarix (0,1,6-Month) Group

Number of subjects included in analysis

497

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[12]

Method

ANCOVA

Parameter type

Adjusted GMT

Point estimate

1.09

Confidence interval

level

95%

sides

2-sided

lower limit

0.91

upper limit

1.29

Notes
[12] - For HPV-18, one month after the third dose, the UL of the two-sided standardized asymptotic 95% CI on the group GMT ratiohad to be below the pre-defined limit of 2.

Statistical analysis 3

Statistical analysis description

Adjusted GMT ratio of the Boostrix+Cervarix Group versus Nimenrix+Cervarix+Boostrix Group in terms of HPV-16 titers.

Comparison groups

Boostrix+Cervarix Group v Nimenrix+Cervarix+Boostrix Group

Number of subjects included in analysis

491

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[13]

Method

ANCOVA

Parameter type

Adjusted GMT

Point estimate

1.19

Confidence interval

level

95%

sides

2-sided

lower limit

0.99

upper limit

1.43

Notes
[13] - For HPV-16, one month after the third dose, the UL of the two-sided standardized asymptotic 95% CI on the group GMT ratiohad to be below the pre-defined limit of 2.

Statistical analysis 4

Statistical analysis description

Adjusted GMT ratio of the Boostrix+Cervarix Group versus Nimenrix+Cervarix+Boostrix Group in terms of HPV-18 titers.

Comparison groups

Boostrix+Cervarix Group v Nimenrix+Cervarix+Boostrix Group

Number of subjects included in analysis

491

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[14]

Method

ANCOVA

Parameter type

Adjusted GMT

Point estimate

1.18

Confidence interval

level

95%

sides

2-sided

lower limit

0.99

upper limit

1.41

Notes
[14] - For HPV-18, one month after the third dose, the UL of the two-sided standardized asymptotic 95% CI on the group GMT ratiohad to be below the pre-defined limit of 2.

Primary: Number of subjects with anti-diphteria (anti-D) and anti-tetanus (anti-T) concentrations equal to or above (≥) 1.0 IU/mL

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End point title

Number of subjects with anti-diphteria (anti-D) and anti-tetanus (anti-T) concentrations equal to or above (≥) 1.0 IU/mL ^[15]

End point description

The antibody concentrations were calculated as geometric mean concentrations (GMCs) and expressed as International Units per milliliter (IU/mL). This analysis was only performed in the groups receiving Boostrix vaccine.

End point type

Primary

End point timeframe

At one month after Boostrix vaccination (Month 1)

Notes
[15] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Boostrix vaccine.

End point values	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	250	256
Units: Participants
Anti-D	235	248
Anti-T	249	256

Statistical analysis 1

Statistical analysis description

Adjusted GMC ratio of the Cervarix+Boostrix Group versus Nimenrix+Cervarix+Boostrix Group in terms of Anti-D titers

Comparison groups

Boostrix+Cervarix Group v Nimenrix+Cervarix+Boostrix Group

Number of subjects included in analysis

506

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[16]

Method

Parameter type

Adjusted GMT Ratio

Point estimate

1.39

Confidence interval

level

95%

sides

2-sided

lower limit

1.2

upper limit

1.6

Notes
[16] - For anti-D the LL of the 2-sided standardised asymptotic 95% CI for the group difference (Co-ad group minus Boostrix group) had to be greater than or equal to the pre-defined limit of -10%.

Statistical analysis 2

Statistical analysis description

Adjusted GMC ratio of the Cervarix+Boostrix Group versus Nimenrix+Cervarix+Boostrix Group in terms of Anti-D titers

Comparison groups

Boostrix+Cervarix Group v Nimenrix+Cervarix+Boostrix Group

Number of subjects included in analysis

506

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[17]

Method

Parameter type

Adjusted GMT ratio

Point estimate

-0.4

Confidence interval

level

95%

sides

2-sided

lower limit

-2.23

upper limit

1.08

Notes
[17] - For anti-T the LL of the 2-sided standardised asymptotic 95% CI for the group difference (Co-ad group minus Boostrix group) had to be greater than or equal to the pre-defined limit of -10%.

Primary: Anti-PT, anti-FHA and anti-PRN antibody concentrations

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End point title

Anti-PT, anti-FHA and anti-PRN antibody concentrations ^[18]

End point description

The antibody concentrations were tabulated as geometric mean concentrations (GMCs) and expressed as international units per milliliter (IU/mL). GMCs were only analyzed in subjects receiving Boostrix vaccination.

End point type

Primary

End point timeframe

At one month after Boostrix vaccination (Month 1)

Notes
[18] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Boostrix vaccine.

End point values	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	247	256
Units: IU/mL
geometric mean (confidence interval 95%)
Anti-PT	52.9 (46.4 to 60.4)	73.2 (65 to 82.5)
Anti-FHA	278.7 (249.5 to 311.2)	472.4 (419.7 to 531.8)
Anti-PRN	193.4 (159 to 235.1)	318.6 (262.4 to 386.8)

Statistical analysis 1

Statistical analysis description

Adjusted GMT ratio of the Nimenrix+Cervarix+Boostrix Group versus Boostrix+ Cervarix Group in terms of anti-PRN titers

Comparison groups

Boostrix+Cervarix Group v Nimenrix+Cervarix+Boostrix Group

Number of subjects included in analysis

503

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[19]

Method

ANCOVA

Parameter type

Adjusted GMT Ratio

Point estimate

1.55

Confidence interval

level

95%

sides

2-sided

lower limit

1.26

upper limit

1.9

Notes
[19] - For anti-PRN the UL of the 2-sided standardised asymptotic 95% CI for the adjusted group ratio of GMCs (Boostrix group/Co-ad group) had to be less than or equal to the pre-defined limit of 1.5

Statistical analysis 2

Statistical analysis description

Adjusted GMT ratio of the Nimenrix+Cervarix Group versus Boostrix+ Cervarix Group in terms of anti-FHA titers

Comparison groups

Boostrix+Cervarix Group v Nimenrix+Cervarix+Boostrix Group

Number of subjects included in analysis

503

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[20]

Method

ANCOVA

Parameter type

Adjusted GMT Ratio

Point estimate

1.65

Confidence interval

level

95%

sides

2-sided

lower limit

1.42

upper limit

1.93

Notes
[20] - For anti-FHA the UL of the 2-sided standardised asymptotic 95% CI for the adjusted group ratio of GMCs (Boostrix group/Co-ad group) had to be less than or equal to the pre-defined limit of 1.5

Statistical analysis 3

Statistical analysis description

Adjusted GMT ratio of the Nimenrix+Cervarix Group versus Boostrix+ Cervarix Group in terms of anti-PT titers

Comparison groups

Boostrix+Cervarix Group v Nimenrix+Cervarix+Boostrix Group

Number of subjects included in analysis

503

Analysis specification

Pre-specified

Analysis type

non-inferiority ^[21]

Method

ANCOVA

Parameter type

Adjusted GMT Ratio

Point estimate

1.39

Confidence interval

level

95%

sides

2-sided

lower limit

1.2

upper limit

1.6

Notes
[21] - For anti-PT the UL of the 2-sided standardised asymptotic 95% CI for the adjusted group ratio of GMCs (Boostrix group/Co-ad group) had to be less than or equal to the pre-defined limit of 1.5

Secondary: Number of subjects with rSBA-MenA, rSBA-MenC, rSBA-MenW-135 and rSBA-MenY antibody titres ≥ 1:8 and ≥ 1:128

Top of page

End point title

Number of subjects with rSBA-MenA, rSBA-MenC, rSBA-MenW-135 and rSBA-MenY antibody titres ≥ 1:8 and ≥ 1:128 ^[22]

End point description

The number of subjects with rSBA-MenA, rSBA-MenC, rSBA-MenW-135 and rSBA-MenY antibody titers ≥ 1:8 and ≥ 1:128 prior to and one month after vaccination with Nimenrix vaccine.

End point type

Secondary

End point timeframe

Prior to and one month after vaccination with Nimenrix (Months 0 and 1)

Notes
[22] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Nimenrix vaccine.

End point values	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Nimenrix+Cervarix+Boostrix Group
Number of subjects analysed	256	255	257
Units: Participants
rSBA-MenA ≥1:8, Month 0	112	118	129
rSBA-MenC ≥1:8, Month 0	34	29	40
rSBA-MenW-135 ≥1:8, Month 0	23	24	22
rSBA-MenY ≥1:8, Month 0	86	102	80
rSBA-MenA ≥1:128, Month 0	78	86	82
rSBA-MenC ≥1:128, Month 0	20	10	23
rSBA-MenW-135 ≥1:128, Month 0	22	23	20
rSBA-MenY ≥1:128, Month 0	84	99	74
rSBA-MenA ≥1:8, Month 1	255	255	255
rSBA-MenC ≥1:8, Month 1	254	253	253
rSBA-MenW-135 ≥1:8, Month 1	253	255	250
rSBA-MenY ≥1:8, Month 1	256	255	255
rSBA-MenA ≥1:128, Month 1	255	255	255
rSBA-MenC ≥1:128, Month 1	254	252	252
rSBA-MenW-135 ≥1:128, Month 1	253	255	250
rSBA-MenY ≥1:128, Month 1	256	255	255

No statistical analyses for this end point

Secondary: rSBA-MenA, rSBA-MenC, rSBA-MenW-135 and rSBA-MenY vaccine response

Top of page

End point title

rSBA-MenA, rSBA-MenC, rSBA-MenW-135 and rSBA-MenY vaccine response ^[23]

End point description

rSBA vaccine response for serogroups A, C, W-135 and Y was defined as: • For initially seronegative subjects (pre-vaccination titre below the cut-off of 1:8): number of subjects with rSBA antibody titres ≥ 1:32 one month after vaccination. • For initially seropositive subjects (pre-vaccination titre ≥ 1:8): number of subjects with rSBA antibody titres at least four times the pre-vaccination antibody titres, one month after vaccination.

End point type

Secondary

End point timeframe

At one month after Nimenrix vaccination (Month 1)

Notes
[23] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Nimenrix vaccine.

End point values	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Nimenrix+Cervarix+Boostrix Group
Number of subjects analysed	256	255	256
Units: Participants
rSBA-MenA	240	235	230
rSBA-MenC	250	251	246
rSBA-MenW-135	252	255	248
rSBA-MenY	245	253	251

No statistical analyses for this end point

Secondary: Number of subjects with anti-T antibody concentrations ≥ 0.1 IU/mL and ≥ 1.0 IU/mL

Top of page

End point title

Number of subjects with anti-T antibody concentrations ≥ 0.1 IU/mL and ≥ 1.0 IU/mL ^[24]

End point description

The antibody concentrations were tabulated as geometric mean concentrations (GMCs) and expressed as international units per milliliter (IU/mL), only for the Nimenrix+Cervarix (1,2,7-Month) Group.

End point type

Secondary

End point timeframe

Prior to and one month after vaccination with Nimenrix (Months 0 and 1)

Notes
[24] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Boostrix vaccine.

End point values	Nimenrix+Cervarix (1,2,7-Month) Group
Number of subjects analysed	255
Units: Participants
Anti-T ≥ 0.1 IU/mL, Month 0	236
Anti-T ≥ 0.1 IU/mL, Month 1	255
Anti-T ≥ 1 IU/mL, Month 0	151
Anti-T ≥ 1 IU/mL, Month 1	253

No statistical analyses for this end point

Secondary: Anti-T antibody concentrations

Top of page

End point title

Anti-T antibody concentrations ^[25]

End point description

The antibody concentrations were calculated as geometric mean concentrations (GMCs) and expressed as international units per milliliter (IU/mL). This analysis was only performed for the Nimenrix+Cervarix (1,2,7-Month) Group.

End point type

Secondary

End point timeframe

Prior to and one month after vaccination with Nimenrix (Months 0 and 1)

Notes
[25] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Boostrix vaccine.

End point values	Nimenrix+Cervarix (1,2,7-Month) Group
Number of subjects analysed	255
Units: IU/mL
geometric mean (confidence interval 95%)
Anti-T, Month 0	1.2 (1 to 1.4)
Anti-T, Month 1	25.4 (22.8 to 28.3)

No statistical analyses for this end point

Secondary: Number of subjects with anti-HPV-16 concentrations ≥ 19 EU/mL and anti-HPV-18 concentrations ≥ 18 EU/mL

Top of page

End point title

Number of subjects with anti-HPV-16 concentrations ≥ 19 EU/mL and anti-HPV-18 concentrations ≥ 18 EU/mL ^[26]

End point description

The antibody concentrations were calculated as geometric mean concentrations (GMCs) and expressed as ELISA units per milliliter (EU/mL).

End point type

Secondary

End point timeframe

Prior to the first dose and one month after the third dose of Cervarix [Month 0 and Month 7/Month 8 in Nimenrix+Cervarix (1,2,7-Month) Group]

Notes
[26] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Cervarix vaccine.

End point values	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Boostrix+Cervarix Group
Number of subjects analysed	246	248	249	247
Units: Participants
Anti-HPV-16, Month 0	17	29	32	22
Anti-HPV-16, Month 7/Month 8	245	248	249	247
Anti-HPV-18, Month 0	11	12	17	14
Anti-HPV-18, Month 7/Month 8	245	248	249	247

No statistical analyses for this end point

Secondary: Number of subjects seroconverted for anti-HPV-16 and anti-HPV-18 antibodies

Top of page

End point title

Number of subjects seroconverted for anti-HPV-16 and anti-HPV-18 antibodies

End point description

Seroconversion rate is defined as the appearance of antibodies (i.e. titers greater than or equal to the cut-off value) in the serum of subjects who are seronegative before vaccination. The antibody concentrations were calculated as geometric mean concentrations (GMCs) and expressed as ELISA units per milliliter (EU/mL).

End point type

Secondary

End point timeframe

Prior to and one month after the third dose of Cervarix (Month 0 and Month 7/Month 8)

End point values	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	235	236	232	230	233
Units: Participants
Anti-HPV-16, Month 0	0	0	0	0	0
Anti-HPV-16, Month 7/Month 8	228	219	217	215	225
Anti-HPV-18, Month 0	0	0	0	0	0
Anti-HPV-18, Month 7/Month 8	234	236	232	230	233

No statistical analyses for this end point

Secondary: Anti-HPV-16 and anti-HPV-18 concentrations in Nimenrix+Cervarix (1,2,7-Month) Group

Top of page

End point title

Anti-HPV-16 and anti-HPV-18 concentrations in Nimenrix+Cervarix (1,2,7-Month) Group ^[27]

End point description

The antibody concentrations were calculated as geometric mean concentrations (GMCs) and expressed as ELISA units per milliliter (EU/mL).

End point type

Secondary

End point timeframe

Prior to and one month after the third dose of Cervarix (Months 0 and 8)

Notes
[27] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the Nimenrix+Cervarix (1,2,7-Month) Group.

End point values	Nimenrix+Cervarix (1,2,7-Month) Group
Number of subjects analysed	246
Units: EU/mL
geometric mean (confidence interval 95%)
Anti-HPV-16, Month 0	10.9 (10.2 to 11.6)
Anti-HPV-16, Month 8	11128.2 (9471.8 to 13074.4)
Anti-HPV-18, Month 0	9.8 (9.3 to 10.4)
Anti-HPV-18, Month 8	5357 (4550.2 to 6306.9)

No statistical analyses for this end point

Secondary: Booster responses for anti-PT, anti-FHA and anti-PRN antibodies

Top of page

End point title

Booster responses for anti-PT, anti-FHA and anti-PRN antibodies ^[28]

End point description

Booster responses to the PT, FHA and PRN antigens were defined as: -For initially seronegative subjects (antibody concentrations: < 2.046 IU/ml for anti-FHA, < 2.187 IU/ml for anti-PRN, < 2.693 IU/ml for anti-PT), antibody concentration ≥ 4*cut_off IU/ml at Month 1 post-vaccination; -For initially seropositive subjects (antibody concentrations: ≥ 2.046 IU/ml for anti-FHA, ≥ 2.187 IU/ml for anti-PRN, ≥ 2.693 IU/ml for anti-PT) with pre-vaccination antibody concentration < 4*cut_off IU/ml : antibody concentration at Month 1 ≥ 4 fold the pre-vaccination antibody concentration; -For initially seropositive subjects (antibody concentrations: ≥ 2.046 IU/ml for anti-FHA, ≥ 2.187 IU/ml for anti-PRN, ≥ 2.693 IU/ml for anti-PT) with pre-vaccination antibody concentration ≥ 4*cut_off IU/ml : antibody concentration at Month 1 ≥ 2 fold the pre-vaccination antibody concentration.

End point type

Secondary

End point timeframe

At one month after Boostrix vaccination (Month 1)

Notes
[28] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Boostrix vaccine.

End point values	Boostrix+Cervarix Group
Number of subjects analysed	256
Units: Participants
Anti-PT	235
Anti-FHA	247
Anti-PRN	248

No statistical analyses for this end point

Secondary: Number of subjects with anti-D and anti-T antibody concentrations ≥ 0.1 IU/mL

Top of page

End point title

Number of subjects with anti-D and anti-T antibody concentrations ≥ 0.1 IU/mL ^[29]

End point description

The antibody concentrations were calculated as geometric mean concentrations (GMCs) and expressed as international units per milliliter (IU/mL).

End point type

Secondary

End point timeframe

Prior to and one month after Boostrix vaccination (Month 0 and Month 1)

Notes
[29] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Boostrix vaccine.

End point values	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	251	256
Units: Participants
Anti-D, Month 0	214	223
Anti-D, Month 1	250	256
Anti-T, Month 0	239	248
Anti-T, Month 1	250	256

No statistical analyses for this end point

Secondary: Anti-D and anti-T antibody concentrations

Top of page

End point title

Anti-D and anti-T antibody concentrations ^[30]

End point description

The antibody concentrations were calculated as geometric mean concentrations (GMCs) and expressed as international units per milliliter (IU/mL).

End point type

Secondary

End point timeframe

Prior to and one month after Boostrix vaccination (Months 0 and 1)

Notes
[30] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Boostrix vaccine.

End point values	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	251	256
Units: IU/mL
geometric mean (confidence interval 95%)
Anti-D, Month 0	0.5 (0.4 to 0.5)	0.5 (0.4 to 0.6)
Anti-D, Month 1	4.7 (4.2 to 5.2)	6.6 (5.9 to 7.4)
Anti-T, Month 0	1.3 (1.1 to 1.5)	1.3 (1.1 to 1.5)
Anti-T, Month 1	25.9 (23.4 to 28.8)	15.4 (14.1 to 16.9)

No statistical analyses for this end point

Secondary: Number of subjects with anti-PT, anti-FHA and anti-PRN antibody concentrations equal to or above the cut-off value

Top of page

End point title

Number of subjects with anti-PT, anti-FHA and anti-PRN antibody concentrations equal to or above the cut-off value ^[31]

End point description

The antibody concentrations were calculated as geometric mean concentrations (GMCs) and expressed as international units per milliliter (IU/mL). Anti-PT assay cut-off=2.693 IU/mL, anti-FHA assay cut-off=2.046 IU/mL, anti-PRN assay cut-off=2.187 IU/mL.

End point type

Secondary

End point timeframe

Prior to and one month after Boostrix vaccination (Months 0 and 1)

Notes
[31] - The end point is not reporting statistics for all the arms in the baseline period. It is expected all the baseline period arms will be reported on when providing values for an end point on the baseline period.
Justification: The analysis was performed only on the groups receiving Boostrix vaccine.

End point values	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	251	256
Units: Participants
Anti-PT, Month 0	156	153
Anti-PT, Month 1	240	252
Anti-FHA, Month 0	235	256
Anti-FHA, Month 1	247	256
Anti-PRN, Month 0	218	229
Anti-PRN, Month 1	246	256

No statistical analyses for this end point

Secondary: Number of subjects reporting solicited local symptoms

Top of page

End point title

Number of subjects reporting solicited local symptoms

End point description

Assessed solicited local symptoms were pain, redness and swelling. Any = occurrence of the symptom regardless of intensity grade. Grade 3 pain = pain that prevented normal activity. Grade 3 redness/swelling = redness/swelling spreading beyond 50 millimeters (mm) of injection site. Symproms were presented by vaccination site. Some groups do not have results for “Dose 2” because solicited local symptoms were not collected for these subjects at the Dose 2 timepoint.

End point type

Secondary

End point timeframe

Days 0-6 following each vaccination

End point values	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	259	259	261	260	261
Units: Participants
Any Pain (Nimenrix), Dose 1	152	140	0	156	0
Grade 3 Pain (Nimenrix), Dose 1	4	3	0	7	0
Any Pain (Boostrix), Dose 1	0	0	0	189	200
Grade 3 Pain (Boostrix), Dose 1	0	0	0	21	15
Any Pain (Cervarix), Dose 1	0	213	205	217	221
Grade 3 Pain (Cervarix), Dose 1	0	8	11	23	18
Any Redness (Nimenrix), Dose 1	57	42	0	54	0
Grade 3 Redness (Nimenrix), Dose 1	4	2	0	0	0
Any Redness (Boostrix), Dose 1	0	0	0	73	53
Grade 3 Redness (Boostrix), Dose 1	0	0	0	2	4
Any Redness (Cervarix), Dose 1	0	56	54	62	48
Grade 3 Redness (Cervarix), Dose 1	0	0	0	1	0
Any Swelling (Nimenrix), Dose 1	40	34	0	58	0
Grade 3 Swelling (Nimenrix), Dose 1	1	1	0	5	0
Any Swelling (Boostrix), Dose 1	0	0	0	79	58
Grade 3 Swelling (Boostrix), Dose 1	0	0	0	5	7
Any Swelling (Cervarix), Dose 1	0	42	37	64	55
Grade 3 Swelling (Cervarix), Dose 1	0	1	1	1	5
Any Pain (Cervarix), Dose 2	193	0	0	0	0
Grade 3 Pain (Cervarix), Dose 2	15	0	0	0	0
Any Redness (Cervarix), Dose 2	43	0	0	0	0
Grade 3 Redness (Cervarix), Dose 2	0	0	0	0	0
Any Swelling (Cervarix), Dose 2	41	0	0	0	0
Grade 3 Swelling (Cervarix), Dose 2	1	0	0	0	0
Any Pain (Nimenrix), Across doses	152	140	0	156	0
Grade 3 Pain (Nimenrix), Across doses	4	3	0	7	0
Any Pain (Boostrix), Across doses	0	0	0	189	200
Grade 3 Pain (Boostrix), Across doses	0	0	0	21	15
Any Pain (Cervarix), Across doses	193	213	205	217	221
Grade 3 Pain (Cervarix), Across doses	15	8	11	23	18
Any Redness (Nimenrix), Across doses	57	42	0	54	0
Grade 3 Redness (Nimenrix), Across doses	4	2	0	0	0
Any Redness (Boostrix), Across doses	0	0	0	73	53
Grade 3 Redness (Boostrix), Across doses	0	0	0	2	4
Any Redness (Cervarix), Across doses	43	56	54	62	48
Grade 3 Redness (Cervarix), Across doses	0	0	0	1	0
Any Swelling (Nimenrix), Across doses	40	34	0	58	0
Grade 3 Swelling (Nimenrix), Across doses	1	1	0	5	0
Any Swelling (Boostrix), Across doses	0	0	0	79	58
Grade 3 Swelling (Boostrix), Across doses	0	0	0	5	7
Any Swelling (Cervarix), Across doses	41	42	37	64	55
Grade 3 Swelling (Cervarix), Across doses	1	1	1	1	5

No statistical analyses for this end point

Secondary: Number of subjects reporting solicited general symptoms

Top of page

End point title

Number of subjects reporting solicited general symptoms

End point description

Assessed solicited general symptoms were arthralgia, fatigue, gastrointestinal symptoms, headache, myalgia, rash, fever [defined as axillary temperature equal to or above 37.5 degrees Celsius (°C)] and urticaria. Any = occurrence of the symptom regardless of intensity grade. Grade 3 symptom = symptom that prevented normal activity. Grade 3 fever = fever > 39.5 °C. Related = symptom assessed by the investigator as related to the vaccination. Some groups do not have results for “Dose 2” because solicited local symptoms were not collected for these subjects at the Dose 2 timepoint.

End point type

Secondary

End point timeframe

Days 0-6 following each vaccination

End point values	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	259	257	259	260	261
Units: Participants
Any Arthralgia, Dose 1	23	18	13	36	23
Grade 3 Arthralgia, Dose 1	0	1	1	1	4
Related Arthralgia, Dose 1	23	18	13	34	23
Any Fatigue, Dose 1	87	95	85	110	101
Grade 3 Fatigue, Dose 1	2	4	2	8	5
Related Fatigue, Dose 1	82	92	79	103	99
Any Gastrointestinal, Dose 1	21	27	23	29	22
Grade 3 Gastrointestinal, Dose 1	1	1	0	2	0
Related Gastrointestinal, Dose 1	19	27	21	26	20
Any Headache, Dose 1	82	94	78	99	95
Grade 3 Headache, Dose 1	5	3	5	5	4
Related Headache, Dose 1	81	89	73	92	85
Any Myalgia, Dose 1	65	83	85	96	101
Grade 3 Myalgia, Dose 1	0	4	6	9	9
Related Myalgia, Dose 1	60	81	82	92	100
Any Rash, Dose 1	4	8	8	6	6
Grade 3 Rash, Dose 1	0	0	0	0	0
Related Rash, Dose 1	1	6	7	6	4
Any Fever, Dose 1	24	32	15	38	27
Grade 3 Fever, Dose 1	0	0	0	0	0
Related Fever, Dose 1	21	31	14	37	25
Any Urticaria, Dose 1	0	4	4	5	5
Grade 3 Urticaria, Dose 1	0	0	0	0	0
Related Urticaria, Dose 1	0	3	4	5	3
Any Arthralgia, Dose 2	18	0	0	0	0
Grade 3 Arthralgia, Dose 2	0	0	0	0	0
Related Arthralgia, Dose 2	18	0	0	0	0
Any Fatigue, Dose 2	61	0	0	0	0
Grade 3 Fatigue, Dose 2	2	0	0	0	0
Related Fatigue, Dose 2	58	0	0	0	0
Any Gastrointestinal, Dose 2	10	0	0	0	0
Grade 3 Gastrointestinal, Dose 2	1	0	0	0	0
Related Gastrointestinal, Dose 2	8	0	0	0	0
Any Headache, Dose 2	58	0	0	0	0
Grade 3 Headache, Dose 2	3	0	0	0	0
Related Headache, Dose 2	55	0	0	0	0
Any Myalgia, Dose 2	73	0	0	0	0
Grade 3 Myalgia, Dose 2	4	0	0	0	0
Related Myalgia, Dose 2	72	0	0	0	0
Any Rash, Dose 2	3	0	0	0	0
Grade 3 Rash, Dose 2	0	0	0	0	0
Related Rash, Dose 2	3	0	0	0	0
Any Fever, Dose 2	11	0	0	0	0
Grade 3 Fever, Dose 2	0	0	0	0	0
Related Fever, Dose 2	10	0	0	0	0
Any Urticaria, Dose 2	2	0	0	0	0
Grade 3 Urticaria, Dose 2	0	0	0	0	0
Related Urticaria, Dose 2	2	0	0	0	0
Any Arthralgia, Across doses	34	18	13	36	23
Grade 3 Arthralgia, Across doses	0	1	1	1	4
Related Arthralgia, Across doses	34	18	13	34	23
Any Fatigue, Across doses	105	95	85	110	101
Grade 3 Fatigue, Across doses	4	4	2	8	5
Related Fatigue, Across doses	98	92	79	103	99
Any Gastrointestinal, Across doses	26	27	23	29	22
Grade 3 Gastrointestinal, Across doses	2	1	0	2	0
Related Gastrointestinal, Across doses	23	27	21	26	20
Any Headache, Across doses	101	94	78	99	95
Grade 3 Headache, Across doses	8	3	5	5	4
Related Headache, Across doses	99	89	73	92	85
Any Myalgia, Across doses	95	83	85	96	101
Grade 3 Myalgia, Across doses	4	4	6	9	9
Related Myalgia, Across doses	91	81	82	92	100
Any Rash, Across doses	7	8	8	6	6
Grade 3 Rash, Across doses	0	0	0	0	0
Related Rash, Across doses	4	6	7	6	4
Any Fever, Across doses	34	32	15	38	27
Grade 3 Fever, Across doses	0	0	0	0	0
Related Fever, Across doses	30	31	14	37	25
Any Urticaria, Across doses	2	4	4	5	5
Grade 3 Urticaria, Across doses	0	0	0	0	0
Related Urticaria, Across doses	2	3	4	5	3

No statistical analyses for this end point

Secondary: Number of subjects with unsolicited adverse events AE(s)

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End point title

Number of subjects with unsolicited adverse events AE(s)

End point description

An unsolicited AE covers any untoward medical occurrence in a clinical investigation subject temporally associated with the use of a medicinal product, whether or not considered related to the medicinal product and reported in addition to those solicited during the clinical study and any solicited symptom with onset outside the specified period of follow-up for solicited symptoms. Any was defined as the occurrence of any unsolicited AE regardless of intensity grade or relation to vaccination. Grade 3 AE = an AE which prevented normal, everyday activities. Related = AE assessed by the investigator as related to the vaccination.

End point type

Secondary

End point timeframe

During Days 0-30 following vaccination with Nimenrix, Boostrix or the first dose of Cervarix

End point values	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	259	259	261	260	261
Units: Participants
Participants	37	35	35	42	39

No statistical analyses for this end point

Secondary: Number of subjects with serious adverse events SAE(s)

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End point title

Number of subjects with serious adverse events SAE(s)

End point description

Serious adverse events (SAEs) assessed include medical occurrences that result in death, are life-threatening, require hospitalization or prolongation of hospitalization or result in disability/incapacity.

End point type

Secondary

End point timeframe

During the entire study period (from Month 0 to Month 8)

End point values	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	259	259	261	260	261
Units: Participants
Participants	3	2	5	7	6

No statistical analyses for this end point

Secondary: Number of subjects with potential immune-mediated diseases (pIMDs)

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End point title

Number of subjects with potential immune-mediated diseases (pIMDs)

End point description

pIMDs are a subset of AEs that include autoimmune diseases and other inflammatory and/or neurologic disorders of interest which may or may not have an autoimmune aetiology.

End point type

Secondary

End point timeframe

During the entire study period (from Month 0 to Month 8)

End point values	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	259	259	261	260	261
Units: Participants
Participants	0	0	0	0	0

No statistical analyses for this end point

Secondary: Number of subjects with new onset chronic illnesses (NOCIs)

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End point title

Number of subjects with new onset chronic illnesses (NOCIs)

End point description

NOCIs include autoimmune disorders, asthma, type I diabetes, allergies.

End point type

Secondary

End point timeframe

During the entire study period (from Month 0 to Month 8)

End point values	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Number of subjects analysed	259	259	261	260	261
Units: Participants
Participants	3	0	1	0	2

No statistical analyses for this end point

Adverse events

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Timeframe for reporting adverse events

Solicited local and general symptoms: Days 0-6 following each vaccination, Unsolicited AEs: Days 0-30 following each vaccination; SAEs: throughout the whole study period (from Month 0 up to Month 8).

Assessment type

Systematic

Dictionary name

MedDRA

Dictionary version

17.0

Reporting group title

Nimenrix+Cervarix (1,2,7-Month) Group

Reporting group description

Reporting group title

Nimenrix+Cervarix (0,1,6-Month) Group

Reporting group description

Reporting group title

Cervarix Group

Reporting group description

Subjects in this group received 3 doses of Cervarix vaccine at Month 0, Month 1 and Month 6, administered intramuscularly (IM) in the deltoid region of the arm.

Reporting group title

Nimenrix+Cervarix+Boostrix Group

Reporting group description

Reporting group title

Boostrix+Cervarix Group

Reporting group description

Serious adverse events	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Total subjects affected by serious adverse events
subjects affected / exposed	3 / 259 (1.16%)	2 / 259 (0.77%)	5 / 261 (1.92%)	7 / 260 (2.69%)	6 / 261 (2.30%)
number of deaths (all causes)	0	0	0	0	1
number of deaths resulting from adverse events	0	0	0	0	0
Injury, poisoning and procedural complications
Stab wound
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	0 / 261 (0.00%)	0 / 260 (0.00%)	1 / 261 (0.38%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Congenital, familial and genetic disorders
Atrial septal defect
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	0 / 261 (0.00%)	1 / 260 (0.38%)	0 / 261 (0.00%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 1	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Pregnancy, puerperium and perinatal conditions
Premature baby
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	0 / 261 (0.00%)	0 / 260 (0.00%)	1 / 261 (0.38%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 1
Abortion incomplete
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	0 / 261 (0.00%)	1 / 260 (0.38%)	0 / 261 (0.00%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 1	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Abortion spontaneous
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	1 / 261 (0.38%)	0 / 260 (0.00%)	0 / 261 (0.00%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 1	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Nervous system disorders
Migraine
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	0 / 261 (0.00%)	0 / 260 (0.00%)	1 / 261 (0.38%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Reproductive system and breast disorders
Ovarian cyst
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	0 / 261 (0.00%)	0 / 260 (0.00%)	1 / 261 (0.38%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Pelvic pain
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	0 / 261 (0.00%)	0 / 260 (0.00%)	1 / 261 (0.38%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Respiratory, thoracic and mediastinal disorders
Neonatal respiratory distress syndrome
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	0 / 261 (0.00%)	0 / 260 (0.00%)	1 / 261 (0.38%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 1
Skin and subcutaneous tissue disorders
Dermatitis atopic
subjects affected / exposed	1 / 259 (0.39%)	0 / 259 (0.00%)	0 / 261 (0.00%)	0 / 260 (0.00%)	0 / 261 (0.00%)
occurrences causally related to treatment / all	0 / 1	0 / 0	0 / 0	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Musculoskeletal and connective tissue disorders
Pain in extremity
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	0 / 261 (0.00%)	1 / 260 (0.38%)	0 / 261 (0.00%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 1	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Infections and infestations
Appendicitis
subjects affected / exposed	2 / 259 (0.77%)	0 / 259 (0.00%)	0 / 261 (0.00%)	1 / 260 (0.38%)	0 / 261 (0.00%)
occurrences causally related to treatment / all	0 / 2	0 / 0	0 / 0	0 / 1	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Dengue fever
subjects affected / exposed	0 / 259 (0.00%)	1 / 259 (0.39%)	2 / 261 (0.77%)	2 / 260 (0.77%)	0 / 261 (0.00%)
occurrences causally related to treatment / all	0 / 0	0 / 1	0 / 2	0 / 2	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Gastroenteritis
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	0 / 261 (0.00%)	1 / 260 (0.38%)	1 / 261 (0.38%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 1	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Influenza
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	1 / 261 (0.38%)	0 / 260 (0.00%)	0 / 261 (0.00%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 1	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Pelvic inflammatory disease
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	1 / 261 (0.38%)	0 / 260 (0.00%)	0 / 261 (0.00%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 1	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Pharyngitis
subjects affected / exposed	0 / 259 (0.00%)	1 / 259 (0.39%)	0 / 261 (0.00%)	0 / 260 (0.00%)	0 / 261 (0.00%)
occurrences causally related to treatment / all	0 / 0	0 / 1	0 / 0	0 / 0	0 / 0
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 0
Metabolism and nutrition disorders
Underweight
subjects affected / exposed	0 / 259 (0.00%)	0 / 259 (0.00%)	0 / 261 (0.00%)	0 / 260 (0.00%)	1 / 261 (0.38%)
occurrences causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 1
deaths causally related to treatment / all	0 / 0	0 / 0	0 / 0	0 / 0	0 / 1

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

Non-serious adverse events	Nimenrix+Cervarix (1,2,7-Month) Group	Nimenrix+Cervarix (0,1,6-Month) Group	Cervarix Group	Nimenrix+Cervarix+Boostrix Group	Boostrix+Cervarix Group
Total subjects affected by non serious adverse events
subjects affected / exposed	235 / 259 (90.73%)	230 / 259 (88.80%)	225 / 261 (86.21%)	238 / 260 (91.54%)	244 / 261 (93.49%)
Nervous system disorders
Headache
subjects affected / exposed	103 / 259 (39.77%)	98 / 259 (37.84%)	78 / 261 (29.89%)	102 / 260 (39.23%)	98 / 261 (37.55%)
occurrences all number	147	99	78	107	101
General disorders and administration site conditions
Fatigue
subjects affected / exposed	105 / 259 (40.54%)	95 / 259 (36.68%)	85 / 261 (32.57%)	110 / 260 (42.31%)	101 / 261 (38.70%)
occurrences all number	148	95	85	110	101
Pain
subjects affected / exposed	217 / 259 (83.78%)	220 / 259 (84.94%)	205 / 261 (78.54%)	228 / 260 (87.69%)	233 / 261 (89.27%)
occurrences all number	345	220	205	228	233
Pyrexia
subjects affected / exposed	35 / 259 (13.51%)	33 / 259 (12.74%)	16 / 261 (6.13%)	39 / 260 (15.00%)	28 / 261 (10.73%)
occurrences all number	36	34	16	39	28
Swelling
subjects affected / exposed	62 / 259 (23.94%)	54 / 259 (20.85%)	37 / 261 (14.18%)	98 / 260 (37.69%)	70 / 261 (26.82%)
occurrences all number	81	54	37	98	70
Gastrointestinal disorders
Gastrointestinal disorder
subjects affected / exposed	26 / 259 (10.04%)	27 / 259 (10.42%)	23 / 261 (8.81%)	29 / 260 (11.15%)	22 / 261 (8.43%)
occurrences all number	31	27	23	29	22
Skin and subcutaneous tissue disorders
Erythema
subjects affected / exposed	78 / 259 (30.12%)	68 / 259 (26.25%)	54 / 261 (20.69%)	90 / 260 (34.62%)	64 / 261 (24.52%)
occurrences all number	100	68	54	90	64
Musculoskeletal and connective tissue disorders
Arthralgia
subjects affected / exposed	34 / 259 (13.13%)	18 / 259 (6.95%)	13 / 261 (4.98%)	36 / 260 (13.85%)	23 / 261 (8.81%)
occurrences all number	41	18	13	36	23
Myalgia
subjects affected / exposed	95 / 259 (36.68%)	83 / 259 (32.05%)	85 / 261 (32.57%)	96 / 260 (36.92%)	101 / 261 (38.70%)
occurrences all number	139	83	85	96	101

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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: Immunogenicity and safety study of GSK Biologicals’ meningococcal vaccine 134612 with or without co-administration of Cervarix and Boostrix in female adolescents and young adults at 9-25 years of age

Trial information

Trial information

Subject disposition

Subject disposition

Baseline characteristics

Baseline characteristics

End points

End points

Primary: Anti-Meningitis antibody titers by serum bactericidal assay using rabbit complement (rSBA)

Primary: Anti-Meningitis antibody titers by serum bactericidal assay using rabbit complement (rSBA)

Primary: Anti-HPV-16 and anti-HPV-18 concentrations

Primary: Anti-HPV-16 and anti-HPV-18 concentrations

Primary: Number of subjects with anti-diphteria (anti-D) and anti-tetanus (anti-T) concentrations equal to or above (≥) 1.0 IU/mL

Primary: Number of subjects with anti-diphteria (anti-D) and anti-tetanus (anti-T) concentrations equal to or above (≥) 1.0 IU/mL

Primary: Anti-PT, anti-FHA and anti-PRN antibody concentrations

Primary: Anti-PT, anti-FHA and anti-PRN antibody concentrations

Secondary: Number of subjects with rSBA-MenA, rSBA-MenC, rSBA-MenW-135 and rSBA-MenY antibody titres ≥ 1:8 and ≥ 1:128

Secondary: Number of subjects with rSBA-MenA, rSBA-MenC, rSBA-MenW-135 and rSBA-MenY antibody titres ≥ 1:8 and ≥ 1:128

Secondary: rSBA-MenA, rSBA-MenC, rSBA-MenW-135 and rSBA-MenY vaccine response

Secondary: rSBA-MenA, rSBA-MenC, rSBA-MenW-135 and rSBA-MenY vaccine response

Secondary: Number of subjects with anti-T antibody concentrations ≥ 0.1 IU/mL and ≥ 1.0 IU/mL

Secondary: Number of subjects with anti-T antibody concentrations ≥ 0.1 IU/mL and ≥ 1.0 IU/mL

Secondary: Anti-T antibody concentrations

Secondary: Anti-T antibody concentrations

Secondary: Number of subjects with anti-HPV-16 concentrations ≥ 19 EU/mL and anti-HPV-18 concentrations ≥ 18 EU/mL

Secondary: Number of subjects with anti-HPV-16 concentrations ≥ 19 EU/mL and anti-HPV-18 concentrations ≥ 18 EU/mL

Secondary: Number of subjects seroconverted for anti-HPV-16 and anti-HPV-18 antibodies

Secondary: Number of subjects seroconverted for anti-HPV-16 and anti-HPV-18 antibodies

Secondary: Anti-HPV-16 and anti-HPV-18 concentrations in Nimenrix+Cervarix (1,2,7-Month) Group

Secondary: Anti-HPV-16 and anti-HPV-18 concentrations in Nimenrix+Cervarix (1,2,7-Month) Group

Secondary: Booster responses for anti-PT, anti-FHA and anti-PRN antibodies

Secondary: Booster responses for anti-PT, anti-FHA and anti-PRN antibodies

Secondary: Number of subjects with anti-D and anti-T antibody concentrations ≥ 0.1 IU/mL

Secondary: Number of subjects with anti-D and anti-T antibody concentrations ≥ 0.1 IU/mL

Secondary: Anti-D and anti-T antibody concentrations

Secondary: Anti-D and anti-T antibody concentrations

Secondary: Number of subjects with anti-PT, anti-FHA and anti-PRN antibody concentrations equal to or above the cut-off value

Secondary: Number of subjects with anti-PT, anti-FHA and anti-PRN antibody concentrations equal to or above the cut-off value

Secondary: Number of subjects reporting solicited local symptoms

Secondary: Number of subjects reporting solicited local symptoms

Secondary: Number of subjects reporting solicited general symptoms

Secondary: Number of subjects reporting solicited general symptoms

Secondary: Number of subjects with unsolicited adverse events AE(s)

Secondary: Number of subjects with unsolicited adverse events AE(s)

Secondary: Number of subjects with serious adverse events SAE(s)

Secondary: Number of subjects with serious adverse events SAE(s)

Secondary: Number of subjects with potential immune-mediated diseases (pIMDs)

Secondary: Number of subjects with potential immune-mediated diseases (pIMDs)

Secondary: Number of subjects with new onset chronic illnesses (NOCIs)

Secondary: Number of subjects with new onset chronic illnesses (NOCIs)

Adverse events

Adverse events

More information

Substantial protocol amendments (globally)

Interruptions (globally)

Limitations and caveats

More information

Clinical Trial Results:
Immunogenicity and safety study of GSK Biologicals’ meningococcal vaccine 134612 with or without co-administration of Cervarix and Boostrix in female adolescents and young adults at 9-25 years of age