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The Effect of Fractional Doses of Pneumococcal Conjugate Vaccines on Immunogenicity and Carriage in Kenyan Infants (FPCV)

Primary Purpose

Pneumococcal Infection, Streptococcus Pneumoniae Infection, Invasive Pneumococcal Disease, Protection Against

Status
Active
Phase
Phase 4
Locations
Kenya
Study Type
Interventional
Intervention
PCV10
PCV13
Sponsored by
London School of Hygiene and Tropical Medicine
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional prevention trial for Pneumococcal Infection focused on measuring Pneumococcal Vaccines;, Immunogenicity, Vaccine, 10-valent pneumococcal vaccine, 13-valent pneumococcal vaccine, Schedule, Pneumococcal Infection, Kenya, Infant, Vaccines, Conjugate, Humans, Immunization schedule, Streptococcus pneumoniae, vaccine, Dose-Response Relationship, immunologic, Equivalence Trial as Topic

Eligibility Criteria

6 Weeks - 8 Weeks (Child)All SexesAccepts Healthy Volunteers

Inclusion Criteria:

  • Healthy infants aged 6-8 weeks of age (HIV positive or negative but with no symptoms of current clinical immunosuppression i.e. HIV infection at WHO clinical stage 1);
  • Parents are willing to provide informed consent for their child to participate in the study
  • Parents and infant are likely to remain in the study area until the infant is 18 months of age and comply with study requirements including the requirement to return to the same health facility to obtain all other childhood vaccines.

Exclusion Criteria:

  • Infants >8 weeks of age at time of enrolment
  • Signs or symptoms of immunosuppression or HIV infection clinical stage 2 or above.
  • Acute illness (e.g. febrile disease) on the day of vaccination
  • Contraindications precluding vaccination (e.g. hypersensitivity to any component of the vaccine, including diphtheria toxoid)
  • Previous PCV vaccination
  • Family are planning to migrate out of the study areas before the end of the study follow-up
  • Family are planning to obtain the subsequent vaccine doses of the routine immunisation schedule elsewhere and therefore their child may receive a full dose under the routine vaccination programme.

Sites / Locations

  • KEMRI Wellcome Trust Research Programme

Arms of the Study

Arm 1

Arm 2

Arm 3

Arm 4

Arm 5

Arm 6

Arm 7

Arm Type

Active Comparator

Experimental

Experimental

Active Comparator

Experimental

Experimental

Active Comparator

Arm Label

Full dose PCV13 (2p+1 schedule)

40% dose PCV13 (2p+1 schedule)

20% dose PCV13 (2p+1 schedule)

Full dose PCV10 (2p+1 schedule)

40% dose PCV10 (2p+1 schedule)

20% dose PCV10 (2p+1 schedule)

Full dose PCV10 (3p+0 schedule)

Arm Description

Full dose PCV13 administration in 2p+1 schedule

Fractional (40%) dose PCV13 administration in 2p+1 schedule

Fractional (20%) dose PCV13 administration in 2p+1 schedule

Full dose PCV10 administration in 2p+1 schedule

Fractional (40%) dose PCV10 administration in 2p+1 schedule

Fractional (20%) dose PCV10 administration in 2p+1 schedule

The current vaccine (PCV10) and schedule (3p+0) in use in the Kenyan routine immunisation programme as an additional comparison arm.

Outcomes

Primary Outcome Measures

Immunogenicity: The ratio of IgG GMCs at 1-month post boost
The ratio of the geometric mean concentrations of IgG after vaccination with 3 full or fractional doses of PCV

Secondary Outcome Measures

Immunogenicity: the proportion of children who 'seroconvert' to vaccine-serotypes after vaccination
The proportion of children with vaccine-serotype specific IgG antibody concentrations more than or equal to 0.35 mcg/ml after vaccination
The proportion of children with evidence of vaccine-serotype carriage
Vaccine-type carriage prevalence across arms
The proportion of children with evidence of vaccine-serotype carriage
Vaccine-type carriage prevalents across arms
The direct vaccine effectiveness of full/fractional doses of PCV13 against carriage of serotypes 6A and 19A
The direct effectiveness of full/fractional doses of PCV13 in preventing carriage of serotypes 6A and 19A compared to that of full dose PCV10
Opsonophagocytic activity of vaccine-induced antibody to 4 serotypes
Functionality of the antibody response

Full Information

First Posted
March 29, 2018
Last Updated
March 10, 2023
Sponsor
London School of Hygiene and Tropical Medicine
Collaborators
University College, London, KEMRI-Wellcome Trust Collaborative Research Program, Bill and Melinda Gates Foundation, National Institute of Health Research (NIHR) Mucosal Pathogens Research Unit (MPRU), Wellcome Trust
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1. Study Identification

Unique Protocol Identification Number
NCT03489018
Brief Title
The Effect of Fractional Doses of Pneumococcal Conjugate Vaccines on Immunogenicity and Carriage in Kenyan Infants
Acronym
FPCV
Official Title
The Effect of Fractional Doses of Pneumococcal Conjugate Vaccines (PCV10 and PCV13) on Immunogenicity and Vaccine-serotype Carriage in Kenyan Infants
Study Type
Interventional

2. Study Status

Record Verification Date
March 2023
Overall Recruitment Status
Active, not recruiting
Study Start Date
March 21, 2019 (Actual)
Primary Completion Date
September 30, 2022 (Actual)
Study Completion Date
April 30, 2023 (Anticipated)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
London School of Hygiene and Tropical Medicine
Collaborators
University College, London, KEMRI-Wellcome Trust Collaborative Research Program, Bill and Melinda Gates Foundation, National Institute of Health Research (NIHR) Mucosal Pathogens Research Unit (MPRU), Wellcome Trust

4. Oversight

Studies a U.S. FDA-regulated Drug Product
Yes
Studies a U.S. FDA-regulated Device Product
No
Product Manufactured in and Exported from the U.S.
Yes
Data Monitoring Committee
Yes

5. Study Description

Brief Summary
Before the introduction of pneumonia vaccines in 2000, between 700,000 - 1 million children died each year as a result of infection with the bacteria Streptococcus pneumoniae and the resulting diseases, namely, meningitis, sepsis and pneumonia. Most of the deaths were in Africa and Asia. Where the vaccines have been introduced, they have been highly effective and have already reduced disease. However, at 10 USD per child, they are not affordable to most low-income countries without financial support from Gavi, the Vaccine Alliance. This project aims to assess whether lower doses of the two commercially available pneumonia vaccines can protect Kenyan infants as well as the full dose. The results could be used to increase the affordability of the pneumonia vaccine, and enable delivery of the vaccine to continue in the absence of Gavi support.
Detailed Description
Background: PCV is currently the most expensive vaccine in the routine immunisation schedule in Gavi-supported countries. This study aims to provide evidence which may enable a substantial decrease in the cost of PCV programmes, therefore increasing the sustainability of PCV programmes in low and middle income countries (LMICs). We propose to assess whether fractional (20% and 40%) doses of pneumococcal conjugate vaccine (PCV10 and PCV13) in a 2p+1 schedule (2 primary doses followed by a booster dose) induce non-inferior immunogenicity and effects on vaccine-serotype carriage when compared to the full dose. These lower doses could convert new 4-dose vials of PCVs into 10- or 20-dose vials, ready for immediate implementation in LMIC programmes. Primary objective: Non-inferior immunogenicity at 1-month post-boost (10 months of age). Non-inferiority will be reached if the lower CI around the ratio of geometric mean concentrations (GMC) of IgG (fractional/full dose) is >0.5 (i.e. the 2-fold criterion). Secondary objectives: Non-inferior immunogenicity at 1-month post-primary series (18 weeks of age). Non-inferiority will be achieved if the lower limit of the 95% confidence interval (CI) around the difference in the proportion of 'responders', children with IgG>=0.35 mcg/ml, (fractional dose group - full dose group) is >-10% for at least 8 of the 10 vaccine types in the PCV10 arms and at least 10 of the 13 vaccine types in the PCV13 arms. The opsonophagocytic activity of the antibody response to 7 serotypes after full/ fractional doses at the 1-month post-boost time point. The direct vaccine effectiveness of full/fractional doses of PCV13 against carriage of serotypes 6A and 19A, with primary analyses at 18 months of age and secondary analyses at 9 months of age. The proportion of children with evidence of vaccine-serotype carriage by trial arm at 9 and 18 months of age. The geometric mean concentration (GMC) of serotype-specific IgG after the primary series of the 2p+1 schedule, prior to boost, at 9 months of age. The geometric mean concentration (GMC) of serotype-specific IgG after three doses of vaccine in a 2p+1 schedule at 18 months of age. The carriage prevalence at 9 and 18 months of age and IgG concentrations at 4 weeks after the primary series after full dose of PCV10 in a 3p+0 schedule, and full/ fractional doses of PCV10/13 in a 2p+1 schedule. Trial design: A phase IV individually-randomised controlled trial of full or fractional (20% or 40%) doses of PCV10/ PCV13, given as a 3-dose schedule to infants: 2 doses at 6 and 14 weeks of age and a booster dose at 9 months (the 2p+1 schedule) or 3 full doses at 6, 10 and 14 weeks of age (the 3p+0 schedule). At 6-8 weeks of age, 300 infants will be enrolled at random into each of the seven trial arms and followed until 18 months of age. The seven trial arms: A. Full dose PCV13 vaccination in a 2p+1 schedule. B. 40% fractional dose PCV13 vaccination in a 2p+1 schedule. C. 20% fractional dose PCV13 vaccination in a 2p+1 schedule. D. Full dose PCV10 vaccination in a 2p+1 schedule. E. 40% fractional dose PCV10 vaccination in a 2p+1 schedule. F. 20% fractional dose PCV10 vaccination in a 2p+1 schedule. G. Full dose PCV10 vaccination in a 3p+0 schedule. This arm would represent the current vaccine and schedule in the Kenyan routine immunisation programme and would act as an additional comparison arm. Study procedures: No study procedures will be conducted without prior parental informed consent. Participants in trial arms A-F will provide 3 or 5 blood samples in the course of the trial at enrolment, 4 weeks post-primary series (approximately 18 weeks of age) and 4 weeks post-boost (approximately 10 months of age); additionally a random selection of half the participants will contribute blood samples pre-boost (9 months of age) and at the last study visit (18 months of age). Participants in trial arm G will provide 2 blood samples (at enrolment and at 4 weeks post-primary series (approximately 18 weeks of age). All participants will provide 2 nasopharyngeal swabs at approximately 9 and 18 months of age and contribute safety data.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Pneumococcal Infection, Streptococcus Pneumoniae Infection, Invasive Pneumococcal Disease, Protection Against
Keywords
Pneumococcal Vaccines;, Immunogenicity, Vaccine, 10-valent pneumococcal vaccine, 13-valent pneumococcal vaccine, Schedule, Pneumococcal Infection, Kenya, Infant, Vaccines, Conjugate, Humans, Immunization schedule, Streptococcus pneumoniae, vaccine, Dose-Response Relationship, immunologic, Equivalence Trial as Topic

7. Study Design

Primary Purpose
Prevention
Study Phase
Phase 4
Interventional Study Model
Parallel Assignment
Model Description
Participants will be randomised to one of seven groups for the duration of the study: A. Full dose PCV13 vaccination in a 2p+1 schedule; B. 40% fractional dose PCV13 vaccination in a 2p+1 schedule; C. 20% fractional dose PCV13 vaccination in a 2p+1 schedule; D. Full dose PCV10 vaccination in a 2p+1 schedule; E. 40% fractional dose PCV10 vaccination in a 2p+1 schedule; F. 20% fractional dose PCV10 vaccination in a 2p+1 schedule; G. Full dose PCV10 vaccination in a 3p+0 schedule.
Masking
ParticipantInvestigatorOutcomes Assessor
Masking Description
Participants, parents of participants and all of the study team apart from the vaccinator will be masked with respect to the infant's allocation to a trial arm between A-F. If randomly allocated to trial arm G, parents and study personnel will be unmasked due to the necessity for trial arm G to receive a different vaccine schedule compared to trial arms A-F. It is thought that this unmasking will have minimal impact on retention, follow up and outcome assessment across the trial arms for primary and secondary outcomes.
Allocation
Randomized
Enrollment
2100 (Actual)

8. Arms, Groups, and Interventions

Arm Title
Full dose PCV13 (2p+1 schedule)
Arm Type
Active Comparator
Arm Description
Full dose PCV13 administration in 2p+1 schedule
Arm Title
40% dose PCV13 (2p+1 schedule)
Arm Type
Experimental
Arm Description
Fractional (40%) dose PCV13 administration in 2p+1 schedule
Arm Title
20% dose PCV13 (2p+1 schedule)
Arm Type
Experimental
Arm Description
Fractional (20%) dose PCV13 administration in 2p+1 schedule
Arm Title
Full dose PCV10 (2p+1 schedule)
Arm Type
Active Comparator
Arm Description
Full dose PCV10 administration in 2p+1 schedule
Arm Title
40% dose PCV10 (2p+1 schedule)
Arm Type
Experimental
Arm Description
Fractional (40%) dose PCV10 administration in 2p+1 schedule
Arm Title
20% dose PCV10 (2p+1 schedule)
Arm Type
Experimental
Arm Description
Fractional (20%) dose PCV10 administration in 2p+1 schedule
Arm Title
Full dose PCV10 (3p+0 schedule)
Arm Type
Active Comparator
Arm Description
The current vaccine (PCV10) and schedule (3p+0) in use in the Kenyan routine immunisation programme as an additional comparison arm.
Intervention Type
Biological
Intervention Name(s)
PCV10
Other Intervention Name(s)
Synflorix (GlaxoSmithKline plc.), 10-valent pneumococcal conjugate vaccine
Intervention Description
Experimental arms will receive a lower dose of the intervention than the marketed dose.
Intervention Type
Biological
Intervention Name(s)
PCV13
Other Intervention Name(s)
Prevnar 13 (Pfizer Inc.), 13-valent pneumococcal conjugate vaccine, Prevnar13
Intervention Description
Experimental arms will receive a lower dose of the intervention than the marketed dose.
Primary Outcome Measure Information:
Title
Immunogenicity: The ratio of IgG GMCs at 1-month post boost
Description
The ratio of the geometric mean concentrations of IgG after vaccination with 3 full or fractional doses of PCV
Time Frame
4-weeks post-boost (approximately 10 months of age)
Secondary Outcome Measure Information:
Title
Immunogenicity: the proportion of children who 'seroconvert' to vaccine-serotypes after vaccination
Description
The proportion of children with vaccine-serotype specific IgG antibody concentrations more than or equal to 0.35 mcg/ml after vaccination
Time Frame
4-weeks post-primary series (approximately 18 weeks of age)
Title
The proportion of children with evidence of vaccine-serotype carriage
Description
Vaccine-type carriage prevalence across arms
Time Frame
Approximately 18 months of age
Title
The proportion of children with evidence of vaccine-serotype carriage
Description
Vaccine-type carriage prevalents across arms
Time Frame
Approximately 9 months of age
Title
The direct vaccine effectiveness of full/fractional doses of PCV13 against carriage of serotypes 6A and 19A
Description
The direct effectiveness of full/fractional doses of PCV13 in preventing carriage of serotypes 6A and 19A compared to that of full dose PCV10
Time Frame
Approximately 18 months of age
Title
Opsonophagocytic activity of vaccine-induced antibody to 4 serotypes
Description
Functionality of the antibody response
Time Frame
Approximately 18 months of age
Other Pre-specified Outcome Measures:
Title
Immunogenicity: the geometric mean concentration (GMC) of serotype-specific IgG
Description
IgG GMCs elicited post-primary series
Time Frame
4-weeks post-primary series (approximately 18 weeks of age)
Title
Safety: the prevalence of adverse events following immunisation by arm
Description
The proportion fo children with adverse events following immunisation by arm
Time Frame
Infants 6weeks-18 months of age
Title
Immunogenicity: The geometric mean concentration (GMC) of serotype-specific IgG after the primary series of the 2p+1 schedule, prior to boost (9 months of age) and at the end of study follow-up at 18 months of age.
Description
IgG GMCs at 9 and 18 months of age
Time Frame
Approximately 9 and 18 months of age

10. Eligibility

Sex
All
Minimum Age & Unit of Time
6 Weeks
Maximum Age & Unit of Time
8 Weeks
Accepts Healthy Volunteers
Accepts Healthy Volunteers
Eligibility Criteria
Inclusion Criteria: Healthy infants aged 6-8 weeks of age (HIV positive or negative but with no symptoms of current clinical immunosuppression i.e. HIV infection at WHO clinical stage 1); Parents are willing to provide informed consent for their child to participate in the study Parents and infant are likely to remain in the study area until the infant is 18 months of age and comply with study requirements including the requirement to return to the same health facility to obtain all other childhood vaccines. Exclusion Criteria: Infants >8 weeks of age at time of enrolment Signs or symptoms of immunosuppression or HIV infection clinical stage 2 or above. Acute illness (e.g. febrile disease) on the day of vaccination Contraindications precluding vaccination (e.g. hypersensitivity to any component of the vaccine, including diphtheria toxoid) Previous PCV vaccination Family are planning to migrate out of the study areas before the end of the study follow-up Family are planning to obtain the subsequent vaccine doses of the routine immunisation schedule elsewhere and therefore their child may receive a full dose under the routine vaccination programme.
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
J. Anthony G Scott, DTMH FMedSci
Organizational Affiliation
London School of Hygiene & Tropical Medicine, Keppel Street, London
Official's Role
Principal Investigator
Facility Information:
Facility Name
KEMRI Wellcome Trust Research Programme
City
Kilifi
Country
Kenya

12. IPD Sharing Statement

Plan to Share IPD
Yes
IPD Sharing Plan Description
The data will be open access and held in the LSHTM data repository (http://datacompass.lshtm.ac.uk/cgi/request_doc?docid=1); Data access will be granted upon reasonable request after the primary analyses of the trial, as specified, are published.
IPD Sharing Time Frame
After the primary analyses of the trial are published
IPD Sharing Access Criteria
Upon reasonable request with pre-specified hypothesis
IPD Sharing URL
http://datacompass.lshtm.ac.uk/cgi/request_doc?docid=1

Learn more about this trial

The Effect of Fractional Doses of Pneumococcal Conjugate Vaccines on Immunogenicity and Carriage in Kenyan Infants

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