PATRICK ANSAH PRINCIPAL INVESTIGATOR 22/02/2016

Similar documents
Development of a Group A meningococcal conjugate vaccine for sub-saharan Africa: clinical trial results

WHO position paper on meningococcal vaccines

WHO posi)on paper on pneumococcal vaccines. Geneva, Switzerland Published in the Weekly Epidemiological Record on 6 Apr 2012

Public health impact of MenAfriVac: the first four years

Mumps vaccine safety, immunogenicity and recommended use in infants <12 months

WHO posi)on paper on influenza vaccines*

Preven&ng Pertussis: Current and Needed Strategies. June 16, PM 8PM

New vaccine technologies: Promising advances may save more lives

Update on Meningococcal A Vaccine Development and Introduction

Syrian Programme Refugees Advice on assessment of immunisation status and recommendations for additional immunisation

Total population 1,212,110. Live births (LB) 43,924. Children <1 year 40,351. Children <5 years 192,340. Children <15 years 510,594

Immunization Program Resources: Planning and Forecasting Immunization Program Managers Meeting Atlanta, Georgia July 11, 2014

Immuniza(on financing in non-gavi countries

Preven&ng Pertussis: Current and Needed Strategies June 16, PM 8PM

Outbreak response in post- OPV2 withdrawal era. Strategic Advisory Group of Experts (SAGE) on immuniza;on, Geneva, 22 October 2014

Polysaccharide and conjugate vaccine responses

MenA vaccine Introduction Country Experience, Ethiopia

History, implementation and impact of MenA conjugate on disease burden in Africa

WHO position paper on rubella vaccines

ESCMID Online Lecture Library

Summary of Product Characteristics

immunisation in New Zealand

Key events in the development of PsA-TT, a new meningococcal conjugate vaccine

Current National Immunisation Schedule Dr Brenda Corcoran National Immunisation Office.

Family and Travel Vaccinations

School Health Workshop Robert S. Bal2more, M.D. Professor of Pediatrics and Epidemiology Yale School of Medicine Yale School of Public Health

2018/19 Immunisation programmes list of additional and enhanced services

Annex 3 Recommendations for the production and control of group C meningococcal conjugate vaccines (Addendum 2003)

SAGE recommendations on non-specific effects of vaccines and their implementation

NHS public health functions agreement Service specification No. 31 Meningococcal group B (MenB) programme

Recommendations for the production and control of group C meningococcal conjugate vaccines

Report from the Polio Working Group Mee5ng. Yagob Al- Mazrou Chair, SAGE Working Group April 12, 2016

Total population 1,265,308,000. Live births (LB) 27,016,000. Children <1 year 25,928,200. Children <5 years 23,818,000. Children <15 years 25,639,000

NHS public health functions agreement Service specification No.6 Meningococcal C (MenC) containing vaccine immunisation programme

Total population 20,675,000. Live births (LB) 349,715. Children <1 year 346,253. Children <5 years 1,778,050. Children <15 years 5,210,100

Study No.: Title: Rationale: Phase: Study Period: Study Design: Centres: Indication: Treatment: Objectives: Primary Outcome/Efficacy Variable:

MVP as an example of a project managed approach to develop a needed vaccine

2017/18 Immunisation programmes list of additional and enhanced services

Expanded Programme on Immunization (EPI)

Public Health Wales Vaccine Preventable Disease Programme

Part C. Clinical evaluation of group C meningococcal conjugate vaccines (Revised 2007)

Conflicts of interest. Pulmonary rehabilita8on. Objec8ves / Outline. Pulmonary rehabilita8on in COPD. Pulmonary rehabilita8on in COPD

From development to delivery: Decision-making for the introduction of a new vaccine

Medical Innovation changing business model. Marie-Paule Kieny, WHO-WIPO-WTO, 5 July 2013

Total population 24,759,000. Live births (LB) 342,458. Children <1 year 337,950. Children <5 years 1,698,664. Children <15 years 5,233,093

NHS public health functions agreement

Antibody Persistence 1 5 Years Following Vaccination With MenAfriVac in African Children Vaccinated at Months of Age

MenC. MenW MenY

Is Immunological Tolerance a Real Concern? William Moss

Pertussis Outbreak Investigation Report. Office of the Chief Medical Officer of Health

Protocol Synopsis. Administrative information

Meningococcal disease and vaccination in the UK

Study No.: Title: Rationale: Phase: Study Period: Study Design Centers: Indication: Treatment: Objectives: Primary Outcome/Efficacy Variable:

The MenAfrivac Experience A Successful Approach. Dr Bernard FRITZELL BFL conseils France

The Danish childhood vaccination program SUMMARY IN ENGLISH

Immunisation Update for Occupational Health

2016/17 Vaccination and Immunisation list of additional services and enhanced services

Table 1: Basic information (per 1,000 LB) 42.4 (per 1,000 LB) 49.7 (per 1,000 LB) 215 (per 100,000 LB)

WHO posi)on paper on hepa))s A vaccines

Protocol. This trial protocol has been provided by the authors to give readers additional information about their work.

Childhood Immunisations Template Guide 2016

VACCINES TRIUMPHS AND TRIBULATIONS. William Schaffner, MD Chairman, Department of Preventive Medicine Vanderbilt University School of Medicine

Invasive Meningococcal Disease - prevention through vaccination

VII THE CHILDHOOD IMMUNISATION PROGRAMME IN SINGAPORE 7. 7

7.0 Nunavut Childhood and Adult Immunization Schedules and Catch-up Aids

Study No.: Title: Rationale: Phase: Study Period: Study Design: Centers: Indication: Treatment: Objectives: Primary Outcome/Efficacy Variable:

Manitoba Health, Healthy Living and Seniors

Conflicts of interest. Objec5ves / Outline. Pulmonary rehabilita5on. Pulmonary rehabilita5on in COPD. Pulmonary rehabilita5on in COPD 11/26/13

Addendum to IPV Introduction Guidelines based on Recommendations of India Expert Advisory Group (IEAG)

Childhood Immunisations Template Guide 2017

Routine Immunization Schedules. Section 2. Newfoundland and Labrador Immunization Manual. Routine Immunization Schedules

TETANUS CONTAINING VACCINE AND EXPERIENCE OF WHO- PQ AND NEW REGISTRATION IN OVERSEAS COUNTRIES. DCVMN-Medigen Workshop from 6-10 March 2017, Taipei

Global and National Trends in Vaccine Preventable Diseases. Dr Brenda Corcoran National Immunisation Office.

Appendix An Assessment Tool to Determine the Validity of Vaccine Doses

OVERVIEW OF THE NATIONAL CHILDHOOD IMMUNISATION PROGRAMME IN SINGAPORE

To demonstrate that DTPa-HBV-IPV/Hib-MenC-TT co-administered with 10Pn, is non-inferior to DTPa-HBV-IPV/Hib coadministered

GAVI ALLIANCE: UPDATE AND FUTURE DIRECTIONS FOR GLOBAL VACCINES AND IMMUNISATIONS

Acceptability of mul0ple injec0ons during a single vaccina0on visit in South Africa and Tanzania

Immunisation Subcommittee of PTAC Meeting held 18 February 2015

Vaccines: Past, Present, and Future. Tapani Ronni, PhD

RECOMMENDED IMMUNIZATIONS

- Infanrix hexa (DTPa-HBV-IPV/Hib): GSK Biologicals combined diphtheria, tetanus, acellular pertussis, hepatitis

NHS public health functions agreement

Immunize. Prevent what s preventable Stakeholder Mee1ng.

kernfamilyhealthcare.com. Si necesita esta información en español, por favor llámenos.

Changes to the Meningococcal C conjugate (MenC) vaccine schedule. Questions and Answers

Current Status of PCV Use and WHO Recommendations

Hyporesponsiveness: Time To Stop Using Meningococcal Polysaccharide Vaccines?

Welcome! Pragmatic Clinical Studies. David Hickam, MD, MPH Program Director Clinical Effectiveness Research. David Hickam, MD, MPH

Invasive Meningococcal Disease - prevention through vaccination

Adult Immunizations. Business Health Care Group (BHCG) April 25, Cathy Edwards. Immunization Program Advisor

School Year ALASKA CHILD CARE & SCHOOL IMMUNIZATION REQUIREMENT CHANGES

Global Health Policy: Vaccines

PDF of Trial CTRI Website URL -

Summer!2016! Undergraduate! Research! Internships!

CDC.gov. Immuniza(on Update: What Providers Need to Know. Vaccine Preventable Diseases 8/31/14

Outsourcing in Clinical Trials 1-2 July 2015

Classification: official 1

NHS public health functions agreement

Transcription:

Evaluation of the Men A specific antibody persistence in Ghanaian children more than five years after immunization with PsA-TT (2.5 μg, 5 μg, or 10 μg polysaccharide concentration) PATRICK ANSAH PRINCIPAL INVESTIGATOR 22/02/2016

Study Ra)onale Circula=ng an=bodies are needed for protec=on from acute meningococcal infec=on. Immune persistence studies are essen=al components of the evalua=on of new meningococcal vaccines. Understanding long term immune persistence helps to inform SAGE and MOH on schedules and vaccina=on programme recommenda=ons and decisions. This study will explore the circula=ng bactericidal an=bodies and IgG concentra=ons in infants and toddler who took part in early vaccine trials during MenAfriVac development programme. This study provides a great opportunity to document the longest term dura=on of the immune response to PsA-TT to date for EPI considera=ons 2 2/7/16

Alignment of Study with Policy Gaps WHO Recommenda)ons for EPI Introduc)on MenAfriVac5 should be used for rou=ne immuniza=on - infants and young children 3-24 mo A 1-dose schedule, at 9 18 months of age based on local programma=c and epidemiologic considera=ons is preferred. If in a specific context there is a compelling reason to vaccinate infants younger than 9 months, a 2-priming dose infant schedule should be used star=ng at 3 months of age, with doses at least 8 weeks apart. One =me catch-up campaign for birth cohorts born since the ini=al mass vaccina=on and which would not be within the age range targeted by the rou=ne immuniza=on schedule. MenAfriVac10 should be used for catch-up and periodic campaigns from 12 months of age onwards unless bridging studies have been conducted and show that MenAfriVac5 can be used in older age groups. Gaps highlighted in the WHO recommenda)on: The need for a booster dose has not been established MenAfriVac 5 µg response is not known in older children 3 20 FEBRUARY 2015, No. 8, 2015, 90, 57 68 h7p://www.who.int/wer

Objec)ve and hypothesis Hypothesis One or more doses of Men A vaccine given in early childhood induces long-term (beyond 5 years) sustained levels of meningococcal A an=bodies. Objec=ves To measure meningococcal group A an=body persistence up to and beyond 5 years aaer vaccina=on in infants and toddlers. Addi=onally other assays will be done to characterise the immune persistence of EPI an=gens up to and beyond five years aaer infant vaccina=on. 4 2/7/16

Study Design This is a longitudinal observa=onal study with 2 =me point surveys at ~5 and again at ~6 years post the final PsA-TT immuniza=on in children who originally received a completed vaccina=on series of PsA-TT in trial PsA-TT-004. A new comparator arm was included: Children who par=cipated in the MenAfriVac campaign of 2012 Matched in terms of age of vaccina=on (12-18 months) with the group who received a single dose of PsA-TT 10 μg (group 3) This provides evidence of persistence from a real =me sefng, while giving a benchmark for the comparison and interpreta=on of all study groups in light of herd immunity post community campaigns. 5 2/7/16

Study Popula)on Study area: Kassena Nankana West District and Kassena Nankana Municipality, Northern Ghana Former subjects from study MVP-PsA-TT-004 who completed their PsA-TT vaccina=on assignment during the study and had their last study visit blood draw at 36 months. A new control group matched in terms of age (12 to 18 months) at =me of vaccine administra=on during the MenAfriVac campaign in 2012 with documenta=on of vaccina=on. 6 2/7/16

Past and Current 004 Study Design 2008-2010 2011-12 2012 n (target) 2015 2016 Pers-004 study Ghana Mass Campaign occurred Date of last Last 9 12 12 18 over 60 days PER 1 PER 2 study Blood mos. mos. (Oct-Nov) 868 Visit Visit vaccina=on Draw Original study PsA-TT-004 - vaccina=on design and age at first vaccina=on Study groups 14 18 wks. PsA-TT-004 Study Pers-004 Study Design A 2.5μg 2.5μg -- 176 1 B 5μg 5μg -- Sep 2011 Poten=al to 175 Mar-10 May have received C 10 µg 10 µg booster 2012 168 during mass campaign 2 -- 10μg -- 170 Blood draw > 5 yrs post final study vaccina=on Blood draw > 6 yrs post final study vaccina=on 3 -- -- 10μg Oct-10 179 10μg 12-18 mos. New Control 160 Based on defined criteria, 868 subjects from PsA-TT-004 were eligible to par)cipate in persistence study 7

Study Endpoints Main endpoint is assessment of immunogenicity. Serum Bactericidal Ac=vity (SBA) A validated assay using baby rabbit complement (rsba) will be used to measure the level (=ter) of func=onal an=body in human sera to Neisseria meningi=dis group A. An=-PsA IgG (ELISA) To measure total IgG levels of an=body (specific IgG concentra=ons) to Neisseria meningi=dis group A capsular polysaccharide. The concentra=on of specific IgG an=bodies in human sera is determined using human standard reference serum pools and appropriate controls Immune responses to various EPI vaccines: measles, diphtheria, pertussis, tetanus, HepB, Hib. Both Men assays are performed by Public Health England, Manchester, UK. 8

Current status Visit 1 Sep-Dec 2015 PsA-TT-004 subjects New Control subjects Invited Recruited Could not be located/ Migrated Refusal to par)cipate Deceased 868 775 68 20 5 160 160 Total 1028 935 All Visit 1 samples for primary analysis and EPI tes=ng have been shipped and lab tes=ng is ongoing. Expec=ng results of interim analysis in May 2016 9

Records of Meningi)s vaccines in study subjects Pers-004 Entered Former study subjects At least 1 dose of Campaign MenAfriVac 775 313 (40.4%)* (of which 213 with a vaccina=on record, remainder oral recollec=on) At least 1 dose of Meningi)s vaccine (other or unspecified received during other reac)ve campaigns) 135 (17.4%) (of which 59 had the campaign dose) No Addi)onal Meningi)s vaccine 386 (49.8%) New control 160 100% 15 (9.4%) 145 (90.6%) *Equal distribu=on of campaign dose across previous treatment groups Provides poten=al to assess a MenAfriVac 10 µg booster given > 2 yrs post primary vaccina=on (Primary vaccina=on +/- Booster) 10

Data Analysis Assess immune response in subjects who received primary vaccina=on and in those who received primary vaccina=on + campaign dose >2 years later. Assess for differences in immune response >5 yrs based on primary vaccina=on dose and schedule Assessment of an=body levels What is a protec=ve immune threshold? 1:128 rsba 2 mcg IgG If responses are adequate, con=nue with second blood draw yr 2 If subject responses are inadequate consider a Protocol amendment: Provide a MenAfriVac 5µg boost and measure responses pre and 28 days post vaccina=on Provide data to SAGE on older age 5 µg response 11

Audience Discussion Assessment of an=body levels What should be considered as the protec=ve immune threshold? 1:128 rsba, 1:8 rsba (lower limit of quan=fica=on)? 2 mcg IgG? > 0.2 mg/ml (lower limit of quan=fica=on)? If subject responses are inadequate should 5 µg vaccina=on be tested (boost)? All or only subset with inadequate response at 5 year =me point? Only test 5 µg (limited subject numbers)? 12

PARTNERS/Collaborators Site: Navrongo Health Research Centre, Ghana Study Monitor: FHI360 Data Management: DiagnoSearch Life Sciences Pvt. Ltd External Laboratory: Public Health England Sponsor: Meningi=s Vaccine Sustainability Project (PATH) Advisors: Serum Ins=tute of India (SIIPL) World Health Organiza=on Funder: Bill & Melinda Gates Founda=on 13

14

Mali Persistence Study (PERS-007) Similar hypothesis as Ghana Study, n=1200 (007), n=160 new age matched control Assess persistence post any circula=ng Men A (campaign in 2010) Dose in study aligns with current plans for a single 5 µg dose in 9-18 mo and campaign dose of 10 µg >1 yr old Allows immune persistence comparison of 5 vs 10 µg in young children over a long period Poten=al to test these children pre and post the catch up campaign being planned in Mali in 2017 (as they would be captured by this campaign) 2010 2011 2012-2013 2014 2015 2016 2017-2018 007 Treatment Groups and Timing Current Alterna=ve Study Design 15 18 Date of Pers-007 study 9 12 mos mos last Vax 10μg 10μg Sep-13 5μg 5μg Sep-13 10μg -- Dec-12 Mali MenAfriVac campaign 5μg -- Dec-12 1 blood draw (3-4 yrs post vaccina=on) 1 blood draw pre catch up campaign 1 blood draw post catch up campaign 15 01/03/16

2024 © healthdocbox.com Privacy Policy | Terms of Service | Feedback