Your search keyword '"Heath, PT"' showing total 44 results

1. Maternal immunization against Group B streptococcus: World Health Organization research and development technological roadmap and preferred product characteristics

Author

Vekemans, J, Moorthy, V, Friede, M, Alderson, MR, Sobanjo-Ter Meulen, A, Baker, CJ, Heath, PT, Madhi, SA, Mehring-Le Doare, K, Saha, SK, Schrag, S, and Kaslow, DC

Subjects

Clinical Trials as Topic, Biomedical Research, Group B streptococcus, Streptococcal Vaccines, Infant, Newborn, Infant, Legislation, Drug, World Health Organization, Antibodies, Bacterial, Article, Streptococcus agalactiae, Gastrointestinal Tract, Technology Transfer, Pregnancy, Maternal immunization, Child, Preschool, Streptococcal Infections, Vagina, Humans, Female, Immunization, Vaccine

Abstract

Group B streptococcus, found in the vagina or lower gastrointestinal tract of about 10-40% of women of reproductive age, is a leading cause of early life invasive bacterial disease, potentially amenable to prevention through maternal immunization during pregnancy. Following a consultation process with global stakeholders, the World Health Organization is herein proposing priority research and development pathways and preferred product characteristics for GBS vaccines, with the aim to facilitate and accelerate vaccine licensure, policy recommendation for wide scale use and implementation.

Published

2019

2. Antibody kinetics between birth and three months of life in healthy infants with natural exposure to Group B streptococcus: A UK cohort study.

Author

Karampatsas K, Hall T, Voysey M, Carreras-Abad C, Cochet M, Ramkhelawon L, Peregrine E, Andrews N, Heath PT, and Le Doare K

Subjects

Humans, Infant, Female, Infant, Newborn, Male, United Kingdom, Fetal Blood immunology, Cohort Studies, Pregnancy, Adult, Serogroup, Immunity, Maternally-Acquired, Antibodies, Bacterial blood, Antibodies, Bacterial immunology, Streptococcus agalactiae immunology, Immunoglobulin G blood, Streptococcal Infections immunology

Abstract

Introduction: Capsular polysaccharide (CPS) serotype-specific Immunoglobulin G (IgG) in cord blood has been proposed as a correlate of protection against invasive Group B Streptococcus (iGBS) disease. Although protective levels are required in infants throughout the window of vulnerability up to 3 months of age, little is known regarding the kinetics of GBS-specific IgG over this period., Methods: We enrolled 33 healthy infants born to mothers colonized with GBS. We collected cord blood and infant blood samples either at one (21-35 days), two (49-63 days), or three months of age (77-91 days). We measured GBS serotype-specific CPS IgG concentrations and calculated the decay rate using a mixed-effects model. We further explored whether the antibody kinetics were affected by common maternal and infant factors and estimated the correlation between IgG concentration at birth and one, two, and three months of age., Results: The half-life estimate of IgG concentration for homologous and non-homologous GBS serotypes in paired samples with detectable IgG levels at both time points was 27.4 (95 % CI: 23.5-32.9) days. The decay rate did not vary by maternal age (p = 0.7), ethnicity (p = 0.1), gravida (p = 0.1), gestation (p = 0.7), and infant sex (p = 0.1). Predicted IgG titres above the assay lower limit of quantification on day 30 strongly correlated with titres at birth (Spearman correlation coefficient 0.71 [95 % CI: 0.60-0.80])., Conclusion: Our results provide a basis for future investigations into the use of antibody kinetics in defining a serocorrelate of protection against late-onset iGBS disease., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: [Paul Heath reports financial support was provided by National Institute for Health Research. MV is a contributor to intellectual property licensed by Oxford University Innovation to AstraZeneca. PTH has conducted studies on behalf of St George’s University of London funded by GBS vaccine manufacturers, including Minervax and Pfizer, but receives no personal funding for these activities. KLD is supported by Future Leaders Fellowships by UK Research and Innovation Future Leaders Fellowship (MR/S016570/1) and has conducted studies on behalf of St George’s University of London funded by GBS vaccine manufacturers, including Minervax and Pfizer, but receives no personal funding for these activities. The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper.]., (Copyright © 2024 The Authors. Published by Elsevier India Pvt Ltd. All rights reserved.)

Published

2024

3. Omicron BA.1-containing mRNA-1273 boosters compared with the original COVID-19 vaccine in the UK: a randomised, observer-blind, active-controlled trial.

Author

Lee IT, Cosgrove CA, Moore P, Bethune C, Nally R, Bula M, Kalra PA, Clark R, Dargan PI, Boffito M, Sheridan R, Moran E, Darton TC, Burns F, Saralaya D, Duncan CJA, Lillie PJ, San Francisco Ramos A, Galiza EP, Heath PT, Girard B, Parker C, Rust D, Mehta S, de Windt E, Sutherland A, Tomassini JE, Dutko FJ, Chalkias S, Deng W, Chen X, Feng J, Tracy L, Zhou H, Miller JM, and Das R

Subjects

Humans, 2019-nCoV Vaccine mRNA-1273, SARS-CoV-2 genetics, Antibodies, Neutralizing, United Kingdom, Immunogenicity, Vaccine, Antibodies, Viral, COVID-19 Vaccines, COVID-19 prevention & control

Abstract

Background: The omicron BA.1 bivalent booster is used globally. Previous open-label studies of the omicron BA.1 (Moderna mRNA-1273.214) booster showed superior neutralising antibody responses against omicron BA.1 and other variants compared with the original mRNA-1273 booster. We aimed to compare the safety and immunogenicity of omicron BA.1 monovalent and bivalent boosters with the original mRNA-1273 vaccine in a large, randomised controlled trial., Methods: In this large, randomised, observer-blind, active-controlled, phase 3 trial in the UK (28 hospital and vaccination clinic sites), individuals aged 16 years or older who had previously received two injections of any authorised or approved COVID-19 vaccine, with or without an mRNA vaccine booster (third dose), were randomly allocated (1:1) using interactive response technology to receive 50 μg omicron BA.1 monovalent or bivalent vaccines or 50 μg mRNA-1273 administered as boosters via deltoid intramuscular injection. The primary outcomes were safety and immunogenicity at day 29, including prespecified non-inferiority and superiority of booster immune responses, based on the neutralising antibody geometric mean concentration (GMC) ratios of the monovalent and bivalent boosters compared with mRNA-1273. Safety was assessed in all participants who received first or second boosters, and primary immunogenicity outcomes were assessed in all participants who received the planned booster dose, had pre-booster and day 29 antibody data, had no major protocol deviations, and who were SARS-CoV-2-negative. The study is registered with EudraCT (2022-000063-51) and ClinicalTrials.gov (NCT05249829) and is ongoing., Findings: Between Feb 16 and March 24, 2022, 724 participants were randomly allocated to receive omicron BA.1 monovalent (n=366) or mRNA-1273 (n=357), and between April 2 and June 17, 2022, 2824 participants were randomly allocated to receive omicron BA.1 bivalent (n=1418) or mRNA-1273 (n=1395) vaccines as second boosters. Median durations (months) between the most recent COVID-19 vaccine and study boosters were similar for omicron BA.1 monovalent (4·0 months [IQR 3·6-4·7]) and mRNA-1273 (4·1 [3·5-4·7]), and for the omicron BA.1 bivalent (5·5 [4·8-6·2]) and mRNA-1273 (5·4 [4·8-6·2]) boosters. The omicron BA.1 monovalent and bivalent boosters elicited superior neutralising GMCs against the omicron BA.1 variant compared with mRNA-1273, with GMC ratios of 1·68 (99% CI 1·45-1·95) and 1·53 (1·41-1·67) at day 29 post-booster doses in participants without previous SARS-CoV-2 infection. Both boosters induced non-inferior ancestral SARS-CoV-2 (Asp614Gly) immune responses with GMCs that were similar for the bivalent (2987·2 [95% CI 2814·9-3169·9]) versus mRNA-1273 (2911·3 [2750·9-3081·0]) and lower for the monovalent (2699·7 [2431·3-2997·7] vs 3020·6 [2776·5-3286·2]) boosters, with respective GMC ratios of 1·05 (99% CI 0·96-1·15) and 0·82 (95% CI 0·74-0·91). Results were comparable regardless of previous SARS-CoV-2 infection status. Incidences of solicited adverse reactions with the omicron BA.1 monovalent (335 [91·3%] of 367 participants) and omicron BA.1 bivalent (1285 [90·4%] of 1421 participants) boosters were similar to those observed previously for mRNA-1273, with no new safety concerns identified and no occurrences of fatal adverse events., Interpretation: Omicron-containing booster vaccines generated superior immunogenicity against omicron BA.1 and comparable immunogenicity against the original strain with no new safety concerns. It remains important to continuously monitor the immune responses and real-world vaccine effectiveness as divergent SARS-CoV-2 variants emerge., Funding: Moderna., Competing Interests: Declaration of interests ITL, BG, CP, DR, SM, EdW, AS, SC, WD, XC, JF, LT, HZ, JMM, and RD are employees of Moderna and hold stock or stock options in the company. PM reports being a speaker or adviser for and receiving research grants from GSK, Sanofi, Novavax, Moderna, MSD, Janssen, Medicago, and AstraZeneca. CB reports being a National Specialty Advisor (NHS England) Immunology and Allergy and receiving funding to their institution to undertake vaccine trials for Janssen, Moderna, AstraZeneca, and Valneva. RN reports being Research Lead for Cambridge and Peterborough Integrated Care Board; and receiving grants from GSK and Novavax. PAK reports being a speaker or adviser for and receiving travel or research grants from GSK, Pfizer, Pharmacosmos, Astellas, Vifor, AstraZeneca, Bayer, Unicyte, Evotec, Fresenius, and Otsuka. PID reports receiving research grants for COVID-19 research studies from Moderna, AstraZeneca, Janssen, and Atea. MBo reports being a speaker or adviser for GSK, Atea, ViiV, MSD, Janssen, Gilead, Cipla, Mylan, and Roche; and receiving research grants from ViiV, MSD, Janssen, Gilead, Novavax, Valneva, and Moderna. FB reports receiving speaker fees and a research grant to their institution from Gilead Sciences. CJAD reports receiving grants from the Wellcome Trust and the Medical Research Council. ASFR reports receiving research grants (to their organisation) from Pfizer, Novavax, Valneva, Moderna, and Janssen. PTH reports being a speaker or adviser for and receiving research grants from Pfizer, Novavax, Valneva, Moderna, and Janssen. JET and FJD are Moderna contractors. All other authors declare no competing interests., (Copyright © 2023 Elsevier Ltd. All rights reserved.)

Published

2023

4. Effect of maternal immunisation with multivalent vaccines containing inactivated poliovirus vaccine (IPV) on infant IPV immune response: A phase 4, multi-centre randomised trial.

Author

Grassly NC, Andrews N, Cooper G, Stephens L, Waight P, Jones CE, Heath PT, Calvert A, Southern J, Martin J, and Miller E

Subjects

Pregnancy, Humans, Infant, Female, Child, Preschool, Middle Aged, Vaccines, Combined, Poliovirus Vaccine, Inactivated adverse effects, Immunization, Secondary, Diphtheria-Tetanus-Pertussis Vaccine, Vaccination, Bacterial Vaccines, Antibodies, Bacterial, Diphtheria-Tetanus-acellular Pertussis Vaccines adverse effects, Poliovirus, Haemophilus Vaccines

Abstract

Multivalent diphtheria, tetanus, acellular pertussis and inactivated poliovirus vaccine (DTaP/IPV) has been offered to pregnant women in the United Kingdom since 2012. To assess the impact of maternal DTaP/IPV immunisation on the infant immune response to IPV, we measured poliovirus-specific neutralising antibodies at 2, 5 and 13 months of age in a randomised, phase 4 study of Repevax or Boostrix/IPV in pregnancy and in a non-randomised group born to women not given DTaP/IPV in pregnancy. Infants whose mothers received DTaP/IPV were less likely to seroconvert after three IPV doses than those whose mothers did not receive DTaP/IPV. At 13 months of age, 63/110 (57.2 %), 46/108 (42.6 %) and 40/108 (37.0 %) were seropositive to types 1 to 3, compared with 20/22 (90.9 %), 20/22 (90.9 %) and 14/20 (70.0 %) (p-values 0.003, <0.001 and 0.012). UK infants whose mothers are given DTaP/IPV in pregnancy may be insufficiently protected against poliomyelitis until their pre-school booster., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published

2023

5. An observational, cohort, multi-centre, open label phase IV extension study comparing preschool DTAP-IPV booster vaccine responses in children whose mothers were randomised to one of two pertussis-containing vaccines or received no pertussis-containing vaccine in pregnancy in England.

Author

Sapuan S, Andrews N, Hallis B, Hole L, Jones CE, Matheson M, Miller E, Snape MD, and Heath PT

Subjects

Child, Preschool, Female, Humans, Infant, Pregnancy, Antibodies, Bacterial blood, Immunoglobulin G blood, Poliomyelitis prevention & control, Vaccines, Combined administration & dosage, Whooping Cough prevention & control, Diphtheria-Tetanus-acellular Pertussis Vaccines administration & dosage, Immunization, Secondary, Poliovirus Vaccine, Inactivated administration & dosage

Abstract

An antenatal pertussis vaccination programme was introduced in 2012 in the UK in the context of a national outbreak of pertussis. It has been shown that a lower antibody response to primary immunisation can be seen for certain pertussis antigens in infants born to women who received pertussis-containing antenatal vaccines, a phenomenon known as blunting. The longer-term impact of this has not been documented previously, and accordingly was evaluated in this study. Children were predominantly recruited from a previous study in which their mothers had received acellular pertussis-containing antenatal vaccines (dTaP 3 -IPV [diphtheria toxoid, tetanus toxoid, three antigen acellular pertussis and inactivated polio] or dTaP 5 -IPV [diphtheria toxoid, tetanus toxoid, five antigen acellular pertussis and inactivated polio]), or no pertussis-containing vaccine. Blood samples were obtained prior to and one month after the acellular pertussis-containing preschool booster (dTaP 5 -IPV) was given at around age 3 years 4 months. Pre- and post-booster immunoglobulin G (IgG) geometric mean concentrations (GMCs) against pertussis toxin, filamentous haemagglutinin, fimbriae 2 & 3, and pertactin, were compared. Prior to the receipt of the preschool booster, there was no difference in the IgG GMCs against pertussis-specific antigens between children born to women vaccinated with dTaP 3 -IPV and dTaP 5 -IPV; however, IgG GMCs against pertussis toxin were significantly lower in children born to women vaccinated with dTaP 3 -IPV compared with children born to unvaccinated women (geometric mean ratio 0.42 [95 % CI 0.22-0.78], p = 0.03). One month after the receipt of the preschool booster there was no differences between the groups. The blunting effect of antenatal pertussis vaccine on pertussis responses in children can persist until preschool age, although it is overcome by the administration of a booster dose. ClinicalTrials.gov registration number: NCT03578120., Competing Interests: Declaration of Competing Interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: ‘Matthew Snape is the director of NISEC, and Paul Heath and Bassam Hallis are members of the NISEC steering committee, but none of them have received any personal funding from NISEC. Christine Jones and Paul Heath have conducted studies on behalf of St George’s University of London (Paul Heath), University of Southampton (Christine Jones) and University Hospital Southampton NHS Foundation Trust (Christine Jones), funded by vaccine manufacturers, including Glaxo Smith Kline (Paul Heath), Medicago (Christine Jones), MinervaX (Christine Jones, Paul Heath), Moderna (Christine Jones), Novovax (Christine Jones), Pfizer (Christine Jones) and ReViral (Christine Jones) within the last three years, but received no personal funding from these sources. Christine Jones has carried out consultancy or been a member of an advisory board or data safety and monitoring board for Moderna, MSD, Pfizer, and Sanofi in the last three years, and she has received remuneration for these activities.’, (Copyright © 2022 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2022

6. Methodology for a correlate of protection for group B Streptococcus: Report from the Bill & Melinda Gates Foundation workshop held on 10 and 11 February 2021.

Author

Gilbert PB, Isbrucker R, Andrews N, Goldblatt D, Heath PT, Izu A, Madhi SA, Moulton L, Schrag SJ, Shang N, Siber G, and Sobanjo-Ter Meulen A

Subjects

Child, Fetal Blood, Humans, Immunoglobulin G, Infant, Infant, Newborn, Serogroup, Streptococcus agalactiae, Vaccination, Streptococcal Infections prevention & control

Abstract

Worldwide, childhood mortality has declined significantly, with improvements in hygiene and vaccinations against common childhood illnesses, yet newborn mortality remains high. Group B Streptococcus (GBS) disease significantly contributes to newborn mortality and is the leading cause of meningitis in infants. Many years of research have demonstrated the potential for maternal vaccination against GBS to confer protection to the infant, and at least three vaccine candidates are currently undergoing clinical trials. Given the relatively low disease incidence, any clinical vaccine efficacy study would need to include at least 40,000 to 60,000 participants. Therefore, a path to vaccine licensure based on a correlate of protection (CoP) would be the preferred route, with post-approval effectiveness studies demonstrating vaccine impact on reduction of disease burden likely to be required as part of conditional marketing approval. This workshop, hosted by the Bill & Melinda Gates Foundation on 10 and 11 February 2021, discussed considerations and potential statistical methodologies for establishing a CoP for GBS disease. Consensus was reached that an antibody marker with global threshold predictive of a high level of vaccine protection would be most beneficial for licensure assessments. IgG binding antibody in cord blood would likely serve as the CoP, with additional studies needed to confirm a high correlation with functional antibody and to demonstrate comparable kinetics of natural versus vaccine-induced antibody. Common analyses of ongoing seroepidemiological studies include estimation of absolute and relative disease risk as a function of infant antibody concentration, with adjustment for confounders of the impact of antibody concentration on infant GBS disease including gestational age and maternal age. Estimation of an antibody concentration threshold indicative of high protection should build in margin for uncertainties from sources including unmeasured confounders, imperfect causal mediation, and variability in point and confidence interval estimates across regions and/or serotypes., (Copyright © 2022.)

Published

2022

7. Post-licensure observational safety study after meningococcal B vaccine 4CMenB (Bexsero) vaccination within the routine UK immunisation program.

Author

Hall GC, Douglas I, Heath PT, Prabhakar P, Rosillon D, Khan J, and Abbing-Karahagopian V

Subjects

Child, Humans, Infant, United Kingdom epidemiology, Vaccination, Meningococcal Infections epidemiology, Meningococcal Infections prevention & control, Meningococcal Vaccines adverse effects, Neisseria meningitidis, Serogroup B

Abstract

The study investigated the safety of 4-component meningococcal serogroup B vaccination (4CMenB) in routine care. 4CMenB exposure and seizures, febrile seizures and Kawasaki disease were identified from The Health Improvement Network (THIN) database of UK electronic primary healthcare records, 2015-2018. A self-controlled case series analysis was completed. Anaphylaxis, Guillain-Barré syndrome and acute disseminated encephalomyelitis were secondary outcomes. A total of 107,231 children aged 1-18 months received ≥1 doses of 4CMenB vaccination. Most 4CMenB exposure (93%) was on the same day as other vaccines within a complete national immunisation program stage. With day 0 as day of vaccination, 43 seizures occurred in days 0-6 after 239,505 doses, and 23 febrile seizures occurred in days 0-6, and 4 Kawasaki disease cases in days 1-28 after 194,929 4CMenB doses. Adjusted incidence rate ratios including all 4CMenB exposures were 1.43 (95%CI: 1.02-2.02) for seizures and 1.72 (95%CI: 1.08-2.75) for febrile seizures. There were insufficient cases to model Kawasaki disease, and no cases of the secondary outcomes in risk periods when they may be associated with the vaccination. This study shows few cases of the outcomes after vaccination including 4CMenB with an increased risk of seizures and febrile seizures. It is not possible to attribute the finding to one specific vaccination as the majority of 4CMenB was given with other vaccinations. Trial registration: NA., Competing Interests: Declaration of Competing Interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: GCH received payment from IQVIA for the conduct of the current study, and payment for consultancy from the GSK group of companies outside the submitted work and has received funding for research and consultancy from a number of pharmaceutical and healthcare companies outside the submitted work. ID received payment from IQVIA for the conduct of the current study, and payment from the GSK group of companies outside the submitted work; PTH received indirect payment from Novartis, Novavax, Pfizer, and the GSK group of companies, outside the submitted work; PP received consulting fees from IQVIA for the current study, and Amgen, BMS, Novartis and the GSK group of companies, outside the submitted work; DR was employed by and held shares from the GSK group of companies; JK received payment from IQVIA for the conduct of the current study; VAK is employed by the GSK group of companies. All authors declare no other financial and non-financial relationships and activities., (Copyright © 2021 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2021

8. Meningococcal carriage in periods of high and low invasive meningococcal disease incidence in the UK: comparison of UKMenCar1-4 cross-sectional survey results.

Author

MacLennan JM, Rodrigues CMC, Bratcher HB, Lekshmi A, Finn A, Oliver J, Wootton M, Ray S, Cameron C, Smith A, Heath PT, Bartolf A, Nolan T, Hughes S, Varghese A, Snape MD, Sewell R, Cunningham R, Stolton A, Kay C, Palmer K, Baxter D, Suggitt D, Zipitis CS, Pemberton N, Jolley KA, Bray JE, Harrison OB, Ladhani SN, Pollard AJ, Borrow R, Gray SJ, Trotter C, and Maiden MCJ

Subjects

Adolescent, Cross-Sectional Studies, Female, Humans, Incidence, Male, Neisseria meningitidis, Neisseria meningitidis, Serogroup C, Prevalence, Risk Factors, Serogroup, United Kingdom epidemiology, Vaccination, Young Adult, Carrier State prevention & control, Meningococcal Infections epidemiology, Meningococcal Infections prevention & control, Meningococcal Vaccines immunology

Abstract

Background: The incidence of invasive meningococcal disease in the UK decreased by approximately four times from 1999 to 2014, with reductions in serogroup C and serogroup B disease. Lower serogroup C invasive meningococcal disease incidence was attributable to implementation of the meningococcal serogroup C conjugate vaccine in 1999, through direct and indirect protection, but no vaccine was implemented against serogroup B disease. UK Meningococcal Carriage surveys 1-3 (UKMenCar1-3), conducted in 1999, 2000, and 2001, were essential for understanding the impact of vaccination. To investigate the decline in invasive meningococcal disease incidence, we did a large oropharyngeal carriage survey in 2014-15, immediately before the changes to meningococcal vaccines in the UK national immunisation schedule., Methods: UKMenCar4 was a cross-sectional survey in adolescents aged 15-19 years who were enrolled from schools and colleges geographically local to one of 11 UK sampling centres between Sept 1, 2014, and March 30, 2015. Participants provided an oropharyngeal swab sample and completed a questionnaire on risk factors for carriage, including social behaviours. Samples were cultured for putative Neisseria spp, which were characterised with serogrouping and whole-genome sequencing. Data from this study were compared with the results from the UKMenCar1-3 surveys (1999-2001)., Findings: From the 19 641 participants (11 332 female, 8242 male, 67 not stated) in UKMenCar4 with culturable swabs and completed risk-factor questionnaires, 1420 meningococci were isolated, with a carriage prevalence of 7·23% (95% CI 6·88-7·60). Carriage prevalence was substantially lower in UKMenCar4 than in the previous surveys: carriage prevalence was 16·6% (95% CI 15·89-17·22; 2306/13 901) in UKMenCar1 (1999), 17·6% (17·05-18·22; 2873/16 295) in UKMenCar2 (2000), and 18·7% (18·12-19·27; 3283/17 569) in UKMenCar3 (2001). Carriage prevalence was lower for all serogroups in UKMenCar4 than in UKMenCar1-3, except for serogroup Y, which was unchanged. The prevalence of carriage-promoting social behaviours decreased from 1999 to 2014-15, with individuals reporting regular cigarette smoking decreasing from 2932 (21·5%) of 13 650 to 2202 (11·2%) of 19 641, kissing in the past week from 6127 (44·8%) of 13 679 to 7320 (37·3%) of 19 641, and attendance at pubs and nightclubs in the past week from 8436 (62·1%) of 13 594 to 7662 (39·0%) of 19 641 (all p<0·0001)., Interpretation: We show that meningococcal carriage prevalence in adolescents sampled nationally during a low incidence period (2014-15) was less than half of that in an equivalent population during a high incidence period (1999-2001). Disease and carriage caused by serogroup C was well controlled by ongoing vaccination. The prevalence of behaviours associated with carriage declined, suggesting that public health policies aimed at influencing behaviour might have further reduced disease., Funding: Wellcome Trust, UK Department of Health, and National Institute for Health Research., (Copyright © 2021 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2021

9. Inclusion of pregnant women in COVID-19 vaccine development.

Author

Heath PT, Le Doare K, and Khalil A

Subjects

COVID-19, COVID-19 Vaccines, Coronavirus Infections immunology, Coronavirus Infections virology, Female, Humans, Pneumonia, Viral virology, Pregnancy, Pregnant People, SARS-CoV-2, Betacoronavirus immunology, Coronavirus Infections prevention & control, Pandemics prevention & control, Pneumonia, Viral prevention & control, Viral Vaccines immunology

Published

2020

10. Randomized clinical trial of DTaP5-HB-IPV-Hib vaccine administered concomitantly with meningococcal serogroup C conjugate vaccines during the primary infant series.

Author

Oliver JL, Sadorge C, Boisnard F, Snape MD, Tomlinson R, Mann R, Rudd P, Bhakthavalsala S, Faust SN, Heath PT, Hughes SM, Borrow R, Thomas S, and Finn A

Subjects

Animals, Antibodies, Bacterial, Diphtheria-Tetanus-Pertussis Vaccine, Humans, Infant, Poliovirus Vaccine, Inactivated, Rabbits, Serogroup, Vaccines, Combined, Vaccines, Conjugate, Haemophilus Vaccines, Haemophilus influenzae type b, Meningococcal Vaccines

Abstract

Background: Concomitant administration of vaccines simplifies delivery. DTaP5-HB-IPV-Hib is a fully liquid, combination vaccine against 6 diseases. This study evaluated the compatibility of DTaP5-HB-IPV-Hib with 2 different meningococcus group C conjugate (MCC) vaccines in infants., Methods: In a phase 3, open-label study, 284 healthy infants from 11 UK centres received DTaP5-HB-IPV-Hib at age 2, 3, and 4 months; 13-valent pneumococcal conjugate vaccine (PCV13) at 2 and 4 months; a Haemophilus influenzae type b (Hib)-MCC vaccine and a measles/mumps/rubella vaccine at 12 months. Participants were randomised 1:1 to receive either an MCC-detoxified tetanus toxin vaccine (MCC-TT; n = 141) or an MCC-Corynebacterium diphtheriae CRM 197 protein vaccine (MCC-CRM; n = 143) at 3 and 4 months. The primary outcome was seroprotection rate (SPR) to MCC (percent with rabbit complement serum bactericidal antibody titer ≥8)., Results: Per protocol analysis, MCC SPRs were 100 and 96.4 one month after the first dose, 100 and 99.1 after the second dose, and 100 and 97.3 after the third (booster) dose of MCC in the MCC-TT and MCC-CRM groups, respectively. One month after all 3 doses of DTaP5-HB-IPV-Hib, immunoglobulin G anti-polyribosylribitol phosphate SPRs (% ≥0.15 µg/mL) were 97.8 in the MCC-TT group and 100 in the MCC-CRM group; anti-hepatitis B antigen SPRs (% ≥10 mIU/mL) were 96.8 and 96.3 in the MCC-TT and MCC-CRM groups, respectively. All participants were seroprotected against diphtheria and tetanus (≥0.01 IU/mL) and poliovirus types 1, 2, and 3 (≥8 dilution), and seroresponse rates to all pertussis antigens were ≥90.4%. Two vaccine-related serious adverse events (transient severe abdominal pain and crying) occurred concomitantly in 1 participant in the MCC-CRM group. Adverse event rates were similar to other studies of DTaP5-HB-IPV-Hib, with pyrexia ≥38 °C in 10.9% of participants following any dose., Conclusions: DTaP5-HB-IPV-Hib can be effectively used in a 2-, 3-, and 4-month infant priming schedule when given with 2 doses of MCC., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020. Published by Elsevier Ltd.)

Published

2020

11. Neonatal seizures: Case definition & guidelines for data collection, analysis, and presentation of immunization safety data.

Author

Pellegrin S, Munoz FM, Padula M, Heath PT, Meller L, Top K, Wilmshurst J, Wiznitzer M, Das MK, Hahn CD, Kucuku M, Oleske J, Vinayan KP, Yozawitz E, Aneja S, Bhat N, Boylan G, Sesay S, Shrestha A, Soul JS, Tagbo B, Joshi J, Soe A, Maltezou HC, Gidudu J, Kochhar S, and Pressler RM

Subjects

Global Health statistics & numerical data, Humans, Immunization statistics & numerical data, Incidence, Infant Health statistics & numerical data, Infant, Newborn, Practice Guidelines as Topic, Seizures diagnosis, Data Collection standards, Immunization adverse effects, Seizures chemically induced

Published

2019

12. The role of immune correlates of protection on the pathway to licensure, policy decision and use of group B Streptococcus vaccines for maternal immunization: considerations from World Health Organization consultations.

Author

Vekemans J, Crofts J, Baker CJ, Goldblatt D, Heath PT, Madhi SA, Le Doare K, Andrews N, Pollard AJ, Saha SK, Schrag SJ, Smith PG, and Kaslow DC

Subjects

Cost-Benefit Analysis, Drug Approval, Female, Humans, Infant, Newborn, Infant, Newborn, Diseases prevention & control, Maternal Health, Pregnancy, Premature Birth prevention & control, Stillbirth, Streptococcal Infections transmission, Streptococcus agalactiae, Pregnancy Complications, Infectious prevention & control, Streptococcal Infections prevention & control, Streptococcal Vaccines immunology, Vaccination legislation & jurisprudence, World Health Organization

Abstract

The development of a group B Streptococcus (GBS) vaccine for maternal immunization constitutes a global public health priority, to prevent GBS-associated early life invasive disease, stillbirth, premature birth, maternal sepsis, adverse neurodevelopmental consequences, and to reduce perinatal antibiotic use. Sample size requirements for the conduct of a randomized placebo-controlled trial to assess vaccine efficacy against the most relevant clinical endpoints, under conditions of appropriate ethical standards of care, constitute a significant obstacle on the pathway to vaccine availability. Alternatively, indirect evidence of protection based on immunologic data from vaccine and sero-epidemiological studies, complemented by data from opsonophagocytic in vitro assays and animal models, could be considered as pivotal data for licensure, with subsequent confirmation of effectiveness against disease outcomes in post-licensure evaluations. Based on discussions initiated by the World Health Organization we present key considerations about the potential role of correlates of protection towards an accelerated pathway for GBS vaccine licensure and wide scale use. Priority activities to support progress to regulatory and policy decision are outlined., (Copyright © 2019 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2019

13. Serocorrelates of protection against infant group B streptococcus disease.

Author

Le Doare K, Kampmann B, Vekemans J, Heath PT, Goldblatt D, Nahm MH, Baker C, Edwards MS, Kwatra G, Andrews N, Madhi SA, Ter Meulen AS, Anderson AS, Corsaro B, Fischer P, and Gorringe A

Subjects

Antibodies, Bacterial immunology, Carrier State blood, Carrier State prevention & control, Female, Humans, Infant, Newborn, Infant, Newborn, Diseases blood, Mothers, Streptococcal Infections blood, Streptococcal Vaccines immunology, Antibodies, Bacterial blood, Infant, Newborn, Diseases prevention & control, Streptococcal Infections prevention & control, Streptococcus agalactiae immunology

Abstract

Group B streptococcus (GBS) is a leading cause of young infant mortality and morbidity globally, with vaccines being developed for over four decades but none licensed to date. A serocorrelate of protection against invasive disease in young infants is being considered to facilitate vaccine early licensure, followed by demonstration of efficacy assessed postlicensure. In this Review, we synthesise the available scientific evidence to define an immune correlate associated with GBS disease risk reduction on the basis of studies of natural infection. We summarise studies that have investigated GBS serum anticapsular or anti-protein antibodies, and studies measuring the association between antibody function and disease risk reduction. We highlight how knowledge on the development of correlates of protection from existing vaccines could be harnessed to facilitate GBS vaccine development. These lessons include aggregation of serocorrelates of protection for individual serotypes, understanding the relationship between immunity derived from natural exposure of adults and vaccine-induced immunity, or using extrapolation of protection from in-vitro immunoassay results. We also highlight key considerations for the assessment of the role of antibodies to derive a serocorrelate of risk reduction in future seroepidemiological studies of GBS disease., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

14. Group B streptococcal disease in UK and Irish infants younger than 90 days, 2014-15: a prospective surveillance study.

Author

O'Sullivan CP, Lamagni T, Patel D, Efstratiou A, Cunney R, Meehan M, Ladhani S, Reynolds AJ, Campbell R, Doherty L, Boyle M, Kapatai G, Chalker V, Lindsay D, Smith A, Davies E, Jones CE, and Heath PT

Subjects

Antibiotic Prophylaxis, Female, Humans, Incidence, Infant, Infant, Newborn, Ireland epidemiology, Male, Microbial Sensitivity Tests, Multilocus Sequence Typing, Pregnancy, Prospective Studies, Risk Factors, Serogroup, Serotyping, Streptococcal Infections microbiology, Streptococcal Infections prevention & control, Streptococcus agalactiae isolation & purification, United Kingdom epidemiology, Streptococcal Infections epidemiology, Streptococcal Infections mortality, Streptococcus agalactiae genetics, Streptococcus agalactiae immunology

Abstract

Background: Group B streptococcus is a leading cause of serious infection in young infants in many countries worldwide. We aimed to define the burden and clinical features of invasive group B streptococcal disease in infants younger than 90 days in the UK and Ireland, together with the characteristics of disease-causing isolates., Methods: Prospective, active national surveillance of invasive group B streptococcal disease in infants younger than 90 days was done from April 1, 2014, to April 30, 2015, through the British Paediatric Surveillance Unit, microbiology reference laboratories, and national public health agencies in the UK and Ireland. Early onset was defined as disease in the first 6 days of life and late onset was defined as 7-89 days of life. Incidence was calculated using livebirths in 2014 (after adjustment for the 13-month surveillance period). Isolates were characterised by serotyping, multilocus sequence typing, and antimicrobial susceptibility testing., Findings: 856 cases of group B streptococcus were identified in 2014-15, an incidence of 0·94 per 1000 livebirths (95% CI 0·88-1·00). Incidence for early-onset disease (n=517) was 0·57 per 1000 livebirths (95% CI 0·52-0·62), and for late-onset disease (n=339) was 0·37 per 1000 livebirths (0·33-0·41). 53 infants died (case fatality rate 6·2%), of whom 27 had early-onset disease (case fatality rate 5·2%) and 26 had late-onset disease (case fatality rate 7·7%). The predominant serotypes were III (241 [60%] of 402 serotyped isolates) and Ia (69 [17%]); five serotypes (Ia, Ib, II, III, V) accounted for 377 (94%) of all serotyped isolates., Interpretation: The incidence of invasive infant group B streptococcal disease in the UK and Ireland has increased since a comparable study done in 2000-01. The burden of early-onset disease has not declined despite the introduction of national prevention guidelines. New strategies for prevention are required., Funding: Meningitis Now., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

15. Cost-effectiveness analysis of maternal immunisation against group B Streptococcus (GBS) disease: A modelling study.

Author

Giorgakoudi K, O'Sullivan C, Heath PT, Ladhani S, Lamagni T, Ramsay M, Al-Janabi H, and Trotter C

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Cost-Benefit Analysis, Female, Humans, Incidence, Infant, Infant, Newborn, Middle Aged, Models, Statistical, Neonatal Sepsis epidemiology, Pregnancy, Streptococcal Infections epidemiology, Streptococcal Vaccines administration & dosage, United Kingdom epidemiology, Young Adult, Neonatal Sepsis economics, Neonatal Sepsis prevention & control, Streptococcal Infections economics, Streptococcal Infections prevention & control, Streptococcal Vaccines economics, Streptococcal Vaccines immunology, Streptococcus agalactiae immunology

Abstract

Background: There is a considerable global burden of invasive group B streptococcal (GBS) disease. Vaccines are being developed for use in pregnant women to offer protection to neonates., Objective: To estimate the potential impact and cost-effectiveness of maternal immunisation against neonatal and maternal invasive GBS disease in the UK., Methods: We developed a decision-tree model encompassing GBS-related events in infants and mothers, following a birth cohort with a time horizon equivalent to average life expectancy (81 years). We parameterised the model using contemporary data from disease surveillance and outcomes in GBS survivors. Costs were taken from NHS sources and research studies. Maternal immunisation in combination with risk-based intrapartum antibiotic prophylaxis (IAP) was compared to the current standard practice of risk-based IAP alone from an NHS and Personal Social Services (health-provider) perspective. We estimated the cases averted and cost per QALY gained through vaccination. One-way sensitivity analysis, scenario analysis and probabilistic sensitivity analysis were performed., Results: An effective maternal immunisation programme could substantially reduce the burden of GBS disease. The deterministic analysis estimated the threshold cost-effective price for a GBS vaccine to be £54 per dose at £20,000/QALY (£71 per dose at £30,000/QALY). Results were most sensitive to assumptions on disease incidence, sequelae rate and vaccine efficacy. Probabilistic analysis showed 90.66% of iterations fell under the £30,000 threshold at a vaccine price of £55. Inclusion of modest prevention of stillbirths and/or, preterm births, carer health impacts, maternal GBS deaths and 1.5% discounting improved cost-effectiveness compared to the base case. Lowering vaccine strain coverage made the vaccine less cost-effective. A key limitation is that the properties of the final GBS vaccine are unknown., Conclusions: Maternal GBS immunisation is expected to be cost-effective, even at a relatively high vaccine price., (Crown Copyright © 2018. Published by Elsevier Ltd. All rights reserved.)

Published

2018

16. Neonatal encephalopathy: Case definition & guidelines for data collection, analysis, and presentation of maternal immunisation safety data.

Author

Sell E, Munoz FM, Soe A, Wiznitzer M, Heath PT, Clarke ED, Spiegel H, Sawlwin D, Šubelj M, Tikhonov I, Mohammad K, and Kochhar S

Subjects

Humans, Infant, Newborn, Adverse Drug Reaction Reporting Systems standards, Brain Diseases epidemiology, Data Collection standards, Epidemiologic Methods, Infant, Newborn, Diseases epidemiology, Vaccination adverse effects

Published

2017

17. Group B streptococcus and respiratory syncytial virus immunisation during pregnancy: a landscape analysis.

Author

Heath PT, Culley FJ, Jones CE, Kampmann B, Le Doare K, Nunes MC, Sadarangani M, Chaudhry Z, Baker CJ, and Openshaw PJM

Subjects

Female, Humans, Immunization statistics & numerical data, Infant, Pregnancy, Respiratory Syncytial Virus Infections immunology, Respiratory Syncytial Virus, Human drug effects, Respiratory Syncytial Virus, Human immunology, Streptococcal Infections microbiology, Streptococcus agalactiae isolation & purification, Vaccination, Immunity, Maternally-Acquired, Immunization methods, Respiratory Syncytial Virus Infections prevention & control, Respiratory Syncytial Virus Vaccines administration & dosage, Streptococcal Infections prevention & control, Streptococcal Vaccines administration & dosage

Abstract

Group B streptococcus and respiratory syncytial virus are leading causes of infant morbidity and mortality worldwide. No licensed vaccines are available for either disease, but vaccines for both are under development. Severe respiratory syncytial virus disease can be prevented by passively administered antibody. The presence of maternal IgG antibody specific to respiratory syncytial virus is associated with reduced prevalence and severity of respiratory syncytial virus disease in the first few weeks of life, whereas maternal serotype-specific anticapsular antibody is associated with protection against both early-onset and late-onset group B streptococcus disease. Therefore, vaccination in pregnancy might protect infants against both diseases. This report describes what is known about immune protection against group B streptococcus and respiratory syncytial virus, identifies knowledge gaps regarding the immunobiology of both diseases, and aims to prioritise research directions in maternal immunisation., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

18. Corrigendum to "Persistence of bactericidal antibodies following booster vaccination with 4CMenB at 12, 18 or 24months and immunogenicity of a fifth dose administered at 4years of age-a phase 3 extension to a randomised controlled trial" [Vaccine 35 (2017) 395-402].

Author

Iro MA, Snape MD, Voysey M, Jawad S, Finn A, Heath PT, Bona G, Esposito S, Diez-Domingo J, Prymula R, Odueyungbo A, Toneatto D, Dull P, and Pollard AJ

Published

2017

19. Association between functional antibody against Group B Streptococcus and maternal and infant colonization in a Gambian cohort.

Author

Le Doare K, Faal A, Jaiteh M, Sarfo F, Taylor S, Warburton F, Humphries H, Birt J, Jarju S, Darboe S, Clarke E, Antonio M, Foster-Nyarko E, Heath PT, Gorringe A, and Kampmann B

Subjects

Adult, Antibodies, Bacterial blood, Carrier State, Child, Child, Preschool, Cohort Studies, Complement C3b immunology, Female, Fetal Blood immunology, Flow Cytometry, Gambia epidemiology, Humans, Immunologic Techniques, Infant, Infant, Newborn, Longitudinal Studies, Mothers, Nasopharynx microbiology, Opsonin Proteins, Pregnancy, Pregnancy Complications, Infectious microbiology, Streptococcal Infections epidemiology, Streptococcal Infections transmission, Streptococcus classification, Streptococcus isolation & purification, Young Adult, Antibodies, Bacterial immunology, Immunity, Maternally-Acquired, Infectious Disease Transmission, Vertical, Streptococcal Infections immunology, Streptococcus growth & development, Streptococcus immunology

Abstract

Background: Vertical transmission of Group B Streptococcus (GBS) is a prerequisite for early-onset disease and a consequence of maternal GBS colonization. Disease protection is associated with maternally-derived anti-GBS antibody. Using a novel antibody-mediated C3b/iC3b deposition flow cytometry assay which correlates with opsonic killing we developed a model to assess the impact of maternally-derived functional anti-GBS antibody on infant GBS colonization from birth to day 60-89 of life., Methods: Rectovaginal swabs and cord blood (birth) and infant nasopharyngeal/rectal swabs (birth, day 6 and day 60-89) were obtained from 750 mother/infant pairs. Antibody-mediated C3b/iC3b deposition with cord and infant sera was measured by flow cytometry., Results: We established that as maternally-derived anti-GBS functional antibody increases, infant colonization decreases at birth and up to three months of life, the critical time window for the development of GBS disease. Further, we observed a serotype (ST)-dependent threshold above which no infant was colonized at birth. Functional antibody above the upper 95th confidence interval for the geometric mean concentration was associated with absence of infant GBS colonization at birth for STII (p<0.001), STIII (p=0.01) and STV (p<0.001). Increased functional antibody was also associated with clearance of GBS between birth and day 60-89., Conclusions: Higher concentrations of maternally-derived antibody-mediated complement deposition are associated with a decreased risk of GBS colonization in infants up to day 60-89 of life. Our findings are of relevance to establish thresholds for protection following vaccination of pregnant women with future GBS vaccines., (Copyright © 2017 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published

2017

20. Persistence of bactericidal antibodies following booster vaccination with 4CMenB at 12, 18 or 24months and immunogenicity of a fifth dose administered at 4years of age-a phase 3 extension to a randomised controlled trial.

Author

Iro MA, Snape MD, Voysey M, Jawad S, Finn A, Heath PT, Bona G, Esposito S, Diez-Domingo J, Prymula R, Odueyungbo A, Toneatto D, Dull P, and Pollard AJ

Subjects

Antigens, Bacterial immunology, Child, Preschool, Complement System Proteins immunology, Czech Republic, Female, Humans, Infant, Italy, Male, Spain, Time Factors, United Kingdom, Antibodies, Bacterial blood, Antibody Formation, Blood Bactericidal Activity, Immunization, Secondary, Meningococcal Vaccines administration & dosage, Meningococcal Vaccines immunology

Abstract

Background: 4CMenB is immunogenic in infants and toddlers. We assessed persistence of human complement serum bactericidal activity (hSBA) following a fourth dose administered at 12, 18 or 24months and characterised the antibody response to a fifth dose administered at 4years of age., Methods: A phase 3, open label, multi-centre extension to a randomised controlled trial conducted in four countries (number of centres): Czech Republic (nineteen), Italy (four), Spain (four) and the United Kingdom (four). Four-year-old children who were either 4CMenB-naïve or had previously received a variety of 3-dose infant priming schedules and a booster vaccine as toddlers (follow-on group) were recruited. Venous blood samples were obtained to determine hSBA against four reference strains; acting as targets to assess immunity to each of the vaccine antigens, NadA (5/99), fHbp (H44/76), PorA (NZ98/254), and NHBA (M10713) at baseline (prior to vaccination, all participants) and one month following a dose of 4CMenB for all vaccine-naïve and follow-on participants primed with the 2, 3, 4 schedule, and a third of follow-on participants primed with a 2, 4, 6month schedule., Results: At baseline (prior to vaccination), the proportion of participants (n=468) with hSBA titers⩾5 was similar across all followon groups: 89-100% against 5/99; 12-35% for H44/76; 8-12% for NZ98/254 and 53-80% for M10713 compared with 5%, 0%, 0%; and 60% respectively, for the vaccine-naïve controls (n=206). Following a dose of 4CMenB at 4years of age, this increased to 100% (5/99), 97-100% (H44/76), 80-95 % (NZ98/254) and 84-100% (M10713) (n=210), compared with 89%, 70%, 24%, and 76% respectively for vaccine-naïve controls (n=192)., Conclusion: Waning of protective antibodies occurred 24–36 months after toddler booster regardless of age at boost. This was least marked against target strains 5/99 and M10713. A robust memory response occurred after a booster dose given at 4 years of age., (Copyright © 2016 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published

2017

21. Use of a booster dose of capsular group C meningococcal glycoconjugate vaccine to demonstrate immunologic memory in children primed with one or two vaccine doses in infancy.

Author

Pace D, Khatami A, Attard-Montalto S, Voysey M, Finn A, Faust SN, Heath PT, Borrow R, Snape MD, and Pollard AJ

Subjects

Blood Bactericidal Activity, Female, Humans, Immunoglobulin G blood, Infant, Male, Vaccines, Conjugate administration & dosage, Vaccines, Conjugate immunology, Antibodies, Bacterial blood, Haemophilus Vaccines administration & dosage, Haemophilus Vaccines immunology, Immunization, Secondary methods, Immunologic Memory, Neisseria meningitidis, Serogroup C immunology, Tetanus Toxoid administration & dosage, Tetanus Toxoid immunology

Abstract

Background: Use of a polysaccharide vaccine challenge to demonstrate immunologic memory after priming with capsular group C meningococcal conjugate vaccines (MenCC) risks induction of immunologic hyporesponsiveness. For this reason, MenCC vaccines are now used as probes of immunologic memory, however, no studies have demonstrated their ability to distinguish primed from unprimed children., Methods: This study was part of a randomised controlled trial investigating the immunogenicity of a booster dose of the combined Haemophilus influenzae type b and MenC-tetanus toxoid vaccine (Hib-MenC-TT) in infants receiving reduced dose MenCC vaccine priming schedules (one MenC-CRM/MenC-TT or two MenC-CRM vaccine doses) compared with an unprimed group. Antibody kinetics were studied in a subset of 269 children by measuring changes in the MenC serum bactericidal antibody, using rabbit complement, (MenC rSBA) titres and MenC specific IgG memory B-cells before and at 6 and 28days following the 12month booster vaccination., Results: At 6days after the 12monthMenCC vaccine, the rise in MenC rSBA titres and MenC specific IgG memory B-cells of the primed groups were significantly higher than the infant MenCC naïve group. Participants primed with one MenC-TT dose had the highest increase in MenC rSBA titres compared with all other groups. The MenC rSBA titres at the 28th compared with the 6th day after boosting was significantly higher in those primed with a single MenC-TT/MenC-CRM vaccine in infancy compared with those who were not primed or who were primed with two doses of the MenC-CRM vaccine., Conclusion: Immunologic memory can be demonstrated by a MenCC booster vaccination but is affected by the type and number of MenCC doses used for infant priming. The MenC rSBA responses can be used to demonstrate successful immunologic priming., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

22. Guideline for collection, analysis and presentation of safety data in clinical trials of vaccines in pregnant women.

Author

Jones CE, Munoz FM, Spiegel HM, Heininger U, Zuber PL, Edwards KM, Lambach P, Neels P, Kohl KS, Gidudu J, Hirschfeld S, Oleske JM, Khuri-Bulos N, Bauwens J, Eckert LO, Kochhar S, Bonhoeffer J, and Heath PT

Subjects

Female, Humans, Infant, Pregnancy Complications, Infectious prevention & control, Statistics as Topic, Vaccines administration & dosage, Clinical Trials as Topic, Pregnancy, Vaccination adverse effects, Vaccines adverse effects

Abstract

Vaccination during pregnancy is increasingly being used as an effective approach for protecting both young infants and their mothers from serious infections. Drawing conclusions from published studies in this area can be difficult because of the inability to compare vaccine trial results across different studies and settings due to the heterogeneity in the definitions of terms used to assess the safety of vaccines in pregnancy and the data collected in such studies. The guidelines proposed in this document have been developed to harmonize safety data collection in all phases of clinical trials of vaccines in pregnant women and apply to data from the mother, fetus and infant. Guidelines on the prioritization of the data to be collected is also provided to allow applicability in various geographic, cultural and resource settings, including high, middle and low-income countries., (Copyright © 2016. Published by Elsevier Ltd.)

Published

2016

23. Neonatal infections: Case definition and guidelines for data collection, analysis, and presentation of immunisation safety data.

Author

Vergnano S, Buttery J, Cailes B, Chandrasekaran R, Chiappini E, Clark E, Cutland C, de Andrade SD, Esteves-Jaramillo A, Guinazu JR, Jones C, Kampmann B, King J, Kochhar S, Macdonald N, Mangili A, de Menezes Martins R, Velasco Muñoz C, Padula M, Muñoz FM, Oleske J, Sanicas M, Schlaudecker E, Spiegel H, Subelj M, Sukumaran L, Tagbo BN, Top KA, Tran D, and Heath PT

Subjects

Bacteremia epidemiology, Bacteremia prevention & control, Data Collection, Female, Humans, Infant, Newborn, Meningitis epidemiology, Meningitis prevention & control, Sepsis epidemiology, Sepsis prevention & control, Statistics as Topic, Communicable Disease Control, Immunization adverse effects, Infections epidemiology, Vaccines adverse effects

Abstract

Maternal vaccination is an important area of research and requires appropriate and internationally comparable definitions and safety standards. The GAIA group, part of the Brighton Collaboration was created with the mandate of proposing standardised definitions applicable to maternal vaccine research. This study proposes international definitions for neonatal infections. The neonatal infections GAIA working group performed a literature review using Medline, EMBASE and the Cochrane collaboration and collected definitions in use in neonatal and public health networks. The common criteria derived from the extensive search formed the basis for a consensus process that resulted in three separate definitions for neonatal blood stream infections (BSI), meningitis and lower respiratory tract infections (LRTI). For each definition three levels of evidence are proposed to ensure the applicability of the definitions to different settings. Recommendations about data collection, analysis and presentation are presented and harmonized with the Brighton Collaboration and GAIA format and other existing international standards for study reporting., (Copyright © 2016. Published by Elsevier Ltd.)

Published

2016

24. Global alignment of immunization safety assessment in pregnancy - The GAIA project.

Author

Bonhoeffer J, Kochhar S, Hirschfeld S, Heath PT, Jones CE, Bauwens J, Honrado Á, Heininger U, Muñoz FM, Eckert L, Steinhoff M, Black S, Padula M, Sturkenboom M, Buttery J, Pless R, and Zuber P

Subjects

Clinical Trials as Topic, Female, Humans, Vaccines administration & dosage, World Health Organization, Global Health, Immunization adverse effects, Pregnancy, Vaccines adverse effects

Abstract

Immunization in pregnancy provides a promising contribution to globally reducing neonatal and under-five childhood mortality and morbidity. Thorough assessment of benefits and risks for the primarily healthy pregnant women and their unborn babies is required. The GAIA project was formed in response to the call of the World Health Organization for a globally concerted approach to actively monitor the safety of vaccines and immunization in pregnancy programs. GAIA aims to improve the quality of outcome data from clinical vaccine trials in pregnant women with a specific focus on the needs and requirements for safety monitoring in LMIC. In the first year of the project, a large and functional network of experts was created. The first outputs include a guidance document for clinical trials of immunization in pregnancy, a basic data collection guide, ten case definitions of key obstetric and neonatal health outcomes, an ontology of key terms and a map of pertinent disease codes. The GAIA Network is designed as an open and growing forum for professionals sharing the GAIA vision and aim. Based on the initial achievements, tools and services are developed to support investigators and strengthen immunization in pregnancy programs with specific focus on LMIC., (Copyright © 2016. Published by Elsevier Ltd.)

Published

2016

25. Guidance for the collection of case report form variables to assess safety in clinical trials of vaccines in pregnancy.

Author

Jones CE, Munoz FM, Kochhar S, Vergnano S, Cutland CL, Steinhoff M, Black S, Heininger U, Bonhoeffer J, and Heath PT

Subjects

Clinical Trials as Topic, Drug-Related Side Effects and Adverse Reactions, Female, Global Health, Humans, Infant, Poverty, Pregnancy Complications, Infectious prevention & control, Records, Statistics as Topic, Data Collection, Pregnancy, Vaccination adverse effects, Vaccines adverse effects

Abstract

Vaccination in pregnancy is an effective strategy to prevent serious infections in mothers and their infants. Safety of this strategy is of principal importance to all stakeholders. As the number of studies assessing safety of vaccines in pregnancy increases, the need to ensure consistent collection and reporting of critical data to allow comparisons and data pooling becomes more important. The Global Alignment of Immunization Safety Assessment in Pregnancy (GAIA) project aims to improve data collection and create a shared understanding of maternal, fetal and neonatal outcomes in order to progress the global agenda for vaccination in pregnancy. The guidance in this document has been developed to harmonize the data collected in case report forms used for safety monitoring in clinical trials of vaccination in pregnant women. Data to be collected is prioritized to allow applicability in diverse research settings, including low and middle-income countries. Standardized data will enable the research community to have a common base upon which to conduct meta-analyses, strengthening the applicability of outcomes to different settings., (Copyright © 2016 The Author(s). Published by Elsevier Ltd.. All rights reserved.)

Published

2016

26. Strengthening the Reporting of Observational Studies in Epidemiology for Newborn Infection (STROBE-NI): an extension of the STROBE statement for neonatal infection research.

Author

Fitchett EJA, Seale AC, Vergnano S, Sharland M, Heath PT, Saha SK, Agarwal R, Ayede AI, Bhutta ZA, Black R, Bojang K, Campbell H, Cousens S, Darmstadt GL, Madhi SA, Meulen AS, Modi N, Patterson J, Qazi S, Schrag SJ, Stoll BJ, Wall SN, Wammanda RD, and Lawn JE

Subjects

Checklist, Global Health, Humans, Infant, Infant Mortality, Infant, Newborn, Observation methods, Epidemiologic Research Design, Epidemiologic Studies, Guidelines as Topic standards, Infant, Newborn, Diseases

Abstract

Neonatal infections are estimated to account for a quarter of the 2·8 million annual neonatal deaths, as well as approximately 3% of all disability-adjusted life-years. Despite this burden, few data are available on incidence, aetiology, and outcomes, particularly regarding impairment. We aimed to develop guidelines for improved scientific reporting of observational neonatal infection studies, to increase comparability and to strengthen research in this area. This checklist, Strengthening the Reporting of Observational Studies in Epidemiology for Newborn Infection (STROBE- NI), is an extension of the STROBE (Strengthening the Reporting of Observational Studies in Epidemiology) statement. STROBE-NI was developed following systematic reviews of published literature (1996-2015), compilation of more than 130 potential reporting recommendations, and circulation of a survey to relevant professionals worldwide, eliciting responses from 147 professionals from 37 countries. An international consensus meeting of 18 participants (with expertise in infectious diseases, neonatology, microbiology, epidemiology, and statistics) identified priority recommendations for reporting, additional to the STROBE statement. Implementation of these STROBE-NI recommendations, and linked checklist, aims to improve scientific reporting of neonatal infection studies, increasing data utility and allowing meta-analyses and pathogen-specific burden estimates to inform global policy and new interventions, including maternal vaccines., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

27. Status of vaccine research and development of vaccines for GBS.

Author

Heath PT

Subjects

Biomedical Research trends, Clinical Trials as Topic, Female, Humans, Infant, Newborn, Meningitis prevention & control, Neonatal Sepsis prevention & control, Pregnancy, Streptococcal Infections epidemiology, Vaccines, Conjugate therapeutic use, Streptococcal Infections prevention & control, Streptococcal Vaccines therapeutic use, Streptococcus agalactiae

Abstract

Streptococcus agalactiae (group B streptococcus (GBS)) is the leading cause of neonatal sepsis and meningitis in many countries. Intrapartum antibiotic strategies have reduced the incidence of early-onset neonatal GBS in a number of countries but have had no impact on late onset GBS infection (LOD). In low/middle income settings, the disease burden remains uncertain although in several countries of Southern Africa appears comparable to or higher than that of high-income countries. As disease may be rapidly fulminating cases can be missed before appropriate samples are obtained and this may lead to underestimation of the true burden. Given the rapid onset and progression within hours of birth as well as the deficiencies in IAP strategies and absence of a solution for preventing LOD, it is clear that administration of a suitable vaccine in pregnancy could provide a better solution in all settings; it should also be cost effective. The current leading vaccine candidates are CPS-protein conjugate vaccines but protein-based vaccines are also in development and one has recently commenced clinical trials., (Copyright © 2016 World Health Organization. Published by Elsevier Ltd.. All rights reserved.)

Published

2016

28. Factors affecting the causality assessment of adverse events following immunisation in paediatric clinical trials: An online survey.

Author

Voysey M, Tavana R, Farooq Y, Heath PT, Bonhoeffer J, and Snape MD

Subjects

Causality, Humans, Surveys and Questionnaires, Adverse Drug Reaction Reporting Systems standards, Clinical Trials as Topic, Drug-Related Side Effects and Adverse Reactions epidemiology, Drug-Related Side Effects and Adverse Reactions etiology, Epidemiologic Methods, Immunization adverse effects

Abstract

Background: Serious adverse events (SAEs) in clinical trials require reporting within 24h, including a judgment of whether the SAE was related to the investigational product(s). Such assessments are an important component of pharmacovigilance, however classification systems for assigning relatedness vary across study protocols. This on-line survey evaluated the consistency of SAE causality assessment among professionals with vaccine clinical trial experience., Methods: Members of the clinical advisory forum of experts (CAFÉ), a Brighton Collaboration online-forum, were emailed a survey containing SAEs from hypothetical vaccine trials which they were asked to classify. Participants were randomised to either two classification options (related/not related to study immunisation) or three options (possibly/probably/unrelated). The clinical scenarios, were (i) leukaemia diagnosed 5 months post-immunisation with a live RSV vaccine, (ii) juvenile idiopathic arthritis (JIA) 3 months post-immunisation with a group A streptococcal vaccine, (iii) developmental delay diagnosed at age 10 months after infant capsular group B meningococcal vaccine, (iv) developmental delay diagnosed at age 10 months after maternal immunisation with a group B streptococcal vaccine., Results: There were 140 respondents (72 two options, 68 three options). Across all respondents, SAEs were considered related to study immunisation by 28% (leukaemia), 74% (JIA), 29% (developmental delay after infant immunisation) and 42% (developmental delay after maternal immunisation). Having only two options made respondents significantly less likely to classify the SAE as immunisation-related for two scenarios (JIA p=0.0075; and maternal immunisation p=0.045). Amongst study investigators (n=43) this phenomenon was observed for three of the four scenarios: (JIA p=0.0236; developmental delay following infant immunisation p=0.0266; and developmental delay after maternal immunisation p=0.0495)., Conclusions: SAE causality assessment is inconsistent amongst study investigators and can be influenced by the classification systems available to them. There is a pressing need for SAE classification systems to be standardised across study protocols., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

29. Immunological effect of administration of sequential doses of Haemophilus influenzae type b and pneumococcal conjugate vaccines in the same versus alternating limbs in the routine infant immunisation schedule: an open-label randomised controlled trial.

Author

Iro MA, Khatami A, Marshall AS, Pace D, Voysey M, McKenna J, Campbell D, Attard-Montalto S, Finn A, White C, Faust SN, Kent A, Heath PT, MacLeod E, Stanford E, Findlow H, Almond R, Bai X, Borrow R, Snape MD, and Pollard AJ

Subjects

Extremities, Female, Healthy Volunteers, Humans, Immunization Schedule, Immunoglobulin G blood, Infant, Male, Malta, Tetanus Toxoid administration & dosage, Tetanus Toxoid immunology, Treatment Outcome, United Kingdom, Vaccines, Conjugate administration & dosage, Vaccines, Conjugate immunology, Antibodies, Bacterial blood, Diphtheria-Tetanus-Pertussis Vaccine administration & dosage, Diphtheria-Tetanus-Pertussis Vaccine immunology, Haemophilus Vaccines administration & dosage, Haemophilus Vaccines immunology, Haemophilus influenzae type b immunology, Neisseria meningitidis immunology, Pneumococcal Vaccines administration & dosage, Pneumococcal Vaccines immunology, Poliovirus Vaccine, Inactivated administration & dosage, Poliovirus Vaccine, Inactivated immunology

Abstract

Background: The use of different limbs for the administration of sequential doses of an intradermal rabies vaccine was shown to result in reduced vaccine immunogenicity. We aimed to assess whether this phenomenon also occurs with routine infant vaccines., Methods: In this open-label, randomised, controlled study, eligible healthy infants 6-12 weeks of age recruited through five clinical trials units (four in the UK and one in Malta) were randomly assigned in a 1:1 ratio to two vaccination groups: consistent limb or alternating limb. Infants in the consistent limb group received the diphtheria-tetanus-acellular pertussis-inactived polio-Haemophilus influenzae type b combined vaccine (DTaP-IPV-Hib) at 2, 3, and 4 months of age, and the pneumococcal conjugate vaccine (PCV13) at 2, 4, and 12 months, all administered to the right leg. Infants in the alternating limb group received DTaP-IPV-Hib in the left leg at 2 months and in the right leg at 3 and 4 months; and PCV13 in the left leg at 2 months, in the right leg at 4 months, and in the left arm at 12 months. All infants in both groups received the combined H influenzae type b and capsular group C Neisseria meningitidis tetanus toxoid conjugate vaccine (Hib-MenC-TT), administered in the left leg at 12 months. Randomisation was achieved by randomly generated codes, with permuted block size of 30, and was stratified by study site. Group allocation was not masked from study staff and parents of participants after enrolment, but group allocation was masked from laboratory staff assessing blood samples. The current study was a prespecified secondary objective of a parent phase 4 trial that assessed the induction of immunity following varying schedules of vaccination with glyco-conjugate capsular group C Neisseria meningitidis (Men C) vaccines in infancy. The objective of the current study was to compare the immunogenicity and reactogenicity of vaccines delivered in either consistent or alternating limbs. Immunogenicity was assessed by comparing serum IgG geometric mean concentrations at 5, 12, 13, and 24 months, analysed per protocol. This study is registered with ClinicalTrials.gov, number NCT01129518., Findings: Between July 5, 2010, and Aug 1, 2013, we enrolled 509 infants and randomly allocated them to the consistent limb group (n=254) or the alternating limb group (n=255). Anti-H influenzae type b anti-polyribosylribitol phosphate IgG geometric mean concentrations were lower in the consistent limb group than in the alternating limb group at 5 months (consistent limb 0·41 μg/mL [95% CI 0·31-0·54] vs alternating limb 0·61 μg/mL [0·45-0·82]; p=0·0268) and at 12 months (0·35 μg/mL [0·28-0·43] vs 0·50 μg/mL [0·40-0·62]; p=0·0136). Anti-tetanus toxoid antibody IgG geometric mean concentrations were lower in the consistent limb group (1·63 IU/mL [95% CI 1·40-1·90]) than in the alternating limb group (2·30 IU/mL [1·97-2·68]) at 13 months (p=0·0008) and at 24 months (0·44 IU/mL [0·37-0·52] vs 0·61 IU/mL [0·51-0·73]; p=0·0074). Anti-pneumococcal IgG geometric mean concentrations were similar between both groups at all timepoints. The proportions of participants who had adverse events did not differ between the two groups., Interpretation: Use of different (alternating) limbs for sequential doses of routine infant vaccines does not reduce, and might enhance, immunogenicity. The underlying mechanism for this finding warrants further research., Funding: NIHR Oxford Biomedical Research Centre and GlaxoSmithKline Biologicals., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

30. Anti-group B Streptococcus antibody in infants born to mothers with human immunodeficiency virus (HIV) infection.

Author

Le Doare K, Allen L, Kampmann B, Heath PT, Taylor S, Hesseling AC, Gorringe A, and Jones CE

Subjects

Cohort Studies, Complement System Proteins immunology, Female, Flow Cytometry, Humans, Infant, Infant, Newborn, Male, Pregnancy, South Africa, Antibodies, Bacterial blood, HIV Infections immunology, Immunity, Maternally-Acquired, Pregnancy Complications, Infectious immunology, Streptococcus agalactiae immunology

Abstract

Background: HIV-exposed uninfected infants have increased infection risk and mortality compared to HIV-unexposed infants. HIV-exposed infants may be at increased risk of invasive GBS disease due to reduced maternal antibody against GBS., Methods: We quantified antibodies that bind to the surface of whole Group B Streptococcus (GBS) of serotypes Ia, Ib, II, III and V using novel flow cytometry assays in South African HIV-infected and non-infected mothers and their uninfected infants. Antibody-mediated complement C3b/iC3b deposition onto GBS of these serotypes was also quantified by a novel flow cytometry assay., Results: Geometric mean concentration (GMC) of both surface-binding anti-GBS antibody and antibody-mediated complement deposition onto GBS were reduced in HIV-infected women (n=46) compared to HIV-uninfected women (n=58) for ST1a (surface-binding: 19.3 vs 29.3; p=0.003; complement deposition: 2.9 vs 5.3 SU/mL; p=0.003), STIb (24.9 vs 47.6; p=0.003; 2.6 vs 4.9 SU/mL; p=0.003), STII (19.8 vs 50.0; p=0.001; 3.1 vs 6.2 SU/mL; p=0.001), STIII (27.8 vs 60.1; p=0.001; 2.8 vs 5.3 SU/mL; p=0.001) and STV (121.9 vs 185.6 SU/mL; p<0.001) and in their infants for STIa (complement deposition 9.4 vs 27.0 SU/mL; p=0.02), STIb (13.4 vs 24.5 SU/mL; p=0.02), STII (14.6 vs 42.7 SU/mL; p=0.03), STIII (26.6 vs 62.7 SU/mL; p=0.03) and STV (90.4 vs 165.8 SU/mL; p=0.04). Median transplacental transfer of antibody from HIV-infected women to their infants was reduced compared to HIV-uninfected women for GBS serotypes II (0.42 [IQR 0.22-0.59] vs 1.0 SU/mL [0.42-1.66]; p<0.001), III (0.54 [0.31-1.03] vs 0.95 SU/mL [0.42-3.05], p=0.05) and V (0.51 [0.28-0.79] vs 0.75 SU/mL [0.26-2.9], p=0.04). The differences between infants remained significant at 16 weeks of age., Conclusions: Maternal HIV infection was associated with lower anti-GBS surface binding antibody concentration and antibody-mediated C3b/iC3b deposition onto GBS bacteria of serotypes Ia, Ib, II, III and V. This may render these infants more susceptible to early and late onset GBS disease., (Crown Copyright © 2014. Published by Elsevier Ltd. All rights reserved.)

Published

2015

31. Trends in bacterial, mycobacterial, and fungal meningitis in England and Wales 2004-11: an observational study.

Author

Okike IO, Ribeiro S, Ramsay ME, Heath PT, Sharland M, and Ladhani SN

Subjects

Adolescent, Adult, Age Distribution, Aged, Child, Child, Preschool, England epidemiology, Escherichia coli, Escherichia coli Infections epidemiology, Escherichia coli Infections microbiology, Female, Humans, Incidence, Infant, Male, Meningitis, Meningococcal epidemiology, Middle Aged, Mycobacterium Infections epidemiology, Mycobacterium Infections microbiology, Pneumococcal Infections epidemiology, Pneumococcal Infections microbiology, Staphylococcal Infections epidemiology, Staphylococcal Infections microbiology, Staphylococcus aureus, Streptococcal Infections epidemiology, Streptococcal Infections microbiology, Streptococcus agalactiae, Streptococcus pneumoniae, Wales epidemiology, Young Adult, Meningitis, Bacterial epidemiology, Meningitis, Bacterial microbiology, Meningitis, Fungal epidemiology, Meningitis, Fungal microbiology

Abstract

Background: Meningitis remains one of the most feared infectious diseases worldwide, yet there are few population-based studies on the epidemiology, causes, or trends over time in meningitis, especially in industrialised countries. Our aim was to do such a study using routinely reported data available in England and Wales., Methods: In England and Wales, UK National Health Service hospitals routinely report laboratory-confirmed pathogens electronically to Public Health England. Records of all positive bacterial, mycobacterial, and fungal results from cerebrospinal fluid or from blood cultures in patients with clinical meningitis were extracted for analysis. The percentage change in annual incidence was estimated using linear regression analysis of the log of the annual incidence., Findings: During 2004-11, 7061 cases of meningitis were reported (mean annual incidence 1·62 per 100,000 people, 95% CI 1·58-1·66), including 2594 cases in children (37%). The incidence of bacterial (1·44 per 100,000 people, 1·41-1·48), fungal (0·09, 0·08-0·10), and mycobacterial (0·09, 0·08-0·09) meningitis remained stable overall and across the age groups, apart from significant year-on-year increases in children younger than 3 months (978 cases; incidence 72·2 per 100,000 people; annual increase 7·4%, 5·1-9·8; p<0·0001) driven mainly by group B streptococci (GBS), and in adults aged 65 years or older (752 cases; incidence 1·2 per 100,000 people; annual increase 3·0%, 1·4-4·8; p<0·0001) primarily because of Escherichia coli. By contrast, meningococcal meningitis rates declined steadily, but remained the most common cause of meningitis in children. Overall, five groups of bacteria accounted for 60% (3790/6286) of bacterial meningitis cases: Neisseria meningitidis (1350 cases, 22%), Streptococcus pneumoniae (1143, 18%), Staphylococcus aureus (652, 10%), GBS (326, 5%), and E coli (319, 5%)., Interpretation: In England and Wales, laboratory-based surveillance shows a remarkably stable incidence of bacterial, fungal, and mycobacterial meningitis in recent years, although there were differences in individual trends among the main pathogens causing meningitis in different age groups., Funding: None., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014

32. Considerations for a phase-III trial to evaluate a group B Streptococcus polysaccharide-protein conjugate vaccine in pregnant women for the prevention of early- and late-onset invasive disease in young-infants.

Author

Madhi SA, Dangor Z, Heath PT, Schrag S, Izu A, Sobanjo-Ter Meulen A, and Dull PM

Subjects

Female, Humans, Infant, Newborn, Infant, Newborn, Diseases microbiology, Infant, Newborn, Diseases mortality, Pregnancy, Pregnancy Complications, Infectious prevention & control, Streptococcal Infections microbiology, Streptococcal Infections mortality, Streptococcus agalactiae classification, Vaccination, Vaccines, Conjugate therapeutic use, Clinical Trials, Phase III as Topic methods, Infant, Newborn, Diseases prevention & control, Infectious Disease Transmission, Vertical prevention & control, Streptococcal Infections prevention & control, Streptococcal Vaccines therapeutic use

Abstract

In 2010, an estimated 393,000 infection-related neonatal deaths occurred worldwide with Group B streptococcus (GBS) being a leading cause. Prevention of early-onset disease (0-6 days; EOD) is currently focused on intra-partum antibiotic prophylaxis to mothers identified as being at risk; such strategies reduce EOD by 75-80% but are resource-intensive and logistically-difficult to implement in developing countries. Vaccination of pregnant women is an alternate strategy for preventing both EOD and late-onset disease (7-89 days; LOD). A trivalent GBS polysaccharide-protein conjugate vaccine (GBS-CV) composed of capsular epitopes from serotypes Ia, Ib and III is undergoing phase-II evaluation among pregnant women in Europe, North America and Africa. These serotypes cause 70-80% of all invasive GBS disease in early-infancy. Maternal anti-GBS antibodies are associated with protection from EOD, however, since a correlate of efficacy has not been defined, a phase III efficacy trial may be required for licensure. Criteria for selecting appropriate sites include sufficiently high GBS incidence in large birth cohorts, as well as adequate clinical and microbiological diagnostic skills and capacities. Alternate pathways to licensure should be explored, e.g. identification of serological correlates of protection with subsequent phase IV studies establishing vaccine-effectiveness against invasive GBS disease. Conducting a randomized, placebo-controlled efficacy trial, however, has the additional advantage of also being able to evaluate the role of GBS contributing to neonatal culture-negative sepsis, stillbirths, prematurity and low-birth weight., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

33. An overview of global GBS epidemiology.

Author

Le Doare K and Heath PT

Subjects

Female, Humans, Infant, Newborn, Meningitis microbiology, Pregnancy, Risk Factors, Sepsis microbiology, Antibiotic Prophylaxis, Infant, Newborn, Diseases microbiology, Streptococcal Infections drug therapy, Streptococcal Infections epidemiology, Streptococcal Infections prevention & control, Streptococcus agalactiae classification, Streptococcus agalactiae drug effects, Streptococcus agalactiae immunology

Abstract

Streptococcus agalactiae (group B streptococcus (GBS)), remains the leading cause of neonatal sepsis and meningitis in many countries and an important cause of disease in pregnant women, immunocompromised adults and the elderly. Intrapartum antibiotic strategies have reduced the incidence of early-onset neonatal GBS where applied, but have had no impact on late onset GBS infection and only a limited impact on disease in pregnant women. In low/middle income settings, the disease burden remains uncertain although in several countries of Southern Africa appears comparable to that of high-income countries. Disease may be rapidly fulminating and cases therefore missed before appropriate samples are obtained. This may lead to significant underestimation of the true burden and be a particular issue in many African and Asian countries; comprehensive epidemiological data from such countries are urgently required. The available data suggest that the serotype distribution of GBS isolates is similar in Africa, Western Pacific, Europe, the Americas and the Eastern Mediterranean regions and has not changed over the past 30 years. Five serotypes (Ia, Ib, II, III, V) account for the majority of disease; conjugate vaccines including some or all of these serotypes therefore hold great promise for preventing this important disease., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

34. Immunoglobulin deficiency in children with Hib vaccine failure.

Author

Ladhani S, Oeser C, Sheldon J, Ramsay M, Booy R, and Heath PT

Subjects

Adolescent, Anti-Bacterial Agents therapeutic use, Bacterial Capsules administration & dosage, Child, Child, Preschool, Dysgammaglobulinemia immunology, Dysgammaglobulinemia microbiology, Female, Follow-Up Studies, Haemophilus Infections drug therapy, Haemophilus Infections epidemiology, Haemophilus Vaccines administration & dosage, Humans, Infant, Logistic Models, Male, Population Surveillance, Prevalence, United Kingdom epidemiology, Antibodies, Bacterial blood, Bacterial Capsules immunology, Dysgammaglobulinemia epidemiology, Haemophilus Infections prevention & control, Haemophilus Vaccines immunology

Abstract

Immunoglobulin deficiency has been reported in 21% of UK children with Hib vaccine failure but its clinical significance and long-term consequences are not known. This study aimed to estimate the prevalence of immunoglobulin deficiency in children with Hib vaccine failure several years after infection and to determine their risk of recurrent infections. The families of children who developed invasive Hib disease after prior immunisation were identified through national surveillance. A completed questionnaire and blood sample was provided by 170 children at a median of 4 years after infection, equivalent to 1035 child-years of follow-up. Nineteen (11.2%) children had immunoglobulin deficiency, including IgA (n=12), IgM (n=5) and all three immunoglobulin classes (n=2). Immunoglobulin deficiency was associated with younger age (<2 years) at initial Hib disease (12/19 [63.2%] vs. 60/151 [39.7%], P=0.05) and parental reporting of their child receiving >2 antibiotic courses annually in early childhood (11/19 [57.9%] vs. 39/151 [25.8%], P=0.004].). In a logistic regression model, Hib vaccine failure cases that had received multiple antibiotic courses in early childhood were 3.8 times (95% CI, 1.4-10.6; P=0.01) more likely to be immunoglobulin deficient at follow-up than those with fewer or no antibiotic courses. Thus, the prevalence of immunoglobulin deficiency in children with Hib vaccine failure at a median of four years after infection is half that reported at the time of the original infection. A proportion of children with Hib vaccine failure, especially where it occurs at a young age, appear to have a maturational delay in development of normal immunoglobulin concentrations., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

35. Predictors of immune response and reactogenicity to AS03B-adjuvanted split virion and non-adjuvanted whole virion H1N1 (2009) pandemic influenza vaccines.

Author

Andrews NJ, Walker WT, Finn A, Heath PT, Collinson AC, Pollard AJ, Snape MD, Faust SN, Waight PA, Hoschler K, Sheasby L, Waddington C, Kerridge S, Chalk J, Reiner A, John T, Fletcher M, Allen R, Fineman N, Wilkins S, Casey M, Michaelis L, Oeser C, Okike I, Ladhani S, and Miller E

Subjects

Adjuvants, Immunologic adverse effects, Antibodies, Viral blood, Child, Child, Preschool, Drug Combinations, Female, Hemagglutination Inhibition Tests, Humans, Infant, Influenza Vaccines administration & dosage, Influenza, Human immunology, Male, Polysorbates adverse effects, Squalene adverse effects, Vaccines, Inactivated administration & dosage, Vaccines, Inactivated adverse effects, Vaccines, Inactivated immunology, Vaccines, Subunit administration & dosage, Vaccines, Subunit adverse effects, Vaccines, Subunit immunology, alpha-Tocopherol adverse effects, Adjuvants, Immunologic administration & dosage, Influenza A Virus, H1N1 Subtype immunology, Influenza Vaccines adverse effects, Influenza Vaccines immunology, Influenza, Human prevention & control, Polysorbates administration & dosage, Squalene administration & dosage, alpha-Tocopherol administration & dosage

Abstract

In 2009, 943 children aged 6 months to 10 years were randomised to receive two doses of an oil-in water AS03B-adjuvanted split virion or a non-adjuvanted whole virion H1N1 (2009) vaccine. The large numbers allowed investigation of possible predictors of immune response and reactogenicity. We used regression analysis to examine the effect of variables including past receipt of seasonal vaccine, antipyretics post-vaccination, interval between doses and pre-existing antibodies to H1N1 (2009) on immunogenicity. We also examined the relationship between immunogenicity and reactogenicity and whether prior infection or underlying conditions affected reactogenicity. For both vaccines, haemagglutination-inhibition titres were 60% higher in children with fever ≥38 °C after vaccination and 29% lower in those previously given seasonal vaccine. Early use of antipyretics did not affect immunogenicity. Post-vaccination titres were higher with longer intervals between doses and in those with evidence of prior infection, but reactogenicity in the latter was unaffected. In the adjuvanted vaccine group, reactions were more common in children with atopy. Both vaccines were safe and immunogenic in those with prior infection. Reduction in the interval between doses for earlier protection would be at the cost of reduced immunogenicity. The effect of seasonal vaccine on immunogenicity merits further investigation., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

36. The immunogenicity of a novel A (H1N1) vaccine in HIV-infected children.

Author

Okike IO, Yung C, Ladhani S, Oeser C, Bennett A, Doerholt K, Storey S, Donaghy S, Butter N, Hoschler K, Sheasby L, Heath PT, and Miller E

Subjects

Adjuvants, Immunologic, Adolescent, Antibodies, Viral blood, CD4 Lymphocyte Count, Child, Child, Preschool, Drug Combinations, Female, HIV-1 isolation & purification, Hemagglutination Inhibition Tests, Humans, Immunization, Secondary methods, Influenza Vaccines administration & dosage, Influenza Vaccines adverse effects, Male, Polysorbates administration & dosage, Polysorbates adverse effects, Squalene administration & dosage, Squalene adverse effects, United Kingdom, Vaccination methods, Viral Load, alpha-Tocopherol administration & dosage, alpha-Tocopherol adverse effects, HIV Infections immunology, Influenza Vaccines immunology

Abstract

Background: In October 2009, the United Kingdom Department of Health recommended vaccination of high-risk groups, including children with HIV, with a novel, oil-in-water AS03(B) adjuvanted Influenza A (H1N1) vaccine (Pandemrix). There were no published data available regarding the immunogenicity of this vaccine in such children., Objectives: This study evaluated the immunogenicity of the adjuvanted Influenza A (H1N1) vaccine in HIV-infected children immunised according to national recommendations and assessed the impact of vaccination on individual CD4 counts and HIV viral loads., Methods: HIV-infected children attending outpatient appointments between 01 November and 31 December 2009 were offered two doses of H1N1 vaccine three weeks apart and a blood test before and 3 weeks after the second dose of vaccine. Serum antibody responses were determined by a haemagglutination inhibition (HAI) assay using standard methods., Results: Of the 39 children recruited for vaccination, 31 (median age 11.2, range 3.0-17.9 years) received both doses of vaccine and provided pre- and post-vaccination blood samples. Eight children (26%) had baseline HAI titres ≥ 1:32. After vaccination, 29 children (94%, 95% CI, 78.6-99.2%) had HAI titres ≥ 1:32 (seroprotection), of whom 27 (87.1%, 95% CI, 70.1-96.4%) had also had a four-fold rise in titres (seroconversion). In the univariate analysis, post-vaccination geometric mean titres (GMTs) were higher among the 21 children receiving highly active anti-retroviral therapy compared with the 10 treatment-naïve children (GMT 406 [95% CI 218-757] vs. 128 [49-336]; P=0.035), but this was no longer statistically significant when adjusted for prevaccine GMTs. There was no significant impact of vaccination on CD4+ T cell count or HIV viral load., Conclusion: The AS03(B)-adjuvanted pandemic Influenza A (H1N1) vaccine is highly immunogenic and appears to be safe in HIV-infected children., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

37. Low serum serotype-specific pneumococcal antibody concentrations in young children with Haemophilus influenzae serotype b (Hib) vaccine failure.

Author

Ladhani S, Borrow R, Heath PT, Ramsay ME, and Booy R

Subjects

Adolescent, Case-Control Studies, Child, Child, Preschool, Haemophilus Infections immunology, Haemophilus Infections prevention & control, Haemophilus influenzae type b classification, Haemophilus influenzae type b immunology, Humans, Risk Factors, Antibodies, Bacterial blood, Haemophilus Vaccines administration & dosage, Pneumococcal Infections immunology

Abstract

Serotype-specific pneumococcal antibody concentrations were measured in 164 children with Hib vaccine failure prior to routine pneumococcal immunisation. Compared with age-matched controls, a higher proportion of cases had non-protective antibody concentrations (< 0.35 microg/ml) for 7/9 (78%) serotypes tested among 2-4 year-olds, 4/9 (44%) among 5-7 year-olds, 1/9 (11%) among 8-11 year-olds and 0/9 (0%) among 12-15 year-olds (chi(2) for trend=14.0, p=0.0002). Cases aged 2-4 years were also more likely to have non-protective antibody concentrations against more serotypes than controls, suggesting that children with Hib vaccine failure may have an intact but physiologically delayed ability to develop protective antibody concentrations against encapsulated organisms., (2010. Published by Elsevier Ltd.)

Published

2010

38. Long-term complications and risk of other serious infections following invasive Haemophilus influenzae serotype b disease in vaccinated children.

Author

Ladhani S, Heath PT, Aibara RJ, Ramsay ME, Slack MPE, Hibberd ML, Pollard AJ, Moxon ER, and Booy R

Subjects

Adolescent, Child, Child, Preschool, Female, Humans, Infant, Male, Risk Factors, Surveys and Questionnaires, Treatment Failure, United Kingdom, Bacterial Capsules administration & dosage, Bacterial Capsules immunology, Haemophilus Infections complications, Haemophilus Infections microbiology, Haemophilus Vaccines administration & dosage, Haemophilus Vaccines immunology, Haemophilus influenzae type b isolation & purification

Abstract

This study describes the long-term complications in children with Haemophilus influenzae serotype b (Hib) vaccine failure and to determine their risk of other serious infections. The families of 323 children with invasive Hib disease after appropriate vaccination (i.e. vaccine failure) were contacted to complete a questionnaire relating to their health and 260 (80.5%) completed the questionnaire. Of the 124 children with meningitis, 18.5% reported serious long-term sequelae and a further 12.1% of parents attributed other problems to Hib meningitis. Overall, 14% (32/231 cases) of otherwise healthy children and 59% (17/29 cases) of children with an underlying condition developed at least one other serious infection requiring hospital admission. In a Poisson regression model, the risk of another serious infection was independently associated with the presence of an underlying medical condition (incidence risk ratio (IRR) 7.6, 95% CI 4.8-12.1; p<0.0001), both parents having had a serious infection (IRR 4.1, 95% CI 1.6-10.3; p=0.003), requirement of more than two antibiotic courses per year (IRR 2.3, 95% CI 1.4-3.6; p=0.001) and the presence of a long-term complication after Hib infection (IRR 1.8, 95% CI 1.1-3.1; p=0.03). Thus, rates of long-term sequelae in children with vaccine failure who developed Hib meningitis are similar to those in unvaccinated children in the pre-vaccine era. One in seven otherwise healthy children (14%) with Hib vaccine failure will go on to suffer another serious infection requiring hospital admission in childhood, which is higher than would be expected for the UK paediatric population., (Copyright 2009 Elsevier Ltd. All rights reserved.)

Published

2010

39. A local reaction at or near injection site: case definition and guidelines for collection, analysis, and presentation of immunization safety data.

Author

Gidudu J, Kohl KS, Halperin S, Hammer SJ, Heath PT, Hennig R, Hoet B, Rothstein E, Schuind A, Varricchio F, and Walop W

Subjects

Data Collection, Data Interpretation, Statistical, Demography, Documentation, Forms and Records Control, Humans, Safety, Terminology as Topic, Immunization adverse effects, Injections adverse effects, Skin pathology, Vaccination adverse effects

Abstract

The need for developing a case definition and guidelines for a local reaction at or near the injection site, methods for the development of the case definition and guidelines as an adverse event following immunization as well as the rationale for selected decisions about the case definition for a local reaction at or near the injection site are explained in the Preamble section. The case definition is structured in 2 levels of diagnostic certainty: level 1 includes any description of morphological or physiological change at or near the injection site that is described or identified by a healthcare provider. Level 2 is any description of morphological or physiological change at or near injection site that is described by any other person. In Guidelines section, the working group recommends to enable meaningful and standardized data collection, analysis, and presentation of information about a local reaction at or near the injection site. However, implementation of all guidelines might not be possible in all settings. The availability of information may vary depending upon resources, geographic region, and whether the source of information is a prospectively designed clinical trial, a post-marketing surveillance or epidemiologic study, or an individual report of a local reaction at injection site.

Published

2008

40. Immunogenicity and induction of immunological memory of the heptavalent pneumococcal conjugate vaccine in preterm UK infants.

Author

Ruggeberg JU, Collins C, Clarke P, Johnson N, Sinha R, Everest N, Chang J, Stanford E, Balmer P, Borrow R, Martin S, Robinson MJ, Moxon ER, Pollard AJ, and Heath PT

Subjects

Antibodies, Bacterial blood, Bacterial Capsules, Female, Haemophilus Vaccines immunology, Heptavalent Pneumococcal Conjugate Vaccine, Humans, Infant, Infant, Newborn, Infant, Premature, Male, Polysaccharides, Bacterial immunology, Streptococcus pneumoniae immunology, Vaccination, Immunologic Memory, Meningococcal Vaccines immunology, Pneumococcal Vaccines immunology

Abstract

Data on the immunogenicity and memory induction of pneumococcal conjugate vaccines in very preterm infants is limited. We vaccinated 69 full term and 68 preterm infants (median gestational age (GA) 30 weeks) with a 7-valent pneumococcal conjugate vaccine (PCV7) at 2/3/4 months of age, followed by a plain polysaccharide booster at 12 months of age. IgG-GMC (ELISA) was significantly lower in preterm infants to six vaccine serotypes (ST) at 2 months and 5 months of age, to five ST at 12 months of age and to three ST at 13 months of age. A significantly lower proportion of preterm infants achieved IgG levels>or=0.35 microg/ml to ST 4, 6B and 9V at 5 months and to ST 4, 6B, 18C, 19F and 23F at 12 months of age. Fold rises following the polysaccharide booster were comparable to those of term infants. At least 93% of both cohorts achieved IgG>or=0.35 microg/ml to all STs following booster vaccination. Pneumococcal conjugate vaccine at an accelerated schedule of 2/3/4 months of age is likely to provide protection against pneumococcal disease for preterm infants. Antibody concentrations wane over the first year of life in both preterm and term infants and booster vaccination is therefore likely to be important.

Published

2007

41. Response of steroid-treated former preterm infants to a single dose of meningococcal C conjugate vaccine.

Author

Clarke P, Robinson MJ, Ahmad I, Bedford-Russell AR, Connell JE, Powell PJ, and Heath PT

Subjects

Child, Preschool, Colony Count, Microbial, Female, Humans, Immunoglobulin G blood, Immunosuppressive Agents administration & dosage, Immunosuppressive Agents therapeutic use, Infant, Infant, Newborn, Male, Meningococcal Infections prevention & control, Meningococcal Vaccines administration & dosage, Steroids administration & dosage, Antibodies, Bacterial blood, Infant, Premature, Meningococcal Vaccines immunology, Neisseria meningitidis immunology, Steroids therapeutic use

Abstract

Attenuated antibody responses have been reported in preterm infants who received neonatal dexamethasone treatment. The duration of immunosuppression may extend into later infancy. This study assessed the immune response of former preterm infants to a single meningococcal serogroup C conjugate (MCC) immunisation given after infancy. A cohort of 49 toddlers born at less than 33 weeks' gestation were given an initial dose of MCC vaccine at a median age of 13 months; 11 had received dexamethasone in the neonatal period. Sera obtained 4 weeks post immunisation were analysed for serum bactericidal antibody (SBA) and serogroup C-specific IgG antibody concentrations. Immune responses were compared with those of an historical cohort of 70 term toddlers given a single dose of the same vaccine at age 13 months. An SBA titre of > or =8 was taken to indicate a protective response. Following a single MCC dose, the SBA geometric mean titre (GMT) for former preterm infants was 249 (95% C.I. 111, 558), not significantly different from that of the historical term cohort whose SBA GMT was 141 (95% C.I. 89, 224) (p=0.06). A significantly lower proportion of former preterm infants achieved a protective SBA titre of > or =8 compared with term infants, 37/48 (77%) versus 64/70 (91%), (p=0.03). For steroid-treated and non steroid-treated subgroups, SBA GMTs were 1237 (95% C.I. 250, 6132) and 154 (62, 385), respectively, and numbers achieving an SBA titre of > or =8 were 10/11 (91%) and 27/37 (73%), (p=0.42). Most children born at <33 weeks' gestation mount a protective immune response to a single MCC vaccine dose given at age 13 months, but fewer former preterm infants attain a protective SBA titre of 8 compared with term infants. Previous neonatal dexamethasone treatment does not appear to attenuate immune response after infancy.

Published

2006

42. Antibody responses to meningococcal (groups A, C, Y and W135) polysaccharide diphtheria toxoid conjugate vaccine in children who previously received meningococcal C conjugate vaccine.

Author

El Bashir H, Heath PT, Papa T, Ruggeberg JU, Johnson N, Sinha R, Balfour G, and Booy R

Subjects

Antibodies, Bacterial analysis, Antibody Formation, Child, Preschool, Diphtheria Toxoid administration & dosage, Diphtheria Toxoid immunology, Double-Blind Method, Humans, Immunologic Memory, Meningitis, Meningococcal immunology, Meningococcal Vaccines administration & dosage, Polysaccharides, Bacterial administration & dosage, Polysaccharides, Bacterial immunology, Vaccines, Conjugate adverse effects, Vaccines, Conjugate immunology, Meningitis, Meningococcal prevention & control, Meningococcal Vaccines immunology, Neisseria meningitidis chemistry

Abstract

A randomised, modified, double-blind trial was conducted in children 2 to < 5 years of age to evaluate immunogenicity and reactogenicity of a meningococcal (serogroups A, C, Y, W135) diphtheria toxoid conjugate vaccine (MCV-4) in healthy children previously vaccinated with a monovalent meningococcal C conjugate vaccine. Participants received one dose of either MCV-4 or Haemophilus influenzae type b vaccine (Hib vaccine, control group). Serum bactericidal antibodies (SBA) were determined in sera obtained before and approximately 28 days following vaccination. MCV-4 was highly immunogenic for serogroups A, C, Y and W135, the response to serogroup C being consistent with a booster response in participants primed with monovalent C conjugate vaccine. No major between-group differences in solicited local and systemic reactions or adverse events (AEs).

Published

2006

43. Nodule at injection site as an adverse event following immunization: case definition and guidelines for data collection, analysis, and presentation.

Author

Rothstein E, Kohl KS, Ball L, Halperin SA, Halsey N, Hammer SJ, Heath PT, Hennig R, Kleppinger C, Labadie J, Varricchio F, Vermeer P, and Walop W

Subjects

Humans, Skin Diseases pathology, Adverse Drug Reaction Reporting Systems standards, Data Collection statistics & numerical data, Data Interpretation, Statistical, Immunization adverse effects, Injections adverse effects, Skin Diseases etiology, Terminology as Topic

Published

2004

44. 4th European conference on vaccinology: societal value of vaccination. The impact of Hib conjugate vaccines in preventing invasive H. influenzae diseases in the UK.

Author

Moxon ER, Heath PT, Booy R, Azzopardi HJ, Slack MP, and Ramsay ME

Subjects

Bacterial Capsules, Humans, Immunization, United Kingdom, Vaccines, Conjugate immunology, Haemophilus Infections prevention & control, Haemophilus Vaccines immunology, Haemophilus influenzae, Polysaccharides, Bacterial immunology

Published

1999