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1. Group B Streptococcus (GBS) colonization is dynamic over time, whilst GBS capsular polysaccharides-specific antibody remains stable

Author

Haeusler, IL, Daniel, O, Isitt, C, Watts, R, Cantrell, L, Feng, S, Cochet, M, Salloum, M, Ikram, S, Hayter, E, Lim, S, Hall, T, Athaide, S, Cosgrove, CA, Tregoning, JS, Le Doare, K, and Wellcome Trust

Subjects
Adult, Male, Group B Streptococcus, colonisation, Immunology, VAGINAL SECRETIONS, DISEASE, SERUM, Streptococcus agalactiae, Polysaccharides, Pregnancy, Streptococcal Infections, capsular-polysaccharides specific antibodies, neonatal infection, Humans, Immunology and Allergy, NASAL, Pregnancy Complications, Infectious, CERVICAL SECRETIONS, Science & Technology, GBS vaccine, colonization, Antibodies, Bacterial, Immunoglobulin A, capsular-polysaccharides-specific antibodies, 1107 Immunology, Immunoglobulin G, mucosal immunity, VACCINATION, Female, Life Sciences & Biomedicine, RESPONSES, TRACT
Abstract

Group B Streptococcus (GBS) is a leading cause of adverse pregnancy outcomes due to invasive infection. This study investigated longitudinal variation in GBS rectovaginal colonization, serum and vaginal GBS capsular polysaccharide (CPS)-specific antibody levels. Non-pregnant women were recruited in the UK and were sampled every 2 weeks over a 12-week period. GBS isolates were taken from recto-vaginal swabs and serotyped by polymerase chain reaction. Serum and vaginal immunoglobulin G (IgG) and nasal immunoglobulin A (IgA) specific to CPS were measured by Luminex, and total IgG/A by ELISA. Seventy women were enrolled, of median age 26. Out of the 66 participants who completed at least three visits: 14/47 (29.8%) women that were GBS negative at screening became positive in follow-up visits and 16/19 (84.2%) women who were GBS positive at screening became negative. There was 50% probability of becoming negative 36 days after the first positive swab. The rate of detectable GBS carriage fluctuated over time, although serum, vaginal, and nasal CPS-specific antibody levels remained constant. Levels of CPS-specific antibodies were higher in the serum of individuals colonized with GBS than in non-colonized, but similar in the vaginal and nasal mucosa. We found correlations between antibody levels in serum and the vaginal and nasal mucosa. Our study demonstrates the feasibility of elution methods to retrieve vaginal and nasal antibodies, and the optimization of immunoassays to measure GBS-CPS-specific antibodies. The difference between the dynamics of colonization and antibody response is interesting and further investigation is required for vaccine development.

Published
2022

2. Systematic review and meta-analysis of the effectiveness and perinatal outcomes of COVID-19 vaccination in pregnancy

Author

Prasad, S, Kalafat, E, Blakeway, H, Townsend, R, O'Brien, P, Morris, E, Draycott, T, Thangaratinam, S, Le Doare, K, Ladhani, S, von Dadelszen, P, Magee, LA, Heath, P, and Khalil, A

Abstract

Safety and effectiveness of COVID-19 vaccines during pregnancy is a particular concern affecting vaccination uptake by this vulnerable group. Here we evaluated evidence from 23 studies including 117,552 COVID-19 vaccinated pregnant people, almost exclusively with mRNA vaccines. We show that the effectiveness of mRNA vaccination against RT-PCR confirmed SARS-CoV-2 infection 7 days after second dose was 89·5% (95% CI 69·0-96·4%, 18,828 vaccinated pregnant people, I2 = 73·9%). The risk of stillbirth was significantly lower in the vaccinated cohort by 15% (pooled OR 0·85; 95% CI 0·73-0·99, 66,067 vaccinated vs. 424,624 unvaccinated, I2 = 93·9%). There was no evidence of a higher risk of adverse outcomes including miscarriage, earlier gestation at birth, placental abruption, pulmonary embolism, postpartum haemorrhage, maternal death, intensive care unit admission, lower birthweight Z-score, or neonatal intensive care unit admission (p > 0.05 for all). COVID-19 mRNA vaccination in pregnancy appears to be safe and is associated with a reduction in stillbirth.

Published
2022

4. Defining operational strengths and gaps relevant to post licensure Group B Streptococcus vaccine effectiveness studies: an expert stakeholder evaluation of the United Kingdom and Uganda

Author

Skirrow, H, Kajungu, D, Le Doare, K, Chantler, T, Kampmann, B, and NATIONAL Institute of Health Research (NIHR)

Subjects
reproductive and urinary physiology
Abstract

A future Group B Streptococcal (GBS) vaccine for pregnant women to protect neonates is likely to be licensed based on evidence of vaccine induced protective antibody levels. Post licensure surveillance to monitor the impact of any future vaccine on GBS disease therefore needs to be clearly defined (in both high and low income settings). A priority research gap is understanding health system preparedness for a GBS vaccine evaluation This expert stakeholder evaluation aimed to describe the UK and Uganda's operational strengths and gaps relevant to post-licensure GBS vaccine studies.

Published
2022

5. A Vaccine Against Group B Streptococcus: Recent Advances

Author

Carreras-Abad, C, Ramkhelawon, L, Heath, PT, and Le Doare, K

Subjects
Group B streptococcus, neonatal sepsis, maternal vaccines, Infant sepsis, infant sepsis, Streptococcus agalactiae, lcsh:Infectious and parasitic diseases, Maternal immunisation, Neonatal sepsis, streptococcus agalactiae, lcsh:RC109-216, Maternal vaccines, maternal immunization, group b streptococcus
Abstract

Clara Carreras-Abad,1,2 Laxmee Ramkhelawon,1 Paul T Heath,1 Kirsty Le Doare1,3,4 1Paediatric Infectious Diseases Research Group and Vaccine Institute, Institute for Infection and Immunity, St George’s, University of London, London, UK; 2Department of Paediatrics, Obstetrics and Gynecology and Preventive Medicine and Public Health, Universitat Autònoma de Barcelona, Barcelona, Spain; 3Pathogen Immunity Group, Public Health England, Porton Down,UK; 4Medical Research Council/Uganda Virus Research Institute and London School of Hygiene and Tropical Medicine, Uganda Research Unit, Entebbe, UgandaCorrespondence: Clara Carreras-AbadPaediatric Infectious Diseases Research Group, Institute for Infection and Immunity, St George’s, University of London, Jenner Wing, Level 2 Mailpoint J2C, Cranmer Terrace, London SW17 0RE, UKEmail ccarrera@sgul.ac.ukAbstract: Group B streptococcus (GBS) causes a high burden of neonatal and infant disease globally. Implementing a vaccine for pregnant women is a promising strategy to prevent neonatal and infant GBS disease and has been identified as a priority by the World Health Organisation (WHO). GBS serotype-specific polysaccharide – protein conjugate vaccines are at advanced stages of development, but a large number of participants would be required to undertake Phase III clinical efficacy trials. Efforts are therefore currently focused on establishing serocorrelates of protection in natural immunity studies as an alternative pathway for licensure of a GBS vaccine, followed by Phase IV studies to evaluate safety and effectiveness. Protein vaccines are in earlier stages of development but are highly promising as they might confer protection irrespective of serotype. Further epidemiological, immunological and health economic studies are required to enable the vaccine to reach its target population as soon as possible.Keywords: Group B streptococcus, Streptococcus agalactiae, maternal vaccines, maternal immunisation, neonatal sepsis, infant sepsis

Published
2020

6. An internally validated prediction model for critical COVID-19 infection and intensive care unit admission in symptomatic pregnant women

Author

Kalafat, E. Prasad, S. Birol, P. Tekin, A.B. Kunt, A. Di Fabrizio, C. Alatas, C. Celik, E. Bagci, H. Binder, J. Le Doare, K. Magee, L.A. Mutlu, M.A. Yassa, M. Tug, N. Sahin, O. Krokos, P. O'brien, P. von Dadelszen, P. Palmrich, P. Papaioannou, G. Ayaz, R. Ladhani, S.N. Kalantaridou, S. Mihmanli, V. Khalil, A.

Abstract

Background: Pregnant women are at an increased risk of mortality and morbidity owing to COVID-19. Many studies have reported on the association of COVID-19 with pregnancy-specific adverse outcomes, but prediction models utilizing large cohorts of pregnant women are still lacking for estimating the risk of maternal morbidity and other adverse events. Objective: The main aim of this study was to develop a prediction model to quantify the risk of progression to critical COVID-19 and intensive care unit admission in pregnant women with symptomatic infection. Study Design: This was a multicenter retrospective cohort study including 8 hospitals from 4 countries (the United Kingdom, Austria, Greece, and Turkey). The data extraction was from February 2020 until May 2021. Included were consecutive pregnant and early postpartum women (within 10 days of birth); reverse transcriptase polymerase chain reaction confirmed SARS-CoV-2 infection. The primary outcome was progression to critical illness requiring intensive care. The secondary outcomes included maternal death, preeclampsia, and stillbirth. The association between the primary outcome and 12 candidate predictors having a known association with severe COVID-19 in pregnancy was analyzed with log-binomial mixed-effects regression and reported as adjusted risk ratios. All the potential predictors were evaluated in 1 model and only the baseline factors in another. The predictive accuracy was assessed by the area under the receiver operating characteristic curves. Results: Of the 793 pregnant women who were positive for SARS-CoV-2 and were symptomatic, 44 (5.5%) were admitted to intensive care, of whom 10 died (1.3%). The ‘mini-COvid Maternal Intensive Therapy’ model included the following demographic and clinical variables available at disease onset: maternal age (adjusted risk ratio, 1.45; 95% confidence interval, 1.07–1.95; P=.015); body mass index (adjusted risk ratio, 1.34; 95% confidence interval, 1.06–1.66; P=.010); and diagnosis in the third trimester of pregnancy (adjusted risk ratio, 3.64; 95% confidence interval, 1.78–8.46; P=.001). The optimism-adjusted area under the receiver operating characteristic curve was 0.73. The ‘full-COvid Maternal Intensive Therapy’ model included body mass index (adjusted risk ratio, 1.39; 95% confidence interval, 1.07–1.95; P=.015), lower respiratory symptoms (adjusted risk ratio, 5.11; 95% confidence interval, 1.81–21.4; P=.007), neutrophil to lymphocyte ratio (adjusted risk ratio, 1.62; 95% confidence interval, 1.36–1.89; P

Published
2022

7. Gastrointestinal, vaginal, nasopharyngeal, and breast milk microbiota profiles and breast milk metabolomic changes in Gambian infants over the first two months of lactation: A prospective cohort study

Author

Karampatsas, K, Faal, A, Jaiteh, M, Garcia-Perez, I, Aller, S, Shaw, AG, Kopytek, A, Witney, AA, Le Doare, K, and The Imperial College Wellcome Trust Centre for Global Health Research

Subjects
Milk, Human, Bacteria, Microbiota, Infant, Newborn, Infant, 1103 Clinical Sciences, General Medicine, Arthritis & Rheumatology, Breast Feeding, RNA, Ribosomal, 16S, Humans, Lactation, Female, Gambia, Prospective Studies
Abstract

Background Microbiota composition in breast milk affects intestinal and respiratory microbiota colonization and the mucosal immune system's development in infants. The metabolomic content of breast milk is thought to interact with the microbiota and may influence developing infant immunity.\ud \ud Methods 107 Gambian mothers and their healthy, vaginally delivered, exclusively breastfed infants were included in our study. We analyzed 32 breast milk samples, 51 maternal rectovaginal swabs and 30 infants' rectal swabs at birth. We also analyzed 9 breast milk samples and 18 infants' nasopharyngeal swabs 60 days post-delivery. We used 16S rRNA gene sequencing to determine the microbiota composition. Metabolomic profiling analysis was performed on colostrum and mature breast milk samples using a multiplatform approach combining 1-H Nuclear Magnetic Resonance Spectroscopy and Gas Chromatography-Mass Spectrometry. \ud \ud Results Bacterial communities were distinct in composition and diversity across different sample types. Breast milk composition changed over the first 60 days of lactation. α-1,4- and α-1,3-fucosylated human milk oligosaccharides, and other 33 key metabolites in breast milk (monosaccharides, sugar alcohols and fatty acids) increased between birth and day 60 of life.\ud \ud Conclusions This study's results indicate that infant gut and respiratory microbiota are unique bacterial communities, distinct from maternal gut and breast milk, respectively. Breast milk microbiota composition and metabolomic profile change throughout lactation. These changes may contribute to the infant's immunological, metabolic, and neurological development and could consist the basis for future interventions to correct disrupted early life microbial\ud colonization.

Published
2022

8. The Italian arm of the PREPARE study: an international project to evaluate and license a maternal vaccine against group B streptococcus

Author

Berardi A., Cassetti T., Creti R., Vocale C., Ambretti S., Sarti M., Facchinetti F., Cose S., van Bijlsma M., van De Beek D., Poyart C., French N., Nielsen M., Musoke P., Davies H., Ovale S., Lugli L., Capretti M. G., Lanari M., Dondi A., Ciccia M., Francavilla R., Lanzoni A., Baroni L., Fornaciari S., Carretto E., Alessandrini C., Lucia G., Perrone S., Calderaro A., Bacchini P., Giugno C., Rota C., Pagano R., Guidi B., Biasucci G., Benenati B., Schiavo R., Piccinini G., Pulvirenti R., Rizzo V., Ancora G., China C., Papa I., Viola L., Pedna M. F., Bua J., Travan L., Busetti M., Santori D., Merazzi D., Papa A., Laura L., Auriti C., Bernaschi P., Vento G., Giordano L., Spanu T., Haass C., Margiotta M. C., Nardella G., De Nittis R., Laforgia N., Loprieno S., Giuseppe L., Moramarco A. M., Tzialla C., Fasolato V., Orlandini S., Decembrino L., Del Campo G., Maiocchi A., Cuttano A., Tuoni C., Barnini S., Carnielli V., Perrone B., Orecchioni F., Visintini F., Arzese A., Heath P., Le Doare K., Neurology, Amsterdam Neuroscience - Neuroinfection & -inflammation, AII - Infectious diseases, Berardi A., Cassetti T., Creti R., Vocale C., Ambretti S., Sarti M., Facchinetti F., Cose S., van Bijlsma M., van De Beek D., Poyart C., French N., Nielsen M., Musoke P., Davies H., Ovale S., Lugli L., Capretti M.G., Lanari M., Dondi A., Ciccia M., Francavilla R., Lanzoni A., Baroni L., Fornaciari S., Carretto E., Alessandrini C., Lucia G., Perrone S., Calderaro A., Bacchini P., Giugno C., Rota C., Pagano R., Guidi B., Biasucci G., Benenati B., Schiavo R., Piccinini G., Pulvirenti R., Rizzo V., Ancora G., China C., Papa I., Viola L., Pedna M.F., Bua J., Travan L., Busetti M., Santori D., Merazzi D., Papa A., Laura L., Auriti C., Bernaschi P., Vento G., Giordano L., Spanu T., Haass C., Margiotta M.C., Nardella G., De Nittis R., Laforgia N., Loprieno S., Giuseppe L., Moramarco A.M., Tzialla C., Fasolato V., Orlandini S., Decembrino L., Del Campo G., Maiocchi A., Cuttano A., Tuoni C., Barnini S., Carnielli V., Perrone B., Orecchioni F., Visintini F., Arzese A., Heath P., and Le Doare K.

Subjects
0301 basic medicine, Pediatrics, medicine.medical_specialty, Group B streptococcus, Sepsi, International Cooperation, 030106 microbiology, Disease, Abortion, Group B, Streptococcus agalactiae, Sepsis, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Streptococcal Infections, medicine, Humans, Meningitis, 030212 general & internal medicine, Newborn, Prevention, Vaccine, Pregnancy Complications, Infectious, Antibiotic prophylaxis, reproductive and urinary physiology, Group B streptococcu, business.industry, Streptococcal Vaccines, Infant, Newborn, lcsh:RJ1-570, lcsh:Pediatrics, Antibiotic Prophylaxis, medicine.disease, Infectious Disease Transmission, Vertical, Meningiti, Pneumonia, Italy, Immunization, Commentary, Female, business
Abstract

Background Group B streptococcus (GBS) is a leading cause of sepsis, pneumonia and meningitis in infants, with long term neurodevelopmental sequelae. GBS may be associated with poor pregnancy outcomes, including spontaneous abortion, stillbirth and preterm birth. Intrapartum antibiotic prophylaxis (IAP) is currently the only way to prevent early-onset disease (presenting at 0 to 6 days of life), although it has no impact on the disease presenting over 6 days of life and its implementation is challenging in resource poor countries. A maternal vaccine against GBS could reduce all GBS manifestations as well as improve pregnancy outcomes, even in low-income countries. Main body The term “PREPARE” designates an international project aimed at developing a maternal vaccination platform to test vaccines against neonatal GBS infections by maternal immunization. It is a non-profit, multi-center, interventional and experimental study (promoted by the St George University of London. [UK]) with the aim of developing a maternal vaccination platform, determining pregnancy outcomes, and defining the extent of GBS infections in children and mothers in Africa. PREPARE also aims to estimate the protective serocorrelates against the main GBS serotypes that cause diseases in Europe and Africa and to conduct two trials on candidate GBS vaccines. PREPARE consists of 6 work packages. In four European countries (Italy, UK, Netherlands, France) the recruitment of cases and controls will start in 2020 and will end in 2022. The Italian PREPARE network includes 41 centers. The Italian network aims to collect: GBS isolates from infants with invasive disease, maternal and neonatal sera (cases); cord sera and GBS strains from colonized mothers whose infants do not develop GBS infection (controls). Short conclusion PREPARE will contribute information on protective serocorrelates against the main GBS serotypes that cause diseases in Europe and Africa. The vaccine that will be tested by the PREPARE study could be an effective strategy to prevent GBS disease.

Published
2020

10. The current state of immunization against Gram-negative bacteria in children: a review of the literature

Author

Broad, J, Le Doare, K, Heath, P, Hallchurch, P, Whelan, I, Boyd, H, Carruthers, E, Sharland, M, and Ladhani, S

Abstract

Purpose of review \ud Gram-negative bacteria (GNB) are a major cause of infection worldwide and multidrug resistance in infants and children. The major pathogens include Klebsiella pneumoniae, Escherichia coli, Enterobacter spp., Pseudomonas aeruginosa and Acinetobacter baumannii. With new antibiotic options limited, immunization is likely to play a critical role in prevention. This review discusses their epidemiology, the current state of vaccine research and potential immunization strategies to protect children. A comprehensive review of the literature, conference abstracts along with web searches was performed to identify current and investigational vaccines against the major GNB in children.\ud \ud Recent findings \ud Phase I--III vaccine trials have been undertaken for the major Gram-negative bacteria but not in infants or children. E. coli is a common infection in immune-competent children, including neonatal sepsis. Several vaccines are in late-phase clinical trials, with some already licensed for recurrent urinary tract infections in women. Klebsiella spp. causes community-acquired and hospital-acquired infections, including sepsis in neonates and immunocompromised children although no vaccine trials have extended beyond early phase 2 trials. P. aeruginosa is a common pathogen in patients with cystic fibrosis. Phase 1--3 vaccine and monoclonal antibody trials are in progress, although candidates provide limited coverage against pathogenic strains. Enterobacter spp. and A. baumannii largely cause hospital-acquired infections with experimental vaccines limited to phase 1 research.\ud \ud Summary \ud The current immunization pipelines for the most prevalent GNB are years away from licensure. Similar to incentives for new antibiotics, global efforts are warranted to expedite the development of effective vaccines.

Published
2020

12. 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

13. Aetiology of invasive bacterial infection and antimicrobial resistance in neonates in sub-Saharan Africa: a systematic review and meta-analysis in line with the STROBE-NI reporting guidelines

Author

Okomo, U, Akpalu, ENK, Le Doare, K, Roca, A, Cousens, S, Jarde, A, Sharland, M, Kampmann, B, and Lawn, JE

Abstract

BACKGROUND: Aetiological data for neonatal infections are essential to inform policies and programme strategies, but such data are scarce from sub-Saharan Africa. We therefore completed a systematic review and meta-analysis of available data from the African continent since 1980, with a focus on regional differences in aetiology and antimicrobial resistance (AMR) in the past decade (2008-18). METHODS: We included data for microbiologically confirmed invasive bacterial infection including meningitis and AMR among neonates in sub-Saharan Africa and assessed the quality of scientific reporting according to Strengthening the Reporting of Observational Studies in Epidemiology for Newborn Infection (STROBE-NI) checklist. We calculated pooled proportions for reported bacterial isolates and AMR. FINDINGS: We included 151 studies comprising data from 84 534 neonates from 26 countries, almost all of which were hospital-based. Of the 82 studies published between 2008 and 2018, insufficient details were reported regarding most STROBE-NI items. Regarding culture positive bacteraemia or sepsis, Staphylococcus aureus, Klebsiella spp, and Escherichia coli accounted for 25% (95% CI 21-29), 21% (16-27), and 10% (8-10) respectively. For meningitis, the predominant identified causes were group B streptococcus 25% (16-33), Streptococcus pneumoniae 17% (9-6), and S aureus 12% (3-25). Resistance to WHO recommended β-lactams was reported in 614 (68%) of 904 cases and resistance to aminoglycosides in 317 (27%) of 1176 cases. INTERPRETATION: Hospital-acquired neonatal infections and AMR are a major burden in Africa. More population-based neonatal infection studies and improved routine surveillance are needed to improve clinical care, plan health systems approaches, and address AMR. Future studies should be reported according to standardised reporting guidelines, such as STROBE-NI, to aid comparability and reduce research waste. FUNDING: Uduak Okomo was supported by a Medical Research Council PhD Studentship.

Published
2019

14. Breast Milk Cytokines and Early Growth in Gambian Infants

Author

Saso, A, Blyuss, O, Munblit, D, Faal, A, Moore, S, and Le Doare, K

Subjects
Breast milk, growth, CHILDREN, Growth, Pediatrics, LEPTIN, Neonate, cytokine, Cytokine, ASSOCIATIONS, Original Research, Science & Technology, PRETERM, Colostrum, COMPONENTS, Immunity, Infant, weight, Weight, TNF-ALPHA, infant, immunity, WEIGHT-GAIN, OLIGOSACCHARIDES, colostrum, UMBILICAL-CORD BLOOD, breast milk, HEALTH, neonate, Life Sciences & Biomedicine
Abstract

Background: Breast milk provides nutrition for infants but also delivers other bioactive factors that have key protective and developmental benefits. In particular, cytokines are thought to play a role in immunomodulation, although little is known about their impact on health outcomes in early life. Objective: The purpose of this pilot study was to evaluate the relationship between cytokines in breast milk and infant growth outcomes in a low-income setting. Methods: 100 mother-infant pairs were followed up to 2-3 months postpartum as part of a prospective longitudinal cohort study in urban Gambia, West Africa. The concentrations of 9 pro-inflammatory cytokines (IL-1β, IL-2, IL-4, IL-6, IL-10, IL-12, IL-13, IFN-γ, TNFα), IGF-1 and TGFβ2 were measured in colostrum within 12 h of birth and in breast milk at the final visit, scheduled between day 60 and 89 postpartum. Infant weight was recorded and converted to weight-for-age Z-scores (WAZ) at the same time points. Growth outcomes were defined in our study as (a) change in WAZ between birth and final visit (b) WAZ at final visit. Linear regression analysis was used to determine the ability of colostrum and breast milk cytokine concentrations to predict growth outcomes up to 2-3 months postpartum. Results: Gambian infants demonstrated growth faltering across the first 2-3 months postpartum. There was no significant relationship between cytokines in colostrum and subsequent change in WAZ between birth and the final visit, in either unadjusted or adjusted models. However, cytokines in mature breast milk, TNFα, IFNγ, IL1β, IL2, IL4, and IL6, were weak negative predictors of WAZ scores at the final visit, in unadjusted models (p < 0.05). When adjusted for maternal anemia (as a proxy for maternal nutrition), TNFα and IL6 remained significant predictors (p < 0.05). Conclusions: Variations in breast milk cytokine levels do not play a substantial role in the growth faltering observed across early infancy. The potential contribution of other factors, such as micronutrients, hormones or human milk oligosaccharides, must be elucidated. Cytokine levels in mature breast milk were weakly predictive of poor infant growth, possibly reflecting a "read-out" of suboptimal maternal health and nutrition.

Published
2019

15. The impact of timing of maternal influenza immunization on infant antibody levels at birth

Author

Zhong, Z, Haltalli, M, Holder, B, Rice, T, Donaldson, B, O'Driscoll, M, Le-Doare, K, Kampmann, B, and Tregoning, JS

Abstract

Pregnant women and infants are at an increased risk of severe disease after influenza infection. Maternal immunization is a potent tool to protect both these at-risk groups. While the primary aim of maternal influenza vaccination is to protect the mother, a secondary benefit is the transfer of protective antibodies to the infant. A recent study using the tetanus, diphtheria and acellular pertussis (Tdap) vaccine indicated that children born to mothers immunized in the second trimester of pregnancy had the highest antibody titres compared to children immunized in the third trimester. The aim of the current study was to investigate how the timing of maternal influenza immunization impacts infant antibody levels at birth. Antibody titres were assessed in maternal and cord blood samples by both immunoglobulin (Ig)G-binding enzyme-linked immunosorbent assay (ELISA) and haemagglutination inhibition assay (HAI). Antibody titres to the H1N1 component were significantly higher in infants born to mothers vaccinated in either the second or third trimesters than infants born to unvaccinated mothers. HAI levels in the infant were significantly lower when maternal immunization was performed less than 4 weeks before birth. These studies confirm that immunization during pregnancy increases the antibody titre in infants. Importantly, antibody levels in cord blood were significantly higher when the mother was vaccinated in either trimesters 2 or 3, although titres were significantly lower if the mother was immunized less than 4 weeks before birth. Based on these data, seasonal influenza vaccination should continue to be given in pregnancy as soon as it becomes available.

Published
2019

17. Mother's Milk: A Purposeful Contribution to the Development of the infant Microbiota and immunity

Author

Le Doare, K, Holder, B, Bassett, A, and Pannaraj, PS

Abstract

Breast milk is the perfect nutrition for infants, a result of millions of years of evolution. In addition to providing a source of nutrition, breast milk contains a diverse array of microbiota and myriad biologically active components that are thought to guide the infant’s developing mucosal immune system. It is believed that bacteria from the mother’s intestine may translocate to breast milk and dynamically transfer to the infant. Such interplay between mother and her infant is a key to establishing a healthy infant intestinal microbiome. These intestinal bacteria protect against many respiratory and diarrheal illnesses, but are subject to environmental stresses such as antibiotic use. Orchestrating the development of the microbiota are the human milk oligosaccharides (HMOs), the synthesis of which are partially determined by the maternal genotype. HMOs are thought to play a role in preventing pathogenic bacterial adhesion though multiple mechanisms, while also providing nutrition for the microbiome. Extracellular vesicles (EVs), including exosomes, carry a diverse cargo, including mRNA, miRNA, and cytosolic and membrane-bound proteins, and are readily detectable in human breast milk. Strongly implicated in cell–cell signaling, EVs could therefore may play a further role in the development of the infant microbiome. This review considers the emerging role of breast milk microbiota, bioactive HMOs, and EVs in the establishment of the neonatal microbiome and the consequent potential for modulation of neonatal immune system development.

Published
2018

18. Vaccination in Pregnancy-Recent Developments

Author

Jones, CE, Calvert, A, and Le Doare, K

Abstract

As early as the 19th century vaccination in pregnancy has been observed to protect both mothers and infants against smallpox, pertussis and tetanus. More recently the pace and\ud focus of maternal vaccination has accelerated, most significantly since the influenza pandemic of 2009. Vaccination in pregnancy boosts the concentration of vaccine-specific antibody in the mother to increase antibody concentration in the infant at birth, providing protection until the period of maximum susceptibility or risk has passed or until the infant has completed the routine infant immunizations.\ud There are now 3 vaccines, which have specific recommendations for routine use in pregnancy in an increasing number of countries, and other vaccines are progressing through clinical trials. Here we review the\ud mechanisms of protection, the current recommendations and future prospects, and evaluation of safety of vaccines in pregnancy.

Published
2018

19. Intrapartum Antibiotic Chemoprophylaxis Policies for the Prevention of Group B Streptococcal Disease Worldwide: Systematic Review

Author

Linda Bartlett, Johan Vekemans, Craig E. Rubens, Anna C. Seale, Shabir A. Madhi, Farah Seedat, Clare L. Cutland, Megan O'Driscoll, Sobanjo-Ter Meulen A, Margaret Ip, Paul T. Heath, Carol J. Baker, Le Doare K, Stephanie J. Schrag, Shampa Saha, Kim Turner, Neal Russell, Joy E Lawn, Beate Kampmann, and Michael G Gravett

Subjects
0301 basic medicine, Microbiology (medical), group B Streptococcus, medicine.drug_class, 030106 microbiology, Antibiotics, Immunology, MEDLINE, Scopus, VACCINE, Streptococcal disease, Disease, Microbiology, Group B, PROPHYLAXIS, Streptococcus agalactiae, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Environmental health, Streptococcal Infections, Medicine, Humans, 030212 general & internal medicine, Pregnancy Complications, Infectious, The Burden of Group B Streptococcus Worldwide for Pregnant Women, Stillbirths, and Children, intrapartum antibiotic chemoprophylaxis, Science & Technology, business.industry, Health Policy, 11 Medical And Health Sciences, Antibiotic Prophylaxis, 06 Biological Sciences, Infectious Disease Transmission, Vertical, 3. Good health, ERA, Infectious Diseases, MICROBIOME, INFECTIONS, Chemoprophylaxis, Female, business, Life Sciences & Biomedicine, Biomedical sciences, GBS Intrapartum Antibiotic Investigator Group
Abstract

There is heterogeneity in intrapartum antibiotic use and implementation of policy varies widely. Global strategies to enhance the prevention of group B streptococcal disease that may include maternal vaccination are needed., Background Intrapartum antibiotic chemoprophylaxis (IAP) prevents most early-onset group B streptococcal (GBS) disease. However, there is no description of how IAP is used around the world. This article is the sixth in a series estimating the burden of GBS disease. Here we aimed to review GBS screening policies and IAP implementation worldwide. Methods We identified data through (1) systematic literature reviews (PubMed/Medline, Embase, Literature in the Health Sciences in Latin America and the Caribbean [LILACS], World Health Organization library database [WHOLIS], and Scopus) and unpublished data from professional societies and (2) an online survey and searches of policies from medical societies and professionals. We included data on whether an IAP policy was in use, and if so whether it was based on microbiological or clinical risk factors and how these were applied, as well as the estimated coverage (percentage of women receiving IAP where indicated). Results We received policy information from 95 of 195 (49%) countries. Of these, 60 of 95 (63%) had an IAP policy; 35 of 60 (58%) used microbiological screening, 25 of 60 (42%) used clinical risk factors. Two of 15 (13%) low-income, 4 of 16 (25%) lower-middle–income, 14 of 20 (70%) upper-middle–income, and 40 of 44 (91%) high-income countries had any IAP policy. The remaining 35 of 95 (37%) had no national policy (25/33 from low-income and lower-middle–income countries). Coverage varied considerably; for microbiological screening, median coverage was 80% (range, 20%–95%); for clinical risk factor–based screening, coverage was 29% (range, 10%–50%). Although there were differences in the microbiological screening methods employed, the individual clinical risk factors used were similar. Conclusions There is considerable heterogeneity in IAP screening policies and coverage worldwide. Alternative global strategies, such as maternal vaccination, are needed to enhance the scope of global prevention of GBS disease.

Published
2017

20. SIgA, TGF-beta 1, IL-10, and TNF alpha in Colostrum Are Associated with Infant Group B Streptococcus Colonization

Author

Le Doare, K, Bellis, K, Faal, A, Birt, J, Munblit, D, Humphries, H, Taylor, S, Warburton, F, Heath, PT, Kampmann, B, and Gorringe, A

Subjects
bacteria, bacterial infections and mycoses, reproductive and urinary physiology
Abstract

Background: Group B Streptococcus (GBS) is a major cause of mortality and morbidity in infants and is associated with transmission from a colonized mother at birth and via infected breastmilk. Although maternal/infant colonization with GBS is common, the majority of infants exposed to GBS remain unaffected. The association between breastmilk immune factors and infant colonization and disease prevention has not been elucidated.\ud \ud Objectives: We have investigated the association between SIgA and cytokines in breastmilk and infant GBS colonization and clearance.\ud \ud Methods: Mother/infant GBS colonization was determined in a prospective cohort of 750 Gambian mother/infant pairs followed to day 89 of life. Anti-GBS secretory IgA bound to the surface of whole bacteria was assessed by flow cytometry and a panel of 12 cytokines quantified by mesoscale discovery in colostrum, breastmilk and serum.\ud \ud Results: Compared with infants receiving low anti-GBS SIgA in colostrum, infants receiving high anti-GBS SIgA were at decreased risk of GBS colonization for serotypes III and V. Infants colonized at day 6 were twice as likely to receive colostrum with high TGF-β1, TNFα, IL10, and IL-6 compared to uncolonized infants. Infants receiving high colostral TGF-β1, TNFα, and IL-6 had two-fold enhanced GBS clearance between birth and day 89.\ud \ud Conclusion: Our results suggest that the infant GBS colonization risk diminishes with increasing anti-GBS SIgA antibody in breastmilk and that key maternally derived cytokines might contribute to protection against infant colonization. These findings might be leveraged to develop interventions including maternal vaccination that may reduce infant GBS colonization.

Published
2017

21. 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
Group B Streptococcus, Adult, Mothers, Article, Cohort Studies, Young Adult, Pregnancy, Neonatal, Nasopharynx, Streptococcal Infections, Humans, Meningitis, Longitudinal Studies, Pregnancy Complications, Infectious, Child, reproductive and urinary physiology, Vaccines, Infant, Newborn, Infant, Streptococcus, Opsonin Proteins, bacterial infections and mycoses, Fetal Blood, Flow Cytometry, Antibodies, Bacterial, Infectious Disease Transmission, Vertical, Child, Preschool, Carrier State, Complement C3b, Immunologic Techniques, bacteria, Female, Gambia, Immunity, Maternally-Acquired
Abstract

Highlights • As maternally-derived anti-GBS antibody increases infant colonization risk decreases. • There is a serotype-specific threshold above which an infant is uncolonised with GBS. • Higher anti-GBS antibody is associated with infant clearance of GBS between birth and 3 months., 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

Published
2017

22. Intrapartum Antibiotic Chemoprophylaxis Policies for the Prevention of Group B Streptococcal Disease Worldwide: Systematic Review

Author

Le Doare, K, O'Driscoll, M, Turner, K, Seedat, F, Russell, NJ, Seale, AC, Heath, PT, Lawn, JE, Baker, CJ, Bartlett, L, Cutland, C, Gravett, MG, Ip, M, Madhi, SA, Rubens, CE, Saha, SK, Schrag, S, Sobanjo-Ter Meulen, A, Vekemans, J, Kampmann, B, and GBS Intrapartum Antibiotic Investigator Group

Abstract

Background: Intrapartum antibiotic chemoprophylaxis (IAP) prevents most early-onset group B streptococcal (GBS) disease. However, there is no description of how IAP is used around the world. This article is the sixth in a series estimating the burden of GBS disease. Here we aimed to review GBS screening policies and IAP implementation worldwide. Methods: We identified data through (1) systematic literature reviews (PubMed/Medline, Embase, Literature in the Health Sciences in Latin America and the Caribbean [LILACS], World Health Organization library database [WHOLIS], and Scopus) and unpublished data from professional societies and (2) an online survey and searches of policies from medical societies and professionals. We included data on whether an IAP policy was in use, and if so whether it was based on microbiological or clinical risk factors and how these were applied, as well as the estimated coverage (percentage of women receiving IAP where indicated). Results: We received policy information from 95 of 195 (49%) countries. Of these, 60 of 95 (63%) had an IAP policy; 35 of 60 (58%) used microbiological screening, 25 of 60 (42%) used clinical risk factors. Two of 15 (13%) low-income, 4 of 16 (25%) lower-middle-income, 14 of 20 (70%) upper-middle-income, and 40 of 44 (91%) high-income countries had any IAP policy. The remaining 35 of 95 (37%) had no national policy (25/33 from low-income and lower-middle-income countries). Coverage varied considerably; for microbiological screening, median coverage was 80% (range, 20%-95%); for clinical risk factor-based screening, coverage was 29% (range, 10%-50%). Although there were differences in the microbiological screening methods employed, the individual clinical risk factors used were similar. Conclusions: There is considerable heterogeneity in IAP screening policies and coverage worldwide. Alternative global strategies, such as maternal vaccination, are needed to enhance the scope of global prevention of GBS disease.

Published
2017

24. Fifteen minute consultation: Managing neonatal and childhood herpes encephalitis

Author

Le Doare, K, Menson, Esse, Patel, Deepak, Lim, Ming, Lyall, Hermione, and Herberg, Jethro

Subjects
SIMPLEX ENCEPHALITIS, Male, Herpesvirus 2, Human, Immunology, Acyclovir, CHILDREN, Herpesvirus 1, Human, DIAGNOSIS, Pediatrics, THERAPY, Antiviral Agents, DISEASE, Best Practice, CEREBROSPINAL-FLUID, Evidence Based Medicine, 1114 Paediatrics And Reproductive Medicine, Humans, Child, Science & Technology, Infant, Newborn, food and beverages, Infant, Infectious Diseases, Neurology, Female, Encephalitis, Herpes Simplex, Neonatology, Life Sciences & Biomedicine
Abstract

Herpes simplex encephalitis (HSE) is the most common single cause of viral encephalitis in infants and children. Treated or untreated, it can be associated with considerable morbidity and mortality, and its presentation is usually insidious and non-specific. Prompt and careful investigation is important in order to establish the diagnosis so that treatment can be optimised. We address some common questions arising when diagnosing and treating presumed HSE throughout childhood.

Published
2014

25. Role of human milk oligosaccharides in Group B Streptococcus colonisation

Author

Andreas, NJ, Al-Khalidi, A, Jaiteh, M, Clarke, E, Hyde, MJ, Modi, N, Holmes, E, Kampmann, B, Mehring Le Doare, K, Wellcome Trust, and Thrasher Research Fund

Subjects
reproductive and urinary physiology
Abstract

Group B Streptococcus (GBS) infection is a major cause of morbidity and mortality in infants. The major risk factor for GBS disease is maternal and subsequent infant colonisation. It is unknown whether human milk oligosaccharides (HMOs) protect against GBS colonisation. HMO production is genetically determined and linked to the Lewis antigen system. We aimed to investigate the association between HMOs and infant GBS colonisation between birth and postnatal day 90. Rectovaginal swabs were collected at delivery, as well as colostrum/breast milk, infant nasopharyngeal and rectal swabs at birth, 6 days and days 60-89 postpartum from 183 Gambian mother/infant pairs. GBS colonisation and serotypes were determined using culture and PCR. (1)H nuclear magnetic resonance spectroscopy was used to characterise the mother's Lewis status and HMO profile in breast milk. Mothers who were Lewis-positive were significantly less likely to be colonised by GBS (X (2)=12.50, P

Published
2016

26. Risk factors for Group B Streptococcus colonisation and disease in Gambian women and their infants

Author

Le Doare, K., Jarju, S., Darboe, S., Warburton, F., Gorringe, A., Heath, P.T., and Kampmann, B.

Subjects
Microbiology (medical), Group B Streptococcus, Vaccines, Infectious Diseases, Immunity, Neonatal infection
Abstract

OBJECTIVES: To determine risk factors for GBS colonisation in Gambian mothers and in their infants from birth to day 60-89 of age. METHODS: Swabs and breastmilk from mothers/infant pairs were collected and cultured on selective agar. Negative samples were analysed for GBS DNA via real-time PCR. Positive isolates were serotyped using multiplex PCR and gel-agarose electrophoresis. RESULTS: Seven hundred and fifty women/infant pairs were recruited. 253 women (33.7%) were GBS-colonised at delivery. The predominant serotypes were: V (55%), II (16%), III (10%), Ia (8%) and Ib (8%). 186 infants were colonised (24.8%) at birth, 181 (24.1%) at 6 days and 96 at day 60-89 (14%). Infants born before 34 weeks of gestation and to women with rectovaginal and breastmilk colonisation at delivery had increased odds of GBS colonisation at birth. Season of birth was associated with increased odds of persistent infant GBS colonisation (dry season vs. wet season AOR 2.9; 95% CI 1.6-5.2). CONCLUSION: GBS colonisation is common in Gambian women at delivery and in their infants to day 60-89 and is dominated by serotype V. In addition to maternal colonisation, breastmilk and season of birth are important risk factors for infant GBS colonisation.

Published
2016

27. Lack of evidence for the efficacy of enhanced surveillance compared to other specific interventions to control neonatal healthcare associated infection outbreaks

Author

Birt, J, Le Doare, K, Kortsalioudaki, C, Lawn, J, Heath, PT, and Sharland, M

Subjects
Cross Infection, Prevention, Outbreaks, Infant, Newborn, Neonates, Infant, Hospital-acquired infection, Disease Outbreaks, 1117 Public Health And Health Services, 1108 Medical Microbiology, Evidence-Based Practice, Intensive Care Units, Neonatal, Tropical Medicine, Humans, Systematic Review, Sentinel Surveillance, 0605 Microbiology
Abstract

BACKGROUND: Despite current prevention efforts, outbreaks of healthcare-associated infections in neonatal units remain high globally, with a considerable burden of mortality and morbidity. METHODS: We searched Medline, Cochrane Library and Outbreak database to identify studies of neonatal healthcare-associated outbreaks between 2005 and 2015 that described interventions to control outbreaks. All studies were evaluated using the ORION guidance. RESULTS: Thirty studies were identified including 17 102 infants of whom 664 (3.9%) became infected. No single intervention was identified that reduced duration or mortality. Studies that introduced multiple interventions had significantly reduced case fatality ratio and outbreak duration compared to those that used basic surveillance only. Low and low-middle income countries reported the fewest interventions to control outbreaks and these studies were also associated with higher mortality than that found in middle and high income countries. CONCLUSIONS: Systematic reporting and formal evaluation of interventions used to reduce healthcare-associated neonatal infection outbreaks is key to identifying containment strategies worldwide.

Published
2015

28. Systematic review and meta-analysis of the effectiveness and perinatal outcomes of COVID-19 vaccination in pregnancy

Author

Kalafat, Erkan (ORCID 0000-0003-0658-138X & YÖK ID 197389), Prasad, S., Blakeway, H., Townsend, R., O’Brien, P., Morris, E., Draycott, T., Thangaratinam, S., Le Doare, K., Ladhani, S., von Dadelszen, P., Magee, L.A., Heath, P., Khalil, A., and School of Medicine

Subjects
COVID-19, SARS-CoV-2 vaccine, Science and technology
Abstract

Safety and effectiveness of COVID-19 vaccines during pregnancy is a particular concern affecting vaccination uptake by this vulnerable group. Here we evaluated evidence from 23 studies including 117,552 COVID-19 vaccinated pregnant people, almost exclusively with mRNA vaccines. We show that the effectiveness of mRNA vaccination against RT-PCR confirmed SARS-CoV-2 infection 7 days after second dose was 89 center dot 5% (95% CI 69 center dot 0-96 center dot 4%, 18,828 vaccinated pregnant people, I-2 = 73 center dot 9%). The risk of stillbirth was significantly lower in the vaccinated cohort by 15% (pooled OR 0 center dot 85; 95% CI 0 center dot 73-0 center dot 99, 66,067 vaccinated vs. 424,624 unvaccinated, I-2 = 93 center dot 9%). There was no evidence of a higher risk of adverse outcomes including miscarriage, earlier gestation at birth, placental abruption, pulmonary embolism, postpartum haemorrhage, maternal death, intensive care unit admission, lower birthweight Z-score, or neonatal intensive care unit admission (p > 0.05 for all). COVID-19 mRNA vaccination in pregnancy appears to be safe and is associated with a reduction in stillbirth. Pregnant women have been disproportionately under-vaccinated against COVID-19, partly because they were excluded from initial trials. This systematic review and meta-analysis supports efficacy of vaccination in pregnancy, and finds no evidence of adverse maternal or perinatal outcomes., NA

Published
2022

29. Evaluation of immunogenicity and reactogenicity of COVID-19 vaccines in pregnant women

Author

H. Blakeway, Z. Amin‐Chowdhury, S. Prasad, E. Kalafat, M. Ismail, F. N. Abdallah, A. Rezvani, G. Amirthalingam, K. Brown, K. Le Doare, P. T. Heath, S. N. Ladhani, A. Khalil, Kalafat, Erkan (ORCID 0000-0003-0658-138X & YÖK ID 197389), Blakeway, H., Amin Chowdhury, Z., Prasad, S., İsmail, M., Abdallah, F.N., Rezvani, A., Amirthalingam, G., Brown, K., Le Doare, K., Heath, P.T., Ladhani, S.N., Khalil, A., and School of Medicine

Subjects
Vaccines, COVID-19 Vaccines, Radiological and Ultrasound Technology, SARS-CoV-2, Adverse event, Antibody, COVID-19, Immunogenicity, Maternal immunization, Pandemic, Pregnancy, Reactogenicity, Vaccine, Obstetrics and Gynecology, General Medicine, Cohort Studies, Acoustics, Obstetrics and gynecology, Radiology, Nuclear medicine, Medical imaging, Reproductive Medicine, Humans, Female, Radiology, Nuclear Medicine and imaging, Longitudinal Studies, RNA, Messenger
Abstract

Objective: severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection in pregnancy is associated with increased risk of adverse maternal and perinatal outcomes. Vaccines are highly effective at preventing severe coronavirus disease 2019 (COVID-19), but there are limited data on COVID-19 vaccines in pregnancy. This study aimed to investigate the reactogenicity and immunogenicity of COVID-19 vaccines in pregnant women when administered according to the 12-week-interval dosing schedule recommended in the UK. Methods: this was a cohort study of pregnant women receiving COVID-19 vaccination between April and September 2021. The outcomes were immunogenicity and reactogenicity after COVID-19 vaccination. Pregnant women were recruited by phone, e-mail and/or text and were vaccinated according to vaccine availability at their local vaccination center. For immunogenicity assessment, blood samples were taken at specific timepoints after each dose to evaluate nucleocapsid protein (N) and spike protein (S) antibody titers. The comparator group comprised non-pregnant female healthcare workers in the same age group who were vaccinated as part of the national immunization program in a contemporaneous longitudinal cohort study. Longitudinal changes in serum antibody titers and association with pregnancy status were assessed using a two-step regression approach. Reactogenicity assessment in pregnant women was undertaken using an online questionnaire. The comparator group comprised non-pregnant women aged 18–49 years who had received two vaccine doses in primary care. The association of pregnancy status with reactogenicity was assessed using logistic regression analysis. Results: overall, 67 pregnant women, of whom 66 had received a mRNA vaccine, and 79 non-pregnant women, of whom 50 had received a mRNA vaccine, were included in the immunogenicity study. Most (61.2%) pregnant women received their first vaccine dose in the third trimester, while 3.0% received it in the first trimester and 35.8% in the second trimester. SARS-CoV-2 S-antibody geometric mean concentrations after mRNA vaccination were not significantly different at 2–6 weeks after the first dose but were significantly lower at 2–6 weeks after the second dose in infection-naïve pregnant compared with non-pregnant women. In pregnant women, prior infection was associated with higher antibody levels at 2–6 weeks after the second vaccine dose. Reactogenicity analysis included 108 pregnant women and 116 non-pregnant women. After the first dose, tiredness and chills were reported less commonly in pregnant compared with non-pregnant women (P = 0.043 and P = 0.029, respectively). After the second dose, feeling generally unwell was reported less commonly (P = 0.046) in pregnant compared with non-pregnant women. Conclusions: using an extended 12-week interval between vaccine doses, antibody responses after two doses of mRNA COVID-19 vaccine were found to be lower in pregnant compared with non-pregnant women. Strong antibody responses were achieved after one dose in previously infected women, regardless of pregnancy status. Pregnant women reported fewer adverse events after both the first and second dose of vaccine. These findings should now be addressed in larger controlled studies., NA

Published
2022

30. COVID-19 Vaccination During Pregnancy: Coverage and Safety

Author

Arezou Rezvani, Kirsty Le Doare, Pat O'Brien, Shamez N Ladhani, Helena Blakeway, Erkan Kalafat, Asma Khalil, Laura A. Magee, Paul T. Heath, Smriti Prasad, Peter von Dadelszen, Kalafat, Erkan (ORCID 0000-0003-0658-138X & YÖK ID 197389), Blakeway, H., Prasad, S., Heath, P.T., Ladhani, S.N., Le Doare, K., Magee, L.A., O'brien, P., Rezvani, A., Dadelszen, P.V., Khalil A., and School of Medicine

Subjects
Neonatal intensive care unit, Vaccination Coverage, Social Determinants of Health, coverage, Management of Technology and Innovation, Ethnicity, Pregnancy Complications, Infectious, Coverage, COVID-19, Immunization, mRNA, Pregnancy, Safety vaccine uptake, SARS-CoV-2, Vaccination, Viral vector, Obstetrics, Original Research: Obstetrics, viral vector, Age Factors, Obstetrics and Gynecology, Gestational age, Stillbirth, Intensive Care Units, Caribbean Region, vaccine uptake, Obstetrics and gynecology, Infant, Small for Gestational Age, Gestation, Premature Birth, Female, Social Deprivation, pregnancy, Cohort study, 2019-nCoV Vaccine mRNA-1273, Adult, safety, medicine.medical_specialty, COVID-19 Vaccines, Fever, Black People, immunization, Congenital Abnormalities, Asian People, ChAdOx1 nCoV-19, Intensive Care Units, Neonatal, medicine, Humans, Propensity Score, BNT162 Vaccine, Proportional Hazards Models, business.industry, Cesarean Section, Postpartum Hemorrhage, Odds ratio, medicine.disease, vaccination, United Kingdom, Obstetric Labor Complications, Logistic Models, Case-Control Studies, Small for gestational age, business
Abstract

Background: concerns have been raised regarding a potential surge of COVID-19 in pregnancy, secondary to the rising numbers of COVID-19 in the community, easing of societal restrictions, and vaccine hesitancy. Although COVID-19 vaccination is now offered to all pregnant women in the United Kingdom; limited data exist on its uptake and safety. Objective: this study aimed to investigate the uptake and safety of COVID-19 vaccination among pregnant women. Study design: this was a cohort study of pregnant women who gave birth at St George's University Hospitals National Health Service Foundation Trust, London, United Kingdom, between March 1, 2020, and July 4, 2021. The primary outcome was uptake of COVID-19 vaccination and its determinants. The secondary outcomes were perinatal safety outcomes. Data were collected on COVID-19 vaccination uptake, vaccination type, gestational age at vaccination, and maternal characteristics, including age, parity, ethnicity, index of multiple deprivation score, and comorbidities. Further data were collected on perinatal outcomes, including stillbirth (fetal death at ?24 weeks’ gestation), preterm birth, fetal and congenital abnormalities, and intrapartum complications. Pregnancy and neonatal outcomes of women who received the vaccine were compared with that of a matched cohort of women with balanced propensity scores. Effect magnitudes of vaccination on perinatal outcomes were reported as mean differences or odds ratios with 95% confidence intervals. Factors associated with antenatal vaccination were assessed with logistic regression analysis. Results: Data were available for 1328 pregnant women of whom 140 received at least 1 dose of the COVID-19 vaccine before giving birth and 1188 women who did not; 85.7% of those vaccinated received their vaccine in the third trimester of pregnancy and 14.3% in the second trimester of pregnancy. Of those vaccinated, 127 (90.7%) received a messenger RNA vaccine and 13 (9.3%) a viral vector vaccine. There was evidence of reduced vaccine uptake in younger women (P=.001), women with high levels of deprivation (ie, fifth quintile of the index of multiple deprivation; P=.008), and women of Afro-Caribbean or Asian ethnicity compared with women of White ethnicity (P[removed].05 for all): stillbirth (0.0% vs 0.2%), fetal abnormalities (2.2% vs 2.5%), postpartum hemorrhage (9.8% vs 9.0%), cesarean delivery (30.8% vs 34.1%), small for gestational age (12.0% vs 12.8%), maternal high-dependency unit or intensive care admission (6.0% vs 4.0%), or neonatal intensive care unit admission (5.3% vs 5.0%). Intrapartum pyrexia (3.7% vs 1.0%; P=.046) was significantly increased but the borderline statistical significance was lost after excluding women with antenatal COVID-19 infection (P=.079). Mixed-effects Cox regression showed that vaccination was not significantly associated with birth at, NA

Published
2021

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