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2. Nasopharyngeal carriage of pneumococcus in children in England up to ten years after PCV13 introduction: persistence of serotypes 3 and 19A and emergence of 7C

Author

Tiley, KS, Ratcliffe, H, Voysey, M, Jefferies, K, Sinclair, G, Carr, M, Colin-Jones, R, Smith, D, Bowman, J, Hart, T, Kandasamy, R, Hinds, J, Gould, K, Berbers, G, Tcherniaeva, I, Robinson, H, Plested, E, Aley, P, and Snape, MD

Subjects
IPD, conjugate, nasopharyngeal, vaccine, Pneumococcal, serotype, invasive, PCV, carriage
Abstract

BACKGROUND: Monitoring changes in pharyngeal carriage of pneumococcus in children following 13-valent pneumococcal conjugate vaccine (PCV13) introduction in the UK in 2010 informs understanding of patterns of invasive pneumococcal disease (IPD) incidence. METHODS: Nasopharyngeal swabs from healthy children vaccinated with PCV13 according to schedule (2, 4, 12 months) were cultured and serotyped. Results for children aged 13-48 months were compared between 2014/15 and 2017/19, and with children aged 6-12 months (2017/20). Blood was obtained from a subset of children for pneumococcal serotype-specific IgG. RESULTS: Total pneumococcal carriage at 13-48 months was 47.9% (473/988) in 2014/15 and 51.8% (412/795) in 2017/19 (p = 0.10); at age 6-12 months this value was 44.6% (274/615). In 2017/19, 2.9% (95% CI 1.8-4.3%) of children aged 13-48 months carried PCV13 serotypes (mainly 3 (1.5%) and 19A (0.8%)) and over 20% carried the additional PCV20 serotypes. Similar proportions of children had IgG ≥0.35 IU/mL for each serotype in 2014/15 and 2017/19.Serotype 7C carriage increased significantly (p

Published
2022

3. Community seroprevalence of SARS-CoV-2 in children and adolescents in England, 2019–2021

Author

Ratcliffe, Helen, primary, Tiley, K S, additional, Andrews, Nick, additional, Amirthalingam, Gayatri, additional, Vichos, I, additional, Morey, E, additional, Douglas, N L, additional, Marinou, S, additional, Plested, Emma, additional, Aley, Parvinder, additional, Galiza, Eva P, additional, Faust, Saul N, additional, Hughes, S, additional, Murray, Clare S, additional, Roderick, Marion, additional, Shackley, Fiona, additional, Oddie, Sam J, additional, Lees, Tim, additional, Turner, D P J, additional, Raman, M, additional, Owens, Stephen, additional, Turner, Paul, additional, Cockerill, H, additional, Lopez Bernal, J, additional, Linley, E, additional, Borrow, Ray, additional, Brown, Kevin, additional, Ramsay, Mary Elizabeth, additional, Voysey, M, additional, and Snape, Matthew D, additional

Published
2022
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4. COVID-19 vaccine effectiveness and variants in Nepal: study protocol for a test-negative case–control study with SARS-CoV-2 genetic sequencing

Author

Bijukchhe, SM, O'Reilly, PJ, Theiss-Nyland, K, Gurung, M, Pokhrel, B, Kelly, S, Acharya, S, Maharjan, S, Shrestha, A, Pandey, B, Lama, M, Shrestha, I, Voysey, M, Eordogh, A, Shrestha, S, Feng, ES, Li, G, Shah, G, and Pollard, AJ

Subjects
General Medicine
Abstract

IntroductionInactivated, viral vector and mRNA vaccines have been used in the Nepali COVID-19 vaccination programme but there is little evidence on the effectiveness of these vaccines in this setting. The aim of this study is to describe COVID-19 vaccine effectiveness in Nepal and provide information on infections with SARS-CoV-2 variants.Methods and analysisThis is a hospital-based, prospective test-negative case–control study conducted at Patan Hospital, Kathmandu. All patients >18 years of age presenting to Patan Hospital with COVID-19-like symptoms who have received a COVID-19 antigen/PCR test are eligible for inclusion. The primary outcome is vaccine effectiveness of licensed COVID-19 vaccines against laboratory-confirmed COVID-19 disease.After enrolment, information will be collected on vaccine status, date of vaccination, type of vaccine, demographics and other medical comorbidities. The primary outcome of interest is laboratory-confirmed SARS-CoV-2 infection. Cases (positive for SARS-CoV-2) and controls (negative for SARS-CoV-2) will be enrolled in a 1:4 ratio. Vaccine effectiveness against COVID-19 disease will be analysed by comparing vaccination status with SARS-CoV-2 test results.Positive SARS-CoV-2 samples will be sequenced to identify circulating variants and estimate vaccine effectiveness against common variants.Measuring vaccine effectiveness and identifying SARS-CoV-2 variants in Nepal will help to inform public health efforts. Describing disease severity in relation to specific SARS-CoV-2 variants and vaccine status will also inform future prevention and care efforts.Ethics and disseminationEthical approval was obtained from the University of Oxford Tropical Ethics Committee (OxTREC) (ref: 561-21) and the Patan Academy of Health Sciences Institutional Review Board (ref: drs2111121578). The protocol and supporting study documents were approved for use by the Nepal Health Research Council (NHRC 550-2021). Results will be disseminated in peer-reviewed journals and to the public health authorities in Nepal.

Published
2023

5. AZD1222/ChAdOx1 nCoV-19 vaccination induces a polyfunctional spike protein-specific Th1 response with a diverse TCR repertoire

Author

Swanson, PA, Padilla, M, Hoyland, W, McGlinchey, K, Fields, PA, Bibi, S, Faust, SN, McDermott, AB, Lambe, T, Pollard, AJ, Durham, NM, Kelly, EJ, AstraZeneca/Oxford/VRC Study Group, Adlou, S, Aley, PK, Angus, B, Anslow, R, Baker, P, Bansal, H, Beveridge, A, Bridges-Webb, A, Ching, S, Cicconi, P, Clutterbuck, EA, Collins, AM, Darton, TC, Demissie, T, Dinesh, T, Douglas, AD, Duncan, CJA, Ewer, KJ, Felle, S, Ferreira, DM, Folegatti, PM, Fuskova, M, Gaudinski, M, Gilbert, SC, Goodman, AL, Gordon, I, Green, CA, Harbolick, E, Hayes, S, Hill, AVS, Hill, H, Jenkin, D, Jepson, BM, Kasanyinga, M, Libri, V, Lillie, PJ, McGregor, AC, Minassian, AM, Mujadidi, YF, Novik, L, Payne, R, Pilataxi, F, Plested, E, Provstgaard-Morys, S, Ramasamy, M, Robinson, H, Sanders, K, Smith, A, Snape, MD, Song, R, Sutherland, RK, Thomson, EC, Toshner, M, Turner, DPJ, Voysey, M, Widge, AT, and Williams, CJ

Abstract

AZD1222 (ChAdOx1 nCoV-19), a replication-deficient simian adenovirus-vectored vaccine, has demonstrated safety, efficacy, and immunogenicity against coronavirus disease 2019 (COVID-19) in clinical trials and real-world studies. We characterized CD4+ and CD8+ T cell responses induced by AZD1222 vaccination in peripheral blood mononuclear cells (PBMCs) from 296 unique vaccine recipients aged 18 to 85 years who enrolled in the phase 2/3 COV002 trial. Total spike protein-specific CD4+ T cell helper type 1 (Th1) and CD8+ T cell responses were increased in AZD1222-vaccinated adults of all ages following two doses of AZD1222. CD4+ Th2 responses following AZD1222 vaccination were not detected. Furthermore, AZD1222-specific Th1 and CD8+ T cells both displayed a high degree of polyfunctionality in all adult age groups. T cell receptor (TCR) β sequences from vaccinated participants mapped against TCR sequences known to react to SARS-CoV-2 revealed substantial breadth and depth across the SARS-CoV-2 spike protein for both AZD1222-induced CD4+ and CD8+ T cell responses. Overall, AZD1222 vaccination induced a polyfunctional Th1-dominated T cell response, with broad CD4+ and CD8+ T cell coverage across the SARS-CoV-2 spike protein.

Published
2021

6. Correlates of protection against symptomatic and asymptomatic SARS-CoV-2 infection

Author

Feng, S, Phillips, DJ, White, T, Sayal, H, Aley, PK, Bibi, S, Dold, C, Fuskova, M, Gilbert, SC, Hirsch, I, Humphries, HE, Jepson, B, Kelly, EJ, Plested, E, Shoemaker, K, Thomas, KM, Vekemans, J, Villafana, TL, Lambe, T, Pollard, AJ, Voysey, M, Adlou, S, Allen, L, Angus, B, Anslow, R, Asselin, M-C, Baker, N, Baker, P, Barlow, T, Beveridge, A, Bewley, KR, Brown, P, Brunt, E, Buttigieg, KR, Camara, S, Charlton, S, Chiplin, E, Cicconi, P, Clutterbuck, EA, Collins, AM, Coombes, NS, Clemens, SAC, Davison, M, Demissie, T, Dinesh, T, Douglas, AD, Duncan, CJA, Emary, KRW, Ewer, KJ, Felle, S, Ferreira, DM, Finn, A, Folegatti, PM, Fothergill, R, Fraser, S, Garlant, H, Gatcombe, L, Godwin, KJ, Goodman, AL, Green, CA, Hallis, B, Hart, TC, Heath, PT, Hill, H, Hill, AVS, Jenkin, D, Kasanyinga, M, Kerridge, S, Knight, C, Leung, S, Libri, V, Lillie, PJ, Marinou, S, McGlashan, J, McGregor, AC, McInroy, L, Minassian, AM, Mujadidi, YF, Penn, EJ, Petropoulos, CJ, Pollock, KM, Proud, PC, Provstgaard-Morys, S, Rajapaska, D, Ramasamy, MN, Sanders, K, Shaik, I, Singh, N, Smith, A, Snape, MD, Song, R, Shrestha, S, Sutherland, RK, Thomson, EC, Turner, DPJ, Webb-Bridges, A, Wrin, T, Williams, CJ, and Group, Oxford COVID Vaccine Trial

Subjects
Male, Antibodies, Viral, Neutralization, Cohort Studies, Multiplex, Asymptomatic Infections, 11 Medical and Health Sciences, Aged, 80 and over, Vaccines, biology, medicine.diagnostic_test, Vaccination, General Medicine, Middle Aged, Titer, Treatment Outcome, Infectious diseases, Female, Antibody, medicine.symptom, Adult, medicine.medical_specialty, COVID-19 Vaccines, Coronavirus disease 2019 (COVID-19), Adolescent, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Immunology, Immunization, Secondary, Asymptomatic, General Biochemistry, Genetics and Molecular Biology, World health, Article, Young Adult, Immune system, Statistical significance, Internal medicine, medicine, Humans, Aged, Infection Control, business.industry, SARS-CoV-2, Patient Acuity, COVID-19, Vaccine efficacy, Antibodies, Neutralizing, United Kingdom, Immunity, Humoral, Immunoassay, biology.protein, business
Abstract

The global supply of COVID-19 vaccines remains limited. An understanding of the immune response that is predictive of protection could facilitate rapid licensure of new vaccines. Data from a randomized efficacy trial of the ChAdOx1 nCoV-19 (AZD1222) vaccine in the United Kingdom was analyzed to determine the antibody levels associated with protection against SARS-CoV-2. Binding and neutralizing antibodies at 28 days after the second dose were measured in infected and noninfected vaccine recipients. Higher levels of all immune markers were correlated with a reduced risk of symptomatic infection. A vaccine efficacy of 80% against symptomatic infection with majority Alpha (B.1.1.7) variant of SARS-CoV-2 was achieved with 264 (95% CI: 108, 806) binding antibody units (BAU)/ml: and 506 (95% CI: 135, not computed (beyond data range) (NC)) BAU/ml for anti-spike and anti-RBD antibodies, and 26 (95% CI: NC, NC) international unit (IU)/ml and 247 (95% CI: 101, NC) normalized neutralization titers (NF50) for pseudovirus and live-virus neutralization, respectively. Immune markers were not correlated with asymptomatic infections at the 5% significance level. These data can be used to bridge to new populations using validated assays, and allow extrapolation of efficacy estimates to new COVID-19 vaccines., Defined levels of SARS-CoV-2-specific binding and neutralizing antibodies elicited by the COVID-19 vaccine ChAdOx1 nCoV-19 are identified as correlates of protection against symptomatic infection.

Published
2021

8. Burden of enteric fever at three urban sites in Africa and Asia: a multicentre population-based study

Author

Meiring, JE, Shakya, M, Khanam, F, Voysey, M, Phillips, MT, Tonks, S, Thindwa, D, Darton, TC, Dongol, S, Karkey, A, Zaman, K, Baker, S, Dolecek, C, Dunstan, SJ, Dougan, G, Holt, KE, Heyderman, RS, Qadri, F, Pitzer, VE, Basnyat, B, Gordon, MA, Clemens, J, Pollard, AJ, Meiring, JE, Shakya, M, Khanam, F, Voysey, M, Phillips, MT, Tonks, S, Thindwa, D, Darton, TC, Dongol, S, Karkey, A, Zaman, K, Baker, S, Dolecek, C, Dunstan, SJ, Dougan, G, Holt, KE, Heyderman, RS, Qadri, F, Pitzer, VE, Basnyat, B, Gordon, MA, Clemens, J, and Pollard, AJ

Abstract

BACKGROUND: Enteric fever is a serious public health concern in many low-income and middle-income countries. Numerous data gaps exist concerning the epidemiology of Salmonella enterica serotype Typhi (S Typhi) and Salmonella enterica serotype Paratyphi (S Paratyphi), which are the causative agents of enteric fever. We aimed to determine the burden of enteric fever in three urban sites in Africa and Asia. METHODS: In this multicentre population-based study, we did a demographic census at three urban sites in Africa (Blantyre, Malawi) and Asia (Kathmandu, Nepal and Dhaka, Bangladesh) between June 1, 2016, and Sept 25, 2018. Households were selected randomly from the demographic census. Participants from within the geographical census area presenting to study health-care facilities were approached for recruitment if they had a history of fever for 72 h or more (later changed to >48 h) or temperature of 38·0°C or higher. Facility-based passive surveillance was done between Nov 11, 2016, and Dec 31, 2018, with blood-culture collection for febrile illness. We also did a community-based serological survey to obtain data on Vi-antibody defined infections. We calculated crude incidence for blood-culture-confirmed S Typhi and S Paratyphi infection, and calculated adjusted incidence and seroincidence of S Typhi blood-culture-confirmed infection. FINDINGS: 423 618 individuals were included in the demographic census, contributing 626 219 person-years of observation for febrile illness surveillance. 624 S Typhi and 108 S Paratyphi A isolates were collected from the blood of 12 082 febrile patients. Multidrug resistance was observed in 44% S Typhi isolates and fluoroquinolone resistance in 61% of S Typhi isolates. In Blantyre, the overall crude incidence of blood-culture confirmed S Typhi was 58 cases per 100 000 person-years of observation (95% CI 48-70); the adjusted incidence was 444 cases per 100 000 person-years of observation (95% credible interval [CrI] 347-717). The corres

Published
2021

9. A Bayesian approach for estimating typhoid fever incidence from large-scale facility-based passive surveillance data

Author

Phillips, MT, Meiring, JE, Voysey, M, Warren, JL, Baker, S, Basnyat, B, Clemens, JD, Dolecek, C, Dunstan, SJ, Dougan, G, Gordon, MA, Thindwa, D, Heyderman, RS, Holt, KE, Qadri, F, Pollard, AJ, Pitzer, VE, Phillips, MT, Meiring, JE, Voysey, M, Warren, JL, Baker, S, Basnyat, B, Clemens, JD, Dolecek, C, Dunstan, SJ, Dougan, G, Gordon, MA, Thindwa, D, Heyderman, RS, Holt, KE, Qadri, F, Pollard, AJ, and Pitzer, VE

Abstract

Decisions about typhoid fever prevention and control are based on estimates of typhoid incidence and their uncertainty. Lack of specific clinical diagnostic criteria, poorly sensitive diagnostic tests, and scarcity of accurate and complete datasets contribute to difficulties in calculating age-specific population-level typhoid incidence. Using data from the Strategic Typhoid Alliance across Africa and Asia program, we integrated demographic censuses, healthcare utilization surveys, facility-based surveillance, and serological surveillance from Malawi, Nepal, and Bangladesh to account for under-detection of cases. We developed a Bayesian approach that adjusts the count of reported blood-culture-positive cases for blood culture detection, blood culture collection, and healthcare seeking-and how these factors vary by age-while combining information from prior published studies. We validated the model using simulated data. The ratio of observed to adjusted incidence rates was 7.7 (95% credible interval [CrI]: 6.0-12.4) in Malawi, 14.4 (95% CrI: 9.3-24.9) in Nepal, and 7.0 (95% CrI: 5.6-9.2) in Bangladesh. The probability of blood culture collection led to the largest adjustment in Malawi, while the probability of seeking healthcare contributed the most in Nepal and Bangladesh; adjustment factors varied by age. Adjusted incidence rates were within or below the seroincidence rate limits of typhoid infection. Estimates of blood-culture-confirmed typhoid fever without these adjustments results in considerable underestimation of the true incidence of typhoid fever. Our approach allows each phase of the reporting process to be synthesized to estimate the adjusted incidence of typhoid fever while correctly characterizing uncertainty, which can inform decision-making for typhoid prevention and control.

Published
2021

10. Tracking science : An alternative for those excluded by citizen science

Author

Liebenberg, L., Ao, A., Lombard, M., Shermer, M., Xhukwe, U., Biesele, M., Xao, D., Carruthers, P., Kxao, O., Hansson, Sven Ove, Langwane, H., Elbroch, L. M., Ui, N., Keeping, D., Humphrey, G., Newman, G., Gaq'o, U., Steventon, J., Kashe, N., Stevenson, R., Benadie, K., du Plessis, P., Minye, J., Kxunta, U., Ludwig, B., Daqm, O., Louw, M., Debe, D., Voysey, M., Liebenberg, L., Ao, A., Lombard, M., Shermer, M., Xhukwe, U., Biesele, M., Xao, D., Carruthers, P., Kxao, O., Hansson, Sven Ove, Langwane, H., Elbroch, L. M., Ui, N., Keeping, D., Humphrey, G., Newman, G., Gaq'o, U., Steventon, J., Kashe, N., Stevenson, R., Benadie, K., du Plessis, P., Minye, J., Kxunta, U., Ludwig, B., Daqm, O., Louw, M., Debe, D., and Voysey, M.

Abstract

In response to recent discussion about terminology, we propose "tracking science" as a term that is more inclusive than citizen science. Our suggestion is set against a post-colonial political background and large-scale migrations, in which "citizen" is becoming an increasingly contentious term. As a diverse group of authors from several continents, our priority is to deliberate a term that is all-inclusive, so that it could be adopted by everyone who participates in science or contributes to scientific knowledge, regardless of socio-cultural background. For example, current citizen science terms used for Indigenous knowledge imply that such practitioners belong to a sub-group that is other, and therefore marginalized. Our definition for "tracking science" does not exclude Indigenous peoples and their knowledge contributions and may provide a space for those who currently participate in citizen science, but want to contribute, explore, and/or operate beyond its confinements. Our suggestion is not that of an immediate or complete replacement of terminology, but that the notion of tracking science can be used to complement the practice and discussion of citizen science where it is contextually appropriate or needed. This may provide a breathing space, not only to explore alternative terms, but also to engage in robust, inclusive discussion on what it means to do science or create scientific knowledge. In our view, tracking science serves as a metaphor that applies broadly to the scientific community-from modern theoretical physics to ancient Indigenous knowledge., QC 20220216

Published
2021
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11. Community seroprevalence of SARS-CoV-2 in children and adolescents in England, 2019–2021

Author

Ratcliffe, Helen, Tiley, K S, Andrews, Nick, Amirthalingam, Gayatri, Vichos, I, Morey, E, Douglas, N L, Marinou, S, Plested, Emma, Aley, Parvinder, Galiza, Eva P, Faust, Saul N, Hughes, S, Murray, Clare S, Roderick, Marion, Shackley, Fiona, Oddie, Sam J, Lees, Tim, Turner, D P J, Raman, M, Owens, Stephen, Turner, Paul, Cockerill, H, Lopez Bernal, J, Linley, E, Borrow, Ray, Brown, Kevin, Ramsay, Mary Elizabeth, Voysey, M, and Snape, Matthew D

Abstract

ObjectiveTo understand community seroprevalence of SARS-CoV-2 in children and adolescents. This is vital to understanding the susceptibility of this cohort to COVID-19 and to inform public health policy for disease control such as immunisation.DesignWe conducted a community-based cross-sectional seroprevalence study in participants aged 0–18 years old recruiting from seven regions in England between October 2019 and June 2021 and collecting extensive demographic and symptom data. Serum samples were tested for antibodies against SARS-CoV-2 spike and nucleocapsid proteins using Roche assays processed at UK Health Security Agency laboratories. Prevalence estimates were calculated for six time periods and were standardised by age group, ethnicity and National Health Service region.ResultsPost-first wave (June–August 2020), the (anti-spike IgG) adjusted seroprevalence was 5.2%, varying from 0.9% (participants 10–14 years old) to 9.5% (participants 5–9 years old). By April–June 2021, this had increased to 19.9%, varying from 13.9% (participants 0–4 years old) to 32.7% (participants 15–18 years old). Minority ethnic groups had higher risk of SARS-CoV-2 seropositivity than white participants (OR 1.4, 95% CI 1.0 to 2.0), after adjusting for sex, age, region, time period, deprivation and urban/rural geography. In children <10 years, there were no symptoms or symptom clusters that reliably predicted seropositivity. Overall, 48% of seropositive participants with complete questionnaire data recalled no symptoms between February 2020 and their study visit.ConclusionsApproximately one-third of participants aged 15–18 years old had evidence of antibodies against SARS-CoV-2 prior to the introduction of widespread vaccination. These data demonstrate that ethnic background is independently associated with risk of SARS-CoV-2 infection in children.Trial registration numberNCT04061382.

Published
2023
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13. Persistent circulation of vaccine serotypes and serotype replacement after 5 years of infant immunization with 13-valent pneumococcal conjugate vaccine in the United Kingdom

Author

Kandasamy, R, Voysey, M, Collins, S, Berbers, G, Robinson, H, Noel, I, Hughes, H, Ndimah, S, Gould, K, Fry, N, Sheppard, C, Ladhani, S, Snape, MD, Hinds, J, Pollard, AJ, Kandasamy, R, Voysey, M, Collins, S, Berbers, G, Robinson, H, Noel, I, Hughes, H, Ndimah, S, Gould, K, Fry, N, Sheppard, C, Ladhani, S, Snape, MD, Hinds, J, and Pollard, AJ

Abstract

Background: Following programmatic introduction of the 13-valent pneumococcal conjugate vaccine (PCV13), there is residual carriage and disease due to PCV13-covered serotypes. Methods. PCV13-immunized children aged 13-48 months, N = 988, were enrolled between February 2014 and August 2015 (“late PCV13”), and had nasopharyngeal pneumococcal carriage compared with 7-valent pneumococcal conjugate vaccine (PCV7) immunized children, N = 567, enrolled between November 2010 and September 2011 (“early PCV13”). Nasopharyngeal pneumococci were molecularserotyped by microarray. Invasive pneumococcal disease (IPD) cases were identified through enhanced national surveillance. Results. Compared with PCV7-immunized children, carriage among PCV13-immunized children was significantly lower for serotypes 19A (odds ratio [OR], 0.08 [95% confidence interval {CI},.02-.25]), 6C (OR, 0.11 [95% CI,.03-.32]), and 7F (8 vs 0 cases). IPD incidence in children <5 years was significantly lower for serotypes 1 (incidence rate ratio [IRR], 0.03 [95% CI, 0-.19]) and 7F (IRR, 0.13 [95% CI,.05-.36]) but not 19A (IRR, 0.6 [95% CI,.3-1.12]) or serotype 3 (IRR, 2.3 [95% CI,.86-6.15]) in the late PCV13 period than in the early PCV13 period. The most significant rises in IPD incidence were for serotypes 8, 12F, and 24F. Conclusions. PCV13 has reduced serotype 19A carriage among vaccinated children. We found no impact of PCV13 on serotype 3 carriage or disease, and emergence of non-PCV13-serotype disease.

Published
2020

14. Assessment of an Antibody-in-Lymphocyte Supernatant Assay for the Etiological Diagnosis of Pneumococcal Pneumonia in Children

Author

Carter, MJ, Gurung, P, Jones, C, Rajkarnikar, S, Kandasamy, R, Gurung, M, Thorson, S, Gautam, MC, Prajapati, KG, Khadka, B, Maharjan, A, Knight, JC, Murdoch, DR, Darton, TC, Voysey, M, Wahl, B, O'Brien, KL, Kelly, S, Ansari, I, Shah, G, Ekström, N, Melin, M, Pollard, AJ, Kelly, DF, Shrestha, S, Carter, MJ, Gurung, P, Jones, C, Rajkarnikar, S, Kandasamy, R, Gurung, M, Thorson, S, Gautam, MC, Prajapati, KG, Khadka, B, Maharjan, A, Knight, JC, Murdoch, DR, Darton, TC, Voysey, M, Wahl, B, O'Brien, KL, Kelly, S, Ansari, I, Shah, G, Ekström, N, Melin, M, Pollard, AJ, Kelly, DF, and Shrestha, S

Abstract

New diagnostic tests for the etiology of childhood pneumonia are needed. We evaluated the antibody-in-lymphocyte supernatant (ALS) assay to detect immunoglobulin (Ig) G secretion from ex vivo peripheral blood mononuclear cell (PBMC) culture, as a potential diagnostic test for pneumococcal pneumonia. We enrolled 348 children with pneumonia admitted to Patan Hospital, Kathmandu, Nepal between December 2015 and September 2016. PBMCs sampled from participants were incubated for 48 h before harvesting of cell culture supernatant (ALS). We used a fluorescence-based multiplexed immunoassay to measure the concentration of IgG in ALS against five conserved pneumococcal protein antigens. Of children with pneumonia, 68 had a confirmed etiological diagnosis: 12 children had pneumococcal pneumonia (defined as blood or pleural fluid culture-confirmed; or plasma CRP concentration ≥60 mg/l and nasopharyngeal carriage of serotype 1 pneumococci), and 56 children had non-pneumococcal pneumonia. Children with non-pneumococcal pneumonia had either a bacterial pathogen isolated from blood (six children); or C-reactive protein <60 mg/l, absence of radiographic consolidation and detection of a pathogenic virus by multiplex PCR (respiratory syncytial virus, influenza viruses, or parainfluenza viruses; 23 children). Concentrations of ALS IgG to all five pneumococcal proteins were significantly higher in children with pneumococcal pneumonia than in children with non-pneumococcal pneumonia. The concentration of IgG in ALS to the best-performing antigen discriminated between children with pneumococcal and non-pneumococcal pneumonia with a sensitivity of 1.0 (95% CI 0.73–1.0), specificity of 0.66 (95% CI 0.52–0.78) and area under the receiver-operating characteristic curve (AUROCC) 0.85 (95% CI 0.75–0.94). Children with pneumococcal pneumonia were older than children with non-pneumococcal pneumonia (median 5.6 and 2.0 years, respectively, p < 0.001). When the analysis was limited to children ≥2

Published
2020

15. The surveillance for enteric fever in Asia project (SEAP), severe typhoid fever surveillance in Africa (SETA), surveillance of enteric fever in India (SEFI), and strategic typhoid alliance across Africa and Asia (STRATAA) population-based enteric fever studies: A review of methodological similarities and differences

Author

Carey, ME, MacWright, WR, Im, J, Meiring, JE, Gibani, MM, Park, SE, Longley, A, Jeon, HJ, Hemlock, C, Yu, AT, Soura, A, Aiemjoy, K, Owusu-Dabo, E, Terferi, M, Islam, S, Lunguya, O, Jacobs, J, Gordon, M, Dolecek, C, Baker, S, Pitzer, VE, Yousafzai, MT, Tonks, S, Clemens, JD, Date, K, Qadri, F, Heyderman, RS, Saha, SK, Basnyat, B, Okeke, IN, Qamar, FN, Voysey, M, Luby, S, Kang, G, Andrews, J, Pollard, AJ, John, J, Garrett, D, Marks, F, Carey, ME, MacWright, WR, Im, J, Meiring, JE, Gibani, MM, Park, SE, Longley, A, Jeon, HJ, Hemlock, C, Yu, AT, Soura, A, Aiemjoy, K, Owusu-Dabo, E, Terferi, M, Islam, S, Lunguya, O, Jacobs, J, Gordon, M, Dolecek, C, Baker, S, Pitzer, VE, Yousafzai, MT, Tonks, S, Clemens, JD, Date, K, Qadri, F, Heyderman, RS, Saha, SK, Basnyat, B, Okeke, IN, Qamar, FN, Voysey, M, Luby, S, Kang, G, Andrews, J, Pollard, AJ, John, J, Garrett, D, and Marks, F

Abstract

Building on previous multicountry surveillance studies of typhoid and others salmonelloses such as the Diseases of the Most Impoverished program and the Typhoid Surveillance in Africa Project, several ongoing blood culture surveillance studies are generating important data about incidence, severity, transmission, and clinical features of invasive Salmonella infections in sub-Saharan Africa and South Asia. These studies are also characterizing drug resistance patterns in their respective study sites. Each study answers a different set of research questions and employs slightly different methodologies, and the geographies under surveillance differ in size, population density, physician practices, access to healthcare facilities, and access to microbiologically safe water and improved sanitation. These differences in part reflect the heterogeneity of the epidemiology of invasive salmonellosis globally, and thus enable generation of data that are useful to policymakers in decision-making for the introduction of typhoid conjugate vaccines (TCVs). Moreover, each study is evaluating the large-scale deployment of TCVs, and may ultimately be used to assess post-introduction vaccine impact. The data generated by these studies will also be used to refine global disease burden estimates. It is important to ensure that lessons learned from these studies not only inform vaccination policy, but also are incorporated into sustainable, low-cost, integrated vaccine-preventable disease surveillance systems.

Published
2020

16. Phase 3 Efficacy Analysis of a Typhoid Conjugate Vaccine Trial in Nepal

Author

Shakya, M, Colin-Jones, R, Theiss-Nyland, K, Voysey, M, Pant, D, Smith, N, Liu, X, Tonks, S, Mazur, O, Farooq, YG, Clarke, J, Hill, J, Adhikari, A, Dongol, S, Karkey, A, Bajracharya, B, Kelly, S, Gurung, M, Baker, S, Neuzil, KM, Shrestha, S, Basnyat, B, Pollard, AJ, and Team, Tyvac Nepal Study

Subjects
Male, medicine.medical_specialty, Adolescent, Endemic Diseases, MEDLINE, Meningococcal Vaccines, Kaplan-Meier Estimate, 030204 cardiovascular system & hematology, Salmonella typhi, complex mixtures, World health, Typhoid fever, 03 medical and health sciences, 0302 clinical medicine, Double-Blind Method, Nepal, Conjugate vaccine, Internal medicine, medicine, Humans, 030212 general & internal medicine, Typhoid Fever, Child, Vaccines, Conjugate, business.industry, Incidence, Incidence (epidemiology), Typhoid-Paratyphoid Vaccines, Infant, General Medicine, bacterial infections and mycoses, medicine.disease, 3. Good health, Child, Preschool, Female, business
Abstract

BACKGROUND Salmonella Typhi is a major cause of fever in children in low- and middle-income countries. A typhoid conjugate vaccine (TCV) that was recently prequalified by the World Health Organization was shown to be efficacious in a human challenge model, but data from efficacy trials in areas where typhoid is endemic are lacking. METHODS In this phase 3, randomized, controlled trial in Lalitpur, Nepal, in which both the participants and observers were unaware of the trial-group assignments, we randomly assigned children who were between 9 months and 16 years of age, in a 1:1 ratio, to receive either a TCV or a capsular group A meningococcal conjugate vaccine (MenA) as a control. The primary outcome was typhoid fever confirmed by blood culture. We present the prespecified analysis of the primary and main secondary outcomes (including an immunogenicity subgroup); the 2-year trial follow-up is ongoing. RESULTS A total of 10,005 participants received the TCV and 10,014 received the MenA vaccine. Blood culture–confirmed typhoid fever occurred in 7 participants who received TCV (79 cases per 100,000 person-years) and in 38 who received MenA vaccine (428 cases per 100,000 person-years) (vaccine efficacy, 81.6%; 95% confidence interval, 58.8 to 91.8; P CONCLUSIONS A single dose of TCV was immunogenic and effective in reducing S. Typhi bacteremia in children 9 months to 16 years of age. (Funded by the Bill and Melinda Gates Foundation; Current Controlled Trials number, ISRCTN43385161. opens in new tab.)

Published
2019

19. 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, Pollard, AJ, and European Men B Vaccine Study Group

Subjects
Male, Time Factors, 4CMenB, Booster dose, Neisseria meningitidis, law.invention, 0302 clinical medicine, Randomized controlled trial, law, Medicine, 030212 general & internal medicine, Czech Republic, Immunogenicity, Venous blood, 11 Medical And Health Sciences, Antibodies, Bacterial, Vaccination, Infectious Diseases, Italy, Child, Preschool, Molecular Medicine, Female, medicine.medical_specialty, Blood Bactericidal Activity, Toddler, Immunization, Secondary, Meningococcal Vaccines, Meningococcal vaccine, 03 medical and health sciences, 030225 pediatrics, Internal medicine, Virology, Immunology and Microbiology(all), Humans, MenW, Reactogenicity, Antigens, Bacterial, General Veterinary, General Immunology and Microbiology, business.industry, Vaccine, Public Health, Environmental and Occupational Health, Infant, Complement System Proteins, 06 Biological Sciences, veterinary(all), United Kingdom, Spain, Immunology, Antibody Formation, 07 Agricultural And Veterinary Sciences, business
Abstract

Background4CMenB 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 24 months and characterised the antibody response to a fifth dose administered at 4 years of age.MethodsA 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, 6 month schedule.ResultsAt 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 4 years 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).ConclusionWaning of protective antibodies occurred 12–36 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.

Published
2017
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21. Evaluation of the Clinical and Microbiological Response to Salmonella Paratyphi A Infection in the First Paratyphoid Human Challenge Model

Author

Dobinson, H.C., Gibani, M.M., Jones, C., Thomaides-Brears, H.B., Voysey, M., Darton, T.C., Waddington, C.S., Campbell, D., Milligan, I., Zhou, L., Shrestha, S., Kerridge, S.A., Peters, A., Stevens, Z., Podda, A., Martin, L.B., D'Alessio, F., Thanh, D.P., Basnyat, B., Baker, S., Angus, B., Levine, M.M., Blohmke, C.J., Pollard, A.J., Baker, Stephen [0000-0003-1308-5755], and Apollo - University of Cambridge Repository

Subjects
Adult, Male, Time Factors, Immunology, enteric fever, Bacteremia, Microbiology, Feces, Young Adult, FEVER, DESIGN, Paratyphoid Fever, Major Article, Humans, paratyphoid infection, 11 Medical and Health Sciences, OUTPATIENT, Science & Technology, Temperature, 06 Biological Sciences, Middle Aged, bacterial infections and mycoses, immune responses, Healthy Volunteers, Editor's Choice, Salmonella enterica paratyphi A, Infectious Diseases, Blood, Salmonella paratyphi A, ENTERICA SEROVAR PARATYPHI, bacteria, ORAL TYPHOID VACCINE, human challenge study, Female, BURDEN, Life Sciences & Biomedicine
Abstract

Summary The safe establishment of a protocol for a human challenge model for Salmonella Paratyphi A can be used to expedite the evaluation of novel vaccine candidates and provides insight into the clinical and immune response to paratyphoid infection., Background. To expedite the evaluation of vaccines against paratyphoid fever, we aimed to develop the first human challenge model of Salmonella enterica serovar Paratyphi A infection. Methods. Two groups of 20 participants underwent oral challenge with S. Paratyphi A following sodium bicarbonate pretreatment at 1 of 2 dose levels (group 1: 1–5 × 103 colony-forming units [CFU] and group 2: 0.5–1 × 103 CFU). Participants were monitored in an outpatient setting with daily clinical review and collection of blood and stool cultures. Antibiotic treatment was started when prespecified diagnostic criteria were met (temperature ≥38°C for ≥12 hours and/or bacteremia) or at day 14 postchallenge. Results. The primary study objective was achieved following challenge with 1–5 × 103 CFU (group 1), which resulted in an attack rate of 12 of 20 (60%). Compared with typhoid challenge, paratyphoid was notable for high rates of subclinical bacteremia (at this dose, 11/20 [55%]). Despite limited symptoms, bacteremia persisted for up to 96 hours after antibiotic treatment (median duration of bacteremia, 53 hours [interquartile range, 24–85 hours]). Shedding of S. Paratyphi A in stool typically preceded onset of bacteremia. Conclusions. Challenge with S. Paratyphi A at a dose of 1–5 × 103 CFU was well tolerated and associated with an acceptable safety profile. The frequency and persistence of bacteremia in the absence of clinical symptoms was notable, and markedly different from that seen in previous typhoid challenge studies. We conclude that the paratyphoid challenge model is suitable for the assessment of vaccine efficacy using endpoints that include bacteremia and/or symptomatology. Clinical Trials Registration. NCT02100397.

Published
2019
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22. Comparison of two schedules of two-dose priming with the ten-valent pneumococcal conjugate vaccine in Nepalese children: an open-label, randomised non-inferiority controlled trial

Author

Kandasamy, R, Gurung, M, Thorson, S, Yu, LM, Galal, U, Voysey, M, Kelly, S, Wahl, B, Berbers, G, Finnegan, K, Ansari, I, Paudel, K, Murdoch, DR, O'Brien, KL, Kelly, DF, Goldblatt, D, Shrestha, S, Pollard, AJ, Kandasamy, R, Gurung, M, Thorson, S, Yu, LM, Galal, U, Voysey, M, Kelly, S, Wahl, B, Berbers, G, Finnegan, K, Ansari, I, Paudel, K, Murdoch, DR, O'Brien, KL, Kelly, DF, Goldblatt, D, Shrestha, S, and Pollard, AJ

Abstract

Background: Nepalese infants receive ten-valent pneumococcal conjugate vaccine (PCV10) with a 1 month interval between priming doses for programmatic reasons. We aimed to investigate whether immune responses to PCV10 serotypes were non-inferior if the second priming dose of PCV10 was delivered at a 1 month interval as opposed to a 2 month interval. Methods: We did an open-label, randomised, parallel group trial in healthy Nepalese infants aged 40–60 days at Patan Hospital, Kathmandu, Nepal. Children were eligible for inclusion if they were healthy, were born at more than or equal to 37 weeks' gestation, were residing in Kathmandu, and had not had any previous vaccinations other than BCG, and oral polio vaccine. Participants were randomly assigned (1:1) by means of a computer-generated list with randomly varying permuted block sizes accessed through a validated web-based interface, to receive PCV10 either at 6 weeks and 10 weeks of age (6 + 10 group) or at 6 weeks and 14 weeks of age (6 + 14 group), with both groups receiving a booster at 9 months of age. Laboratory staff, masked to study intervention, analysed serum samples for antibodies against PCV10 serotypes by ELISA. The primary outcome was to determine whether the 6 + 10 schedule was non-inferior to the 6 + 14 schedule at 9 months of age, on the basis of the proportion of infants with serotype-specific IgG greater than or equal to 0·35 μg/mL. Non-inferiority was established with a 10% margin, and the primary endpoint was measured in a modified intention-to-treat population, which included only participants who successfully had a blood sample collected. This trial is registered at ClinicalTrials.gov, number NCT02385513. Findings: Between Aug 21, 2015, and April 4, 2016, 304 Nepalese children were randomly assigned to either the 6 + 10 group (n=152) or the 6 + 14 group (n=152). At 9 months of age, the 6 + 10 schedule was non-inferior for serotype 5 (79 [55·2%] of 143 vs 78 [53·4%] of 146, difference 1·82% [95% C

Published
2019

23. Effects of repeat prenatal corticosteroids given to women at risk of preterm birth: An individual participant data meta-analysis

Author

Myers, JE, Crowther, CA, Middleton, PF, Voysey, M, Askie, L, Zhang, S, Martlow, TK, Aghajafari, F, Asztalos, E, Brocklehurst, P, Dutta, S, Garite, TJ, Guinn, DA, Hallman, M, Hardy, P, Lee, M-J, Maurel, K, Mazumder, P, McEvoy, C, Murphy, KE, Peltoniemi, OM, Thom, EA, Wapner, RJ, Doyle, LW, Myers, JE, Crowther, CA, Middleton, PF, Voysey, M, Askie, L, Zhang, S, Martlow, TK, Aghajafari, F, Asztalos, E, Brocklehurst, P, Dutta, S, Garite, TJ, Guinn, DA, Hallman, M, Hardy, P, Lee, M-J, Maurel, K, Mazumder, P, McEvoy, C, Murphy, KE, Peltoniemi, OM, Thom, EA, Wapner, RJ, and Doyle, LW

Abstract

BACKGROUND: Infants born preterm compared with infants born at term are at an increased risk of dying and of serious morbidities in early life, and those who survive have higher rates of neurological impairments. It remains unclear whether exposure to repeat courses of prenatal corticosteroids can reduce these risks. This individual participant data (IPD) meta-analysis (MA) assessed whether repeat prenatal corticosteroid treatment given to women at ongoing risk of preterm birth in order to benefit their infants is modified by participant or treatment factors. METHODS AND FINDINGS: Trials were eligible for inclusion if they randomised women considered at risk of preterm birth who had already received an initial, single course of prenatal corticosteroid seven or more days previously and in which corticosteroids were compared with either placebo or no placebo. The primary outcomes for the infants were serious outcome, use of respiratory support, and birth weight z-scores; for the children, they were death or any neurosensory disability; and for the women, maternal sepsis. Studies were identified using the Cochrane Pregnancy and Childbirth search strategy. Date of last search was 20 January 2015. IPD were sought from investigators with eligible trials. Risk of bias was assessed using criteria from the Cochrane Collaboration. IPD were analysed using a one-stage approach. Eleven trials, conducted between 2002 and 2010, were identified as eligible, with five trials being from the United States, two from Canada, and one each from Australia and New Zealand, Finland, India, and the United Kingdom. All 11 trials were included, with 4,857 women and 5,915 infants contributing data. The mean gestational age at trial entry for the trials was between 27.4 weeks and 30.2 weeks. There was no significant difference in the proportion of infants with a serious outcome (relative risk [RR] 0.92, 95% confidence interval [CI] 0.82 to 1.04, 5,893 infants, 11 trials, p = 0.33 for heterogeneit

Published
2019

24. Effects of repeat prenatal corticosteroids given to women at risk of preterm birth:an individual participant data meta-analysis

Author

Crowther, C. A. (Caroline A.), Middleton, P. F. (Philippa F.), Voysey, M. (Merryn), Askie, L. (Lisa), Zhang, S. (Sasha), Martlow, T. K. (Tanya K.), Aghajafari, F. (Fariba), Asztalos, E. V. (Elizabeth V.), Brocklehurst, P. (Peter), Dutta, S. (Sourabh), Garite, T. J. (Thomas J.), Guinn, D. A. (Debra A.), Hallman, M. (Mikko), Hardy, P. (Pollyanna), Lee, M.-J. (Men-Jean), Maurel, K. (Kimberley), Mazumder, P. (Premasish), McEvoy, C. (Cindy), Murphy, K. E. (Kellie E.), Peltoniemi, O. M. (Outi M.), Thom, E. A. (Elizabeth A.), Wapner, R. J. (Ronald J.), Doyle, L. W. (Lex W.), Crowther, C. A. (Caroline A.), Middleton, P. F. (Philippa F.), Voysey, M. (Merryn), Askie, L. (Lisa), Zhang, S. (Sasha), Martlow, T. K. (Tanya K.), Aghajafari, F. (Fariba), Asztalos, E. V. (Elizabeth V.), Brocklehurst, P. (Peter), Dutta, S. (Sourabh), Garite, T. J. (Thomas J.), Guinn, D. A. (Debra A.), Hallman, M. (Mikko), Hardy, P. (Pollyanna), Lee, M.-J. (Men-Jean), Maurel, K. (Kimberley), Mazumder, P. (Premasish), McEvoy, C. (Cindy), Murphy, K. E. (Kellie E.), Peltoniemi, O. M. (Outi M.), Thom, E. A. (Elizabeth A.), Wapner, R. J. (Ronald J.), and Doyle, L. W. (Lex W.)

Abstract

Background: Infants born preterm compared with infants born at term are at an increased risk of dying and of serious morbidities in early life, and those who survive have higher rates of neurological impairments. It remains unclear whether exposure to repeat courses of prenatal corticosteroids can reduce these risks. This individual participant data (IPD) meta-analysis (MA) assessed whether repeat prenatal corticosteroid treatment given to women at ongoing risk of preterm birth in order to benefit their infants is modified by participant or treatment factors. Methods and findings: Trials were eligible for inclusion if they randomised women considered at risk of preterm birth who had already received an initial, single course of prenatal corticosteroid seven or more days previously and in which corticosteroids were compared with either placebo or no placebo. The primary outcomes for the infants were serious outcome, use of respiratory support, and birth weight z-scores; for the children, they were death or any neurosensory disability; and for the women, maternal sepsis. Studies were identified using the Cochrane Pregnancy and Childbirth search strategy. Date of last search was 20 January 2015. IPD were sought from investigators with eligible trials. Risk of bias was assessed using criteria from the Cochrane Collaboration. IPD were analysed using a one-stage approach. Eleven trials, conducted between 2002 and 2010, were identified as eligible, with five trials being from the United States, two from Canada, and one each from Australia and New Zealand, Finland, India, and the United Kingdom. All 11 trials were included, with 4,857 women and 5,915 infants contributing data. The mean gestational age at trial entry for the trials was between 27.4 weeks and 30.2 weeks. There was no significant difference in the proportion of infants with a serious outcome (relative risk [RR] 0.92, 95% confidence interval [CI] 0.82 to 1.04, 5,893 infants, 11 trials, p = 0.33 for het

Published
2019

25. The impact of vaccination and prior exposure on stool shedding of Salmonella Typhi and Salmonella Paratyphi in 6 controlled human infection studies

Author

Gibani, M.M., Voysey, M., Jin, C., Jones, C., Thomaides-Brears, H., Jones, E., Baker, P., Morgan, M., Simmons, A., Gordon, M.A., Cerundolo, V., Pitzer, V.E., Angus, B., Levine, M.M., Darton, T.C., and Pollard, A.J.

Subjects
Immunology, CHILDREN, TOXOID CONJUGATE VACCINE, IMMUNOGENICITY, Microbiology, Salmonella Typhi, complex mixtures, Feces, fluids and secretions, FEVER, Paratyphoid Fever, Humans, Typhoid Fever, Articles and Commentaries, indirect effects, 11 Medical and Health Sciences, Bacterial Shedding, Science & Technology, Typhoid-Paratyphoid Vaccines, GLOBAL BURDEN, 06 Biological Sciences, EFFICACY, MODEL, Infectious Diseases, stool shedding, Salmonella paratyphi A, Vi-polysaccharide vaccine, bacteria, TRIAL, typhoid conjugate vaccine, Life Sciences & Biomedicine
Abstract

Six Salmonella Typhi or Paratyphi human challenge studies were conducted, and daily stool cultures performed. Vi-containing vaccines reduced bacterial shedding, Ty21a or an experimental vaccine did not. Higher Vi immunoglobulin G titers were associated with reduced shedding., Background Shedding of Salmonella Typhi or Paratyphi in the stool or urine leads to contamination of food or water, which is a prerequisite for transmission of enteric fever. Currently, there are limited data on the effect of vaccination or prior exposure on stool shedding. Methods Six Salmonella Typhi or Paratyphi human challenge studies were conducted between 2011 and 2017. Participants were either unvaccinated or vaccinated with 1 of 4 vaccines: Vi-polysaccharide (Vi-PS), Vi-tetanus-toxoid conjugate vaccine (Vi-TT), live oral Ty21a vaccine, or an experimental vaccine (M01ZH09). Daily stool cultures were collected for 14 days after challenge. Results There were 4934 stool samples collected from 430 volunteers. Participants who received Vi-PS or Vi-TT shed less than unvaccinated participants (odds ratio [OR], 0.34; 95% confidence interval [CI], 0.15–0.77; P = .010 and OR, 0.41; 95% CI, 0.19–0.91, P = .029 for Vi-PS and Vi-TT, respectively). Higher anti-Vi immunoglobulin G titers were associated with less shedding of S. Typhi (P < .0001). A nonsignificant reduction in shedding was associated with Ty21a vaccine (OR, 0.57; 95% CI, 0.27–1.20; P = .140). Individuals previously exposed to S. Typhi shed less than previously unexposed individuals (OR, 0.30; 95% CI, 0.1–0.8; P = .016). Shedding of S. Typhi was more common than S. Paratyphi. Conclusions Prior vaccination with Vi vaccines, or natural infection, reduces onward transmission of S. Typhi. Field trials of Vi-TT should be designed to detect indirect protection, reflecting the consequence of reduced stool shedding observed in the human challenge model.

Published
2018

26. Serotype-Specific Correlates of Protection for Pneumococcal Carriage: An Analysis of Immunity in 19 Countries

Author

Voysey, M, Fanshawe, TR, Kelly, DF, O'Brien, KL, Kandasamy, R, Shrestha, S, Thorson, S, Hinds, J, Pollard, AJ, Voysey, M, Fanshawe, TR, Kelly, DF, O'Brien, KL, Kandasamy, R, Shrestha, S, Thorson, S, Hinds, J, and Pollard, AJ

Abstract

Background. Pneumococcal conjugate vaccines (PCVs) provide direct protection against disease in those vaccinated, and interrupt transmission through the prevention of nasopharyngeal (NP) carriage. Methods. We analyzed immunogenicity data from 5224 infants who received PCV in prime-boost schedules. We defned any increase in antibody between the 1-month postpriming visit and the booster dose as an indication of NP carriage ("seroincidence"). We calculated antibody concentrations using receiver operating characteristic curves, and used generalized additive models to compute their protective efcacy against seroincidence. To support seroincidence as a marker of carriage, we compared seroincidence in a randomized immunogenicity trial in Nepal with the serotype-specifc prevalence of carriage in the same community. Results. In Nepalese infants, seroincidence of carriage closely correlated with serotype-specifc carriage prevalence in the community. In the larger data set, antibody concentrations associated with seroincidence were lowest for serotypes 6B and 23F (0.50 μg/mL and 0.63 μg/mL, respectively), and highest for serotypes 19F and 14 (2.54 μg/mL and 2.48 μg/mL, respectively). Te protective efcacy of antibody at these levels was 62% and 74% for serotypes 6B and 23F, and 87% and 84% for serotypes 19F and 14. Protective correlates were on average 2.15 times higher in low/lower middle-income countries than in high/upper middle-income countries (geometric mean ratio, 2.15 [95% confdence interval, 1.46-3.17]; P =.0024). Conclusions. Antibody concentrations associated with protection vary between serotypes. Higher antibody concentrations are required for protection in low-income countries. Tese fndings are important for global vaccination policy, to interrupt transmission by protecting against carriage.

Published
2018

27. Identification of novel serodiagnostic signatures of typhoid fever using a salmonella proteome array

Author

Darton, T.C., Baker, S., Randall, A., Dongol, S., Karkey, A., Voysey, M., Carter, M.J., Jones, C., Trappl, K., Pablo, J., Hung, C., Teng, A., Shandling, A., Le, T., Walker, C., Molina, D., Andrews, J., Arjyal, A., Basnyat, B., Pollard, A.J., Blohmke, C.J., Baker, Stephen [0000-0003-1308-5755], and Apollo - University of Cambridge Repository

Subjects
machine learning, enteric fever, antibody response, serodiagnostics, controlled human infection model, bacterial infections and mycoses, Microbiology, Salmonella Typhi, fever diagnostics, Original Research, rapid diagnostic tests
Abstract

Current diagnostic tests for typhoid fever, the disease caused by Salmonella Typhi, are poor. We aimed to identify serodiagnostic signatures of typhoid fever by assessing microarray signals to 4,445 S. Typhi antigens in sera from 41 participants challenged with oral S. Typhi. We found broad, heterogeneous antibody responses with increasing IgM/IgA signals at diagnosis. In down-selected 250-antigen arrays we validated responses in a second challenge cohort (n = 30), and selected diagnostic signatures using machine learning and multivariable modeling. In four models containing responses to antigens including flagellin, OmpA, HlyE, sipC, and LPS, multi-antigen signatures discriminated typhoid (n = 100) from other febrile bacteremia (n = 52) in Nepal. These models contained combinatorial IgM, IgA, and IgG responses to 5 antigens (ROC AUC, 0.67 and 0.71) or 3 antigens (0.87), although IgA responses to LPS also performed well (0.88). Using a novel systematic approach we have identified and validated optimal serological diagnostic signatures of typhoid fever.

Published
2017

29. Effect of Oral Dexamethasone Without Immediate Antibiotics vs Placebo on Acute Sore Throat in Adults

Author

Hayward, GN, Hay, AD, Moore, MV, Jawad, S, Williams, N, Voysey, M, Cook, J, Allen, J, Thompson, M, Little, P, Perera, R, Wolstenholme, J, Harman, K, and Heneghan, C

Subjects
General & Internal Medicine, 11 Medical And Health Sciences
Abstract

Importance Acute sore throat poses a significant burden on primary care and is a source of inappropriate antibiotic prescribing. Corticosteroids could be an alternative symptomatic treatment. Objective To assess the clinical effectiveness of oral corticosteroids for acute sore throat in the absence of antibiotics. Design, Setting, and Participants Double-blind, placebo-controlled randomized trial (April 2013-February 2015; 28-day follow-up completed April 2015) conducted in 42 family practices in South and West England, enrolled 576 adults recruited on the day of presentation to primary care with acute sore throat not requiring immediate antibiotic therapy. Interventions Single oral dose of 10 mg of dexamethasone (n = 293) or identical placebo (n = 283). Main Outcomes and Measures Primary: proportion of participants experiencing complete resolution of symptoms at 24 hours. Secondary: complete resolution at 48 hours, duration of moderately bad symptoms (based on a Likert scale, 0, normal; 6, as bad as it could be), visual analog symptom scales (0-100 mm; 0, no symptom to 100, worst imaginable), health care attendance, days missed from work or education, consumption of delayed antibiotics or other medications, adverse events. Results Among 565 eligible participants who were randomized (median age, 34 years [interquartile range, 26.0-45.5 year]; 75.2% women; 100% completed the intervention), 288 received dexamethasone; 277, placebo. At 24 hours, 65 participants (22.6%) in the dexamethasone group and 49 (17.7%) in the placebo group achieved complete resolution of symptoms, for a risk difference of 4.7% (95% CI, −1.8% to 11.2%) and a relative risk of 1.28 (95% CI; 0.92 to 1.78; P = .14). At 24 hours, participants receiving dexamethasone were not more likely than those receiving placebo to have complete symptom resolution. At 48 hours, 102 participants (35.4%) in the dexamethasone group vs 75 (27.1%) in the placebo group achieved complete resolution of symptoms, for a risk difference of 8.7% (95% CI, 1.2% to 16.2%) and a relative risk of 1.31 (95% CI, 1.02 to 1.68; P = .03). This difference also was observed in participants not offered delayed antibiotic prescription, for a risk difference of 10.3% (95% CI, 0.6% to 20.1%) and a relative risk of 1.37 (95% CI, 1.01 to 1.87; P = .046). There were no significant differences in any other secondary outcomes. Conclusions and Relevance Among adults presenting to primary care with acute sore throat, a single dose of oral dexamethasone compared with placebo did not increase the proportion of patients with resolution of symptoms at 24 hours. However, there was a significant difference at 48 hours.

Published
2017

30. An appraisal of the clinical features of paediatric enteric fever including a systematic review and meta-analysis of the age stratified disease occurence

Author

Britto, C, Pollard, A, Voysey, M, and Blohmke, C

Abstract

Children bear a substantial proportion of the enteric fever disease burden in endemic areas. Controversy persistis regarding which age groups are most affected, leading to uncertainty about optimal intervention strategies. We performed a systematic review and meta-analysis of studies in Asia and Africa to compare the relative proportion of children with enteric fever in the

Published
2017

32. Persistence of immunity after vaccination with a capsular group B meningococcal vaccine in 3 different toddler schedules

Author

Sadarangani, M, Sell, T, Iro, MA, Snape, MD, Voysey, M, Finn, A, Heath, PT, Bona, G, Esposito, S, Diez-Domingo, J, Prymula, R, Odueyungbo, A, Toneatto, D, Pollard, AJ, and European MenB Vaccine Study Group

Abstract

BACKGROUND: One schedule for the capsular group B meningococcal vaccine 4CMenB is 2 doses that are administered 2 months apart for children aged 12-23 months, with a booster dose 12-24 months later. Our objective was to provide data on persistence of human serum bactericidal antibody (hSBA) titres in children up to 4 years of age after initial doses at 12-24 months, and immunogenicity of a booster dose at 48 months of age compared with vaccine-naive children. METHODS: Children previously immunized, as part of a randomized controlled trial, with 2 doses of 4CMenB vaccine at 12-24 months of age received a booster at 4 years of age. Vaccine-naive age-matched toddlers received 2 doses of 4CMenB. Human serum bactericidal antibody titres against reference strains H44/76, 5/99, NZ98/254 and M10713 were evaluated before and after innoculation with 4CMenB vaccine in 4-year-old children. RESULTS: Of 332 children in the study, 123 had previously received 4CMenB and 209 were vaccine-naive controls. Before the booster, the proportions of participants (previously vaccinated groups compared with controls) with hSBA titres of 1:5 or more were as follows: 9%-11% v. 1% (H44/76), 84%-100% v. 4% (5/99), 0%-18% v. 0% (NZ98/254) and 59%-60% v. 60% (M10713). After 1 dose of 4CMenB in previously immunized children, the proportions of participants achieving hSBA titres of 1:5 or more were 100% (H44/76 and 5/99), 70%-100% (NZ98/254) and 90%-100% (M10713). INTERPRETATION: We found that waning of hSBA titres by 4 years of age occurred after 2 doses of 4CMenB vaccine administered at 12-24 months, and doses at 12-24 months have a priming effect on the immune system. A booster may be necessary to maintain hSBA titres of 1:5 or more among those children with increased disease risk. Trial registration: ClinicalTrials.gov, no. NCT01717638

Published
2017

33. Assessing the neuroprotective benefits for babies of antenatal magnesium sulphate: An individual participant data meta-analysis

Author

Myers, JE, Crowther, CA, Middleton, PF, Voysey, M, Askie, L, Duley, L, Pryde, PG, Marret, S, Doyle, LW, Myers, JE, Crowther, CA, Middleton, PF, Voysey, M, Askie, L, Duley, L, Pryde, PG, Marret, S, and Doyle, LW

Abstract

BACKGROUND: Babies born preterm are at an increased risk of dying in the first weeks of life, and those who survive have a higher rate of cerebral palsy (CP) compared with babies born at term. The aim of this individual participant data (IPD) meta-analysis (MA) was to assess the effects of antenatal magnesium sulphate, compared with no magnesium treatment, given to women at risk of preterm birth on important maternal and fetal outcomes, including survival free of CP, and whether effects differed by participant or treatment characteristics such as the reason the woman was at risk of preterm birth, why treatment was given, the gestational age at which magnesium sulphate treatment was received, or the dose and timing of the administration of magnesium sulphate. METHODS AND FINDINGS: Trials in which women considered at risk of preterm birth (<37 weeks' gestation) were randomised to magnesium sulphate or control treatment and where neurologic outcomes for the baby were reported were eligible for inclusion. The primary outcomes were infant death or CP and severe maternal outcome potentially related to treatment. Studies were identified based on the Cochrane Pregnancy and Childbirth search strategy using the terms [antenatal or prenatal] and [magnesium] and [preterm or premature or neuroprotection or 'cerebral palsy']. The date of the last search was 28 February 2017. IPD were sought from investigators with eligible trials. Risk of bias was assessed using criteria from the Cochrane Collaboration. For each prespecified outcome, IPD were analysed using a 1-stage approach. All 5 trials identified were included, with 5,493 women and 6,131 babies. Overall, there was no clear effect of magnesium sulphate treatment compared with no treatment on the primary infant composite outcome of death or CP (relative risk [RR] 0.94, 95% confidence interval (CI) 0.85 to 1.05, 6,131 babies, 5 trials, p = 0.07 for heterogeneity of treatment effect across trials). In the prespecified sensitivity

Published
2017

34. Immunogenicity and reactogenicity of novel adenovirus type 26 and modified vaccinia Ankara-vectored Ebola vaccines: A randomized clinical trial

Author

Milligan, ID, Gibani, MMM, Sewell, R, Clutterbuck, EA, Campbell, DFY, Plested, E, Nuthall, E, Voysey, M, Silva Reyes, L, McElrath, MJ, De Rosa, SC, Frahm, N, Cohen, KW, Shukarev, G, Orzabal, N, van Duijnhoven, W, Truyers, C, Bachmayer, N, Splinter, D, Samy, N, Grazia Pau, M, Schuitemaker, H, Luhn, K, Callendret, B, Van Hoof, J, Douoguih, M, Ewer, K, Angus, BJ, Pollard, AJ, and Snape, MD

Subjects
viruses
Abstract

Importance Developing effective vaccines against Ebola virus is a global priority. Objective To evaluate an adenovirus-type 26 vector vaccine encoding Ebola glycoprotein (Ad26.ZEBOV) and a modified vaccinia Ankara vector vaccine, encoding glycoproteins from Ebola virus, Sudan virus, Marburg virus and Tai Forest virus nucleoprotein (MVA-BN-Filo). Design, Setting and Participants Single-center, randomized, placebo-controlled, observer-blind, phase I trial performed in Oxford, UK, enrolling healthy 18 to 50 year-olds from December 2014; 8-month follow-up completed October 2015. Intervention Participants were randomized into 4 groups, within which they were simultaneously randomized 5:1 to study vaccines/placebo. Those receiving active vaccines were primed with Ad26.ZEBOV (5x10^10 viral particles) or MVA-BN-Filo (1x10^8 median tissue culture infective dose) and boosted with the alternative vaccine 28 or 56-days later. A fifth, open-label group received Ad26.ZEBOV boosted by MVA-BN-Filo 14-days later. Outcome and Measures The primary outcomes were safety and tolerability. All adverse events were recorded until 21 days following each immunization; serious adverse events were recorded throughout the trial. Secondary outcomes were humoral and cellular immune responses to immunization, as assessed by enzyme-linked immunosorbent assay and enzyme-linked immunospot performed at baseline and from 7-days following each immunization until 8-months following priming immunization. Results Among 87 study participants (median age 38.5 years, 66.7% female), 72 were randomized into 4 groups of 18, and 15 were included in the open-label group. Four did not receive a booster dose; 67 of 75 study vaccine recipients were followed up at 8 months. No vaccine-related serious adverse events occurred. No participant became febrile following MVA-BN-Filo compared with 3/60 (5%; 95% CI 1%-14%) of participants receiving Ad26.ZEBOV in the randomized groups. In the open-label group 4/15 (27%; 8%-55%) Ad26.ZEBOV recipients experienced fever. In the randomized groups, 28/29 (97%; 82%-99.9%) of Ad26.ZEBOV and 7/30 (23%; 10%-42%)MVA-BN-Filo recipients had detectable Ebola glycoprotein-specific IgG 28-days following primary immunization. All vaccine recipients had specific IgG detectable 21-days post-boost and at 8-month follow-up. Within randomized groups, at day 7 post-boost at least 86% of vaccine recipients showed Ebola-specific T cell responses. Conclusions and Relevance In this phase 1 study of healthy volunteers, immunization with Ad26.ZEBOV or MVA-BN-Filo did not result in any vaccine-related serious adverse events. An immune response was observed following primary immunization with Ad26.ZEBOV; boosting by MVA-BN-Filo resulted in sustained elevation of specific immunity. These vaccines are being further assessed in phase 2 and 3 studies.

Published
2016

35. Persistence of bactericidal antibodies following infant serogroup B meningococcal immunization (4CMenB) and booster dose response at 12, 18 or 24 months of age

Author

Snape, MD, Pollard, AJ, Voysey, M, Finn, A, Bona, G, Esposito, S, Principi, N, Diez-Domingo, J, Sokal, E, Kieninger, D, Prymula, R, Dull, PM, Kohl, I, Barone, M, Wang, H, and Toneatto, D

Abstract

Background: A serogroup B meningococcal vaccine (4CMenB) is licensed for infant use in countries including Canada, Australia and those of the European Union. Data on serum bactericidal antibody (hSBA) waning and the ideal timing of a ‘toddler’ booster dose are essential to optimise vaccine utilization. Methods: An open-labeled, multicenter phase-2b follow-on European study conducted from 2009 to 2012. Participants previously receiving 4CMenB with routine vaccines at 2,4,6 or 2,3,4 months (246Con and 234Con) or at 2,4,6 months intercalated with routine vaccines (246Int) received a booster dose at 12, 18 or 24 months. 4CMenB-naïve ‘Control’ participants aged 12, 18 or 24 months received two doses of 4CMenB two months apart. Results: 1588 participants were recruited. At 12 months, prior to any booster doses, the proportions with hSBA titers ≥ 1:5 for strain 44/76-SL (testing vaccine component fHBP) were 73% (120/165) for the ‘246Con’ group, 85% (125/147) for ‘246Int’, 57% (51/90) for ‘234Con’ and 13% (26/199) for Controls. For strain 5/99 (NadA) proportions were ≥ 96% (all 4CMenB-recipients) and 1% (Controls). For strain NZ98/254 (PorA) these were 18-35% (4CMenB-recipients) and 1% (Controls). By 24 months, 4CMenB-recipient proportions were 13%–22% (44/76-SL), 82%-94% (5/99) and 7-13% (NZ98/254) and in Controls ≤ 4%. Following a 12-month booster-dose ≥ 95% of previously immunized participants had titers ≥1:5 (all strains). Conclusions: A 4CMenB booster-dose can overcome waning hSBA titers after early-infant immunization. Administration at 12 months could help to maintain immunity during an age of high risk, and the persistence of this response requires further study.

Published
2016

36. Applying the intention-to-treat principle in practice: Guidance on handling randomisation errors

Author

Yelland, L, Sullivan, T, Voysey, M, Cook, J, and al., E

Abstract

BACKGROUND: The intention-to-treat principle states that all randomised participants should be analysed in their randomised group. The implications of this principle are widely discussed in relation to the analysis, but have received limited attention in the context of handling errors that occur during the randomisation process. The aims of this article are to (1) demonstrate the potential pitfalls of attempting to correct randomisation errors and (2) provide guidance on handling common randomisation errors when they are discovered that maintains the goals of the intention-to-treat principle. METHODS: The potential pitfalls of attempting to correct randomisation errors are demonstrated and guidance on handling common errors is provided, using examples from our own experiences. RESULTS: We illustrate the problems that can occur when attempts are made to correct randomisation errors and argue that documenting, rather than correcting these errors, is most consistent with the intention-to-treat principle. When a participant is randomised using incorrect baseline information, we recommend accepting the randomisation but recording the correct baseline data. If ineligible participants are inadvertently randomised, we advocate keeping them in the trial and collecting all relevant data but seeking clinical input to determine their appropriate course of management, unless they can be excluded in an objective and unbiased manner. When multiple randomisations are performed in error for the same participant, we suggest retaining the initial randomisation and either disregarding the second randomisation if only one set of data will be obtained for the participant, or retaining the second randomisation otherwise. When participants are issued the incorrect treatment at the time of randomisation, we propose documenting the treatment received and seeking clinical input regarding the ongoing treatment of the participant. CONCLUSION: Randomisation errors are almost inevitable and should be reported in trial publications. The intention-to-treat principle is useful for guiding responses to randomisation errors when they are discovered.

Published
2015

37. Non-specific immunological effects of selected routine childhood immunisations: Systematic review

Author

Kandasamy, R, Voysey, M, McQuaid, F, De Nie, K, Ryan, R, Orr, O, Uhlig, U, Sande, C, O'Connor, D, Pollard, AJ, Kandasamy, R, Voysey, M, McQuaid, F, De Nie, K, Ryan, R, Orr, O, Uhlig, U, Sande, C, O'Connor, D, and Pollard, AJ

Abstract

Objective: To identify and characterise non-specific immunological effects after routine childhood vaccines against BCG, measles, diphtheria, pertussis, and tetanus. Design: Systematic review of randomised controlled trials, cohort studies, and case-control studies. Data sources: Embase, PubMed, Cochrane library, and Trip searched between 1947 and January 2014. Publications submitted by a panel of experts in the specialty were also included. Eligibility criteria for selecting studies: All human studies reporting non-specific immunological effects after vaccination with standard childhood immunisations. Studies using recombinant vaccines, no vaccine at all, or reporting only vaccine specific outcomes were excluded. The primary aim was to systematically identify, assemble, and review all available studies and data on the possible nonspecific or heterologous immunological effects of BCG; measles; mumps, measles, and rubella (MMR); diphtheria; tetanus; and pertussis vaccines. Results: The initial search yielded 11 168 references; 77 manuscripts met the inclusion criteria for data analysis. In most included studies (48%) BCG was the vaccine intervention. The final time point of outcome measurement was primarily performed (70%) between one and 12 months after vaccination. There was a high risk of bias in the included studies, with no single study rated low risk across all assessment criteria. A total of 143 different immunological variables were reported, which, in conjunction with differences in measurement units and summary statistics, created a high number of combinations thus precluding any meta-analysis. Studies that compared BCG vaccinated with unvaccinated groups showed a trend towards increased IFN-γ production in vitro in the vaccinated groups. Increases were also observed for IFN-γ measured after BCG vaccination in response to in vitro stimulation with microbial antigens from Candida albicans, tetanus toxoid, Staphylococcus aureas, lipopolysaccharide, and hepati

Published
2016

38. The predicted persistence and kinetics of antibody decline 9 years after pre-school booster vaccination in UK children

Author

Voysey, M, Kandasamy, R, Yu, LM, Baudin, M, Sadorge, C, Thomas, S, John, T, Pollard, AJ, Voysey, M, Kandasamy, R, Yu, LM, Baudin, M, Sadorge, C, Thomas, S, John, T, and Pollard, AJ

Abstract

Background Long term follow-up of vaccine trials is essential to establish the duration of protection. In the context of worldwide concern about rising pertussis incidence, estimates of antibody persistence after vaccination, which do not account for the rise in antibody due to natural boosting or infection, may overestimate the degree of protection afforded by pertussis vaccines. Methods This was a 5 year follow up study of a randomised controlled trial of diphtheria, tetanus, pertussis and polio booster vaccines in UK children aged 3.5–5 years. Antibody persistence was measured at 1 month, 1, 3, and 5 years after vaccination and the kinetics of antibody decline were modelled longitudinally. Estimates of predicted antibody persistence 9 years after the pre-school booster were derived from model parameters. Results Antibody levels 9 years after vaccination were predicted to be above accepted thresholds for protection for diphtheria, tetanus and polio. Antibody responses to pertussis toxoid were undetectable in 49% of children at the 5 year follow up visit, and responses were predicted to be undetectable in 69% (95% CI 45–88%) of children by the time of their teenage booster at 13–14 years of age. Conclusions There is no defined correlate of protection for pertussis. However, the large proportion of participants in this study with undetectable pertussis antibody levels at both measured and predicted timepoints suggests sub-optimal immunity in adolescence. Adding pertussis to the teenage booster for UK children as is done in other countries, would enhance immunity in adolescence.

Published
2016

39. Dexamethasone versus standard treatment for postoperative nausea and vomiting in gastrointestinal surgery: randomised controlled trial (DREAMS Trial)

Author

Ravikumar, R., Bartlett, D., Morton, D., Berkman, L., Bodenham-Chilton, H., Deeks, J. J., Handley, K., Magill, L., Hamilton, E., Hepburn, E., Hwang, M-J, Mirza, N., Wilkey, A., Magill, M. le Breuilly L., Wilcockson, A., Mehta, S., Burtenshaw, A., Hawkins, W., Voysey, M., Blazeby, J., Smith, I., Stocken, D., Abbott, S., Hwang, M., Karim, A., Luke, D. P., McArthur, D., Mistry, P., Richardson, J., Youssef, H., Ravi, K., Goodfellow, P. B., Gupta, R., Joy, H., Eardley, N., McFaul, C., Vimalachandran, D., Harmston, C., Froggatt, P., Krishnan, P., Pathare, S., Shanmugam, V., Yiannakou, Y. J., Fawole, A., Macklin, C., Mcenhill, J., Narula, H., Riad, T., Rose, A., Chambers, J., Ekere, C., Hough, M., Hull, J., Knight, H. P., Lamparelli, M. J., Lewis, M., Pulletz, M., Siddiqi, N., Stubbs, B., Subramanian, K., Swanton, R., Costigan, S., O'Connell, G., Patel, P. K., Ali, A., Ang, C., Chapman, M. A. S., Shariff, U., Thompson, C., Yates, A. Williamson J., Leinhardt, D. J., Simenacz, M., Harris, S., Loveless, P., Mohsen, Y., Myers, A., Prabhudesai, A., Vanagov, S., Aryal, K., Lal, R., Millican, D., Panagiotopopoulou, I., Shankar, K., Dube, M., Tansley, J., Hill, J., Addison, S., Church, R., Nath, J., Valap, S., Dhrampal, A., Nortje, J., Payne, J., Sargen, K., Speakman, C., Deloughry, J., Elkington, T., Dennis, R., Ghosh, S., Martin, J., Stoker, M., Akerman, N., Basheer, M., Drury, N., Parchment-Smith, C., Sandhu, R., Srinivasa, R., Varma, S., Walwyn, S., Syed, N., Bromilow, J., Colling, P., Reschreiter, H., Senapati, A., Howse, F., Tzouliadis, L., Bach, S., Brookes, A., Cagigas, C., Dimitriou, N., Fallis, S., Futaba, K., Hill, A., Izbal, A., Leong, K., Manji, M., Milns, P., Murray, A., Nicol, D., Pinkney, T., Ramcharam, S., Royle, T. J., Scarpinata, R., Smart, C., Smart, S., Suggett, N., Sutherland, S., Tam, Y. H. M., Torrance, A., Wall, M., Vakis, S., Bassuini, M., Garner, J., Maz, S., Mottahedeh, M., Smith, M., Withers, M., Krishnamourthy, R., Paraoan, M., Thomas, P., Chesshire, N., Davies, S., Gold, S., Hamzah, I., Hurst, N., Khoo, C. K., Kiani, S., Liptrot, S., Lund, J., Millard, C., Morris, C., Reynolds, J. R., Selvaraj, I., Simpson, A., Speake, W., Tou, S., Chambers, W., Gee, A. S., Grice, A., Johnston, D., Miller, Q., Pittman, J., Price, D., Telford, R., Barrow, E., Coldwell, C., Crighton, I., Raymond, T., Richmond, S., Cheetham, M., Kulemeka, G., Carraretto, M., Huddart, S., Kirk-Bayley, J., Moor, D., Scott, M., Asif, M., Awan, R., Bethune, R., Chadwick, M., Cook, T., Courtney, E., Dalton, S., Lim, A., Williamson, M. E. R., Wood, J., Scott, R., Branagan, G., Bellin, J., Browning, D., Bulso, V., Carter, N., Cruikshank, N., Gill, K., Hulme, N., Leno, E., Newbould, D., Thumbe, V., Sankar, K., Sivasubramaniam, S., Wakhle, R., Walton, R., Zulueta, L., Ahmad, S. M., Kaur, G., Longbottom, D., Nnaji, M., Ramamoorthy, A., Thomas, J., Botteril, I., Miskovic, D., Sagar, P. M., Bhuptani, S., Kennedy, R., Jenkins, I., Littler, S., Arnold, G., Buchanan, G., Con, A., Dawson, P., Lawrie, S., Lowe, J., Malhotra, S., Paraskeva, P., Richards, S., Sidhu, V., Ziprin, P., Kruchek, D., Kuttler, A., Mohammad, K., Nasser, T., Rehman, H., Siddiqui, K., Siddiqui, A., Sindhu, Q., Soliman, M., Solkar, M., Thota, S., Renehan, A., Selvasekar, C., Melsom, H., Agarwal, A. K., Borowski, D., Brohi, F., Garg, D., Gill, T., Mahadevan, V., Sharma, A., Tabaqchali, M. A., Alce, T., Navapurkar, A., Page, V., Stambach, T., Capozzi, P., Coe, P., Conroy, P., Duff, S., Grey, T., Hill, O., Nicholson, J., Nolan, D., Pollard, J., Ramesh, A., Sabar, M., Telford, K., Davies, D., Wilson, J., and Yates, D.

Subjects
Adult, Male, medicine.medical_specialty, Treatment outcome, Dexamethasone, law.invention, Eating, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Double-Blind Method, Randomized controlled trial, Preanesthetic Medication, 030202 anesthesiology, law, medicine, Humans, Postoperative Period, 030212 general & internal medicine, Young adult, Aged, Aged, 80 and over, business.industry, Research, Standard treatment, Recovery of Function, General Medicine, Length of Stay, Middle Aged, Surgery, Intestines, Treatment Outcome, Multicenter study, Anesthesia, Injections, Intravenous, Postoperative Nausea and Vomiting, Antiemetics, Female, medicine.symptom, business, Postoperative nausea and vomiting, medicine.drug
Abstract

Objectives To determine whether preoperative dexamethasone reduces postoperative vomiting in patients undergoing elective bowel surgery and whether it is associated with other measurable benefits during recovery from surgery, including quicker return to oral diet and reduced length of stay. Design Pragmatic two arm parallel group randomised trial with blinded postoperative care and outcome assessment. Setting 45 UK hospitals. Participants 1350 patients aged 18 or over undergoing elective open or laparoscopic bowel surgery for malignant or benign pathology. Interventions Addition of a single dose of 8 mg intravenous dexamethasone at induction of anaesthesia compared with standard care. Main outcome measures Primary outcome: reported vomiting within 24 hours reported by patient or clinician. Secondary outcomes: vomiting with 72 and 120 hours reported by patient or clinician; use of antiemetics and postoperative nausea and vomiting at 24, 72, and 120 hours rated by patient; fatigue and quality of life at 120 hours or discharge and at 30 days; time to return to fluid and food intake; length of hospital stay; adverse events. Results 1350 participants were recruited and randomly allocated to additional dexamethasone (n=674) or standard care (n=676) at induction of anaesthesia. Vomiting within 24 hours of surgery occurred in 172 (25.5%) participants in the dexamethasone arm and 223 (33.0%) allocated standard care (number needed to treat (NNT) 13, 95% confidence interval 5 to 22; P=0.003). Additional postoperative antiemetics were given (on demand) to 265 (39.3%) participants allocated dexamethasone and 351 (51.9%) allocated standard care (NNT 8, 5 to 11; P

Published
2017

40. Symptom burden and outcomes of patients with platinum resistant/refractory recurrent ovarian cancer: a reality check: results of stage 1 of the gynecologic cancer intergroup symptom benefit study

Author

Friedlander, M, Stockler, M, O'Connell, R, Voysey, M, Oza, A, Gillies, K, Donovan, H, Martyn, J, Sjoquist, K, Butow, P, and King, M

Abstract

BACKGROUND: The aim of chemotherapy in patients with platinum resistant ovarian cancer is palliation. Patients' experience of symptoms is not well documented, and the impact of treatment on symptoms has not been evaluated in clinical trials. We report symptom burden and treatment outcomes from stage 1 of the Gynecological Cancer Intergroup (GCIG) Symptom Benefit Study. METHODS: One hundred twenty-six patients receiving palliative chemotherapy completed 5 validated health-related quality-of-life questionnaires before starting treatment and before each cycle. They also reported their expected and perceived benefits from treatment. Physicians documented the reasons for treatment and adverse events including symptoms at baseline and estimated the number of cycles of treatment that patients would receive. RESULTS: Palliation was the major reason for chemotherapy. At baseline, all patients were symptomatic (almost 70% had ≥9 symptoms). Patients had high expectation of benefit from treatment. Only 41% of patients received the predicted number of cycles with most stopping early (≤2 cycles) due to progression, death, or adverse effects. Treatment was associated with significant toxicity, with discordance between patient report and physician grading. Although RECIST response rates were low (8.5%), 40% of the patients were reported to have had a clinical benefit and almost 50% of symptomatic patients also reported symptom improvement. CONCLUSIONS: Patients had a complex array of symptoms and significant symptom burden, which was commonly the reason for treatment. Although chemotherapy improved symptoms in about half of the patients, many did not benefit and progressed rapidly. Our findings support research into the use of patient reported outcome measures to document symptoms, adverse events, and subjective benefit, both in clinical trials and in clinical practice, in this patient population. Our findings highlight the need to develop prognostic models to better select patients for treatment, and this is an aim of stage 2 of the GCIG Symptom Benefit Study.

Published
2014

41. Comparison of two-dose priming plus 9-month booster with a standard three-dose priming schedule for a ten-valent pneumococcal conjugate vaccine in Nepalese infants: A randomised, controlled, open-label, non-inferiority trial

Author

Hamaluba, M, Kandasamy, R, Upreti, SR, Subedi, GR, Shrestha, S, Bhattarai, S, Gurung, M, Pradhan, R, Voysey, M, Gurung, S, Pradhan, S, Thapa, AK, Maharjan, R, Kiran, U, Kerridge, SA, Hinds, J, van der Klis, F, Snape, MD, Murdoch, DR, Kelly, S, Kelly, DF, Adhikari, N, Thorson, S, Pollard, AJ, Hamaluba, M, Kandasamy, R, Upreti, SR, Subedi, GR, Shrestha, S, Bhattarai, S, Gurung, M, Pradhan, R, Voysey, M, Gurung, S, Pradhan, S, Thapa, AK, Maharjan, R, Kiran, U, Kerridge, SA, Hinds, J, van der Klis, F, Snape, MD, Murdoch, DR, Kelly, S, Kelly, DF, Adhikari, N, Thorson, S, and Pollard, AJ

Abstract

Background: Use of pneumococcal conjugate vaccines (PCVs) in resource-poor countries has focused on early infant immunisation with little emphasis on protection in late infancy and beyond. Boosting of the immune response later in infancy might provide improved persistence of immunogenicity into early childhood, however data are scarce. The aim of this study was to investigate if a two-dose prime with booster at age 9 months compared with a three-dose prime-only PCV schedule provided non-inferior immunogenicity in early infancy and superior persistence of antibody responses in early childhood. Methods: We did an open-label, randomised, parallel group, controlled trial in healthy infants aged 40-60 days from Kathmandu, Nepal. Participants were randomly allocated (4:4:5 ratio) to receive PCV10 in addition to routine immunisations either as a two-dose prime and boost (2+1), three-dose prime (3+0), or two doses after completion of the initial study phase (0+2). We used a computer generated randomisation list with randomly varying block sizes. We followed up participants at age 2-4 years together with a group of unvaccinated controls. Sera were analysed for opsonophagocytic activity, protein D, and PCV10 serotype-specific IgG. Laboratory staff was masked to intervention group assignment. The primary outcome measure was to determine the proportion of participants in the 2+1 group at age 10 months with specific IgG for serotypes 1, 5, and 14 of at least 0·2 μg/mL in the per-protocol population. The secondary outcomes were non-inferiority (within 10% levels) at age 18 weeks for the proportion of participants in the 2+1 group compared with the 3+0 group with serotypes 1, 5, and 14 specific IgG of at least 0·2 μg/mL; the proportion of participants with PCV10 serotype-specific IgG of at least 0·2 μg/mL and opsonophagocytic activity reciprocal titre of at least 8 at ages 18 weeks and 10 months; and nasopharyngeal pneumococcal serotype-specific carriage rates at age 9 months in e

Published
2015

42. Applying the intention-to-treat principle in practice: Guidance on handling randomisation errors

Author

Yelland, LN, Sullivan, TR, Voysey, M, Lee, KJ, Cook, JA, Forbes, AB, Yelland, LN, Sullivan, TR, Voysey, M, Lee, KJ, Cook, JA, and Forbes, AB

Abstract

BACKGROUND: The intention-to-treat principle states that all randomised participants should be analysed in their randomised group. The implications of this principle are widely discussed in relation to the analysis, but have received limited attention in the context of handling errors that occur during the randomisation process. The aims of this article are to (1) demonstrate the potential pitfalls of attempting to correct randomisation errors and (2) provide guidance on handling common randomisation errors when they are discovered that maintains the goals of the intention-to-treat principle. METHODS: The potential pitfalls of attempting to correct randomisation errors are demonstrated and guidance on handling common errors is provided, using examples from our own experiences. RESULTS: We illustrate the problems that can occur when attempts are made to correct randomisation errors and argue that documenting, rather than correcting these errors, is most consistent with the intention-to-treat principle. When a participant is randomised using incorrect baseline information, we recommend accepting the randomisation but recording the correct baseline data. If ineligible participants are inadvertently randomised, we advocate keeping them in the trial and collecting all relevant data but seeking clinical input to determine their appropriate course of management, unless they can be excluded in an objective and unbiased manner. When multiple randomisations are performed in error for the same participant, we suggest retaining the initial randomisation and either disregarding the second randomisation if only one set of data will be obtained for the participant, or retaining the second randomisation otherwise. When participants are issued the incorrect treatment at the time of randomisation, we propose documenting the treatment received and seeking clinical input regarding the ongoing treatment of the participant. CONCLUSION: Randomisation errors are almost inevitable and shoul

Published
2015

44. The effects of lowering LDL cholesterol with statin therapy in people at low risk of vascular disease: meta-analysis of individual data from 27 randomised trials

Author

Mihaylova, B., Emberson, J., Blackwell, L., Keech, A., Simes, J., Barnes, E.H., Voysey, M., Gray, A., Collins, R., Baigent, C., Lemos, J. de, Braunwald, E., Blazing, M., Murphy, S., Downs, J.R., Gotto, A., Clearfield, M., Holdaas, H., Gordon, D., Davis, B., Koren, M., Dahlof, B., Poulter, N., Sever, P., Knopp, R.H., Fellstrom, B., Jardine, A., Schmieder, R., Zannad, F., Goldbourt, U., Kaplinsky, E., Colhoun, H.M., Betteridge, D.J., Durrington, P.N., Hitman, G.A., Fuller, J., Neil, A., Wanner, C., Krane, V., Sacks, F., Moye, L., Pfeffer, M., Hawkins, C.M., Kjekshus, J., Wedel, H., Wikstrand, J., Barter, P., Tavazzi, L., Maggioni, A., Marchioli, R., Tognoni, G., Franzosi, M.G., Bloomfield, H., Robins, S., Armitage, J., Parish, S., Peto, R., Sleight, P., Pedersen, T.R., Ridker, P.M., Holman, R., Meade, T., MacMahon, S., Marschner, I., Tonkin, A., Shaw, J., Serruys, P.W., Nakamura, H., Knatterud, G., Furberg, C., Byington, R., Macfarlane, P., Cobbe, S., Ford, I., Murphy, M., Blauw, G.J., Packard, C., Shepherd, J., Pedersen, T., Wilhelmsen, L., Cannon, C., Bowman, L., Landray, M., Rosa, J. la, Rossouw, J., Probstfield, J., and Cholesterol Treatment Trialists

Published
2012

45. Glycemic control over 5 years in 4,900 people with type 2 diabetes: real-world diabetes therapy in a clinical trial cohort

Author

Best, J, Drury, P, Davis, T, Taskinen, MR, Kesäniemi, Y, Scott, R, Pardy, C, Voysey, M, and Keech, A

Abstract

OBJECTIVE: Glycemic control in type 2 diabetes generally worsens over time, requiring intensification of therapy. The Fenofibrate Intervention and Event Lowering in Diabetes (FIELD) trial provided the opportunity to observe glycemic control in a real-world setting. We assessed the adequacy of metformin, sulfonylureas, and insulin to maintain glycemic control and their effects on weight. RESEARCH DESIGN AND METHODS: Diabetes control was measured at baseline and yearly for a median of 5 years in the 4,900 patients from the nonintervention arm of this study allocated to placebo. RESULTS: Median HbA(1c) was 6.9% at baseline and increased by an average of 0.22% over 5 years (P < 0.001). Median weight was 86.3 kg at baseline and decreased by 0.4 kg over 5 years (P = 0.002). Baseline therapy was lifestyle measures only in 27%, oral agents without insulin in 59%, and insulin in 14% (7% also taking oral agents). Over 5 years, insulin use increased to 32% (21% also taking oral agents). Use of oral agents remained similar at 56%. Only 2% of patients at baseline and 4% after 5 years were taking oral agents other than metformin or sulfonylureas. Initiation of insulin therapy in 855 patients produced a sustained reduction of HbA(1c) from a median of 8.2 to 7.7%, with a weight gain of 4.6 kg over 5 years. CONCLUSIONS: With intensification of traditional therapies, glycemic control deteriorated very little over 5 years in a large cohort of type 2 diabetes. However, the requirement for insulin therapy doubled, at the expense of significant weight gain and risk of hypoglycemia.

Published
2012

46. Antenatal magnesium individual participant data international collaboration: assessing the benefits for babies using the best level of evidence (AMICABLE)

Author

Crowther, C, Middleton, P, Askie, L, Doyle, L, Bubner, T, and Voysey, M

Subjects
medicine.medical_specialty, Medicine (miscellaneous), Infant, Premature, Diseases, Prenatal care, Magnesium Sulfate, Nursing, Pregnancy, Risk Factors, Infant Mortality, Protocol, medicine, Humans, Fetal Death, Randomized Controlled Trials as Topic, Evidence-Based Medicine, Fetal death, Obstetrics, business.industry, Cerebral Palsy, Individual participant data, Infant, Newborn, Pregnancy Outcome, Magnesium sulphate, Prenatal Care, Preterm birth, Evidence-based medicine, Infant newborn, Infant mortality, Meta-analysis, Neuroprotective Agents, Premature Birth, Individual patient data, Female, business
Abstract

BackgroundThe primary aim of this study is to assess, using individual participant data (IPD) meta-analysis, the effects of administration of antenatal magnesium sulphate given to women at risk of preterm birth on important clinical outcomes for their child such as death and neurosensory disability. The secondary aim is to determine whether treatment effects differ depending on important pre-specified participant and treatment characteristics, such as reasons at risk of preterm birth, gestational age, or type, dose and mode of administration of magnesium sulphate.MethodsDesignThe Antenatal Magnesium Individual Participant Data (IPD) International Collaboration: assessing the benefits for babies using the best level of evidence (AMICABLE) Group will perform an IPD meta-analysis to answer these important clinical questions.Setting/TimelineThe AMICABLE Group was formed in 2009 with data collection commencing late 2010.Inclusion CriteriaFive trials involving a total 6,145 babies are eligible for inclusion in the IPD meta-analysis.Primary study outcomesFor the infants/children: Death or cerebral palsy. For the women: Any severe maternal outcome potentially related to treatment (death, respiratory arrest or cardiac arrest).DiscussionResults are expected to be publicly available in 2012.

Published
2012

47. The effects of lowering LDL cholesterol with statin therapy in people at low risk of vascular disease: meta-analysis of individual data from 27 randomised trials

Author

Cholesterol Treatment Trialists' (CTT) Collaborators, . (inc. Me, T, Mihaylova, B, Emberson, J, Blackwell, L, Keech, A, Simes, J, Barnes, EH, Voysey, M, Gray, A, Collins, R, and Baigent, C

Abstract

BACKGROUND Statins reduce LDL cholesterol and prevent vascular events, but their net effects in people at low risk of vascular events remain uncertain. METHODS This meta-analysis included individual participant data from 22 trials of statin versus control (n=134,537; mean LDL cholesterol difference 1·08 mmol/L; median follow-up 4·8 years) and five trials of more versus less statin (n=39,612; difference 0·51 mmol/L; 5·1 years). Major vascular events were major coronary events (ie, non-fatal myocardial infarction or coronary death), strokes, or coronary revascularisations. Participants were separated into five categories of baseline 5-year major vascular event risk on control therapy (no statin or low-intensity statin) (

Published
2012

48. Safety and immunogenicity of novel respiratory syncytial virus (RSV) vaccines based on the RSV viral proteins F, N and M2-1 encoded by simian adenovirus (PanAd3-RSV) and MVA (MVA-RSV); protocol for an open-label, dose-escalation, single-centre, phase 1 clinical trial in healthy adults

Author

Green, C A, primary, Scarselli, E, additional, Voysey, M, additional, Capone, S, additional, Vitelli, A, additional, Nicosia, A, additional, Cortese, R, additional, Thompson, A J, additional, Sande, C S, additional, de Lara, Catherine, additional, Klenerman, P, additional, and Pollard, A J, additional

Published
2015
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49. Understanding paratyphoid infection: study protocol for the development of a human model of Salmonella enterica serovar Paratyphi A challenge in healthy adult volunteers

Author

McCullagh, D., primary, Dobinson, H. C., additional, Darton, T., additional, Campbell, D., additional, Jones, C., additional, Snape, M., additional, Stevens, Z., additional, Plested, E., additional, Voysey, M., additional, Kerridge, S., additional, Martin, L. B., additional, Angus, B., additional, and Pollard, A. J., additional

Published
2015
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50. Immunogenicity of reduced dose priming schedules of serogroup C meningococcal conjugate vaccine followed by booster at 12 months in infants: open label randomised controlled trial

Author

Pace, D., primary, Khatami, A., additional, McKenna, J., additional, Campbell, D., additional, Attard-Montalto, S., additional, Birks, J., additional, Voysey, M., additional, White, C., additional, Finn, A., additional, Macloed, E., additional, Faust, S. N., additional, Kent, A. L., additional, Heath, P. T., additional, Borrow, R., additional, Snape, M. D., additional, and Pollard, A. J., additional

Published
2015
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