Your search keyword '"Agnandji, Selidji T."' showing total 11 results

1. Readiness in preventing filovirus epidemics by use of the marketed vaccines against Zaire Ebola virus disease as prototypes.

Author

Agnandji, Selidji T, Essone, Paulin N, Medaglini, Donata, and Massinga Loembe, Marguerite

Subjects

*EBOLA virus disease, *EPIDEMICS, *PREPAREDNESS, *PROTOTYPES, *VACCINES

Published

2024

2. Prostration and the prognosis of death in African children with severe malaria.

Author

Agnandji, Selidji T., Recker, Mario, Mordmüller, Benjamin, Glöckner, Stephan, Adegnika, Akim A., Lell, Bertrand, Otieno, Lucas, Otieno, Walter, Owusu-Agyei, Seth, Asante, Kwaku P., Agbenyega, Tsiri, Ansong, Daniel, Macete, Eusebio, Aide, Pedro, Sorgho, Hermann, Tinto, Halidou, Mturi, Neema, Lusingu, John P.A., Gesase, Samwel, and Hoffman, Irving

Subjects

*CHILD death, *MALARIA, *AFRICANS, *SUB-Saharan Africans, *COMA, *DISEASE risk factors

Abstract

• Prostration is associated with death from malaria in sub-Saharan African children. • Consideration of prostration increases predictive model performance. • Risk factors of mortality due to malaria show pronounced inter-study variations. • Simple risk scores are important tools for rapid clinical risk stratification. Malaria is still one of the main reasons for hospitalization in children living in sub-Saharan Africa. Rapid risk stratification at admission is essential for optimal medical care and improved prognosis. Whereas coma, deep breathing, and, to a lesser degree, severe anemia are established predictors of malaria-related death, the value of assessing prostration for risk stratification is less certain. Here we used a retrospective multi-center analysis comprising over 33,000 hospitalized children from four large studies, including two observational studies from the Severe Malaria in African Children network, a randomized controlled treatment study, and the phase-3-clinical RTS,S-malaria vaccine trial, to evaluate known risk factors of mortality and with a specific emphasis on the role of prostration. Despite comparable age profiles of the participants, we found significant inter- and intra-study variation in the incidence of fatal malaria as well as in the derived risk ratios associated with the four risk factors: coma, deep breathing, anemia, and prostration. Despite pronounced variations, prostration was significantly associated with an increased risk of mortality (P <0.001) and its consideration resulted in improved predictive performance, both in a multivariate model and a univariate model based on the Lambaréné Organ Dysfunction Score. Prostration is an important clinical criterion to determine severe pediatric malaria with possible fatal outcomes. [ABSTRACT FROM AUTHOR]

Published

2023

3. Replication, safety and immunogenicity of the vectored Ebola vaccine rVSV-ΔG-ZEBOV-GP in a sub-Saharan African paediatric population: A randomised controlled, open-label trial in children aged 1-12 years living in Lambaréné, Gabon.

Author

Alabi, Ayodele, Kokou, Kossiwa, Mahmoudou, Saidou, Kavishna, Ranmali, Nakka, Sravya S., Rothenberger, Sylvia, Musangomunei, Fungai P., Olubiyi, Bisola F., Bie-Ondo, Juste C., Kabwende, Anita L., Velavan, Thirumalaisamy P., Medaglini, Donata, Nakaya, Helder I., Engler, Olivier, Harandi, Ali M., Siegrist, Claire-Anne, Kremsner, Peter G., and Agnandji, Selidji T.

Abstract

Unlike adults, children experienced stronger and longer vector replication in plasma and shedding in saliva following rVSVΔG-ZEBOV-GP vaccination. The resulting risks of immunosuppression or immune hyperactivation leading to increased Adverse Events (AEs) and altered antibody responses are concerns that have been addressed in the present manuscript. Children aged 1–12 years living in Gabon received either rVSVΔG-ZEBOV-GP (ERVEBO®) vaccine or the varicella-zoster virus (VZV) vaccine (VZV). The concentration of rVSVΔG vector in blood and saliva, the occurrence of AEs up to day 28; the anti-rVSVΔG-ZEBOV-GP and anti-VZV IgG antibody titres, neutralising and avidity functions of anti-rVSVΔG-ZEBOV-GP by day 365; were assessed in serum. (PACTR202005733552021) In the rVSVΔG-ZEBOV-GP group, 70% and 7% of children had >0 copies/ml of rVSVΔG respectively in plasma by day 3 and in saliva by day 14 after vaccination, with no detection on day 28. Significantly higher but transient AEs occurred in the rVSVΔG-ZEBOV-GP group. Both vaccines induced seroconversion on day 28 and sustainable IgG antibody titres by day 365. Avidity and neutralisation functions of the anti-rVSVΔG-ZEBOV-GP antibodies peaked at day 28 and were maintained by day 365. The replication and shedding do not affect the favourable risk-benefit balance of the rVSVΔG-ZEBOV-GP in children. • Replication and shedding of the rVSVΔG-ZEBOV-GP vaccine not prolonged in children. • Replication-competent rVSVΔG-ZEBOV-GP induced sustainable and functional antibodies. • The rVSVΔG-ZEBOV-GP replication does not induce any unexpected adverse event. • Single dose of rVSVΔG-ZEBOV-GP is safe and immunogenic in Central African children. [ABSTRACT FROM AUTHOR]

Published

2024

4. Safety and efficacy of praziquantel in pregnant women infected with Schistosoma haematobium in Lambaréné, Gabon – Clinical results from the randomized, single-blinded, controlled freeBILy-Gabon trial.

Author

Gerstenberg, Jacob, Honkpehedji, Yabo J., Dejon-Agobe, Jean-Claude, Mahmoudou, Saidou, Recker, Mario, Mba, Romuald Beh, Maloum, Moustapha Nzamba, Lontchi, Romeo Laclong, Moure, Paul A. Nguema, Meulah, Brice, Zinsou, Jeannot F., Edoa, Jean-Ronald, Adegbite, Bayode R., Ramharter, Michael, Lell, Bertrand, Agnandji, Selidji T., Kremsner, Peter G., Corstjens, Paul L.A.M., Hoekstra, Pytsje T., and van Dam, Govert J.

Subjects

*PREGNANCY outcomes, *SCHISTOSOMA haematobium, *PREGNANT women, *RANDOMIZED controlled trials, *SCHISTOSOMIASIS

Abstract

• Praziquantel (PZQ) is well-tolerated in pregnant women with previously known side effects. • PZQ-based treatment in pregnancy shows high efficacy for cure rate and egg reduction rate. • Treatment of urogenital schistosomiasis during pregnancy improves maternal anemia. • PZQ treatment during pregnancy has no impact on the birthweight of newborns. • There were no signs of increased adverse birth outcomes following treatment. Despite evidence of praziquantel's (PZQ) safety for treating schistosomiasis in pregnancy, many countries withhold treatment. Only two randomized controlled trials have investigated PZQ in pregnancy, none involving Schistosoma haematobium. Pregnant women during the second trimester in Lambaréné (Gabon) were screened for S. haematobium infection using urine microscopy and circulating anodic antigen detection. Participants positive for either test were randomized (3:1) to single-dose PZQ 40 mg/kg during pregnancy versus no treatment during pregnancy. Investigators were blinded for allocation. Primary outcomes were reduction of egg (egg reduction rate [ERR]) and antigen production (infection reduction rate [IRR]) while explorative outcomes included assessment of cure rate, adverse events, maternal hemoglobin levels, maternal anemia prevalence at delivery, pregnancy outcomes, and newborn anthropometric parameters. Of 761 women screened 165 were eligible and randomized (intervention n = 124, control n = 41). Of them, 124 completed the study (n = 90 and n = 34, respectively). Treatment led to a significantly higher ERR (95.0% [91-97%] vs 27.0% [−42-63%]) and IRR (95% [91-97%] vs 56% [14-78%]). Common adverse events were dizziness, nausea, and vomiting. Maternal anemia at delivery was significantly lower in the intervention group (odds ratio: 0.40 [0.16;0.96], P = 0.04). No increased risk for adverse pregnancy outcomes was observed. This first randomized controlled trial investigating PZQ in pregnant women with S. haematobium found PZQ to be safe, effective, and reducing maternal anemia. We recommend treating confirmed infections to prevent morbidity in pregnant women. [ABSTRACT FROM AUTHOR]

Published

2024

5. Cortisol and susceptibility to malaria during pregnancy

Author

Bouyou-Akotet, Marielle K., Adegnika, Ayola A., Agnandji, Selidji T., Ngou-Milama, Edouard, Kombila, Maryvonne, Kremsner, Peter G., and Mavoungou, Elie

Subjects

*HYDROCORTISONE, *PREGNANCY, *MALARIA, *PROTOZOAN diseases

Abstract

Abstract: We measured cortisol and prolactin concentrations in the peripheral venous blood of 23 non-pregnant and 59 pregnant Gabonese women from the second trimester of pregnancy until delivery. Cortisol concentrations were significantly higher in primigravidae women than in multigravidae women between 20 and 25 weeks'' gestational age (166 vs. 132 ng/ml, respectively), between 28 and 37 weeks (226 vs. 161 ng/ml) and at delivery (287 vs. 188 ng/ml). Conversely, plasma prolactin levels were highest in multigravidae women. Cortisol and prolactin concentrations both increased with the period of pregnancy (P =0.01 and P <0.01, respectively), suggesting that a sustained increase in cortisol level underlies the increased susceptibility of pregnant women, particularly primigravidae women, to malaria. In support of this hypothesis, we found a significant association between cortisol concentration and Plasmodium falciparum infection, on the one hand, and strong correlations with parasite load in P. falciparum-infected primigravidae women, on the other hand (rho between 0.35 and 0.45 with P <0.01). [Copyright &y& Elsevier]

Published

2005

6. Identification of potential novel hosts and the risk of infection with lymphocytic choriomeningitis virus in humans in Gabon, Central Africa.

Author

Ushijima, Yuri, Abe, Haruka, Ozeki, Takehiro, Ondo, Georgelin N., Mbadinga, Marien J.V.M., Bikangui, Rodrigue, Nze-Nkogue, Chimène, Akomo-Okoue, Etienne F., Ella, Ghislain W.E., Koumba, Lilian B.M., Nso, Branly C.B.B., Mintsa-Nguema, Rodrigue, Makouloutou-Nzassi, Patrice, Makanga, Boris K., Nguelet, Fred L.M., Zadeh, Vahid R., Urata, Shuzo, Mbouna, Armel V.N., Massinga-Loembe, Marguerite, and Agnandji, Selidji T.

Subjects

*LYMPHOCYTIC choriomeningitis virus, *VIRAL antibodies, *ENZYME-linked immunosorbent assay, *SHREWS, *RODENTS

Abstract

• This serological study examined LCMV infection in Gabonese residents. • The overall seroprevalence was 21.5%, with adult males being at high risk. • Investigations of wildlife indicated a broader host range for LCMV. Lymphocytic choriomeningitis virus (LCMV), a human pathogenic arenavirus, is distributed worldwide. However, no human cases have been reported in Africa. This study aimed to investigate the current situation and potential risks of LCMV infection in Gabon, Central Africa. A total of 492 human samples were screened to detect LCMV genome RNA and anti-LCMV IgG antibodies using reverse transcription-quantitative PCR and enzyme-linked immunosorbent assay (ELISA), respectively. ELISA-positive samples were further examined using a neutralization assay. Viral RNAs and antibodies were also analyzed in 326 animal samples, including rodents, shrews, and bushmeat. While no LCMV RNA was detected in human samples, the overall seroprevalence was 21.5% and was significantly higher in male and adult populations. The neutralization assay identified seven samples with neutralizing activity. LCMV RNA was detected in one species of rodent (Lophuromys sikapusi) and a porcupine, and anti-LCMV IgG antibodies were detected in four rodents and three shrews. This study determined for the first time the seroprevalence of LCMV in Gabon, and revealed that local rodents, shrews, and porcupines in areas surrounding semi-urban cities posed an infection risk. Hence, LCMV infection should be considered a significant public health concern in Africa. [ABSTRACT FROM AUTHOR]

Published

2021

7. Burden of disease in Gabon caused by loiasis: a cross-sectional survey.

Author

Veletzky, Luzia, Hergeth, Jennifer, Stelzl, Daniel R, Mischlinger, Johannes, Manego, Rella Zoleko, Mombo-Ngoma, Ghyslain, McCall, Matthew B B, Adegnika, Ayôla A, Agnandji, Selidji T, Metzger, Wolfram G, Matsiegui, Pierre B, Lagler, Heimo, Mordmüller, Benjamin, Budke, Christine, and Ramharter, Michael

Subjects

*INFECTION control, *SYMPTOMS, *HELMINTHIASIS, *RURAL population, *PARASITIC diseases, *JOINT pain, *RESEARCH, *NEMATODES, *ANIMAL experimentation, *CROSS-sectional method, *RESEARCH methodology, *PUBLIC health, *DISEASES, *EVALUATION research, *MEDICAL cooperation, *COMPARATIVE studies, *FILARIASIS, *DISEASE prevalence, *ECONOMIC aspects of diseases, *LONGITUDINAL method, *QUALITY-adjusted life years

Abstract

Background: Loiasis is a highly prevalent helminth infection found in distinct regions of sub-Saharan Africa. The disease has been considered to be of minor clinical significance, but this belief is being increasingly challenged by recent evidence. We aimed to prospectively quantify the overall burden of disease caused by loiasis in an endemic region of Gabon, using disability-adjusted life years (DALYs).Methods: We did a cross-sectional survey during 2017 and 2018 in rural Gabon. Volunteers underwent diagnostic tests for loiasis and were given a standardised questionnaire on symptoms. Participants reporting eye worm migration or harbouring Loa loa microfilariae were defined as loiasis positive. Morbidity-based DALYs associated with loiasis were estimated for the rural population of Gabon.Findings: Between Sept 1, 2017 and May 31, 2018, 1235 participants residing in 38 villages in the Gabonese departments of Tsamba-Magotsi and Ogooué et des Lacs were screened. 626 (50·8%) of 1232 eligible participants had loiasis. 520 (42·2%) of 1232 participants reported eye worm migration. 478 (93·9%) of 509 individuals with eye worm migration also reported associated pain, and 397 (78·6%) of 505 reported vision disturbances. After correcting for age and sex, loiasis was significantly associated with a variety of symptoms, including transient painful oedema (adjusted odds ratio 1·76 [95% CI 1·37-2·26]) and arthralgia (1·30 [1·01-1·69]). Application of attributable fractions of correlating symptoms resulted in 412·9 (95% CI 273·9-567·7) morbidity-based DALYs per 100 000 people in rural Gabon.Interpretation: Loiasis, with the pathognomonic sign of eye worm migration, appears to not be benign, but severely impeding to affected individuals. Furthermore, loiasis is associated with substantial morbidity, comparable to that of other neglected tropical parasitic diseases. These findings call for reconsideration of L loa as a relevant pathogen in affected populations, with a need for more concerted research and control of these infections.Funding: Federal Ministry of Science, Research and Economy of Austria, and the European Union. [ABSTRACT FROM AUTHOR]

Published

2020

8. Re-emergence of dengue virus serotype 3 infections in Gabon in 2016–2017, and evidence for the risk of repeated dengue virus infections.

Author

Abe, Haruka, Ushijima, Yuri, Loembe, Marguerite M., Bikangui, Rodrigue, Nguema-Ondo, Georgelin, Mpingabo, Patrick I., Zadeh, Vahid R., Pemba, Christelle M., Kurosaki, Yohei, Igasaki, Yui, de Vries, Sophia G., Grobusch, Martin P., Agnandji, Selidji T., Lell, Bertrand, and Yasuda, Jiro

Subjects

*DENGUE viruses, *VIRUS diseases, *INFECTION, *DENGUE, *NUCLEOTIDE sequencing

Abstract

• Dengue virus serotype 3 (DENV-3) was detected in febrile patients in Gabon. • Most of the DENV-3-positive patients were also positive for anti-DENV IgG. • The phylogenetic analysis inferred that DENV-3 has been stably maintained in Gabon. • Whole-genome sequencing of DENV-3 revealed a number of amino acid substitutions. Dengue outbreaks, mainly caused by dengue virus serotype 2 (DENV-2), occurred in 2007 and in 2010 in Gabon, Central Africa. However, information on DENV infections has been insufficient since 2010. The aim of this study was to investigate the current DENV infection scenario and the risk of repeated infections in Gabon. During 2015–2017, serum samples were collected from enrolled febrile participants and were tested for DENV infection using RT-qPCR. DENV-positive samples were analyzed for a history of previous DENV infection(s) using ELISA. The complete DENV genome was sequenced to analyze the phylogeny of Gabonese DENV strains. DENV-3 was exclusively detected, with a high rate of anti-DENV IgG seropositivity among DENV-3-positive participants. DENV-3 showed higher infection rates in adults and the infection was seasonal with peaks in the rainy seasons. Phylogenetic analysis revealed that Gabonese DENV-3 originated from West African strains and has been circulating continuously in Gabon since at least 2010, when the first DENV-3 case was reported. These findings indicate stable DENV-3 circulation and the risk of repeated DENV infections in Gabon, highlighting the need for continuous monitoring to control DENV infections. [ABSTRACT FROM AUTHOR]

Published

2020

9. Immunogenicity of the RTS,S/AS01 malaria vaccine and implications for duration of vaccine efficacy: secondary analysis of data from a phase 3 randomised controlled trial.

Author

White, Michael T, Verity, Robert, Griffin, Jamie T, Asante, Kwaku Poku, Owusu-Agyei, Seth, Greenwood, Brian, Drakeley, Chris, Gesase, Samwel, Lusingu, John, Ansong, Daniel, Adjei, Samuel, Agbenyega, Tsiri, Ogutu, Bernhards, Otieno, Lucas, Otieno, Walter, Agnandji, Selidji T, Lell, Bertrand, Kremsner, Peter, Hoffman, Irving, and Martinson, Francis

Subjects

*MALARIA, *VACCINE effectiveness, *RANDOMIZED controlled trials, *CIRCUMSPOROZOITE protein, *TARGETED drug delivery, *PLASMODIUM falciparum, *PREVENTION, *VACCINATION, *MALARIA prevention, *CLINICAL medicine, *CLINICAL trials, *COMPARATIVE studies, *IMMUNIZATION, *IMMUNOGENETICS, *IMMUNOGLOBULINS, *RESEARCH methodology, *EVALUATION of medical care, *MEDICAL cooperation, *PROTEINS, *PROTOZOA, *RESEARCH, *RESEARCH funding, *VACCINES, *EVALUATION research, *TREATMENT effectiveness, *DISEASE incidence, *CHEMICAL inhibitors

Abstract

Background: The RTS,S/AS01 malaria vaccine targets the circumsporozoite protein, inducing antibodies associated with the prevention of Plasmodium falciparum infection. We assessed the association between anti-circumsporozoite antibody titres and the magnitude and duration of vaccine efficacy using data from a phase 3 trial done between 2009 and 2014.Methods: Using data from 8922 African children aged 5-17 months and 6537 African infants aged 6-12 weeks at first vaccination, we analysed the determinants of immunogenicity after RTS,S/AS01 vaccination with or without a booster dose. We assessed the association between the incidence of clinical malaria and anti-circumsporozoite antibody titres using a model of anti-circumsporozoite antibody dynamics and the natural acquisition of protective immunity over time.Findings: RTS,S/AS01-induced anti-circumsporozoite antibody titres were greater in children aged 5-17 months than in those aged 6-12 weeks. Pre-vaccination anti-circumsporozoite titres were associated with lower immunogenicity in children aged 6-12 weeks and higher immunogenicity in those aged 5-17 months. The immunogenicity of the booster dose was strongly associated with immunogenicity after primary vaccination. Anti-circumsporozoite titres wane according to a biphasic exponential distribution. In participants aged 5-17 months, the half-life of the short-lived component of the antibody response was 45 days (95% credible interval 42-48) and that of the long-lived component was 591 days (557-632). After primary vaccination 12% (11-13) of the response was estimated to be long-lived, rising to 30% (28-32%) after a booster dose. An anti-circumsporozoite antibody titre of 121 EU/mL (98-153) was estimated to prevent 50% of infections. Waning anti-circumsporozoite antibody titres predict the duration of efficacy against clinical malaria across different age categories and transmission intensities, and efficacy wanes more rapidly at higher transmission intensity.Interpretation: Anti-circumsporozoite antibody titres are a surrogate of protection for the magnitude and duration of RTS,S/AS01 efficacy, with or without a booster dose, providing a valuable surrogate of effectiveness for new RTS,S formulations in the age groups considered.Funding: UK Medical Research Council. [ABSTRACT FROM AUTHOR]

Published

2015

10. Epidemiology of Human Herpes Virus 8 in Pregnant Women and their Newborns - A cross-sectional delivery survey in Central Gabon.

Author

Capan-Melser, Mesküre, Mombo-Ngoma, Ghyslain, Akerey-Diop, Daisy, Basra, Arti, Manego-Zoleko, Rella, Würbel, Heike, Lötsch, Felix, Groger, Mirjam, Skoll, Michael, Schwing, Julia, Schipulle, Ulla, Matsiegui, Pierre-Blaise, González, Raquel, Menendez, Clara, Kremsner, Peter G., Adegnika, Ayôla A., Agnandji, Selidji T., and Ramharter, Michael

Subjects

*HERPESVIRUS diseases, *PREGNANCY complications, *DISEASE prevalence, *NEONATAL diseases, *CROSS-sectional method, *PATIENTS

Abstract

Summary Objectives On the background of a high prevalence of HHV-8 infection in pre-pubertal Central African children, this study investigated the potential for in utero transmission of HHV-8. Patients Gabonese pregnant women were invited to provide peripheral and cord blood samples for serological and PCR diagnostics of HHV-8 infection at delivery for this cross-sectional survey. Results Out of 344 participants 120 (35%, 95% CI: 30-40%) were serologically positive for HHV-8. 31% (95% CI: 22-40%) of cord blood samples of seropositive women had detectable IgG antibodies. Among all seropositive participants HHV-8 was detected by PCR in one maternal peripheral blood sample at delivery (1%, 95% CI: 0.2-7%) and in none of cord blood samples. There was no association between demographic characteristics and infection status. Similarly, there was no difference in risk for premature delivery, low birth weight, and maternal anaemia in HHV-8 seropositive women. Discussion These data suggest a high seroprevalence of HHV-8 infection in pregnant women, however viraemia at delivery does not commonly occur in Central Africa. Based on these observations it may be speculated that infection of children may occur more commonly either antepartum or later on in infancy and childhood. [ABSTRACT FROM AUTHOR]

Published

2015

11. Efficacy of RTS,S malaria vaccines: individual-participant pooled analysis of phase 2 data.

Author

Bejon, Philip, White, Michael T, Olotu, Ally, Bojang, Kalifa, Lusingu, John PA, Salim, Nahya, Otsyula, Nekoye N, Agnandji, Selidji T, Asante, Kwaku Poku, Owusu-Agyei, Seth, Abdulla, Salim, and Ghani, Azra C

Subjects

*MALARIA vaccines, *CLINICAL trials, *MALARIA treatment, *DRUG efficacy, *REGRESSION analysis, *PUBLIC health

Abstract

Summary: Background: The efficacy of RTS,S/AS01 as a vaccine for malaria is being tested in a phase 3 clinical trial. Early results show significant, albeit partial, protection against clinical malaria and severe malaria. To ascertain variations in vaccine efficacy according to covariates such as transmission intensity, choice of adjuvant, age at vaccination, and bednet use, we did an individual-participant pooled analysis of phase 2 clinical data. Methods: We analysed data from 11 different sites in Africa, including 4453 participants. We measured heterogeneity in vaccine efficacy by estimating the interactions between covariates and vaccination in pooled multivariable Cox regression and Poisson regression analyses. Endpoints for measurement of vaccine efficacy were infection, clinical malaria, severe malaria, and death. We defined transmission intensity levels according to the estimated local parasite prevalence in children aged 2–10 years (PrP2–10), ranging from 5% to 80%. Choice of adjuvant was either AS01 or AS02. Findings: Vaccine efficacy against all episodes of clinical malaria varied by transmission intensity (p=0·001). At low transmission (PrP2–10 10%) vaccine efficacy was 60% (95% CI 54 to 67), at moderate transmission (PrP2–10 20%) it was 41% (21 to 57), and at high transmission (PrP2–10 70%) the efficacy was 4% (−10 to 22). Vaccine efficacy also varied by adjuvant choice (p<0·0001)—eg, at low transmission (PrP2–10 10%), efficacy varied from 60% (95% CI 54 to 67) for AS01 to 47% (14 to 75) for AS02. Variations in efficacy by age at vaccination were of borderline significance (p=0·038), and bednet use and sex were not significant covariates. Vaccine efficacy (pooled across adjuvant choice and transmission intensity) varied significantly (p<0·0001) according to time since vaccination, from 36% efficacy (95% CI 24 to 45) at time of vaccination to 0% (−38 to 38) after 3 years. Interpretation: Vaccine efficacy against clinical disease was of limited duration and was not detectable 3 years after vaccination. Furthermore, efficacy fell with increasing transmission intensity. Outcomes after vaccination cannot be gauged accurately on the basis of one pooled efficacy figure. However, predictions of public-health outcomes of vaccination will need to take account of variations in efficacy by transmission intensity and by time since vaccination. Funding: Medical Research Council (UK); Bill & Melinda Gates Foundation Vaccine Modelling Initiative; Wellcome Trust. [ABSTRACT FROM AUTHOR]

Published

2013