Your search keyword '"Tamboura, B"' showing total 72 results

1. EVALUATION DE LA QUALITE DE VIE APRES MASTECTOMIE POUR CANCER DU SEIN AU CHU GABRIEL TOURE.

Author

Doumbia, S., Traoré, S. O., Kané, M. B., Pamateck, S., Sanogo, S. A., Saye, Z., Doumbia, A. A., Karembé, B., Tounkara, I., Sylla, N., Tamboura, B., Camara, A., Yomaté, A., Fané, S., Yomane, J. R., Diarra, B., Traoré, Y., Schantz, C., Guindo, S., and Téguété, I.

Abstract

Copyright of Mali Médical is the property of Mali Medical, Faculte de Medecine, de Pharmacie et d'Odonto-stomatologie and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2024

2. Antistatic polymeric materials

Author

Yudaev, P.A., primary, Tamboura, B., additional, and Chistyakov, E.M., additional

Published

2023

3. Diarrhoeal disease and subsequent risk of death in infants and children residing in low-income and middle-income countries: analysis of the GEMS case-control study and 12-month GEMS-1A follow-on study

Author

Levine, MM, Nasrin, D, Acacio, S, Bassat, Q, Powell, H, Tennant, SM, Sow, SO, Sur, D, Zaidi, AKM, Faruque, ASG, Hossain, MJ, Alonso, PL, Breiman, RF, O'Reilly, CE, Mintz, ED, Omore, R, Ochieng, JB, Oundo, JO, Tamboura, B, Sanogo, D, Onwuchekwa, U, Manna, B, Ramamurthy, T, Kanungo, S, Ahmed, S, Qureshi, S, Quadri, F, Hossain, A, Das, SK, Antonio, M, Saha, D, Mandomando, I, Blackwelder, WC, Farag, T, Wu, Y, Houpt, ER, Verweiij, JJ, Sommerfelt, H, Nataro, JP, Robins-Browne, RM, Kotloff, KL, Levine, MM, Nasrin, D, Acacio, S, Bassat, Q, Powell, H, Tennant, SM, Sow, SO, Sur, D, Zaidi, AKM, Faruque, ASG, Hossain, MJ, Alonso, PL, Breiman, RF, O'Reilly, CE, Mintz, ED, Omore, R, Ochieng, JB, Oundo, JO, Tamboura, B, Sanogo, D, Onwuchekwa, U, Manna, B, Ramamurthy, T, Kanungo, S, Ahmed, S, Qureshi, S, Quadri, F, Hossain, A, Das, SK, Antonio, M, Saha, D, Mandomando, I, Blackwelder, WC, Farag, T, Wu, Y, Houpt, ER, Verweiij, JJ, Sommerfelt, H, Nataro, JP, Robins-Browne, RM, and Kotloff, KL

Abstract

BACKGROUND: The Global Enteric Multicenter Study (GEMS) was a 3-year case-control study that measured the burden, aetiology, and consequences of moderate-to-severe diarrhoea (MSD) in children aged 0-59 months. GEMS-1A, a 12-month follow-on study, comprised two parallel case-control studies, one assessing MSD and the other less-severe diarrhoea (LSD). In this report, we analyse the risk of death with each diarrhoea type and the specific pathogens associated with fatal outcomes. METHODS: GEMS was a prospective, age-stratified, matched case-control study done at seven sites in Africa and Asia. Children aged 0-59 months with MSD seeking care at sentinel health centres were recruited along with one to three randomly selected matched community control children without diarrhoea. In the 12-month GEMS-1A follow-on study, children with LSD and matched controls, in addition to children with MSD and matched controls, were recruited at six of the seven sites; only cases of MSD and controls were enrolled at the seventh site. We compared risk of death during the period between enrolment and one follow-up household visit done about 60 days later (range 50-90 days) in children with MSD and LSD and in their respective controls. Approximately 50 pathogens were detected using, as appropriate, classic bacteriology, immunoassays, gel-based PCR and reverse transcriptase PCR, and quantitative real-time PCR (qPCR). Specimens from a subset of GEMS cases and controls were also tested by a TaqMan Array Card that compartmentalised probe-based qPCR for 32 enteropathogens. FINDINGS: 223 (2·0%) of 11 108 children with MSD and 43 (0·3%) of 16 369 matched controls died between study enrolment and the follow-up visit at about 60 days (hazard ratio [HR] 8·16, 95% CI 5·69-11·68, p<0·0001). 12 (0·4%) of 2962 children with LSD and seven (0·2%) of 4074 matched controls died during the follow-up period (HR 2·78, 95% CI 0·95-8·11, p=0·061). Risk of death was lower in children with dysenteric MSD than in ch

Published

2020

4. Colonization factors among enterotoxigenic Escherichia coli isolates from children with moderate-to-severe diarrhea and from matched controls in the Global Enteric Multicenter Study (GEMS)

Author

Torres, AG, Vidal, RM, Muhsen, K, Tennant, SM, Svennerholm, A-M, Sow, SO, Sur, D, Zaidi, AKM, Faruque, ASG, Saha, D, Adegbola, R, Hossain, MJ, Alonso, PL, Breiman, RF, Bassat, Q, Tamboura, B, Sanogo, D, Onwuchekwa, U, Manna, B, Ramamurthy, T, Kanungo, S, Ahmed, S, Qureshi, S, Quadri, F, Hossain, A, Das, SK, Antonio, M, Mandomando, I, Nhampossa, T, Acacio, S, Omore, R, Ochieng, JB, Oundo, JO, Mintz, ED, O'Reilly, CE, Berkeley, LY, Livio, S, Panchalingam, S, Nasrin, D, Farag, TH, Wu, Y, Sommerfelt, H, Robins-Browne, RM, Del Canto, F, Hazen, TH, Rasko, DA, Kotloff, KL, Nataro, JP, Levine, MM, Torres, AG, Vidal, RM, Muhsen, K, Tennant, SM, Svennerholm, A-M, Sow, SO, Sur, D, Zaidi, AKM, Faruque, ASG, Saha, D, Adegbola, R, Hossain, MJ, Alonso, PL, Breiman, RF, Bassat, Q, Tamboura, B, Sanogo, D, Onwuchekwa, U, Manna, B, Ramamurthy, T, Kanungo, S, Ahmed, S, Qureshi, S, Quadri, F, Hossain, A, Das, SK, Antonio, M, Mandomando, I, Nhampossa, T, Acacio, S, Omore, R, Ochieng, JB, Oundo, JO, Mintz, ED, O'Reilly, CE, Berkeley, LY, Livio, S, Panchalingam, S, Nasrin, D, Farag, TH, Wu, Y, Sommerfelt, H, Robins-Browne, RM, Del Canto, F, Hazen, TH, Rasko, DA, Kotloff, KL, Nataro, JP, and Levine, MM

Abstract

BACKGROUND: Enterotoxigenic Escherichia coli (ETEC) encoding heat-stable enterotoxin (ST) alone or with heat-labile enterotoxin (LT) cause moderate-to-severe diarrhea (MSD) in developing country children. The Global Enteric Multicenter Study (GEMS) identified ETEC encoding ST among the top four enteropathogens. Since the GEMS objective was to provide evidence to guide development and implementation of enteric vaccines and other interventions to diminish diarrheal disease morbidity and mortality, we examined colonization factor (CF) prevalence among ETEC isolates from children age <5 years with MSD and from matched controls in four African and three Asian sites. We also assessed strength of association of specific CFs with MSD. METHODOLOGY/PRINCIPAL FINDINGS: MSD cases enrolled at healthcare facilities over three years and matched controls were tested in a standardized manner for many enteropathogens. To identify ETEC, three E. coli colonies per child were tested by polymerase chain reaction (PCR) to detect genes encoding LT, ST; confirmed ETEC were examined by PCR for major CFs (Colonization Factor Antigen I [CFA/I] or Coli Surface [CS] antigens CS1-CS6) and minor CFs (CS7, CS12, CS13, CS14, CS17, CS18, CS19, CS20, CS21, CS30). ETEC from 806 cases had a single toxin/CF profile in three tested strains per child. Major CFs, components of multiple ETEC vaccine candidates, were detected in 66.0% of LT/ST and ST-only cases and were associated with MSD versus matched controls by conditional logistic regression (p≤0.006); major CFs detected in only 25.0% of LT-only cases weren't associated with MSD. ETEC encoding exclusively CS14, identified among 19.9% of 291 ST-only and 1.5% of 259 LT/ST strains, were associated with MSD (p = 0.0011). No other minor CF exhibited prevalence ≥5% and significant association with MSD. CONCLUSIONS/SIGNIFICANCE: Major CF-based efficacious ETEC vaccines could potentially prevent up to 66% of pediatric MSD cases due to ST-encoding ETEC in develo

Published

2019

5. The incidence, aetiology, and adverse clinical consequences of less severe diarrhoeal episodes among infants and children residing in low-income and middle-income countries: a 12-month case-control study as a follow-on to the Global Enteric Multicenter Study (GEMS)

Author

Kotloff, KL, Nasrin, D, Blackwelder, WC, Wu, Y, Farag, T, Panchalingham, S, Sow, SO, Sur, D, Zaidi, AKM, Faruque, ASG, Saha, D, Alonso, PL, Tamboura, B, Sanogo, D, Onwuchekwa, U, Manna, B, Ramamurthy, T, Kanungo, S, Ahmed, S, Qureshi, S, Quadri, F, Hossain, A, Das, SK, Antonio, M, Hossain, MJ, Mandomando, I, Acacio, S, Biswas, K, Tennant, SM, Verweij, JJ, Sommerfelt, H, Nataro, JP, Robins-Browne, RM, Levine, MM, Kotloff, KL, Nasrin, D, Blackwelder, WC, Wu, Y, Farag, T, Panchalingham, S, Sow, SO, Sur, D, Zaidi, AKM, Faruque, ASG, Saha, D, Alonso, PL, Tamboura, B, Sanogo, D, Onwuchekwa, U, Manna, B, Ramamurthy, T, Kanungo, S, Ahmed, S, Qureshi, S, Quadri, F, Hossain, A, Das, SK, Antonio, M, Hossain, MJ, Mandomando, I, Acacio, S, Biswas, K, Tennant, SM, Verweij, JJ, Sommerfelt, H, Nataro, JP, Robins-Browne, RM, and Levine, MM

Abstract

BACKGROUND: Diarrheal diseases remain a leading cause of illness and death among children younger than 5 years in low-income and middle-income countries. The Global Enteric Multicenter Study (GEMS) has described the incidence, aetiology, and sequelae of medically attended moderate-to-severe diarrhoea (MSD) among children aged 0-59 months residing in censused populations in sub-Saharan Africa and south Asia, where most child deaths occur. To further characterise this disease burden and guide interventions, we extended this study to include children with episodes of less-severe diarrhoea (LSD) seeking care at health centres serving six GEMS sites. METHODS: We report a 1-year, multisite, age-stratified, matched case-control study following on to the GEMS study. Six sites (Bamako, Mali; Manhiça, Mozambique; Basse, The Gambia; Mirzapur, Bangladesh; Kolkata, India; and Bin Qasim Town, Karachi, Pakistan) participated in this study. Children aged 0-59 months at each site who sought care at a sentinel hospital or health centre during a 12-month period were screened for diarrhoea. New (onset after ≥7 diarrhoea-free days) and acute (onset within the previous 7 days) episodes of diarrhoea in children who had sunken eyes, whose skin lost turgor, who received intravenous hydration, who had dysentery, or who were hospitalised were eligible for inclusion as MSD. The remaining new and acute diarrhoea episodes among children who sought care at the same health centres were considered LSD. We aimed to enrol the first eight or nine eligible children with MSD and LSD at each site during each fortnight in three age strata: infants (aged 0-11 months), toddlers (aged 12-23 months), and young children (aged 24-59 months). For each included case of MSD or LSD, we enrolled one to three community control children without diarrhoea during the previous 7 days. From patients and controls we collected clinical and epidemiological data, anthropometric measurements, and faecal samples to identify ent

Published

2019

6. Maternal influenza vaccination and the risk of laboratory-confirmed influenza among household contacts under the age of five in Mali

Author

Buchwald, A., primary, Booth, A., additional, Tamboura, B., additional, Haidara, F., additional, Coulibaly, F., additional, Diallo, F., additional, Sow, S., additional, Blackwelder, W., additional, Kotloff, K., additional, Levine, M., additional, and Tapia, M., additional

Published

2018

7. Association of C-reactive protein with bacterial and respiratory syncytial virus-associated pneumonia among children aged <5 years in the PERCH study

Author

Higdon, M.M. (Melissa M.), Le, T. (Tham), O'Brien, K.L. (Katherine L.), Murdoch, D.R. (David R.), Prosperi, C. (Christine), Baggett, H.C. (Henry C.), Brooks, W.A. (W. Abdullah), Feikin, D.R. (Daniel R.), Hammitt, L.L. (Laura L.), Howie, S.R.C. (Stephen R.C.), Kotloff, K.L. (Karen L.), Levine, O.S. (Orin S.), Scott, J.A.G. (J. Anthony G.), Thea, D.M. (Donald M.), Awori, J.O. (Juliet O.), Baillie, V.L. (Vicky L.), Cascio, S. (Stephanie), Chuananon, S. (Somchai), DeLuca, A.N. (Andrea N.), Driscoll, A.J. (Amanda J.), Ebruke, B.E. (Bernard E.), Endtz, H.P. (Hubert), Kaewpan, A. (Anek), Kahn, G. (Geoff), Karani, A. (Angela), Karron, R. (Ruth), Moore, D.P. (David P.), Park, D.E. (Daniel E.), Rahman, M.Z. (Mohammed Ziaur), Salaudeen, R. (Rasheed), Seidenberg, P. (Phil), Somwe, S.W. (Somwe Wa), Sylla, M. (Mamadou), Tapia, M.D. (Milagritos D.), Zeger, S.L. (Scott L.), Knoll, M.D. (Maria Deloria), Madhi, S.A. (Shabir A.), Fancourt, N. (Nicholas), Fu, W. (Wei), Kagucia, E.W. (E. Wangeci), Li, M. (Mengying), Wu, Z. (Zhenke), Watson, N.L. (Nora L.), Crawley, J. (Jane), Zaman, K. (Khalequ), Goswami, D. (Doli), Hossain, L. (Lokman), Jahan, Y. (Yasmin), Ashraf, H. (Hasan), Antonio, M. (Martin), McLellan, J. (Jessica), Machuka, E. (Eunice), Shamsul, A. (Arifin), Zaman, S.M.A. (Syed M.A.), Mackenzie, G. (Grant), Morpeth, S.C. (Susan C.), Kamau, A. (Alice), Kazungu, S. (Sidi), Ominde, M.S. (Micah Silaba), Sow, S.O. (Samba O.), Tamboura, B. (Boubou), Onwuchekwa, U. (Uma), Kourouma, N. (Nana), Toure, A. (Aliou), Adrian, P.V. (Peter), Kuwanda, L. (Locadiah), Mudau, A. (Azwifarwi), Groome, M.J. (Michelle J.), Mahomed, N. (Nasreen), Thamthitiwat, S. (Somsak), Maloney, S.A. (Susan A.), Bunthi, C. (Charatdao), Rhodes, J. (Julia), Sawatwong, P. (Pongpun), Akarasewi, P. (Pasakorn), Mwananyanda, L. (Lawrence), Chipeta, J. (James), Mwansa, J. (James), Kwenda, G. (Geoffrey), Anderson, T.P. (Trevor P.), Mitchell, J. (Joanne), Higdon, M.M. (Melissa M.), Le, T. (Tham), O'Brien, K.L. (Katherine L.), Murdoch, D.R. (David R.), Prosperi, C. (Christine), Baggett, H.C. (Henry C.), Brooks, W.A. (W. Abdullah), Feikin, D.R. (Daniel R.), Hammitt, L.L. (Laura L.), Howie, S.R.C. (Stephen R.C.), Kotloff, K.L. (Karen L.), Levine, O.S. (Orin S.), Scott, J.A.G. (J. Anthony G.), Thea, D.M. (Donald M.), Awori, J.O. (Juliet O.), Baillie, V.L. (Vicky L.), Cascio, S. (Stephanie), Chuananon, S. (Somchai), DeLuca, A.N. (Andrea N.), Driscoll, A.J. (Amanda J.), Ebruke, B.E. (Bernard E.), Endtz, H.P. (Hubert), Kaewpan, A. (Anek), Kahn, G. (Geoff), Karani, A. (Angela), Karron, R. (Ruth), Moore, D.P. (David P.), Park, D.E. (Daniel E.), Rahman, M.Z. (Mohammed Ziaur), Salaudeen, R. (Rasheed), Seidenberg, P. (Phil), Somwe, S.W. (Somwe Wa), Sylla, M. (Mamadou), Tapia, M.D. (Milagritos D.), Zeger, S.L. (Scott L.), Knoll, M.D. (Maria Deloria), Madhi, S.A. (Shabir A.), Fancourt, N. (Nicholas), Fu, W. (Wei), Kagucia, E.W. (E. Wangeci), Li, M. (Mengying), Wu, Z. (Zhenke), Watson, N.L. (Nora L.), Crawley, J. (Jane), Zaman, K. (Khalequ), Goswami, D. (Doli), Hossain, L. (Lokman), Jahan, Y. (Yasmin), Ashraf, H. (Hasan), Antonio, M. (Martin), McLellan, J. (Jessica), Machuka, E. (Eunice), Shamsul, A. (Arifin), Zaman, S.M.A. (Syed M.A.), Mackenzie, G. (Grant), Morpeth, S.C. (Susan C.), Kamau, A. (Alice), Kazungu, S. (Sidi), Ominde, M.S. (Micah Silaba), Sow, S.O. (Samba O.), Tamboura, B. (Boubou), Onwuchekwa, U. (Uma), Kourouma, N. (Nana), Toure, A. (Aliou), Adrian, P.V. (Peter), Kuwanda, L. (Locadiah), Mudau, A. (Azwifarwi), Groome, M.J. (Michelle J.), Mahomed, N. (Nasreen), Thamthitiwat, S. (Somsak), Maloney, S.A. (Susan A.), Bunthi, C. (Charatdao), Rhodes, J. (Julia), Sawatwong, P. (Pongpun), Akarasewi, P. (Pasakorn), Mwananyanda, L. (Lawrence), Chipeta, J. (James), Mwansa, J. (James), Kwenda, G. (Geoffrey), Anderson, T.P. (Trevor P.), and Mitchell, J. (Joanne)

Abstract

Background. Lack of a gold standard for identifying bacterial and viral etiologies of pneumonia has limited evaluation of C-reactive protein (CRP) for identifying bacterial pneumonia. We evaluated the sensitivity and specificity of CRP for identifying bacterial vs respiratory syncytial virus (RSV) pneumonia in the Pneumonia Etiology Research for Child Health (PERCH) multicenter case-control study. Methods. We measured serum CRP levels in cases with World Health Organization-defined severe or very severe pneumonia and a subset of community controls. We evaluated the sensitivity and specificity of elevated CRP for "confirmed" bacterial pneumonia (positive blood culture or positive lung aspirate or pleural fluid culture or polymerase chain reaction [PCR]) compared to "RSV pneumonia" (nasopharyngeal/oropharyngeal or induced sputum PCR-positive without confirmed/suspected bacterial pneumonia). Receiver operating characteristic (ROC) curves were constructed to assess the performance of elevated CRP in distinguishing these cases. Results. Among 601 human immunodeficiency virus (HIV)-negative tested controls, 3% had CRP ≥40 mg/L. Among 119 HIVnegative cases with confirmed bacterial pneumonia, 77% had CRP ≥40 mg/L compared with 17% of 556 RSV pneumonia cases. The ROC analysis produced an area under the curve of 0.87, indicating very good discrimination; a cut-point of 37.1 mg/L best discriminated confirmed bacterial pneumonia (sensitivity 77%) from RSV pneumonia (specificity 82%). CRP ≥100 mg/L substantially improved specificity over CRP ≥40 mg/L, though at a loss to sensitivity. Conclusions. Elevated CRP was positively associated with confirmed bacterial pneumonia and negatively associated with RSV pneumonia in PERCH. CRP may be useful for distinguishing bacterial from RSV-associated pneumonia, although its role in discriminating against other respiratory viral-associated pneumonia needs further study.

Published

2017

8. Standardization of laboratory methods for the PERCH study

Author

Driscoll, A.J. (Amanda J.), Karron, R. (Ruth), Morpeth, S.C. (Susan C.), Bhat, N. (Niranjan), Levine, O.S. (Orin S.), Baggett, H.C. (Henry C.), Brooks, W.A. (W. Abdullah), Feikin, D.R. (Daniel R.), Hammitt, L.L. (Laura L.), Howie, S.R.C. (Stephen R. C.), Knoll, M.D. (Maria Deloria), Kotloff, K.L. (Karen L.), Madhi, S.A. (Shabir A.), Scott, J.A.G. (J. Anthony G.), Thea, D.M. (Donald M.), Adrian, P.V. (Peter), Ahmed, D. (Dilruba), Alam, M. (Muntasir), Anderson, T.P. (Trevor P.), Antonio, M. (Martin), Baillie, V.L. (Vicky L.), Dione, M. (Michel), Endtz, H.P. (Hubert), Gitahi, C. (Caroline), Karani, A. (Angela), Kwenda, G. (Geoffrey), Maiga, A.A. (Abdoul Aziz), McClellan, J. (Jessica), Mitchell, J.L. (Joanne L.), Morailane, P. (Palesa), Mugo, D. (Daisy), Mwaba, J. (John), Mwansa, J. (James), Mwarumba, S. (Salim), Nyongesa, S. (Sammy), Panchalingam, S. (Sandra), Rahman, M. (Mustafizur), Sawatwong, P. (Pongpun), Tamboura, B. (Boubou), Toure, A. (Aliou), Whistler, T. (Toni), O'Brien, K.L. (Katherine L.), Murdoch, D.R. (David R.), Driscoll, A.J. (Amanda J.), Karron, R. (Ruth), Morpeth, S.C. (Susan C.), Bhat, N. (Niranjan), Levine, O.S. (Orin S.), Baggett, H.C. (Henry C.), Brooks, W.A. (W. Abdullah), Feikin, D.R. (Daniel R.), Hammitt, L.L. (Laura L.), Howie, S.R.C. (Stephen R. C.), Knoll, M.D. (Maria Deloria), Kotloff, K.L. (Karen L.), Madhi, S.A. (Shabir A.), Scott, J.A.G. (J. Anthony G.), Thea, D.M. (Donald M.), Adrian, P.V. (Peter), Ahmed, D. (Dilruba), Alam, M. (Muntasir), Anderson, T.P. (Trevor P.), Antonio, M. (Martin), Baillie, V.L. (Vicky L.), Dione, M. (Michel), Endtz, H.P. (Hubert), Gitahi, C. (Caroline), Karani, A. (Angela), Kwenda, G. (Geoffrey), Maiga, A.A. (Abdoul Aziz), McClellan, J. (Jessica), Mitchell, J.L. (Joanne L.), Morailane, P. (Palesa), Mugo, D. (Daisy), Mwaba, J. (John), Mwansa, J. (James), Mwarumba, S. (Salim), Nyongesa, S. (Sammy), Panchalingam, S. (Sandra), Rahman, M. (Mustafizur), Sawatwong, P. (Pongpun), Tamboura, B. (Boubou), Toure, A. (Aliou), Whistler, T. (Toni), O'Brien, K.L. (Katherine L.), and Murdoch, D.R. (David R.)

Abstract

The Pneumonia Etiology Research for Child Health study was conducted across diverse research sites and relied on standardized clinical and laboratory methods for the accurate and meaningful interpretation of pneumonia etiology data. Blood, respiratory specimens, and urine were collected from children aged 1-5months hospitalized with severe or very severe pneumonia and community controls of the same age without severe pneumonia and were tested with an extensive array of laboratory diagnostic tests. A standardized testing algorithm and standard operating procedures were applied across all study sites. Site laboratories received uniform training, equipment, and reagents for core testing methods. Standardization was further assured by routine teleconferences, in-person meetings, site monitoring visits, and internal a

Published

2017

9. Standardization of Laboratory Methods for the PERCH Study

Author

Driscoll, AJ, Karron, RA, Morpeth, SC, Bhat, N, Levine, OS, Baggett, HC, Brooks, WA, Feikin, DR, Hammitt, LL, Howie, SRC, Knoll, MD, Kotloff, KL, Madhi, SA, Scott, JAG, Thea, DM, Adrian, PV, Ahmed, D, Alam, M, Anderson, TP, Antonio, M, Baillie, VL, Dione, M, Endtz, Hubert, Gitahi, C, Karani, A, Kwenda, G, Maiga, AA, McClellan, J, Mitchell, JL, Morailane, P, Mugo, D, Mwaba, J, Mwansa, J, Mwarumba, S, Nyongesa, S, Panchalingam, S, Rahman, M, Sawatwong, P, Tamboura, B, Toure, A, Whistler, T, O'Brien, KL, Murdoch, DR, Driscoll, AJ, Karron, RA, Morpeth, SC, Bhat, N, Levine, OS, Baggett, HC, Brooks, WA, Feikin, DR, Hammitt, LL, Howie, SRC, Knoll, MD, Kotloff, KL, Madhi, SA, Scott, JAG, Thea, DM, Adrian, PV, Ahmed, D, Alam, M, Anderson, TP, Antonio, M, Baillie, VL, Dione, M, Endtz, Hubert, Gitahi, C, Karani, A, Kwenda, G, Maiga, AA, McClellan, J, Mitchell, JL, Morailane, P, Mugo, D, Mwaba, J, Mwansa, J, Mwarumba, S, Nyongesa, S, Panchalingam, S, Rahman, M, Sawatwong, P, Tamboura, B, Toure, A, Whistler, T, O'Brien, KL, and Murdoch, DR

Published

2017

10. Pharyngeal carriage of Neisseria species in the African meningitis belt

Author

Diallo, K, Maiden, M, Bennett, J, Rebbetts, L, Watkins, E, Trotter, C, Timbine, Y, Tamboura, B, Sow, S, Issaka, B, Dano, I, Collard, J, Dieng, M, Diallo, A, Mihret, A, Ali, O, Aseffa, A, Quaye, S, Bugri, A, Osei, I, Gamougam, K, Mbainadji, L, Douglas, D, Gadzama, G, Sambo, Z, Omotara, B, Nascimento, M, Woukeu, A, Manigert, O, Borrow, R, Stuart, J, and Greenwood, B

Abstract

Objectives. Neisseria meningitidis, together with the non-pathogenic Neisseria species (NPNs), are members of the complex microbiota of the human pharynx. This paper investigates the influence of NPNs on the epidemiology of meningococcal infection. Methods. Neisseria isolates were collected during 18 surveys conducted in six countries in the African meningitis belt between 2010 and 2012 and characterized at the rplF locus to determine species and at the variable region of the fetA antigen gene. Prevalence and risk factors for carriage were analyzed. Results. A total of 4694 isolates of Neisseria were obtained from 46034 pharyngeal swabs, a carriage prevalence of 10.2% (95% CI, 9.8-10.5). Five Neisseria species were identified, the most prevalent NPN being Neisseria lactamica. Six hundred and thirty-six combinations of rplF/fetA_VR alleles were identified, each defined as a Neisseria strain type. There was an inverse relationship between carriage of N. meningitidis and of NPNs by age group, gender and season, whereas carriage of both N. meningitidis and NPNs was negatively associated with a recent history of meningococcal vaccination. Conclusion. Variations in the prevalence of NPNs by time, place and genetic type may contribute to the particular epidemiology of meningococcal disease in the African meningitis belt.

Published

2016

11. The diversity of meningococcal carriage across the african meningitis belt and the impact of vaccination with a group a meningococcal conjugate vaccine

Author

Ali, O., Aseffa, A., Bedru, A., Lema, T., Moti, T., Tekletsion, Y., Worku, A., Xabher, H. G., Yamuah, L., Boukary, R. M., Collard, J. M., Dano, I. D., Habiboulaye, I., Issaka, B., Jusot, J. F., Ousmane, S., Rabe, I., Daugla, D. M., Gami, J. P., Gamougam, K., Mbainadji, L., Naibei, N., Narbe, M., Toralta, J., Berthe, A., Diallo, K., Keita, M., Onwuchekwa, U., Sow, S. O., Tamboura, B., Traore, A., Toure, A., Clark, T., Mayer, L., Amodu, M., Beida, O., Gadzama, G., Omotara, B., Sambo, Z., Yahya, S., Chandramohan, D., Greenwood, B. M., Hassan-King, M., Manigart, O., Nascimento, M., Stuart, J. M., Woukeu, A., Basta, N. E., Bai, X. L., Borrow, R., Findlow, H., Alavo, S., Bassene, H., Diallo, A., Dieng, M., Doucouré, S., Gomis, J. F., Ndiaye, A., Sokhna, Cheikh, Trape, Jean-François, Akalifa, B., Forgor, A., Hodgson, A., Osei, I., Quaye, S. L., Williams, J., Wontuo, P., Irving, T., Trotter, C. L., Bennett, J., Hill, D., Harrison, O., Maiden, M. C., Rebbetts, L., and Watkins, E.

Subjects

meningococcus, Africa, meningitis, Neisseria meningitidis, carriage

Abstract

Background. Study of meningococcal carriage is essential to understanding the epidemiology of Neisseria meningitidis infection. Methods. Twenty cross-sectional carriage surveys were conducted in 7 countries in the African meningitis belt; 5 surveys were conducted after introduction of a new serogroup A meningococcal conjugate vaccine (MenAfriVac). Pharyngeal swab specimens were collected, and Neisseria species were identified by microbiological and molecular techniques. Results. A total of 1687 of 48 490 participants (3.4%; 95% confidence interval [CI], 3.2%-3.6%) carried meningococci. Carriage was more frequent in individuals aged 5-14 years, relative to those aged 15-29 years (adjusted odds ratio [OR], 1.41; 95% CI, 1.25-1.60); in males, relative to females (adjusted OR, 1.17; 95% CI, 1.10-1.24); in individuals in rural areas, relative to those in urban areas (adjusted OR, 1.44; 95% CI, 1.28-1.63); and in the dry season, relative to the rainy season (adjusted OR, 1.54; 95% CI, 1.37-1.75). Forty-eight percent of isolates had genes encoding disease-associated polysaccharide capsules; genogroup W predominated, and genogroup A was rare. Strain diversity was lower in countries in the center of the meningitis belt than in Senegal or Ethiopia. The prevalence of genogroup A fell from 0.7% to 0.02% in Chad following mass vaccination with MenAfriVac. Conclusions. The prevalence of meningococcal carriage in the African meningitis belt is lower than in industrialized countries and is very diverse and dynamic, even in the absence of vaccination.

Published

2015

12. The Burden of Cryptosporidium Diarrheal Disease among Children < 24 Months of Age in Moderate/High Mortality Regions of Sub-Saharan Africa and South Asia, Utilizing Data from the Global Enteric Multicenter Study (GEMS)

Author

Kosek, M, Sow, SO, Muhsen, K, Nasrin, D, Blackwelder, WC, Wu, Y, Farag, TH, Panchalingam, S, Sur, D, Zaidi, AKM, Faruque, ASG, Saha, D, Adegbola, R, Alonso, PL, Breiman, RF, Bassat, Q, Tamboura, B, Sanogo, D, Onwuchekwa, U, Manna, B, Ramamurthy, T, Kanungo, S, Ahmed, S, Qureshi, S, Quadri, F, Hossain, A, Das, SK, Antonio, M, Hossain, MJ, Mandomando, I, Nhampossa, T, Acacio, S, Omore, R, Oundo, JO, Ochieng, JB, Mintz, ED, O'Reilly, CE, Berkeley, LY, Livio, S, Tennant, SM, Sommerfelt, H, Nataro, JP, Ziv-Baran, T, Robins-Browne, RM, Mishcherkin, V, Zhang, J, Liu, J, Houpt, ER, Kotloff, KL, Levine, MM, Kosek, M, Sow, SO, Muhsen, K, Nasrin, D, Blackwelder, WC, Wu, Y, Farag, TH, Panchalingam, S, Sur, D, Zaidi, AKM, Faruque, ASG, Saha, D, Adegbola, R, Alonso, PL, Breiman, RF, Bassat, Q, Tamboura, B, Sanogo, D, Onwuchekwa, U, Manna, B, Ramamurthy, T, Kanungo, S, Ahmed, S, Qureshi, S, Quadri, F, Hossain, A, Das, SK, Antonio, M, Hossain, MJ, Mandomando, I, Nhampossa, T, Acacio, S, Omore, R, Oundo, JO, Ochieng, JB, Mintz, ED, O'Reilly, CE, Berkeley, LY, Livio, S, Tennant, SM, Sommerfelt, H, Nataro, JP, Ziv-Baran, T, Robins-Browne, RM, Mishcherkin, V, Zhang, J, Liu, J, Houpt, ER, Kotloff, KL, and Levine, MM

Abstract

BACKGROUND: The importance of Cryptosporidium as a pediatric enteropathogen in developing countries is recognized. METHODS: Data from the Global Enteric Multicenter Study (GEMS), a 3-year, 7-site, case-control study of moderate-to-severe diarrhea (MSD) and GEMS-1A (1-year study of MSD and less-severe diarrhea [LSD]) were analyzed. Stools from 12,110 MSD and 3,174 LSD cases among children aged <60 months and from 21,527 randomly-selected controls matched by age, sex and community were immunoassay-tested for Cryptosporidium. Species of a subset of Cryptosporidium-positive specimens were identified by PCR; GP60 sequencing identified anthroponotic C. parvum. Combined annual Cryptosporidium-attributable diarrhea incidences among children aged <24 months for African and Asian GEMS sites were extrapolated to sub-Saharan Africa and South Asian regions to estimate region-wide MSD and LSD burdens. Attributable and excess mortality due to Cryptosporidium diarrhea were estimated. FINDINGS: Cryptosporidium was significantly associated with MSD and LSD below age 24 months. Among Cryptosporidium-positive MSD cases, C. hominis was detected in 77.8% (95% CI, 73.0%-81.9%) and C. parvum in 9.9% (95% CI, 7.1%-13.6%); 92% of C. parvum tested were anthroponotic genotypes. Annual Cryptosporidium-attributable MSD incidence was 3.48 (95% CI, 2.27-4.67) and 3.18 (95% CI, 1.85-4.52) per 100 child-years in African and Asian infants, respectively, and 1.41 (95% CI, 0.73-2.08) and 1.36 (95% CI, 0.66-2.05) per 100 child-years in toddlers. Corresponding Cryptosporidium-attributable LSD incidences per 100 child-years were 2.52 (95% CI, 0.33-5.01) and 4.88 (95% CI, 0.82-8.92) in infants and 4.04 (95% CI, 0.56-7.51) and 4.71 (95% CI, 0.24-9.18) in toddlers. We estimate 2.9 and 4.7 million Cryptosporidium-attributable cases annually in children aged <24 months in the sub-Saharan Africa and India/Pakistan/Bangladesh/Nepal/Afghanistan regions, respectively, and ~202,000 Cryptosporidium-attributable deat

Published

2016

13. Meningococcal carriage in the African meningitis belt

Author

Ali, O., Aseffa, A., Bedru, A., Lemma, T., Moti, T., Worku, A., Xabher, H. G., Yamuah, L., Boukary, R. M., Collard, J. M., Dano, I. D., Habiboulaye, I., Issaka, B., Jusot, J. F., Ousmane, S., Rabe, I., Clark, T., Mayer, L., Gami, J. P., Gamougam, K., Kodbesse, B., Naibei, N., Ngadoua, C., Mbainadji, L., Moto, D. D., Narbe, M., Toralta, J., Berthe, A., Keita, M., Diallo, K., Onwuchekwa, U., Sow, S. O., Tamboura, B., Traore, A., Toure, A., Amodu, M., Beida, O., Gadzama, G., Omotara, B., Sambo, Z., Yahya, S., Chandramohan, D., Greenwood, B., Hassan-King, M., Manigart, O., Nascimento, M., Stuart, J., Woukeu, A., Bai, X. L., Borrow, R., Findlow, H., Avalo, S., Bassene, H., Diallo, A., Dieng, M., Doucouré, S., Gomis, J. F., Ndiaye, A., Sokhna, Cheikh, Trape, Jean-François, Akalifa, B., Forgor, A., Hodgson, A., Osei, I., Quaye, S., Williams, J., Wontuo, P., Basta, N., Irving, T., Trotter, C., Bennett, J., Hill, D., Harrison, O., Rebbetts, L., Maiden, M., Tekletsion, Y., and Watkins, E.

Subjects

meningococcal carriage, MenAfriCar, meningococcus, Africa, Neisseria meningitidis, meningococcal vaccines

Abstract

A meningococcal serogroup A polysaccharide/tetanus toxoid conjugate vaccine (PsA-TT) (MenAfriVac) is being deployed in countries of the African meningitis belt. Experience with other polysaccharide/protein conjugate vaccines has shown that an important part of their success has been their ability to prevent the acquisition of pharyngeal carriage and hence to stop transmission and induce herd immunity. If PsA-TT is to achieve the goal of preventing epidemics, it must be able to prevent the acquisition of pharyngeal carriage as well as invasive meningococcal disease and whether PsA-TT can prevent pharyngeal carriage needs to be determined. To address this issue, a consortium (the African Meningococcal Carriage (MenAfriCar) consortium) was established in 2009 to investigate the pattern of meningococcal carriage in countries of the African meningitis belt prior to and after the introduction of PsA-TT. This article describes how the consortium was established, its objectives and the standardised field and laboratory methods that were used to achieve these objectives. The experience of the MenAfriCar consortium will help in planning future studies on the epidemiology of meningococcal carriage in countries of the African meningitis belt and elsewhere.

Published

2013

14. Shigella Isolates From the Global Enteric Multicenter Study Inform Vaccine Development

Author

Livio, S., primary, Strockbine, N. A., additional, Panchalingam, S., additional, Tennant, S. M., additional, Barry, E. M., additional, Marohn, M. E., additional, Antonio, M., additional, Hossain, A., additional, Mandomando, I., additional, Ochieng, J. B., additional, Oundo, J. O., additional, Qureshi, S., additional, Ramamurthy, T., additional, Tamboura, B., additional, Adegbola, R. A., additional, Hossain, M. J., additional, Saha, D., additional, Sen, S., additional, Faruque, A. S. G., additional, Alonso, P. L., additional, Breiman, R. F., additional, Zaidi, A. K. M., additional, Sur, D., additional, Sow, S. O., additional, Berkeley, L. Y., additional, O'Reilly, C. E., additional, Mintz, E. D., additional, Biswas, K., additional, Cohen, D., additional, Farag, T. H., additional, Nasrin, D., additional, Wu, Y., additional, Blackwelder, W. C., additional, Kotloff, K. L., additional, Nataro, J. P., additional, and Levine, M. M., additional

Published

2014

15. Burden and aetiology of diarrhoeal disease in infants and young children in developing countries (the Global Enteric Multicenter Study, GEMS): a prospective, case-control study

Author

Kotloff, KL, Nataro, JP, Blackwelder, WC, Nasrin, D, Farag, TH, Panchalingam, S, Wu, Y, Sow, SO, Sur, D, Breiman, RF, Faruque, ASG, Zaidi, AKM, Saha, D, Alonso, PL, Tamboura, B, Sanogo, D, Onwuchekwa, U, Manna, B, Ramamurthy, T, Kanungo, S, Ochieng, JB, Omore, R, Oundo, JO, Hossain, A, Das, SK, Ahmed, S, Qureshi, S, Quadri, F, Adegbola, RA, Antonio, M, Hossain, MJ, Akinsola, A, Mandomando, I, Nhampossa, T, Acacio, S, Biswas, K, O'Reilly, CE, Mintz, ED, Berkeley, LY, Muhsen, K, Sommerfelt, H, Robins-Browne, RM, Levine, MM, Kotloff, KL, Nataro, JP, Blackwelder, WC, Nasrin, D, Farag, TH, Panchalingam, S, Wu, Y, Sow, SO, Sur, D, Breiman, RF, Faruque, ASG, Zaidi, AKM, Saha, D, Alonso, PL, Tamboura, B, Sanogo, D, Onwuchekwa, U, Manna, B, Ramamurthy, T, Kanungo, S, Ochieng, JB, Omore, R, Oundo, JO, Hossain, A, Das, SK, Ahmed, S, Qureshi, S, Quadri, F, Adegbola, RA, Antonio, M, Hossain, MJ, Akinsola, A, Mandomando, I, Nhampossa, T, Acacio, S, Biswas, K, O'Reilly, CE, Mintz, ED, Berkeley, LY, Muhsen, K, Sommerfelt, H, Robins-Browne, RM, and Levine, MM

Abstract

BACKGROUND: Diarrhoeal diseases cause illness and death among children younger than 5 years in low-income countries. We designed the Global Enteric Multicenter Study (GEMS) to identify the aetiology and population-based burden of paediatric diarrhoeal disease in sub-Saharan Africa and south Asia. METHODS: The GEMS is a 3-year, prospective, age-stratified, matched case-control study of moderate-to-severe diarrhoea in children aged 0-59 months residing in censused populations at four sites in Africa and three in Asia. We recruited children with moderate-to-severe diarrhoea seeking care at health centres along with one to three randomly selected matched community control children without diarrhoea. From patients with moderate-to-severe diarrhoea and controls, we obtained clinical and epidemiological data, anthropometric measurements, and a faecal sample to identify enteropathogens at enrolment; one follow-up home visit was made about 60 days later to ascertain vital status, clinical outcome, and interval growth. FINDINGS: We enrolled 9439 children with moderate-to-severe diarrhoea and 13,129 control children without diarrhoea. By analysing adjusted population attributable fractions, most attributable cases of moderate-to-severe diarrhoea were due to four pathogens: rotavirus, Cryptosporidium, enterotoxigenic Escherichia coli producing heat-stable toxin (ST-ETEC; with or without co-expression of heat-labile enterotoxin), and Shigella. Other pathogens were important in selected sites (eg, Aeromonas, Vibrio cholerae O1, Campylobacter jejuni). Odds of dying during follow-up were 8·5-fold higher in patients with moderate-to-severe diarrhoea than in controls (odd ratio 8·5, 95% CI 5·8-12·5, p<0·0001); most deaths (167 [87·9%]) occurred during the first 2 years of life. Pathogens associated with increased risk of case death were ST-ETEC (hazard ratio [HR] 1·9; 0·99-3·5) and typical enteropathogenic E coli (HR 2·6; 1·6-4·1) in infants aged 0-11 months, and Cryptosporidium (HR

Published

2013

16. Diagnostic Microbiologic Methods in the GEMS-1 Case/Control Study

Author

Panchalingam, S, Antonio, M, Hossain, A, Mandomando, I, Ochieng, B, Oundo, J, Ramamurthy, T, Tamboura, B, Zaidi, AKM, Petri, W, Houpt, E, Murray, P, Prado, V, Vidal, R, Steele, D, Strockbine, N, Sansonetti, P, Glass, RI, Robins-Browne, RM, Tauschek, M, Svennerholm, A-M, Kotloff, K, Levine, MM, Nataro, JP, Panchalingam, S, Antonio, M, Hossain, A, Mandomando, I, Ochieng, B, Oundo, J, Ramamurthy, T, Tamboura, B, Zaidi, AKM, Petri, W, Houpt, E, Murray, P, Prado, V, Vidal, R, Steele, D, Strockbine, N, Sansonetti, P, Glass, RI, Robins-Browne, RM, Tauschek, M, Svennerholm, A-M, Kotloff, K, Levine, MM, and Nataro, JP

Abstract

To understand the etiology of moderate-to-severe diarrhea among children in high mortality areas of sub-Saharan Africa and South Asia, we performed a comprehensive case/control study of children aged <5 years at 7 sites. Each site employed an identical case/control study design and each utilized a uniform comprehensive set of microbiological assays to identify the likely bacterial, viral and protozoal etiologies. The selected assays effected a balanced consideration of cost, robustness and performance, and all assays were performed at the study sites. Identification of bacterial pathogens employed streamlined conventional bacteriologic biochemical and serological algorithms. Diarrheagenic Escherichia coli were identified by application of a multiplex polymerase chain reaction assay for enterotoxigenic, enteroaggregative, and enteropathogenic E. coli. Rotavirus, adenovirus, Entamoeba histolytica, Giardia enterica, and Cryptosporidium species were detected by commercially available enzyme immunoassays on stool samples. Samples positive for adenovirus were further evaluated for adenovirus serotypes 40 and 41. We developed a novel multiplex assay to detect norovirus (types 1 and 2), astrovirus, and sapovirus. The portfolio of diagnostic assays used in the GEMS study can be broadly applied in developing countries seeking robust cost-effective methods for enteric pathogen detection.

Published

2012

17. Age-specific prevalence estimates and risk factors for asymptomatic Neisseria meningitidis carriage in Bamako, Mali

Author

Basta, N., primary, Sow, S., additional, Berthe, A., additional, Tamboura, B., additional, Onwuchekwa, U., additional, Haidara, F. Cheick, additional, Watkins, E., additional, Bennett, J., additional, Maiden, M., additional, Weiss, N., additional, and Halloran, M.E., additional

Published

2012

18. L'Épopée de Sunjara, d'après Lansine Diabate de Kela

Author

Duintjer, E., Jansen, J.A.M.M., and Tamboura, B.

Published

1995

19. Genomic Characterization of Enteroaggregative Escherichia coli From Children in Mali

Author

Boisen, N., primary, Scheutz, F., additional, Rasko, D. A., additional, Redman, J. C., additional, Persson, S., additional, Simon, J., additional, Kotloff, K. L., additional, Levine, M. M., additional, Sow, S., additional, Tamboura, B., additional, Toure, A., additional, Malle, D., additional, Panchalingam, S., additional, Krogfelt, K. A., additional, and Nataro, J. P., additional

Published

2011

20. Histo-Blood Group Antigen Null Phenotypes Associated With a Decreased Risk of Clinical Rotavirus Vaccine Failure Among Children <2 Years of Age Participating in the Vaccine Impact on Diarrhea in Africa (VIDA) Study in Kenya, Mali, and the Gambia.

Author

Schwartz LM, Oshinsky J, Reymann M, Esona MD, Bowen MD, Jahangir Hossain M, Zaman SMA, Jones JCM, Antonio M, Badji H, Sarwar G, Sow SO, Sanogo D, Keita AM, Tamboura B, Traoré A, Onwuchekwa U, Omore R, Verani JR, Awuor AO, Ochieng JB, Juma J, Ogwel B, Parashar UD, Tate JE, Kasumba IN, Tennant SM, Neuzil KM, Rowhani-Rahbar A, Elizabeth Halloran M, Atmar RL, Pasetti MF, and Kotloff KL

Subjects

Humans, Gambia, Kenya epidemiology, Mali epidemiology, Diarrhea epidemiology, Diarrhea prevention & control, Phenotype, Blood Group Antigens genetics, Rotavirus Vaccines, Rotavirus Infections epidemiology, Rotavirus Infections prevention & control, Rotavirus genetics

Abstract

Background: Previously studied risk factors for rotavirus vaccine failure have not fully explained reduced rotavirus vaccine effectiveness in low-income settings. We assessed the relationship between histo-blood group antigen (HBGA) phenotypes and clinical rotavirus vaccine failure among children <2 years of age participating in the Vaccine Impact on Diarrhea in Africa Study in 3 sub-Saharan African countries., Methods: Saliva was collected and tested for HBGA phenotype in children who received rotavirus vaccine. The association between secretor and Lewis phenotypes and rotavirus vaccine failure was examined overall and by infecting rotavirus genotype using conditional logistic regression in 218 rotavirus-positive cases with moderate-to-severe diarrhea and 297 matched healthy controls., Results: Both nonsecretor and Lewis-negative phenotypes (null phenotypes) were associated with decreased rotavirus vaccine failure across all sites (matched odds ratio, 0.30 [95% confidence interval: 0.16-0.56] or 0.39 [0.25-0.62], respectively]. A similar decrease in risk against rotavirus vaccine failure among null HBGA phenotypes was observed for cases with P[8] and P[4] infection and their matched controls. While we found no statistically significant association between null HBGA phenotypes and vaccine failure among P[6] infections, the matched odds ratio point estimate for Lewis-negative individuals was >4., Conclusions: Our study demonstrated a significant relationship between null HBGA phenotypes and decreased rotavirus vaccine failure in a population with P[8] as the most common infecting genotype. Further studies are needed in populations with a large burden of P[6] rotavirus diarrhea to understand the role of host genetics in reduced rotavirus vaccine effectiveness., Competing Interests: Potential conflicts of interest. All authors: No reported conflicts. All authors have submitted the ICMJE Form for Disclosure of Potential Conflicts of Interest. Conflicts that the editors consider relevant to the content of the manuscript have been disclosed., (© The Author(s) 2023. Published by Oxford University Press on behalf of Infectious Diseases Society of America.)

Published

2023

21. Moderate-to-Severe Diarrhea and Stunting Among Children Younger Than 5 Years: Findings From the Vaccine Impact on Diarrhea in Africa (VIDA) Study.

Author

Nasrin D, Liang Y, Powell H, Casanova IG, Sow SO, Hossain MJ, Omore R, Sanogo D, Tamboura B, Zaman SMA, Antonio M, Jones JCM, Awuor AO, Kasumba IN, Ochieng JB, Badji H, Verani JR, Widdowson MA, Roose A, Jamka LP, Tennant SM, Ramakrishnan U, and Kotloff KL

Subjects

Humans, Child, Child, Preschool, Infant, Prospective Studies, Case-Control Studies, Africa South of the Sahara epidemiology, Diarrhea epidemiology, Growth Disorders epidemiology

Abstract

Background: Stunting affects >20% of children <5 years old worldwide and disproportionately impacts underserved communities. The Vaccine Impact on Diarrhea in Africa (VIDA) Study examined the association between an episode of moderate-to-severe diarrhea (MSD) and the risk of subsequent stunting in children <5 years living in 3 sub-Saharan African countries., Methods: In this prospective, matched, case-control study among children <5 years, data were collected over 36 months from 2 groups. "Children with MSD" visited a health center within 7 days of illness onset experiencing ≥3 loose stools/day plus sunken eyes, poor skin turgor, dysentery, intravenous rehydration, or hospitalization. "Children without MSD" were enrolled from the community within 14 days of the index MSD child; they were diarrhea-free during the previous 7 days and were matched to the index case by age, sex, and residence. Using generalized linear mixed-effects models, we estimated the effect of an MSD episode on odds of being stunted, defined as height-for-age z-scores <-2, at a follow-up visit 2-3 months post-enrollment., Results: The proportion of stunting at enrollment was similar when 4603 children with MSD and 5976 children without MSD were compared (21.8% vs 21.3%; P = .504). Among children not stunted at enrollment, those with MSD had 30% higher odds of being stunted at follow-up than children without MSD after controlling for age, sex, study site, and socioeconomic status (adjusted OR: 1.30; 95% CI: 1.05-1.62: P = .018)., Conclusions: Children <5 years in sub-Saharan Africa without stunting experienced an increased likelihood of stunting during 2-3 months following an episode of MSD. Strategies for control of early childhood diarrhea should be integrated into programs intended to reduce childhood stunting., Competing Interests: Potential conflicts of interest. I. G. C. reports receiving grant funding from the National Heart, Lung, and Blood Institute (NHLBI) and consulting fees from the University of California, San Francisco. They also report receiving travel support from Research in Implementation Science for Equity program from the University of San Francisco institute to travel to San Francisco. K. L. K. reports consultation fees and travel support from PATH and the University of Washington related to diarrheal diseases and grant support to her institution from the National Institute of Allergy and Infections Diseases, Institut Pasteur, and the Bill & Melinda Gates Foundation. M.-A. W. reports receiving funding from the Centers for Disease Control and Prevention (CDC) and Institute of Tropical Medicine. S. M. T. reports multiple grants paid to her institution from the National Institutes of Health (NIH), Bill & Melinda Gates Foundation (BMGF), Wellcome Trust, Affinivax, Lumen Biosciences, PATH, and Medical Research Council. She also reports payments as royalties related to intellectual property for Salmonella vaccines and Klebsiella/Pseudomonas vaccines and consulting fees and travel support from the University of Washington for a grant proposal. She also reports holding multiple planned, issued, and pending patents on Salmonella, Klebsiella, and Pseudomonas vaccines and hold multiple unpaid committee roles with the American Society of Tropical Medicine and Hygiene. Y. L. reports receiving the following grants or contracts paid to their institution: R01NS122855, U54CK000615-01, 1R18 HS027750-01, R03 AG067927, U01 AI143493, U01 AI148054, U01 AI148081, NCT04078022, HHS-NIH-NIAID-BAA2018, R01 HD093946-01, 2R01-DA026868-06A1, 2R01-AA014988-12A1, R01 AA014988-S1, R01 DK109323, R01-NR016269, Geneva Foundation (National Institute for Allergy and Infectious Diseases [NIAID] prime), R01-HD075936, and BAA FY2018-OADS-01. They also report serving as the Data Safety Monitoring Board statistician for the clinical trial entitled “Matching Perfusion and Metabolic Activity in HFpEF (MPMA),” and reviewed data from National Institute on Drug Abuse/National Institute on Alcohol Abuse and Alcoholism (NIDA/NIAAA) studies involving human subjects. All other authors report no potential conflicts. All authors have submitted the ICMJE Form for Disclosure of Potential Conflicts of Interest. Conflicts that the editors consider relevant to the content of the manuscript have been disclosed., (© The Author(s) 2023. Published by Oxford University Press on behalf of Infectious Diseases Society of America.)

Published

2023

22. Pathogens Associated With Linear Growth Faltering in Children With Diarrhea and Impact of Antibiotic Treatment: The Global Enteric Multicenter Study.

Author

Nasrin D, Blackwelder WC, Sommerfelt H, Wu Y, Farag TH, Panchalingam S, Biswas K, Saha D, Jahangir Hossain M, Sow SO, Reiman RFB, Sur D, Faruque ASG, Zaidi AKM, Sanogo D, Tamboura B, Onwuchekwa U, Manna B, Ramamurthy T, Kanungo S, Omore R, Ochieng JB, Oundo JO, Das SK, Ahmed S, Qureshi S, Quadri F, Adegbola RA, Antonio M, Mandomando I, Nhampossa T, Bassat Q, Roose A, O'Reilly CE, Mintz ED, Ramakrishnan U, Powell H, Liang Y, Nataro JP, Levine MM, and Kotloff KL

Subjects

Case-Control Studies, Child, Cryptosporidium isolation & purification, Diarrhea epidemiology, Diarrhea microbiology, Escherichia coli isolation & purification, Female, Humans, Infant, Male, Shigella isolation & purification, Anti-Bacterial Agents therapeutic use, Cryptosporidiosis drug therapy, Cryptosporidium pathogenicity, Diarrhea drug therapy, Escherichia coli pathogenicity, Growth Disorders etiology, Shigella pathogenicity

Abstract

Background: The association between childhood diarrheal disease and linear growth faltering in developing countries is well described. However, the impact attributed to specific pathogens has not been elucidated, nor has the impact of recommended antibiotic treatment., Methods: The Global Enteric Multicenter Study enrolled children with moderate to severe diarrhea (MSD) seeking healthcare at 7 sites in sub-Saharan Africa and South Asia. At enrollment, we collected stool samples to identify enteropathogens. Length/height was measured at enrollment and follow-up, approximately 60 days later, to calculate change in height-for-age z scores (ΔHAZ). The association of pathogens with ΔHAZ was tested using linear mixed effects regression models., Results: Among 8077 MSD cases analyzed, the proportion with stunting (HAZ below -1) increased from 59% at enrollment to 65% at follow-up (P < .0001). Pathogens significantly associated with linear growth decline included Cryptosporidium (P < .001), typical enteropathogenic Escherichia coli (P = .01), and untreated Shigella (P = .009) among infants (aged 0-11 months) and enterotoxigenic E. coli encoding heat-stable toxin (P < .001) and Cryptosporidium (P = .03) among toddlers (aged 12-23 months). Shigella-infected toddlers given antibiotics had improved linear growth (P = .02)., Conclusions: Linear growth faltering among children aged 0-23 months with MSD is associated with specific pathogens and can be mitigated with targeted treatment strategies, as demonstrated for Shigella., (© The Author(s) 2021. Published by Oxford University Press for the Infectious Diseases Society of America.)

Published

2021

23. The Etiology of Childhood Pneumonia in Mali: Findings From the Pneumonia Etiology Research for Child Health (PERCH) Study.

Author

Tapia MD, Sylla M, Driscoll AJ, Touré A, Kourouma N, Sissoko S, Tamboura B, Diakité AA, Panchalingam S, Keïta AM, Tennant S, Onwuchekwa U, Roose A, Deloria Knoll M, Higdon MM, Prosperi C, Hammitt LL, Feikin DR, Murdoch DR, O'Brien KL, Sow SO, and Kotloff KL

Subjects

AIDS-Related Opportunistic Infections diagnosis, AIDS-Related Opportunistic Infections epidemiology, AIDS-Related Opportunistic Infections etiology, AIDS-Related Opportunistic Infections prevention & control, Bayes Theorem, Case-Control Studies, Child Health, Child, Preschool, Developing Countries, Female, Hospitalization, Humans, Infant, Logistic Models, Male, Mali epidemiology, Patient Acuity, Pneumonia diagnosis, Pneumonia epidemiology, Pneumonia prevention & control, Risk Factors, Pneumonia etiology

Abstract

Background: We present findings from the Pneumonia Etiology Research for Child Health (PERCH) site in Bamako, Mali., Methods: Cases were patients 28 days to 59 months of age, admitted to hospital with severe or very severe pneumonia (2005 World Health Organization definition). Community controls were frequency matched by age. Both provided nasopharyngeal and oropharyngeal swabs for multiplex polymerase chain reaction and Streptococcus pneumoniae culture. Cases underwent blood culture and induced sputum culture for Mycobacterium tuberculosis. A subset had pleural fluid and lung aspirates collected for culture and polymerase chain reaction. Primary analyses included participants with negative or unknown HIV status (HIV-) and cases with abnormal chest radiographs (CXR+). Cases and controls were compared using logistic regression adjusting for age. Etiologic fractions were calculated by a Bayesian nested partially latent class analysis, the PERCH integrated analysis., Results: Between January 1, 2012, and January 14, 2014, we enrolled 241 CXR+/HIV- cases and 725 HIV- controls. Compared with controls, cases were more likely to have moderate-to-severe wasting (43.1% vs. 14.1%, P < 0.001) and stunting (26.6% vs. 9.4%, P < 0.001). Predominant etiologies were respiratory syncytial virus [24.0%; 95% credible interval (CrI): 18.3%-31.1%], S. pneumoniae (15.2%; 95% CrI: 9.5-21.6), human metapneumovirus (11.8%; 95% CrI: 8.3%-16.2%) and parainfluenza virus type 3 (9.0%; 95% CrI: 5.8%-13.3%). Case fatality was 13.3%, with Staphylococcus aureus, Pneumocystis jirovecii and Haemophilus influenzae type b predominating (40% of fatal cases)., Conclusions: PERCH uncovered high case fatality among children with severe pneumonia in Mali, highlighting a role for new interventions (eg, respiratory syncytial virus vaccines) and a need to improve vaccine coverage and strengthen healthcare delivery., Competing Interests: The authors have no conflicts of interest to disclose. M.D.K. has received funding for consultancies from Merck, Pfizer and Novartis and grant funding from Merck. M.M.H. has received grant funding from Pfizer. L.L.H. has received grant funding from Pfizer and GlaxoSmithKline. C.P. has received grant funding from Merck. K.L.O. has received grant funding from GlaxoSmithKline and Pfizer and participated on technical advisory boards for Merck, Sanofi-Pasteur, PATH, Affinivax and ClearPath. K.L.K. has received grant funding from Merck Sharp & Dohme. The other authors have no funding or conflicts of interest to disclose., (Copyright © 2021 The Author(s). Published by Wolters Kluwer Health, Inc.)

Published

2021

24. Characteristics of Salmonella Recovered From Stools of Children Enrolled in the Global Enteric Multicenter Study.

Author

Kasumba IN, Pulford CV, Perez-Sepulveda BM, Sen S, Sayed N, Permala-Booth J, Livio S, Heavens D, Low R, Hall N, Roose A, Powell H, Farag T, Panchalingham S, Berkeley L, Nasrin D, Blackwelder WC, Wu Y, Tamboura B, Sanogo D, Onwuchekwa U, Sow SO, Ochieng JB, Omore R, Oundo JO, Breiman RF, Mintz ED, O'Reilly CE, Antonio M, Saha D, Hossain MJ, Mandomando I, Bassat Q, Alonso PL, Ramamurthy T, Sur D, Qureshi S, Zaidi AKM, Hossain A, Faruque ASG, Nataro JP, Kotloff KL, Levine MM, Hinton JCD, and Tennant SM

Subjects

Anti-Bacterial Agents pharmacology, Child, Child, Preschool, Humans, Kenya epidemiology, Multilocus Sequence Typing, Phylogeny, Salmonella typhimurium genetics, Salmonella Infections epidemiology

Abstract

Background: The Global Enteric Multicenter Study (GEMS) determined the etiologic agents of moderate-to-severe diarrhea (MSD) in children under 5 years old in Africa and Asia. Here, we describe the prevalence and antimicrobial susceptibility of nontyphoidal Salmonella (NTS) serovars in GEMS and examine the phylogenetics of Salmonella Typhimurium ST313 isolates., Methods: Salmonella isolated from children with MSD or diarrhea-free controls were identified by classical clinical microbiology and serotyped using antisera and/or whole-genome sequence data. We evaluated antimicrobial susceptibility using the Kirby-Bauer disk-diffusion method. Salmonella Typhimurium sequence types were determined using multi-locus sequence typing, and whole-genome sequencing was performed to assess the phylogeny of ST313., Results: Of 370 Salmonella-positive individuals, 190 (51.4%) were MSD cases and 180 (48.6%) were diarrhea-free controls. The most frequent Salmonella serovars identified were Salmonella Typhimurium, serogroup O:8 (C2-C3), serogroup O:6,7 (C1), Salmonella Paratyphi B Java, and serogroup O:4 (B). The prevalence of NTS was low but similar across sites, regardless of age, and was similar among both cases and controls except in Kenya, where Salmonella Typhimurium was more commonly associated with cases than controls. Phylogenetic analysis showed that these Salmonella Typhimurium isolates, all ST313, were highly genetically related to isolates from controls. Generally, Salmonella isolates from Asia were resistant to ciprofloxacin and ceftriaxone, but African isolates were susceptible to these antibiotics., Conclusions: Our data confirm that NTS is prevalent, albeit at low levels, in Africa and South Asia. Our findings provide further evidence that multidrug-resistant Salmonella Typhimurium ST313 can be carried asymptomatically by humans in sub-Saharan Africa., (© The Author(s) 2021. Published by Oxford University Press for the Infectious Diseases Society of America.)

Published

2021

25. The Clinical Presentation of Culture-positive and Culture-negative, Quantitative Polymerase Chain Reaction (qPCR)-Attributable Shigellosis in the Global Enteric Multicenter Study and Derivation of a Shigella Severity Score: Implications for Pediatric Shigella Vaccine Trials.

Author

Pavlinac PB, Platts-Mills JA, Tickell KD, Liu J, Juma J, Kabir F, Nkeze J, Okoi C, Operario DJ, Uddin J, Ahmed S, Alonso PL, Antonio M, Becker SM, Breiman RF, Faruque ASG, Fields B, Gratz J, Haque R, Hossain A, Hossain MJ, Jarju S, Qamar F, Iqbal NT, Kwambana B, Mandomando I, McMurry TL, Ochieng C, Ochieng JB, Ochieng M, Onyango C, Panchalingam S, Kalam A, Aziz F, Qureshi S, Ramamurthy T, Roberts JH, Saha D, Sow SO, Stroup SE, Sur D, Tamboura B, Taniuchi M, Tennant SM, Roose A, Toema D, Wu Y, Zaidi A, Nataro JP, Levine MM, Houpt ER, and Kotloff KL

Subjects

Case-Control Studies, Child, Diarrhea epidemiology, Humans, Infant, Polymerase Chain Reaction, Dysentery, Bacillary diagnosis, Dysentery, Bacillary epidemiology, Shigella genetics, Vaccines

Abstract

Background: Shigella is a leading cause of childhood diarrhea and target for vaccine development. Microbiologic and clinical case definitions are needed for pediatric field vaccine efficacy trials., Methods: We compared characteristics of moderate to severe diarrhea (MSD) cases in the Global Enteric Multicenter Study (GEMS) between children with culture positive Shigella to those with culture-negative, quantitative polymerase chain reaction (qPCR)-attributable Shigella (defined by an ipaH gene cycle threshold <27.9). Among Shigella MSD cases, we determined risk factors for death and derived a clinical severity score., Results: Compared to culture-positive Shigella MSD cases (n = 745), culture-negative/qPCR-attributable Shigella cases (n = 852) were more likely to be under 12 months, stunted, have a longer duration of diarrhea, and less likely to have high stool frequency or a fever. There was no difference in dehydration, hospitalization, or severe classification from a modified Vesikari score. Twenty-two (1.8%) Shigella MSD cases died within the 14-days after presentation to health facilities, and 59.1% of these deaths were in culture-negative cases. Age <12 months, diarrhea duration prior to presentation, vomiting, stunting, wasting, and hospitalization were associated with mortality. A model-derived score assigned points for dehydration, hospital admission, and longer diarrhea duration but was not significantly better at predicting 14-day mortality than a modified Vesikari score., Conclusions: A composite severity score consistent with severe disease or dysentery may be a pragmatic clinical endpoint for severe shigellosis in vaccine trials. Reliance on culture for microbiologic confirmation may miss a substantial number of Shigella cases but is currently required to measure serotype specific immunity., (© The Author(s) 2020. Published by Oxford University Press for the Infectious Diseases Society of America.)

Published

2021

26. Diarrhoeal disease and subsequent risk of death in infants and children residing in low-income and middle-income countries: analysis of the GEMS case-control study and 12-month GEMS-1A follow-on study.

Author

Levine MM, Nasrin D, Acácio S, Bassat Q, Powell H, Tennant SM, Sow SO, Sur D, Zaidi AKM, Faruque ASG, Hossain MJ, Alonso PL, Breiman RF, O'Reilly CE, Mintz ED, Omore R, Ochieng JB, Oundo JO, Tamboura B, Sanogo D, Onwuchekwa U, Manna B, Ramamurthy T, Kanungo S, Ahmed S, Qureshi S, Quadri F, Hossain A, Das SK, Antonio M, Saha D, Mandomando I, Blackwelder WC, Farag T, Wu Y, Houpt ER, Verweiij JJ, Sommerfelt H, Nataro JP, Robins-Browne RM, and Kotloff KL

Subjects

Case-Control Studies, Child, Preschool, Female, Follow-Up Studies, Humans, Infant, Infant, Newborn, Male, Mortality, Prospective Studies, Developing Countries statistics & numerical data, Diarrhea epidemiology, Diarrhea mortality, Global Burden of Disease statistics & numerical data, Poverty statistics & numerical data

Abstract

Background: The Global Enteric Multicenter Study (GEMS) was a 3-year case-control study that measured the burden, aetiology, and consequences of moderate-to-severe diarrhoea (MSD) in children aged 0-59 months. GEMS-1A, a 12-month follow-on study, comprised two parallel case-control studies, one assessing MSD and the other less-severe diarrhoea (LSD). In this report, we analyse the risk of death with each diarrhoea type and the specific pathogens associated with fatal outcomes., Methods: GEMS was a prospective, age-stratified, matched case-control study done at seven sites in Africa and Asia. Children aged 0-59 months with MSD seeking care at sentinel health centres were recruited along with one to three randomly selected matched community control children without diarrhoea. In the 12-month GEMS-1A follow-on study, children with LSD and matched controls, in addition to children with MSD and matched controls, were recruited at six of the seven sites; only cases of MSD and controls were enrolled at the seventh site. We compared risk of death during the period between enrolment and one follow-up household visit done about 60 days later (range 50-90 days) in children with MSD and LSD and in their respective controls. Approximately 50 pathogens were detected using, as appropriate, classic bacteriology, immunoassays, gel-based PCR and reverse transcriptase PCR, and quantitative real-time PCR (qPCR). Specimens from a subset of GEMS cases and controls were also tested by a TaqMan Array Card that compartmentalised probe-based qPCR for 32 enteropathogens., Findings: 223 (2·0%) of 11 108 children with MSD and 43 (0·3%) of 16 369 matched controls died between study enrolment and the follow-up visit at about 60 days (hazard ratio [HR] 8·16, 95% CI 5·69-11·68, p<0·0001). 12 (0·4%) of 2962 children with LSD and seven (0·2%) of 4074 matched controls died during the follow-up period (HR 2·78, 95% CI 0·95-8·11, p=0·061). Risk of death was lower in children with dysenteric MSD than in children with non-dysenteric MSD (HR 0·20, 95% CI 0·05-0·87, p=0·032), and lower in children with LSD than in those with non-dysenteric MSD (HR 0·29, 0·14-0·59, p=0·0006). In children younger than 24 months with MSD, infection with typical enteropathogenic Escherichia coli, enterotoxigenic E coli encoding heat-stable toxin, enteroaggregative E coli, Shigella spp (non-dysentery cases), Aeromonas spp, Cryptosporidium spp, and Entamoeba histolytica increased risk of death. Of 61 deaths in children aged 12-59 months with non-dysenteric MSD, 31 occurred among 942 children qPCR-positive for Shigella spp and 30 deaths occurred in 1384 qPCR-negative children (HR 2·2, 95% CI 1·2-3·9, p=0·0090), showing that Shigella was strongly associated with increased risk of death., Interpretation: Risk of death is increased following MSD and, to a lesser extent, LSD. Considering there are approximately three times more cases of LSD than MSD in the population, more deaths are expected among children with LSD than in those with MSD. Because the major attributable LSD-associated and MSD-associated pathogens are the same, implementing vaccines and rapid diagnosis and treatment interventions against these major pathogens are rational investments., Funding: Bill & Melinda Gates Foundation., (Copyright © 2020 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2020

27. Epidemiology, Risk Factors, and Outcomes of Respiratory Syncytial Virus Infections in Newborns in Bamako, Mali.

Author

Buchwald AG, Tamboura B, Tennant SM, Haidara FC, Coulibaly F, Doumbia M, Diallo F, Keita AM, Sow SO, Kotloff KL, Levine MM, and Tapia MD

Subjects

Female, Hospitalization, Humans, Incidence, Infant, Infant, Newborn, Male, Mali epidemiology, Pregnancy, Risk Factors, Respiratory Syncytial Virus Infections epidemiology, Respiratory Syncytial Virus, Human

Abstract

Background: Few studies describe the respiratory syncytial virus (RSV) burden in African populations, and most have utilized hospital-based surveillance. In Mali, no community-based studies exist of the incidence or epidemiology of RSV infection. This study provides the first estimates of RSV incidence in Mali., Methods: In a cohort of infants enrolled in a clinical trial of maternal influenza vaccination, we estimate incidence of RSV-associated febrile illness in the first 6 months of life and identify risk factors for RSV infection and progression to severe disease. Infants (N = 1871) were followed from birth to 6 months of age and visited weekly to detect pneumonia and influenza-like illness. Baseline covariates were explored as risk factors for RSV febrile illness and RSV pneumonia or hospitalization., Results: Incidence of RSV illness was estimated at 536.8 per 1000 person-years, and 86% (131/153) of RSV illness episodes were positive for RSV-B. RSV illness was most frequent in the fifth month of life and associated with having older mothers and with lower parity. The incidence of RSV-associated hospitalizations was 45.6 per 1000 person-years. Among infants with RSV illness, males were more likely to be hospitalized. The incidence of RSV pneumonia was 29 cases per 1000 person-years., Conclusions: In the first 6 months of life, Malian infants have a high incidence of RSV illness, primarily caused by RSV-B. Prevention of early RSV will require passive protection via maternal immunization in pregnancy. Mali is the first country where RSV-B has been identified as the dominant subtype, with potential implications for vaccine development., (© The Author(s) 2019. Published by Oxford University Press for the Infectious Diseases Society of America.)

Published

2020

28. Impact of the addition of azithromycin to antimalarials used for seasonal malaria chemoprevention on antimicrobial resistance of Streptococcus pneumoniae.

Author

Hema-Ouangraoua S, Aziz Maiga A, Cairns M, Zongo I, Frédéric N, Serge Yerbanga R, Tamboura B, Badji H, Gore-Langton G, Kuepfer I, Tinto H, Sagara I, Dicko A, Sow SO, Chandrahoman D, Greenwood B, and Bosco Ouedraogo J

Subjects

Burkina Faso epidemiology, Chemoprevention, Child Health Services, Child, Preschool, Drug Resistance, Bacterial, Female, Humans, Infant, Malaria prevention & control, Male, Mali epidemiology, Seasons, Streptococcus pneumoniae isolation & purification, Antimalarials pharmacology, Azithromycin pharmacology, Malaria epidemiology, Streptococcus pneumoniae drug effects

Abstract

Objective: A trial was conducted in Burkina Faso and Mali to investigate whether addition of azithromycin to the antimalarials used for seasonal malaria chemoprevention reduces mortality and hospital admissions of children. We tested the sensitivity of nasal isolates of Streptococcus pneumoniae obtained during this trial to azithromycin and other antibiotics., Methods: Azithromycin or placebo was administered monthly, in combination with the antimalarials used for seasonal malaria chemoprevention, for four months, over the annual malaria transmission seasons of 2014, 2015, and 2016. Nasopharyngeal swabs were collected from 2773 Burkinabe and 2709 Malian children on seven occasions: in July and December each year prior to and after drug administration, and at a final survey in early 2018. Pneumococci were isolated from nasopharyngeal swabs and tested for sensitivity to azithromycin and other antibiotics., Results: A total of 5482 samples were collected. In Burkina Faso, the percentage of pneumococcal isolates resistant to azithromycin among children who had received it increased from 4.9% (95% CI: 2.4%, 9.9%) before the intervention to 25.6% (95% CI: 17.6%, 35.7%) afterward. In Mali, the increase was from 7.6% (95% CI: 3.8%, 14.4%) to 68.5% (95% CI: 55.1%, 79.4%). The percentage of resistant isolates remained elevated (17.7% (95% CI: 11.1%, 27.1%) in Burkina Faso and 19.1% (95% CI: 13.5%, 26.3%) in Mali) among children who had received azithromycin 1 year after stopping the intervention. An increase in resistance to azithromycin was also observed in children who had received a placebo but it was less marked., Conclusion: Addition of azithromycin to the antimalarial combination used for seasonal malaria chemoprevention was associated with an increase in resistance of pneumococci to azithromycin and erythromycin, which persisted 1 year after the last administration of azithromycin., (© 2019 John Wiley & Sons Ltd.)

Published

2019

29. The incidence, aetiology, and adverse clinical consequences of less severe diarrhoeal episodes among infants and children residing in low-income and middle-income countries: a 12-month case-control study as a follow-on to the Global Enteric Multicenter Study (GEMS).

Author

Kotloff KL, Nasrin D, Blackwelder WC, Wu Y, Farag T, Panchalingham S, Sow SO, Sur D, Zaidi AKM, Faruque ASG, Saha D, Alonso PL, Tamboura B, Sanogo D, Onwuchekwa U, Manna B, Ramamurthy T, Kanungo S, Ahmed S, Qureshi S, Quadri F, Hossain A, Das SK, Antonio M, Hossain MJ, Mandomando I, Acácio S, Biswas K, Tennant SM, Verweij JJ, Sommerfelt H, Nataro JP, Robins-Browne RM, and Levine MM

Subjects

Age Factors, Case-Control Studies, Child, Preschool, Diarrhea complications, Diarrhea etiology, Diarrhea, Infantile complications, Diarrhea, Infantile etiology, Female, Humans, Incidence, Infant, Infant, Newborn, Male, Developing Countries statistics & numerical data, Diarrhea epidemiology, Diarrhea, Infantile epidemiology

Abstract

Background: Diarrheal diseases remain a leading cause of illness and death among children younger than 5 years in low-income and middle-income countries. The Global Enteric Multicenter Study (GEMS) has described the incidence, aetiology, and sequelae of medically attended moderate-to-severe diarrhoea (MSD) among children aged 0-59 months residing in censused populations in sub-Saharan Africa and south Asia, where most child deaths occur. To further characterise this disease burden and guide interventions, we extended this study to include children with episodes of less-severe diarrhoea (LSD) seeking care at health centres serving six GEMS sites., Methods: We report a 1-year, multisite, age-stratified, matched case-control study following on to the GEMS study. Six sites (Bamako, Mali; Manhiça, Mozambique; Basse, The Gambia; Mirzapur, Bangladesh; Kolkata, India; and Bin Qasim Town, Karachi, Pakistan) participated in this study. Children aged 0-59 months at each site who sought care at a sentinel hospital or health centre during a 12-month period were screened for diarrhoea. New (onset after ≥7 diarrhoea-free days) and acute (onset within the previous 7 days) episodes of diarrhoea in children who had sunken eyes, whose skin lost turgor, who received intravenous hydration, who had dysentery, or who were hospitalised were eligible for inclusion as MSD. The remaining new and acute diarrhoea episodes among children who sought care at the same health centres were considered LSD. We aimed to enrol the first eight or nine eligible children with MSD and LSD at each site during each fortnight in three age strata: infants (aged 0-11 months), toddlers (aged 12-23 months), and young children (aged 24-59 months). For each included case of MSD or LSD, we enrolled one to three community control children without diarrhoea during the previous 7 days. From patients and controls we collected clinical and epidemiological data, anthropometric measurements, and faecal samples to identify enteropathogens at enrolment, and we performed a follow-up home visit about 60 days later to ascertain vital status, clinical outcome, and interval growth. Primary outcomes were to characterise, for MSD and LSD, the pathogen-specific attributable risk and population-based incidence values, and to assess the frequency of adverse clinical consequences associated with these two diarrhoeal syndromes., Findings: From Oct 31, 2011, to Nov 14, 2012, we recruited 2368 children with MSD, 3174 with LSD, and one to three randomly selected community control children without diarrhoea matched to cases with MSD (n=3597) or LSD (n=4236). Weighted adjusted population attributable fractions showed that most attributable cases of MSD and LSD were due to rotavirus, Cryptosporidium spp, enterotoxigenic Escherichia coli encoding heat-stable toxin (with or without genes encoding heat-labile enterotoxin), and Shigella spp. The attributable incidence per 100 child-years for LSD versus MSD, by age stratum, for rotavirus was 22·3 versus 5·5 (0-11 months), 9·8 versus 2·9 (12-23 months), and 0·5 versus 0·2 (24-59 months); for Cryptosporidium spp was 3·6 versus 2·3 (0-11 months), 4·3 versus 0·6 (12-23 months), and 0·3 versus 0·1 (24-59 months); for enterotoxigenic E coli encoding heat-stable toxin was 4·2 versus 0·1 (0-11 months), 5·2 versus 0·0 (12-23 months), and 1·1 versus 0·2 (24-59 months); and for Shigella spp was 1·0 versus 1·3 (0-11 months), 3·1 versus 2·4 (12-23 months), and 0·8 versus 0·7 (24-59 months). Participants with both MSD and LSD had significantly more linear growth faltering than controls at follow-up., Interpretation: Inclusion of participants with LSD markedly expands the population of children who experience adverse clinical and nutritional outcomes from acute diarrhoeal diseases. Since MSD and LSD have similar aetiologies, interventions targeting rotavirus, Shigella spp, enterotoxigenic E coli producing heat-stable toxin, and Cryptosporidium spp might substantially reduce the diarrhoeal disease burden and its associated nutritional faltering., Funding: Bill & Melinda Gates Foundation., (Copyright © 2019 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2019

30. Colonization factors among enterotoxigenic Escherichia coli isolates from children with moderate-to-severe diarrhea and from matched controls in the Global Enteric Multicenter Study (GEMS).

Author

Vidal RM, Muhsen K, Tennant SM, Svennerholm AM, Sow SO, Sur D, Zaidi AKM, Faruque ASG, Saha D, Adegbola R, Hossain MJ, Alonso PL, Breiman RF, Bassat Q, Tamboura B, Sanogo D, Onwuchekwa U, Manna B, Ramamurthy T, Kanungo S, Ahmed S, Qureshi S, Quadri F, Hossain A, Das SK, Antonio M, Mandomando I, Nhampossa T, Acácio S, Omore R, Ochieng JB, Oundo JO, Mintz ED, O'Reilly CE, Berkeley LY, Livio S, Panchalingam S, Nasrin D, Farag TH, Wu Y, Sommerfelt H, Robins-Browne RM, Del Canto F, Hazen TH, Rasko DA, Kotloff KL, Nataro JP, and Levine MM

Subjects

Africa epidemiology, Asia epidemiology, Case-Control Studies, Child, Preschool, Female, Genotype, Humans, Infant, Infant, Newborn, Male, Polymerase Chain Reaction, Prevalence, Enterotoxigenic Escherichia coli genetics, Enterotoxigenic Escherichia coli isolation & purification, Escherichia coli Infections epidemiology, Escherichia coli Infections microbiology, Fimbriae Proteins genetics, Virulence Factors genetics

Abstract

Background: Enterotoxigenic Escherichia coli (ETEC) encoding heat-stable enterotoxin (ST) alone or with heat-labile enterotoxin (LT) cause moderate-to-severe diarrhea (MSD) in developing country children. The Global Enteric Multicenter Study (GEMS) identified ETEC encoding ST among the top four enteropathogens. Since the GEMS objective was to provide evidence to guide development and implementation of enteric vaccines and other interventions to diminish diarrheal disease morbidity and mortality, we examined colonization factor (CF) prevalence among ETEC isolates from children age <5 years with MSD and from matched controls in four African and three Asian sites. We also assessed strength of association of specific CFs with MSD., Methodology/principal Findings: MSD cases enrolled at healthcare facilities over three years and matched controls were tested in a standardized manner for many enteropathogens. To identify ETEC, three E. coli colonies per child were tested by polymerase chain reaction (PCR) to detect genes encoding LT, ST; confirmed ETEC were examined by PCR for major CFs (Colonization Factor Antigen I [CFA/I] or Coli Surface [CS] antigens CS1-CS6) and minor CFs (CS7, CS12, CS13, CS14, CS17, CS18, CS19, CS20, CS21, CS30). ETEC from 806 cases had a single toxin/CF profile in three tested strains per child. Major CFs, components of multiple ETEC vaccine candidates, were detected in 66.0% of LT/ST and ST-only cases and were associated with MSD versus matched controls by conditional logistic regression (p≤0.006); major CFs detected in only 25.0% of LT-only cases weren't associated with MSD. ETEC encoding exclusively CS14, identified among 19.9% of 291 ST-only and 1.5% of 259 LT/ST strains, were associated with MSD (p = 0.0011). No other minor CF exhibited prevalence ≥5% and significant association with MSD., Conclusions/significance: Major CF-based efficacious ETEC vaccines could potentially prevent up to 66% of pediatric MSD cases due to ST-encoding ETEC in developing countries; adding CS14 extends coverage to ~77%., Competing Interests: I have read the journal's policy and the authors of this manuscript have the following competing interests. We note that the following authors are involved in the development of vaccines to prevent diarrhea caused by enterotoxigenic Escherichia coli: James P. Nataro: Has been named in patents for technology that may have relevance for ETEC vaccine technology; JPN is also a co-investigator on grants from non-profit agencies that support ETEC vaccine development. Halvor Sommerfelt: Has been named in patents for technology that may have relevance for ETEC vaccine technology including: INT Application Number PCT/IB2014/000267; INT Publication Number WO2014128555 A2 “ETEC Vaccine”. European Patent Application No. 14711297.3 United States Patent Application No. 14/769,342. China Patent Application No. 201480022329.6. Puntervoll P, Sommerfelt H, Clements J, Nataro JP, Zhang W, Taxt A. HS is also a co-investigator on grants from non-profit agencies that support ETEC vaccine development Ann-Mari Svennerholm: Has shares in the University of Göteborg spin-out biotech company Gotovax AB which is entitled to royalty from Scandinavian Biopharma on sales in travelers of the ETEC vaccine Etvax if it becomes a commercial product. A-MS is a co-inventor on ETEC vaccine patent application owned by Scandinavian Biopharma and has a research grant from the Swedish Foundation for Strategic Research for infection biology research. Myron M. Levine: Is a co-inventor of patents for ETEC vaccine technology including US patent #6,902,736 B2. “Isolation and characterization of the CSA operon (ETEC-CS4 pili) and methods of using same.” He is a member of the Scientific Advisory Board of the PaxVax Corporation. MML is also the recipient for grants relevant to ETEC vaccine development including the Enteric Center of Excellence for Translational Research (Enteric-CETR) “Immunoprophylactic Strategies to Control Emerging Enteric Infections” (NIAID U19AI109776; MML, PI)

Published

2019

31. Maternal Influenza Vaccination and the Risk of Laboratory-Confirmed Influenza Among Household Contacts Under the Age of Five in Mali.

Author

Buchwald AG, Tamboura B, Haidara FC, Coulibaly F, Doumbia M, Diallo F, Boudova S, Keita AM, Sow SO, Kotloff K, Levine M, and Tapia MD

Subjects

Adult, Child, Preschool, Family, Female, Humans, Incidence, Infant, Influenza A Virus, H1N1 Subtype isolation & purification, Influenza Vaccines therapeutic use, Influenza, Human prevention & control, Male, Mali, Mothers, Pregnancy, Risk Factors, Influenza Vaccines administration & dosage, Influenza, Human diagnosis, Influenza, Human transmission, Vaccination statistics & numerical data

Abstract

Influenza transmission is increased among household contacts. Vaccination decreases transmission; however it is unclear how vaccinating a single individual alters disease risk among household contacts, particularly in regions with low vaccination coverage. Pregnant women were randomized to influenza or control vaccination. Households were visited weekly until infants born to enrolled women reached 6 months. Household contacts younger than 5 years were tested for laboratory-confirmed influenza (LCI). Incidence of LCI and rate ratios (RtR) comparing incidence between vaccine groups were calculated. The secondary infection rate (SIR) was calculated for households where LCI was detected. The H1N1 strain in the vaccine was a match for circulating H1N1 during the study, thus, all analyses were performed for H1N1-LCI and any LCI. A total of 5,345 household contacts younger than 5 years followed for a mean of 228 days (standard deviation [SD] = 45 days) experienced 2,957 influenza-like illness episodes. Incidence of any LCI and H1N1-LCI was 23 ( N = 276) and 7.3 per 100,000 days ( N = 89), respectively. Household contacts of women who received influenza vaccine had fewer LCI (RtR = 0.90; 95% CI: 0.71, 1.14) and fewer H1N1-LCI (RtR = 0.73; 95% CI: 0.48, 1.11) episodes than contacts in control households. Incidence of LCI and household SIR were low in households of women enrolled in an influenza vaccine trial in Mali. Although low incidence made statistical significance difficult to detect, there was a trend for decreased rates of H1N1-LCI in households where a pregnant mother received influenza vaccination.

Published

2019

32. Characterization of Invasive Salmonella Serogroup C1 Infections in Mali.

Author

Fuche FJ, Sen S, Jones JA, Nkeze J, Permala-Booth J, Tapia MD, Sow SO, Tamboura B, Touré A, Onwuchekwa U, Sylla M, Kotloff KL, and Tennant SM

Subjects

Adolescent, Child, Child, Preschool, Female, Gastroenteritis epidemiology, Humans, Infant, Male, Mali epidemiology, Salmonella Infections epidemiology, Salmonella enteritidis pathogenicity, Salmonella typhimurium pathogenicity, Serogroup, Gastroenteritis etiology, Incidence, Salmonella Infections diagnosis

Abstract

Nontyphoidal Salmonella (NTS) are the leading cause of foodborne infections worldwide and a major cause of bloodstream infections in infants and HIV-infected adults in sub-Saharan Africa (SSA). Salmonella Typhimurium (serogroup B) and Salmonella Enteritidis (serogroup D) are the most common serovars in this region. However, data describing rarer invasive NTS serovars, particularly those belonging to serogroups C1 and C2, circulating in SSA are lacking. We previously conducted systematic blood culture surveillance on pediatric patients in Bamako, Mali, from 2002 to 2014, and the results showed that serovars Typhimurium and Enteritidis accounted for 32% and 36% of isolates, respectively. Here, we present data on 27 Salmonella serogroup C1 strains that were isolated during this previous study. The strains were typed by serum agglutination and multilocus sequence typing (MLST). Sixteen strains were Salmonella Paratyphi C, four were Salmonella Colindale, and two were Salmonella Virchow. Interestingly, five strains were identified as the very rare Salmonella Brazzaville using a combination of serum agglutination and flagellin gene typing. Phenotypic characterization showed that Salmonella Brazzaville produced biofilm and exhibited catalase activity, which were not statistically different from the gastroenteritis-associated Salmonella Typhimurium sequence type (ST) 19. All tested Salmonella Paratyphi C strains were poor biofilm producers and showed significantly less catalase activity than Salmonella Typhimurium ST19. Overall, our study provides insight into the Salmonella serogroup C1 serovars that cause invasive disease in infants in Mali. In addition, we show that MLST and flagellin gene sequencing, in association with traditional serum agglutination, are invaluable tools to help identify rare Salmonella serovars.

Published

2018

33. Meningococcal carriage within households in the African meningitis belt: A longitudinal pilot study.

Author

Basta NE, Berthe A, Keita M, Onwuchekwa U, Tamboura B, Traore A, Hassan-King M, Manigart O, Nascimento M, Stuart JM, Trotter C, Blake J, Carr AD, Gray SJ, Newbold LS, Deng Y, Wolfson J, Halloran ME, Greenwood B, Borrow R, and Sow SO

Subjects

Adolescent, Adult, Child, Child, Preschool, Cross-Sectional Studies, Family Characteristics, Female, Humans, Infant, Longitudinal Studies, Male, Mali epidemiology, Mass Screening, Meningitis, Meningococcal epidemiology, Meningococcal Infections transmission, Neisseria meningitidis, Serogroup A isolation & purification, Pharynx microbiology, Pilot Projects, Young Adult, Carrier State epidemiology, Carrier State microbiology, Meningococcal Infections epidemiology, Neisseria meningitidis isolation & purification

Abstract

Objectives: Carriers of Neisseria meningitidis are a key source of transmission. In the African meningitis belt, where risk of meningococcal disease is highest, a greater understanding of meningococcal carriage dynamics is needed., Methods: We randomly selected an age-stratified sample of 400 residents from 116 households in Bamako, Mali, and collected pharyngeal swabs in May 2010. A month later, we enrolled all 202 residents of 20 of these households (6 with known carriers) and collected swabs monthly for 6 months prior to MenAfriVac vaccine introduction and returned 10 months later to collect swabs monthly for 3 months. We used standard bacteriological methods to identify N. meningitidis carriers and fit hidden Markov models to assess acquisition and clearance overall and by sex and age., Results: During the cross-sectional study 5.0% of individuals (20/400) were carriers. During the longitudinal study, 73 carriage events were identified from 1422 swabs analyzed, and 16.3% of individuals (33/202) were identified as carriers at least once. The majority of isolates were non-groupable; no serogroup A carriers were identified., Conclusions: Our results suggest that the duration of carriage with any N. meningitidis averages 2.9 months and that males and children acquire and lose carriage more frequently in an urban setting in Mali. Our study informed the design of a larger study implemented in seven countries of the African meningitis belt., (Copyright © 2017 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2018

34. Direct Detection of Shigella in Stool Specimens by Use of a Metagenomic Approach.

Author

Liu J, Almeida M, Kabir F, Shakoor S, Qureshi S, Zaidi A, Li S, Tamboura B, Sow SO, Mandomando I, Alonso PL, Ramamurthy T, Sur D, Kotloff K, Nataro J, Levine MM, Stine OC, and Houpt E

Subjects

Computational Biology, DNA, Bacterial genetics, Dysentery, Bacillary microbiology, Feces chemistry, Humans, Phylogeny, Real-Time Polymerase Chain Reaction, Sensitivity and Specificity, Sequence Analysis, DNA, Shigella classification, Shigella genetics, Software, Bacteriological Techniques methods, Dysentery, Bacillary diagnosis, Feces microbiology, Metagenomics, Shigella isolation & purification

Abstract

The underestimation of Shigella species as a cause of childhood diarrhea disease has become increasingly apparent with quantitative PCR (qPCR)-based diagnostic methods versus culture. We sought to confirm qPCR-based detection of Shigella via a metagenomics approach. Three groups of samples were selected from diarrheal cases from the Global Enteric Multicenter Study: nine Shigella culture-positive and qPCR-positive (culture + qPCR + ) samples, nine culture-negative but qPCR-positive (culture - qPCR + ) samples, and nine culture-negative and qPCR-negative (culture - qPCR - ) samples. Fecal DNA was sequenced using paired-end Illumina HiSeq, whereby 3.26 × 10 8 ± 5.6 × 10 7 high-quality reads were generated for each sample. We used Kraken software to compare the read counts specific to " Shigella " among the three groups. The proportions of Shigella -specific nonhuman sequence reads between culture + qPCR + (0.65 ± 0.42%) and culture - qPCR + (0.55 ± 0.31%) samples were similar (Mann-Whitney U test, P = 0.627) and distinct from the culture - qPCR - group (0.17 ± 0.15%, P < 0.05). The read counts of sequences previously targeted by Shigella/ enteroinvasive Escherichia coli (EIEC) qPCR assays, namely, ipaH , virA , virG , ial , ShET2 , and ipaH3 , were also similar between the culture + qPCR + and culture - qPCR + groups and distinct from the culture - qPCR - groups ( P < 0.001). Kraken performed well versus other methods: its precision and recall of Shigella were excellent at the genus level but variable at the species level. In summary, metagenomic sequencing indicates that Shigella /EIEC qPCR-positive samples are similar to those of Shigella culture-positive samples in Shigella sequence composition, thus supporting qPCR as an accurate method for detecting Shigella ., (Copyright © 2018 Liu et al.)

Published

2018

35. Randomized, Placebo-Controlled, Double-Blind Phase 2 Trial Comparing the Reactogenicity and Immunogenicity of a Single Standard Dose to Those of a High Dose of CVD 103-HgR Live Attenuated Oral Cholera Vaccine, with Shanchol Inactivated Oral Vaccine as an Open-Label Immunologic Comparator.

Author

Sow SO, Tapia MD, Chen WH, Haidara FC, Kotloff KL, Pasetti MF, Blackwelder WC, Traoré A, Tamboura B, Doumbia M, Diallo F, Coulibaly F, Onwuchekwa U, Kodio M, Tennant SM, Reymann M, Lam DF, Gurwith M, Lock M, Yonker T, Smith J, Simon JK, and Levine MM

Subjects

Administration, Oral, Adult, Antibodies, Bacterial immunology, Double-Blind Method, Female, Humans, Male, Vaccination methods, Young Adult, Cholera immunology, Cholera Vaccines immunology, Cholera Vaccines pharmacology, Immunogenicity, Vaccine immunology, Vaccines, Attenuated immunology

Abstract

Reactive immunization with a single-dose cholera vaccine that could rapidly (within days) protect immunologically naive individuals during virgin soil epidemics, when cholera reaches immunologically naive populations that have not experienced cholera for decades, would facilitate cholera control. One dose of attenuated Vibrio cholerae O1 classical Inaba vaccine CVD 103-HgR (Vaxchora) containing ≥2 × 10 8 CFU induces vibriocidal antibody seroconversion (a correlate of protection) in >90% of U.S. adults. A previous CVD 103-HgR commercial formulation required ≥2 × 10 9 CFU to elicit high levels of seroconversion in populations in developing countries. We compared the vibriocidal responses of Malians (individuals 18 to 45 years old) randomized to ingest a single ≥2 × 10 8 -CFU standard dose ( n = 50) or a ≥2 × 10 9 -CFU high dose ( n = 50) of PaxVax CVD 103-HgR with buffer or two doses ( n = 50) of Shanchol inactivated cholera vaccine (the immunologic comparator). To maintain blinding, participants were dosed twice 2 weeks apart; CVD 103-HgR recipients ingested placebo 2 weeks before or after ingesting vaccine. Seroconversion (a ≥4-fold vibriocidal titer rise) between the baseline and 14 days after CVD 103-HgR ingestion and following the first and second doses of Shanchol were the main outcomes measured. By day 14 postvaccination, the rates of seroconversion after ingestion of a single standard dose and a high dose of CVD 103-HgR were 71.7% (33/46 participants) and 83.3% (40/48 participants), respectively. The rate of seroconversion following the first dose of Shanchol, 56.0% (28/50 participants), was significantly lower than that following the high dose of CVD 103-HgR ( P = 0.003). The vibriocidal geometric mean titer (GMT) of the high dose of CVD 103-HgR exceeded the GMT of the standard dose at day 14 (214 versus 95, P = 0.045) and was ∼2-fold higher than the GMT on day 7 and day 14 following the first Shanchol dose ( P > 0.05). High-dose CVD 103-HgR is recommended for accelerated evaluation in developing countries to assess its efficacy and practicality in field situations. (This study has been registered at ClinicalTrials.gov under registration no. NCT02145377.)., (Copyright © 2017 Sow et al.)

Published

2017

36. Epidemiology of influenza in West Africa after the 2009 influenza A(H1N1) pandemic, 2010-2012.

Author

Talla Nzussouo N, Duque J, Adedeji AA, Coulibaly D, Sow S, Tarnagda Z, Maman I, Lagare A, Makaya S, Elkory MB, Kadjo Adje H, Shilo PA, Tamboura B, Cisse A, Badziklou K, Maïnassara HB, Bara AO, Keita AM, Williams T, Moen A, Widdowson MA, and McMorrow M

Subjects

Adolescent, Adult, Africa, Western epidemiology, Aged, Child, Child, Preschool, Female, Humans, Infant, Influenza A Virus, H1N1 Subtype pathogenicity, Influenza A Virus, H3N2 Subtype pathogenicity, Influenza, Human virology, Male, Middle Aged, Seasons, Severe Acute Respiratory Syndrome epidemiology, Severe Acute Respiratory Syndrome virology, Young Adult, Influenza, Human epidemiology

Abstract

Background: Over the last decade, capacity for influenza surveillance and research in West Africa has strengthened. Data from these surveillance systems showed influenza A(H1N1)pdm09 circulated in West Africa later than in other regions of the continent., Methods: We contacted 11 West African countries to collect information about their influenza surveillance systems (number of sites, type of surveillance, sampling strategy, populations sampled, case definitions used, number of specimens collected and number of specimens positive for influenza viruses) for the time period January 2010 through December 2012., Results: Of the 11 countries contacted, 8 responded: Burkina Faso, Cote d'Ivoire, Mali, Mauritania, Niger, Nigeria, Sierra Leone and Togo. Countries used standard World Health Organization (WHO) case definitions for influenza-like illness (ILI) and severe acute respiratory illness (SARI) or slight variations thereof. There were 70 surveillance sites: 26 SARI and 44 ILI. Seven countries conducted SARI surveillance and collected 3114 specimens of which 209 (7%) were positive for influenza viruses. Among influenza-positive SARI patients, 132 (63%) were influenza A [68 influenza A(H1N1)pdm09, 64 influenza A(H3N2)] and 77 (37%) were influenza B. All eight countries conducted ILI surveillance and collected 20,375 specimens, of which 2278 (11%) were positive for influenza viruses. Among influenza-positive ILI patients, 1431 (63%) were influenza A [820 influenza A(H1N1)pdm09, 611 influenza A(H3N2)] and 847 (37%) were influenza B. A majority of SARI and ILI case-patients who tested positive for influenza (72% SARI and 59% ILI) were children aged 0-4 years, as were a majority of those enrolled in surveillance. The seasonality of influenza and the predominant influenza type or subtype varied by country and year., Conclusions: Influenza A(H1N1)pdm09 continued to circulate in West Africa along with influenza A(H3N2) and influenza B during 2010-2012. Although ILI surveillance systems produced a robust number of samples during the study period, more could be done to strengthen surveillance among hospitalized SARI case-patients. Surveillance systems captured young children but lacked data on adults and the elderly. More data on risk groups for severe influenza in West Africa are needed to help shape influenza prevention and clinical management policies and guidelines.

Published

2017

37. The Effect of Antibiotic Exposure and Specimen Volume on the Detection of Bacterial Pathogens in Children With Pneumonia.

Author

Driscoll AJ, Deloria Knoll M, Hammitt LL, Baggett HC, Brooks WA, Feikin DR, Kotloff KL, Levine OS, Madhi SA, O'Brien KL, Scott JAG, Thea DM, Howie SRC, Adrian PV, Ahmed D, DeLuca AN, Ebruke BE, Gitahi C, Higdon MM, Kaewpan A, Karani A, Karron RA, Mazumder R, McLellan J, Moore DP, Mwananyanda L, Park DE, Prosperi C, Rhodes J, Saifullah M, Seidenberg P, Sow SO, Tamboura B, Zeger SL, and Murdoch DR

Subjects

Anti-Bacterial Agents administration & dosage, Bacteria genetics, Bacteria pathogenicity, Bacteriological Techniques, Case-Control Studies, Child, Preschool, Female, Humans, Infant, Infant, Newborn, Internationality, Male, Molecular Diagnostic Techniques, Nasopharynx microbiology, Oropharynx microbiology, Pneumonia, Bacterial drug therapy, Pneumonia, Bacterial etiology, Real-Time Polymerase Chain Reaction, Sputum microbiology, Streptococcus pneumoniae genetics, Anti-Bacterial Agents therapeutic use, Bacteria drug effects, Bacteria isolation & purification, Pneumonia, Bacterial diagnosis, Pneumonia, Bacterial microbiology

Abstract

Background.: Antibiotic exposure and specimen volume are known to affect pathogen detection by culture. Here we assess their effects on bacterial pathogen detection by both culture and polymerase chain reaction (PCR) in children., Methods.: PERCH (Pneumonia Etiology Research for Child Health) is a case-control study of pneumonia in children aged 1-59 months investigating pathogens in blood, nasopharyngeal/oropharyngeal (NP/OP) swabs, and induced sputum by culture and PCR. Antibiotic exposure was ascertained by serum bioassay, and for cases, by a record of antibiotic treatment prior to specimen collection. Inoculated blood culture bottles were weighed to estimate volume., Results.: Antibiotic exposure ranged by specimen type from 43.5% to 81.7% in 4223 cases and was detected in 2.3% of 4863 controls. Antibiotics were associated with a 45% reduction in blood culture yield and approximately 20% reduction in yield from induced sputum culture. Reduction in yield of Streptococcus pneumoniae from NP culture was approximately 30% in cases and approximately 32% in controls. Several bacteria had significant but marginal reductions (by 5%-7%) in detection by PCR in NP/OP swabs from both cases and controls, with the exception of S. pneumoniae in exposed controls, which was detected 25% less frequently compared to nonexposed controls. Bacterial detection in induced sputum by PCR decreased 7% for exposed compared to nonexposed cases. For every additional 1 mL of blood culture specimen collected, microbial yield increased 0.51% (95% confidence interval, 0.47%-0.54%), from 2% when volume was ≤1 mL to approximately 6% for ≥3 mL., Conclusions.: Antibiotic exposure and blood culture volume affect detection of bacterial pathogens in children with pneumonia and should be accounted for in studies of etiology and in clinical management., (© The Author 2017. Published by Oxford University Press for the Infectious Diseases Society of America.)

Published

2017

38. Evaluation of Pneumococcal Load in Blood by Polymerase Chain Reaction for the Diagnosis of Pneumococcal Pneumonia in Young Children in the PERCH Study.

Author

Deloria Knoll M, Morpeth SC, Scott JAG, Watson NL, Park DE, Baggett HC, Brooks WA, Feikin DR, Hammitt LL, Howie SRC, Kotloff KL, Levine OS, O'Brien KL, Thea DM, Ahmed D, Antonio M, Awori JO, Baillie VL, Chipeta J, Deluca AN, Dione M, Driscoll AJ, Higdon MM, Jatapai A, Karron RA, Mazumder R, Moore DP, Mwansa J, Nyongesa S, Prosperi C, Seidenberg P, Siludjai D, Sow SO, Tamboura B, Zeger SL, Murdoch DR, and Madhi SA

Subjects

Case-Control Studies, Child, Preschool, Female, Genes, Bacterial, Humans, Infant, Infant, Newborn, Internationality, Male, Nasopharynx microbiology, Real-Time Polymerase Chain Reaction methods, Streptococcus pneumoniae genetics, Streptococcus pneumoniae isolation & purification, Bacterial Load, DNA, Bacterial blood, Pneumonia, Pneumococcal diagnosis, Pneumonia, Pneumococcal microbiology, Streptococcus pneumoniae physiology

Abstract

Background.: Detection of pneumococcus by lytA polymerase chain reaction (PCR) in blood had poor diagnostic accuracy for diagnosing pneumococcal pneumonia in children in 9 African and Asian sites. We assessed the value of blood lytA quantification in diagnosing pneumococcal pneumonia., Methods.: The Pneumonia Etiology Research for Child Health (PERCH) case-control study tested whole blood by PCR for pneumococcus in children aged 1-59 months hospitalized with signs of pneumonia and in age-frequency matched community controls. The distribution of load among PCR-positive participants was compared between microbiologically confirmed pneumococcal pneumonia (MCPP) cases, cases confirmed for nonpneumococcal pathogens, nonconfirmed cases, and controls. Receiver operating characteristic analyses determined the "optimal threshold" that distinguished MCPP cases from controls., Results.: Load was available for 290 of 291 cases with pneumococcal PCR detected in blood and 273 of 273 controls. Load was higher in MCPP cases than controls (median, 4.0 × 103 vs 0.19 × 103 copies/mL), but overlapped substantially (range, 0.16-989.9 × 103 copies/mL and 0.01-551.9 × 103 copies/mL, respectively). The proportion with high load (≥2.2 log10 copies/mL) was 62.5% among MCPP cases, 4.3% among nonconfirmed cases, 9.3% among cases confirmed for a nonpneumococcal pathogen, and 3.1% among controls. Pneumococcal load in blood was not associated with respiratory tract illness in controls (P = .32). High blood pneumococcal load was associated with alveolar consolidation on chest radiograph in nonconfirmed cases, and with high (>6.9 log10 copies/mL) nasopharyngeal/oropharyngeal load and C-reactive protein ≥40 mg/L (both P < .01) in nonconfirmed cases but not controls., Conclusions.: Quantitative pneumococcal PCR in blood has limited diagnostic utility for identifying pneumococcal pneumonia in individual children, but may be informative in epidemiological studies., (© The Author 2017. Published by Oxford University Press for the Infectious Diseases Society of America.)

Published

2017

39. Detection of Pneumococcal DNA in Blood by Polymerase Chain Reaction for Diagnosing Pneumococcal Pneumonia in Young Children From Low- and Middle-Income Countries.

Author

Morpeth SC, Deloria Knoll M, Scott JAG, Park DE, Watson NL, Baggett HC, Brooks WA, Feikin DR, Hammitt LL, Howie SRC, Kotloff KL, Levine OS, Madhi SA, O'Brien KL, Thea DM, Adrian PV, Ahmed D, Antonio M, Bunthi C, DeLuca AN, Driscoll AJ, Githua LP, Higdon MM, Kahn G, Karani A, Karron RA, Kwenda G, Makprasert S, Mazumder R, Moore DP, Mwansa J, Nyongesa S, Prosperi C, Sow SO, Tamboura B, Whistler T, Zeger SL, and Murdoch DR

Subjects

Child, Hospitalized, Child, Preschool, Female, Humans, Infant, Infant, Newborn, Internationality, Male, N-Acetylmuramoyl-L-alanine Amidase genetics, Pneumonia, Pneumococcal microbiology, Polymerase Chain Reaction methods, Poverty, Sensitivity and Specificity, Streptococcus pneumoniae genetics, DNA, Bacterial blood, Pneumonia, Pneumococcal diagnosis, Streptococcus pneumoniae isolation & purification

Abstract

Background.: We investigated the performance of polymerase chain reaction (PCR) on blood in the diagnosis of pneumococcal pneumonia among children from 7 low- and middle-income countries., Methods.: We tested blood by PCR for the pneumococcal autolysin gene in children aged 1-59 months in the Pneumonia Etiology Research for Child Health (PERCH) study. Children had World Health Organization-defined severe or very severe pneumonia or were age-frequency-matched community controls. Additionally, we tested blood from general pediatric admissions in Kilifi, Kenya, a PERCH site. The proportion PCR-positive was compared among cases with microbiologically confirmed pneumococcal pneumonia (MCPP), cases without a confirmed bacterial infection (nonconfirmed), cases confirmed for nonpneumococcal bacteria, and controls., Results.: In PERCH, 7.3% (n = 291/3995) of cases and 5.5% (n = 273/4987) of controls were blood pneumococcal PCR-positive (P < .001), compared with 64.3% (n = 36/56) of MCPP cases and 6.3% (n = 243/3832) of nonconfirmed cases (P < .001). Blood pneumococcal PCR positivity was higher in children from the 5 African countries (5.5%-11.5% among cases and 5.3%-10.2% among controls) than from the 2 Asian countries (1.3% and 1.0% among cases and 0.8% and 0.8% among controls). Among Kilifi general pediatric admissions, 3.9% (n = 274/6968) were PCR-positive, including 61.7% (n = 37/60) of those with positive blood cultures for pneumococcus., Discussion.: The utility of pneumococcal PCR on blood for diagnosing childhood pneumococcal pneumonia in the 7 low- and middle-income countries studied is limited by poor specificity and by poor sensitivity among MCPP cases., (© The Author 2017. Published by Oxford University Press for the Infectious Diseases Society of America.)

Published

2017

40. Standardization of Laboratory Methods for the PERCH Study.

Author

Driscoll AJ, Karron RA, Morpeth SC, Bhat N, Levine OS, Baggett HC, Brooks WA, Feikin DR, Hammitt LL, Howie SRC, Knoll MD, Kotloff KL, Madhi SA, Scott JAG, Thea DM, Adrian PV, Ahmed D, Alam M, Anderson TP, Antonio M, Baillie VL, Dione M, Endtz HP, Gitahi C, Karani A, Kwenda G, Maiga AA, McClellan J, Mitchell JL, Morailane P, Mugo D, Mwaba J, Mwansa J, Mwarumba S, Nyongesa S, Panchalingam S, Rahman M, Sawatwong P, Tamboura B, Toure A, Whistler T, O'Brien KL, and Murdoch DR

Subjects

Algorithms, Child, Preschool, Data Accuracy, Female, HIV Infections, Humans, Infant, Male, Pneumonia, Bacterial diagnosis, Pneumonia, Viral diagnosis, Quality Control, Reference Standards, Respiratory Tract Infections etiology, Clinical Laboratory Techniques standards, Pneumonia diagnosis, Pneumonia etiology, Specimen Handling standards

Abstract

The Pneumonia Etiology Research for Child Health study was conducted across 7 diverse research sites and relied on standardized clinical and laboratory methods for the accurate and meaningful interpretation of pneumonia etiology data. Blood, respiratory specimens, and urine were collected from children aged 1-59 months hospitalized with severe or very severe pneumonia and community controls of the same age without severe pneumonia and were tested with an extensive array of laboratory diagnostic tests. A standardized testing algorithm and standard operating procedures were applied across all study sites. Site laboratories received uniform training, equipment, and reagents for core testing methods. Standardization was further assured by routine teleconferences, in-person meetings, site monitoring visits, and internal and external quality assurance testing. Targeted confirmatory testing and testing by specialized assays were done at a central reference laboratory., (© The Author 2017. Published by Oxford University Press for the Infectious Diseases Society of America.)

Published

2017

41. Aeromonas-Associated Diarrhea in Children Under 5 Years: The GEMS Experience.

Author

Qamar FN, Nisar MI, Quadri F, Shakoor S, Sow SO, Nasrin D, Blackwelder WC, Wu Y, Farag T, Panchalingham S, Sur D, Qureshi S, Faruque AS, Saha D, Alonso PL, Breiman RF, Bassat Q, Tamboura B, Ramamurthy T, Kanungo S, Ahmed S, Hossain A, Das SK, Antonio M, Hossain MJ, Mandomando I, Tennant SM, Kotloff KL, Levine MM, and Zaidi AK

Subjects

Africa South of the Sahara epidemiology, Bangladesh epidemiology, Case-Control Studies, Child, Preschool, Coinfection, Diarrhea etiology, Diarrhea microbiology, Dysentery epidemiology, Dysentery etiology, Dysentery microbiology, Dysentery, Bacillary complications, Dysentery, Bacillary microbiology, Female, Gram-Negative Bacterial Infections complications, Gram-Negative Bacterial Infections microbiology, Humans, Infant, Logistic Models, Male, Pakistan epidemiology, Risk Factors, Socioeconomic Factors, Aeromonas isolation & purification, Diarrhea epidemiology, Dysentery, Bacillary epidemiology, Gram-Negative Bacterial Infections epidemiology, Shigella isolation & purification

Abstract

We report the clinical findings, epidemiology, and risk factors for moderate-to-severe diarrhea (MSD) associated with Aeromonas species in children 0-59 months of age, from the Global Enteric Multicenter Study, conducted at three sites in south Asia and four sites in sub-Saharan Africa. Children with MSD were enrolled along with controls matched for age, gender, and neighborhood. Pooled, age-stratified conditional logistic regression models were applied to evaluate the association of Aeromonas infection controlling for coinfecting pathogens and sociodemographic variables. A pooled, age-stratified, multivariate logistic regression analysis was done to identify risk factors associated with Aeromonas positivity in MSD cases. A total of 12,110 cases and 17,291 matched controls were enrolled over a period of 48 months. Aeromonas was identified as a significant pathogen in 736 cases of MSD in Pakistan and Bangladesh (22.2%). Aeromonas remained a significant pathogen even after adjustment for the presence of other pathogens and sociodemographic factors. Odds ratio (OR) for Aeromonas were higher in the presence of Shigella (matched OR: 6.2, 95% confidence interval [CI]: 1.9-20.2). Cases of Aeromonas were likely to present with dysentery, particularly in the 0-11 months (OR: 1.4, 95% CI 1.0-2.0) and 12-23 months (OR: 1.8, 95% CI: 1.3-2.5) age group. The odds of Aeromonas increased with increasing degree of stunting, being highest for severe stunting (OR: 10.1, 95% CI: 3.6-28.9). Aeromonas is a significant pathogen for MSD in Pakistan and Bangladesh. Presence of dysentery and co-occurrence with other pathogens, notably Shigella spp. are significant features of Aeromonas-associated diarrhea., Competing Interests: Farah Naz Qamar received research training support from the National Institute of Health's Fogarty International Center (1 D43 TW007585-01)., (© The American Society of Tropical Medicine and Hygiene.)

Published

2016

42. Use of quantitative molecular diagnostic methods to identify causes of diarrhoea in children: a reanalysis of the GEMS case-control study.

Author

Liu J, Platts-Mills JA, Juma J, Kabir F, Nkeze J, Okoi C, Operario DJ, Uddin J, Ahmed S, Alonso PL, Antonio M, Becker SM, Blackwelder WC, Breiman RF, Faruque AS, Fields B, Gratz J, Haque R, Hossain A, Hossain MJ, Jarju S, Qamar F, Iqbal NT, Kwambana B, Mandomando I, McMurry TL, Ochieng C, Ochieng JB, Ochieng M, Onyango C, Panchalingam S, Kalam A, Aziz F, Qureshi S, Ramamurthy T, Roberts JH, Saha D, Sow SO, Stroup SE, Sur D, Tamboura B, Taniuchi M, Tennant SM, Toema D, Wu Y, Zaidi A, Nataro JP, Kotloff KL, Levine MM, and Houpt ER

Subjects

Adenoviridae isolation & purification, Adenoviridae pathogenicity, Africa epidemiology, Asia epidemiology, Bacteria isolation & purification, Bacteria pathogenicity, Bacterial Infections diagnosis, Campylobacter isolation & purification, Campylobacter pathogenicity, Case-Control Studies, Child, Preschool, Coinfection, Cryptosporidium isolation & purification, Cryptosporidium pathogenicity, Diarrhea epidemiology, Escherichia coli isolation & purification, Escherichia coli pathogenicity, Female, Humans, Incidence, Infant, Male, Rotavirus isolation & purification, Rotavirus pathogenicity, Shigella isolation & purification, Shigella pathogenicity, Virus Diseases diagnosis, Viruses isolation & purification, Viruses pathogenicity, Cost of Illness, Diarrhea microbiology, Diarrhea virology

Abstract

Background: Diarrhoea is the second leading cause of mortality in children worldwide, but establishing the cause can be complicated by diverse diagnostic approaches and varying test characteristics. We used quantitative molecular diagnostic methods to reassess causes of diarrhoea in the Global Enteric Multicenter Study (GEMS)., Methods: GEMS was a study of moderate to severe diarrhoea in children younger than 5 years in Africa and Asia. We used quantitative real-time PCR (qPCR) to test for 32 enteropathogens in stool samples from cases and matched asymptomatic controls from GEMS, and compared pathogen-specific attributable incidences with those found with the original GEMS microbiological methods, including culture, EIA, and reverse-transcriptase PCR. We calculated revised pathogen-specific burdens of disease and assessed causes in individual children., Findings: We analysed 5304 sample pairs. For most pathogens, incidence was greater with qPCR than with the original methods, particularly for adenovirus 40/41 (around five times), Shigella spp or enteroinvasive Escherichia coli (EIEC) and Campylobactor jejuni o C coli (around two times), and heat-stable enterotoxin-producing E coli ([ST-ETEC] around 1·5 times). The six most attributable pathogens became, in descending order, Shigella spp, rotavirus, adenovirus 40/41, ST-ETEC, Cryptosporidium spp, and Campylobacter spp. Pathogen-attributable diarrhoeal burden was 89·3% (95% CI 83·2-96·0) at the population level, compared with 51·5% (48·0-55·0) in the original GEMS analysis. The top six pathogens accounted for 77·8% (74·6-80·9) of all attributable diarrhoea. With use of model-derived quantitative cutoffs to assess individual diarrhoeal cases, 2254 (42·5%) of 5304 cases had one diarrhoea-associated pathogen detected and 2063 (38·9%) had two or more, with Shigella spp and rotavirus being the pathogens most strongly associated with diarrhoea in children with mixed infections., Interpretation: A quantitative molecular diagnostic approach improved population-level and case-level characterisation of the causes of diarrhoea and indicated a high burden of disease associated with six pathogens, for which targeted treatment should be prioritised., Funding: Bill & Melinda Gates Foundation., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

43. Maternal immunisation with trivalent inactivated influenza vaccine for prevention of influenza in infants in Mali: a prospective, active-controlled, observer-blind, randomised phase 4 trial.

Author

Tapia MD, Sow SO, Tamboura B, Tégueté I, Pasetti MF, Kodio M, Onwuchekwa U, Tennant SM, Blackwelder WC, Coulibaly F, Traoré A, Keita AM, Haidara FC, Diallo F, Doumbia M, Sanogo D, DeMatt E, Schluterman NH, Buchwald A, Kotloff KL, Chen WH, Orenstein EW, Orenstein LAV, Villanueva J, Bresee J, Treanor J, and Levine MM

Subjects

Adult, Female, Humans, Immunization, Immunization Schedule, Infant, Infant, Newborn, Influenza, Human mortality, Mali, Meningococcal Vaccines administration & dosage, Prospective Studies, Vaccination methods, Adjuvants, Immunologic administration & dosage, Influenza Vaccines administration & dosage, Influenza, Human immunology, Influenza, Human prevention & control

Abstract

Background: Despite the heightened risk of serious influenza during infancy, vaccination is not recommended in infants younger than 6 months. We aimed to assess the safety, immunogenicity, and efficacy of maternal immunisation with trivalent inactivated influenza vaccine for protection of infants against a first episode of laboratory-confirmed influenza., Methods: We did this prospective, active-controlled, observer-blind, randomised phase 4 trial at six referral centres and community health centres in Bamako, Mali. Third-trimester pregnant women (≥28 weeks' gestation) were randomly assigned (1:1), via a computer-generated, centre-specific list with alternate block sizes of six or 12, to receive either trivalent inactivated influenza vaccine or quadrivalent meningococcal vaccine. Study personnel administering vaccines were not masked to treatment allocation, but allocation was concealed from clinicians, laboratory personnel, and participants. Infants were visited weekly until age 6 months to detect influenza-like illness; laboratory-confirmed influenza diagnosed with RT-PCR. We assessed two coprimary objectives: vaccine efficacy against laboratory-confirmed influenza in infants born to women immunised any time prepartum (intention-to-treat population), and vaccine efficacy in infants born to women immunised at least 14 days prepartum (per-protocol population). The primary outcome was the occurrence of a first case of laboratory-confirmed influenza by age 6 months. This trial is registered with ClinicalTrials.gov, number NCT01430689., Findings: We did this trial from Sept 12, 2011, to Jan 28, 2014. Between Sept 12, 2011, and April 18, 2013, we randomly assigned 4193 women to receive trivalent inactivated influenza vaccine (n=2108) or quadrivalent meningococcal vaccine (n=2085). There were 4105 livebirths; 1797 (87%) of 2064 infants in the trivalent inactivated influenza vaccine group and 1793 (88%) of 2041 infants in the quadrivalent meningococcal vaccine group were followed up until age 6 months. We recorded 5279 influenza-like illness episodes in 2789 (68%) infants, of which 131 (2%) episodes were laboratory-confirmed influenza. 129 (98%) cases of laboratory-confirmed influenza were first episodes (n=77 in the quadrivalent meningococcal vaccine group vs n=52 in the trivalent inactivated influenza vaccine group). In the intention-to-treat population, overall infant vaccine efficacy was 33·1% (95% CI 3·7-53·9); in the per-protocol population, vaccine efficacy was 37·3% (7·6-57·8). Vaccine efficacy remained robust during the first 4 months of follow-up (67·9% [95% CI 35·1-85·3] by intention to treat and 70·2% [35·7-87·6] by per protocol), before diminishing during the fifth month (57·3% [30·6-74·4] and 60·7 [33·8-77·5], respectively). Adverse event rates in women and infants were similar among groups. Pain at the injection site was more common in women given quadrivalent meningococcal vaccine than in those given trivalent inactivated influenza vaccine (n=253 vs n=132; p<0·0001), although 354 [92%] reactions were mild. Obstetrical and non-obstetrical serious adverse events were reported in 60 (3%) women in the quadrivalent meningococcal vaccine group and 61 (3%) women in the trivalent inactivated influenza vaccine group. Presumed neonatal infection was more common in infants in the trivalent inactivated influenza vaccine group than in those in the quadrivalent meningococcal vaccine group (n=60 vs n=37; p=0·02). No serious adverse events were related to vaccination., Interpretation: Vaccination of pregnant women with trivalent inactivated influenza vaccine in Mali-a poorly resourced country with high infant mortality-was technically and logistically feasible and protected infants from laboratory-confirmed influenza for 4 months. With adequate financing to procure the vaccine, implementation will parallel the access to antenatal care and immunisation coverage of pregnant women with tetanus toxoid., Funding: Bill & Melinda Gates Foundation., (Copyright © 2016 Tapia et al. Open Access article distributed under the terms of CC BY. Published by Elsevier Ltd.. All rights reserved.)

Published

2016

44. The Burden of Cryptosporidium Diarrheal Disease among Children < 24 Months of Age in Moderate/High Mortality Regions of Sub-Saharan Africa and South Asia, Utilizing Data from the Global Enteric Multicenter Study (GEMS).

Author

Sow SO, Muhsen K, Nasrin D, Blackwelder WC, Wu Y, Farag TH, Panchalingam S, Sur D, Zaidi AK, Faruque AS, Saha D, Adegbola R, Alonso PL, Breiman RF, Bassat Q, Tamboura B, Sanogo D, Onwuchekwa U, Manna B, Ramamurthy T, Kanungo S, Ahmed S, Qureshi S, Quadri F, Hossain A, Das SK, Antonio M, Hossain MJ, Mandomando I, Nhampossa T, Acácio S, Omore R, Oundo JO, Ochieng JB, Mintz ED, O'Reilly CE, Berkeley LY, Livio S, Tennant SM, Sommerfelt H, Nataro JP, Ziv-Baran T, Robins-Browne RM, Mishcherkin V, Zhang J, Liu J, Houpt ER, Kotloff KL, and Levine MM

Subjects

Afghanistan epidemiology, Africa South of the Sahara epidemiology, Asia epidemiology, Case-Control Studies, Child, Preschool, Cryptosporidiosis parasitology, Cryptosporidium classification, Cryptosporidium genetics, Cryptosporidium immunology, Cryptosporidium isolation & purification, Data Mining methods, Developing Countries economics, Developing Countries statistics & numerical data, Diarrhea epidemiology, Diarrhea parasitology, Female, Gastrointestinal Diseases mortality, Gastrointestinal Diseases parasitology, Humans, Immunoassay, Incidence, India epidemiology, Infant, Infant, Newborn, Male, Polymerase Chain Reaction, Cost of Illness, Cryptosporidiosis epidemiology, Cryptosporidiosis mortality, Diarrhea mortality, Feces parasitology, Gastrointestinal Diseases epidemiology

Abstract

Background: The importance of Cryptosporidium as a pediatric enteropathogen in developing countries is recognized., Methods: Data from the Global Enteric Multicenter Study (GEMS), a 3-year, 7-site, case-control study of moderate-to-severe diarrhea (MSD) and GEMS-1A (1-year study of MSD and less-severe diarrhea [LSD]) were analyzed. Stools from 12,110 MSD and 3,174 LSD cases among children aged <60 months and from 21,527 randomly-selected controls matched by age, sex and community were immunoassay-tested for Cryptosporidium. Species of a subset of Cryptosporidium-positive specimens were identified by PCR; GP60 sequencing identified anthroponotic C. parvum. Combined annual Cryptosporidium-attributable diarrhea incidences among children aged <24 months for African and Asian GEMS sites were extrapolated to sub-Saharan Africa and South Asian regions to estimate region-wide MSD and LSD burdens. Attributable and excess mortality due to Cryptosporidium diarrhea were estimated., Findings: Cryptosporidium was significantly associated with MSD and LSD below age 24 months. Among Cryptosporidium-positive MSD cases, C. hominis was detected in 77.8% (95% CI, 73.0%-81.9%) and C. parvum in 9.9% (95% CI, 7.1%-13.6%); 92% of C. parvum tested were anthroponotic genotypes. Annual Cryptosporidium-attributable MSD incidence was 3.48 (95% CI, 2.27-4.67) and 3.18 (95% CI, 1.85-4.52) per 100 child-years in African and Asian infants, respectively, and 1.41 (95% CI, 0.73-2.08) and 1.36 (95% CI, 0.66-2.05) per 100 child-years in toddlers. Corresponding Cryptosporidium-attributable LSD incidences per 100 child-years were 2.52 (95% CI, 0.33-5.01) and 4.88 (95% CI, 0.82-8.92) in infants and 4.04 (95% CI, 0.56-7.51) and 4.71 (95% CI, 0.24-9.18) in toddlers. We estimate 2.9 and 4.7 million Cryptosporidium-attributable cases annually in children aged <24 months in the sub-Saharan Africa and India/Pakistan/Bangladesh/Nepal/Afghanistan regions, respectively, and ~202,000 Cryptosporidium-attributable deaths (regions combined). ~59,000 excess deaths occurred among Cryptosporidium-attributable diarrhea cases over expected if cases had been Cryptosporidium-negative., Conclusions: The enormous African/Asian Cryptosporidium disease burden warrants investments to develop vaccines, diagnostics and therapies.

Published

2016

45. Evolution of atypical enteropathogenic E. coli by repeated acquisition of LEE pathogenicity island variants.

Author

Ingle DJ, Tauschek M, Edwards DJ, Hocking DM, Pickard DJ, Azzopardi KI, Amarasena T, Bennett-Wood V, Pearson JS, Tamboura B, Antonio M, Ochieng JB, Oundo J, Mandomando I, Qureshi S, Ramamurthy T, Hossain A, Kotloff KL, Nataro JP, Dougan G, Levine MM, Robins-Browne RM, and Holt KE

Subjects

Africa epidemiology, Asia epidemiology, Escherichia coli Infections epidemiology, Escherichia coli Infections microbiology, Genetic Variation, Genome, Bacterial, Phylogeny, Sequence Analysis, DNA, Enteropathogenic Escherichia coli classification, Enteropathogenic Escherichia coli genetics, Escherichia coli Proteins genetics, Evolution, Molecular, Genomic Islands, Genotype, Phosphoproteins genetics

Abstract

Atypical enteropathogenic Escherichia coli (aEPEC) is an umbrella term given to E. coli that possess a type III secretion system encoded in the locus of enterocyte effacement (LEE), but lack the virulence factors (stx, bfpA) that characterize enterohaemorrhagic E. coli and typical EPEC, respectively. The burden of disease caused by aEPEC has recently increased in industrialized and developing nations, yet the population structure and virulence profile of this emerging pathogen are poorly understood. Here, we generated whole-genome sequences of 185 aEPEC isolates collected during the Global Enteric Multicenter Study from seven study sites in Asia and Africa, and compared them with publicly available E. coli genomes. Phylogenomic analysis revealed ten distinct widely distributed aEPEC clones. Analysis of genetic variation in the LEE pathogenicity island identified 30 distinct LEE subtypes divided into three major lineages. Each LEE lineage demonstrated a preferred chromosomal insertion site and different complements of non-LEE encoded effector genes, indicating distinct patterns of evolution of these lineages. This study provides the first detailed genomic framework for aEPEC in the context of the EPEC pathotype and will facilitate further studies into the epidemiology and pathogenicity of EPEC by enabling the detection and tracking of specific clones and LEE variants.

Published

2016

46. Genomic diversity of EPEC associated with clinical presentations of differing severity.

Author

Hazen TH, Donnenberg MS, Panchalingam S, Antonio M, Hossain A, Mandomando I, Ochieng JB, Ramamurthy T, Tamboura B, Qureshi S, Quadri F, Zaidi A, Kotloff KL, Levine MM, Barry EM, Kaper JB, Rasko DA, and Nataro JP

Subjects

Enteropathogenic Escherichia coli isolation & purification, Genes, Bacterial, Genomics, Humans, Phylogeny, Virulence Factors genetics, Diarrhea microbiology, Diarrhea pathology, Enteropathogenic Escherichia coli classification, Enteropathogenic Escherichia coli genetics, Escherichia coli Infections microbiology, Escherichia coli Infections pathology, Genetic Variation

Abstract

Enteropathogenic Escherichia coli (EPEC) are diarrhoeagenic E. coli, and are a significant cause of gastrointestinal illness among young children in developing countries. Typical EPEC are identified by the presence of the bundle-forming pilus encoded by a virulence plasmid, which has been linked to an increased severity of illness, while atypical EPEC lack this feature. Comparative genomics of 70 total EPEC from lethal (LI), non-lethal symptomatic (NSI) or asymptomatic (AI) cases of diarrhoeal illness in children enrolled in the Global Enteric Multicenter Study was used to investigate the genomic differences in EPEC isolates obtained from individuals with various clinical outcomes. A comparison of the genomes of isolates from different clinical outcomes identified genes that were significantly more prevalent in EPEC isolates of symptomatic and lethal outcomes than in EPEC isolates of asymptomatic outcomes. These EPEC isolates exhibited previously unappreciated phylogenomic diversity and combinations of virulence factors. These comparative results highlight the diversity of the pathogen, as well as the complexity of the EPEC virulence factor repertoire.

Published

2016

47. Invasive Nontyphoidal Salmonella Infections Among Children in Mali, 2002-2014: Microbiological and Epidemiologic Features Guide Vaccine Development.

Author

Tapia MD, Tennant SM, Bornstein K, Onwuchekwa U, Tamboura B, Maiga A, Sylla MB, Sissoko S, Kourouma N, Toure A, Malle D, Livio S, Sow SO, and Levine MM

Subjects

Adolescent, Bacteremia epidemiology, Bacteremia microbiology, Child, Child, Preschool, Communicable Diseases, Emerging, Drug Discovery, Epidemiological Monitoring, Female, Humans, Infant, Male, Mali epidemiology, Salmonella Infections mortality, Salmonella Infections prevention & control, Salmonella enterica classification, Salmonella enteritidis isolation & purification, Salmonella typhimurium isolation & purification, Seasons, Serogroup, Salmonella Infections epidemiology, Salmonella Infections microbiology, Salmonella Vaccines, Salmonella enterica isolation & purification

Abstract

Background: In 2002, following establishment of a clinical microbiology laboratory in the government hospital that admits children with severe illnesses in Bamako, Mali, surveillance to identify pathogens causing invasive bacterial infections (septicemia, bacteremia, meningitis, etc) was initiated., Methods: Parents/guardians of children aged <16 years admitted to l'Hôpital Gabriel Touré with high fever or clinical syndromes compatible with focal invasive bacterial disease were asked for consent to culture their child's blood/body fluid. Standard bacteriologic techniques speciated isolates; Salmonella serovars were determined., Results: From July 2002 through June 2014, 687 nontyphoidal Salmonella (NTS) isolates were obtained from 667 children; 667 yielded a single serovar and 20 grew 2 Salmonella serovars, 1 being NTS. Four serovars accounted for 87% of the 687 NTS isolates, including Salmonella Enteritidis (n = 244 [35.5%]), Salmonella Typhimurium (n = 221 [32.2%]), I:4,[5],12:i:- (n = 42 [6.1%]), and Salmonella Dublin (n = 89 [13.0%]). Of 553 patients with invasive NTS from whom 1 of the 4 predominant serovars was isolated in pure culture, 448 (81.0%) were aged <5 years and case fatality was 20.3%; Salmonella Enteritidis case fatality (27.8%) was higher than for other serovars (P = .0009). NTS disease showed a seasonal peak following the rainy season and into the cool, dry season. Since 2010, Salmonella Enteritidis cases have risen and Salmonella Typhimurium fallen., Conclusions: NTS has become the predominant invasive pathogen as Haemophilus influenzae type b and pneumococcal vaccine use in Mali has diminished invasive disease due to those pathogens. The age distribution and limited serovars involved make control of NTS disease by vaccines epidemiologically feasible, if products under development prove safe and efficacious., (© The Author 2015. Published by Oxford University Press on behalf of the Infectious Diseases Society of America. All rights reserved. For Permissions, please e-mail: journals.permissions@oup.com.)

Published

2015

48. Bacterial Factors Associated with Lethal Outcome of Enteropathogenic Escherichia coli Infection: Genomic Case-Control Studies.

Author

Donnenberg MS, Hazen TH, Farag TH, Panchalingam S, Antonio M, Hossain A, Mandomando I, Ochieng JB, Ramamurthy T, Tamboura B, Zaidi A, Levine MM, Kotloff K, Rasko DA, and Nataro JP

Subjects

Case-Control Studies, Child, Child, Preschool, Escherichia coli Proteins genetics, Genes, Bacterial, Genomics, Humans, Infant, Multigene Family, O Antigens genetics, Enteropathogenic Escherichia coli genetics, Escherichia coli Infections mortality

Abstract

Background: Typical enteropathogenic Escherichia coli (tEPEC) strains were associated with mortality in the Global Enteric Multicenter Study (GEMS). Genetic differences in tEPEC strains could underlie some of the variability in clinical outcome., Methods: We produced draft genome sequences of all available tEPEC strains from GEMS lethal infections (LIs) and of closely matched EPEC strains from GEMS subjects with non-lethal symptomatic infections (NSIs) and asymptomatic infections (AIs) to identify gene clusters (potential protein encoding sequences sharing ≥90% nucleotide sequence identity) associated with lethality., Results: Among 14,412 gene clusters identified, the presence or absence of 392 was associated with clinical outcome. As expected, more gene clusters were associated with LI versus AI than LI versus NSI. The gene clusters more prevalent in strains from LI than those from NSI and AI included those encoding proteins involved in O-antigen biogenesis, while clusters encoding type 3 secretion effectors EspJ and OspB were among those more prevalent in strains from non-lethal infections. One gene cluster encoding a variant of an NleG ubiquitin ligase was associated with LI versus AI, while two other nleG clusters had the opposite association. Similar associations were found for two nleG gene clusters in an additional, larger sample of NSI and AI GEMS strains., Conclusions: Particular genes are associated with lethal tEPEC infections. Further study of these factors holds potential to unravel the mechanisms underlying severe disease and to prevent adverse outcomes.

Published

2015

49. Streptococcal pharyngitis in schoolchildren in Bamako, Mali.

Author

Tapia MD, Sow SO, Tamboura B, Keita MM, Berthe A, Samake M, Nataro JP, Onwuchekwa UO, Penfound TA, Blackwelder W, Dale JB, and Kotloff KL

Subjects

Adolescent, Child, Child, Preschool, Female, Humans, Male, Mali epidemiology, Pharyngitis diagnosis, Predictive Value of Tests, Prospective Studies, Streptococcal Infections diagnosis, Students statistics & numerical data, Pharyngitis epidemiology, Pharyngitis microbiology, Streptococcal Infections epidemiology, Streptococcal Infections microbiology, Streptococcus pyogenes isolation & purification

Abstract

Background: Group A streptococcus (GAS) pharyngitis is associated with high rates of rheumatic heart disease in developing countries. We sought to identify guidelines for empiric treatment of pharyngitis in low-resource settings. To inform the design of GAS vaccines, we determined the emm types associated with pharyngitis among African schoolchildren., Methods: Surveillance for pharyngitis was conducted among children 5-16 years of age attending schools in Bamako, Mali. Students were encouraged to visit a study clinician when they had a sore throat. Enrollees underwent evaluation and throat swab for isolation of GAS. Strains were emm typed by standard methods., Results: GAS was isolated from 449 (25.5%) of the 1,759 sore throat episodes. Painful cervical adenopathy was identified in 403 children (89.8%) with GAS infection and was absent in 369 uninfected children (28.2%). Emm type was determined in 396 (88.2%) of the 449 culture-positive children; 70 types were represented and 14 types accounted for 49% of isolates. Based on the proportion of the 449 isolates bearing emm types included in the 30-valent vaccine (31.0%) plus nonvaccine types previously shown to react to vaccine-induced bactericidal antibodies (44.1%), the vaccine could protect against almost 75% of GAS infections among Bamako schoolchildren., Conclusions: Two promising strategies could reduce rheumatic heart disease in low-resource settings. Administering antibiotics to children with sore throat and tender cervical adenopathy could treat most GAS-positive children while reducing use of unnecessary antibiotics for uninfected children. Broad coverage against M types associated with pharyngitis in Bamako schoolchildren might be achieved with the 30-valent GAS vaccine under development.

Published

2015

50. Microbiota that affect risk for shigellosis in children in low-income countries.

Author

Lindsay B, Oundo J, Hossain MA, Antonio M, Tamboura B, Walker AW, Paulson JN, Parkhill J, Omore R, Faruque AS, Das SK, Ikumapayi UN, Adeyemi M, Sanogo D, Saha D, Sow S, Farag TH, Nasrin D, Li S, Panchalingam S, Levine MM, Kotloff K, Magder LS, Hungerford L, Sommerfelt H, Pop M, Nataro JP, and Stine OC

Subjects

Age Factors, Biodiversity, Case-Control Studies, Child, Preschool, Developing Countries, Diarrhea diagnosis, Diarrhea epidemiology, Diarrhea microbiology, Dysentery, Bacillary diagnosis, Feces microbiology, Feces virology, Gastrointestinal Tract microbiology, Gastrointestinal Tract virology, Genes, Bacterial, Humans, Infant, Infant, Newborn, Metagenome, Odds Ratio, RNA, Ribosomal, 16S genetics, Risk, Severity of Illness Index, Shigella classification, Dysentery, Bacillary epidemiology, Dysentery, Bacillary microbiology, Microbiota, Shigella genetics

Abstract

Pathogens in the gastrointestinal tract exist within a vast population of microbes. We examined associations between pathogens and composition of gut microbiota as they relate to Shigella spp./enteroinvasive Escherichia coli infection. We analyzed 3,035 stool specimens (1,735 nondiarrheal and 1,300 moderate-to-severe diarrheal) from the Global Enteric Multicenter Study for 9 enteropathogens. Diarrheal specimens had a higher number of enteropathogens (diarrheal mean 1.4, nondiarrheal mean 0.95; p<0.0001). Rotavirus showed a negative association with Shigella spp. in cases of diarrhea (odds ratio 0.31, 95% CI 0.17-0.55) and had a large combined effect on moderate-to-severe diarrhea (odds ratio 29, 95% CI 3.8-220). In 4 Lactobacillus taxa identified by 16S rRNA gene sequencing, the association between pathogen and disease was decreased, which is consistent with the possibility that Lactobacillus spp. are protective against Shigella spp.-induced diarrhea. Bacterial diversity of gut microbiota was associated with diarrhea status, not high levels of the Shigella spp. ipaH gene.

Published

2015