Your search keyword '"Voong Vinh, Phat"' showing total 98 results

1. Changing epidemiology and antimicrobial susceptibility of bloodstream infections at a Vietnamese infectious diseases hospital (2010–2020)

Author

Nguyen, Hoang Thu Trang, Chau, Vinh, Nguyen, Phu Huong Lan, Du, Hong Duc, Nguyen, Luong Nha Phuong, Le, Thi Quynh Ngan, Huynh, Phuong Thao, Nguyen, Thi Nguyen To, Tran, Thi Ngoc Dung, Voong, Vinh Phat, Ha, Thanh Tuyen, Nguyen, Pham Nhu Quynh, Baker, Stephen, Thwaites, Guy, Rabaa, Maia, and Pham, Duy Thanh

Published

2024

2. Development and validation of multiplex real-time PCR for simultaneous detection of six bacterial pathogens causing lower respiratory tract infections and antimicrobial resistance genes

Author

Tran Thi Ngoc Dung, Voong Vinh Phat, Chau Vinh, Nguyen Phu Huong Lan, Nguyen Luong Nha Phuong, Le Thi Quynh Ngan, Guy Thwaites, Louise Thwaites, Maia Rabaa, Anh T. K. Nguyen, and Pham Thanh Duy

Subjects

Real-time PCR, Lower respiratory tract infections, Antimicrobial resistance, Melting curve analysis, Molecular diagnostics, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background Klebsiella pneumoniae, Acinetobacter baumannii, Pseudomonas aeruginosa, Escherichia coli, Streptococcus pneumoniae and Staphylococcus aureus are major bacterial causes of lower respiratory tract infections (LRTIs) globally, leading to substantial morbidity and mortality. The rapid increase of antimicrobial resistance (AMR) in these pathogens poses significant challenges for their effective antibiotic therapy. In low-resourced settings, patients with LRTIs are prescribed antibiotics empirically while awaiting several days for culture results. Rapid pathogen and AMR gene detection could prompt optimal antibiotic use and improve outcomes. Methods Here, we developed multiplex quantitative real-time PCR using EvaGreen dye and melting curve analysis to rapidly identify six major pathogens and fourteen AMR genes directly from respiratory samples. The reproducibility, linearity, limit of detection (LOD) of real-time PCR assays for pathogen detection were evaluated using DNA control mixes and spiked tracheal aspirate. The performance of RT-PCR assays was subsequently compared with the gold standard, conventional culture on 50 tracheal aspirate and sputum specimens of ICU patients. Results The sensitivity of RT-PCR assays was 100% for K. pneumoniae, A. baumannii, P. aeruginosa, E. coli and 63.6% for S. aureus and the specificity ranged from 87.5% to 97.6%. The kappa correlation values of all pathogens between the two methods varied from 0.63 to 0.95. The limit of detection of target bacteria was 1600 CFU/ml. The quantitative results from the PCR assays demonstrated 100% concordance with quantitative culture of tracheal aspirates. Compared to culture, PCR assays exhibited higher sensitivity in detecting mixed infections and S. pneumoniae. There was a high level of concordance between the detection of AMR gene and AMR phenotype in single infections. Conclusions Our multiplex quantitative RT-PCR assays are fast and simple, but sensitive and specific in detecting six bacterial pathogens of LRTIs and their antimicrobial resistance genes and should be further evaluated for clinical utility.

Published

2024

3. The clinical features and genomic epidemiology of carbapenem-resistant Acinetobacter baumannii infections at a tertiary hospital in Vietnam

Author

Duong Thi Hong Diep, Huynh Minh Tuan, Kha My Ngoc, Chau Vinh, Tran Thi Ngoc Dung, Voong Vinh Phat, Quynh Nguyen, Dong Thi Hoai Tam, Lam Vinh Nien, Bui Thi Hanh Duyen, Cao Thi Phung, Nguyen Hoang Bac, Tran Diep Tuan, Guy Thwaites, Maia A. Rabaa, and Duy Thanh Pham

Subjects

Acinetobacter baumannii, Carbapenem resistance, Whole genome sequencing, Hospital-acquired infections, Nosocomial infections, Microbiology, QR1-502

Abstract

ABSTRACT: Objectives: To characterise the clinical features of Acinetobacter baumannii infections and investigate the phylogenetic structure and transmission dynamics of A. baumannii in Vietnam. Methods: Between 2019 and 2020, a surveillance of A. baumannii (AB) infections was conducted at a tertiary hospital in Ho Chi Minh City, Vietnam. Risk factors for in-hospital mortality were analysed using logistic regressions. Whole-genome sequence data were used to characterise genomic species, sequence types (STs), antimicrobial resistance genes, surface antigens, and phylogenetic relatedness of AB isolates. Results: Eighty-four patients with AB infections were enrolled in the study, 96% of whom were hospital-acquired. Half of the AB isolates were identified from ICU-admitted patients, while the remaining isolates were from non-ICU patients. The overall in-hospital mortality was 56%, with associated risk factors including advanced age, ICU stay, exposure to mechanical ventilation/central venous catheterization, pneumonia as source of AB infection, prior use of linezolid/aminoglycosides, and AB treatment with colistin-based therapy. Nearly 91% of isolates were carbapenem-resistant; 92% were multidrug-resistant; and 6% were colistin-resistant. ST2, ST571, and ST16 were the three dominant carbapenem-resistant A. baumannii (CRAB) genotypes, exhibiting distinct AMR gene profiles. Phylogenetic analysis of CRAB ST2 isolates together with previously published ST2 collection provided evidence of intra- and inter-hospital transmission of this clone. Conclusions: Our study highlights a high prevalence of carbapenem resistance and multidrug resistance in A. baumannii and elucidates the spread of CRAB within and between hospitals. Strengthening infection control measures and routine genomic surveillance are crucial to reducing the spread of CRAB and detecting novel pan-drug-resistant variants in a timely fashion.

Published

2023

4. The seroincidence of childhood Shigella sonnei infection in Ho Chi Minh City, Vietnam.

Author

Nick K Jones, Trang Nguyen Hoang Thu, Ruklanthi de Alwis, Corinne Thompson, Ha Thanh Tuyen, Tran Do Hoang Nhu, Voong Vinh Phat, Pham Duc Trung, Phung Khanh Lam, Bui Thi Thuy Tien, Hoang Thi Diem Tuyet, Lu Lan Vi, Nguyen Van Vinh Chau, Nhi Le Thi Quynh, and Stephen Baker

Subjects

Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270

Abstract

BackgroundShigella sonnei is a pathogen of growing global importance as a cause of diarrhoeal illness in childhood, particularly in transitional low-middle income countries (LMICs). Here, we sought to determine the incidence of childhood exposure to S. sonnei infection in a contemporary transitional LMIC population, where it represents the dominant Shigella species.MethodsParticipants were enrolled between the age of 12-36 months between June and December 2014. Baseline characteristics were obtained through standardized electronic questionnaires, and serum samples were collected at 6-month intervals over two years of follow-up. IgG antibody against S. sonnei O-antigen (anti-O) was measured using an enzyme-linked immunosorbent assay (ELISA). A four-fold increase in ELISA units (EU) with convalescent IgG titre >10.3 EU was taken as evidence of seroconversion between timepoints.ResultsA total of 3,498 serum samples were collected from 748 participants; 3,170 from the 634 participants that completed follow-up. Measures of anti-O IgG varied significantly by calendar month (p = 0.03). Estimated S. sonnei seroincidence was 21,451 infections per 100,000 population per year (95% CI 19,307-23,834), with peak incidence occurring at 12-18 months of age. Three baseline factors were independently associated with the likelihood of seroconversion; ever having breastfed (aOR 2.54, CI 1.22-5.26), history of prior hospital admission (aOR 0.57, CI 0.34-0.95), and use of a toilet spray-wash in the household (aOR 0.42, CI 0.20-0.89).ConclusionsIncidence of S. sonnei exposure in Ho Chi Minh City is substantial, with significant reduction in the likelihood of exposure as age increases beyond 2 years.

Published

2023

5. An evaluation of purified Salmonella Typhi protein antigens for the serological diagnosis of acute typhoid fever.

Author

Tran Vu Thieu, Nga, Trinh Van, Tan, Tran Tuan, Anh, Klemm, Elizabeth, Nguyen Ngoc Minh, Chau, Voong Vinh, Phat, Pham Thanh, Duy, Ho Ngoc Dan, Thanh, Pham Duc, Trung, Langat, Pinky, Martin, Laura, Galan, Jorge, Liang, Li, Felgner, Philip, Davies, D, de Jong, Hanna, Maude, Rapeephan, Fukushima, Masako, Wijedoru, Lalith, Ghose, Aniruddha, Samad, Rasheda, Dondorp, Arjen, Faiz, Abul, Darton, Thomas, Pollard, Andrew, Thwaites, Guy, Dougan, Gordon, Parry, Christopher, and Baker, Stephen

Subjects

Bangladesh, Diagnostics, Enteric fever, Febrile disease, IgM, Salmonella Typhi, Typhoid fever, Vi polysaccharide, Antibodies, Bacterial, Antigens, Bacterial, Bacteriological Techniques, Bangladesh, Humans, Immunoglobulin M, Polysaccharides, Bacterial, Salmonella typhi, Typhoid Fever

Abstract

OBJECTIVES: The diagnosis of typhoid fever is a challenge. Aiming to develop a typhoid diagnostic we measured antibody responses against Salmonella Typhi (S. Typhi) protein antigens and the Vi polysaccharide in a cohort of Bangladeshi febrile patients. METHODS: IgM against 12 purified antigens and the Vi polysaccharide was measured by ELISA in plasma from patients with confirmed typhoid fever (n = 32), other confirmed infections (n = 17), and healthy controls (n = 40). ELISAs with the most specific antigens were performed on plasma from 243 patients with undiagnosed febrile disease. RESULTS: IgM against the S. Typhi protein antigens correlated with each other (rho > 0.8), but not against Vi (rho 0.85, respectively. Applying a dynamic cut-off to patients with undiagnosed febrile disease suggested that 34-58% had an IgM response indicative of typhoid. CONCLUSIONS: We evaluated the diagnostic potential of several S. Typhi antigens; our assays give good sensitivity and specificity, but require further assessment in differing patient populations.

Published

2017

6. A retrospective investigation of the population structure and geospatial distribution ofSalmonellaParatyphi A in Kathmandu, Nepal

Author

Mylona, Elli, primary, Duy, Pham Thanh, additional, Keane, Jacqueline, additional, Dongol, Sabina, additional, Basnyat, Buddha, additional, Dolecek, Christiane, additional, Voong Vinh, Phat, additional, Tran Vu Thieu, Nga, additional, Nguyen Thi Nguyen, To, additional, Karkey, Abhilasha, additional, and Baker, Stephen, additional

Published

2024

7. An observational study of breakthrough SARS-CoV-2 Delta variant infections among vaccinated healthcare workers in Vietnam

Author

Nguyen Van Vinh Chau, Nghiem My Ngoc, Lam Anh Nguyet, Vo Minh Quang, Nguyen Thi Han Ny, Dao Bach Khoa, Nguyen Thanh Phong, Le Mau Toan, Nguyen Thi Thu Hong, Nguyen Thi Kim Tuyen, Voong Vinh Phat, Le Nguyen Truc Nhu, Nguyen Huynh Thanh Truc, Bui Thi Ton That, Huynh Phuong Thao, Tran Nguyen Phuong Thao, Vo Trong Vuong, Tran Thi Thanh Tam, Ngo Tan Tai, Ho The Bao, Huynh Thi Kim Nhung, Nguyen Thi Ngoc Minh, Nguyen Thi My Tien, Nguy Cam Huy, Marc Choisy, Dinh Nguyen Huy Man, Dinh Thi Bich Ty, Nguyen To Anh, Le Thi Tam Uyen, Tran Nguyen Hoang Tu, Lam Minh Yen, Nguyen Thanh Dung, Le Manh Hung, Nguyen Thanh Truong, Tran Tan Thanh, Guy Thwaites, and Le Van Tan

Subjects

Delta variant, Oxford-AstraZeneca, COVID-19, vaccine breakthrough, Vietnam, Medicine (General), R5-920

Abstract

ABSTRACT: Background: Data on breakthrough SARS-CoV-2 Delta variant infections in vaccinated individuals are limited. Methods: We studied breakthrough infections among Oxford-AstraZeneca vaccinated healthcare workers in an infectious diseases hospital in Vietnam. We collected demographic and clinical data alongside serial PCR testing, measurement of SARS-CoV-2 antibodies, and viral whole-genome sequencing. Findings: Between 11th–25th June 2021 (7-8 weeks after the second dose), 69 staff tested positive for SARS-CoV-2. 62 participated in the study. Most were asymptomatic or mildly symptomatic and all recovered. Twenty-two complete-genome sequences were obtained; all were Delta variant and were phylogenetically distinct from contemporary viruses obtained from the community or from hospital patients admitted prior to the outbreak. Viral loads inferred from Ct values were 251 times higher than in cases infected with the original strain in March/April 2020. Median time from diagnosis to negative PCR was 21 days (range 8–33). Neutralizing antibodies (expressed as percentage of inhibition) measured after the second vaccine dose, or at diagnosis, were lower in cases than in uninfected, fully vaccinated controls (median (IQR): 69.4 (50.7-89.1) vs. 91.3 (79.6-94.9), p=0.005 and 59.4 (32.5-73.1) vs. 91.1 (77.3-94.2), p=0.002). There was no correlation between vaccine-induced neutralizing antibody levels and peak viral loads or the development of symptoms. Interpretation: Breakthrough Delta variant infections following Oxford-AstraZeneca vaccination may cause asymptomatic or mild disease, but are associated with high viral loads, prolonged PCR positivity and low levels of vaccine-induced neutralizing antibodies. Epidemiological and sequence data suggested ongoing transmission had occurred between fully vaccinated individuals. Funding: Wellcome and NIH/NIAID

Published

2021

8. Evolutionary histories and antimicrobial resistance in Shigella flexneri and Shigella sonnei in Southeast Asia

Author

Chung The, Hao, Bodhidatta, Ladaporn, Pham, Duy Thanh, Mason, Carl J., Ha Thanh, Tuyen, Voong Vinh, Phat, Turner, Paul, Hem, Sopheak, Dance, David A. B., Newton, Paul N., Phetsouvanh, Rattanaphone, Davong, Viengmon, Thwaites, Guy E., Thomson, Nicholas R., Baker, Stephen, and Rabaa, Maia A.

Published

2021

9. A retrospective investigation of the population structure and geospatial distribution of Salmonella Paratyphi A in Kathmandu, Nepal.

Author

Mylona, Elli, Pham Thanh, Duy, Keane, Jacqueline A., Dongol, Sabina, Basnyat, Buddha, Dolecek, Christiane, Voong Vinh, Phat, Tran Vu Thieu, Nga, Nguyen Thi Nguyen, To, Karkey, Abhilasha, and Baker, Stephen

Subjects

SALMONELLA enterica serovar Typhi, TYPHOID fever, LOCATION data, SALMONELLA typhi, WHOLE genome sequencing, SALMONELLA

Abstract

Salmonella Paratyphi A, one of the major etiologic agents of enteric fever, has increased in prevalence in recent decades in certain endemic regions in comparison to S. Typhi, the most prevalent cause of enteric fever. Despite this increase, data on the prevalence and molecular epidemiology of S. Paratyphi A remain generally scarce. Here, we analysed the whole genome sequences of 216 S. Paratyphi A isolates originating from Kathmandu, Nepal between 2005 and 2014, of which 200 were from patients with acute enteric fever and 16 from the gallbladder of people with suspected chronic carriage. By exploiting the recently developed genotyping framework for S. Paratyphi A (Paratype), we identified several genotypes circulating in Kathmandu. Notably, we observed an unusual clonal expansion of genotype 2.4.3 over a four-year period that spread geographically and systematically replaced other genotypes. This rapid genotype replacement is hypothesised to have been driven by both reduced susceptibility to fluoroquinolones and genetic changes to virulence factors, such as functional and structural genes encoding the type 3 secretion systems. Finally, we show that person-to-person is likely the most common mode of transmission and chronic carriers seem to play a limited role in maintaining disease circulation. Author summary: Enteric (typhoid) fever is caused by bacteria of Salmonella enterica species, specifically Salmonella Typhi and Salmonella Paratyphi A. While the former is most commonly identified as the causative agent of enteric fever, S. Paratyphi A is increasing in prevalence in many endemic areas like Nepal. However, the understanding of the phylogenetic structure and population dynamics of this organism, as well as transmission patterns, remains incomplete. Here, we provide a detailed phylogenetic analysis of S. Paratyphi A isolated from enteric fever patients in Nepal through whole genome sequence analysis, combined with epidemiological observations, such as water source use, and chronological and location data. We observed an unusual expansion of a genotype (genetic ID) that replaced other genotypes in the area, indicative of changes in circulating population composition. This expansion is hypothesised to have been driven by reduction in antibiotic susceptibility and changes on bacterial structures that are important for pathogenicity. Our data also suggest person-to-person as the most likely mode of transmission for this pathogen. Understanding of S. Paratyphi A population structure, sources of infection, and transmission will help develop policies for enteric fever management, particularly prior to vaccine introduction, as changes in population composition may affect vaccine efficacy. [ABSTRACT FROM AUTHOR]

Published

2024

10. The Identification of Enteric Fever-Specific Antigens for Population-Based Serosurveillance

Author

Mylona, Elli, primary, Hefele, Lisa, additional, Tran Vu Thieu, Nga, additional, Trinh Van, Tan, additional, Nguyen Ngoc Minh, Chau, additional, Tran Tuan, Anh, additional, Karkey, Abhilasha, additional, Dongol, Sabina, additional, Basnyat, Buddha, additional, Voong Vinh, Phat, additional, Ho Ngoc Dan, Thanh, additional, Russell, Paula, additional, Charles, Richelle C, additional, Parry, Christopher M, additional, and Baker, Stephen, additional

Published

2023

11. A universal genome sequencing method for rotavirus A from human fecal samples which identifies segment reassortment and multi-genotype mixed infection

Author

Tran Thi Ngoc Dung, Pham Thanh Duy, October M. Sessions, Uma K. Sangumathi, Voong Vinh Phat, Pham Thi Thanh Tam, Nguyen Thi Nguyen To, Tran My Phuc, Tran Thi Hong Chau, Nguyen Ngoc Minh Chau, Ngoc Nguyen Minh, Guy E. Thwaites, Maia A. Rabaa, and Stephen Baker

Subjects

Rotavirus A, Genomics, Phylogenetics, Genome sequencing, Reassortment, Co-infection, Biotechnology, TP248.13-248.65, Genetics, QH426-470

Abstract

Abstract Background Genomic characterization of rotavirus (RoV) has not been adopted at large-scale due to the complexity of obtaining sequences for all 11 segments, particularly when feces are used as starting material. Methods To overcome these limitations, we developed a novel RoV capture and genome sequencing method combining commercial enzyme immunoassay plates and a set of routinely used reagents. Results Our approach had a 100% success rate, producing >90% genome coverage for diverse RoV present in fecal samples (Ct

Published

2017

12. The development and validation of multiplex real-time PCRs with fluorescent melting curve analysis for simultaneous detection of six bacterial pathogens of lower respiratory tract infections and antimicrobial resistance genes

Author

Tran Thi Ngoc Dung, Voong Vinh Phat, Chau Vinh, Nguyen Phu Huong Lan, Nguyen Luong Nha Phuong, Le Thi Quynh Ngan, Guy Thwaites, Louise Thwaites, Maia Rabaa, Nguyen Thi Kim Anh, and Pham Thanh Duy

Abstract

Klebsiella pneumoniae, Acinetobacter baumannii, Pseudomonas aeruginosa, Escherichia coli, Streptococcus pneumoniae and Staphylococcus aureusare among the major bacterial causative agents of lower respiratory tract infections (LRTIs), causing substantial morbidity and mortality globally. The rapid increase of antimicrobial resistance (AMR) in these pathogens poses significant challenges for effective antibiotic therapy of LRTIs. In low-resourced settings, the diagnostics of LRTIs relies heavily on microbiological culture and patients are often treated with empirical antibiotics while awaiting several days for culture results. Rapid detection of LRTIs pathogens and AMR genes could prompt early antibiotic switching and inform antibiotic treatment duration. In this study, we developed multiplex quantitative real-time PCRs using EvaGreen dye and melting curve analysis (MCA) to rapidly identify the six major LRTIs pathogens and their AMR genes directly from the tracheal aspirate and sputum samples. The accuracy of RT-PCRs was assessed by comparing its performance against the gold standard, conventional culture method on 50 tracheal aspirate and sputum specimens. Our RT-PCR assays had 100% sensitivity forK. pneumoniae, A. baumannii, P. aeruginosa, E. coliand 63.6% forS. aureusand the specificity ranked from 87.5% to 97.6%. The kappa correlation values of all pathogens between the two methods varied from 0.63 to 0.95. The limit of detection (LOD) of target bacteria in multiplex RT-PCRs was 1600 CFU/mL. Compared to the culture results, PCR assays exhibited higher sensitivity in detecting mixed infections andS. pneumoniae. Our findings also demonstrated a high level of concordance between the detection of AMR gene and AMR phenotype in single infections. We conclude that our multiplex quantitative RT-PCRs with fluorescence MCA is simple but sensitive and specific in detecting six major drug resistant bacterial pathogens of LRTIs and should be further evaluated for clinical utility.

Published

2023

13. Dissecting the molecular evolution of fluoroquinolone-resistant Shigella sonnei

Author

Chung The, Hao, Boinett, Christine, Pham Thanh, Duy, Jenkins, Claire, Weill, Francois-Xavier, Howden, Benjamin P., Valcanis, Mary, De Lappe, Niall, Cormican, Martin, Wangchuk, Sonam, Bodhidatta, Ladaporn, Mason, Carl J., Nguyen, To Nguyen Thi, Ha Thanh, Tuyen, Voong, Vinh Phat, Duong, Vu Thuy, Nguyen, Phu Huong Lan, Turner, Paul, Wick, Ryan, Ceyssens, Pieter-Jan, Thwaites, Guy, Holt, Kathryn E., Thomson, Nicholas R., Rabaa, Maia A., and Baker, Stephen

Published

2019

14. The epidemiology and aetiology of diarrhoeal disease in infancy in southern Vietnam: a birth cohort study

Author

Katherine L. Anders, Corinne N. Thompson, Nguyen Thi Van Thuy, Nguyen Minh Nguyet, Le Thi Phuong Tu, Tran Thi Ngoc Dung, Voong Vinh Phat, Nguyen Thi Hong Van, Nguyen Trong Hieu, Nguyen Thi Hong Tham, Phan Thi Thanh Ha, Le Bich Lien, Nguyen Van Vinh Chau, Stephen Baker, and Cameron P. Simmons

Subjects

Diarrhoeal disease, Infectious diarrhoea, Infants, Epidemiology, Cohort study, Rotavirus, Infectious and parasitic diseases, RC109-216

Abstract

Objectives: Previous studies indicate a high burden of diarrhoeal disease in Vietnamese children, however longitudinal community-based data on burden and aetiology are limited. The findings from a large, prospective cohort study of diarrhoeal disease in infants in southern Vietnam are presented herein. Methods: Infants were enrolled at birth in urban Ho Chi Minh City and a semi-rural district in southern Vietnam, and followed for 12 months (n = 6706). Diarrhoeal illness episodes were identified through clinic-based passive surveillance, hospital admissions, and self-reports. Results: The minimum incidence of diarrhoeal illness in the first year of life was 271/1000 infant-years of observation for the whole cohort. Rotavirus was the most commonly detected pathogen (50% of positive samples), followed by norovirus (24%), Campylobacter (20%), Salmonella (18%), and Shigella (16%). Repeat infections were identified in 9% of infants infected with rotavirus, norovirus, Shigella, or Campylobacter, and 13% of those with Salmonella infections. Conclusions: The minimum incidence of diarrhoeal disease in infants in both urban and semi-rural settings in southern Vietnam was quantified prospectively. A large proportion of laboratory-diagnosed disease was caused by rotavirus and norovirus. These data highlight the unmet need for a rotavirus vaccine in Vietnam and provide evidence of the previously unrecognized burden of norovirus in infants.

Published

2015

15. A Double-blind, Randomized, Placebo-controlled Trial of Lactobacillus acidophilus for the Treatment of Acute Watery Diarrhea in Vietnamese Children

Author

Hong Chau, Tran Thi, Minh Chau, Nguyen Ngoc, Hoang Le, Nhat Thanh, Chung The, Hao, Voong Vinh, Phat, Nguyen To, Nguyen Thi, Ngoc, Nguyen Minh, Tuan, Ha Manh, Chau Ngoc, Tang Le, Kolader, Marion-Eliette, Farrar, Jeremy J., Wolbers, Marcel, Thwaites, Guy E., and Baker, Stephen

Published

2018

16. Correction: The repurposing of Tebipenem pivoxil as alternative therapy for severe gastrointestinal infections caused by extensively drug-resistant Shigella spp

Author

Fernández Álvaro, Elena, primary, Voong Vinh, Phat, additional, de Cozar, Cristina, additional, Willé, David R, additional, Urones, Beatriz, additional, Cortés, Alvaro, additional, Price, Alan, additional, Tran Do Hoang, Nhu, additional, Ha Thanh, Tuyen, additional, McCloskey, Molly, additional, Shaheen, Shareef, additional, Dayao, Denise, additional, Martinot, Amanda, additional, de Mercado, Jaime, additional, Castañeda, Pablo, additional, García-Perez, Adolfo, additional, Singa, Benson, additional, Pavlinac, Patricia, additional, Walson, Judd, additional, Martínez-Martínez, Maria Santos, additional, Arnold, Samuel LM, additional, Tzipori, Saul, additional, Pages, Lluis Ballell, additional, and Baker, Stephen, additional

Published

2022

17. The repurposing of Tebipenem pivoxil as alternative therapy for severe gastrointestinal infections caused by extensively drug-resistant Shigella spp

Author

Fernández Álvaro, Elena, primary, Voong Vinh, Phat, additional, de Cozar, Cristina, additional, Willé, David R, additional, Urones, Beatriz, additional, Cortés, Alvaro, additional, Price, Alan, additional, Tran Do Hoang, Nhu, additional, Ha Thanh, Tuyen, additional, McCloskey, Molly, additional, Shaheen, Shareef, additional, Dayao, Denise, additional, Martinot, Amanda, additional, de Mercado, Jaime, additional, Castañeda, Pablo, additional, García-Perez, Adolfo, additional, Singa, Benson, additional, Pavlinac, Patricia, additional, Walson, Judd, additional, Martínez-Martínez, Maria Santos, additional, Arnold, Samuel LM, additional, Tzipori, Saul, additional, Ballell Pages, Lluis, additional, and Baker, Stephen, additional

Published

2022

18. Author response: The repurposing of Tebipenem pivoxil as alternative therapy for severe gastrointestinal infections caused by extensively drug-resistant Shigella spp

Author

Fernández Álvaro, Elena, primary, Voong Vinh, Phat, additional, de Cozar, Cristina, additional, Willé, David R, additional, Urones, Beatriz, additional, Cortés, Alvaro, additional, Price, Alan, additional, Tran Do Hoang, Nhu, additional, Ha Thanh, Tuyen, additional, McCloskey, Molly, additional, Shaheen, Shareef, additional, Dayao, Denise, additional, Martinot, Amanda, additional, de Mercado, Jaime, additional, Castañeda, Pablo, additional, García-Perez, Adolfo, additional, Singa, Benson, additional, Pavlinac, Patricia, additional, Walson, Judd, additional, Martínez-Martínez, Maria Santos, additional, Arnold, Samuel LM, additional, Tzipori, Saul, additional, Ballell Pages, Lluis, additional, and Baker, Stephen, additional

Published

2022

19. The evolutionary history of Shigella flexneri serotype 6 in Asia

Author

Mai, Si-Nguyen T., primary, Bodhidatta, Ladaporn, additional, Turner, Paul, additional, Wangchuk, Sonam, additional, Ha Thanh, Tuyen, additional, Voong Vinh, Phat, additional, Pham, Duy Thanh, additional, Rabaa, Maia A., additional, Thwaites, Guy E., additional, Thomson, Nicholas R., additional, Baker, Stephen, additional, and Chung The, Hao, additional

Published

2021

20. Tebipenem as an oral alternative for the treatment of typhoid caused by XDRSalmonellaTyphi

Author

Mylona, Elli, primary, Voong Vinh, Phat, additional, Qureshi, Sonia, additional, Karkey, Abhilasha, additional, Dongol, Sabina, additional, Ha Thanh, Tuyen, additional, Walson, Judd, additional, Ballell, Lluis, additional, Fernández Álvaro, Elena, additional, Qamar, Farah, additional, and Baker, Stephen, additional

Published

2021

21. Transmission of SARS-CoV-2 Delta Variant Among Vaccinated Healthcare Workers, Vietnam

Author

Nguyen Van Vinh Chau, Nghiem My Ngoc, Lam Anh Nguyet, Vo Minh Quang, Nguyen Thi Han Ny, Dao Bach Khoa, Nguyen Thanh Phong, Le Mau Toan, Nguyen Thi Thu Hong, Nguyen Thi Kim Tuyen, Voong Vinh Phat, Le Nguyen Truc Nhu, Nguyen Huynh Thanh Truc, Bui Thi Ton That, Huynh Phuong Thao, Tran Nguyen Phuong Thao, Vo Trong Vuong, Tran Thi Thanh Tam, Ngo Tan Tai, Ho The Bao, Huynh Thi Kim Nhung, Nguyen Thi Ngoc Minh, Nguyen Thi My Tien, Nguy Cam Huy, Marc Choisy, Dinh Nguyen Huy Man, Dinh Thi Bich Ty, Nguyen To Anh, Le Thi Tam Uyen, Tran Nguyen Hoang Tu, Lam Minh Yen, Nguyen Thanh Dung, Le Manh Hung, Nguyen Thanh Truong, Tran Tan Thanh, Guy Thwaites, and Le Van Tan

Subjects

Delta, History, medicine.medical_specialty, Polymers and Plastics, biology, business.industry, Transmission (medicine), Institutional review board, Industrial and Manufacturing Engineering, Vaccination, Internal medicine, Health care, medicine, biology.protein, Business and International Management, Antibody, business, Neutralizing antibody, Viral load

Abstract

Background: Data on breakthrough SARS-CoV-2 Delta variant infections are limited. Methods: We studied breakthrough infections among healthcare workers of a major infectious diseases hospital in Vietnam. We collected demographics, vaccination history and results of PCR diagnosis alongside clinical data. We measured SARS-CoV-2 (neutralizing) antibodies at diagnosis, and at week 1, 2 and 3 after diagnosis. We sequenced the viruses using ARTIC protocol. Findings: Between 11th–25th June 2021 (week 7–8 after dose 2), 69 healthcare workers were tested positive for SARS-CoV-2. 62 participated in the clinical study. 49 were (pre)symptomatic with one requiring oxygen supplementation. All recovered uneventfully. 23 complete-genome sequences were obtained. They all belonged to the Delta variant, and were phylogenetically distinct from the contemporary Delta variant sequences obtained from community transmission cases, suggestive of ongoing transmission between the workers. Viral loads of breakthrough Delta variant infection cases were 251 times higher than those of cases infected with old strains detected between March-April 2020. Time from diagnosis to PCR negative was 8–33 days (median: 21). Neutralizing antibody levels after vaccination and at diagnosis of the cases were lower than those in the matched uninfected controls. There was no correlation between vaccine-induced neutralizing antibody levels and viral loads or the development of symptoms. Interpretation: Breakthrough Delta variant infections are associated with high viral loads, prolonged PCR positivity, and low levels of vaccine-induced neutralizing antibodies, explaining the transmission between the vaccinated people. Physical distancing measures remain critical to reduce SARS-CoV-2 Delta variant transmission. Funding: Wellcome (106680/B/14/Z and 204904/Z/16/Z). Declaration of Interest: None to declare. Ethical Approval: The study was approved by the Institutional Review Board of HTD and the Oxford Tropical Research Ethics Committee, University of Oxford, UK.

Published

2021

22. Fitness benefits in fluoroquinolone-resistant Salmonella Typhi in the absence of antimicrobial pressure

Author

Stephen Baker, Pham Thanh Duy, Tran Vu Thieu Nga, Tran Thi Ngoc Dung, Voong Vinh Phat, Tran Thuy Chau, A Keith Turner, Jeremy Farrar, and Maciej F Boni

Subjects

Salmonella, typhoid, fitness cost, epistasis, fluoroquinolone, Medicine, Science, Biology (General), QH301-705.5

Abstract

Fluoroquinolones (FQ) are the recommended antimicrobial treatment for typhoid, a severe systemic infection caused by the bacterium Salmonella enterica serovar Typhi. FQ-resistance mutations in S. Typhi have become common, hindering treatment and control efforts. Using in vitro competition experiments, we assayed the fitness of eleven isogenic S. Typhi strains with resistance mutations in the FQ target genes, gyrA and parC. In the absence of antimicrobial pressure, 6 out of 11 mutants carried a selective advantage over the antimicrobial-sensitive parent strain, indicating that FQ resistance in S. Typhi is not typically associated with fitness costs. Double-mutants exhibited higher than expected fitness as a result of synergistic epistasis, signifying that epistasis may be a critical factor in the evolution and molecular epidemiology of S. Typhi. Our findings have important implications for the management of drug-resistant S. Typhi, suggesting that FQ-resistant strains would be naturally maintained even if fluoroquinolone use were reduced.

Published

2013

23. Colonization with Staphylococcus aureus and Klebsiella pneumoniae causes infections in a Vietnamese intensive care unit

Author

Thuy, Duong Bich, primary, Campbell, James, additional, Thuy, Cao Thu, additional, Hoang, Nguyen Van Minh, additional, Voong Vinh, Phat, additional, Nguyen, To Nguyen Thi, additional, Nguyen Ngoc Minh, Chau, additional, Pham, Duy Thanh, additional, Rabaa, Maia A., additional, Lan, Nguyen Phu Huong, additional, Hao, Nguyen Van, additional, Thwaites, Guy E., additional, Thwaites, C. Louise, additional, Baker, Stephen, additional, Chau, Nguyen Van Vinh, additional, and Chung The, Hao, additional

Published

2021

24. South Asia as a Reservoir for the Global Spread of Ciprofloxacin-Resistant Shigella sonnei: A Cross-Sectional Study

Author

Chung The, Hao, Rabaa, Maia A., Pham Thanh, Duy, De Lappe, Niall, Cormican, Martin, Valcanis, Mary, Howden, Benjamin P., Wangchuk, Sonam, Bodhidatta, Ladaporn, Mason, Carl J., Nguyen Thi Nguyen, To, Vu Thuy, Duong, Thompson, Corinne N., Phu Huong Lan, Nguyen, Voong Vinh, Phat, Ha Thanh, Tuyen, Turner, Paul, Sar, Poda, Thwaites, Guy, Thomson, Nicholas R., Holt, Kathryn E., and Baker, Stephen

Subjects

Mutation -- Research, Public health -- Analysis, Shigella sonnei -- Research, Diarrhea -- Care and treatment, Ciprofloxacin -- Usage, Biological sciences

Abstract

Background Antimicrobial resistance is a major issue in the Shigellae, particularly as a specific multidrug-resistant (MDR) lineage of Shigella sonnei (lineage III) is becoming globally dominant. Ciprofloxacin is a recommended treatment for Shigella infections. However, ciprofloxacin-resistant S. sonnei are being increasingly isolated in Asia and sporadically reported on other continents. We hypothesized that Asia is a primary hub for the recent international spread of ciprofloxacin-resistant S. sonnei. Methods and Findings We performed whole-genome sequencing on a collection of 60 contemporaneous ciprofloxacin-resistant S. sonnei isolated in four countries within Asia (Vietnam, n = 11; Bhutan, n = 12; Thailand, n = 1; Cambodia, n = 1) and two outside of Asia (Australia, n = 19; Ireland, n = 16). We reconstructed the recent evolutionary history of these organisms and combined these data with their geographical location of isolation. Placing these sequences into a global phylogeny, we found that all ciprofloxacin-resistant S. sonnei formed a single clade within a Central Asian expansion of lineage III. Furthermore, our data show that resistance to ciprofloxacin within S. sonnei may be globally attributed to a single clonal emergence event, encompassing sequential gyrA-S83L, parC-S80I, and gyrA-D87G mutations. Geographical data predict that South Asia is the likely primary source of these organisms, which are being regularly exported across Asia and intercontinentally into Australia, the United States and Europe. Our analysis was limited by the number of S. sonnei sequences available from diverse geographical areas and time periods, and we cannot discount the potential existence of other unsampled reservoir populations of antimicrobial-resistant S. sonnei. Conclusions This study suggests that a single clone, which is widespread in South Asia, is likely driving the current intercontinental surge of ciprofloxacin-resistant S. sonnei and is capable of establishing endemic transmission in new locations. Despite being limited in geographical scope, our work has major implications for understanding the international transfer of antimicrobial-resistant pathogens, with S. sonnei acting as a tractable model for studying how antimicrobial-resistant Gram-negative bacteria spread globally., Author(s): Hao Chung The 1, Maia A. Rabaa 1,2, Duy Pham Thanh 1, Niall De Lappe 3, Martin Cormican 4, Mary Valcanis 5, Benjamin P. Howden 5, Sonam Wangchuk 6, [...]

Published

2016

25. Evaluation of Luminex xTAG Gastrointestinal Pathogen Panel Assay for Detection of Multiple Diarrheal Pathogens in Fecal Samples in Vietnam

Author

Bui Duc Phu, Maia A. Rabaa, Stephen Baker, Nguyen Van Hung, Nguyen Van Xang, Hoang Le Phuc, Tran My Phuc, Nguyen Dong, Pham Thi Thanh Tam, Voong Vinh Phat, Pham Van Minh, Dang Thao Huong, Ton Thi Thanh Ha, Guy E. Thwaites, Nguyen Thi Thanh Huong, Corinne N. Thompson, Vu Thuy Duong, Lu Lan Vi, Tran Thi Ngoc Dung, Le Thi Phuong, Nguyen Minh Ngoc, Pham Duc Trung, Ha Thanh Tuyen, Le Thi Phuong Tu, and James Campbell

Subjects

Adult, Diarrhea, Male, 0301 basic medicine, Microbiology (medical), medicine.medical_specialty, Microbiological culture, Adolescent, 030106 microbiology, medicine.disease_cause, Sensitivity and Specificity, Feces, Young Adult, 03 medical and health sciences, Rotavirus, Epidemiology, Genotype, medicine, Humans, Multiplex, Child, Pathogen, Aged, Aged, 80 and over, Immunoassay, Bacteria, business.industry, Infant, Newborn, Infant, Bacteriology, Middle Aged, Clostridium difficile, 3. Good health, Vietnam, Child, Preschool, Viruses, Immunology, Norovirus, Female, business

Abstract

Diarrheal disease is a complex syndrome that remains a leading cause of global childhood morbidity and mortality. The diagnosis of enteric pathogens in a timely and precise manner is important for making treatment decisions and informing public health policy, but accurate diagnosis is a major challenge in industrializing countries. Multiplex molecular diagnostic techniques may represent a significant improvement over classical approaches. We evaluated the Luminex xTAG gastrointestinal pathogen panel (GPP) assay for the detection of common enteric bacterial and viral pathogens in Vietnam. Microbiological culture and real-time PCR were used as gold standards. The tests were performed on 479 stool samples collected from people admitted to the hospital for diarrheal disease throughout Vietnam. Sensitivity and specificity were calculated for the xTAG GPP for the seven principal diarrheal etiologies. The sensitivity and specificity for the xTAG GPP were >88% for Shigella spp., Campylobacter spp., rotavirus, norovirus genotype 1/2 (GI/GII), and adenovirus compared to those of microbiological culture and/or real-time PCR. However, the specificity was low (∼60%) for Salmonella species. Additionally, a number of important pathogens that are not identified in routine hospital procedures in this setting, such as Cryptosporidium spp. and Clostridium difficile , were detected with the GPP. The use of the Luminex xTAG GPP for the detection of enteric pathogens in settings, like Vietnam, would dramatically improve the diagnostic accuracy and capacity of hospital laboratories, allowing for timely and appropriate therapy decisions and a wider understanding of the epidemiology of pathogens associated with severe diarrheal disease in low-resource settings.

Published

2016

26. The epidemiology and aetiology of diarrhoeal disease in infancy in southern Vietnam: a birth cohort study

Author

Phan Thi Thanh Ha, Corinne N. Thompson, Le Bich Lien, Stephen Baker, Nguyen Trong Hieu, Tran Thi Ngoc Dung, Katherine L. Anders, Voong Vinh Phat, Le Thi Phuong Tu, Cameron P. Simmons, Nguyen Van Vinh Chau, Nguyen Thi Van Thuy, Nguyen Thi Hong Tham, Nguyen Minh Nguyet, and Nguyen Thi Hong Van

Subjects

Microbiology (medical), Rotavirus, Male, medicine.medical_specialty, Pediatrics, Epidemiology, viruses, medicine.disease_cause, Article, Rotavirus Infections, lcsh:Infectious and parasitic diseases, fluids and secretions, medicine, Humans, lcsh:RC109-216, Prospective Studies, Prospective cohort study, Caliciviridae Infections, business.industry, Incidence (epidemiology), Incidence, Infectious diarrhoea, Norovirus, virus diseases, Infant, General Medicine, Diarrhoeal disease, Rotavirus vaccine, 3. Good health, Infectious Diseases, Vietnam, Cohort, Diarrhea, Infantile, Female, business, Cohort study, Infants, Follow-Up Studies

Abstract

Highlights • The diarrhoeal disease burden in a large, prospective infant cohort in Vietnam is defined. • Minimum incidence of clinic-based diarrhoea in infants: 271/1000 infant-years. • Rotavirus was most commonly identified, followed by norovirus and bacterial pathogens. • Frequent repeat infections with the same pathogen within 1 year. • Inclusion of rotavirus in the immunization schedule for Vietnam is warranted., Summary Objectives Previous studies indicate a high burden of diarrhoeal disease in Vietnamese children, however longitudinal community-based data on burden and aetiology are limited. The findings from a large, prospective cohort study of diarrhoeal disease in infants in southern Vietnam are presented herein. Methods Infants were enrolled at birth in urban Ho Chi Minh City and a semi-rural district in southern Vietnam, and followed for 12 months (n = 6706). Diarrhoeal illness episodes were identified through clinic-based passive surveillance, hospital admissions, and self-reports. Results The minimum incidence of diarrhoeal illness in the first year of life was 271/1000 infant-years of observation for the whole cohort. Rotavirus was the most commonly detected pathogen (50% of positive samples), followed by norovirus (24%), Campylobacter (20%), Salmonella (18%), and Shigella (16%). Repeat infections were identified in 9% of infants infected with rotavirus, norovirus, Shigella, or Campylobacter, and 13% of those with Salmonella infections. Conclusions The minimum incidence of diarrhoeal disease in infants in both urban and semi-rural settings in southern Vietnam was quantified prospectively. A large proportion of laboratory-diagnosed disease was caused by rotavirus and norovirus. These data highlight the unmet need for a rotavirus vaccine in Vietnam and provide evidence of the previously unrecognized burden of norovirus in infants.

Published

2015

27. A universal genome sequencing method for rotavirus A from human fecal samples which identifies segment reassortment and multi-genotype mixed infection

Author

Stephen Baker, Nguyen Thi Nguyen To, Maia A. Rabaa, Ngoc Nguyen Minh, Tran Thi Hong Chau, October M. Sessions, Nguyen Chau, Pham Thi Thanh Tam, Pham Thanh Duy, Tran My Phuc, Uma K. Sangumathi, Tran Thi Ngoc Dung, Voong Vinh Phat, Guy E. Thwaites, Baker, Stephen [0000-0003-1308-5755], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Rotavirus, DNA, Complementary, lcsh:QH426-470, Genotype, lcsh:Biotechnology, 030106 microbiology, Reassortment, Rotavirus A, Genomics, Genome, Viral, Biology, Remotely operated underwater vehicle, medicine.disease_cause, Genome sequencing, Genome, DNA sequencing, 03 medical and health sciences, Feces, lcsh:TP248.13-248.65, Genetics, medicine, Humans, Phylogeny, Sequence Analysis, RNA, Methodology Article, Viral Load, 3. Good health, Co-infection, Phylogenetics, lcsh:Genetics, 030104 developmental biology, DNA microarray, Antibody capture, Reassortant Viruses, Biotechnology

Abstract

Background Genomic characterization of rotavirus (RoV) has not been adopted at large-scale due to the complexity of obtaining sequences for all 11 segments, particularly when feces are used as starting material. Methods To overcome these limitations, we developed a novel RoV capture and genome sequencing method combining commercial enzyme immunoassay plates and a set of routinely used reagents. Results Our approach had a 100% success rate, producing >90% genome coverage for diverse RoV present in fecal samples (Ct

Published

2017

28. Open Source Drug Discovery with the Malaria Box Compound Collection for Neglected Diseases and Beyond

Author

Institute for Medical Engineering and Science, Harvard University--MIT Division of Health Sciences and Technology, Bhatia, Sangeeta N, Van Voorhis, Wesley C., Adams, John H., Adelfio, Roberto, Ahyong, Vida, Akabas, Myles H., Alano, Pietro, Alday, Aintzane, Yesmalie, Alemán Resto, Alsibaee, Aishah, Alzualde, Ainhoa, Andrews, Katherine T., Avery, Simon V., Avery, Vicky M., Ayong, Lawrence, Baker, Mark, Baker, Stephen, Ben Mamoun, Choukri, Bickle, Quentin, Bounaadja, Lotfi, Bowling, Tana, Bosch, Jürgen, Boucher, Lauren E., Boyom, Fabrice F., Brea, Jose, Brennan, Marian, Burton, Audrey, Caffrey, Conor R., Camarda, Grazia, Carrasquilla, Manuela, Carter, Dee, Cassera, Maria Belen, Ken, Chih-Chien Cheng, Chindaudomsate, Worathad, Chubb, Anthony, Colon, Beatrice L., Colón-López, Daisy D., Corbett, Yolanda, Crowther, Gregory J., Cowan, Noemi, D’Alessandro, Sarah, Le Dang, Na, Delves, Michael, DeRisi, Joseph L., Du, Alan Y., Duffy, Sandra, Abd El-Salam El-Sayed, Shimaa, Ferdig, Michael T., Fernández Robledo, José A., Fidock, David A., Florent, Isabelle, Fokou, Patrick V. T., Galstian, Ani, Gamo, Francisco Javier, Gokool, Suzanne, Gold, Ben, Golub, Todd, Goldgof, Gregory M., Guha, Rajarshi, Guiguemde, W. Armand, Gural, Nil, Guy, R. Kiplin, Hansen, Michael A. E., Hanson, Kirsten K., Hemphill, Andrew, Hooft van Huijsduijnen, Rob, Horii, Takaaki, Horrocks, Paul, Hughes, Tyler B., Huston, Christopher, Igarashi, Ikuo, Ingram-Sieber, Katrin, Itoe, Maurice A., Jadhav, Ajit, Naranuntarat Jensen, Amornrat, Jensen, Laran T., Jiang, Rays H. Y., Kaiser, Annette, Keiser, Jennifer, Ketas, Thomas, Kicka, Sebastien, Kim, Sunyoung, Kirk, Kiaran, Kumar, Vidya P., Kyle, Dennis E., Lafuente, Maria Jose, Landfear, Scott, Lee, Nathan, Lee, Sukjun, Lehane, Adele M., Li, Fengwu, Little, David, Liu, Liqiong, Llinás, Manuel, Loza, Maria I., Lubar, Aristea, Lucantoni, Leonardo, Lucet, Isabelle, Maes, Louis, Mancama, Dalu, Mansour, Nuha R., March, Sandra, McGowan, Sheena, Medina Vera, Iset, Meister, Stephan, Mercer, Luke, Mestres, Jordi, Mfopa, Alvine N., Misra, Raj N., Moon, Seunghyun, Moore, John P., Morais Rodrigues da Costa, Francielly, Müller, Joachim, Muriana, Arantza, Nakazawa Hewitt, Stephen, Nare, Bakela, Nathan, Carl, Narraidoo, Nathalie, Nawaratna, Sujeevi, Ojo, Kayode K., Ortiz, Diana, Panic, Gordana, Papadatos, George, Parapini, Silvia, Patra, Kailash, Pham, Ngoc, Prats, Sarah, Plouffe, David M., Poulsen, Sally-Ann, Pradhan, Anupam, Quevedo, Celia, Quinn, Ronald J., Rice, Christopher A., Ruecker, Andrea, St. Onge, Robert, Salgado Ferreira, Rafaela, Samra, Jasmeet, Robinett, Natalie G., Schlecht, Ulrich, Schmitt, Marjorie, Silva Villela, Filipe, Silvestrini, Francesco, Sinden, Robert, Smith, Dennis A., Soldati, Thierry, Spitzmüller, Andreas, Stamm, Serge Maximilian, Sullivan, David J., Sullivan, William, Suresh, Sundari, Suzuki, Brian M., Suzuki, Yo, Swamidass, S. Joshua, Taramelli, Donatella, Tchokouaha, Lauve R. Y., Theron, Anjo, Thomas, David, Tonissen, Kathryn F., Townson, Simon, Tripathi, Abhai K., Trofimov, Valentin, Udenze, Kenneth O., Ullah, Imran, Vallieres, Cindy, Vigil, Edgar, Vinetz, Joseph M., Voong Vinh, Phat, Vu, Hoan, Watanabe, Nao-aki, Weatherby, Kate, White, Pamela M., Wilks, Andrew F., Winzeler, Elizabeth A., Wojcik, Edward, Wree, Melanie, Wu, Wesley, Yokoyama, Naoaki, Zollo, Paul H. A., Abla, Nada, Blasco, Benjamin, Burrows, Jeremy, Laleu, Benoît, Leroy, Didier, Spangenberg, Thomas, Wells, Timothy, Willis, Paul A., Institute for Medical Engineering and Science, Harvard University--MIT Division of Health Sciences and Technology, Bhatia, Sangeeta N, Van Voorhis, Wesley C., Adams, John H., Adelfio, Roberto, Ahyong, Vida, Akabas, Myles H., Alano, Pietro, Alday, Aintzane, Yesmalie, Alemán Resto, Alsibaee, Aishah, Alzualde, Ainhoa, Andrews, Katherine T., Avery, Simon V., Avery, Vicky M., Ayong, Lawrence, Baker, Mark, Baker, Stephen, Ben Mamoun, Choukri, Bickle, Quentin, Bounaadja, Lotfi, Bowling, Tana, Bosch, Jürgen, Boucher, Lauren E., Boyom, Fabrice F., Brea, Jose, Brennan, Marian, Burton, Audrey, Caffrey, Conor R., Camarda, Grazia, Carrasquilla, Manuela, Carter, Dee, Cassera, Maria Belen, Ken, Chih-Chien Cheng, Chindaudomsate, Worathad, Chubb, Anthony, Colon, Beatrice L., Colón-López, Daisy D., Corbett, Yolanda, Crowther, Gregory J., Cowan, Noemi, D’Alessandro, Sarah, Le Dang, Na, Delves, Michael, DeRisi, Joseph L., Du, Alan Y., Duffy, Sandra, Abd El-Salam El-Sayed, Shimaa, Ferdig, Michael T., Fernández Robledo, José A., Fidock, David A., Florent, Isabelle, Fokou, Patrick V. T., Galstian, Ani, Gamo, Francisco Javier, Gokool, Suzanne, Gold, Ben, Golub, Todd, Goldgof, Gregory M., Guha, Rajarshi, Guiguemde, W. Armand, Gural, Nil, Guy, R. Kiplin, Hansen, Michael A. E., Hanson, Kirsten K., Hemphill, Andrew, Hooft van Huijsduijnen, Rob, Horii, Takaaki, Horrocks, Paul, Hughes, Tyler B., Huston, Christopher, Igarashi, Ikuo, Ingram-Sieber, Katrin, Itoe, Maurice A., Jadhav, Ajit, Naranuntarat Jensen, Amornrat, Jensen, Laran T., Jiang, Rays H. Y., Kaiser, Annette, Keiser, Jennifer, Ketas, Thomas, Kicka, Sebastien, Kim, Sunyoung, Kirk, Kiaran, Kumar, Vidya P., Kyle, Dennis E., Lafuente, Maria Jose, Landfear, Scott, Lee, Nathan, Lee, Sukjun, Lehane, Adele M., Li, Fengwu, Little, David, Liu, Liqiong, Llinás, Manuel, Loza, Maria I., Lubar, Aristea, Lucantoni, Leonardo, Lucet, Isabelle, Maes, Louis, Mancama, Dalu, Mansour, Nuha R., March, Sandra, McGowan, Sheena, Medina Vera, Iset, Meister, Stephan, Mercer, Luke, Mestres, Jordi, Mfopa, Alvine N., Misra, Raj N., Moon, Seunghyun, Moore, John P., Morais Rodrigues da Costa, Francielly, Müller, Joachim, Muriana, Arantza, Nakazawa Hewitt, Stephen, Nare, Bakela, Nathan, Carl, Narraidoo, Nathalie, Nawaratna, Sujeevi, Ojo, Kayode K., Ortiz, Diana, Panic, Gordana, Papadatos, George, Parapini, Silvia, Patra, Kailash, Pham, Ngoc, Prats, Sarah, Plouffe, David M., Poulsen, Sally-Ann, Pradhan, Anupam, Quevedo, Celia, Quinn, Ronald J., Rice, Christopher A., Ruecker, Andrea, St. Onge, Robert, Salgado Ferreira, Rafaela, Samra, Jasmeet, Robinett, Natalie G., Schlecht, Ulrich, Schmitt, Marjorie, Silva Villela, Filipe, Silvestrini, Francesco, Sinden, Robert, Smith, Dennis A., Soldati, Thierry, Spitzmüller, Andreas, Stamm, Serge Maximilian, Sullivan, David J., Sullivan, William, Suresh, Sundari, Suzuki, Brian M., Suzuki, Yo, Swamidass, S. Joshua, Taramelli, Donatella, Tchokouaha, Lauve R. Y., Theron, Anjo, Thomas, David, Tonissen, Kathryn F., Townson, Simon, Tripathi, Abhai K., Trofimov, Valentin, Udenze, Kenneth O., Ullah, Imran, Vallieres, Cindy, Vigil, Edgar, Vinetz, Joseph M., Voong Vinh, Phat, Vu, Hoan, Watanabe, Nao-aki, Weatherby, Kate, White, Pamela M., Wilks, Andrew F., Winzeler, Elizabeth A., Wojcik, Edward, Wree, Melanie, Wu, Wesley, Yokoyama, Naoaki, Zollo, Paul H. A., Abla, Nada, Blasco, Benjamin, Burrows, Jeremy, Laleu, Benoît, Leroy, Didier, Spangenberg, Thomas, Wells, Timothy, and Willis, Paul A.

Abstract

A major cause of the paucity of new starting points for drug discovery is the lack of interaction between academia and industry. Much of the global resource in biology is present in universities, whereas the focus of medicinal chemistry is still largely within industry. Open source drug discovery, with sharing of information, is clearly a first step towards overcoming this gap. But the interface could especially be bridged through a scale-up of open sharing of physical compounds, which would accelerate the finding of new starting points for drug discovery. The Medicines for Malaria Venture Malaria Box is a collection of over 400 compounds representing families of structures identified in phenotypic screens of pharmaceutical and academic libraries against the Plasmodium falciparum malaria parasite. The set has now been distributed to almost 200 research groups globally in the last two years, with the only stipulation that information from the screens is deposited in the public domain. This paper reports for the first time on 236 screens that have been carried out against the Malaria Box and compares these results with 55 assays that were previously published, in a format that allows a meta-analysis of the combined dataset. The combined biochemical and cellular assays presented here suggest mechanisms of action for 135 (34%) of the compounds active in killing multiple life-cycle stages of the malaria parasite, including asexual blood, liver, gametocyte, gametes and insect ookinete stages. In addition, many compounds demonstrated activity against other pathogens, showing hits in assays with 16 protozoa, 7 helminths, 9 bacterial and mycobacterial species, the dengue fever mosquito vector, and the NCI60 human cancer cell line panel of 60 human tumor cell lines. Toxicological, pharmacokinetic and metabolic properties were collected on all the compounds, assisting in the selection of the most promising candidates for murine proof-of-concept experiments and medicinal chemis

Published

2017

29. High levels of contamination and antimicrobial-resistant non-typhoidal Salmonella serovars on pig and poultry farms in the Mekong Delta of Vietnam

Author

Juliet E. Bryant, James Campbell, Ngo Thi Hoa, Voong Vinh Phat, Vo Be Hien, Nguyen Van Minh Hoang, D. T. Duy, Juan Carrique-Mas, Nguyen Van Cuong, Le Thi Phuong Tu, Guy E. Thwaites, Bach Tuan Kiet, Stephen Baker, and Corinne N. Thompson

Subjects

Serotype, Salmonella, Veterinary medicine, Nalidixic acid, 040301 veterinary sciences, Epidemiology, Swine, animal diseases, Biology, medicine.disease_cause, Poultry, 0403 veterinary science, 03 medical and health sciences, Feces, Antibiotic resistance, Ampicillin, Drug Resistance, Bacterial, medicine, Prevalence, Animals, Gastrointestinal Infections, Animal Husbandry, Serotyping, 2. Zero hunger, 0303 health sciences, Salmonella Infections, Animal, 030306 microbiology, 04 agricultural and veterinary sciences, Original Papers, zoonoses, Multiple drug resistance, Ciprofloxacin, Infectious Diseases, Vietnam, Environmental Pollution, medicine.drug

Abstract

SUMMARYWe investigated the prevalence, diversity, and antimicrobial resistance (AMR) profiles of non-typhoidalSalmonella(NTS) and associated risk factors on 341 pig, chicken, and duck farms in Dong Thap province (Mekong Delta, Vietnam). Sampling was stratified by species, district (four categories), and farm size (three categories). Pooled faeces, collected using boot swabs, were tested using ISO 6575: 2002 (Annex D). Isolates were serogrouped; group B isolates were tested by polymerase chain reaction to detectS.Typhimurium and (monophasic) serovar 4,[5],12:i:- variants. The farm-level adjusted NTS prevalence was 64·7%, 94·3% and 91·3% for chicken, duck and pig farms, respectively. Factors independently associated with NTS were duck farms [odds ratio (OR) 21·2], farm with >50 pigs (OR 11·9), pig farm with 5–50 pigs (OR 4·88) (vs. chickens), and frequent rodent sightings (OR 2·3). BothS. Typhimurium and monophasicS.Typhimurium were more common in duck farms. Isolates had a high prevalence of resistance (77·6%) against tetracycline, moderate resistance (20–30%) against chloramphenicol, sulfamethoxazole-trimethoprim, ampicillin and nalidixic acid, and low resistance (S.Typhimurium and other group B isolates (excludingS. Typhimurium) and pig farms. The unusually high prevalence of NTS on Mekong Delta farms poses formidable challenges for control.

Published

2016

30. Fitness benefits in fluoroquinolone-resistant Salmonella Typhi in the absence of antimicrobial pressure

Author

Tran Vu Thieu Nga, Tran Thi Ngoc Dung, Pham Thanh Duy, Stephen Baker, Tran Thuy Chau, A. Keith Turner, Jeremy Farrar, Voong Vinh Phat, and Maciej F. Boni

Subjects

epistasis, Salmonella, QH301-705.5, Science, fitness cost, Microbial Sensitivity Tests, medicine.disease_cause, Salmonella typhi, fluoroquinolone, complex mixtures, General Biochemistry, Genetics and Molecular Biology, Typhoid fever, Microbiology, 03 medical and health sciences, medicine, Biology (General), 030304 developmental biology, Microbiology and Infectious Disease, 0303 health sciences, Mutation, General Immunology and Microbiology, Molecular epidemiology, biology, 030306 microbiology, General Neuroscience, Drug Resistance, Microbial, Epistasis, Genetic, General Medicine, medicine.disease, biology.organism_classification, Antimicrobial, bacterial infections and mycoses, 3. Good health, Anti-Bacterial Agents, Epidemiology and Global Health, Epistasis, Medicine, bacteria, Other, Bacteria, typhoid, Research Article, Fluoroquinolones

Abstract

Fluoroquinolones (FQ) are the recommended antimicrobial treatment for typhoid, a severe systemic infection caused by the bacterium Salmonella enterica serovar Typhi. FQ-resistance mutations in S. Typhi have become common, hindering treatment and control efforts. Using in vitro competition experiments, we assayed the fitness of eleven isogenic S. Typhi strains with resistance mutations in the FQ target genes, gyrA and parC. In the absence of antimicrobial pressure, 6 out of 11 mutants carried a selective advantage over the antimicrobial-sensitive parent strain, indicating that FQ resistance in S. Typhi is not typically associated with fitness costs. Double-mutants exhibited higher than expected fitness as a result of synergistic epistasis, signifying that epistasis may be a critical factor in the evolution and molecular epidemiology of S. Typhi. Our findings have important implications for the management of drug-resistant S. Typhi, suggesting that FQ-resistant strains would be naturally maintained even if fluoroquinolone use were reduced. DOI: http://dx.doi.org/10.7554/eLife.01229.001, eLife digest The fluoroquinolones are a group of antimicrobials that are used to treat a variety of life-threatening bacterial infections, including typhoid fever. Before the introduction of antimicrobials, the mortality rate from typhoid fever was 10–20%. Prompt treatment with fluoroquinolones has reduced this to less than 1%, and has also decreased the severity of symptoms suffered by people with the disease. Now, however, the usefulness of many antimicrobials, including the fluoroquinolones, is threatened by the evolution of antimicrobial resistance within the bacterial populations being treated. Drug resistance in bacteria typically arises through specific mutations, or following the acquisition of antimicrobial resistance genes from other bacteria. It is thought that the frequent use of antimicrobials in human and animal health puts selective pressure on bacterial populations, allowing bacterial strains with mutations or genes that confer antimicrobial resistance to survive, while bacterial strains that are sensitive to the antimicrobials die out. At first it was thought that specific mutations conferring antimicrobial resistance came at a fitness cost, which would mean that such mutations would be rare in the absence of antimicrobials. Now, based on research into typhoid fever, Baker et al. describe a system in which the majority of evolutionary routes to drug resistance are marked by significant fitness benefits, even in the absence of antimicrobial exposure. Typhoid is caused by a bacterial pathogen known as Salmonella Typhi, and mutations in two genes—gyrA and parC—result in resistance to fluoroquinolones. Baker et al. show that mutations in these genes confer a measurable fitness advantage over strains without these mutations, even in the absence of exposure to fluoroquinolones. Moreover, strains with two mutations in one of these genes exhibited a higher than predicted fitness, suggesting that there is a synergistic interaction between the two mutations. This work challenges the dogma that antimicrobial resistant organisms have a fitness disadvantage in the absence of antimicrobials, and suggests that increasing resistance to the fluoroquinolones is not solely driven by excessive use of this important group of drugs. DOI: http://dx.doi.org/10.7554/eLife.01229.002

Published

2016

31. Open Source Drug Discovery with the Malaria Box Compound Collection for Neglected Diseases and Beyond

Author

Phillips, Margaret A., Van Voorhis, Wesley C., Adams, John H., Adelfio, Roberto, Ahyong, Vida, Akabas, Myles H., Alano, Pietro, Alday, Aintzane, Alsibaee, Aishah, Alzualde, Ainhoa, Andrews, Katherine T., Avery, Simon V., Avery, Vicky M., Ayong, Lawrence, Baker, Mark, Baker, Stephen, Ben Mamoun, Choukri, Bhatia, Sangeeta, Bickle, Quentin, Bounaadja, Lotfi, Bowling, Tana, Boucher, Lauren E., Boyom, Fabrice F., Brea, Jose, Brennan, Marian, Burton, Audrey, Caffrey, Conor R., Camarda, Grazia, Carrasquilla, Manuela, Carter, Dee, Belen Cassera, Maria, Chih-Chien Cheng, Ken, Chindaudomsate, Worathad, Chubb, Anthony, Colon, Beatrice L., Corbett, Yolanda, Crowther, Gregory J., Cowan, Noemi, Le Dang, Na, Delves, Michael, DeRisi, Joseph L., Du, Alan Y., Duffy, Sandra, Abd El-Salam El-Sayed, Shimaa, Ferdig, Michael T., Fidock, David A., Florent, Isabelle, Fokou, Patrick V. T., Galstian, Ani, Gamo, Francisco Javier, Gokool, Suzanne, Gold, Ben, Golub, Todd, Goldgof, Gregory M., Guha, Rajarshi, Guiguemde, W. Armand, Gural, Nil, Guy, R. Kiplin, Hansen, Michael A. E., Hanson, Kirsten K., Hemphill, Andrew, Hooft van Huijsduijnen, Rob, Horii, Takaaki, Horrocks, Paul, Hughes, Tyler B., Huston, Christopher, Igarashi, Ikuo, Ingram-Sieber, Katrin, Itoe, Maurice A., Jadhav, Ajit, Naranuntarat Jensen, Amornrat, Jensen, Laran T., Jiang, Rays H.Y., Kaiser, Annette, Keiser, Jennifer, Ketas, Thomas, Kicka, Sebastien, Kim, Sunyoung, Kirk, Kiaran, Kumar, Vidya P., Kyle, Dennis E., Lafuente, Maria Jose, Landfear, Scott, Lee, Nathan, Lee, Sukjun, Lehane, Adele M., Li, Fengwu, Little, David, Liu, Liqiong, Loza, Maria I., Lubar, Aristea, Lucantoni, Leonardo, Lucet, Isabelle, Maes, Louis, Mancama, Dalu, Mansour, Nuha R., March, Sandra, McGowan, Sheena, Medina Vera, Iset, Meister, Stephan, Mercer, Luke, Mestres, Jordi, Mfopa, Alvine N., Misra, Raj N., Moon, Seunghyun, Moore, John P., Morais Rodrigues da Costa, Francielly, Muriana, Arantza, Nakazawa Hewitt, Stephen, Nare, Bakela, Nathan, Carl, Narraidoo, Nathalie, Nawaratna, Sujeevi, Ojo, Kayode K., Ortiz, Diana, Panic, Gordana, Papadatos, George, Parapini, Silvia, Patra, Kailash, Pham, Ngoc, Prats, Sarah, Plouffe, David M., Poulsen, Sally-Ann, Pradhan, Anupam, Quevedo, Celia, Quinn, Ronald J., Rice, Christopher A., Abdo Rizk, Mohamed, Ruecker, Andrea, St. Onge, Robert, Salgado Ferreira, Rafaela, Samra, Jasmeet, Robinett, Natalie G., Schlecht, Ulrich, Schmitt, Marjorie, Silva Villela, Filipe, Silvestrini, Francesco, Sinden, Robert, Smith, Dennis A., Soldati, Thierry, Stamm, Serge Maximilian, Sullivan, David J., Sullivan, William, Suresh, Sundari, Suzuki, Brian M., Suzuki, Yo, Swamidass, S. Joshua, Taramelli, Donatella, Tchokouaha, Lauve R.Y., Theron, Anjo, Thomas, David, Tonissen, Kathryn F., Townson, Simon, Tripathi, Abhai K., Trofimov, Valentin, Udenze, Kenneth O., Ullah, Imran, Vallieres, Cindy, Vigil, Edgar, Vinetz, Joseph M., Voong Vinh, Phat, Vu, Hoan, Watanabe, Nao-aki, Weatherby, Kate, White, Pamela M., Wilks, Andrew F., Winzeler, Elizabeth A., Wojcik, Edward, Wree, Melanie, Wu, Wesley, Yokoyama, Naoaki, Zollo, Paul H. A., Abla, Nada, Blasco, Benjamin, Burrows, Jeremy, Leroy, Didier, Spangenberg, Thomas, Wells, Timothy, and Willis, Paul A.

Abstract

A major cause of the paucity of new starting points for drug discovery is the lack of interaction between academia and industry. Much of the global resource in biology is present in universities, whereas the focus of medicinal chemistry is still largely within industry. Open source drug discovery, with sharing of information, is clearly a first step towards overcoming this gap. But the interface could especially be bridged through a scale-up of open sharing of physical compounds, which would accelerate the finding of new starting points for drug discovery. The Medicines for Malaria Venture Malaria Box is a collection of over 400 compounds representing families of structures identified in phenotypic screens of pharmaceutical and academic libraries against the Plasmodium falciparum malaria parasite. The set has now been distributed to almost 200 research groups globally in the last two years, with the only stipulation that information from the screens is deposited in the public domain. This paper reports for the first time on 236 screens that have been carried out against the Malaria Box and compares these results with 55 assays that were previously published, in a format that allows a meta-analysis of the combined dataset. The combined biochemical and cellular assays presented here suggest mechanisms of action for 135 (34%) of the compounds active in killing multiple life-cycle stages of the malaria parasite, including asexual blood, liver, gametocyte, gametes and insect ookinete stages. In addition, many compounds demonstrated activity against other pathogens, showing hits in assays with 16 protozoa, 7 helminths, 9 bacterial and mycobacterial species, the dengue fever mosquito vector, and the NCI60 human cancer cell line panel of 60 human tumor cell lines. Toxicological, pharmacokinetic and metabolic properties were collected on all the compounds, assisting in the selection of the most promising candidates for murine proof-of-concept experiments and medicinal chemistry programs. The data for all of these assays are presented and analyzed to show how outstanding leads for many indications can be selected. These results reveal the immense potential for translating the dispersed expertise in biological assays involving human pathogens into drug discovery starting points, by providing open access to new families of molecules, and emphasize how a small additional investment made to help acquire and distribute compounds, and sharing the data, can catalyze drug discovery for dozens of different indications. Another lesson is that when multiple screens from different groups are run on the same library, results can be integrated quickly to select the most valuable starting points for subsequent medicinal chemistry efforts.

Published

2016

32. In vitro activity of colistin in antimicrobial combination against carbapenem-resistant Acinetobacter baumannii isolated from patients with ventilator-associated pneumonia in Vietnam

Author

Pham Thi Thanh Tam, Nguyen Thi Khanh Nhu, Huynh Thi Loan, Louise Thwaites, Nguyen Phu Huong Lan, Stephen Baker, Tran Tinh Hien, Nguyen Van Vinh Chau, Ho Dang Trung Nghia, Vien Le Minh, Christopher M. Parry, Tran Vu Thieu Nga, Guy E. Thwaites, Ha Thanh Tuyen, Tran Do Hoang Nhu, Nguyen Van Hao, Lam Minh Yen, James Campbell, Voong Vinh Phat, and Corinne N. Thompson

Subjects

Acinetobacter baumannii, Microbiology (medical), Imipenem, Genotype, Ceftazidime, Microbial Sensitivity Tests, Microbiology, Meropenem, beta-Lactam Resistance, 03 medical and health sciences, 0302 clinical medicine, Intensive care, medicine, polycyclic compounds, Cluster Analysis, Humans, 030212 general & internal medicine, 0303 health sciences, biology, Colistin, Antimicrobial Agents and Chemotherapy, 030306 microbiology, Ventilator-associated pneumonia, Pneumonia, Ventilator-Associated, Drug Synergism, General Medicine, biochemical phenomena, metabolism, and nutrition, Antimicrobial, medicine.disease, biology.organism_classification, bacterial infections and mycoses, Hospitals, Standard, Anti-Bacterial Agents, 3. Good health, Carbapenems, Vietnam, bacteria, Multilocus Sequence Typing, medicine.drug

Abstract

Acinetobacter baumannii has become one of the major infection threats in intensive care units (ICUs) globally. Since 2008, A. baumannii has been the leading cause of ventilator-associated pneumonia (VAP) in our ICU at an infectious disease hospital in southern Vietnam. The emergence of this pathogen in our setting is consistent with the persistence of a specific clone exhibiting resistance to carbapenems. Antimicrobial combinations may be a strategy to treat infections caused by these carbapenem-resistant A. baumannii. Therefore, we assessed potential antimicrobial combinations against local carbapenem-resistant A. baumannii by measuring in vitro interactions of colistin with four antimicrobials that are locally certified for treating VAP. We first performed antimicrobial susceptibility testing and multilocus variable number tandem repeat analysis (MLVA) genotyping on 74 A. baumannii isolated from quantitative tracheal aspirates from patients with VAP over an 18-month period. These 74 isolates could be subdivided into 21 main clusters by MLVA and >80 % were resistant to carbapenems. We selected 56 representative isolates for in vitro combination synergy testing. Synergy was observed in four (7 %), seven (13 %), 20 (36 %) and 38 (68 %) isolates with combinations of colistin with ceftazidime, ceftriaxone, imipenem and meropenem, respectively. Notably, more carbapenem-resistant A. baumannii isolates (36/43; 84 %) exhibited synergistic activity with a combination of colistin and meropenem than carbapenem-susceptible A. baumannii isolates (2/13; 15 %) (P = 0.023; Fisher's exact test). Our findings suggest that combinations of colistin and meropenem should be considered when treating carbapenem-resistant A. baumannii infections in Vietnam, and we advocate clinical trials investigating combination therapy for VAP.

Published

2015

33. A prospective multi-center observational study of children hospitalized with diarrhea in Ho Chi Minh City, Vietnam

Author

Nguyen Van Minh Hoang, Ha Manh Tuan, James Campbell, Hoang Le Phuc, Maia A. Rabaa, Nguyen Minh Ngoc, My Vu Tra Phan, Tran Thi Ngoc Dung, Ha Vinh, Ha Thanh Tuyen, Corinne N. Thompson, Nguyen Van Vinh Chau, Tran Tinh Hien, Claire Jenkins, Tang Chi Thuong, Stephen Baker, Guy E. Thwaites, Pham Thi Ngoc Tuyet, Nguyen Tran Chinh, Le Thi Phuong Tu, Keisuke Yoshihara, Cao Thu Thuy, Nguyen Thanh Vinh, Tran Thi Thu Nga, Vu Thuy Duong, Pham Van Minh, Voong Vinh Phat, Pham Thanh Duy, and Tran Vu Thieu Nga

Subjects

Diarrhea, Male, Rotavirus, Pediatrics, medicine.medical_specialty, Cross-sectional study, Microbial Sensitivity Tests, medicine.disease_cause, Rotavirus Infections, 03 medical and health sciences, 0302 clinical medicine, Antibiotic resistance, Anti-Infective Agents, Virology, medicine, Humans, Prospective Studies, 030212 general & internal medicine, Medical prescription, Caliciviridae Infections, Demography, 0303 health sciences, Bacteria, 030306 microbiology, business.industry, Campylobacter, Norovirus, Infant, Bacterial Infections, Articles, 3. Good health, Hospitalization, Cross-Sectional Studies, Infectious Diseases, Vietnam, Child, Preschool, Etiology, Female, Parasitology, Seasons, medicine.symptom, business

Abstract

We performed a prospective multicenter study to address the lack of data on the etiology, clinical and demographic features of hospitalized pediatric diarrhea in Ho Chi Minh City (HCMC), Vietnam. Over 2,000 (1,419 symptomatic and 609 non-diarrheal control) children were enrolled in three hospitals over a 1-year period in 2009–2010. Aiming to detect a panel of pathogens, we identified a known diarrheal pathogen in stool samples from 1,067/1,419 (75.2%) children with diarrhea and from 81/609 (13.3%) children without diarrhea. Rotavirus predominated in the symptomatic children (664/1,419; 46.8%), followed by norovirus (293/1,419; 20.6%). The bacterial pathogens Salmonella, Campylobacter, and Shigella were cumulatively isolated from 204/1,419 (14.4%) diarrheal children and exhibited extensive antimicrobial resistance, most notably to fluoroquinolones and third-generation cephalosporins. We suggest renewed efforts in generation and implementation of policies to control the sale and prescription of antimicrobials to curb bacterial resistance and advise consideration of a subsidized rotavirus vaccination policy to limit the morbidity due to diarrheal disease in Vietnam.

Published

2015

34. Novel porcine-like human G26P[19] rotavirus identified in hospitalized paediatric diarrhea patients in Ho Chi Minh City, Vietnam

Author

Juliet E. Bryant, Tran Thi Ngoc Dung, Celeste M. Donato, Mark E. J. Woolhouse, Daniel Cowley, Pham Hong Anh, Phan Vu Tra My, Guy E. Thwaites, Voong Vinh Phat, Ha Vinh, Stephen Baker, Carl D. Kirkwood, Paul Kellam, and Maia A. Rabaa

Subjects

RNA viruses, Diarrhea, Rotavirus, STRAIN, Genotype, Short Communication, viruses, Molecular Sequence Data, Reassortment, CHILDREN, Biology, medicine.disease_cause, Rotavirus Infections, 03 medical and health sciences, 07 Agricultural and Veterinary Sciences, Virology, medicine, Humans, PHYLOGENIES, 11 Medical and Health Sciences, Phylogeny, 030304 developmental biology, CLOSE RELATIONSHIP, Inpatients, 0303 health sciences, Disease surveillance, NSP1, Science & Technology, ORIGIN, Animal, 030306 microbiology, Transmission (medicine), SEQUENCE-ANALYSIS, virus diseases, 06 Biological Sciences, Vaccine efficacy, GENOMIC ANALYSIS, 3. Good health, Biotechnology & Applied Microbiology, Vietnam, Child, Preschool, GROUP-A ROTAVIRUSES, VP4 GENES, medicine.symptom, Life Sciences & Biomedicine

Abstract

During a hospital-based diarrhoeal disease study conducted in Ho Chi Minh City, Vietnam from 2009 to 2010, we identified four symptomatic children infected with G26P[19] rotavirus (RV) – an atypical variant that has not previously been reported in human gastroenteritis. To determine the genetic structure and investigate the origin of this G26P[19] strain, the whole genome of a representative example was characterized, revealing a novel genome constellation: G26–P[19]–I5–R1–C1–M1–A8–N1–T1–E1–H1. The genome segments were most closely related to porcine (VP7, VP4, VP6 and NSP1) and Wa-like porcine RVs (VP1–3 and NSP2–5). We proposed that this G26P[19] strain was the product of zoonotic transmission coupled with one or more reassortment events occurring in human and/or animal reservoirs. The identification of such strains has potential implications for vaccine efficacy in south-east Asia, and outlines the utility of whole-genome sequencing for studying RV diversity and zoonotic potential during disease surveillance.

Published

2014

35. Open Source Drug Discovery with the Malaria Box Compound Collection for Neglected Diseases and Beyond

Author

Van Voorhis, Wesley C., primary, Adams, John H., additional, Adelfio, Roberto, additional, Ahyong, Vida, additional, Akabas, Myles H., additional, Alano, Pietro, additional, Alday, Aintzane, additional, Alemán Resto, Yesmalie, additional, Alsibaee, Aishah, additional, Alzualde, Ainhoa, additional, Andrews, Katherine T., additional, Avery, Simon V., additional, Avery, Vicky M., additional, Ayong, Lawrence, additional, Baker, Mark, additional, Baker, Stephen, additional, Ben Mamoun, Choukri, additional, Bhatia, Sangeeta, additional, Bickle, Quentin, additional, Bounaadja, Lotfi, additional, Bowling, Tana, additional, Bosch, Jürgen, additional, Boucher, Lauren E., additional, Boyom, Fabrice F., additional, Brea, Jose, additional, Brennan, Marian, additional, Burton, Audrey, additional, Caffrey, Conor R., additional, Camarda, Grazia, additional, Carrasquilla, Manuela, additional, Carter, Dee, additional, Belen Cassera, Maria, additional, Chih-Chien Cheng, Ken, additional, Chindaudomsate, Worathad, additional, Chubb, Anthony, additional, Colon, Beatrice L., additional, Colón-López, Daisy D., additional, Corbett, Yolanda, additional, Crowther, Gregory J., additional, Cowan, Noemi, additional, D’Alessandro, Sarah, additional, Le Dang, Na, additional, Delves, Michael, additional, DeRisi, Joseph L., additional, Du, Alan Y., additional, Duffy, Sandra, additional, Abd El-Salam El-Sayed, Shimaa, additional, Ferdig, Michael T., additional, Fernández Robledo, José A., additional, Fidock, David A., additional, Florent, Isabelle, additional, Fokou, Patrick V. T., additional, Galstian, Ani, additional, Gamo, Francisco Javier, additional, Gokool, Suzanne, additional, Gold, Ben, additional, Golub, Todd, additional, Goldgof, Gregory M., additional, Guha, Rajarshi, additional, Guiguemde, W. Armand, additional, Gural, Nil, additional, Guy, R. Kiplin, additional, Hansen, Michael A. E., additional, Hanson, Kirsten K., additional, Hemphill, Andrew, additional, Hooft van Huijsduijnen, Rob, additional, Horii, Takaaki, additional, Horrocks, Paul, additional, Hughes, Tyler B., additional, Huston, Christopher, additional, Igarashi, Ikuo, additional, Ingram-Sieber, Katrin, additional, Itoe, Maurice A., additional, Jadhav, Ajit, additional, Naranuntarat Jensen, Amornrat, additional, Jensen, Laran T., additional, Jiang, Rays H. Y., additional, Kaiser, Annette, additional, Keiser, Jennifer, additional, Ketas, Thomas, additional, Kicka, Sebastien, additional, Kim, Sunyoung, additional, Kirk, Kiaran, additional, Kumar, Vidya P., additional, Kyle, Dennis E., additional, Lafuente, Maria Jose, additional, Landfear, Scott, additional, Lee, Nathan, additional, Lee, Sukjun, additional, Lehane, Adele M., additional, Li, Fengwu, additional, Little, David, additional, Liu, Liqiong, additional, Llinás, Manuel, additional, Loza, Maria I., additional, Lubar, Aristea, additional, Lucantoni, Leonardo, additional, Lucet, Isabelle, additional, Maes, Louis, additional, Mancama, Dalu, additional, Mansour, Nuha R., additional, March, Sandra, additional, McGowan, Sheena, additional, Medina Vera, Iset, additional, Meister, Stephan, additional, Mercer, Luke, additional, Mestres, Jordi, additional, Mfopa, Alvine N., additional, Misra, Raj N., additional, Moon, Seunghyun, additional, Moore, John P., additional, Morais Rodrigues da Costa, Francielly, additional, Müller, Joachim, additional, Muriana, Arantza, additional, Nakazawa Hewitt, Stephen, additional, Nare, Bakela, additional, Nathan, Carl, additional, Narraidoo, Nathalie, additional, Nawaratna, Sujeevi, additional, Ojo, Kayode K., additional, Ortiz, Diana, additional, Panic, Gordana, additional, Papadatos, George, additional, Parapini, Silvia, additional, Patra, Kailash, additional, Pham, Ngoc, additional, Prats, Sarah, additional, Plouffe, David M., additional, Poulsen, Sally-Ann, additional, Pradhan, Anupam, additional, Quevedo, Celia, additional, Quinn, Ronald J., additional, Rice, Christopher A., additional, Abdo Rizk, Mohamed, additional, Ruecker, Andrea, additional, St. Onge, Robert, additional, Salgado Ferreira, Rafaela, additional, Samra, Jasmeet, additional, Robinett, Natalie G., additional, Schlecht, Ulrich, additional, Schmitt, Marjorie, additional, Silva Villela, Filipe, additional, Silvestrini, Francesco, additional, Sinden, Robert, additional, Smith, Dennis A., additional, Soldati, Thierry, additional, Spitzmüller, Andreas, additional, Stamm, Serge Maximilian, additional, Sullivan, David J., additional, Sullivan, William, additional, Suresh, Sundari, additional, Suzuki, Brian M., additional, Suzuki, Yo, additional, Swamidass, S. Joshua, additional, Taramelli, Donatella, additional, Tchokouaha, Lauve R. Y., additional, Theron, Anjo, additional, Thomas, David, additional, Tonissen, Kathryn F., additional, Townson, Simon, additional, Tripathi, Abhai K., additional, Trofimov, Valentin, additional, Udenze, Kenneth O., additional, Ullah, Imran, additional, Vallieres, Cindy, additional, Vigil, Edgar, additional, Vinetz, Joseph M., additional, Voong Vinh, Phat, additional, Vu, Hoan, additional, Watanabe, Nao-aki, additional, Weatherby, Kate, additional, White, Pamela M., additional, Wilks, Andrew F., additional, Winzeler, Elizabeth A., additional, Wojcik, Edward, additional, Wree, Melanie, additional, Wu, Wesley, additional, Yokoyama, Naoaki, additional, Zollo, Paul H. A., additional, Abla, Nada, additional, Blasco, Benjamin, additional, Burrows, Jeremy, additional, Laleu, Benoît, additional, Leroy, Didier, additional, Spangenberg, Thomas, additional, Wells, Timothy, additional, and Willis, Paul A., additional

Published

2016

36. A novel ciprofloxacin-resistant subclade of H58 Salmonella Typhi is associated with fluoroquinolone treatment failure

Author

Pham Thanh, Duy, primary, Karkey, Abhilasha, additional, Dongol, Sabina, additional, Ho Thi, Nhan, additional, Thompson, Corinne N, additional, Rabaa, Maia A, additional, Arjyal, Amit, additional, Holt, Kathryn E, additional, Wong, Vanessa, additional, Tran Vu Thieu, Nga, additional, Voong Vinh, Phat, additional, Ha Thanh, Tuyen, additional, Pradhan, Ashish, additional, Shrestha, Saroj Kumar, additional, Gajurel, Damoder, additional, Pickard, Derek, additional, Parry, Christopher M, additional, Dougan, Gordon, additional, Wolbers, Marcel, additional, Dolecek, Christiane, additional, Thwaites, Guy E, additional, Basnyat, Buddha, additional, and Baker, Stephen, additional

Published

2016

37. South Asia as a reservoir for the global spread of ciprofloxacin resistant Shigella sonnei

Author

Chung The, Hao, primary, Rabaa, Maia A, additional, Pham Thanh, Duy, additional, De Lappe, Niall, additional, Cormican, Martin, additional, Howden, Benjamin P, additional, Wangchuk, Sonam, additional, Bodhidatta, Ladaporn, additional, Jeffries, Carl, additional, Nguyen Thi Nguyen, To, additional, Vu Thuy, Duong, additional, Thompson, Corinne N, additional, Phu Huong Lan, Nguyen, additional, Voong Vinh, Phat, additional, Ha Thanh, Tuyen, additional, Turner, Paul, additional, Sar, Poda, additional, Thwaites, Guy E, additional, Thompson, Nicholas R, additional, Holt, Kathryn E, additional, and Baker, Stephen, additional

Published

2016

38. Author response: A novel ciprofloxacin-resistant subclade of H58 Salmonella Typhi is associated with fluoroquinolone treatment failure

Author

Pham Thanh, Duy, primary, Karkey, Abhilasha, additional, Dongol, Sabina, additional, Ho Thi, Nhan, additional, Thompson, Corinne N, additional, Rabaa, Maia A, additional, Arjyal, Amit, additional, Holt, Kathryn E, additional, Wong, Vanessa, additional, Tran Vu Thieu, Nga, additional, Voong Vinh, Phat, additional, Ha Thanh, Tuyen, additional, Pradhan, Ashish, additional, Shrestha, Saroj Kumar, additional, Gajurel, Damoder, additional, Pickard, Derek, additional, Parry, Christopher M, additional, Dougan, Gordon, additional, Wolbers, Marcel, additional, Dolecek, Christiane, additional, Thwaites, Guy E, additional, Basnyat, Buddha, additional, and Baker, Stephen, additional

Published

2016

39. The Ecological Dynamics of Fecal Contamination and Salmonella Typhi and Salmonella Paratyphi A in Municipal Kathmandu Drinking Water

Author

Karkey, Abhilasha, primary, Jombart, Thibaut, additional, Walker, Alan W., additional, Thompson, Corinne N., additional, Torres, Andres, additional, Dongol, Sabina, additional, Tran Vu Thieu, Nga, additional, Pham Thanh, Duy, additional, Tran Thi Ngoc, Dung, additional, Voong Vinh, Phat, additional, Singer, Andrew C., additional, Parkhill, Julian, additional, Thwaites, Guy, additional, Basnyat, Buddha, additional, Ferguson, Neil, additional, and Baker, Stephen, additional

Published

2016

40. Author response: Fitness benefits in fluoroquinolone-resistant Salmonella Typhi in the absence of antimicrobial pressure

Author

Tran Thuy Chau, Pham Thanh Duy, Tran Vu Thieu Nga, Tran Thi Ngoc Dung, A. Keith Turner, Jeremy Farrar, Voong Vinh Phat, Stephen Baker, and Maciej F. Boni

Subjects

business.industry, Medicine, Antimicrobial, business, Fluoroquinolone resistant Salmonella, Microbiology

Published

2013

41. Salmonella Typhi and Salmonella Paratyphi A elaborate distinct systemic metabolite signatures during enteric fever

Author

Näsström, Elin, primary, Vu Thieu, Nga Tran, additional, Dongol, Sabina, additional, Karkey, Abhilasha, additional, Voong Vinh, Phat, additional, Ha Thanh, Tuyen, additional, Johansson, Anders, additional, Arjyal, Amit, additional, Thwaites, Guy, additional, Dolecek, Christiane, additional, Basnyat, Buddha, additional, Baker, Stephen, additional, and Antti, Henrik, additional

Published

2014

42. A Double-blind, Randomized, Placebo-controlled Trial of Lactobacillus acidophilusfor the Treatment of Acute Watery Diarrhea in Vietnamese Children

Author

Hong Chau, Tran Thi, Minh Chau, Nguyen Ngoc, Hoang Le, Nhat Thanh, Chung The, Hao, Voong Vinh, Phat, Nguyen To, Nguyen Thi, Ngoc, Nguyen Minh, Tuan, Ha Manh, Chau Ngoc, Tang Le, Kolader, Marion-Eliette, Farrar, Jeremy J., Wolbers, Marcel, Thwaites, Guy E., and Baker, Stephen

Abstract

Supplemental Digital Content is available in the text.

Published

2018

43. Identification of Salmonella enterica Serovar Typhi Genotypes by Use of Rapid Multiplex Ligation-Dependent Probe Amplification

Author

Pham Thanh, Duy, primary, Tran Vu Thieu, Nga, additional, Tran Thuy, Chau, additional, Lodén, Martin, additional, Tuin, Kiki, additional, Campbell, James I., additional, Van Minh Hoang, Nguyen, additional, Voong Vinh, Phat, additional, Farrar, Jeremy J., additional, Holt, Kathryn E., additional, Dougan, Gordon, additional, and Baker, Stephen, additional

Published

2013

44. Differential Epidemiology of Salmonella Typhi and Paratyphi A in Kathmandu, Nepal: A Matched Case Control Investigation in a Highly Endemic Enteric Fever Setting

Author

Karkey, Abhilasha, primary, Thompson, Corinne N., additional, Tran Vu Thieu, Nga, additional, Dongol, Sabina, additional, Le Thi Phuong, Tu, additional, Voong Vinh, Phat, additional, Arjyal, Amit, additional, Martin, Laura B., additional, Rondini, Simona, additional, Farrar, Jeremy J., additional, Dolecek, Christiane, additional, Basnyat, Buddha, additional, and Baker, Stephen, additional

Published

2013

45. A Prospective Multi-Center Observational Study of Children Hospitalized with Diarrhea in Ho Chi Minh City, Vietnam.

Author

Thompson, Corinne N., My V. T. Phan, Nguyen Van Minh Hoang, Pham Van Minh, Nguyen Thanh Vinh, Cao Thu Thuy, Tran Thi Thu Nga, Rabaa, Maia A., Pham Thanh Duy, Tran Thi Ngoc Dung, Voong Vinh Phat, Tran Vu Thieu Nga, Le Thi Phuong Tu, Ha Thanh Tuyen, Keisuke Yoshihara, Jenkins, Claire, Vu Thuy Duong, Hoang Le Phuc, Pham Thi Ngoc Tuyet, and Nguyen Minh Ngoc

Published

2015

46. Differential Epidemiology of Salmonella Typhi and Paratyphi A in Kathmandu, Nepal: A Matched Case Control Investigation in a Highly Endemic Enteric Fever Setting.

Author

Karkey, Abhilasha, Thompson, Corinne N., Tran Vu Thieu, Nga, Dongol, Sabina, Le Thi Phuong, Tu, Voong Vinh, Phat, Arjyal, Amit, Martin, Laura B., Rondini, Simona, Farrar, Jeremy J., Dolecek, Christiane, Basnyat, Buddha, and Baker, Stephen

Subjects

SALMONELLA typhi, CASE-control method, TYPHOID vaccines, LOGISTIC regression analysis, HEALTH behavior

Abstract

Background: Enteric fever, a systemic infection caused by the bacteria Salmonella Typhi and Salmonella Paratyphi A, is endemic in Kathmandu, Nepal. Previous work identified proximity to poor quality water sources as a community-level risk for infection. Here, we sought to examine individual-level risk factors related to hygiene and sanitation to improve our understanding of the epidemiology of enteric fever in this setting. Methodology and principal findings: A matched case-control analysis was performed through enrollment of 103 blood culture positive enteric fever patients and 294 afebrile community-based age and gender-matched controls. A detailed questionnaire was administered to both cases and controls and the association between enteric fever infection and potential exposures were examined through conditional logistic regression. Several behavioral practices were identified as protective against infection with enteric fever, including water storage and hygienic habits. Additionally, we found that exposures related to poor water and socioeconomic status are more influential in the risk of infection with S. Typhi, whereas food consumption habits and migration play more of a role in risk of S. Paratyphi A infection. Conclusions and significance: Our work suggests that S. Typhi and S. Paratyphi A follow different routes of infection in this highly endemic setting and that sustained exposure to both serovars probably leads to the development of passive immunity. In the absence of a polyvalent vaccine against S. Typhi and S. Paratyphi A, we advocate better systems for water treatment and storage, improvements in the quality of street food, and vaccination with currently available S. Typhi vaccines. [ABSTRACT FROM AUTHOR]

Published

2013

47. Identification of Salmonella entericaSerovar Typhi Genotypes by Use of Rapid Multiplex Ligation-Dependent Probe Amplification

Author

Pham Thanh, Duy, Tran Vu Thieu, Nga, Tran Thuy, Chau, Lodén, Martin, Tuin, Kiki, Campbell, James I., Van Minh Hoang, Nguyen, Voong Vinh, Phat, Farrar, Jeremy J., Holt, Kathryn E., Dougan, Gordon, and Baker, Stephen

Abstract

ABSTRACTSalmonella entericaserovar Typhi, the causative agent of typhoid fever, is highly clonal and genetically conserved, making isolate subtyping difficult. We describe a standardized multiplex ligation-dependent probe amplification (MLPA) genotyping scheme targeting 11 key phylogenetic markers of the S. Typhi genome. The MLPA method demonstrated 90% concordance with single nucleotide polymorphism (SNP) typing, the gold standard for S. Typhi genotyping, and had the ability to identify isolates of the H58 haplotype, which is associated with resistance to multiple antimicrobials. Additionally, the assay permitted the detection of fluoroquinolone resistance-associated mutations in the DNA gyrase-encoding gene gyrAand the topoisomerase gene parCwith a sensitivity of 100%. The MLPA methodology is simple and reliable, providing phylogenetically and phenotypically relevant genotyping information. This MLPA scheme offers a more-sensitive and interpretable alternative to the nonphylogenetic subgrouping methodologies that are currently used in reference and research laboratories in areas where typhoid is endemic.

Published

2013

48. Open source drug discovery with the malaria box compound collection for neglected diseases and beyond

Author

Van Voorhis, Wesley C., Adams, John H., Adelfio, Roberto, Ahyong, Vida, Akabas, Myles H., Alano, Pietro, Alday, Aintzane, Alemán Resto, Yesmalie, Alsibaee, Aishah, Alzualde, Ainhoa, Andrews, Katherine T., Avery, Simon V., Avery, Vicky M., Ayong, Lawrence, Baker, Mark, Baker, Stephen, Ben Mamoun, Choukri, Bhatia, Sangeeta, Bickle, Quentin, Bounaadja, Lotfi, Bowling, Tana, Bosch, Jürgen, Boucher, Lauren E., Boyom, Fabrice F., Brea, Jose, Brennan, Marian, Burton, Audrey, Caffrey, Conor R., Camarda, Grazia, Carrasquilla, Manuela, Carter, Dee, Belen Cassera, Maria, Chih-Chien Cheng, Ken, Chindaudomsate, Worathad, Chubb, Anthony, Colon, Beatrice L., Colón-López, Daisy D., Corbett, Yolanda, Crowther, Gregory J., Cowan, Noemi, D'Alessandro, Sarah, Le Dang, Na, Delves, Michael, DeRisi, Joseph L., Du, Alan Y., Duffy, Sandra, Abd El-Salam El-Sayed, Shimaa, Ferdig, Michael T., Fernández Robledo, José A., Fidock, David A., Florent, Isabelle, Fokou, Patrick V. T., Galstian, Ani, Gamo, Francisco Javier, Gokool, Suzanne, Gold, Ben, Golub, Todd, Goldgof, Gregory M., Guha, Rajarshi, Guiguemde, W. Armand, Gural, Nil, Guy, R. Kiplin, Hansen, Michael A. E., Hanson, Kirsten K., Hemphill, Andrew, Hooft van Huijsduijnen, Rob, Horii, Takaaki, Horrocks, Paul, Hughes, Tyler B., Huston, Christopher, Igarashi, Ikuo, Ingram-Sieber, Katrin, Itoe, Maurice A., Jadhav, Ajit, Naranuntarat Jensen, Amornrat, Jensen, Laran T., Jiang, Rays H. Y., Kaiser, Annette, Keiser, Jennifer, Ketas, Thomas, Kicka, Sebastien, Kim, Sunyoung, Kirk, Kiaran, Kumar, Vidya P., Kyle, Dennis E., Lafuente, Maria Jose, Landfear, Scott, Lee, Nathan, Lee, Sukjun, Lehane, Adele M., Li, Fengwu, Little, David, Liu, Liqiong, Llinás, Manuel, Loza, Maria I., Lubar, Aristea, Lucantoni, Leonardo, Lucet, Isabelle, Maes, Louis, Mancama, Dalu, Mansour, Nuha R., March, Sandra, McGowan, Sheena, Medina Vera, Iset, Meister, Stephan, Mercer, Luke, Mestres, Jordi, Mfopa, Alvine N., Misra, Raj N., Moon, Seunghyun, Moore, John P., Morais Rodrigues da Costa, Francielly, Müller, Joachim, Muriana, Arantza, Nakazawa Hewitt, Stephen, Nare, Bakela, Nathan, Carl, Narraidoo, Nathalie, Nawaratna, Sujeevi, Ojo, Kayode K., Ortiz, Diana, Panic, Gordana, Papadatos, George, Parapini, Silvia, Patra, Kailash, Pham, Ngoc, Prats, Sarah, Plouffe, David M., Poulsen, Sally-Ann, Pradhan, Anupam, Quevedo, Celia, Quinn, Ronald J., Rice, Christopher A., Abdo Rizk, Mohamed, Ruecker, Andrea, St Onge, Robert, Salgado Ferreira, Rafaela, Samra, Jasmeet, Robinett, Natalie G., Schlecht, Ulrich, Schmitt, Marjorie, Silva Villela, Filipe, Silvestrini, Francesco, Sinden, Robert, Smith, Dennis A., Soldati, Thierry, Spitzmüller, Andreas, Stamm, Serge Maximilian, Sullivan, David J., Sullivan, William, Suresh, Sundari, Suzuki, Brian M., Suzuki, Yo, Swamidass, S. Joshua, Taramelli, Donatella, Tchokouaha, Lauve R. Y., Theron, Anjo, Thomas, David, Tonissen, Kathryn F., Townson, Simon, Tripathi, Abhai K., Trofimov, Valentin, Udenze, Kenneth O., Ullah, Imran, Vallieres, Cindy, Vigil, Edgar, Vinetz, Joseph M., Voong Vinh, Phat, Vu, Hoan, Watanabe, Nao-Aki, Weatherby, Kate, White, Pamela M., Wilks, Andrew F., Winzeler, Elizabeth A., Wojcik, Edward, Wree, Melanie, Wu, Wesley, Yokoyama, Naoaki, Zollo, Paul H. A., Abla, Nada, Blasco, Benjamin, Burrows, Jeremy, Laleu, Benoît, Leroy, Didier, Spangenberg, Thomas, Wells, Timothy, and Willis, Paul A.

Subjects

3. Good health

49. An evaluation of purified Salmonella Typhi protein antigens for the serological diagnosis of acute typhoid fever

Author

Tran Vu Thieu, Nga, Trinh Van, Tan, Tran Tuan, Anh, Klemm, Elizabeth J, Nguyen Ngoc Minh, Chau, Voong Vinh, Phat, Pham Thanh, Duy, Ho Ngoc Dan, Thanh, Pham Duc, Trung, Langat, Pinky, Martin, Laura B, Galan, Jorge, Liang, Li, Felgner, Philip L, Davies, D Huw, De Jong, Hanna K, Maude, Rapeephan R, Fukushima, Masako, Wijedoru, Lalith, Ghose, Aniruddha, Samad, Rasheda, Dondorp, Arjen M, Faiz, Abul, Darton, Thomas C, Pollard, Andrew J, Thwaites, Guy E, Dougan, Gordon, Parry, Christopher M, and Baker, Stephen

Subjects

Bangladesh, Antigens, Bacterial, Bacteriological Techniques, IgM, Febrile disease, Polysaccharides, Bacterial, Enteric fever, Salmonella typhi, bacterial infections and mycoses, complex mixtures, Antibodies, Bacterial, 3. Good health, Immunoglobulin M, Humans, Typhoid Fever, Diagnostics, Vi polysaccharide

Abstract

OBJECTIVES: The diagnosis of typhoid fever is a challenge. Aiming to develop a typhoid diagnostic we measured antibody responses against Salmonella Typhi (S. Typhi) protein antigens and the Vi polysaccharide in a cohort of Bangladeshi febrile patients. METHODS: IgM against 12 purified antigens and the Vi polysaccharide was measured by ELISA in plasma from patients with confirmed typhoid fever (n = 32), other confirmed infections (n = 17), and healthy controls (n = 40). ELISAs with the most specific antigens were performed on plasma from 243 patients with undiagnosed febrile disease. RESULTS: IgM against the S. Typhi protein antigens correlated with each other (rho > 0.8), but not against Vi (rho < 0.6). Typhoid patients exhibited higher IgM against 11/12 protein antigens and Vi than healthy controls and those with other infections. Vi, PilL, and CdtB exhibited the greatest sensitivity and specificity. Specificity and sensitivity was improved when Vi was combined with a protein antigen, generating sensitivities and specificities of 0.80 and >0.85, respectively. Applying a dynamic cut-off to patients with undiagnosed febrile disease suggested that 34-58% had an IgM response indicative of typhoid. CONCLUSIONS: We evaluated the diagnostic potential of several S. Typhi antigens; our assays give good sensitivity and specificity, but require further assessment in differing patient populations.

50. Dissecting the molecular evolution of fluoroquinolone-resistant Shigella sonnei

Author

Chung The, Hao, Boinett, Christine, Pham Thanh, Duy, Jenkins, Claire, Weill, Francois-Xavier, Howden, Benjamin P, Valcanis, Mary, De Lappe, Niall, Cormican, Martin, Wangchuk, Sonam, Bodhidatta, Ladaporn, Mason, Carl J, Nguyen, To Nguyen Thi, Ha Thanh, Tuyen, Voong, Vinh Phat, Duong, Vu Thuy, Nguyen, Phu Huong Lan, Turner, Paul, Wick, Ryan, Ceyssens, Pieter-Jan, Thwaites, Guy, Holt, Kathryn E, Thomson, Nicholas R, Rabaa, Maia A, and Baker, Stephen

Subjects

DNA Topoisomerase IV, Molecular Epidemiology, Shigella sonnei, Bayes Theorem, biochemical phenomena, metabolism, and nutrition, bacterial infections and mycoses, Polymorphism, Single Nucleotide, digestive system diseases, 3. Good health, Anti-Bacterial Agents, Europe, Evolution, Molecular, Ciprofloxacin, DNA Gyrase, Drug Resistance, Bacterial, Mutation, Asia, Western, bacteria, Humans, Directed Molecular Evolution, Asia, Southeastern, Genome, Bacterial, Phylogeny, Dysentery, Bacillary, Fluoroquinolones

Abstract

Shigella sonnei increasingly dominates the international epidemiological landscape of shigellosis. Treatment options for S. sonnei are dwindling due to resistance to several key antimicrobials, including the fluoroquinolones. Here we analyse nearly 400 S. sonnei whole genome sequences from both endemic and non-endemic regions to delineate the evolutionary history of the recently emergent fluoroquinolone-resistant S. sonnei. We reaffirm that extant resistant organisms belong to a single clonal expansion event. Our results indicate that sequential accumulation of defining mutations (gyrA-S83L, parC-S80I, and gyrA-D87G) led to the emergence of the fluoroquinolone-resistant S. sonnei population around 2007 in South Asia. This clone was then transmitted globally, resulting in establishments in Southeast Asia and Europe. Mutation analysis suggests that the clone became dominant through enhanced adaptation to oxidative stress. Experimental evolution reveals that under fluoroquinolone exposure in vitro, resistant S. sonnei develops further intolerance to the antimicrobial while the susceptible counterpart fails to attain complete resistance.