Your search keyword '"Sin Reaksmey"' showing total 7 results

1. Correction: Rapid Diagnostic Tests for Dengue Virus Infection in Febrile Cambodian Children: Diagnostic Accuracy and Incorporation into Diagnostic Algorithms.

Author

Michael J Carter, Kate R Emary, Catherine E Moore, Christopher M Parry, Soeng Sona, Hor Putchhat, Sin Reaksmey, Ngoun Chanpheaktra, Nicole Stoesser, Andrew D M Dobson, Nicholas P J Day, Varun Kumar, and Stuart D Blacksell

Subjects

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

Published

2016

2. Rapid diagnostic tests for dengue virus infection in febrile Cambodian children: diagnostic accuracy and incorporation into diagnostic algorithms.

Author

Michael J Carter, Kate R Emary, Catrin E Moore, Christopher M Parry, Soeng Sona, Hor Putchhat, Sin Reaksmey, Ngoun Chanpheaktra, Nicole Stoesser, Andrew D M Dobson, Nicholas P J Day, Varun Kumar, and Stuart D Blacksell

Subjects

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

Abstract

Dengue virus (DENV) infection is prevalent across tropical regions and may cause severe disease. Early diagnosis may improve supportive care. We prospectively assessed the Standard Diagnostics (Korea) BIOLINE Dengue Duo DENV rapid diagnostic test (RDT) to NS1 antigen and anti-DENV IgM (NS1 and IgM) in children in Cambodia, with the aim of improving the diagnosis of DENV infection.We enrolled children admitted to hospital with non-localised febrile illnesses during the 5-month DENV transmission season. Clinical and laboratory variables, and DENV RDT results were recorded at admission. Children had blood culture and serological and molecular tests for common local pathogens, including reference laboratory DENV NS1 antigen and IgM assays. 337 children were admitted with non-localised febrile illness over 5 months. 71 (21%) had DENV infection (reference assay positive). Sensitivity was 58%, and specificity 85% for RDT NS1 and IgM combined. Conditional inference framework analysis showed the additional value of platelet and white cell counts for diagnosis of DENV infection. Variables associated with diagnosis of DENV infection were not associated with critical care admission (70 children, 21%) or mortality (19 children, 6%). Known causes of mortality were melioidosis (4), other sepsis (5), and malignancy (1). 22 (27%) children with a positive DENV RDT had a treatable other infection.The DENV RDT had low sensitivity for the diagnosis of DENV infection. The high co-prevalence of infections in our cohort indicates the need for a broad microbiological assessment of non-localised febrile illness in these children.

Published

2015

3. A prospective study of the causes of febrile illness requiring hospitalization in children in Cambodia.

Author

Kheng Chheng, Michael J Carter, Kate Emary, Ngoun Chanpheaktra, Catrin E Moore, Nicole Stoesser, Hor Putchhat, Soeng Sona, Sin Reaksmey, Paul Kitsutani, Borann Sar, H Rogier van Doorn, Nguyen Hanh Uyen, Le Van Tan, Daniel H Paris, Stuart D Blacksell, Premjit Amornchai, Vanaporn Wuthiekanun, Christopher M Parry, Nicholas P J Day, and Varun Kumar

Subjects

Medicine, Science

Abstract

BACKGROUND:Febrile illnesses are pre-eminent contributors to morbidity and mortality among children in South-East Asia but the causes are poorly understood. We determined the causes of fever in children hospitalised in Siem Reap province, Cambodia. METHODS AND FINDINGS:A one-year prospective study of febrile children admitted to Angkor Hospital for Children, Siem Reap. Demographic, clinical, laboratory and outcome data were comprehensively analysed. Between October 12(th) 2009 and October 12(th) 2010 there were 1225 episodes of febrile illness in 1180 children. Median (IQR) age was 2.0 (0.8-6.4) years, with 850 (69%) episodes in children

Published

2013

4. Subpopulations of Staphylococcus aureus clonal complex 121 are associated with distinct clinical entities.

Author

Kevin Kurt, Jean-Philippe Rasigade, Frederic Laurent, Richard V Goering, Helena Žemličková, Ivana Machova, Marc J Struelens, Andreas E Zautner, Silva Holtfreter, Barbara Bröker, Stephen Ritchie, Sin Reaksmey, Direk Limmathurotsakul, Sharon J Peacock, Christiane Cuny, Franziska Layer, Wolfgang Witte, and Ulrich Nübel

Subjects

Medicine, Science

Abstract

We investigated the population structure of Staphylococcus aureus clonal complex CC121 by mutation discovery at 115 genetic housekeeping loci from each of 154 isolates, sampled on five continents between 1953 and 2009. In addition, we pyro-sequenced the genomes from ten representative isolates. The genome-wide SNPs that were ascertained revealed the evolutionary history of CC121, indicating at least six major clades (A to F) within the clonal complex and dating its most recent common ancestor to the pre-antibiotic era. The toxin gene complement of CC121 isolates was correlated with their SNP-based phylogeny. Moreover, we found a highly significant association of clinical phenotypes with phylogenetic affiliations, which is unusual for S. aureus. All isolates evidently sampled from superficial infections (including staphylococcal scalded skin syndrome, bullous impetigo, exfoliative dermatitis, conjunctivitis) clustered in clade F, which included the European epidemic fusidic-acid resistant impetigo clone (EEFIC). In comparison, isolates from deep-seated infections (abscess, furuncle, pyomyositis, necrotizing pneumonia) were disseminated in several clades, but not in clade F. Our results demonstrate that phylogenetic lineages with distinct clinical properties exist within an S. aureus clonal complex, and that SNPs serve as powerful discriminatory markers, able to identify these lineages. All CC121 genomes harboured a 41-kilobase prophage that was dissimilar to S. aureus phages sequenced previously. Community-associated MRSA and MSSA from Cambodia were extremely closely related, suggesting this MRSA arose in the region.

Published

2013

5. Early diagnostic indicators of dengue versus other febrile illnesses in Asia and Latin America (IDAMS study): a multicentre, prospective, observational study

Author

Hasan, Zabir, Wanderley Lopes Gomes, Kilma, Soares Mesquita, Lyvia Patricia, Braga, Cynthia, Castanha, Priscila M.S., Cordeiro, Marli T., Damasceno, Luana, Chuop, Bophal, Ouk, Sonyrath, Sin, Reaksmey, Sun, Sopheary, Alvarez Vera, Mayling, Barahona, Guillermo, Cruz, Bladimir, Beck, Dorothea, Gaczkowski, Roger, Junghanss, Thomas, Morales, Ivonne, Wirths, Marius, Natkunam, Santha Kumari, Ho, Bee Kiau, AbuBakar, Sazaly, Abd-Jamil, Juraina, Syed Omar, Sharifah Faridah, Lizarazo, Erley F., Vincenti-González, María F., Tovar, Robert, Cao Thi, Tam, Dinh Thi Tri, Hong, Huynh Le Anh, Huy, Huynh Thi Le, Duyen, Lai Thi Cong, Thanh, Nguyen Thi Hong, Van, Nguyen Thi My, Linh, Tran Thi Nhu, Thuy, Truong Thi Thu, Thuy, Banh Thi, Nuoi, Huynh Lam Thuy, Trinh, Nguyen Thi Thu, Hiep, Tran Thi Kim, Van, Vo Thanh, Luan, Dang Thi, Bich, Dinh Thi Thu, Huong, Dinh Van, Huy, Nguyen Nguyen, Huyen, Vu Thi Thu, Huong, Rosenberger, Kerstin D, Phung Khanh, Lam, Tobian, Frank, Chanpheaktra, Ngoun, Kumar, Varun, Lum, Lucy Chai See, Sathar, Jameela, Pleités Sandoval, Ernesto, Marón, Gabriela M, Laksono, Ida Safitri, Mahendradhata, Yodi, Sarker, Malabika, Rahman, Ridwanur, Caprara, Andrea, Souza Benevides, Bruno, Marques, Ernesto T A, Magalhaes, Tereza, Brasil, Patrícia, Amaral Calvet, Guilherme, Tami, Adriana, Bethencourt, Sarah E, Dong Thi Hoai, Tam, Nguyen Tan Thanh, Kieu, Tran Van, Ngoc, Nguyen Tran, Nam, Do Chau, Viet, Yacoub, Sophie, Nguyen Van, Kinh, Guzmán, María G, Martinez, Pedro A, Nguyen Than Ha, Quyen, Simmons, Cameron P, Wills, Bridget A, Geskus, Ronald B, and Jaenisch, Thomas

Published

2023

6. Early diagnostic indicators of dengue versus other febrile illnesses in Asia and Latin America (IDAMS study): a multicentre, prospective, observational study

Author

Rosenberger, Kerstin D, primary, Phung Khanh, Lam, additional, Tobian, Frank, additional, Chanpheaktra, Ngoun, additional, Kumar, Varun, additional, Lum, Lucy Chai See, additional, Sathar, Jameela, additional, Pleités Sandoval, Ernesto, additional, Marón, Gabriela M, additional, Laksono, Ida Safitri, additional, Mahendradhata, Yodi, additional, Sarker, Malabika, additional, Rahman, Ridwanur, additional, Caprara, Andrea, additional, Souza Benevides, Bruno, additional, Marques, Ernesto T A, additional, Magalhaes, Tereza, additional, Brasil, Patrícia, additional, Amaral Calvet, Guilherme, additional, Tami, Adriana, additional, Bethencourt, Sarah E, additional, Dong Thi Hoai, Tam, additional, Nguyen Tan Thanh, Kieu, additional, Tran Van, Ngoc, additional, Nguyen Tran, Nam, additional, Do Chau, Viet, additional, Yacoub, Sophie, additional, Nguyen Van, Kinh, additional, Guzmán, María G, additional, Martinez, Pedro A, additional, Nguyen Than Ha, Quyen, additional, Simmons, Cameron P, additional, Wills, Bridget A, additional, Geskus, Ronald B, additional, Jaenisch, Thomas, additional, Hasan, Zabir, additional, Wanderley Lopes Gomes, Kilma, additional, Soares Mesquita, Lyvia Patricia, additional, Braga, Cynthia, additional, Castanha, Priscila M.S., additional, Cordeiro, Marli T., additional, Damasceno, Luana, additional, Chuop, Bophal, additional, Ouk, Sonyrath, additional, Sin, Reaksmey, additional, Sun, Sopheary, additional, Alvarez Vera, Mayling, additional, Barahona, Guillermo, additional, Cruz, Bladimir, additional, Beck, Dorothea, additional, Gaczkowski, Roger, additional, Junghanss, Thomas, additional, Morales, Ivonne, additional, Wirths, Marius, additional, Natkunam, Santha Kumari, additional, Ho, Bee Kiau, additional, AbuBakar, Sazaly, additional, Abd-Jamil, Juraina, additional, Syed Omar, Sharifah Faridah, additional, Lizarazo, Erley F., additional, Vincenti-González, María F., additional, Tovar, Robert, additional, Cao Thi, Tam, additional, Dinh Thi Tri, Hong, additional, Huynh Le Anh, Huy, additional, Huynh Thi Le, Duyen, additional, Lai Thi Cong, Thanh, additional, Nguyen Thi Hong, Van, additional, Nguyen Thi My, Linh, additional, Tran Thi Nhu, Thuy, additional, Truong Thi Thu, Thuy, additional, Banh Thi, Nuoi, additional, Huynh Lam Thuy, Trinh, additional, Nguyen Thi Thu, Hiep, additional, Tran Thi Kim, Van, additional, Vo Thanh, Luan, additional, Dang Thi, Bich, additional, Dinh Thi Thu, Huong, additional, Dinh Van, Huy, additional, Nguyen Nguyen, Huyen, additional, and Vu Thi Thu, Huong, additional

Published

2023

7. Subpopulations of Staphylococcus aureus clonal complex 121 are associated with distinct clinical entities

Author

Christiane Cuny, Richard V. Goering, Silva Holtfreter, Andreas E. Zautner, Kevin Kurt, Barbara M. Bröker, Helena Žemličková, Marc Struelens, Wolfgang Witte, Stephen Ritchie, Jean-Philippe Rasigade, Sharon J. Peacock, Ulrich Nübel, Franziska Layer, Sin Reaksmey, Frédéric Laurent, Direk Limmathurotsakul, Ivana Machova, and Horsburgh, Malcolm James

Subjects

Bacterial Diseases, Epidemiology, lcsh:Medicine, medicine.disease_cause, Bullous impetigo, Exfoliative dermatitis, lcsh:Science, Clade, Phylogeny, Staphylococci, Genetics, 0303 health sciences, Multidisciplinary, Genes, Essential, Phylogenetic tree, Genomics, Staphylococcal Infections, 3. Good health, Bacterial Pathogens, Phenotype, Infectious Diseases, Staphylococcus aureus, Medical Microbiology, Medicine, Research Article, Bacterial Toxins, Biology, Staphylococcal infections, Polymorphism, Single Nucleotide, Microbiology, Infectious Disease Epidemiology, 03 medical and health sciences, CC121, Phylogenetics, medicine, Humans, 030304 developmental biology, Evolutionary Biology, Population Biology, 030306 microbiology, lcsh:R, Comparative Genomics, medicine.disease, Methicillin-resistant Staphylococcus aureus, Microbial Evolution, lcsh:Q, Genome, Bacterial

Abstract

We investigated the population structure of Staphylococcus aureus clonal complex CC121 by mutation discovery at 115 genetic housekeeping loci from each of 154 isolates, sampled on five continents between 1953 and 2009. In addition, we pyro-sequenced the genomes from ten representative isolates. The genome-wide SNPs that were ascertained revealed the evolutionary history of CC121, indicating at least six major clades (A to F) within the clonal complex and dating its most recent common ancestor to the pre-antibiotic era. The toxin gene complement of CC121 isolates was correlated with their SNP-based phylogeny. Moreover, we found a highly significant association of clinical phenotypes with phylogenetic affiliations, which is unusual for S. aureus. All isolates evidently sampled from superficial infections (including staphylococcal scalded skin syndrome, bullous impetigo, exfoliative dermatitis, conjunctivitis) clustered in clade F, which included the European epidemic fusidic-acid resistant impetigo clone (EEFIC). In comparison, isolates from deep-seated infections (abscess, furuncle, pyomyositis, necrotizing pneumonia) were disseminated in several clades, but not in clade F. Our results demonstrate that phylogenetic lineages with distinct clinical properties exist within an S. aureus clonal complex, and that SNPs serve as powerful discriminatory markers, able to identify these lineages. All CC121 genomes harboured a 41-kilobase prophage that was dissimilar to S. aureus phages sequenced previously. Community-associated MRSA and MSSA from Cambodia were extremely closely related, suggesting this MRSA arose in the region. peerReviewed

Published

2013