BACKGROUND: typhoid fever remains a public health problem in Vietnam, with a significant burden in the Mekong River delta region. Typhoid fever is caused by the bacterial pathogen Salmonella enterica serovar Typhi (S. Typhi), which is frequently multidrug resistant with reduced susceptibility to fluoroquinolone-based drugs, the first choice for the treatment of typhoid fever. We used a GoldenGate (Illumina) assay to type 1,500 single nucleotide polymorphisms (SNPs) and analyse the genetic variation of S. Typhi isolated from 267 typhoid fever patients in the Mekong delta region participating in a randomized trial conducted between 2004 and 2005. PRINCIPAL FINDINGS: the population of S. Typhi circulating during the study was highly clonal, with 91% of isolates belonging to a single clonal complex of the S. Typhi H58 haplogroup. The patterns of disease were consistent with the presence of an endemic haplotype H58-C and a localised outbreak of S. Typhi haplotype H58-E2 in 2004. H58-E2-associated typhoid fever cases exhibited evidence of significant geo-spatial clustering along the Sông H u branch of the Mekong River. Multidrug resistance was common in the established clone H58-C but not in the outbreak clone H58-E2, however all H58 S. Typhi were nalidixic acid resistant and carried a Ser83Phe amino acid substitution in the gyrA gene. SIGNIFICANCE: the H58 haplogroup dominates S. Typhi populations in other endemic areas, but the population described here was more homogeneous than previously examined populations, and the dominant clonal complex (H58-C, -E1, -E2) observed in this study has not been detected outside Vietnam. IncHI1 plasmid-bearing S. Typhi H58-C was endemic during the study period whilst H58-E2, which rarely carried the plasmid, was only transient, suggesting a selective advantage for the plasmid. These data add insight into the outbreak dynamics and local molecular epidemiology of S. Typhi in southern Vietnam.
展开▼
机译:背景:伤寒一直是越南的公共卫生问题,在湄公河三角洲地区是一个沉重的负担。伤寒是由细菌性病原肠小肠沙门氏菌(伤寒沙门氏菌)引起的,它通常是多药耐药的,对氟喹诺酮类药物的敏感性降低,氟喹诺酮类药物是治疗伤寒的首选药物。我们使用GoldenGate(Illumina)分析方法对1,500个单核苷酸多态性(SNP)进行了分析,并分析了参与湄公河三角洲地区267例伤寒患者的伤寒沙门氏菌的遗传变异,该患者参加了2004年至2005年进行的一项随机试验。 :在研究期间流通的鼠伤寒沙门氏菌种群是高度克隆的,其中91%的分离株属于鼠伤寒沙门氏菌H58单倍体的单个克隆复合体。疾病的模式与地方性单倍型H58-C的存在和鼠伤寒沙门氏菌单倍型H58-E2在2004年的局部爆发相一致。与H58-E2相关的伤寒病例显示出沿Söng有明显地理空间聚集的证据湄公河的u支。在已建立的克隆H58-C中普遍存在多药耐药性,但在暴发克隆H58-E2中则不常见,但是所有H58 S. Typhi均对萘啶酸具有耐药性,并在gyrA基因中带有Ser83Phe氨基酸取代。重要性:H58单倍体在其他地方性流行地区占伤寒沙门氏菌种群,但此处描述的种群比以前检查的种群更均一,本研究中观察到的优势克隆复合体(H58-C,-E1,-E2)尚未发现在越南以外被发现。在研究期间,携带IncHI1质粒的伤寒沙门氏菌H58-C是地方病,而很少携带该质粒的H58-E2仅是瞬时的,表明该质粒具有选择性优势。这些数据为越南南部的伤寒沙门氏菌的爆发动态和局部分子流行病学提供了见识。
展开▼
