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单系登革热病毒2型群体内的临床结果和基因差异

Clinical outcome and genetic differences within a monophyletic Dengue virus type 2 population.

作者信息

Hapuarachchi Hapuarachchige Chanditha, Chua Rachel Choon Rong, Shi Yuan, Thein Tun Lin, Lee Linda Kay, Lee Kim Sung, Lye David Chien, Ng Lee Ching, Leo Yee Sin

机构信息

Environmental Health Institute, National Environment Agency, 11 Biopolis Way, #06-05-08, Singapore 138667.

Institute of Infectious Diseases and Epidemiology, Tan Tock Seng Hospital, 11 Jalan Tan Tock Seng, Singapore 308433.

出版信息

PLoS One. 2015 Mar 26;10(3):e0121696. doi: 10.1371/journal.pone.0121696. eCollection 2015.

Abstract

The exact mechanisms of interplay between host and viral factors leading to severe dengue are yet to be fully understood. Even though previous studies have implicated specific genetic differences of Dengue virus (DENV) in clinical severity and virus attenuation, similar studies with large-scale, whole genome screening of monophyletic virus populations are limited. Therefore, in the present study, we compared 89 whole genomes of DENV-2 cosmopolitan clade III isolates obtained from patients diagnosed with dengue fever (DF, n = 58), dengue hemorrhagic fever (DHF, n = 30) and dengue shock syndrome (DSS, n = 1) in Singapore between July 2010 and January 2013, in order to determine the correlation of observed viral genetic differences with clinical outcomes. Our findings showed no significant difference between the number of primary and secondary infections that progressed to DHF and DSS (p>0.05) in our study cohort. Despite being highly homogenous, study isolates possessed 39 amino acid substitutions of which 10 substitutions were fixed in three main groups of virus isolates. None of those substitutions were specifically associated with DHF and DSS. Notably, two evolutionarily unique virus groups possessing C-P43T+NS1-S103T+NS2A-V83I+NS3-R337K+ NS3-I600T+ NS5-P136S and NS2A-T119N mutations were exclusively found in patients with DF, the benign form of DENV infections. Those mutants were significantly associated with mild disease outcome. These observations indicated that disease progression into DHF and DSS within our patient population was more likely to be due to host than virus factors. We hypothesize that selection for potentially less virulent groups of DENV-2 in our study cohort may be an evolutionary adaptation of viral strains to extend their survival in the human-mosquito transmission cycle.

摘要

导致严重登革热的宿主与病毒因素之间相互作用的确切机制尚未完全明了。尽管先前的研究表明登革病毒(DENV)的特定基因差异与临床严重程度及病毒减毒有关,但针对单系病毒群体进行大规模全基因组筛查的类似研究却很有限。因此,在本研究中,我们比较了2010年7月至2013年1月期间从新加坡诊断为登革热(DF,n = 58)、登革出血热(DHF,n = 30)和登革休克综合征(DSS,n = 1)的患者中获得的89个DENV-2泛热带分支III分离株的全基因组,以确定观察到的病毒基因差异与临床结果之间的相关性。我们的研究结果显示,在我们的研究队列中,进展为DHF和DSS的初次感染和二次感染数量之间没有显著差异(p>0.05)。尽管研究分离株高度同源,但它们有39个氨基酸替换,其中10个替换在三个主要病毒分离株组中是固定的。这些替换中没有一个与DHF和DSS有特异性关联。值得注意的是,两个具有进化独特性的病毒组,分别具有C-P43T+NS1-S103T+NS2A-V83I+NS3-R337K+ NS3-I600T+ NS5-P136S和NS2A-T119N突变,仅在DF患者(DENV感染的良性形式)中发现。这些突变体与轻症疾病结果显著相关。这些观察结果表明,在我们的患者群体中,疾病进展为DHF和DSS更可能是由于宿主因素而非病毒因素。我们推测,在我们的研究队列中选择潜在毒性较低的DENV-2病毒组可能是病毒株的一种进化适应,以延长它们在人蚊传播循环中的生存时间。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f0f0/4374945/a84e5848ece7/pone.0121696.g001.jpg

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