Upsurge and spread of G3 rotaviruses in Eastern India (2014-2016): Full genome analyses reveals heterogeneity within Wa-like genomic constellation

被引:16
作者
Banerjee, Anindita [1 ]
Lo, Mahadeb [1 ]
Indwar, Pallavi [1 ]
Deb, Alok K. [1 ]
Das, Santasabuj [1 ]
Manna, Byomkesh [1 ]
Dutta, Shanta [1 ]
Bhadra, Uchhal K. [2 ]
Bhattacharya, Mala [3 ]
Okamoto, Keinosuke [4 ]
Chawla-Sarkar, Mamta [1 ]
机构
[1] ICMR NICED, Kolkata 700010, India
[2] Infect Dis & Beliaghata Gen ID&BG Hosp, Kolkata 700010, India
[3] Dr BC Roy Post Grad Inst Pediat Sci, Kolkata 700054, India
[4] Okayama Univ Infect Dis, Indian Council Med Res, Natl Inst Cholera & Enter Dis, Collaborat Res Ctr, Kolkata 700010, India
关键词
Eastern India; Wa-like heterogeneous G3 rotavirus; Whole genome sequencing; Inter-genogroup reassortment; Mutation; HOSPITAL-BASED SURVEILLANCE; CHILDREN LESS-THAN-5 YEARS; MOLECULAR CHARACTERIZATION; SOUTH-INDIA; P GENOTYPES; EQUINE-LIKE; IN-VIVO; DIARRHEA; STRAINS; GASTROENTERITIS;
D O I
10.1016/j.meegid.2018.05.026
中图分类号
R51 [传染病];
学科分类号
100401 ;
摘要
Advent of new strains and shift in predominantly circulating genotypes are characteristics of group- A rotavirus (RVA), one of the major causes of childhood gastroenteritis. During diarrheal disease surveillance at Kolkata, India (2014-2016), a shift in circulating RVA strains from G1P[8] to G3P[8] was seen. Stool samples from children (n = 3048) with acute gastroenteritis were tested of which 38.7% were RVA positive. G1 was the predominant strain (65.3%) in 2014-2015 whereas in late 2015 and 2016, G3 became the preponderant strain (44.6%). In the past decade G3 strains were not observed in this region, we conducted whole genome sequencing of representative strains to gain insight into the phenomenon of emergence and genetic constellation of these circulating human G3 strains. The analyses revealed intergenogroup reassortment in G3P [4] strains (among Wa and DS-1-like genogroup) whereas G3P[8] strains were authentic Wa-like. Phylogenetic analysis revealed Kolkata G3 strains as polymorphic and thus they formed two sub-clusters due to antigenic differences in their VP7 protein. One of the sub-clusters had the wild-type threonine at 87 amino acid position while another subcluster had an isoleucine mutation. Presence of additional N-linked glycosylation site at amino acid 283 of VP7 glycoprotein suggests that the major neutralizing epitope on the VP7 (G3) of RotaTeq vaccine differs from the currently circulating G3 strains. The study is important as efficiency of rotavirus vaccine depends on the circulating heterogeneous genotype constellations. Continuous monitoring of circulating RVA strains in endemic settings like India is therefore important in pre- and post-vaccination period to monitor the emergence of new reassortant genotypes in addition to assessing vaccine efficacy.
引用
收藏
页码:158 / 174
页数:17
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