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Literature DB >> 26407694

Direct whole-genome deep-sequencing of human respiratory syncytial virus A and B from Vietnamese children identifies distinct patterns of inter- and intra-host evolution.

Lien Anh Ha Do¹, Andreas Wilm², H Rogier van Doorn^1,3, Ha Minh Lam¹, Shuzhen Sim², Rashmi Sukumaran², Anh Tuan Tran⁴, Bach Hue Nguyen⁴, Thi Thu Loan Tran⁵, Quynh Huong Tran⁵, Quoc Bao Vo⁵, Nguyen Anh Tran Dac⁵, Hong Nhien Trinh⁴, Thi Thanh Hai Nguyen⁴, Bao Tinh Le Binh⁴, Khanh Le⁴, Minh Tien Nguyen⁴, Quang Tung Thai⁴, Thanh Vu Vo⁴, Ngoc Quang Minh Ngo⁴, Thi Kim Huyen Dang⁵, Ngoc Huong Cao⁵, Thu Van Tran⁵, Lu Viet Ho⁵, Jeremy Farrar¹, Menno de Jong^1,3,6, Swaine Chen², Niranjan Nagarajan², Juliet E Bryant^1,3, Martin L Hibberd².

Abstract

Human respiratory syncytial virus (RSV) is the major cause of lower respiratory tract infections in children ,2 years of age. Little is known about RSV intra-host genetic diversity over the course of infection or about the immune pressures that drive RSV molecular evolution. We performed whole-genome deep-sequencing on 53 RSV-positive samples (37 RSV subgroup A and 16 RSV subgroup B) collected from the upper airways of hospitalized children in southern Vietnam over two consecutive seasons. RSV A NA1 and RSV B BA9 were the predominant genotypes found in our samples, consistent with other reports on global RSV circulation during the same period. For both RSV A and B, the M gene was the most conserved, confirming its potential as a target for novel therapeutics. The G gene was the most variable and was the only gene under detectable positive selection. Further, positively selected sites inG were found in close proximity to and in some cases overlapped with predicted glycosylation motifs, suggesting that selection on amino acid glycosylation may drive viral genetic diversity. We further identified hotspots and coldspots of intra-host genetic diversity in the RSV genome, some of which may highlight previously unknown regions of functional importance.

Entities: Chemical Disease Species

Mesh：

Substances：
Viral Proteins

Year: 2015 PMID： 26407694 PMCID： PMC4804761 DOI： 10.1099/jgv.0.000298

Source DB: PubMed Journal: J Gen Virol ISSN： 0022-1317 Impact factor: 3.891

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