Abstract

Respiratory syncytial virus (RSV) is a major cause of acute respiratory infections (ARIs) in children worldwide and can cause high mortality, especially in developing countries. However, information on the clinical and molecular characteristics of RSV infection in developing countries is limited. From April 2010 to May 2011, 1,082 nasopharyngeal swabs were collected from children with ARI admitted to the Children's Hospital 2, Ho Chi Minh City, Vietnam. Samples were screened for RSV and genotyped by reverse transcription-PCR and sequencing. Demographic and clinical data was also recorded. RSV was found in 23.8% (257/1,082) of samples. RSV A was the dominant subgroup, accounting for 91.4% (235/257), followed by RSV B, 5.1% (13/257), and 9 cases (3.5%) were mixed infection of these subgroups. The phylogenetic analysis revealed that all group A strains belonged to the GA2 genotype. All group B strains belonged to the recently identified BA genotype, and further clustered into 2 recently described subgenotypes BA9 and BA10. One GA2 genotype strain had a premature stop codon which shortened the G protein length. RSV infection was significantly associated with younger age and higher severity score than those without. Co-infection with other viruses did not affect disease severity. RSV A caused more severe disease than RSV B. The results from this study will not only contribute to the growing database on the molecular diversity of RSV circulating worldwide but may be also useful in clinical management and vaccine development.

Highlights

  • Respiratory syncytial virus (RSV) is the major cause of acute respiratory infections (ARIs) among infants and young children worldwide [1]

  • The clinical presentations can vary from mild upper respiratory tract infections (URTIs) to life threatening bronchiolitis and pneumonia which result in significant pediatric hospitalization and economic burden [2]

  • The aims of this study were to investigate the molecular epidemiology of RSV infections, as well as to compare the clinical characteristics of diseases caused by group A and B strains in hospitalized children in Ho Chi Minh City, Vietnam

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Summary

Introduction

Respiratory syncytial virus (RSV) is the major cause of acute respiratory infections (ARIs) among infants and young children worldwide [1]. RSV can cause re-infections throughout life with milder disease, indicating that either RSV infection induces an inadequate immune response or genetic variability of RSV is extensive [4]. RSV is divided into two major groups, A and B, initially based on the reaction of the virus with monoclonal antibodies against the major structural glycoproteins G and F [5] and later by genetic analysis [6]. The attachment glycoprotein G is the most divergent viral protein, both between and within the two groups, and a major target for neutralizing and protective antibody responses [7]

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