NK cell immunophenotypic and genotypic analysis of infants with severe respiratory syncytial virus infection
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Respiratory syncytial virus (RSV) is the leading cause of severe lower respiratory tract infection in infants. Reduced numbers of NK cells have been reported in infants with severe RSV infection; however, the precise role of NK cells during acute RSV infection is unclear. In this study the NK and T cell phenotypes, LILRB1 gene polymorphisms and KIR genotypes of infants hospitalized with RSV infection were analyzed. Compared to controls, infants with acute RSV infection showed a higher proportion of LILRB1 T cells; in addition, a subgroup of infants with RSV infection showed an increase in LILRB1 NK cells. No differences in NKG2C, NKG2A, or CD161 expression between RSV infected infants and controls were observed. LILRB1 genotype distribution of the rs3760860 A>G, and rs3760861 A>G single nucleotide polymorphisms differed between infants with RSV infection and healthy donors, whereas no differences in any of the KIR genes were observed. Our results suggest that LILRB1 participates in the pathogenesis of RSV infection. Further studies are needed to define the role of LILRB1 NK in response to RSV and to confirm an association between LILRB1 polymorphisms and the risk of severe RSV infection. © 2015 The Societies and Wiley Publishing Asia Pty Ltd.
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Respiratory syncytial virus (RSV) is the leading cause of severe lower respiratory tract infection in infants. Reduced numbers of NK cells have been reported in infants with severe RSV infection; however, the precise role of NK cells during acute RSV infection is unclear. In this study the NK and T cell phenotypes, LILRB1 gene polymorphisms and KIR genotypes of infants hospitalized with RSV infection were analyzed. Compared to controls, infants with acute RSV infection showed a higher proportion of LILRB1%2b T cells; in addition, a subgroup of infants with RSV infection showed an increase in LILRB1%2b NK cells. No differences in NKG2C, NKG2A, or CD161 expression between RSV infected infants and controls were observed. LILRB1 genotype distribution of the rs3760860 A>G, and rs3760861 A>G single nucleotide polymorphisms differed between infants with RSV infection and healthy donors, whereas no differences in any of the KIR genes were observed. Our results suggest that LILRB1 participates in the pathogenesis of RSV infection. Further studies are needed to define the role of LILRB1%2b NK in response to RSV and to confirm an association between LILRB1 polymorphisms and the risk of severe RSV infection. © 2015 The Societies and Wiley Publishing Asia Pty Ltd.
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LILRB1; NK cells; Respiratory syncytial virus; Respiratory tract infection CD161 antigen; killer cell immunoglobulin like receptor; natural killer cell receptor; natural killer cell receptor NKG2A; natural killer cell receptor NKG2C; unclassified drug; immunoglobulin receptor; killer cell immunoglobulin like receptor; leukocyte antigen; LILRB1 protein, human; Article; controlled study; disease severity; female; gene; gene expression; gene frequency; genotyping technique; hospitalized infant; human; immunophenotyping; infant; KIR gene; LILRB1 gene; major clinical study; male; natural killer cell; respiratory syncytial virus infection; single nucleotide polymorphism; genetics; genotype; Human respiratory syncytial virus; immunology; isolation and purification; natural killer cell; physiology; respiratory syncytial virus infection; respiratory tract infection; T lymphocyte; virology; Respiratory syncytial virus; Rice stripe virus; Antigens, CD; Genotype; Humans; Infant; Killer Cells, Natural; Male; Polymorphism, Single Nucleotide; Receptors, Immunologic; Receptors, KIR; Respiratory Syncytial Virus Infections; Respiratory Syncytial Viruses; Respiratory Tract Infections; T-Lymphocytes
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