Literature DB >> 12867649

Subgroup C avian metapneumovirus (MPV) and the recently isolated human MPV exhibit a common organization but have extensive sequence divergence in their putative SH and G genes.

D Toquin1, C de Boisseson2, V Beven2, D A Senne3, N Eterradossi1.   

Abstract

The genes encoding the putative small hydrophobic (SH), attachment (G) and polymerase (L) proteins of the Colorado isolate of subgroup C avian pneumovirus (APV) were entirely or partially sequenced. They all included metapneumovirus (MPV)-like gene start and gene end sequences. The deduced Colorado SH protein shared 26.9 and 21.7 % aa identity with its counterpart in human MPV (hMPV) and APV subgroup A, respectively, but its only significant aa similarities were to hMPV. Conserved features included a common hydrophobicity profile with an unique transmembrane domain and the conservation of most extracellular cysteine residues. The Colorado putative G gene encoded several ORFs, the longer of which encoded a 252 aa long type II glycoprotein with aa similarities to hMPV G only (20.6 % overall aa identity with seven conserved N-terminal residues). The putative Colorado G protein shared, at best, 21.0 % aa identity with its counterparts in the other APV subgroups and did not contain the extracellular cysteine residues and short aa stretch highly conserved in other APVs. The N-terminal end of the Colorado L protein exhibited 73.6 and 54.9 % aa identity with hMPV and APV subgroup A, respectively, with four aa blocks highly conserved among Pneumovirus: Phylogenetic analysis performed on the nt sequences confirmed that the L sequences from MPVs were genetically related, whereas analysis of the G sequences revealed that among MPVs, only APV subgroups A, B and D clustered together, independently of both the Colorado isolate and hMPV, which shared weak genetic relatedness at the G gene level.

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Year:  2003        PMID: 12867649     DOI: 10.1099/vir.0.19043-0

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


  13 in total

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Authors:  D Toquin; O Guionie; V Jestin; F Zwingelstein; C Allee; N Eterradossi
Journal:  Virus Genes       Date:  2006-02       Impact factor: 2.332

3.  Recovery of avian metapneumovirus subgroup C from cDNA: cross-recognition of avian and human metapneumovirus support proteins.

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Journal:  J Virol       Date:  2006-06       Impact factor: 5.103

4.  An S101P substitution in the putative cleavage motif of the human metapneumovirus fusion protein is a major determinant for trypsin-independent growth in vero cells and does not alter tissue tropism in hamsters.

Authors:  Jeanne H Schickli; Jasmine Kaur; Nancy Ulbrandt; Richard R Spaete; Roderick S Tang
Journal:  J Virol       Date:  2005-08       Impact factor: 5.103

5.  Expression of recombinant small hydrophobic protein for serospecific detection of avian pneumovirus subgroup C.

Authors:  Lizhong Luo; Marta I Sabara; Yan Li
Journal:  Clin Diagn Lab Immunol       Date:  2005-01

6.  Human metapneumovirus G protein is highly conserved within but not between genetic lineages.

Authors:  Chin-Fen Yang; Chiaoyin K Wang; Sharon J Tollefson; Linda D Lintao; Alexis Liem; Marla Chu; John V Williams
Journal:  Arch Virol       Date:  2013-02-06       Impact factor: 2.574

7.  Isolation and characterization of a subtype C avian metapneumovirus circulating in Muscovy ducks in China.

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8.  Genetic diversity and evolution of human metapneumovirus fusion protein over twenty years.

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9.  Glycoprotein gene truncation in avian metapneumovirus subtype C isolates from the United States.

Authors:  Binu T Velayudhan; Qingzhong Yu; Carlos N Estevez; Kakambi V Nagaraja; David A Halvorson
Journal:  Virus Genes       Date:  2008-07-29       Impact factor: 2.332

10.  Molecular comparisons of full length metapneumovirus (MPV) genomes, including newly determined French AMPV-C and -D isolates, further supports possible subclassification within the MPV Genus.

Authors:  Paul A Brown; Evelyne Lemaitre; François-Xavier Briand; Céline Courtillon; Olivier Guionie; Chantal Allée; Didier Toquin; Marie-Hélène Bayon-Auboyer; Véronique Jestin; Nicolas Eterradossi
Journal:  PLoS One       Date:  2014-07-18       Impact factor: 3.240

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