AVM

Mutation site	A63V
Virus	Human respiratory syncytial virus
Mutation level	Amino acid Level
Gene/protein/region type	G
Gene ID	1494474
Country	USA
Mutation type	nonsynonymous mutation
Genotype/subtype/clade	-
Sample	cell line
Variants	-
Viral reference sequence	KF713490.1
Drug/antibody/vaccine	Benzimidazole analogs
Transmissibility	-
Transmission mechanism	-
Pathogenicity	-
Pathogenicity mechanism	-
Immune escape mutation	-
Immune escape mechanism	-
RT-PCR primers probes	-

Protein name	Attachment glycoprotein
Uniprot protein ID	P03423
Protein length	298 amino acids
Protein description	G protein is another target for neutralizing antibodies and it is a type II integral membrane protein composed of 298AA and weights ~ 90 kDa. It is vastly glycosylated and it is expressed in secreted and membrane-anchored forms called Gs and Gm, respectively. Gs is linked to neutralization inhibition, while Gm is related to viral attachment. This hostvirus membrane attachment is mediated by heparin sulfate proteoglycans receptor interaction. The antigenic variation is situated in the mucin domain of G protein at both C- and N- terminal ends. N- and O-glycosylation enables the protein to mature and enhances immune escape mechanisms. Other feature includes a central conserved region (CX3C motif) which is responsible for CX3CR1 binding to diminish inflammatory cytokines release.

Pubmed ID	26116756
Clinical information	No
Disease	-
Published year	2015
Journal	Antiviral Research
Title	Benzimidazole analogs inhibit respiratory syncytial virus G protein function
Author	Carrie W. Evans,Colm Atkins,Ashish Pathak,Brian E. Gilbert,James W. Noah
Evidence	The mutation (A63V) occurs in the N-terminal region of the G protein within the transmembrane domain. Fig.3D shows the extended amino acid sequence of the transmembrane domain surrounding the point mutation. The region containing the mutation is conserved