Charged amino acid variability related to N-glyco -sylation and epitopes in A/H3N2 influenza: Hem -agglutinin and neuraminidase.

Charged amino acid variability related to N-glyco -sylation and epitopes in A/H3N2 influenza: Hem -agglutinin and neuraminidase.

The A/H3N2 influenza viruses circulated in humans have been shown to undergo antigenic drift, a process in which amino acid mutations result from nucleotide substitutions. There are few reports regarding the charged amino acid mutations. The purpose of this paper is to explore the relations between...

Full description

Bibliographic Details
Main Authors: Zhong-Zhou Huang, Liang Yu, Ping Huang, Li-Jun Liang, Qing Guo
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2017-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5510802?pdf=render
id doaj-fddcb40a32774a28be63c83f6295f77a
record_format Article
spelling doaj-fddcb40a32774a28be63c83f6295f77a2020-11-24T20:45:28ZengPublic Library of Science (PLoS)PLoS ONE1932-62032017-01-01127e017823110.1371/journal.pone.0178231Charged amino acid variability related to N-glyco -sylation and epitopes in A/H3N2 influenza: Hem -agglutinin and neuraminidase.Zhong-Zhou HuangLiang YuPing HuangLi-Jun LiangQing GuoThe A/H3N2 influenza viruses circulated in humans have been shown to undergo antigenic drift, a process in which amino acid mutations result from nucleotide substitutions. There are few reports regarding the charged amino acid mutations. The purpose of this paper is to explore the relations between charged amino acids, N-glycosylation and epitopes in hemagglutinin (HA) and neuraminidase (NA).A total of 700 HA genes (691 NA genes) of A/H3N2 viruses were chronologically analyzed for the mutational variants in amino acid features, N-glycosylation sites and epitopes since its emergence in 1968.It was found that both the number of HA N-glycosylation sites and the electric charge of HA increased gradually up to 2016. The charges of HA and HA1 increased respectively 1.54-fold (+7.0 /+17.8) and 1.08-fold (+8.0/+16.6) and the number of NGS in nearly doubled (7/12). As great diversities occurred in 1990s, involving Epitope A, B and D mutations, the charged amino acids in Epitopes A, B, C and D in HA1 mutated at a high frequency in global circulating strains last decade. The charged amino acid mutations in Epitopes A (T135K) has shown high mutability in strains near years, resulting in a decrease of NGT135-135. Both K158N and K160T not only involved mutations charged in epitope B, but also caused a gain of NYT158-160. Epitope B and its adjacent N-glycosylation site NYT158-160 mutated more frequently, which might be under greater immune pressure than the rest.The charged amino acid mutations in A/H3N2 Influenza play a significant role in virus evolution, which might cause an important public health issue. Variability related to both the epitopes (A and B) and N-glycosylation is beneficial for understanding the evolutionary mechanisms, disease pathogenesis and vaccine research.http://europepmc.org/articles/PMC5510802?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Zhong-Zhou Huang
Liang Yu
Ping Huang
Li-Jun Liang
Qing Guo
spellingShingle Zhong-Zhou Huang
Liang Yu
Ping Huang
Li-Jun Liang
Qing Guo
Charged amino acid variability related to N-glyco -sylation and epitopes in A/H3N2 influenza: Hem -agglutinin and neuraminidase.
PLoS ONE
author_facet Zhong-Zhou Huang
Liang Yu
Ping Huang
Li-Jun Liang
Qing Guo
author_sort Zhong-Zhou Huang
title Charged amino acid variability related to N-glyco -sylation and epitopes in A/H3N2 influenza: Hem -agglutinin and neuraminidase.
title_short Charged amino acid variability related to N-glyco -sylation and epitopes in A/H3N2 influenza: Hem -agglutinin and neuraminidase.
title_full Charged amino acid variability related to N-glyco -sylation and epitopes in A/H3N2 influenza: Hem -agglutinin and neuraminidase.
title_fullStr Charged amino acid variability related to N-glyco -sylation and epitopes in A/H3N2 influenza: Hem -agglutinin and neuraminidase.
title_full_unstemmed Charged amino acid variability related to N-glyco -sylation and epitopes in A/H3N2 influenza: Hem -agglutinin and neuraminidase.
title_sort charged amino acid variability related to n-glyco -sylation and epitopes in a/h3n2 influenza: hem -agglutinin and neuraminidase.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2017-01-01
description The A/H3N2 influenza viruses circulated in humans have been shown to undergo antigenic drift, a process in which amino acid mutations result from nucleotide substitutions. There are few reports regarding the charged amino acid mutations. The purpose of this paper is to explore the relations between charged amino acids, N-glycosylation and epitopes in hemagglutinin (HA) and neuraminidase (NA).A total of 700 HA genes (691 NA genes) of A/H3N2 viruses were chronologically analyzed for the mutational variants in amino acid features, N-glycosylation sites and epitopes since its emergence in 1968.It was found that both the number of HA N-glycosylation sites and the electric charge of HA increased gradually up to 2016. The charges of HA and HA1 increased respectively 1.54-fold (+7.0 /+17.8) and 1.08-fold (+8.0/+16.6) and the number of NGS in nearly doubled (7/12). As great diversities occurred in 1990s, involving Epitope A, B and D mutations, the charged amino acids in Epitopes A, B, C and D in HA1 mutated at a high frequency in global circulating strains last decade. The charged amino acid mutations in Epitopes A (T135K) has shown high mutability in strains near years, resulting in a decrease of NGT135-135. Both K158N and K160T not only involved mutations charged in epitope B, but also caused a gain of NYT158-160. Epitope B and its adjacent N-glycosylation site NYT158-160 mutated more frequently, which might be under greater immune pressure than the rest.The charged amino acid mutations in A/H3N2 Influenza play a significant role in virus evolution, which might cause an important public health issue. Variability related to both the epitopes (A and B) and N-glycosylation is beneficial for understanding the evolutionary mechanisms, disease pathogenesis and vaccine research.
url http://europepmc.org/articles/PMC5510802?pdf=render
work_keys_str_mv AT zhongzhouhuang chargedaminoacidvariabilityrelatedtonglycosylationandepitopesinah3n2influenzahemagglutininandneuraminidase
AT liangyu chargedaminoacidvariabilityrelatedtonglycosylationandepitopesinah3n2influenzahemagglutininandneuraminidase
AT pinghuang chargedaminoacidvariabilityrelatedtonglycosylationandepitopesinah3n2influenzahemagglutininandneuraminidase
AT lijunliang chargedaminoacidvariabilityrelatedtonglycosylationandepitopesinah3n2influenzahemagglutininandneuraminidase
AT qingguo chargedaminoacidvariabilityrelatedtonglycosylationandepitopesinah3n2influenzahemagglutininandneuraminidase
_version_ 1716814661321490432

Similar Items