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Low Polymerase Activity Attributed to PA Drives the Acquisition of the PB2 E627K Mutation of H7N9 Avian Influenza Virus in Mammals.

MBio. 2019-06; 
LiangLibin,JiangLi,LiJunping,ZhaoQingqing,WangJinguang,HeXijun,HuangShanyu,WangQian,ZhaoYuhui,WangGuangwen,SunNan,DengGuohua,ShiJianzhong,TianGuobin,ZengXianying,JiangYongping,LiuLiling,LiuJinxiong,ChenPucheng,BuZhigao,KawaokaYoshihiro,ChenHualan,LiChen
Products/Services Used Details Operation
Catalog Antibody The following primary antibodies were purchased from commercial sources: rabbit anti-PB2 polyclonal antibody (PAb) (GeneTex), rabbit anti-PB1 PAb (GeneTex), rabbit anti-PA PAb (GeneTex), rabbit anti-ANP32A monoclonal antibody (MAb) (Cell Signaling Technology), rabbit antiGAPDH PAb (Proteintech), mouse anti-actin MAb (Santa Cruz), and mouse anti-GST MAb (GenScript Biotech). The secondary antibodies DyLight 800 goat anti-mouse IgG(H L) and DyLight 800 goat anti-rabbit IgG(H L) (KPL) were used for Western blotting. Get A Quote

摘要

Avian influenza viruses (AIVs) must acquire mammalian-adaptive mutations before they can efficiently replicate in and transmit among humans. The PB2 E627K mutation is known to play a prominent role in the mammalian adaptation of AIVs. The H7N9 AIVs that emerged in 2013 in China easily acquired the PB2 E627K mutation upon replication in humans. Here, we generate a series of reassortant or mutant H7N9 AIVs and test them in mice. We show that the low polymerase activity attributed to the viral PA protein is the intrinsic driving force behind the emergence of PB2 E627K during H7N9 AIV replication in mice. Four residues in the N-terminal region of PA are critical in mediating the PB2 E627K acquisition. Notably, ... More

关键词

ANP32A,H7N9,PB2 E627K mutation,avian influenza virus,viral PA protein,viral adaptation in mammals,viral polyme