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痘苗病毒穿透蛋白的鉴定

Identification of a vaccinia virus penetration protein.

作者信息

Ichihashi Y, Takahashi T, Oie M

机构信息

Department of Virology, Faculty of Medicine, Niigata University, Japan.

出版信息

Virology. 1994 Aug 1;202(2):834-43. doi: 10.1006/viro.1994.1405.

Abstract

A vaccinia virus structural protein responsible for infection was identified by monoclonal antibodies (mAb). Two mAbs (2D5 and 8C2) neutralized the virus at a dilution of about 10(5). The 2D5 mAb reacted with VP29K under standard immunoblotting conditions and with a 23-kDa protein when virus was dissociated under nonreducing conditions. The 8C2 mAb reacted with the 23-kDa protein, but not with VP29K. Two-dimensional electrophoresis demonstrated that the 23-kDa protein was the nonreduced form of VP29K. Since they possess the same N-terminal amino acid sequence, the protein was renamed VP23-29K. The gene that encoded it was HindIII A17L ORF. The VP23-29K-dependent process of infection did not occur during the adsorption phase at 4 degrees, and trypsin-treated virus could complete the process within 10 min at 37 degrees. One half of the trypsin-treated intracellular mature virus (IMV) achieved the process within 20 min, but for normal IMV this time period was 2 hr. VP23-29K had function for the early step of penetration, and the functional site in the nonreduced 23-kDa form was masked to some extent in normal virus. The late cell fusion by the fusion positive (F+) D1 mutant proceeded in neutral pH. Cells infected with F- IHD-J strain virus did not fuse, but a short treatment with pH 5 medium developed cell fusion. Both of the cell fusions were inhibited by the 2D5 and 8C2 mAbs. Virion VP23-29K was suggested to be the fusion protein for the early penetration and the late cell fusion phases of vaccinia infection cycle.

摘要

通过单克隆抗体(mAb)鉴定出一种负责感染的痘苗病毒结构蛋白。两种单克隆抗体(2D5和8C2)在约10⁵的稀释度下中和病毒。2D5单克隆抗体在标准免疫印迹条件下与VP29K反应,在非还原条件下使病毒解离时与一种23 kDa的蛋白质反应。8C2单克隆抗体与23 kDa的蛋白质反应,但不与VP29K反应。二维电泳表明,23 kDa的蛋白质是VP29K的非还原形式。由于它们具有相同的N端氨基酸序列,该蛋白质被重新命名为VP23 - 29K。编码它的基因是HindIII A17L开放阅读框。依赖VP23 - 29K的感染过程在4℃吸附阶段不发生,经胰蛋白酶处理的病毒在37℃下10分钟内可完成该过程。一半经胰蛋白酶处理的细胞内成熟病毒(IMV)在20分钟内可完成该过程,但正常IMV则需要2小时。VP23 - 29K在穿透的早期步骤中起作用,正常病毒中未还原的23 kDa形式的功能位点在一定程度上被掩盖。融合阳性(F +)D1突变体的晚期细胞融合在中性pH下进行。感染F - IHD - J株病毒的细胞不融合,但用pH 5培养基短暂处理可诱导细胞融合。两种细胞融合均被2D5和8C2单克隆抗体抑制。病毒粒子VP23 - 29K被认为是痘苗感染周期早期穿透和晚期细胞融合阶段的融合蛋白。

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