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地方性鼻肿瘤病毒包膜需要非常酸性的pH值来激活融合和感染。

Enzootic nasal tumor virus envelope requires a very acidic pH for fusion activation and infection.

作者信息

Côté Marceline, Kucharski Thomas J, Liu Shan-Lu

机构信息

Department of Microbiology and Immunology, McGill University, Montreal, Quebec H3A 2B4, Canada.

出版信息

J Virol. 2008 Sep;82(18):9023-34. doi: 10.1128/JVI.00648-08. Epub 2008 Jul 16.

Abstract

Enzootic nasal tumor virus (ENTV) is a close relative of jaagsiekte sheep retrovirus (JSRV), and the two viruses use the same receptor, hyaluronidase 2 (Hyal2), for cell entry. We report here that, unlike the JSRV envelope (Env) protein, the ENTV Env protein does not induce cell fusion at pHs of 5.0 and above but requires a much lower pH (4.0 to 4.5) for fusion to occur. The entry of ENTV Env pseudovirions was substantially inhibited by bafilomycin A1 (BafA1) but was surprisingly enhanced by lysosomotropic agents and lysosomal protease inhibitors following a 4- to 6-h treatment period; of note, prolonged treatment with BafA1 or ammonium chloride completely blocked ENTV entry. Unlike typical pH-dependent viruses, ENTV Env pseudovirions were virtually resistant to inactivation at a low pH (4.5 or 5.0). Using chimeras formed from ENTV and JSRV Env proteins, we demonstrated that the transmembrane (TM) subunit of ENTV Env is primarily responsible for its unusually low pH requirement for fusion but found that the surface (SU) subunit of ENTV Env also critically influences its relatively low and pH-dependent fusion activity. Furthermore, the poor infectivity of ENTV pseudovirions in human cells was significantly improved by either replacing the SU subunit of ENTV Env with that of JSRV Env or overexpressing the functional Hyal2 receptor in target cells, suggesting that ENTV SU-Hyal2 interaction is likely to be the limiting step for viral infectivity. Collectively, our data reveal that the fusogenicity of ENTV Env is intrinsically lower than that of JSRV Env and that ENTV requires a more acidic pH for fusion, which may occur in an intracellular compartment(s) distinct from that used by JSRV.

摘要

地方性鼻肿瘤病毒(ENTV)是绵羊肺腺瘤逆转录病毒(JSRV)的近亲,这两种病毒利用相同的受体——透明质酸酶2(Hyal2)进入细胞。我们在此报告,与JSRV包膜(Env)蛋白不同,ENTV Env蛋白在pH值为5.0及以上时不会诱导细胞融合,但需要低得多的pH值(4.0至4.5)才能发生融合。巴弗洛霉素A1(BafA1)可显著抑制ENTV Env假病毒颗粒的进入,但令人惊讶的是,在4至6小时的处理期后,溶酶体促渗剂和溶酶体蛋白酶抑制剂可增强其进入;值得注意的是,用BafA1或氯化铵进行长时间处理会完全阻断ENTV的进入。与典型的pH依赖性病毒不同,ENTV Env假病毒颗粒在低pH值(4.5或5.0)下几乎对失活具有抗性。利用由ENTV和JSRV Env蛋白形成的嵌合体,我们证明ENTV Env的跨膜(TM)亚基主要负责其异常低的融合pH值要求,但发现ENTV Env的表面(SU)亚基也对其相对较低的pH依赖性融合活性有至关重要的影响。此外,通过用JSRV Env的SU亚基替换ENTV Env的SU亚基或在靶细胞中过表达功能性Hyal2受体,可显著提高ENTV假病毒颗粒在人细胞中的感染性,这表明ENTV SU-Hyal2相互作用可能是病毒感染性的限制步骤。总体而言,我们的数据表明,ENTV Env的融合性本质上低于JSRV Env,并且ENTV需要更酸性的pH值进行融合,这可能发生在与JSRV不同的细胞内区室中。

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