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猿猴病毒40的小窝蛋白介导的内吞作用之后是对布雷菲德菌素A敏感的向内质网的转运,病毒在内质网中解体。

Caveolar endocytosis of simian virus 40 is followed by brefeldin A-sensitive transport to the endoplasmic reticulum, where the virus disassembles.

作者信息

Norkin Leonard C, Anderson Howard A, Wolfrom Scott A, Oppenheim Ariella

机构信息

Department of Microbiology, University of Massachusetts, Amherst, Massachusetts 01003-5720, USA.

出版信息

J Virol. 2002 May;76(10):5156-66. doi: 10.1128/jvi.76.10.5156-5166.2002.

Abstract

Simian virus 40 (SV40) enters cells by atypical endocytosis mediated by caveolae that transports the virus to the endoplasmic reticulum (ER) instead of to the endosomal-lysosomal compartment, which is the usual destination for viruses and other cargo that enter by endocytosis. We show here that SV4O is transported to the ER via an intermediate compartment that contains beta-COP, which is best known as a component of the COPI coatamer complexes that are required for the retrograde retrieval pathway from the Golgi to the ER. Additionally, transport of SV40 to the ER, as well as infection, is sensitive to brefeldin A. This drug acts by specifically inhibiting the ARF1 GTPase, which is known to regulate assembly of COPI coat complexes on Golgi cisternae. Moreover, some beta-COP colocalizes with intracellular caveolin-1, which was previously shown to be present on a new organelle (termed the caveosome) that is an intermediate in the transport of SV40 to the ER (L. Pelkmans, J. Kartenbeck, and A. Helenius, Nat. Cell Biol. 3:473-483, 2001). We also show that the internal SV40 capsid proteins VP2 and VP3 become accessible to immunostaining starting at about 5 h. Most of that immunostaining overlays the ER, with some appearing outside of the ER. In contrast, immunostaining with anti-SV40 antisera remains confined to the ER.

摘要

猴病毒40(SV40)通过小窝介导的非典型内吞作用进入细胞,这种作用将病毒转运至内质网(ER),而非通常内吞作用进入细胞的病毒及其他物质所到达的内体-溶酶体区室。我们在此表明,SV40通过一个包含β-COP的中间区室转运至内质网,β-COP最为人所知的是作为COPI衣被蛋白复合物的一个组分,而该复合物是从高尔基体到内质网的逆行回收途径所必需的。此外,SV40向内质网的转运以及感染对布雷菲德菌素A敏感。这种药物通过特异性抑制ARF1 GTP酶起作用,已知该酶可调节高尔基体潴泡上COPI衣被复合物的组装。而且,一些β-COP与细胞内小窝蛋白-1共定位,先前已表明小窝蛋白-1存在于一个新细胞器(称为小窝体)上,该细胞器是SV40转运至内质网过程中的一个中间体(L. 佩尔克曼斯、J. 卡尔滕贝克和A. 海伦尼乌斯,《自然细胞生物学》3:473 - 483,2001)。我们还表明,从大约5小时开始,内部SV40衣壳蛋白VP2和VP3可被免疫染色检测到。大部分免疫染色覆盖内质网,有些出现在内质网之外。相比之下,用抗SV40抗血清进行的免疫染色仍局限于内质网。

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