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重组脊髓灰质炎病毒2C和2BC在人细胞中引起的膜重排和囊泡诱导

Membrane rearrangement and vesicle induction by recombinant poliovirus 2C and 2BC in human cells.

作者信息

Cho M W, Teterina N, Egger D, Bienz K, Ehrenfeld E

机构信息

Department of Molecular Biology and Biochemistry, University of California at Irvine 92717.

出版信息

Virology. 1994 Jul;202(1):129-45. doi: 10.1006/viro.1994.1329.

Abstract

Poliovirus (PV)-infected cells undergo extensive proliferation and rearrangement of intracellular smooth membranes to generate vesicles on which viral RNA replication occurs. PV proteins 2C and 2BC are known to be tightly associated with these membranous replication complexes and have been proposed to be involved in the formation of these virus-induced vesicles. We have expressed these proteins, and proteins with mutations in the putative nucleotide (NTP) binding motifs, in human cells using recombinant vaccinia viruses and T7 RNA polymerase-directed transcription. To ascertain the subcellular localization properties of these proteins in the absence of other PV proteins and to determine whether they induced ultrastructural changes, cells expressing 2C and 2BC proteins were examined by immunofluorescence (IF) microscopy, electron microscopy (EM), and immuno-EM (IEM). The cytoplasm of cells expressing either 2C or 2BC exhibited vesicles of 50-350 nm in diameter, which resembled those found in PV-infected cells. Both 2C and 2BC were associated with these vesicles. Mutations in the putative NTP binding motif did not affect vesicle induction by 2C or 2BC. Despite the membrane reorganization and vesicle formation induced by 2C and 2BC proteins, no enhanced synthesis of lipid was observed. Guanidine hydrochloride at a concentration that inhibits PV replication, did not have significant effects on the IF patterns of either 2C or 2BC. An additional prominent alteration in cells expressing 2C, but not 2BC, was the formation of extensive tubular membrane structures with a myelin-like arrangement in the lumen of the rough endoplasmic reticulum. IEM analyses showed that 2C was associated with these structures. In the presence of other PV proteins, the tubular membrane structures induced by 2C were not detected. These structures are not observed in poliovirus-infected cells, but likely indicate a novel property of 2C that induces a complex interaction with intracellular membranes.

摘要

脊髓灰质炎病毒(PV)感染的细胞会经历细胞内光滑膜的广泛增殖和重排,以产生病毒RNA复制发生的囊泡。已知PV蛋白2C和2BC与这些膜性复制复合物紧密相关,并被认为参与了这些病毒诱导囊泡的形成。我们利用重组痘苗病毒和T7 RNA聚合酶指导的转录,在人细胞中表达了这些蛋白以及在假定的核苷酸(NTP)结合基序中具有突变的蛋白。为了确定这些蛋白在没有其他PV蛋白情况下的亚细胞定位特性,并确定它们是否诱导超微结构变化,通过免疫荧光(IF)显微镜、电子显微镜(EM)和免疫电子显微镜(IEM)检查了表达2C和2BC蛋白的细胞。表达2C或2BC的细胞的细胞质中呈现出直径为50 - 350 nm的囊泡,这些囊泡与在PV感染细胞中发现的囊泡相似。2C和2BC都与这些囊泡相关。假定的NTP结合基序中的突变并不影响2C或2BC诱导囊泡的形成。尽管2C和2BC蛋白诱导了膜重排和囊泡形成,但未观察到脂质合成增强。抑制PV复制的盐酸胍浓度对2C或2BC的IF模式没有显著影响。在表达2C而非2BC的细胞中,另一个显著变化是在粗面内质网腔内形成了具有髓鞘样排列结构的广泛管状膜结构。IEM分析表明2C与这些结构相关。在存在其他PV蛋白的情况下,未检测到由2C诱导的管状膜结构。这些结构在脊髓灰质炎病毒感染的细胞中未观察到,但可能表明2C具有一种与细胞内膜诱导复杂相互作用的新特性。

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