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传染性胃肠炎病毒发病机制的遗传基础。

Genetic basis for the pathogenesis of transmissible gastroenteritis virus.

作者信息

Wesley R D, Woods R D, Cheung A K

机构信息

National Animal Disease Center, U.S. Department of Agriculture, Ames, Iowa 50010.

出版信息

J Virol. 1990 Oct;64(10):4761-6. doi: 10.1128/JVI.64.10.4761-4766.1990.

Abstract

Intracellular RNAs of an avirulent small-plaque (SP) transmissible gastroenteritis virus variant and the parent virulent Miller strain of transmissible gastroenteritis virus were compared. Northern RNA blotting showed that the Miller strain contained eight intracellular RNA species. RNAs 1, 2(S), 5, 6(M), 7(N), and 8 were similar in size for both viruses; however, the SP variant lacked subgenomic RNAs 3 and 4. Instead, the SP virus contained an altered RNA species (delta 4) that was slightly smaller than RNA 4. S1 nuclease protection experiments showed a deletion of approximately 450 nucleotides in the SP genome downstream of the peplomer S gene. Sequencing of cDNA clones confirmed that SP virus contained a 462-nucleotide deletion, eliminating the transcriptional recognition sequences for both RNAs 3 and 4. These RNAs encode open reading frames A and B, respectively. An alternative consensus recognition sequence was not readily apparent for the delta 4 RNA species of SP virus. Since open reading frame A is missing in SP virus, it is not essential for a productive infection. The status of the potential protein encoded by open reading frame B is not clear, because it may be missing or just truncated. Nevertheless, these genes appear to be the contributing entities for transmissible gastroenteritis virus virulence, SP morphology, tissue tropism, and/or persistence in swine leukocytes.

摘要

对一种无毒力的小蚀斑(SP)可传播性胃肠炎病毒变种和可传播性胃肠炎病毒的亲本有毒力的米勒毒株的细胞内RNA进行了比较。RNA印迹分析表明,米勒毒株含有8种细胞内RNA种类。两种病毒的RNA 1、2(S)、5、6(M)、7(N)和8大小相似;然而,SP变种缺少亚基因组RNA 3和4。相反,SP病毒含有一种改变的RNA种类(δ4),其略小于RNA 4。S1核酸酶保护实验表明,SP基因组在纤突蛋白S基因下游缺失了约450个核苷酸。cDNA克隆测序证实,SP病毒含有462个核苷酸的缺失,消除了RNA 3和4的转录识别序列。这些RNA分别编码开放阅读框A和B。对于SP病毒的δ4 RNA种类,未轻易发现替代的共有识别序列。由于SP病毒中缺少开放阅读框A,因此它对于有效的感染并非必需。由开放阅读框B编码的潜在蛋白质的状态尚不清楚,因为它可能缺失或只是被截断。然而,这些基因似乎是可传播性胃肠炎病毒毒力、SP形态、组织嗜性和/或在猪白细胞中持续存在的相关因素。

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