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编码鼠轮状病毒外衣壳蛋白VP4和VP7的基因不是宿主范围限制和毒力的主要决定因素。

Murine rotavirus genes encoding outer capsid proteins VP4 and VP7 are not major determinants of host range restriction and virulence.

作者信息

Broome R L, Vo P T, Ward R L, Clark H F, Greenberg H B

机构信息

Veterinary Medical Unit, Veterans Affairs Medical Center, Palo Alto, California 94304.

出版信息

J Virol. 1993 May;67(5):2448-55. doi: 10.1128/JVI.67.5.2448-2455.1993.

DOI:10.1128/JVI.67.5.2448-2455.1993
PMID:8386262
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC237563/
Abstract

Simian rotavirus (RRV) and murine rotavirus (EDIM-RW) differ dramatically in the oral inoculum required to cause diarrheal disease in neonatal mouse pups and in their ability to spread and cause disease in uninoculated littermates. A genetic approach was used to explore the molecular basis of these differences. Reassortant viruses were produced in vivo by coinfecting infant mice with RRV and EDIM-RW. Reassortant viruses were isolated by plaque purification of progeny virus obtained from mouse pup intestines on MA104 cells. The plaque-purified reassortants were evaluated for 50% diarrhea dose (DD50) and for the ability to spread and cause diarrhea in uninoculated littermates. The parental RRV strain had a DD50 of 10(5) PFU per animal, while the EDIM-RW parental strain had a DD50 of less than 1 PFU per animal. RRV never spreads from inoculated to uninoculated littermates and causes disease. Twenty-three reassortants were tested. Of great interest were the reassortants D1/5 and C3/2, which derived genes 4 and 7 (encoding VP4 and VP7) from RRV. These viruses had a DD50 similar or identical to that of EDIM-RW and spread efficiently from inoculated mouse pups to uninoculated pups. We conclude that the major outer capsid proteins VP4 and VP7 are not primarily responsible for virulence or host range restriction in the mouse model using a homologous murine rotavirus.

摘要

猿猴轮状病毒(RRV)和鼠轮状病毒(EDIM-RW)在引起新生小鼠腹泻疾病所需的口服接种量以及在未接种的同窝小鼠中传播和引发疾病的能力方面存在显著差异。采用遗传学方法探究这些差异的分子基础。通过将RRV和EDIM-RW共同感染幼鼠在体内产生重配病毒。通过对从小鼠肠道获得的子代病毒在MA104细胞上进行噬斑纯化来分离重配病毒。对噬斑纯化的重配病毒进行50%腹泻剂量(DD50)评估以及在未接种的同窝小鼠中传播和引起腹泻能力的评估。亲本RRV毒株的DD50为每只动物10(5) PFU,而亲本EDIM-RW毒株的DD50小于每只动物1 PFU。RRV从不从接种小鼠传播到未接种的同窝小鼠并引发疾病。测试了23种重配病毒。其中,重配病毒D1/5和C3/2特别引人关注,它们从RRV获得了基因4和7(分别编码VP4和VP7)。这些病毒的DD50与EDIM-RW相似或相同,并且能有效地从接种的小鼠传播到未接种的小鼠。我们得出结论,在使用同源鼠轮状病毒的小鼠模型中,主要的外衣壳蛋白VP4和VP7并非毒力或宿主范围限制的主要决定因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8981/237563/51530b2dc302/jvirol00026-0035-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8981/237563/51530b2dc302/jvirol00026-0035-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8981/237563/51530b2dc302/jvirol00026-0035-a.jpg

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