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鼻病毒-可溶性细胞间黏附分子-1复合物的形成及病毒体的构象变化。

Formation of rhinovirus-soluble ICAM-1 complexes and conformational changes in the virion.

作者信息

Hoover-Litty H, Greve J M

机构信息

Institute for Molecular Biologicals, Miles Research Center, West Haven, Connecticut 06516-4175.

出版信息

J Virol. 1993 Jan;67(1):390-7. doi: 10.1128/JVI.67.1.390-397.1993.

DOI:10.1128/JVI.67.1.390-397.1993
PMID:8093221
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC237375/
Abstract

Viral receptors serve both to target viruses to specific cell types and to actively promote the entry of bound virus into cells. Human rhinoviruses (HRVs) can form complexes in vitro with a truncated soluble form of the HRV cell surface receptor, ICAM-1. These complexes appear to be stoichiometric, with approximately 60 ICAM molecules bound per virion or 1 ICAM-1 molecule per icosahedral face of the capsid. The complex can have two fates, either dissociating to yield free virus and free ICAM-1 or uncoating to break down to an 80S empty capsid which has released VP4, viral RNA, and ICAM-1. This uncoating in vitro mimics the uncoating of virus during infection of cells. The stability of the virus-receptor complex is dependent on temperature and the rhinovirus serotype. HRV serotype 14 (HRV14)-ICAM-1 complexes rapidly uncoat, HRV16 forms a stable virus-ICAM complex which does not uncoat detectably at 34 degrees C, and HRV3 has an intermediate phenotype. Rhinovirus can also uncoat after exposure to mildly acidic pH. The sensitivities of individual rhinovirus serotypes to ICAM-1-mediated virus uncoating do not correlate with uncoating promoted by incubation at low pH, suggesting that these two means of virus destabilization occur by different mechanisms. Soluble ICAM-1 and low pH do not act synergistically to promote uncoating. The rate of uncoating does appear to be inversely related to virus affinity for its receptor.

摘要

病毒受体既可以将病毒靶向特定细胞类型,又能积极促进结合的病毒进入细胞。人鼻病毒(HRV)在体外可与HRV细胞表面受体ICAM-1的截短可溶性形式形成复合物。这些复合物似乎是化学计量的,每个病毒粒子结合约60个ICAM分子,或衣壳的每个二十面体面结合1个ICAM-1分子。该复合物有两种命运,要么解离产生游离病毒和游离ICAM-1,要么脱壳分解为已释放VP4、病毒RNA和ICAM-1的80S空衣壳。这种体外脱壳模拟了病毒在细胞感染过程中的脱壳。病毒-受体复合物的稳定性取决于温度和鼻病毒血清型。HRV血清型14(HRV14)-ICAM-1复合物迅速脱壳,HRV16形成稳定的病毒-ICAM复合物,在34℃下不会明显脱壳,而HRV3具有中间表型。鼻病毒在暴露于轻度酸性pH后也会脱壳。单个鼻病毒血清型对ICAM-1介导的病毒脱壳的敏感性与在低pH孵育促进的脱壳无关,这表明这两种使病毒不稳定的方式是通过不同机制发生的。可溶性ICAM-1和低pH不会协同作用促进脱壳。脱壳速率似乎与病毒对其受体的亲和力呈负相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b70e/237375/a2c3415aee37/jvirol00022-0415-b.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b70e/237375/8bf54d4d7786/jvirol00022-0415-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b70e/237375/a2c3415aee37/jvirol00022-0415-b.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b70e/237375/8bf54d4d7786/jvirol00022-0415-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b70e/237375/a2c3415aee37/jvirol00022-0415-b.jpg

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