Casasnovas J M, Springer T A
Center for Blood Research, Boston, Massachusetts 02115.
J Virol. 1994 Sep;68(9):5882-9. doi: 10.1128/JVI.68.9.5882-5889.1994.
We have examined the pathway of rhinovirus interaction with soluble intercellular adhesion molecule 1 (sICAM-1). Binding of sICAM-1 to rhinovirus serotypes 3 and 14 gives particles with sedimentation coefficients from 145 to 120S, depending on the amount of sICAM-1 bound. The formation of 120S particles is faster and more extensive at a neutral pH than at an acidic pH. A large number of receptors (> 30) can bind to human rhinovirus 3 without disruption. Disruption by sICAM-1 of rhinovirus that yields 80S particles is strongly temperature dependent and is antagonized by a low pH. Interestingly, sICAM-1 remains bound to the viral capsid after RNA is released, although in smaller amounts than those observed for the native virus. We have found heterogeneity both between and within 80S particle preparations in the VP4 content and number of bound receptors. The ability of the virus to remain bound to its receptor during the uncoating process may facilitate the transport of the viral genome into the cytoplasm in vivo.
我们研究了鼻病毒与可溶性细胞间黏附分子1(sICAM-1)相互作用的途径。sICAM-1与3型和14型鼻病毒结合会产生沉降系数在145至120S之间的颗粒,这取决于结合的sICAM-1的量。在中性pH条件下,120S颗粒的形成比在酸性pH条件下更快且更广泛。大量受体(>30个)可以与人鼻病毒3型结合而不被破坏。sICAM-1对鼻病毒的破坏产生80S颗粒,这强烈依赖于温度,并且在低pH条件下受到拮抗。有趣的是,RNA释放后,sICAM-1仍与病毒衣壳结合,尽管其数量比天然病毒中观察到的要少。我们发现在80S颗粒制剂之间以及制剂内部,VP4含量和结合受体数量存在异质性。病毒在脱壳过程中保持与受体结合的能力可能有助于病毒基因组在体内转运到细胞质中。
