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细胞肝素硫酸在病毒致病性中是如何发挥作用的?

How does cellular heparan sulfate function in viral pathogenicity?

机构信息

Department of Viral Encephalitis, Institute for Viral Disease Control and Prevention, Chinese Center for Disease Control and Prevention and State Key Laboratory for Infectious Disease Prevention and Control (SKLID), Beijing 100052, China.

出版信息

Biomed Environ Sci. 2011 Feb;24(1):81-7. doi: 10.3967/0895-3988.2011.01.011.

Abstract

Heparan sulfate (HS) is ubiquitously expressed on the surfaces and in the extracellular matrix of virtually all cell types, making it an ideal receptor for viral infection. Compared with wild-type viruses, cell culture-adapted laboratory strains exhibit more efficient binding to cellular HS receptors. HS-binding viruses are typically cleared faster from the circulation and cause lower viremia than their non-HS-binding counterparts, suggesting that the HS-binding phenotype is a tissue culture adaptation that lowers virus fitness in vivo. However, when inoculated intracranially, efficient cell attachment through HS binding can contribute to viral neurovirulence. The primary aim of this review is to discuss the roles of HS binding in viral pathogenicity, including peripheral virulence and neurovirulence. Understanding how heparan sulfate functions during virus infection in vivo may prove critical for elucidating the molecular mechanism of viral pathogenesis, and may contribute to the development of therapeutics targeting HS.

摘要

硫酸乙酰肝素(HS)广泛表达于几乎所有细胞类型的表面和细胞外基质中,使其成为病毒感染的理想受体。与野生型病毒相比,细胞培养适应的实验室株表现出与细胞 HS 受体更有效的结合。与非 HS 结合的病毒相比,HS 结合的病毒通常更快地从循环中清除,并导致更低的病毒血症,这表明 HS 结合表型是一种组织培养适应,降低了病毒在体内的适应性。然而,当颅内接种时,通过 HS 结合的有效细胞附着有助于病毒的神经毒力。本综述的主要目的是讨论 HS 结合在病毒致病性中的作用,包括外周毒力和神经毒力。了解硫酸乙酰肝素在体内病毒感染过程中的作用可能对阐明病毒发病机制的分子机制至关重要,并可能有助于开发针对 HS 的治疗方法。

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