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突触传递和 HIV 感染对抗病毒药物的敏感性。

Synaptic transmission and the susceptibility of HIV infection to anti-viral drugs.

机构信息

Department of Mathematics, Rowland Hall, University of California, Irvine, CA 92697, USA.

出版信息

Sci Rep. 2013;3:2103. doi: 10.1038/srep02103.

Abstract

Cell-to-cell viral transmission via virological synapses has been argued to reduce susceptibility of the virus population to anti-viral drugs through multiple infection of cells, contributing to low-level viral persistence during therapy. Using a mathematical framework, we examine the role of synaptic transmission in treatment susceptibility. A key factor is the relative probability of individual virions to infect a cell during free-virus and synaptic transmission, a currently unknown quantity. If this infection probability is higher for free-virus transmission, then treatment susceptibility is lowest if one virus is transferred per synapse, and multiple infection of cells increases susceptibility. In the opposite case, treatment susceptibility is minimized for an intermediate number of virions transferred per synapse. Hence, multiple infection via synapses does not simply lower treatment susceptibility. Without further experimental investigations, one cannot conclude that synaptic transmission provides an additional mechanism for the virus to persist at low levels during anti-viral therapy.

摘要

通过病毒学突触的细胞间病毒传播,通过细胞的多次感染,被认为降低了病毒群体对抗病毒药物的敏感性,从而导致治疗期间病毒持续低水平存在。我们使用数学框架来研究突触传递在治疗敏感性中的作用。一个关键因素是单个病毒在游离病毒和突触传递过程中感染细胞的相对概率,这是一个目前未知的数量。如果游离病毒传播的感染概率更高,那么每个突触转移一个病毒时,治疗敏感性最低,如果细胞的多次感染增加了敏感性。相反,如果每个突触转移的病毒数量适中,则治疗敏感性最小化。因此,通过突触的多次感染并不会简单地降低治疗敏感性。在没有进一步的实验研究的情况下,不能得出结论认为突触传递为病毒在抗病毒治疗期间持续低水平提供了额外的机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/14ca/3696900/364217ac8feb/srep02103-f1.jpg

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