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载体蛋白 SLC35A1 和 SLC30A1 在 VSV 病毒感染时对细胞存活起着相反的作用。

The transporters SLC35A1 and SLC30A1 play opposite roles in cell survival upon VSV virus infection.

机构信息

CeMM Research Center for Molecular Medicine of the Austrian Academy of Sciences, 1090, Vienna, Austria.

Center for Physiology and Pharmacology, Medical University of Vienna, 1090, Vienna, Austria.

出版信息

Sci Rep. 2019 Jul 18;9(1):10471. doi: 10.1038/s41598-019-46952-9.

Abstract

Host factor requirements for different classes of viruses have not been fully unraveled. Replication of the viral genome and synthesis of viral proteins within the human host cell are associated with an increased demand for nutrients and specific metabolites. With more than 400 acknowledged members to date in humans, solute carriers (SLCs) represent the largest family of transmembrane proteins dedicated to the transport of ions and small molecules such as amino acids, sugars and nucleotides. Consistent with their impact on cellular metabolism, several SLCs have been implicated as host factors affecting the viral life cycle and the cellular response to infection. In this study, we aimed at characterizing the role of host SLCs in cell survival upon viral infection by performing unbiased genetic screens using a focused CRISPR knockout library. Genetic screens with the cytolytic vesicular stomatitis virus (VSV) showed that the loss of two SLCs genes, encoding the sialic acid transporter SLC35A1/CST and the zinc transporter SLC30A1/ZnT1, affected cell survival upon infection. Further characterization of these genes suggests a role for both of these transporters in the apoptotic response induced by VSV, offering new insights into the cellular response to oncolytic virus infections.

摘要

宿主因子对不同类型病毒的需求尚未完全阐明。病毒基因组的复制和病毒蛋白在人宿主细胞中的合成与对营养物质和特定代谢物的需求增加有关。迄今为止,人类已确认有超过 400 种成员,溶质载体(SLCs)是专门用于运输离子和小分子(如氨基酸、糖和核苷酸)的最大跨膜蛋白家族。鉴于它们对细胞代谢的影响,一些 SLC 已被认为是影响病毒生命周期和细胞对感染反应的宿主因子。在这项研究中,我们通过使用靶向 CRISPR 敲除文库进行无偏遗传筛选,旨在通过对病毒感染后的细胞存活进行特征分析,来研究宿主 SLC 在病毒感染过程中的作用。使用细胞溶胞性单纯疱疹病毒(VSV)进行的遗传筛选表明,编码唾液酸转运蛋白 SLC35A1/CST 和锌转运蛋白 SLC30A1/ZnT1 的两个 SLC 基因的缺失会影响感染后的细胞存活。对这些基因的进一步表征表明,这两种转运蛋白都在 VSV 诱导的凋亡反应中发挥作用,为细胞对溶瘤病毒感染的反应提供了新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0034/6639343/e4521e501bf0/41598_2019_46952_Fig1_HTML.jpg

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