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SNARE蛋白SEC22B在抗原交叉呈递中作用的批判性分析

A Critical Analysis of the Role of SNARE Protein SEC22B in Antigen Cross-Presentation.

作者信息

Wu S Julia, Niknafs Yashar S, Kim Stephanie H, Oravecz-Wilson Katherine, Zajac Cynthia, Toubai Tomomi, Sun Yaping, Prasad Jayendra, Peltier Daniel, Fujiwara Hideaki, Hedig Israel, Mathewson Nathan D, Khoriaty Rami, Ginsburg David, Reddy Pavan

机构信息

Program in Immunology, University of Michigan Medical School, Ann Arbor, MI 48109, USA; Medical Scientist Training Program, University of Michigan Medical School, Ann Arbor, MI 48109, USA.

Medical Scientist Training Program, University of Michigan Medical School, Ann Arbor, MI 48109, USA; Cellular and Molecular Biology Program, University of Michigan Medical School, Ann Arbor, MI 48109, USA.

出版信息

Cell Rep. 2017 Jun 27;19(13):2645-2656. doi: 10.1016/j.celrep.2017.06.013.

DOI:10.1016/j.celrep.2017.06.013
PMID:28658614
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5539946/
Abstract

Cross-presentation initiates immune responses against tumors and viral infections by presenting extracellular antigen on MHC I to activate CD8 T cell-mediated cytotoxicity. In vitro studies in dendritic cells (DCs) established SNARE protein SEC22B as a specific regulator of cross-presentation. However, the in vivo contribution of SEC22B to cross-presentation has not been tested. To address this, we generated DC-specific Sec22b knockout (CD11c-Cre Sec22b) mice. Contrary to the paradigm, SEC22B-deficient DCs efficiently cross-present both in vivo and in vitro. Although in vitro small hairpin RNA (shRNA)-mediated Sec22b silencing in bone-marrow-derived dendritic cells (BMDCs) reduced cross-presentation, treatment of SEC22B-deficient BMDCs with the same shRNA produced a similar defect, suggesting the Sec22b shRNA modulates cross-presentation through off-target effects. RNA sequencing of Sec22b shRNA-treated SEC22B-deficient BMDCs demonstrated several changes in the transcriptome. Our data demonstrate that contrary to the accepted model, SEC22B is not necessary for cross-presentation, cautioning against extrapolating phenotypes from knockdown studies alone.

摘要

交叉呈递通过将细胞外抗原呈递于MHC I 来激活CD8 T细胞介导的细胞毒性,从而启动针对肿瘤和病毒感染的免疫反应。在树突状细胞(DC)中的体外研究确定SNARE蛋白SEC22B为交叉呈递的特异性调节因子。然而,SEC22B在体内对交叉呈递的作用尚未得到验证。为了解决这个问题,我们构建了DC特异性Sec22b基因敲除(CD11c-Cre Sec22b)小鼠。与传统观念相反,SEC22B缺陷的DC在体内和体外均能有效地进行交叉呈递。虽然在体外,用小发夹RNA(shRNA)介导的骨髓来源的树突状细胞(BMDC)中Sec22b沉默会降低交叉呈递,但用相同的shRNA处理SEC22B缺陷的BMDC也会产生类似的缺陷,这表明Sec22b shRNA通过脱靶效应调节交叉呈递。对用Sec22b shRNA处理的SEC22B缺陷的BMDC进行RNA测序,结果显示转录组有多处变化。我们的数据表明,与公认的模型相反,SEC22B对于交叉呈递并非必需,这警示我们不能仅从敲低研究中推断表型。

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