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番茄异戊烯化RAB受体蛋白1调节模式识别受体LeEIX2的转运和降解,影响先天免疫反应。

Tomato Prenylated RAB Acceptor Protein 1 Modulates Trafficking and Degradation of the Pattern Recognition Receptor LeEIX2, Affecting the Innate Immune Response.

作者信息

Pizarro Lorena, Leibman-Markus Meirav, Schuster Silvia, Bar Maya, Meltz Tal, Avni Adi

机构信息

School of Plant Sciences and Food Security, Tel Aviv University, Tel Aviv, Israel.

Department of Plant Pathology and Weed Research, Agricultural Research Organization, Volcani Center, Rishon LeZion, Israel.

出版信息

Front Plant Sci. 2018 Mar 1;9:257. doi: 10.3389/fpls.2018.00257. eCollection 2018.

Abstract

Plants recognize microbial/pathogen associated molecular patterns (MAMP/PAMP) through pattern recognition receptors (PRRs) triggering an immune response against pathogen progression. MAMP/PAMP triggered immune response requires PRR endocytosis and trafficking for proper deployment. LeEIX2 is a well-known RLP-PRR, able to recognize and respond to the fungal MAMP/PAMP ethylene-inducing xylanase (EIX), and its function is highly dependent on intracellular trafficking. Identifying protein machinery components regulating LeEIX2 intracellular trafficking is crucial to our understanding of LeEIX2 mediated immune responses. In this work, we identified a novel trafficking protein, SlPRA1A, a predicted regulator of RAB, as an interactor of LeEIX2. Overexpression of SlPRA1A strongly decreases LeEIX2 endosomal localization, as well as LeEIX2 protein levels. Accordingly, the innate immune responses to EIX are markedly reduced by SlPRA1A overexpression, presumably due to a decreased LeEIX2 availability. Studies into the role of SlPRA1A in LeEIX2 trafficking revealed that LeEIX2 localization in multivesicular bodies/late endosomes is augmented by SlPRA1A. Furthermore, inhibiting vacuolar function prevents the LeEIX2 protein level reduction mediated by SlPRA1A, suggesting that SlPRA1A may redirect LeEIX2 trafficking to the vacuole for degradation. Interestingly, SlPRA1A overexpression reduces the amount of several RLP-PRRs, but does not affect the protein level of receptor-like kinase PRRs, suggesting a specific role of SlPRA1A in RLP-PRR trafficking and degradation.

摘要

植物通过模式识别受体(PRR)识别微生物/病原体相关分子模式(MAMP/PAMP),从而触发针对病原体进展的免疫反应。MAMP/PAMP触发的免疫反应需要PRR的内吞作用和运输,以实现正确的部署。LeEIX2是一种著名的类受体蛋白(RLP)-PRR,能够识别并响应真菌MAMP/PAMP乙烯诱导木聚糖酶(EIX),其功能高度依赖于细胞内运输。鉴定调节LeEIX2细胞内运输的蛋白质机制成分对于我们理解LeEIX2介导的免疫反应至关重要。在这项工作中,我们鉴定了一种新的运输蛋白SlPRA1A,它是RAB的预测调节因子,作为LeEIX2的相互作用蛋白。SlPRA1A的过表达强烈降低了LeEIX2的内体定位以及LeEIX2蛋白水平。因此,SlPRA1A的过表达显著降低了对EIX的先天免疫反应,这可能是由于LeEIX2的可用性降低所致。对SlPRA1A在LeEIX2运输中的作用研究表明,SlPRA1A增强了LeEIX2在多泡体/晚期内体中的定位。此外,抑制液泡功能可防止SlPRA1A介导的LeEIX2蛋白水平降低,这表明SlPRA1A可能将LeEIX2运输重定向至液泡进行降解。有趣的是,SlPRA1A的过表达减少了几种RLP-PRR的数量,但不影响类受体激酶PRR的蛋白水平,这表明SlPRA1A在RLP-PRR运输和降解中具有特定作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/048f/5838007/d2ebd6f5c091/fpls-09-00257-g001.jpg

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