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水杨酸介导的植物免疫信号传导中的Cullin-RING泛素连接酶

Cullin-RING ubiquitin ligases in salicylic acid-mediated plant immune signaling.

作者信息

Furniss James J, Spoel Steven H

机构信息

Institute of Molecular Plant Sciences, School of Biological Sciences, University of Edinburgh Edinburgh, UK.

出版信息

Front Plant Sci. 2015 Mar 13;6:154. doi: 10.3389/fpls.2015.00154. eCollection 2015.

Abstract

Plant immune responses against biotrophic pathogens are regulated by the signaling hormone salicylic acid (SA). SA establishes immunity by regulating a variety of cellular processes, including programmed cell death (PCD) to isolate and kill invading pathogens, and development of systemic acquired resistance (SAR) which provides long-lasting, broad-spectrum resistance throughout the plant. Central to these processes is post-translational modification of SA-regulated signaling proteins by ubiquitination, i.e., the covalent addition of small ubiquitin proteins. Emerging evidence indicates SA-induced protein ubiquitination is largely orchestrated by Cullin-RING ligases (CRLs), which recruit specific substrates for ubiquitination using interchangeable adaptors. Ligation of ubiquitin chains interlinked at lysine 48 leads to substrate degradation by the 26S proteasome. Here we discuss how CRL-mediated degradation of both nucleotide-binding/leucine-rich repeat domain containing immune receptors and SA-induced transcription regulators are critical for functional PCD and SAR responses, respectively. By placing these recent findings in context of knowledge gained in other eukaryotic model species, we highlight potential alternative roles for processive ubiquitination in regulating the activity of SA-mediated immune responses.

摘要

植物针对活体营养型病原体的免疫反应受信号激素水杨酸(SA)调控。SA通过调节多种细胞过程来建立免疫,这些过程包括程序性细胞死亡(PCD)以隔离和杀死入侵的病原体,以及系统获得性抗性(SAR)的形成,SAR能为整株植物提供持久、广谱的抗性。这些过程的核心是通过泛素化对SA调控的信号蛋白进行翻译后修饰,即小泛素蛋白的共价添加。新出现的证据表明,SA诱导的蛋白泛素化很大程度上由Cullin-RING连接酶(CRL)协调,CRL利用可互换的衔接子招募特定底物进行泛素化。赖氨酸48处相互连接的泛素链的连接导致底物被26S蛋白酶体降解。在此,我们讨论CRL介导的含核苷酸结合/富含亮氨酸重复结构域的免疫受体和SA诱导的转录调节因子的降解如何分别对功能性PCD和SAR反应至关重要。通过将这些最新发现置于在其他真核模式物种中获得的知识背景下,我们强调了持续性泛素化在调节SA介导的免疫反应活性中的潜在替代作用。

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