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外被体亚基 Exo70B2 与免疫信号和自噬有关。

Exocyst subunit Exo70B2 is linked to immune signaling and autophagy.

机构信息

Faculty of Biology, Cell Biology, University of Freiburg, 79104 Freiburg, Germany.

Leibniz Institute of Plant Biochemistry, 06120 Halle (Saale), Germany.

出版信息

Plant Cell. 2021 Apr 17;33(2):404-419. doi: 10.1093/plcell/koaa022.

Abstract

During the immune response, activation of the secretory pathway is key to mounting an effective response, while gauging its output is important to maintain cellular homeostasis. The Exo70 subunit of the exocyst functions as a spatiotemporal regulator by mediating numerous interactions with proteins and lipids. However, a molecular understanding of the exocyst regulation remains challenging. We show that, in Arabidopsis thaliana, Exo70B2 behaves as a bona fide exocyst subunit. Conversely, treatment with the salicylic acid (SA) defence hormone analog benzothiadiazole (BTH), or the immunogenic peptide flg22, induced Exo70B2 transport into the vacuole. We reveal that Exo70B2 interacts with AUTOPHAGY-RELATED PROTEIN 8 (ATG8) via two ATG8-interacting motives (AIMs) and its transport into the vacuole is dependent on autophagy. In line with its role in immunity, we discovered that Exo70B2 interacted with and was phosphorylated by the kinase MPK3. Mimicking phosphorylation had a dual impact on Exo70B2: first, by inhibiting localization at sites of active secretion, and second, it increased the interaction with ATG8. Phosphonull variants displayed higher effector-triggered immunity (ETI) and were hypersensitive to BTH, which induce secretion and autophagy. Our results suggest a molecular mechanism by which phosphorylation diverts Exo70B2 from the secretory into the autophagy pathway for its degradation, to dampen secretory activity.

摘要

在免疫反应中,激活分泌途径对于产生有效的反应至关重要,而衡量其输出对于维持细胞内稳态也很重要。外泌体的 Exo70 亚基通过介导与蛋白质和脂质的众多相互作用,作为时空调节剂发挥作用。然而,对外泌体调控的分子理解仍然具有挑战性。我们表明,在拟南芥中,Exo70B2 是一种真正的外泌体亚基。相反,用防御激素水杨酸(SA)类似物苯并噻二唑(BTH)或免疫肽 flg22 处理,会诱导 Exo70B2 转运到液泡中。我们揭示了 Exo70B2 通过两个 ATG8 相互作用基序(AIM)与自噬相关蛋白 8(ATG8)相互作用,其转运到液泡中依赖于自噬。与它在免疫中的作用一致,我们发现 Exo70B2 与激酶 MPK3 相互作用并被其磷酸化。模拟磷酸化对 Exo70B2 有双重影响:首先,通过抑制在活跃分泌部位的定位,其次,它增加了与 ATG8 的相互作用。磷酸化突变体表现出更高的效应触发免疫(ETI),并且对 BTH 更敏感,BTH 诱导分泌和自噬。我们的结果表明了一种分子机制,即通过磷酸化将 Exo70B2 从分泌途径转向自噬途径进行降解,以抑制分泌活性。

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