Complex Structures of the Abscisic Acid Receptor PYL3/RCAR13 Reveal a Unique Regulatory Mechanism

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• 作者：Xingliang Zhang¹ ; Qi Zhang¹ ; Qi Xin² ; Lin Yu¹ ; Zheng Wang³ ; Wei Wu¹ ; Lun Jiang¹ ; Guoqiang Wang¹ ; Wenli Tian¹ ; Zengqin Deng¹ ; Yang Wang¹ ; Zhao Liu¹ ; Jiafu Long³ ; Zhizhong Gong² ; Zhongzhou Chen¹ ; ⁴ ; ^{chenzhongzhou@cau.edu.cn}
• 刊名：Structure
• 出版年：2012
• 期刊代码：143_09692126
• 类别：bio
• 出版时间：9 May, 2012
• 卷：20
• 期：5
• 页码：780-790
• 文件大小：1342 K

摘要

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Summary

Abscisic acid (ABA) controls many physiological processes and mediates adaptive responses to abiotic stresses. The ABA signaling mechanisms for abscisic acid receptors PYR/PYL/RCAR (PYLs) were reported. However, it remains unclear whether the molecular mechanisms are suitable for other PYLs. Here, complex structures of PYL3 with (+)-ABA, pyrabactin and HAB1 are reported. An unexpected trans-homodimer intermediate observed in the crystal is confirmed in solution. ABA-bound PYL3 greatly promotes the generation of monomeric PYL3, which can excessively increase the efficiency of inhibiting PP2Cs. Structure-guided biochemical experiments show that Ser195 accounts for the key intermediate. Interestingly, pyrabactin binds to PYL3 in a distinct nonproductive mode with gate closure, which sheds light on the design of agonists and antagonists for abscisic acid receptors. According to different conformations of ligand-bound PYLs,聽the PYLs family can be divided into three subclasses, among which the trans-dimeric subclass, represented by PYL3, reveals a distinct regulatory mechanism.