The Province and Ministry Co-sponsored Collaborative Innovation Center for Medical Epigenetics, Key Laboratory of Immune Microenvironment and Disease (Ministry of Education), Haihe Laboratory of Cell Ecosystem, School of Basic Medical Sciences, Tianjin Medical University, 300070, Tianjin, China.
Department of Pharmacology, Tianjin Key Laboratory of Inflammatory Biology, Center for Cardiovascular Diseases, Tianjin Medical University, 300070, Tianjin, China.
Nat Commun. 2023 Apr 29;14(1):2474. doi: 10.1038/s41467-023-38173-6.
The ribosome-associated quality-control (RQC) pathway degrades aberrant nascent polypeptides arising from ribosome stalling during translation. In mammals, the E3 ligase Pirh2 mediates the degradation of aberrant nascent polypeptides by targeting the C-terminal polyalanine degrons (polyAla/C-degrons). Here, we present the crystal structure of Pirh2 bound to the polyAla/C-degron, which shows that the N-terminal domain and the RING domain of Pirh2 form a narrow groove encapsulating the alanine residues of the polyAla/C-degron. Affinity measurements in vitro and global protein stability assays in cells further demonstrate that Pirh2 recognizes a C-terminal A/S-X-A-A motif for substrate degradation. Taken together, our study provides the molecular basis underlying polyAla/C-degron recognition by Pirh2 and expands the substrate recognition spectrum of Pirh2.
核糖体相关质量控制 (RQC) 途径降解翻译过程中核糖体停滞导致的异常新生多肽。在哺乳动物中,E3 连接酶 Pirh2 通过靶向 C 末端聚丙氨酸降解元件 (polyAla/C-degrons) 介导异常新生多肽的降解。在这里,我们展示了与 polyAla/C-degron 结合的 Pirh2 的晶体结构,该结构表明 Pirh2 的 N 端结构域和 RING 结构域形成一个狭窄的凹槽,包裹着 polyAla/C-degron 的丙氨酸残基。体外亲和力测量和细胞内整体蛋白质稳定性测定进一步表明,Pirh2 识别 C 末端 A/S-X-A-A 基序进行底物降解。总之,我们的研究为 Pirh2 识别 polyAla/C-degron 提供了分子基础,并扩展了 Pirh2 的底物识别谱。
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