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ANKRA2 的锚重复序列识别 3M 综合征蛋白 CCDC8 上的 PxLPxL 基序。

Ankyrin repeats of ANKRA2 recognize a PxLPxL motif on the 3M syndrome protein CCDC8.

机构信息

The Rosalind & Morris Goodman Cancer Research Center, Department of Medicine, McGill University, Montréal, QC H3A 1A3, Canada; Department of Breast Cancer, The Third Affiliated Hospital, Kunming Medical University, Yunnan 650118, China.

Structural Genomics Consortium, University of Toronto, 101 College Street, Toronto, ON M5G 1L7, Canada.

出版信息

Structure. 2015 Apr 7;23(4):700-12. doi: 10.1016/j.str.2015.02.001. Epub 2015 Mar 5.

Abstract

Peptide motifs are often used for protein-protein interactions. We have recently demonstrated that ankyrin repeats of ANKRA2 and the paralogous bare lymphocyte syndrome transcription factor RFXANK recognize PxLPxL/I motifs shared by megalin, three histone deacetylases, and RFX5. We show here that that CCDC8 is a major partner of ANKRA2 but not RFXANK in cells. The CCDC8 gene is mutated in 3M syndrome, a short-stature disorder with additional facial and skeletal abnormalities. Two other genes mutated in this syndrome encode CUL7 and OBSL1. While CUL7 is a ubiquitin ligase and OBSL1 associates with the cytoskeleton, little is known about CCDC8. Binding and structural analyses reveal that the ankyrin repeats of ANKRA2 recognize a PxLPxL motif at the C-terminal region of CCDC8. The N-terminal part interacts with OBSL1 to form a CUL7 ligase complex. These results link ANKRA2 unexpectedly to 3M syndrome and suggest novel regulatory mechanisms for histone deacetylases and RFX7.

摘要

肽基序常用于蛋白质-蛋白质相互作用。我们最近证明,ANKRA2 的锚蛋白重复序列和同源的 bare lymphocyte syndrome 转录因子 RFXANK 识别 megalin、三种组蛋白去乙酰化酶和 RFX5 共享的 PxLPxL/I 基序。我们在这里表明,CCDC8 是 ANKRA2 的主要伴侣,但不是细胞中 RFXANK 的主要伴侣。CCDC8 基因在 3M 综合征中发生突变,这是一种身材矮小的疾病,伴有额外的面部和骨骼异常。该综合征中另外两个突变的基因编码 CUL7 和 OBSL1。虽然 CUL7 是一种泛素连接酶,OBSL1 与细胞骨架相关,但对 CCDC8 知之甚少。结合和结构分析表明,ANKRA2 的锚蛋白重复序列识别 CCDC8 C 端区域的 PxLPxL 基序。N 端部分与 OBSL1 相互作用形成 CUL7 连接酶复合物。这些结果出人意料地将 ANKRA2 与 3M 综合征联系起来,并为组蛋白去乙酰化酶和 RFX7 提出了新的调节机制。

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