Structural studies of reelin N-terminal region provides insights into a unique structural arrangement and functional multimerization

卷绕 DAB1 终端(电信) 糖蛋白 受体 体系结构域 细胞生物学 表皮生长因子 C端 信号转导 生物 化学 分子生物学 神经科学 氨基酸 遗传学 计算机科学 企业架构框架 电信 程序设计语言 软件 软件体系结构
作者
Masamichi Nagae,Kei Suzuki,N. Yasui,Terukazu Nogi,Takao Kohno,Mitsuharu Hattori,Junichi Takagi
出处
期刊:Journal of Biochemistry [Oxford University Press]
卷期号:169 (5): 555-564 被引量:6
标识
DOI:10.1093/jb/mvaa144
摘要

Abstract The large, secreted glycoprotein reelin regulates embryonic brain development as well as adult brain functions. Although reelin binds to its receptors via its central part, the N-terminal region directs multimer formation and is critical for efficient signal transduction. In fact, the inhibitory antibody CR-50 interacts with the N-terminal region and prevents higher-order multimerization and signalling. Reelin is a multidomain protein in which the central part is composed of eight characteristic repeats, named reelin repeats, each of which is further divided by insertion of a epidermal growth factor (EGF) module into two subrepeats. In contrast, the N-terminal region shows unique ‘irregular’ domain architecture since it comprises three consecutive subrepeats without the intervening EGF module. Here, we determined the crystal structure of the murine reelin fragment named RX-R1 including the irregular region and the first reelin repeat at 2.0-Å resolution. The overall structure of RX-R1 has a branched Y-shaped form. Interestingly, two incomplete subrepeats cooperatively form one entire subrepeat structure, though an additional subrepeat is inserted between them. We further reveal that Arg335 of RX-R1 is crucial for binding CR-50. A possible self-association mechanism via the N-terminal region is proposed based on our results.

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