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βII血影蛋白中与fodaxin(A60)发生轴突特异性相互作用所需的独特序列的定义。

Definition of a sequence unique in beta II spectrin required for its axon-specific interaction with fodaxin (A60).

作者信息

Hayes N V, Phillips G W, Carden M J, Baines A J

机构信息

Research School of Biosciences, University of Kent, Canterbury, England.

出版信息

J Neurochem. 1997 Apr;68(4):1686-95. doi: 10.1046/j.1471-4159.1997.68041686.x.

DOI:10.1046/j.1471-4159.1997.68041686.x
PMID:9084442
Abstract

Spectrin isotypes segregate in neurons and are differentially distributed between axons and somatodendritic compartments. Their functions in those compartments are likely to be mediated by proteins that interact selectively with one or other isotype. Fodaxin (an axon-specific protein previously termed A60) colocalizes in CNS neurons with axonal spectrin and in vitro binds brain spectrin (a mixture of alpha I, beta I, and beta II polypeptides) but not erythrocyte spectrin (alpha I and beta I). Because alpha II and beta II spectrin polypeptides are enriched in axons, we investigated a possible binding of fodaxin to the types of spectrin found in axons. Fodaxin did not bind to isolated brain alpha chains. Bacterially expressed C-terminal segments 18-19 of beta II spectrin bound to fodaxin and inhibited the binding of fodaxin to whole brain spectrin. By contrast, recombinant segments 18-19 of the somatodendritic beta I sigma 2 spectrin showed no interaction with fodaxin. Within beta II, fodaxin binding activity was localized to residues 2,087-2,198, which are unique to beta II and link between the end of segment 18 and the pleckstrin homology domain in segment 19. The divergent regions of sequence in segments 19 of beta II and beta I sigma 2 are candidates to mediate the isotype-specific functions of spectrin. Fodaxin is the first protein to be described that discriminates between the unique regions of beta spectrin isoforms.

摘要

血影蛋白异构体在神经元中分离,并且在轴突和胞体树突区域之间呈差异分布。它们在这些区域的功能可能由与一种或另一种异构体选择性相互作用的蛋白质介导。Fodaxin(一种先前称为A60的轴突特异性蛋白质)在中枢神经系统神经元中与轴突血影蛋白共定位,并且在体外与脑血影蛋白(αI、βI和βII多肽的混合物)结合,但不与红细胞血影蛋白(αI和βI)结合。由于αII和βII血影蛋白多肽在轴突中富集,我们研究了Fodaxin与轴突中发现的血影蛋白类型之间可能的结合。Fodaxin不与分离的脑α链结合。细菌表达的βII血影蛋白的C末端片段18 - 19与Fodaxin结合,并抑制Fodaxin与全脑血影蛋白的结合。相比之下,胞体树突βIσ2血影蛋白的重组片段18 - 19与Fodaxin没有相互作用。在βII内,Fodaxin结合活性定位于2087 - 2198位残基,这些残基是βII特有的,连接片段18的末端和片段19中的普列克底物蛋白同源结构域。βII和βIσ2片段19中不同的序列区域是介导血影蛋白异构体特异性功能的候选区域。Fodaxin是第一个被描述的能够区分β血影蛋白异构体独特区域的蛋白质。

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