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Intronic splicing enhancers, cognate splicing factors and context-dependent regulation rules.


ABSTRACT: Most human genes produce multiple splicing isoforms with distinct functions. To systematically understand splicing regulation, we conducted an unbiased screen and identified >100 intronic splicing enhancers (ISEs), clustered by sequence similarity. All ISEs functioned in multiple cell types and in heterologous introns, and patterns of distribution and conservation across pre-mRNA regions were similar to those of exonic splicing silencers. Consistently, all ISEs inhibited use of splice sites from exons. Putative trans-factors of each ISE group were identified and validated. Five distinct groups were recognized by hnRNP H and hnRNP F, whose C-terminal domains were sufficient to render context-dependent activities of ISEs. The sixth group was controlled by factors that either activate or suppress splicing. We provide a comprehensive picture of general ISE activities and suggest new models of how single elements can function oppositely, depending on locations and binding factors.

SUBMITTER: Wang Y 

PROVIDER: S-EPMC3753194 | biostudies-literature | 2012 Oct

REPOSITORIES: biostudies-literature

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Intronic splicing enhancers, cognate splicing factors and context-dependent regulation rules.

Wang Yang Y   Ma Meng M   Xiao Xinshu X   Wang Zefeng Z  

Nature structural & molecular biology 20120916 10


Most human genes produce multiple splicing isoforms with distinct functions. To systematically understand splicing regulation, we conducted an unbiased screen and identified >100 intronic splicing enhancers (ISEs), clustered by sequence similarity. All ISEs functioned in multiple cell types and in heterologous introns, and patterns of distribution and conservation across pre-mRNA regions were similar to those of exonic splicing silencers. Consistently, all ISEs inhibited use of splice sites from  ...[more]

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