外显子
拼接因子
RNA结合蛋白
外显子剪接增强剂
SR蛋白
分子生物学
剪接体
作者
Barbara A. Sosnowski,John M. Belote,Michael McKeown
出处
期刊:Cell
[Elsevier]
日期:1989-08-11
卷期号:58 (3): 449-459
被引量:244
标识
DOI:10.1016/0092-8674(89)90426-1
摘要
Abstract Sex-specific alternative splicing of RNA from the Drosophila transformer gene involves competition between two 3′ splice sites. In the absence of Sex-lethal activity (as in males), only one site functions; in the presence of Sex-lethal activity (as in females), both sites function. Information for sex-specific splice site choice is contained within the intron itself. Deletions of the splice site used in males lead to Sex-lethal -independent use of the otherwise female-specific site. The relative amounts of unspliced and spliced RNA derived from these mutant genes do not change with changes in Sex-lethal activity. Specific nucleotide changes in the non-sex-specific splice site do not affect splicing activity but eliminate Sex-lethal -induced regulation. A deletion removing material between the two splice sites does not eliminate sex-specific regulation, while a deletion of the female splice site leads to a female-specific increase in unspliced RNA. These results are consistent with a model in which female-specific factors block the function of the non-sex-specific 3′ splice site.
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