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A FUNCTIONAL ASSOCIATION BETWEEN THE 5' AND 3' SPLICE SITES IS ESTABLISHED IN THE EARLIEST PRESPLICEOSOME COMPLEX (E) IN MAMMALS
被引:151
作者:
MICHAUD, S
REED, R
机构:
[1] Cellular and Molecular Physiology, Cell/Developmental Biology Program, Harvard Medical School, Boston
关键词:
E-COMPLEX;
5' AND 3' SPLICE SITES;
SPLICE SITE SELECTION;
SPLICING FACTORS;
SNRNP;
SUBSTRATE COMPETITION ASSAY;
D O I:
10.1101/gad.7.6.1008
中图分类号:
Q2 [细胞生物学];
学科分类号:
071009 ;
090102 ;
摘要:
The earliest detectable mammalian prespliceosome complex (E) contains the non-snRNP splicing factor U2AF, U1 snRNP, and several spliceosome-associated proteins (SAPs). We show that specific complexes, designated E3' and E5', assemble independently on RNAs containing only a 3' or 5' splice site, respectively. U2AF is enriched in E3', whereas U1 snRNP is enriched in E5'. Using a highly sensitive substrate-competition assay, we show that both the 5' splice site and the pyrimidine tract at the 3' splice site are required for efficient E complex assembly on intact pre-mRNA. We conclude that the 5' and 3' splice sites are associated functionally as early as E complex by either direct or indirect interactions between U1 snRNP and U2AF. Our observations predict that E complex assembly is a major control point for establishing splice site selection in both constitutively and alternatively spliced pre-mRNAs.
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页码:1008 / 1020
页数:13
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