Accumulation of a novel spliceosomal complex on pre-mRNAs containing branch site mutations.
AUTOR(ES)
Champion-Arnaud, P
RESUMO
Pre-mRNA assembles into spliceosomal complexes in the stepwise pathway E-->A-->B-->C. We show that mutations in the metazoan branchpoint sequence (BPS) have no apparent effect on E complex formation but block the assembly of the A complex and the UV cross-linking of U2 small nuclear ribonucleoprotein particle (snRNP) proteins. Unexpectedly, a novel complex, designated E*, assembles on pre-mRNAs containing BPS mutations. Unlike the E complex, the E* complex accumulates in the presence of ATP. U1 snRNP and U2AF, which are tightly bound to pre-mRNA in the E complex, are not tightly bound in the E* complex. Significantly, previous work showed that U1 snRNP and U2AF become destabilized from pre-mRNA after E complex assembly on normal pre-mRNAs. Thus, our data are consistent with a model in which there are two steps in the transition from the E complex to the A complex (E-->E*-->A). In the first step, U1 snRNP and U2AF are destabilized in an ATP-dependent, BPS-independent reaction. In the second step, the stable binding of U2 snRNP occurs in a BPS-dependent reaction.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=230826Documentos Relacionados
- Mapping of branch sites in trans-spliced pre-mRNAs of Trypanosoma brucei.
- In vitro splicing pathways of pre-mRNAs containing multiple intervening sequences?
- Introns excised from immunoglobulin pre-mRNAs exist as discrete species.
- Selection of splice sites in pre-mRNAs with short internal exons.
- Natural trans-splicing in carnitine octanoyltransferase pre-mRNAs in rat liver
