Human Splicing Factor SF3a, but Not SF1, Is Essential for Pre-mRNA Splicing In Vivo
AUTOR(ES)
Tanackovic, Goranka
FONTE
The American Society for Cell Biology
RESUMO
The three subunits of human splicing factor SF3a are essential for the formation of the functional 17S U2 snRNP and prespliceosome assembly in vitro. RNAi-mediated depletion indicates that each subunit is essential for viability of human cells. Knockdown of single subunits results in a general block in splicing strongly suggesting that SF3a is a constitutive splicing factor in vivo. In contrast, splicing of several endogenous and reporter pre-mRNAs is not affected after knockdown of SF1, which functions at the onset of spliceosome assembly in vitro and is essential for cell viability. Thus, SF1 may only be required for the splicing of a subset of pre-mRNAs. We also observe a reorganization of U2 snRNP components in SF3a-depleted cells, where U2 snRNA and U2-B″ are significantly reduced in nuclear speckles and the nucleoplasm, but still present in Cajal bodies. Together with the observation that the 17S U2 snRNP cannot be detected in extracts from SF3a-depleted cells, our results provide further evidence for a function of Cajal bodies in U2 snRNP biogenesis.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=551499Documentos Relacionados
- Functional analysis of pre-mRNA splicing factor SF2/ASF structural domains.
- A dual role for BBP/ScSF1 in nuclear pre-mRNA retention and splicing
- Identification of galectin-3 as a factor in pre-mRNA splicing.
- The human splicing factor ASF/SF2 can specifically recognize pre-mRNA 5' splice sites.
- SMNrp is an essential pre-mRNA splicing factor required for the formation of the mature spliceosome
