The Drosophila U2 snRNP protein U2A' has an essential function that is SNF/U2B'' independent

doi:10.1093/nar/29.18.3841

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Nucleic Acids Research, 2001, Vol. 29, No. 18 3841-3847
© 2001 Oxford University Press

The Drosophila U2 snRNP protein U2A' has an essential function that is SNF/U2B'' independent

Alexis A. Nagengast and Helen K. Salz^*

Department of Genetics, Case Western Reserve University, School of Medicine, 10900 Euclid Avenue, Cleveland, OH 44106-4955, USA

Recruitment of the U2 snRNP to the pre-mRNA is an essentialstep in spliceosome assembly. Although the protein componentsof the U2 snRNP have been identified, their individual contributionsto function are poorly defined. In vitro studies with the Drosophilaand human proteins suggest that two of the U2 snRNP-specificproteins, U2A' and U2B'', function exclusively as a dimer. InDrosophila the presence of the U2B'' counterpart, Sans-Fille(SNF), in the U2 snRNP is dispensable for viability, suggestingthat SNF is not necessary for U2 snRNP function in vivo. Withthe identification of a single U2A'-like protein in the Drosophilagenome, we can now investigate the relationship between SNFand its putative binding partner in vivo. Here we show thatDrosophila U2A' protein interacts with SNF in vivo and, likeits human counterpart, is U2 snRNP specific. Unexpectedly, however,we find that loss of function causes lethality, suggesting thatU2A', but not SNF, is critical for U2 snRNP function. Moreover,although we demonstrate that several domains in the SNF proteinare important for the interaction with the Drosophila U2A' protein,including a redundant domain at the normally dispensable C-terminus,we find that U2A' does not require heterodimer formation foreither its vital function or U2 snRNP assembly. Thus togetherthese data demonstrate that in Drosophila U2A' has an essentialfunction that is unrelated to its role as the partner proteinof SNF/U2B''.

^* To whom correspondence should be addressed. Tel: +1 216 3682879; Fax: +1 216 368 3432; Email: hks{at}po.cwru.edu

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