Different forms of Ultrabithorax proteins generated by alternative splicing are functionally equivalent.
AUTOR(ES)
Busturia, A
RESUMO
The Ubx gene of Drosophila normally produces several forms of Ubx proteins through alternative splicing of two microexons. We describe here two new viable Ubx mutations that show similar and almost wild-type adult phenotypes. Molecular characterization has shown that one of them, UbxMX17, is an inversion within the Ubx transcription unit including one of the microexons involved in alternative splicing. This results in mutant flies possessing a very abnormal array of Ubx proteins, probably including spliced forms not present in wild-type flies. Yet these protein products successfully substitute for the normal ones and allow virtually normal Ubx function. We argue that the different Ubx proteins are developmentally equivalent and that the slight mutant phenotype observed in UbxMX17 flies is not due to the abnormal set of Ubx proteins but to a breakpoint in a cis-regulatory region.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=552105Documentos Relacionados
- Functionally distinct insulin receptors generated by tissue-specific alternative splicing.
- Multiple Oct2 isoforms are generated by alternative splicing.
- Multiple Oct2 isoforms are generated by alternative splicing
- The dopamine D2 receptor: two molecular forms generated by alternative splicing.
- The two zinc fingers in the human immunodeficiency virus type 1 nucleocapsid protein are not functionally equivalent.
