The rat alpha-tropomyosin gene generates a minimum of six different mRNAs coding for striated, smooth, and nonmuscle isoforms by alternative splicing.

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Mol Cell Biol. 1988 February; 8(2): 679-694

The rat alpha-tropomyosin gene generates a minimum of six different mRNAs coding for striated, smooth, and nonmuscle isoforms by alternative splicing.

D F Wieczorek, C W Smith and B Nadal-Ginard

Laboratory of Molecular and Cellular Cardiology, Howard Hughes Medical Institute, Boston, Massachusetts.

ABSTRACT

Tropomyosin (TM), a ubiquitous protein, is a component of thecontractile apparatus of all cells. In nonmuscle cells, it isfound in stress fibers, while in sarcomeric and nonsarcomericmuscle, it is a component of the thin filament. Several differentTM isoforms specific for nonmuscle cells and different typesof muscle cell have been described. As for other contractileproteins, it was assumed that smooth, striated, and nonmuscleisoforms were each encoded by different sets of genes. Throughthe use of S1 nuclease mapping, RNA blots, and 5' extensionanalyses, we showed that the rat alpha-TM gene, whose expressionwas until now considered to be restricted to muscle cells, generatesmany different tissue-specific isoforms. The promoter of thegene appears to be very similar to other housekeeping promotersin both its pattern of utilization, being active in most celltypes, and its lack of any canonical sequence elements. Therat alpha-TM gene is split into at least 13 exons, 7 of whichare alternatively spliced in a tissue-specific manner. Thisgene arrangement, which also includes two different 3' ends,generates a minimum of six different mRNAs each with the capacityto code for a different protein. These distinct TM isoformsare expressed specifically in nonmuscle and smooth and striated(cardiac and skeletal) muscle cells. The tissue-specific expressionand developmental regulation of these isoforms is, therefore,produced by alternative mRNA processing. Moreover, structuraland sequence comparisons among TM genes from different phylasuggest that alternative splicing is evolutionarily a very oldevent that played an important role in gene evolution and mighthave appeared concomitantly with or even before constitutivesplicing.

Mol Cell Biol. 1988 February; 8(2): 679-694

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