AI Article Synopsis

  • The StAR gene produces two mRNA forms (1.6 kb and 3.5 kb) that differ mainly in the length of their 3'-UTR due to alternative polyadenylation.
  • Br-cAMP selectively stimulates the production of the more unstable 3.5 kb mRNA, which degrades rapidly after Br-cAMP is removed, while the 1.6 kb mRNA degrades more slowly.
  • The instability of the 3.5 kb mRNA is influenced by its 3'-UTR and requires specific sequences, and this selective synthesis may help the cell quickly adjust StAR activity in response to changes in the environment.

Article Abstract

The steroidogenic acute regulator (StAR) gene is transcribed to 1.6 kb and 3.5 kb mRNAs that differ only through the length of the 3'-untranslated region (3'-UTR). These forms result from alternative polyadenylation sites in exon 7. These sites are utilized similarly in unstimulated adrenal cells whereas Br-cAMP selectively stimulates 3.5 kb mRNA. After removal of Br-cAMP, 3.5 kb mRNA declines rapidly (t(1/2) = 2 h) while 1.6 kb mRNA responds more slowly. This selective degradation is more evident in testis MA10 cells and is seen even in the presence of Br-cAMP. Transfection of Y-1 cells with CMV promoted StAR vectors confirmed that the 3.5 kb form is less stable and that Br-cAMP slowly increases this instability. Basal instability resides solely in the extended 3'-UTR which contains AU-rich elements. Br-cAMP enhances this degradation of 3.5 kb mRNA but additionally requires translated and 5'-UTR sequences. Degradation of both forms is arrested by inhibitors of transcription or translation, indicating that mRNA stability is coupled to these processes independent of the extended 3'-UTR. Br-cAMP stimulates substantial selective synthesis of 3.5 kb StAR mRNA despite this instability. The preferential generation of the unstable form may facilitate rapid increases and decreases of StAR activity in response to external changes.

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Source
http://dx.doi.org/10.1016/j.jsbmb.2005.02.011DOI Listing

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