Characterization of the mouse transforming growth factor-beta 1 promoter and activation by the Ha-ras oncogene.

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Mol Cell Biol. 1991 January; 11(1): 84-92

Characterization of the mouse transforming growth factor-beta 1 promoter and activation by the Ha-ras oncogene.

A G Geiser, S J Kim, A B Roberts and M B Sporn

Laboratory of Chemoprevention, National Cancer Institute, Bethesda, Maryland 20892.

ABSTRACT

We have cloned and sequenced a mouse genomic transforming growthfactor beta 1 (TGF-beta 1) DNA fragment that includes the 5'untranslated and regulatory regions of the gene. High-sequencehomology with the human TGF-beta 1 gene (66% nucleotide identityin 2.7 kb of DNA upstream of the translational start site) suggestedevolutionary conservation of transcriptional regulation forTGF-beta 1. The absence of TATA or CAAT box sequences but thepresence of several Sp1-binding and AP-2-like sequences in thepromoter region was noted, as previously reported for the humangene. Two transcriptional initiation sites separated by 290bp were identified by S1 nuclease analysis; these correspondedto transcripts with 866 and 576 nucleotides of 5' untranslatedleader sequence. S1 analysis of different mouse tissues indicatedthat the two transcripts were present in the same ratio eventhough the total level of TGF-beta 1 mRNA transcripts variedbetween tissues. Promoter activity adjacent to both transcriptionalstart sites was demonstrated by using chloramphenicol acetyltransferasefusion genes assayed in mouse AKR-2B fibroblast cells. Transcriptionalactivation of the promoter by the Ha-ras oncogene was also demonstrated.The minimal promoter constructs (113 and 104 bp 5' of the firstand second transcriptional start sites, respectively) were sufficientfor induction by Ha-ras. These studies characterize the 5' structureand basal promoter activity of the mouse TGF-beta 1 gene aswell as the transcriptional activation of TGF-beta 1 by theHa-ras oncogene.

Mol Cell Biol. 1991 January; 11(1): 84-92

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