Literature DB >> 9349499

Activation of the c-fos SRE through SAP-1a.

H Masutani1, L Magnaghi-Jaulin, S Ait-Si-Ali, R Groisman, P Robin, A Harel-Bellan, S Ait Si Ali.   

Abstract

TCFs, which are members of the Ets family of transcription factors, are recruited to the Serum Response Element (SRE) in the c-fos promoter by SRF. These Ets proteins, which are substrates for the MAP kinases, are direct targets of the Ras/MAP kinase signal transduction pathway. In this paper, we demonstrate that one of the TCFs, SAP-1a, displays a significant level of autonomous binding to the SRE Ets box. In contrast to previous observations, deletion of the SRF binding domain did not modulate the autonomous binding of SAP-1a. Also, the autonomous binding was not modulated by the phosphorylation of SAP-1a by MAP kinases. The autonomous binding was also detected in live cells: transfected SAP-1a was able to restore the response of a CArG-less SRE in PC12 cells. The response occurred in the absence of SRF recruitment since a mutant of SAP-1a in which the B-box, a domain required for interaction with SRF, had been deleted was still able to transactivate the CArG-less SRE. The transactivation was repressed by a Ras transdominant negative mutant, indicating the involvement of the Ras/MAP kinase pathway. Taken together, these data demonstrate that SAP-1a is capable of binding to the c-fos SRE in the absence of SRF.

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Year:  1997        PMID: 9349499     DOI: 10.1038/sj.onc.1201328

Source DB:  PubMed          Journal:  Oncogene        ISSN: 0950-9232            Impact factor:   9.867


  6 in total

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2.  Autonomously binding protein detected on ets box of c-fos serum response element in proliferating cells.

Authors:  H Masutani; L Magnaghi-Jaulin; R Groisman; S Ait-Si-Ali; P Robin; L L Pritchard; A Harel-Bellan
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  6 in total

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