Advanced search
Publication Cover
Molecular and Cellular Biology Volume 21, 2001 - Issue 10
Submit an article Journal homepage
10
Views
11
CrossRef citations to date
0
Altmetric
Transcriptional Regulation

Human TAFII130 Is a Coactivator for NFATp

Loree J. KimDepartment of Chemistry and Biochemistry, University of Colorado at Boulder, Boulder, Colorado80309-0215
,
Anita G. SetoDepartment of Chemistry and Biochemistry, University of Colorado at Boulder, Boulder, Colorado80309-0215
,
Tuan N. NguyenDepartment of Chemistry and Biochemistry, University of Colorado at Boulder, Boulder, Colorado80309-0215
&
James A. GoodrichDepartment of Chemistry and Biochemistry, University of Colorado at Boulder, Boulder, Colorado80309-0215Correspondence[email protected]
Pages 3503-3513 | Received 06 Oct 2000, Accepted 20 Feb 2001, Published online: 28 Mar 2023
 
Sample our Bioscience journals, sign in here to start your access, Latest two full volumes FREE to you for 14 days

Abstract

NFATp is one member of a family of transcriptional activators that regulate the expression of cytokine genes. To study mechanisms of NFATp transcriptional activation, we established a reconstituted transcription system consisting of human components that is responsive to activation by full-length NFATp. The TATA-associated factor (TAFII) subunits of the TFIID complex were required for NFATp-mediated activation in this transcription system, since TATA-binding protein (TBP) alone was insufficient in supporting activated transcription. In vitro interaction assays revealed that human TAFII130 (hTAFII130) and itsDrosophila melanogaster homolog dTAFII110 bound specifically and reproducibly to immobilized NFATp. Sequences contained in the C-terminal domain of NFATp (amino acids 688 to 921) were necessary and sufficient for hTAFII130 binding. A partial TFIID complex assembled from recombinant hTBP, hTAFII250, and hTAFII130 supported NFATp-activated transcription, demonstrating the ability of hTAFII130 to serve as a coactivator for NFATp in vitro. Overexpression of hTAFII130 in Cos-1 cells inhibited NFATp activation of a luciferase reporter. These studies demonstrate that hTAFII130 is a coactivator for NFATp and represent the first biochemical characterization of the mechanism of transcriptional activation by the NFAT family of activators.

ACKNOWLEDGMENTS

We thank Tim Hoey, Naoko Tanese, Robert Tjian, and Anne Whalen for reagents and advice. J.A.G. is grateful to Robert Tjian and Tom Cech for their generous support, especially during the early stages of this work.

This research was supported by a Public Health Service grant, GM-55235, from the National Institutes of Health. J.A.G. is currently a Pew Scholar in the Biomedical Sciences and was a Special Fellow of the Leukemia Society of America during the early stages of this work. L.J.K. was supported in part by an NIH Predoctoral Training Grant, T32 GM08345, and by Beverly Sears Dean's Small Grants (University of Colorado).

Log in via your institution

Access through your institution

Log in to Taylor & Francis Online

Restore content access

Restore content access for purchases made as guest
Purchase options * Save for later

PDF download + Online access

  • 48 hours access to article PDF & online version
  • Article PDF can be downloaded
  • Article PDF can be printed
USD 61.00 Add to cart

Issue Purchase

  • 30 days online access to complete issue
  • Article PDFs can be downloaded
  • Article PDFs can be printed
USD 265.00 Add to cart

* Local tax will be added as applicable

Related Research

People also read lists articles that other readers of this article have read.

Recommended articles lists articles that we recommend and is powered by our AI driven recommendation engine.

Cited by lists all citing articles based on Crossref citations.
Articles with the Crossref icon will open in a new tab.