1. Academic Validation
  2. The TRAP220 component of a thyroid hormone receptor- associated protein (TRAP) coactivator complex interacts directly with nuclear receptors in a ligand-dependent fashion

The TRAP220 component of a thyroid hormone receptor- associated protein (TRAP) coactivator complex interacts directly with nuclear receptors in a ligand-dependent fashion

  • Proc Natl Acad Sci U S A. 1998 Jul 7;95(14):7939-44. doi: 10.1073/pnas.95.14.7939.
C X Yuan 1 M Ito J D Fondell Z Y Fu R G Roeder
Affiliations

Affiliation

  • 1 Laboratory of Biochemistry and Molecular Biology, The Rockefeller University, New York, NY 10021, USA.
Abstract

Cognate cDNAs are described for 2 of the 10 thyroid hormone receptor-associated proteins (TRAPs) that are immunopurified with Thyroid Hormone Receptor alpha (TRalpha) from ligand-treated HeLa (alpha-2) cells. Both TRAP220 and TRAP100 contain LXXLL domains found in Other nuclear receptor-interacting proteins and both appear to reside in a single complex with Other TRAPs (in the absence of TR). However, only TRAP220 shows a direct ligand-dependent interaction with TRalpha, and these interactions are mediated through the C terminus of TRalpha and (at least in part) the LXXLL domains of TRAP220. TRAP220 also interacts with Other nuclear receptors [vitamin D receptor, retinoic acid receptor alpha, retinoid X receptor alpha, peroxisome proliferation-activated receptor (PPAR) alpha, PPARgamma and, to a lesser extent, Estrogen Receptor] in a ligand-dependent manner, whereas TRAP100 shows only marginal interactions with Estrogen Receptor, retinoid X receptor alpha, PPARalpha, and PPARgamma. Consistent with these results, TRAP220 moderately stimulates human TRalpha-mediated transcription in transfected cells, whereas a fragment containing the LXXLL motifs acts as a dominant negative inhibitor of nuclear receptor-mediated transcription both in transfected cells (TRalpha) and in cell free transcription systems (TRalpha and vitamin D receptor). These studies indicate that TRAP220 plays a major role in anchoring Other TRAPs to TRalpha during the function of the TRalpha-TRAP complex and, further, that TRAP220 (possibly along with Other TRAPs) may be a global coactivator for the Nuclear Receptor Superfamily.

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