Determinants of coactivator LXXLL motif specificity in nuclear receptor transcriptional activation

EM McInerney, DW Rose, SE Flynn… - Genes & …, 1998 - genesdev.cshlp.org
EM McInerney, DW Rose, SE Flynn, S Westin, TM Mullen, A Krones, J Inostroza, J Torchia
Genes & development, 1998genesdev.cshlp.org
Ligand-dependent activation of gene transcription by nuclear receptors is dependent on the
recruitment of coactivators, including a family of related NCoA/SRC factors, via a region
containing three helical domains sharing an LXXLL core consensus sequence, referred to
as LXDs. In this manuscript, we report receptor-specific differential utilization of LXXLL-
containing motifs of the NCoA-1/SRC-1 coactivator. Whereas a single LXD is sufficient for
activation by the estrogen receptor, different combinations of two, appropriately spaced …
Ligand-dependent activation of gene transcription by nuclear receptors is dependent on the recruitment of coactivators, including a family of related NCoA/SRC factors, via a region containing three helical domains sharing an LXXLL core consensus sequence, referred to as LXDs. In this manuscript, we report receptor-specific differential utilization of LXXLL-containing motifs of the NCoA-1/SRC-1 coactivator. Whereas a single LXD is sufficient for activation by the estrogen receptor, different combinations of two, appropriately spaced, LXDs are required for actions of the thyroid hormone, retinoic acid, peroxisome proliferator-activated, or progesterone receptors. The specificity of LXD usage in the cell appears to be dictated, at least in part, by specific amino acids carboxy-terminal to the core LXXLL motif that may make differential contacts with helices 1 and 3 (or 3′) in receptor ligand-binding domains. Intriguingly, distinct carboxy-terminal amino acids are required for PPARγ activation in response to different ligands. Related LXXLL-containing motifs in NCoA-1/SRC-1 are also required for a functional interaction with CBP, potentially interacting with a hydrophobic binding pocket. Together, these data suggest that the LXXLL-containing motifs have evolved to serve overlapping roles that are likely to permit both receptor-specific and ligand-specific assembly of a coactivator complex, and that these recognition motifs underlie the recruitment of coactivator complexes required for nuclear receptor function.
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