2003
DOI: 10.1021/jm021080f
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Thyroid Receptor Ligands. 1. Agonist Ligands Selective for the Thyroid Receptor β1

Abstract: Endogenous thyroid receptor hormones 3,5,3',5'-tetraiodo-l-thyronine (T(4), 1) and 3,5,3'-triiodo-l-thyronine (T(3), 2) exert a significant effects on growth, development, and homeostasis in mammals. They regulate important genes in intestinal, skeletal, and cardiac muscles, the liver, and the central nervous system, influence overall metabolic rate, cholesterol and triglyceride levels, and heart rate, and affect mood and overall sense of well being. The literature suggests many or most effects of thyroid horm… Show more

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Cited by 141 publications
(142 citation statements)
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“…The TR ligand-binding cavity (LBC), like that of other NRs, lies in the core of the C-terminal ligand-binding domain (LBD) (6). TR␤-selective binding of GC-1 (Ϸ5-fold) and KB141 (Ϸ10-fold) is dependent on a single TR subtype-specific residue in the LBC, TR␤Asn-331 and TR␣Ser-277 (7,8). These lie in a hydrophilic region of the LBC that contacts charged groups of the T 3 amino propionate group, and pocket swap mutations that reverse the identity of these residues also reverse TR preference for GC-1 and KB141.…”
mentioning
confidence: 99%
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“…The TR ligand-binding cavity (LBC), like that of other NRs, lies in the core of the C-terminal ligand-binding domain (LBD) (6). TR␤-selective binding of GC-1 (Ϸ5-fold) and KB141 (Ϸ10-fold) is dependent on a single TR subtype-specific residue in the LBC, TR␤Asn-331 and TR␣Ser-277 (7,8). These lie in a hydrophilic region of the LBC that contacts charged groups of the T 3 amino propionate group, and pocket swap mutations that reverse the identity of these residues also reverse TR preference for GC-1 and KB141.…”
mentioning
confidence: 99%
“…These lie in a hydrophilic region of the LBC that contacts charged groups of the T 3 amino propionate group, and pocket swap mutations that reverse the identity of these residues also reverse TR preference for GC-1 and KB141. X-ray structural analysis indicates that TR␤Asn-331 repositions Arg-282 relative to its TR␣ equivalent (Arg-228), and this facilitates hydrogen bond formation between the Arg-282 side chain and the GC-1 or KB141 carboxylate group (7)(8)(9). TR␤-selective binding of GC-24 (Ϸ40-fold) is partly dependent on Asn-331␤ but involves another mechanism (10); ligand occupies the LBC and conserved hydrophobic regions of helices (H) 3 and 11 open to form an extension to the LBC that accommodates a bulky GC-24 phenyl group.…”
mentioning
confidence: 99%
“…The two major subtypes of the thyroid hormone receptors that mediate these responses, TR␣ and TR␤, are the products of different genes and are also differentially processed to each yield two isoforms. It has been argued that modulation of heart rate and rhythm is mediated predominantly by activation of TR␣ 1 (2)(3)(4), and as a result, recent pharmaceutical research efforts have focused on developing specific TR␤ 1 agonists (5)(6)(7)(8).…”
mentioning
confidence: 99%
“…Point of VIEW www.acschemicalbiology.org VOL.1 NO.9 • ACS CHEMICAL BIOLOGY compound 3 (13) and TR␤ bound to T 3 (1) (14) is shown (Figure 2).…”
mentioning
confidence: 99%
“…In contrast, GC-1 (12) and compound 3 (13) are selective agonists of TR␤ because they bind substantially more tightly to this protein subtype. Several available X-ray structures of TRs bound to ligands (13)(14)(15)(16) show that the selective binding of GC-1 (2) and compound 3 to TR␤ appears to result from participation of the carboxylate moiety in a hydrogen bonding network that includes the TR␤ Asn331 residue.…”
mentioning
confidence: 99%