Mutations in thyroid hormone receptor α (TRα), a ligand-inducible transcription factor, cause resistance to thyroid hormone α (RTHα). This disorder is characterized by tissue-specific hormone refractoriness and hypothyroidism due to the inhibition of target gene expression by mutant TRα-corepressor complexes. Using biophysical approaches, we show that RTHα-associated TRα mutants devoid of ligand-dependent transcription activation function unexpectedly retain the ability to bind thyroid hormone. Visualization of the ligand T3 within the crystal structure of a prototypic TRα mutant validates this notion. This finding prompted the synthesis of different thyroid hormone analogues, identifying a lead compound, ES08, which dissociates corepressor from mutant human TRα more efficaciously than T3. ES08 rescues developmental anomalies in a zebrafish model of RTHα and induces target gene expression in TRα mutation-containing cells from an RTHα patient more effectively than T3. Our observations provide proof of principle for developing synthetic ligands that can relieve transcriptional repression by the mutant TRα-corepressor complex for treatment of RTHα.
Structure-Guided Approach to Relieving Transcriptional Repression in Resistance to Thyroid Hormone α.
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作者:Romartinez-Alonso Beatriz, Agostini Maura, Jones Heulyn, McLellan Jayde, Sood D Eilidh, Tomkinson Nicholas, Marelli Federica, Gentile Ilaria, Visser W Edward, Schoenmakers Erik, Fairall Louise, Privalsky Martin, Moran Carla, Persani Luca, Chatterjee Krishna, Schwabe John W R
| 期刊: | Molecular and Cellular Biology | 影响因子: | 2.700 |
| 时间: | 2022 | 起止号: | 2022 Feb 17; 42(2):e0036321 |
| doi: | 10.1128/MCB.00363-21 | ||
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