A novel point mutation of the human glucocorticoid receptor gene causes primary generalized glucocorticoid resistance through impaired interaction with the LXXLL motif of the p160 coactivators: dissociation of the transactivating and transreppressive activities.

[cushing syndrome]

Primary generalized glucocorticoid resistance is a rare genetic disorder characterized by generalized , partial , target-tissue insensitivity to glucocorticoids . The molecular basis of the condition has been ascribed to inactivating mutations in the human glucocorticoid receptor (hGR ) gene .The objective of the study was to present three new cases caused by a novel mutation in the hGR gene and to delineate the molecular mechanisms through which the mutant receptor impairs glucocorticoid signal transduction .T he index case (father ) and his two daughters presented with increased urinary free cortisol excretion and resistance of the hypothalamic -pituitary -adrenal axis to dexamethasone suppression in the absence of clinical manifestations suggestive of Cushing syndrome . All subjects harbored a novel , heterozygous , point mutation (T â†’G ) at nucleotide position 1724 of the hGR gene , which resulted in substitution of valine by glycine at amino acid 575 of the receptor . Compared with the wild-type receptor , the hGRÎ±V 575 G demonstrated a significant (33 %) reduction in its ability to transactivate the mouse mammary tumor virus promoter in response to dexamethasone , a 50 % decrease in its affinity for the ligand , and a 2 .5 -fold delay in nuclear translocation . Although it did not exert a dominant negative effect on the wild-type receptor and preserved its ability to bind to DNA , hGRÎ±V 575 G displayed significantly enhanced (âˆ¼ 80 %) ability to transrepress the nuclear factor -Îº Î’ signaling pathway . Finally , the mutant receptor hGRÎ±V 575 G demonstrated impaired interaction with the LXXLL motif of the glucocorticoid receptor-interacting protein 1 coactivator in vitro and in computer-based structural simulation via its defective activation function-2 (AF-2 ) domain .The natural mutant receptor hGRÎ±V 575 G causes primary generalized glucocorticoid resistance by affecting multiple steps in the glucocorticoid signaling cascade , including the affinity for the ligand , the time required for nuclear translocation , and the interaction with the glucocorticoid-interacting protein-1 coactivator .

Diseases
Validation

Diseases presenting "primary generalized glucocorticoid resistance" symptom

cushing syndrome

A novel point mutation of the human glucocorticoid receptor gene causes primary generalized glucocorticoid resistance through impaired interaction with the LXXLL motif of the p160 coactivators: dissociation of the transactivating and transreppressive activities.

[cushing syndrome]

Diseases presenting "primary generalized glucocorticoid resistance" symptom

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