Structural Mechanism of a Partial Glucocorticoid Receptor Agonist Functioning as a Mineralocorticoid Receptor Antagonist
Xu Liu

TL;DR
This paper explains how vamorolone, a drug for muscular dystrophy, works as a glucocorticoid receptor agonist and mineralocorticoid receptor antagonist, reducing inflammation without harmful side effects.
Contribution
The study reveals the structural mechanism of vamorolone's dual action through X-ray crystallography and biochemical analysis.
Findings
Vamorolone acts as a partial GR agonist and MR antagonist due to the absence of a key hydrogen bond.
The drug's unique binding profile alters coregulator interactions and gene expression to avoid side effects.
Structural insights suggest a new approach for designing drugs with anti-inflammatory and cardiac-protective benefits.
Abstract
The Glucocorticoid Receptor (GR) and Mineralocorticoid Receptor (MR) are homologous ligand-activated transcription factors that regulate extensive downstream gene expression networks involved in metabolism, development, electrolyte homeostasis, and inflammation. Various GR agonists have been developed for their anti-inflammatory effects in treating diverse disorders. However, many GR agonists also act as MR agonists, leading to undesirable side effects such as increased cardiac fibrosis and cardiomyopathy. MR antagonists are typically developed to circumvent the defects caused by MR overactivation, providing cardiac-protective benefits. Vamorolone is a recently FDA-approved drug that represents a most promising treatment by simultaneously suppressing inflammation and cardiomyopathy in Duchenne muscular dystrophy (DMD) patients. It acts on both GR and MR but avoids safety concerns of…
Genes, proteins, chemicals, diseases, species, mutations and cell lines named across the full text — each resolved to its canonical identifier and authoritative record.
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Taxonomy
TopicsHormonal Regulation and Hypertension · Estrogen and related hormone effects · Ion Transport and Channel Regulation
