What question did this study set out to answer?

To discover and optimize selective glucocorticoid receptor antagonists that are structurally simplified and demonstrate in vivo activity.

April 10, 2026

Development of Structurally Simplified, Non-azadecalin Glucocorticoid Antagonists which Demonstrate In Vivo Activity

Key Points

To discover and optimize selective glucocorticoid receptor antagonists that are structurally simplified and demonstrate in vivo activity.
Discovery and optimization of piperazine-based GR antagonists
Utilization of insights from relacorilant
Progressing compounds to in vivo proof of concept studies
Identification of several compounds with desired profiles
Three key compounds advanced to in vivo studies
Demonstrated in vivo activity in select compounds

Abstract

Glucocorticoid receptor antagonists (GR antagonists) are a class of compounds developed to inhibit the activation of the glucocorticoid receptor and they have been used to treat a range of conditions such as Cushing's syndrome, diabetes, glaucoma, and depression. We report herein the discovery and optimization of a series of selective piperazine-based GR antagonists and discuss how key learnings from the discovery of relacorilant (CORT125134) were utilized to identify a simplified scaffold. Several compounds were identified with the desired profile and 3 key compounds were progressed to in vivo proof of concept studies.

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Development of Structurally Simplified, Non-azadecalin Glucocorticoid Antagonists which Demonstrate In Vivo Activity

Key Points

Abstract

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