Sobetirome: A case history of bench-to-clinic drug discovery and development

Thomas S. Scanlan

doi:10.1007/s10741-008-9122-x

Sobetirome: A case history of bench-to-clinic drug discovery and development

Thomas S. Scanlan

Chemical Physiology and Biochemistry

Research output: Contribution to journal › Review article › peer-review

65 Scopus citations

Abstract

Sobetirome, also known as GC-1 and QRX-431, is a member of a class of compounds known as selective thyromimetics (Scanlan et al., Curr Opin Drug Discov Dev 4:614-622). These compounds are synthetic structural analogs of thyroid hormone that have tissuespecific thyroid hormone actions. Many of the compounds in this class, including sobetirome, also are subtypeselective thyroid hormone receptor (TR) agonists. Sobetirome selectively binds to and activates TRβ over TRα and this receptor selectivity led to the hypothesis that sobetirome would lower cholesterol through activation of liver TRβ without stimulating cardiac function through TRα activation in the heart. The tissue selective thyromimetic properties of sobetirome have been demonstrated in numerous animal models, which led to its clinical development as a novel cholesterol-lowering agent. This review will describe the discovery and development journey of sobetirome as a case history.

Original language	English (US)
Pages (from-to)	177-182
Number of pages	6
Journal	Heart Failure Reviews
Volume	15
Issue number	2
DOIs	https://doi.org/10.1007/s10741-008-9122-x
State	Published - Mar 2010

Keywords

Cardiac-sparing
Cholesterol
GC-1
Thyroid hormone
Thyromimetic

ASJC Scopus subject areas

Cardiology and Cardiovascular Medicine

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10.1007/s10741-008-9122-x

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title = "Sobetirome: A case history of bench-to-clinic drug discovery and development",

abstract = "Sobetirome, also known as GC-1 and QRX-431, is a member of a class of compounds known as selective thyromimetics (Scanlan et al., Curr Opin Drug Discov Dev 4:614-622). These compounds are synthetic structural analogs of thyroid hormone that have tissuespecific thyroid hormone actions. Many of the compounds in this class, including sobetirome, also are subtypeselective thyroid hormone receptor (TR) agonists. Sobetirome selectively binds to and activates TRβ over TRα and this receptor selectivity led to the hypothesis that sobetirome would lower cholesterol through activation of liver TRβ without stimulating cardiac function through TRα activation in the heart. The tissue selective thyromimetic properties of sobetirome have been demonstrated in numerous animal models, which led to its clinical development as a novel cholesterol-lowering agent. This review will describe the discovery and development journey of sobetirome as a case history.",

keywords = "Cardiac-sparing, Cholesterol, GC-1, Thyroid hormone, Thyromimetic",

author = "Scanlan, {Thomas S.}",

note = "Funding Information: Acknowledgments I wish to thank John Baxter and Robert Flett-erick for engaging me in and teaching me about the wonderful field of thyroid hormone action. I wish to further thank my former students and postdocs, particularly Hikari Yoshihara and Grazia Chiellini, for bringing GC-1 to life. A hearty {\textquoteleft}{\textquoteleft}thank you{\textquoteright}{\textquoteright} also goes to all of my collaborators around the world, whose work described here illuminated the utility of GC-1 as a research tool and potential therapeutic agent. I am very grateful to the team at QuatRx Pharmaceuticals who brought sobetirome to life, and who educated and included me in a fascinating journey of drug development. Finally, I am indebted to the National Institute of Diabetes & Digestive & Kidney Diseases of the National Institutes of Health for generous and continuous financial support of this research program.",

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doi = "10.1007/s10741-008-9122-x",

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N2 - Sobetirome, also known as GC-1 and QRX-431, is a member of a class of compounds known as selective thyromimetics (Scanlan et al., Curr Opin Drug Discov Dev 4:614-622). These compounds are synthetic structural analogs of thyroid hormone that have tissuespecific thyroid hormone actions. Many of the compounds in this class, including sobetirome, also are subtypeselective thyroid hormone receptor (TR) agonists. Sobetirome selectively binds to and activates TRβ over TRα and this receptor selectivity led to the hypothesis that sobetirome would lower cholesterol through activation of liver TRβ without stimulating cardiac function through TRα activation in the heart. The tissue selective thyromimetic properties of sobetirome have been demonstrated in numerous animal models, which led to its clinical development as a novel cholesterol-lowering agent. This review will describe the discovery and development journey of sobetirome as a case history.

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Sobetirome: A case history of bench-to-clinic drug discovery and development

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Keywords

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