Therapeutic Potential of VIVIT, a Selective Peptide Inhibitor of Nuclear Factor of Activated T Cells, in Cardiovascular Disorders

Overview

Journal Cardiovasc Drug Rev

Specialties Cardiology & Vascular Diseases
Pharmacology

Date 2007 Jul 7

PMID 17614939

Citations 41

Authors

Haixiang Yu

Theo J C Van Berkel

Erik A L Biessen

Affiliations

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Abstract

Cardiovascular disease is the major cause of death in industrialized nations. Targeted intervention in calcineurin, a calmodulin-dependent, calcium-activated phosphatase and its substrate, nuclear factor of activated T cells (NFAT), was demonstrated to be effective in the treatment of cardiovascular diseases. Although effective in the disruption of calcineurin phosphatase activity, cyclosporin A (CsA) and FK506 also resulted in undesired side effects and toxicity, prompting the discovery of VIVIT, a novel peptide inhibitor. VIVIT selectively and potently inhibits calcineurin/NFAT interaction, but does not compromise calcineurin phosphatase activity and non-NFAT-mediated signaling. VIVIT displays a favorable therapeutic profile as a potential drug candidate and constitutes a useful tool in exploring calcineurin-NFAT functionality. This review describes the development of VIVIT peptide as a selective NFAT inhibitor and its application as a therapeutic agent in cardiovascular disorders including cardiac hypertrophy, restenosis, atherosclerosis, and angiogenesis.

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