Small-molecule inhibitors of ferrochelatase are antiangiogenic agents

Activity of the heme synthesis enzyme ferrochelatase (FECH) is implicated in multiple diseases. In particular, it is a mediator of neovascularization in the eye and thus an appealing therapeutic target for preventing blindness. However, no drug-like direct FECH inhibitors are known. Here, we set out to identify small-molecule inhibitors of FECH as potential therapeutic leads using a high-throughput screening approach to identify potent inhibitors of FECH activity. A structure-activity relationship study of a class of triazolopyrimidinone hits yielded drug-like FECH inhibitors. These compounds inhibit FECH in cells, bind the active site in cocrystal structures, and are antiangiogenic in multiple in vitro assays. One of these promising compounds was antiangiogenic in vivo in a mouse model of choroidal neovascularization. This foundational work may be the basis for new therapeutic agents to combat not only ocular neovascularization but also other diseases characterized by FECH activity.

Keywords

angiogenesis, choroid, endothelial, ferrochelatase, heme, inhibitor, neovascularization, screening, structure-activity relationship, triazolopyrimidinone

Cite As

Sishtla, K., Lambert-Cheatham, N., Lee, B., Han, D. H., Park, J., Sardar Pasha, S. P. B., Lee, S., Kwon, S., Muniyandi, A., Park, B., Odell, N., Waller, S., Park, I. Y., Lee, S. J., Seo, S.-Y., & Corson, T. W. (2022). Small-molecule inhibitors of ferrochelatase are antiangiogenic agents. Cell Chemical Biology. https://doi.org/10.1016/j.chembiol.2022.01.001

ISSN

2451-9456

Journal

Cell Chemical Biology

Rights

IUPUI Open Access Policy

Source

Author

Type

Article

Permanent Link

https://hdl.handle.net/1805/28030

DOI

https://doi.org/10.1016/j.chembiol.2022.01.001

Version

Author's manuscript

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Open Access Policy Articles
Department of Ophthalmology Works

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