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Regulation of iron homeostasis mediated by the heme-binding protein DAP1 (damage resistance protein 1) via the P450 protein ERG11/CYP51.

J Biol Chem.. 2007-12;  282(50):36543 - 36551
Rolf J. Craven, Julia C. Mallory, and Randal A. Hand. Department of Molecular and Biomedical Pharmacology, University of Kentucky, Lexington, Kentucky 40536, USA.
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摘要

Fungal infections arise frequently in immunocompromised patients, and sterol synthesis is a primary pathway targeted by antifungal drugs. In particular, the P450 protein Erg11/Cyp51 catalyzes a critical step in ergosterol synthesis, and the azole class of antifungal drugs inhibits Erg11. Dap1 is a heme-binding protein related to cytochrome b5 that activates Erg11, so that cells lacking Dap1 accumulate the Erg11 substrate and are hypersensitive to Erg11 inhibitors. Heme binding by Dap1 is crucial for its function, and point mutants in its heme-binding domain render Dap1 inactive for sterol biosynthesis and DNA damage resistance. Like Dap1, the human homologue, PGRMC1/Hpr6, also regulates sterol synthesis and DNA... More

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