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Literature DB >> 20456960

Synthesis and evaluation of verticipyrone analogues as mitochondrial complex I inhibitors.

Simon J Leiris¹, Omar M Khdour, Zachary J Segerman, Krystal S Tsosie, Jean-Charles Chapuis, Sidney M Hecht.

Abstract

Verticipyrone has recently been isolated from the culture broth of Verticillium sp. and shown to inhibit NADH fumarate reductase, as well as NADH oxidoreductase (complex I) of the mitochondrial electron transport chain. In order to assess the structural elements in verticipyrone essential for complex I inhibitor, 15 structural analogues were prepared and analyzed for their effects on mitochondrial NADH oxidoreductase and NADH oxidase activities. Also measured were the abilities of several of the analogues to inhibit respiration as judged by a shift to glycolysis, and to inhibit the growth of several mammalian cell lines. The nature of the pyrone ring was shown to be important to potency of inhibition, as was the length and nature of substituents in the side chain of the analogues. Copyright 2010 Elsevier Ltd. All rights reserved.

Entities: CellLine Chemical Disease Gene Species

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Year: 2010 PMID： 20456960 PMCID： PMC6426446 DOI： 10.1016/j.bmc.2010.03.070

Source DB: PubMed Journal: Bioorg Med Chem ISSN： 0968-0896 Impact factor: 3.641

17 in total

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6. Verticipyrone, a new NADH-fumarate reductase inhibitor, produced by Verticillium sp. FKI-1083.

Authors: Hideaki Ui; Kazuro Shiomi; Hideaki Suzuki; Hiroko Hatano; Hiromi Morimoto; Yuichi Yamaguchi; Rokuro Masuma; Toshiaki Sunazuka; Hiroyuki Shimamura; Kimitoshi Sakamoto; Kiyoshi Kita; Hideto Miyoshi; Hiroshi Tomoda; Satoshi Omura
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Authors: Frank Surup; Oliver Wagner; Jan von Frieling; Michael Schleicher; Stefanie Oess; Peter Müller; Stephanie Grond
Journal: J Org Chem Date: 2007-06-12 Impact factor: 4.354

Synthesis and evaluation of verticipyrone analogues as mitochondrial complex I inhibitors.

1. Total synthesis and biological evaluation of verticipyrone and analogues.

2. Synthesis and characterization of Deltalac-acetogenins that potently inhibit mitochondrial complex I.

3. Novel inhibitors of human histone deacetylases: design, synthesis, enzyme inhibition, and cancer cell growth inhibition of SAHA-based non-hydroxamates.

4. Total synthesis and complete assignment of the stereostructure of a cytotoxic bromotriterpene polyether (+)-aurilol.

5. Pectenotoxin-2 synthetic studies. 2. Construction and conjoining of ABC and DE Eastern hemisphere subtargets.

6. Verticipyrone, a new NADH-fumarate reductase inhibitor, produced by Verticillium sp. FKI-1083.

7. The iromycins, a new family of pyridone metabolites from Streptomyces sp. I. Structure, NOS inhibitory activity, and biosynthesis.

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