PLoS ONE (Jan 2014)

Fomiroid A, a novel compound from the mushroom Fomitopsis nigra, inhibits NPC1L1-mediated cholesterol uptake via a mode of action distinct from that of ezetimibe.

  • Tomohiro Chiba,
  • Tsuyoshi Sakurada,
  • Rie Watanabe,
  • Kohji Yamaguchi,
  • Yasuhisa Kimura,
  • Noriyuki Kioka,
  • Hirokazu Kawagishi,
  • Michinori Matsuo,
  • Kazumitsu Ueda

DOI
https://doi.org/10.1371/journal.pone.0116162
Journal volume & issue
Vol. 9, no. 12
p. e116162

Abstract

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Hypercholesterolemia is one of the key risk factors for coronary heart disease, a major cause of death in developed countries. Suppression of NPC1L1-mediated dietary and biliary cholesterol absorption is predicted to be one of the most effective ways to reduce the risk of hypercholesterolemia. In a screen for natural products that inhibit ezetimibe glucuronide binding to NPC1L1, we found a novel compound, fomiroid A, in extracts of the mushroom Fomitopsis nigra. Fomiroid A is a lanosterone derivative with molecular formula C30H48O3. Fomiroid A inhibited ezetimibe glucuronide binding to NPC1L1, and dose-dependently prevented NPC1L1-mediated cholesterol uptake and formation of esterified cholesterol in NPC1L1-expressing Caco2 cells. Fomiroid A exhibited a pharmacological chaperone activity that corrected trafficking defects of the L1072T/L1168I mutant of NPC1L1. Because ezetimibe does not have such an activity, the binding site and mode of action of fomiroid A are likely to be distinct from those of ezetimibe.