Vella Fanny, Ferry Gilles, Delagrange Philippe, Boutin Jean A
Pharmacologie Moléculaire et Cellulaire, Institut de Recherches Servier, 125, Chemin de Ronde 78290 Croissy-sur-Seine, France.
Biochem Pharmacol. 2005 Dec 19;71(1-2):1-12. doi: 10.1016/j.bcp.2005.09.019. Epub 2005 Oct 25.
Quinone reductase 2 has been discovered in 1961 and rediscovered in 1997. Because of its sequence homology with quinone reductase 1, it has been suspected to detoxify quinones. Ten years later, evidences begin to point to a versatile role of this enzyme. Indeed, QR2 is strongly suspected to be the molecular target of anti-malarian drugs such as chloroquin or paraquine, and of red wine-derived resveratrol that might be responsible for the so-called French paradox. It also is identical to the melatonin binding site MT3, and might therefore be a rationale explanation for the antioxidant role of melatonin. Finally QR2 might be implicated in the toxicity, in vivo, of quinones such as menadione. The present commentary attempts to summarize this information and discusses a series of hypotheses.
醌还原酶2于1961年被发现,并于1997年被重新发现。由于其与醌还原酶1的序列同源性,人们怀疑它能使醌解毒。十年后,证据开始指向这种酶的多种作用。事实上,强烈怀疑QR2是氯喹或帕拉喹等抗疟药物以及可能导致所谓法国悖论的红酒来源白藜芦醇的分子靶点。它也与褪黑素结合位点MT3相同,因此可能是褪黑素抗氧化作用的一个合理的解释。最后,QR2可能与甲萘醌等醌在体内的毒性有关。本评论试图总结这些信息并讨论一系列假设。
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