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Expression of ATP binding cassette-transporter ABCG1 prevents cell death by transporting cytotoxic 7beta-hydroxycholesterol
Authors:Engel Thomas  Kannenberg Frank  Fobker Manfred  Nofer Jerzy-Roch  Bode Guenther  Lueken Aloys  Assmann Gerd  Seedorf Udo
Affiliation:Leibniz-Institute for Arteriosclerosis Research, Westphalian Wilhelms-University, 48149 Muenster, Germany. engeltho@uni-muenster.de
Abstract:Oxysterols result from cholesterol by enzymatic or oxidative processes. Some exert cytotoxic effects leading to necrosis or apoptosis. Detoxification of these compounds mainly occurs in the liver and requires transport from peripheral tissues towards it. Some ATP-binding cassette transporters are involved in export of cytotoxic compounds. In the current study, we investigated whether ABC transporter family member G1 (ABCG1) may be involved in oxysterol transport, since its gene expression is highly responsive to oxysterol loading. TetOff HeLa cells stably expressing ABCG1 showed decreased mass uptake of 7beta-hydroxycholesterol (7beta-HC) whereas that of other physiologically relevant oxysterols was unaffected. Application of 7beta-HC to ABCG1 expressing cells induced hyperpolarization of mitochondrial membrane potential and production of reactive oxygen species, indicating energy consumption by the ATP-binding cassette transporter when it is activated by its correct substrate. Our study points to detoxification as one of potential cellular functions of ABCG1. We assume that ABCG1 protects against 7beta-HC-induced cell death, an important role in prevention of neurodegenerative and cardiovascular disease.
Keywords:ABC, ATP-binding cassette   ABCA1, ABC transporter family member A1   ABCG1, ABC transporter family member G1   DHE, dihydroethidium   HA, heamagglutinin   HC, hydroxycholesterol   LXR, liver-X-receptor   RXR, retinoid-X-receptor   TMRE, tetramethylrhodamine ethyl ester
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