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外源性补充辅酶Q10可预防HMG-CoA还原酶抑制剂引起的血浆辅酶Q减少。

Exogenous CoQ10 supplementation prevents plasma ubiquinone reduction induced by HMG-CoA reductase inhibitors.

作者信息

Bargossi A M, Grossi G, Fiorella P L, Gaddi A, Di Giulio R, Battino M

机构信息

Dipartimento di Medicina Interna, Universita' di Bologna, Italy.

出版信息

Mol Aspects Med. 1994;15 Suppl:s187-93. doi: 10.1016/0098-2997(94)90028-0.

DOI:10.1016/0098-2997(94)90028-0
PMID:7752830
Abstract

The biosynthetic pathway of the CoQ polyisoprenoid side chain, starting from acetyl-CoA and proceeding through mevalonate and isopentenylpyrophosphate, is the same as that of cholesterol. We performed this study to evaluate whether vastatins (hypocholesterolemic drugs that inhibit HMG-CoA reductase) modify blood levels of ubiquinone. Thirty-four unrelated outpatients with hypercholesterolemia (IIa phenotype) were treated with 20 mg of simvastatin for a 6-month period (group S) or with 20 mg of simvastatin plus 100 mg CoQ10 (group US). The following parameters were evaluated at time 0, 45, 90, 135 and 180 days: total plasma cholesterol (TC), HDL-cholesterol, LDL-cholesterol (LDL-C), triglycerides (TG), apo A1, apo B and CoQ10 in plasma and platelets. In the S group, there was a marked decrease in TC and LDL-C (from 290.3 mg/dl to 228.7 mg/dl for TC and from 228.7 mg/dl to 167.6 mg/dl for LDL-C) and in plasma CoQ10 levels from 1.08 mg/dl to 0.80 mg/dl. In contrast, in the US group we observed a significant increase of CoQ10 in plasma (from 1.20 to 1.48 mg/dl) while the hypocholesterolemic effect was similar to that observed in the S group. Platelet CoQ10 also decreased in the S group (from 104 to 90 ng/mg) and increased in the US group (from 95 to 145 ng/mg). This study demonstrates that simvastatin lowers both LDL-C and apo B plasma levels together with the plasma and platelet levels of CoQ10, and that CoQ10 therapy prevents both plasma and platelet CoQ10 decrease, without affecting the cholesterol lowering effect of simvastatin.

摘要

辅酶Q多异戊二烯侧链的生物合成途径与胆固醇相同,都是从乙酰辅酶A开始,经过甲羟戊酸和异戊烯基焦磷酸。我们开展这项研究是为了评估他汀类药物(抑制HMG-CoA还原酶的降胆固醇药物)是否会改变血液中辅酶Q的水平。34名无亲缘关系的高胆固醇血症门诊患者(IIa型)接受了为期6个月的治疗,其中一组(S组)服用20毫克辛伐他汀,另一组(US组)服用20毫克辛伐他汀加100毫克辅酶Q10。在第0、45、90、135和180天评估了以下参数:血浆总胆固醇(TC)、高密度脂蛋白胆固醇、低密度脂蛋白胆固醇(LDL-C)、甘油三酯(TG)、载脂蛋白A1、载脂蛋白B以及血浆和血小板中的辅酶Q10。在S组中,TC和LDL-C显著降低(TC从290.3毫克/分升降至228.7毫克/分升,LDL-C从228.7毫克/分升降至167.6毫克/分升),血浆辅酶Q10水平从1.08毫克/分升降至0.80毫克/分升。相比之下,在US组中,我们观察到血浆中辅酶Q10显著增加(从1.20毫克/分升增至1.48毫克/分升),而降胆固醇效果与S组相似。S组中血小板辅酶Q10也降低了(从104降至90纳克/毫克),US组中则升高了(从95升至145纳克/毫克)。这项研究表明,辛伐他汀降低了LDL-C和载脂蛋白B的血浆水平以及血浆和血小板中的辅酶Q10水平,并且辅酶Q10治疗可防止血浆和血小板中辅酶Q10降低,同时不影响辛伐他汀的降胆固醇效果。

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