超长链饱和脂肪酸混合物D - 003与聚二十碳烯醇对大鼠体内脂质过氧化的影响。
Effects of D-003, a mixture of very long chain saturated fatty acids, and policosanol on in vivo lipid peroxidation in rats.
作者信息
Pérez Yohani, Más Rosa, González Rosa María, Jiménez Sonia, Molina Vivian
机构信息
Center of Natural Products, National Center for Scientific Research, Havana City, Cuba.
出版信息
Arzneimittelforschung. 2008;58(3):126-30. doi: 10.1055/s-0031-1296481.
BACKGROUND
D-003 and policosanol (CAS 557-61-9), specific and distinct mixtures of high molecular weight primary aliphatic acids and alcohols, respectively, have shown to inhibit lipid peroxidation in vivo, but comparative studies between their effects on lipid peroxidation processes had not been conducted before.
OBJECTIVE
To compare the effects of D-003 and policosanol on markers of lipid peroxidation in vivo in rats.
METHODS
Male Wistar rats were distributed into 9 groups: a control group treated with acacia gum/water vehicle, 4 with policosanol and 4 with D-003, both treatments at 5, 25, 100 and 250 mg/kg. Treatments were administered during 4 weeks.
RESULTS
Both treatments significantly and dose-dependently reduced plasma malondyaldehide (MDA) and total peroxides. Nevertheless, while D-003 was effective from 5 mg/kg, the lowest effective dose of policosanol was 25 mg/kg. The maximal effects of both treatments were obtained with 100 mg/kg, but greater in D-003 than in policosanol group, and the same occurred across all doses tested. MDA concentrations generated with the enzymatic system in liver homogenates were also significantly and dose-dependently inhibited with both treatments. The lowest effective doses of D-003 and policosanol were 5 and 100 mg/kg, respectively, and the highest inhibitions of about 80% (D-003) and 11% (policosanol). D-003 was more effective than policosanol in all comparisons. D-003 was also more effective than policosanol for lowering MDA concentrations generated with the no enzymatic system, but in these conditions policosanol was effective from 25 mg/kg and produced an inhibition somewhat greater (about 29%) than on MDA-generated by the enzymatic system. Both policosanol and D-003 did not modify the activity of endogenous antioxidant enzymes compared with the controls.
CONCLUSIONS
D-003 (5-250 mg/kg) orally administered for 4 weeks was more effective than policosanol for lowering all the lipid peroxidation markers assessed, like plasma MDA and total peroxides, and MDA concentrations generated by the enzymatic and non-enzymatic oxidant systems of liver homogenates. The inhibitions with D-003 were marked and dose-dependent. Neither D-003 nor policosanol modified the activity of enzymes involved in the endogenic antioxidant defensive system.
背景
D - 003和多廿烷醇(CAS 557 - 61 - 9)分别是高分子量伯脂肪酸和醇的特定且不同的混合物,已显示出在体内抑制脂质过氧化的作用,但此前尚未对它们对脂质过氧化过程的影响进行比较研究。
目的
比较D - 003和多廿烷醇对大鼠体内脂质过氧化标志物的影响。
方法
将雄性Wistar大鼠分为9组:一组用阿拉伯胶/水载体处理作为对照组,4组用多廿烷醇处理,4组用D - 003处理,两种处理的剂量均为5、25、100和250 mg/kg。处理持续4周。
结果
两种处理均显著且剂量依赖性地降低了血浆丙二醛(MDA)和总过氧化物。然而,D - 003从5 mg/kg起就有效,而多廿烷醇的最低有效剂量为25 mg/kg。两种处理在100 mg/kg时均达到最大效果,但D - 003组的效果大于多廿烷醇组,且在所有测试剂量下均如此。两种处理对肝匀浆中酶系统产生的MDA浓度也有显著且剂量依赖性的抑制作用。D - 003和多廿烷醇的最低有效剂量分别为5和100 mg/kg,最高抑制率分别约为80%(D - 003)和11%(多廿烷醇)。在所有比较中,D - 003比多廿烷醇更有效。对于降低非酶系统产生的MDA浓度,D - 003也比多廿烷醇更有效,但在这些条件下,多廿烷醇从25 mg/kg起有效,其产生的抑制作用(约29%)比酶系统产生的MDA的抑制作用稍大。与对照组相比,多廿烷醇和D - 003均未改变内源性抗氧化酶的活性。
结论
口服给予D - 003(5 - 250 mg/kg)4周,在降低所有评估的脂质过氧化标志物方面比多廿烷醇更有效,这些标志物包括血浆MDA和总过氧化物,以及肝匀浆酶促和非酶促氧化系统产生的MDA浓度。D - 003的抑制作用显著且呈剂量依赖性。D - 003和多廿烷醇均未改变内源性抗氧化防御系统中相关酶的活性。
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