首页> 外文期刊>Journal of Internal Medicine >Increased lipolysis by secretory phospholipase A(2) group V of lipoproteins in diabetic dyslipidaemia.
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Increased lipolysis by secretory phospholipase A(2) group V of lipoproteins in diabetic dyslipidaemia.

机译:糖尿病性血脂异常的脂蛋白分泌性磷脂酶A(2)组V增加脂解作用。

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BACKGROUND: Lipolysis of lipoproteins by secretory phospholipase A(2) group V (sPLA(2)-V) promotes inflammation, lipoprotein aggregation and foam cell formation--all considered as atherogenic mechanisms. OBJECTIVE: In this study, we compared the susceptibility to sPLA(2)-V lipolysis of VLDL and LDL from individuals with type 2 diabetes and the metabolic syndrome (T2D-MetS) and from healthy controls. Design. VLDL and LDL were isolated from 38 T2D-MetS subjects and 38 controls, treated pair-wise. Extent of sPLA(2)-V lipolysis was measured as release of nonesterified free fatty acids (NEFA). In a subset of the subjects, lipoprotein composition was determined as a relationship between lipid and apolipoprotein components. RESULTS: Mean paired increase in sPLA(2)-V lipolysis after 1 h for T2D-MetS versus control was 2.0 micromol NEFA l(-1) for VLDL (P = 0.004) and 0.75 micromol NEFA l(-1) for LDL (P = 0.001). There were also substantial differences in lipoprotein composition between the groups. T2D-MetS VLDLhad higher triglyceride and cholesterol contents than control VLDL. T2D-MetS LDL was smaller and contained more triglycerides and less cholesterol than control LDL. Both VLDL and LDL from T2D-MetS subjects also contained more apolipoprotein CIII per particle. CONCLUSION: VLDL and LDL from T2D-MetS individuals were more susceptible to sPLA(2)-V lipolysis than those from control individuals. This may result in elevated levels of NEFA and lysophosphatidylcholine, both in circulation and in LDL, possibly contributing to the elevated inflammatory state and increased risk of cardiovascular diseases seen in these individuals.
机译:背景:脂蛋白由分泌磷脂酶A(2)组V(sPLA(2)-V)脂解促进炎症,脂蛋白聚集和泡沫细胞形成-所有这些都被认为是致动脉粥样硬化的机制。目的:在本研究中,我们比较了患有2型糖尿病和代谢综合征(T2D-MetS)的人和健康对照者对sDL-(s)-V脂解VLDL和LDL的敏感性。设计。 VLDL和LDL是从38位T2D-MetS受试者和38位对照中分离出来的,成对治疗。 sPLA(2)-V脂解的程度以未酯化的游离脂肪酸(NEFA)的释放来衡量。在受试者的一个子集中,脂蛋白组成被确定为脂质和载脂蛋白成分之间的关​​系。结果:T2D-MetS与对照组相比,1小时后sPLA(2)-V脂解的平均配对增加为VLDL(2.03)(-1)(-1)(LDL)(P = 0.004)和LDL(-1)(0.75)(-1)(-1)(0.75) P = 0.001)。两组之间脂蛋白组成也存在实质性差异。 T2D-MetS VLDL的甘油三酸酯和胆固醇含量高于对照VLDL。与对照LDL相比,T2D-MetS LDL较小,甘油三酸酯含量更高,胆固醇含量更低。来自T2D-MetS受试者的VLDL和LDL的每个颗粒还含有更多的载脂蛋白CIII。结论:T2D-MetS个体的VLDL和LDL比对照组个体更易受sPLA(2)-V脂解作用。这可能导致循环中和低密度脂蛋白中NEFA和溶血磷脂酰胆碱的水平升高,可能导致这些个体出现炎症状态升高和心血管疾病的风险增加。

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