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Dysfunctional High-Density Lipoprotein: An Innovative Target for Proteomics and Lipidomics

机译:功能障碍的高密度脂蛋白:蛋白质组学和脂质组学的创新目标。

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High-Density Lipoprotein-Cholesterol (HDL-C) is regarded as an important protective factor against cardiovascular disease, with abundant evidence of an inverse relationship between its serum levels and risk of cardiovascular disease, as well as various antiatherogenic, antioxidant, and anti-inflammatory properties. Nevertheless, observations of hereditary syndromes featuring scant HDL-C concentration in absence of premature atherosclerotic disease suggest HDL-C levels may not be the best predictor of cardiovascular disease. Indeed, the beneficial effects of HDL may not depend solely on their concentration, but also on their quality. Distinct subfractions of this lipoprotein appear to be constituted by specific protein-lipid conglomerates necessary for different physiologic and pathophysiologic functions. However, in a chronic inflammatory microenvironment, diverse components of the HDL proteome and lipid core suffer alterations, which propel a shift towards a dysfunctional state, where HDL-C becomes proatherogenic, prooxidant, and proinflammatory. This heterogeneity highlights the need for further specialized molecular studies in this aspect, in order to achieve a better understanding of this dysfunctional state; with an emphasis on the potential role for proteomics and lipidomics as valuable methods in the search of novel therapeutic approaches for cardiovascular disease.
机译:高密度脂蛋白胆固醇(HDL-C)被认为是抵抗心血管疾病的重要保护因素,有充分的证据表明其血清水平与心血管疾病的风险以及各种抗动脉粥样硬化,抗氧化剂和抗胆固醇药物之间存在反比关系。炎性特性。然而,在没有过早的动脉粥样硬化性疾病的情况下,以HDL-C浓度较低为特征的遗传综合征的观察结果表明,HDL-C水平可能不是心血管疾病的最佳预测指标。实际上,HDL的有益效果可能不仅取决于其浓度,还取决于其质量。该脂蛋白的不同亚组分似乎由不同生理和病理生理功能所必需的特定蛋白-脂质聚集体组成。然而,在慢性炎性微环境中,HDL蛋白质组和脂质核心的各种成分均发生变化,从而推动向功能失调状态的转变,HDL-C变成促动脉粥样硬化,促氧化剂和促炎。这种异质性凸显了在这方面需要进一步进行专门的分子研究,以便更好地了解这种功能障碍的状态。特别强调蛋白质组学和脂质组学作为寻找心血管疾病新治疗方法的有价值方法的潜在作用。

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