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Assays of plasma dehydrocholesteryl esters and oxysterols from Smith-Lemli-Opitz syndrome patients

机译:Smith-Lemli-Opitz综合征患者血浆脱氢胆固醇酯和氧固醇的含量测定

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摘要

Smith-Lemli-Opitz syndrome (SLOS) is caused by mutations in the gene encoding 3β-hydroxysterol-Δ7-reductase and as a result of this defect, 7-dehydrocholesterol (7-DHC) and 8-dehydrocholesterol (8-DHC) accumulate in the fluids and tissues of patients with this syndrome. Both 7- and 8-DHC are susceptible to peroxidation reactions, and several biologically active DHC oxysterols are found in cell and animal models of SLOS. Ex vivo oxidation of DHCs can be a confounding factor in the analysis of these sterols and their esters, and we developed HPLC/MS methods that permit the direct analysis of cholesterol, 7-DHC, 8-DHC, and their esters in human plasma, thus avoiding ex vivo oxidation. In addition, three oxysterols were classified as endogenously formed products by the use of an isotopically-labeled 7-DHC (d7-7-DHC) added to the sample before workup, followed by MS analysis of products formed. Analysis of 17 SLOS plasma samples shows that 8-DHC linoleate correlates better with the SLOS severity score of the patients than other sterols or metabolites, including cholesterol and 7-DHC. Levels of 7-ketocholesterol also correlate with the SLOS severity score. 8-DHC esters should have utility as surrogate markers of severity in SLOS for prognostication and as endpoints in clinical trials.
机译:Smith-Lemli-Opitz综合征(SLOS)是由3β-羟基甾醇-Δ 7 -还原酶编码基因的突变引起的,并且由于该缺陷而导致7-脱氢胆固醇(7-DHC)和8 -脱氢胆固醇(8-DHC)积累在患有这种综合征的患者的体液和组织中。 7-DHC和8-DHC都易于发生过氧化反应,在SLOS的细胞和动物模型中发现了几种具有生物活性的DHC氧固醇。 DHC的离体氧化可能是分析这些固醇及其酯类的一个混杂因素,我们开发了HPLC / MS方法,可以直接分析人血浆中的胆固醇,7-DHC,8-DHC及其酯类,因此避免了离体氧化。另外,通过使用在处理后添加到样品中的同位素标记的7-DHC(d7-7-DHC),将三种氧固醇归类为内源性形成的产物,然后对形成的产物进行MS分析。对17种SLOS血浆样品的分析表明,与其他固醇或代谢物(包括胆固醇和7-DHC)相比,8-DHC亚油酸酯与患者的SLOS严重程度评分相关性更好。 7-酮胆固醇水平也与SLOS严重程度评分相关。 8-DHC酯应作为SLOS严重程度的替代标志物进行预后,并作为临床试验的终点。

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