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Total sulfane sulfur bioavailability reflects ethnic and gender disparities in cardiovascular disease

机译:硫磺的总生物利用度反映了心血管疾病的种族和性别差异

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Hydrogen sulfide (H2S) has emerged as an important physiological and pathophysiological signaling molecule in the cardiovascular system influencing vascular tone, cytoprotective responses, redox reactions, vascular adaptation, and mitochondrial respiration. However, bioavailable levels of H2S in its various biochemical metabolite forms during clinical cardiovascular disease remain poorly understood. We performed a case-controlled study to quantify and compare the bioavailability of various biochemical forms of H2S in patients with and without cardiovascular disease (CVD). In our study, we used the reverse-phase high performance liquid chromatography monobromobimane assay to analytically measure bioavailable pools of H2S. Single nucleotide polymorphisms (SNPs) were also identified using DNA Pyrosequencing. We found that plasma acid labile sulfide levels were significantly reduced in Caucasian females with CVD compared with those without the disease. Conversely, plasma bound sulfane sulfur levels were significantly reduced in Caucasian males with CVD compared with those without the disease. Surprisingly, gender differences of H2S bioavailability were not observed in African Americans, although H2S bioavailability was significantly lower overall in this ethnic group compared to Caucasians. We also performed SNP analysis of H2S synthesizing enzymes and found a significant increase in cystathionine gamma-lyase (CTH) 1364?G-T allele frequency in patients with CVD compared to controls. Lastly, plasma H2S bioavailability was found to be predictive for cardiovascular disease in Caucasian subjects as determined by receiver operator characteristic analysis. These findings reveal that plasma H2S bioavailability could be considered a biomarker for CVD in an ethnic and gender manner. Cystathionine gamma-lyase 1346?G-T SNP might also contribute to the risk of cardiovascular disease development.
机译:硫化氢(H 2 S)已成为心血管系统中影响血管紧张度,细胞保护反应,氧化还原反应,血管适应性和线粒体呼吸作用的重要生理和病理生理信号分子。然而,人们对临床心血管疾病中各种生化代谢物形式的H 2 S的生物利用水平的了解仍然很少。我们进行了一项病例对照研究,以量化和比较各种有无心血管疾病(CVD)患者H 2 S的生化形式的生物利用度。在我们的研究中,我们使用反相高效液相色谱单溴二苯胺测定法来分析测量H 2 S的生物利用度。单核苷酸多态性(SNPs)也使用DNA焦磷酸测序进行了鉴定。我们发现与没有该疾病的女性相比,患有CVD的白种女性的血浆酸不稳定硫化物水平显着降低。相反,与未患该病的男性相比,患有CVD的白人男性的血浆结合的硫烷硫水平显着降低。令人惊讶的是,尽管与白人相比,该族裔人群中H 2 S的生物利用度总体上显着降低,但在非洲裔美国人中并未观察到H 2 S的生物利用度存在性别差异。我们还对H 2 合成酶进行了SNP分析,发现与对照组相比,CVD患者的胱硫醚γ-裂合酶(CTH)1364ΔG-T等位基因频率显着增加。最后,通过接受者操作者特征分析确定,血浆H 2 S生物利用度可预测白种人受试者的心血管疾病。这些发现表明血浆H 2 S的生物利用度可以被认为是种族和性别的CVD生物标志物。胱硫醚γ-裂合酶1346?G-T SNP也可能导致心血管疾病的发展。

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