线粒体 DNA 拷贝数与外周动脉疾病患者的全因死亡率和心血管事件相关。
Mitochondrial DNA copy number is associated with all-cause mortality and cardiovascular events in patients with peripheral arterial disease.
机构信息
From the, Department of Genetics and Pharmacology, Institute of Genetic Epidemiology, Medical University of Innsbruck, Innsbruck, Austria.
Department of Vascular Surgery, Medical University of Innsbruck, Innsbruck, Austria.
出版信息
J Intern Med. 2020 May;287(5):569-579. doi: 10.1111/joim.13027. Epub 2020 Feb 9.
BACKGROUND
Dysfunctional mitochondria have an influence on inflammation and increased oxidative stress due to an excessive production of reactive oxygen species. The mitochondrial DNA copy number (mtDNA-CN) is a potential biomarker for mitochondrial dysfunction and has been associated with various diseases. However, results were partially contrasting which might have been caused by methodological difficulties to quantify mtDNA-CN.
OBJECTIVE
We aimed to investigate whether mtDNA-CN is associated with peripheral arterial disease (PAD) as well as all-cause mortality and cardiovascular events during seven years of follow-up.
METHODS
A total of 236 male patients with PAD from the Cardiovascular Disease in Intermittent Claudication (CAVASIC) study were compared with 249 age- and diabetes-matched controls. MtDNA-CN was measured with a well-standardized plasmid-normalized quantitative PCR-based assay determining the ratio between mtDNA-CN and nuclear DNA.
RESULTS
Individuals in the lowest quartile of mtDNA-CN had a twofold increased risk for PAD which, however, was no longer significant after adjusting for leukocytes and platelets. About 67 of the 236 patients had already experienced a cardiovascular event at baseline and those in the lowest mtDNA-CN quartile had a 2.34-fold increased risk for these events (95% CI 1.08-5.13). During follow-up, 37 PAD patients died and 66 patients experienced a cardiovascular event. Patients in the lowest mtDNA-CN quartile had hazard ratios of 2.66 (95% CI 1.27-5.58) for all-cause-mortality and 1.82 (95% CI 1.02-3.27) for cardiovascular events compared with the combined quartile 2-4 (adjusted for age, smoking, CRP, diabetes, prevalent cardiovascular disease, leukocytes and platelets).
CONCLUSION
This investigation supports the hypothesis of mitochondrial dysfunction in peripheral arterial disease and shows an association of low mtDNA-CNs with all-cause-mortality and prevalent and incident cardiovascular disease in PAD patients with intermittent claudication.
背景
功能失调的线粒体由于活性氧物质的过度产生而影响炎症和增加氧化应激。线粒体 DNA 拷贝数(mtDNA-CN)是线粒体功能障碍的潜在生物标志物,与各种疾病有关。然而,结果部分相互矛盾,这可能是由于定量 mtDNA-CN 的方法学困难造成的。
目的
我们旨在研究 mtDNA-CN 是否与外周动脉疾病(PAD)以及七年随访期间的全因死亡率和心血管事件相关。
方法
将 236 名来自间歇性跛行心血管疾病(CAVASIC)研究的男性 PAD 患者与 249 名年龄和糖尿病匹配的对照组进行比较。使用经过良好标准化的质粒归一化定量 PCR 测定法测量 mtDNA-CN,该测定法确定 mtDNA-CN 与核 DNA 的比率。
结果
mtDNA-CN 最低四分位数的个体患 PAD 的风险增加了两倍,但在调整白细胞和血小板后,这不再具有统计学意义。大约 236 名患者中有 67 名在基线时已经发生了心血管事件,mtDNA-CN 最低四分位数的患者发生这些事件的风险增加了 2.34 倍(95%CI 1.08-5.13)。在随访期间,37 名 PAD 患者死亡,66 名患者发生心血管事件。mtDNA-CN 最低四分位数的患者的全因死亡率和心血管事件的风险比分别为 2.66(95%CI 1.27-5.58)和 1.82(95%CI 1.02-3.27),与四分位 2-4 合并(调整年龄、吸烟、CRP、糖尿病、已确诊的心血管疾病、白细胞和血小板)。
结论
本研究支持外周动脉疾病中线粒体功能障碍的假说,并表明间歇性跛行 PAD 患者中低 mtDNA-CNs 与全因死亡率以及普遍存在和新发心血管疾病相关。
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