血清线粒体抑制物质在评估肾脏危害中的临床价值:韩国一项社区前瞻性研究。

Endocrinology and metabolism (Seoul, Korea) Pub Date : 2021-12-01 Epub Date: 2021-11-26 DOI:10.3803/EnM.2021.1226
Hoon Sung Choi, Jin Taek Kim, Hong Kyu Lee, Wook Ha Park, Youngmi Kim Pak, Sung Woo Lee
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引用次数: 1

摘要

背景:线粒体功能障碍与几种肾脏疾病密切相关。然而,没有研究评估血清线粒体抑制物质(MIS)和芳烃受体配体(AhRL)水平对肾脏的潜在危害。方法:我们使用了安松市一个前瞻性社区队列的1511名参与者的血清MIS和AhRL水平和临床肾脏预后。MIS的评估基于细胞内三磷酸腺苷(MIS- atp)或活性氧(MIS- ros)的产生。结果:在平均6.9年的随访期间,84名参与者(5.6%)肾功能迅速下降。在MIS-ATP最低四分位数组中,患者年龄较大且具有代谢有害参数。在多因素logistic回归分析中,较高的MIS-ATP与快速下降的几率降低相关:比值比(OR)增加1%为0.977(95%可信区间[CI], 0.957 ~ 0.998;P=0.031),而较高的MIS-ROS与快速衰退的几率增加略有相关(OR, 1.014;95% CI, 0.999 ~ 1.028;P = 0.055)。然而,血清AhRL与肾功能的快速下降无关。在亚组分析中,MIS对肾脏的危害在高血压和低基线肾功能的人群中尤为明显。结论:血清MIS与肾功能快速下降独立相关,而血清AhRL与肾功能快速下降无关。肾脏危害对血清MIS的临床意义需要在未来的研究中进一步评估。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Clinical Value of Serum Mitochondria-Inhibiting Substances in Assessing Renal Hazards: A Community-Based Prospective Study in Korea.

Clinical Value of Serum Mitochondria-Inhibiting Substances in Assessing Renal Hazards: A Community-Based Prospective Study in Korea.

Background: Mitochondrial dysfunction is strongly associated with several kidney diseases. However, no studies have evaluated the potential renal hazards of serum mitochondria-inhibiting substance (MIS) and aryl hydrocarbon receptor ligand (AhRL) levels.

Methods: We used serum level of MIS and AhRL and clinical renal outcomes from 1,511 participants of a prospective community-based cohort in Ansung. MIS was evaluated based on intracellular adenosine triphosphate (MIS-ATP) or reactive oxygen species (MIS-ROS) generation measured using cell-based assays.

Results: During a mean 6.9-year follow-up, 84 participants (5.6%) developed a rapid decline in kidney function. In the lowest quartile group of MIS-ATP, patients were older and had metabolically deleterious parameters. In multivariate logistic regression analysis, higher MIS-ATP was associated with decreased odds for rapid decline: the odds ratio (OR) of 1% increase was 0.977 (95% confidence interval [CI], 0.957 to 0.998; P=0.031), while higher MIS-ROS was marginally associated with increased odds for rapid decline (OR, 1.014; 95% CI, 0.999 to 1.028; P=0.055). However, serum AhRL was not associated with the rapid decline in kidney function. In subgroup analysis, the renal hazard of MIS was particularly evident in people with hypertension and low baseline kidney function.

Conclusion: Serum MIS was independently associated with a rapid decline in kidney function, while serum AhRL was not. The clinical implication of renal hazard on serum MIS requires further evaluation in future studies.

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