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细胞生物能量学作为卟啉症患者生物标志物的可行性。

Feasibility of cellular bioenergetics as a biomarker in porphyria patients.

作者信息

Chacko Balu, Culp Matilda Lillian, Bloomer Joseph, Phillips John, Kuo Yong-Fang, Darley-Usmar Victor, Singal Ashwani K

机构信息

Department of Pathology and Mitochondrial Medicine Laboratory, University of Alabama at Birmingham, Birmingham, AL, United States.

Division of Gastroenterology and Hepatology, University of Alabama at Birmingham, Birmingham, AL, United States.

出版信息

Mol Genet Metab Rep. 2019 Jan 29;19:100451. doi: 10.1016/j.ymgmr.2019.100451. eCollection 2019 Jun.

Abstract

Porphyria is a group of metabolic disorders due to altered enzyme activities within the heme biosynthetic pathway. It is a systemic disease with multiple potential contributions to mitochondrial dysfunction and oxidative stress. Recently, it has become possible to measure mitochondrial function from cells isolated from peripheral blood (cellular bioenergetics) using the XF96 analyzer (). Mitochondrial respiration in these cells is measured with the addition of activators and inhibitors of respiration. The output is measured as the O consumption rate (OCR) at basal conditions, ATP linked, proton leak, maximal, reserve capacity, non-mitochondrial, and oxidative burst. We performed cellular bioenergetics on 22 porphyria (12 porphyria cutanea tarda (PCT), seven acute hepatic porphyria (AHP), and three erythropoietic protoporphyria (EPP)) patients and 18 age and gender matched healthy controls. Of porphyria cases, eight were active (2 PCT, 1 EPP, and 5 AHP) and 14 in biochemical remission. The OCR were decreased in patients compared to healthy controls. The bioenergetic profile was significantly lower when measuring proton leak and the non-mitochondrial associated OCR in the eight active porphyria patients when compared to 18 healthy controls. In conclusion, we demonstrate that the bioenergetic profile and mitochondrial activities assessed in porphyria patients and is different than in healthy control individuals. Further, our novel preliminary findings suggest the existence of a mitochondrial dysfunction in porphyria and this may be used as potential non-invasive biomarker for disease activity. This needs to be assessed with a systematic examination in a larger patient cohort. Studies are also suggested to examine mitochondrial metabolism as basis to understand mechanisms of these findings and deriving mitochondrial based therapies for porphyria.

摘要

卟啉病是一组由于血红素生物合成途径中酶活性改变而导致的代谢紊乱疾病。它是一种全身性疾病,对线粒体功能障碍和氧化应激有多种潜在影响。最近,使用XF96分析仪()从外周血分离的细胞(细胞生物能量学)中测量线粒体功能已成为可能。在这些细胞中,通过添加呼吸激活剂和抑制剂来测量线粒体呼吸。输出结果以基础条件下的氧消耗率(OCR)、ATP相关、质子泄漏、最大、储备能力、非线粒体和氧化爆发来衡量。我们对22例卟啉病患者(12例迟发性皮肤卟啉病(PCT)、7例急性肝卟啉病(AHP)和3例红细胞生成性原卟啉病(EPP))以及18名年龄和性别匹配的健康对照进行了细胞生物能量学研究。在卟啉病病例中,8例处于活动期(2例PCT、1例EPP和5例AHP),14例处于生化缓解期。与健康对照相比,患者的OCR降低。与18名健康对照相比,在测量8例活动期卟啉病患者的质子泄漏和非线粒体相关OCR时,生物能量学特征显著降低。总之,我们证明了卟啉病患者评估的生物能量学特征和线粒体活性与健康对照个体不同。此外,我们的新的初步发现表明卟啉病中存在线粒体功能障碍,这可能用作疾病活动的潜在非侵入性生物标志物。这需要在更大的患者队列中进行系统检查来评估。还建议进行研究,以线粒体代谢为基础来理解这些发现的机制,并推导基于线粒体的卟啉病治疗方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/660b/6355507/3d1b73d18de0/gr1.jpg

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