Mitochondrial Genome Alterations, Cytochrome C Oxidase Activity, and Oxidative Stress: Implications in Primary Open-angle Glaucoma.

Q3 Medicine

Journal of Current Glaucoma Practice Pub Date : 2022-09-01 DOI:10.5005/jp-journals-10078-1376

Kuldeep Mohanty, Swetasmita Mishra, Rima Dada, Tanuj Dada

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Abstract

Aim: To evaluate mitochondrial genome alterations, cytochrome c oxidase (COX) activity, and oxidative stress in primary open-angle glaucoma (POAG).

Methodology: Whole mitochondrial genome was screened in 75 POAG cases and 105 controls by polymerase chain reaction (PCR) sequencing. COX activity was measured from peripheral blood mononuclear cells (PBMCs). A protein modeling study was done to evaluate the impact of G222E variant on protein function. Levels of 8-hydroxy-2-deoxyguanosine (8-OHdG), 8-isoprostane (8-IP), and total antioxidant capacity (TAC) were also measured.

Results: A total of 156 and 79 mitochondrial nucleotide variations were found in the cohort of 75 POAG patients and 105 controls, respectively. Ninety-four (60.26%) variations spanned the coding region, and 62 (39.74%) variations spanned noncoding regions (D-loop, 12SrRNA, and 16SrRNA) of mitochondrial genome in POAG patients. Out of 94 nucleotide changes in coding region, 68 (72.34%) were synonymous changes, 23 (24.46%) non-synonymous, and three (3.19%) were found in the region coding for transfer ribonucleic acid (tRNA). Three changes (p.E192K in ND1, p.L128Q in ND2, and p.G222E in COX2) were found to be pathogenic. Twenty-four (32.0%) patients were positive for either of these pathogenic mitochondrial deoxyribonucleic acid (mtDNA) nucleotide changes. Majority of cases (18.7%) had pathogenic mutation in COX2 gene. Patients who harbored pathogenic mtDNA change in COX2 gene had significantly lower levels of COX activity (p < 0.0001) and TAC (p = 0.004), and higher levels of 8-IP (p = 0.01) as compared to patients who did not harbor this mtDNA. G222E changed the electrostatic potential and adversely impacted protein function of COX2 by affecting nonpolar interactions with neighboring subunits.

Conclusion: Pathogenic mtDNA mutations were present in POAG patients, which were associated with reduced COX activity and increased levels of oxidative stress.

Clinical significance: POAG patients should be evaluated for mitochondrial mutations and oxidative stress and may be managed accordingly with antioxidant therapies.

How to cite this article: Mohanty K, Mishra S, Dada R, et al. Mitochondrial Genome Alterations, Cytochrome C Oxidase Activity, and Oxidative Stress: Implications in Primary Open-angle Glaucoma. J Curr Glaucoma Pract 2022;16(3):158-165.

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线粒体基因组改变、细胞色素C氧化酶活性和氧化应激：原发性开角型青光眼的意义。

目的：评价原发性开角型青光眼（POAG）患者线粒体基因组的改变、细胞色素c氧化酶（COX）活性和氧化应激。从外周血单个核细胞（PBMC）中测量COX活性。进行了蛋白质建模研究，以评估G222E变体对蛋白质功能的影响。还测量了8-羟基-2-脱氧鸟苷（8-OHdG）、8-异丙烷（8-IP）和总抗氧化能力（TAC）的水平。结果：在75名POAG患者和105名对照组中，分别发现156和79个线粒体核苷酸变异。POAG患者线粒体基因组的94个（60.26%）变异跨越编码区，62个（39.74%）变异跨越非编码区（D-环、12SrRNA和16SrRNA）。在编码区的94个核苷酸变化中，68个（72.34%）是同义变化，23个（24.46%）是非同义变化，在编码转移核糖核酸（tRNA）的区域中发现了3个（3.19%）。发现三种变化（ND1中的p.E192K、ND2中的p.L128Q和COX2中的p.G222E）具有致病性。24名（32.0%）患者的这些致病性线粒体脱氧核糖核酸（mtDNA）核苷酸变化均呈阳性。大多数病例（18.7%）存在COX2基因的致病性突变。与未携带该mtDNA的患者相比，携带COX2基因致病性mtDNA变化的患者的COX活性水平（p＜0.0001）和TAC水平（p＝0.004）显著较低，8-IP水平较高（p＝0.01）。G222E通过影响与相邻亚基的非极性相互作用，改变了静电电位并对COX2的蛋白质功能产生不利影响。结论：POAG患者存在致病性mtDNA突变，这与COX活性降低和氧化应激水平升高有关。临床意义：POAG患者应评估线粒体突变和氧化应激，并可通过抗氧化疗法进行相应治疗。如何引用这篇文章：Mohanty K，Mishra S，Dada R等。线粒体基因组改变，细胞色素C氧化酶活性和氧化应激：原发性开角型青光眼的意义。《青光眼临床杂志》2022；16（3）:158-165。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Current Glaucoma Practice Medicine-Ophthalmology

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1.00

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