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两例重症肌无力患者眼部成纤维细胞中的线粒体生物能量学

Mitochondrial bioenergetics in ocular fibroblasts of two myasthenia gravis cases.

作者信息

Europa Tarin A, Nel Melissa, Lebeko Maribanyana R, Heckmann Jeannine M

机构信息

Neurology Research Group, UCT Neurosciences Institute, University of Cape Town, Cape Town, South Africa.

Neurology Division, Department of Medicine, University of Cape Town, Cape Town, South Africa.

出版信息

IBRO Neurosci Rep. 2022 Apr 21;12:297-302. doi: 10.1016/j.ibneur.2022.04.007. eCollection 2022 Jun.

Abstract

Myasthenia gravis (MG) is a rare, treatable, antibody-mediated disease characterized by fatigable muscle weakness of extraocular muscles (EOMs) and non-ocular skeletal muscles. The antibodies are directed against muscle-endplate proteins, most frequently the acetylcholine receptor (AChR) alpha-subunit. Although most MG patients respond to immunosuppressive treatment, some individuals, frequently with African-genetic ancestry, develop treatment-resistant ophthalmoplegia (OP-MG). Although the underlying pathogenetic mechanisms of OP-MG remain unknown, experimental rodent models of MG showed upregulation of genes involved in oxidative metabolism in muscles. EOMs are highly dependent on oxidative metabolism. We opportunistically sampled EOM-tendons of two rare OP-MG patients (and non-MG controls) undergoing re-alignment surgery, and established ocular fibroblast cultures. Metabolic assays were performed on these live cells to assess real-time differences in energy metabolism. To study the cellular bioenergetic profiles in the context of MG, we exposed the cultures to homologous 5% MG sera for 24 h, vs. growth media, from two independent MG patients (with circulating AChR-antibodies) and five controls without MG, and estimated the fold change in oxygen consumption rates in response to three compounds which inhibit different mitochondrial chain complexes. Quantitative PCR (qPCR) was performed in cells before and after MG sera exposure, to assess transcript levels of mitochondrial genes, and which were altered in experimental MG. In response to the mitochondrial stressors, basal oxidative metabolism parameters were similar between OP-MG and control fibroblasts (p = 0.81). However, after exposure to MG sera, bioenergetic parameters (oxygen consumption rate as an indicator of oxidative phosphorylation; extracellular acidification rate as an indicator of glycolysis), were induced to higher levels in OP-MG fibroblasts compared to controls (2.6-fold vs 1.5-fold; p = 0.031) without evidence of mitochondrial insufficiency in the OP-MG ocular fibroblasts. In support of the bioenergetic responses to the same MG sera, gene transcripts of and in ocular fibroblasts also showed significant upregulation (p ≤ 0.041), but similarly in OP-MG and control cases. Taken together we showed similar basal and metabolic adaptive responses after exposure to mitochondrial inhibitors in ocular fibroblasts derived from OP-MG cases and controls, although the OP-MG cells showed greater activation in response to MG conditions. These pilot results in orbital-derived tissues provide support for myasthenic-induced changes in cellular metabolism and evidence that orbital fibroblasts may be useful for dynamic bioenergetic assessments.

摘要

重症肌无力(MG)是一种罕见的、可治疗的、抗体介导的疾病,其特征为眼外肌(EOMs)和非眼部骨骼肌出现易疲劳性肌无力。抗体靶向肌肉终板蛋白,最常见的是乙酰胆碱受体(AChR)α亚基。尽管大多数MG患者对免疫抑制治疗有反应,但一些个体(通常具有非洲遗传血统)会发展为治疗抵抗性眼肌麻痹(OP - MG)。尽管OP - MG的潜在发病机制尚不清楚,但MG的实验性啮齿动物模型显示肌肉中参与氧化代谢的基因上调。眼外肌高度依赖氧化代谢。我们对两名接受重新排列手术的罕见OP - MG患者(以及非MG对照)的眼外肌腱进行了机会性采样,并建立了眼成纤维细胞培养物。对这些活细胞进行代谢测定,以评估能量代谢的实时差异。为了研究MG背景下的细胞生物能量谱,我们将培养物暴露于来自两名独立MG患者(有循环AChR抗体)和五名无MG对照的同源5% MG血清中24小时,与生长培养基相比,并估计了对三种抑制不同线粒体链复合物的化合物反应时氧消耗率的变化倍数。在MG血清暴露前后对细胞进行定量PCR(qPCR),以评估线粒体基因的转录水平,这些基因在实验性MG中发生了改变。响应线粒体应激源时,OP - MG和对照成纤维细胞的基础氧化代谢参数相似(p = 0.81)。然而,暴露于MG血清后,与对照相比,OP - MG成纤维细胞中的生物能量参数(以氧消耗率作为氧化磷酸化的指标;以细胞外酸化率作为糖酵解的指标)被诱导到更高水平(2.6倍对1.5倍;p = 0.031),且OP - MG眼成纤维细胞中没有线粒体功能不全的证据。为了支持对相同MG血清的生物能量反应,眼成纤维细胞中相关基因的转录本也显示出显著上调(p≤0.041),但在OP - MG和对照病例中情况相似。综上所述,我们发现源自OP - MG病例和对照的眼成纤维细胞在暴露于线粒体抑制剂后具有相似的基础和代谢适应性反应,尽管OP - MG细胞在MG条件下表现出更大的激活。这些来自眼眶组织的初步结果为重症肌无力诱导的细胞代谢变化提供了支持,并证明眼眶成纤维细胞可能有助于进行动态生物能量评估。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b047/9210483/e414633bdb0f/gr1.jpg

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