A case of sudden cardiac death due to mitochondrial disease

A 25-year-old, emaciated man without medical treatment was found to have died suddenly at home by his mother. At autopsy, there were no injuries to his body, but significant circulatory insufficiency was observed. Electron microscopy revealed abnormal mitochondria in cells of the cardiac conduction system. The conduction system was filled with mitochondrial size abnormalities and mitochondrial cristae abnormalities. No notable abnormal findings were observed in other organs. Genetic examination of the blood revealed the mitochondrial pathogenetic variant m.3243A>G. Epileptic seizures, diabetic ketoacidosis, and hyperosmolar hyperglycemic state were unlikely to be the cause of sudden death. The cause of death was diagnosed as arrhythmia possibly induced by the failure of the cardiac conduction system due to mitochondrial disease. This is a rare case of sudden death caused by an accumulation of abnormal mitochondria in the cardiac conduction system.     

COX20基因变异线粒体复合物Ⅳ缺乏症相关的遗传性周围神经病4例病例系列报告及文献复习

背景：原发性线粒体病具有高度的临床和遗传异质性，其中周围神经是线粒体病的常见受累器官之一。 目的：总结COX20基因变异相关周围神经病的临床表型及遗传学特征。 设计：病例系列报告。 方法：回顾性收集2018年5月至2020年5月复旦大学附属儿科医院诊治的COX20基因变异相关周围神经病患儿的临床资料，总结其临床表现、基因检测结果及治疗效果，并以“COX20”、“线粒体复合物Ⅳ缺乏症（Complex Ⅳ deficiency）”为关键词检索中英文数据库。检索时间均为从建库至2021年12月。总结已报道COX20基因变异与临床表型的关系。 主要结局指标：临床表型和COX20基因变异位点。 结果：4例患儿纳入分析，男、女各2例，其中3例自幼运动发育落后。4例均在儿童期起病，均以行走不稳为首发症状。肌电图均提示多发性周围神经损害改变，感觉神经轴索受累为主。4例患儿均携带COX20基因复合杂合变异，包括错义变异2个，无义变异和移码变异各1个，其中移码变异c.262delG(p.E88Kfs*35)尚未见报道。文献复习目前共报道COX基因变异18个家系22例患儿（包括本文病例）,起病中位年龄为5（1.0~17）岁，22例均以行走困难或步态不稳起病，11例（50.0%）有精神运动发育迟滞，病程中14例(63.6%)出现构音障碍，14例(63.6%)出现肌力下降和/或足部畸形，8例（36.4%）出现共济失调，6例(27.3%)出现肌张力障碍，5例（22.7%）存在认知倒退等。21例患儿行神经传导及肌电图检查，19例(90.5%)提示多发性周围神经病变。头颅（18例）及脊髓（10例）MR检查提示，脊髓萎缩4例（40%），小脑萎缩4例（22.2%）。9例患儿已无法独立行走，丧失独立行走能力中位年龄为10（7~21）岁。目前共报道9个变异位点，4种变异类型，其中错义变异5个，剪切变异2个，无义变异和移码变异各1个。 结论：COX20基因变异患者多早期起病，以周围神经系统病变为主要表现，可合并构音障碍、共济失调、肌张力障碍、认知倒退等，病情逐渐进展，致残率高。COX20基因变异类型以错义变异最常见。     

补中益气汤对于肝再生线粒体能量代谢的研究概况＊

肝再生的机制非常复杂，线粒体功能障碍所引起的能量供给不足是影响因素之一，但其机理亟待研究。严重肝损害时肝细胞ATP供应减少、线粒体能量代谢异常，导致肝再生受到抑制。补中益气汤为李东垣所创，其具补中益气、升阳举陷之功，有实验证实补中益气汤具有保护线粒体功能、增加线粒体能量代谢的作用，从而促进肝再生。本文综述补中益气汤总方与其中各类中药对线粒体能量代谢的保护作用，从而为促进肝再生提供新的治疗手段并对改善病人预后有重要意义。     

Resolving a 150-year-old paternity case in Mormon history using DTC autosomal DNA testing of distant relatives

Although autosomal DNA testing has been available for a number of years, its use to reconstruct genetic profiles of people that lived centuries in the past is relatively recent and there are no published cases where it was employed to verify a kinship relation, likely to be an alleged paternity, that occurred one and a half century ago.DNA testing has already been employed to study the ancestry and posterity of Joseph Smith Jr., founder of the Latter-day Saint (Mormon) movement. Thanks to information found on the paternally inherited Y chromosome, a number of alleged paternities have been disproved, but obviously this analysis is not effective for alleged daughters. Likewise, his reconstructed mitogenome sequence, reported here for the first time, provides information about his maternal ancestry, but is useless in any paternity questions due to the strict maternal inheritance. Among all the children attributed to Joseph Smith Jr., Josephine Lyon, born in 1844, is perhaps the most frequently mentioned.In the current study, 56 individuals, mostly direct descendants of Joseph Smith Jr. and Josephine Lyon, had their autosomal DNA tested to verify Josephine’s biological paternity. Nearly 600,000 autosomal SNPs from each subject were typed and detailed genealogical data were compiled. The absence of shared DNA between Josephine’s grandson and Joseph Smith Jr.’s five great-grandchildren together with various amounts of autosomal DNA shared by the same individual with four other relatives of Windsor Lyon is a clear indication that Josephine was not related to the Smith, but to the Lyon’s family. These inferences were also verified using kinship analyses and likelihood ratio calculations.     

Methodological considerations for near-infrared spectroscopy to assess mitochondrial capacity after spinal cord injury

Background: Skeletal muscle mitochondrial activity is reduced by?～?50–60% after SCI, resulting in impaired energy expenditure, glucose utilization and insulin sensitivity. Near infra-red spectroscopy (NIRS) is a non-invasive tool that can be used to assess mitochondrial capacity.

Objectives: (1) Highlight methodological limitations impacting data acquisition and analysis such as subcutaneous adipose tissue (SAT) thickness, movement artifacts, inadequate muscle stimulation, light interference, and ischemic discomfort. (2) Provide technical considerations to improve data acquisition and analysis. This may serve as guidance to other researchers and clinicians using NIRS.

Study Design: cross-sectional observational design.

Settings: Clinical research medical center.

Participants: Sixteen men with 1?>?year post motor complete SCI.

Methods: NIRS signals were obtained from right vastus lateralis muscle utilizing a portable system. Signals were fit to a mono-exponential curve.

Outcome Measures: Rate constant and r ² values for the fit curve, indirectly measures mitochondrial capacity.

Results: Only four participants produced data with accepted rate constants of 0.002–0.013?s^?1 and r ² of 0.71–0.87. Applications of studentized residuals ≥2.5 resulted in sparing data from another four participants with rate constants of 0.010–0.018?s^?1and r ² values ranging from 0.86–0.99.

Conclusions: Several limitations may challenge the use of NIRS to assess mitochondrial capacity after SCI. Acknowledging these limitations and applying additional data processing techniques may overcome the discussed limitations and facilitate data sparing.     

Does perturbation in the mitochondrial protein folding pave the way for neurodegeneration diseases?

Mitochondria, which are cell compartments that are widely present in eukaryotic cells, have been shown to be involved in a variety of synthetic, metabolic, and signaling processes, thereby playing a vital role in cells. The mitochondrial unfolded protein response (mtUPR) is a response in which mitochondria reverse the signal to the nucleus and maintain mitochondrial protein homeostasis when unfolded and misfolded proteins continue to accumulate. Multiple neurodegeneration diseases, including Alzheimer's disease (AD), Parkinson’s disease (PD), and familial amyotrophic lateral sclerosis (fALS), are public health challenges. Every year, countless efforts are expended trying to clarify the pathogenesis and treatment of neurological disorders, which are associated with mitochondrial dysfunction to some extent. Numerous studies have shown that mtUPR is involved in and plays an important role in the pathogenesis of neurological disorders, but the exact mechanism of the disorders is still unclear. Further study of the process of mtUPR in neurological disorders can help us more accurately understand their pathogenesis in order to provide new therapeutic targets. In this paper, we briefly review mtUPR signaling in Caenorhabditis elegans (C. elegans) and mammals and summarize the role of mtUPR in neurodegeneration diseases, including AD, PD and fALS.     

莱菔硫烷诱导线粒体裂变抑制血管生成

目的 探讨莱菔硫烷对血管生成的影响及其可能机制。方法 体外实验以原代人脐静脉血管内皮细胞为研究模型，以1‰ 二甲基亚砜（dimethyl sulfoxide，DMSO）干预作为对照。应用WST-1试剂盒检测不同浓度莱菔硫烷（5～100μmol/L）对原代人脐静脉血管内皮细胞增殖活性的影响，采用小管形成实验和Transwell迁移实验分析莱菔硫烷干预（10μmol/L）对原代人脐静脉血管内皮细胞管腔生成、迁移能力的影响，采用Mito-Tracker Green FM染料标记线粒体结合共聚焦显微镜成像技术观察莱菔硫烷（10μmol/L）干预后线粒体形态学改变，以及蛋白免疫印迹法检测线粒体动态相关蛋白包括线粒体融合蛋白1/2、动力相关蛋白1表达水平，以及血管内皮生长因子的蛋白表达。结果 5μmol/L莱菔硫烷干预24h对人脐静脉血管内皮细胞增殖活性无显著影响，而 ≥ 10μmol/L 莱菔硫烷干预则抑制了人脐静脉血管内皮细胞活性，10、20、40、80、100μmol/L干预组抑制率分别为（17.82±5.80）%（P=0.009）、（35.33±6.26）%（P<0.001）、（65.29±4.26）%（P<0.001）、（66.82±3.94）%（P<0.001）及（68.05±2.54）%（P<0.001），IC50为38.15μmol/L。为避免过高干预剂量所致严重毒性效应，我们将选取10μmol/L作为主要干预剂量。与对照组相比，10μmol/L 莱菔硫烷干预显著抑制人脐静脉血管内皮细胞血管生成能力，其中迁移能力降低了（42.98±9.21）%（P=0.018），而管腔样结构形成能力，包括管腔数量、节点数和管腔总长度则分别降低了（83.94±18.36）%（P=0.011）、（59.22±25.60）%（P=0.021）及（50.49±23.44）%（P=0.025）。人脐静脉血管内皮细胞血管生成能力被莱菔硫烷抑制同时，伴有线粒体动态紊乱、线粒体裂变的发生。相对于对照组而言，10μmol/L 莱菔硫烷干预组线粒体网络数、纵横比显著减少（27.39±22.46）%（P=0.006）、（11.37±8.26）%（P<0.001），而圆度显著增加（11.97±12.07）%（P<0.001）。与此相对应的是，10μmol/L莱菔硫烷干预显著上调促裂变蛋白而抑制促融合蛋白表达，动力相关蛋白1表达相当于对照组的（1.71±0.039）倍（P<0.001），而线粒体融合蛋白1/2表达则分别相当于对照组的（59.30+1.50）%（P=0.006）和（74.75±11.84）%（P=0.031）。同时，血管内皮生长因子蛋白表达则相当于对照组的（65.66±9.49）%（P=0.003）。结论 莱菔硫烷具有抑制血管生成活性，其机制可能与其促进血管内皮细胞线粒体裂变有关。     

以脾胃为中心的葛根相关配伍对糖尿病心肌病大鼠受损心肌线粒体的改善作用

目的:观察葛根及其配伍对糖尿病心肌病(DCM)大鼠心肌线粒体质量变化的影响,探寻治疗糖尿病心肌病的最优配伍及机制。方法:采用链脲佐菌素腹腔注射进行模型大鼠制备,并将60只成模大鼠随机分为模型组6.5 g/(kg·d)、达美康组16.7 mg/(kg·d)、葛根组1.04 g/(kg·d)、葛芪组2.6 g/(kg·d)、葛参组2.6 g/(kg·d)、葛蒌组4.48g/(kg·d)及葛芪参蒌组7.6 g/(kg·d)各8只,同时选取空白大鼠8只,为对照组6.5 g/(kg·d)。各组依据上述剂量,以相应药物持续灌胃9周后,对比各组心肌线粒体超微结构变化、心肌线粒体膜电位变化及心肌ATP变化情况。结果:电镜显示各药物干预组心肌线粒体超微结构较模型组均有不同程度的改善,其中葛芪参蒌组改善效果最为明显,与空白组无明显差异; 流式细胞仪检测显示:各干预组波峰均在模型组、空白组之间; 其中葛芪参蒌组、葛参组、葛根组波峰位于达美康组右侧; 葛芪组、葛蒌组则位于达美康组左侧; 以葛芪参蒌组波峰与空白组最为接近。心肌ATP浓度检测显示:各中药干预组心肌ATP浓度均较模型组有所提升(P<0.05),其中葛芪参蒌组ATP值较其余各干预组提升最为明显(P<0.05),但仍低于空白组(P>0.05)。结论:葛根相关配伍均能够对心肌线粒体结构、心肌线粒体膜电位进行正向调控,进而使因糖尿病心肌病导致的心肌线粒体受损得以恢复,其中以益气、化瘀、祛痰三法合用的组方原则进行配伍的葛芪参蒌方改善效果最优。可见其治疗机制可能是通过益气、化瘀、祛痰的协同作用,正向调控心肌线粒体质量而达到治疗目的。