庚酸和中链支链脂肪酸作为中链酰基辅酶 A 脱氢酶缺乏症的补充治疗。
Heptanoic and medium branched-chain fatty acids as anaplerotic treatment for medium chain acyl-CoA dehydrogenase deficiency.
机构信息
Division of Genetic and Genomic Medicine, Department of Pediatrics, School of Medicine, UPMC Children's Hospital of Pittsburgh, University of Pittsburgh; Pittsburgh, PA 15224, USA.
Division of Genetic and Genomic Medicine, Department of Pediatrics, School of Medicine, UPMC Children's Hospital of Pittsburgh, University of Pittsburgh; Pittsburgh, PA 15224, USA; Department of Human Genetics, School of Public Health, University of Pittsburgh; Pittsburgh, PA 15260, USA.
出版信息
Mol Genet Metab. 2023 Nov;140(3):107689. doi: 10.1016/j.ymgme.2023.107689. Epub 2023 Aug 25.
Triheptanoin (triheptanoylglycerol) has shown value as anaplerotic therapy for patients with long chain fatty acid oxidation disorders but is contraindicated in medium-chain acyl-CoA dehydrogenase (MCAD) deficiency. In search for anaplerotic therapy for patients with MCAD deficiency, fibroblasts from three patients homozygous for the most common mutation, ACADM, were treated with fatty acids hypothesized not to require MCAD for their metabolism, including heptanoic (C7; the active component of triheptanoin), 2,6-dimethylheptanoic (dMC7), 6-amino-2,4-dimethylheptanoic (AdMC7), or 4,8-dimethylnonanoic (dMC9) acids. Their effectiveness as anaplerotic fatty acids was assessed in live cells by monitoring changes in cellular oxygen consumption rate (OCR) and mitochondrial protein lysine succinylation, which reflects cellular succinyl-CoA levels, using immunofluorescence (IF) staining. Krebs cycle intermediates were also quantitated in these cells using targeted metabolomics. The four fatty acids induced positive changes in OCR parameters, consistent with their oxidative catalysis and utilization. Increases in cellular IF staining of succinylated lysines were observed, indicating that the fatty acids were effective sources of succinyl-CoA in the absence of media glucose, pyruvate, and lipids. The ability of MCAD deficient cells to metabolize C7 was confirmed by the ability of extracts to enzymatically utilize C7-CoA as substrate but not C8-CoA. To evaluate C7 therapeutic potential in vivo, Acadm mice were treated with triheptanoin for seven days. Dose dependent increase in plasma levels of heptanoyl-, valeryl-, and propionylcarnitine indicated efficient metabolism of the medication. The pattern of the acylcarnitine profile paralleled resolution of liver pathology including reversing hepatic steatosis, increasing hepatic glycogen content, and increasing hepatocyte protein succinylation, all indicating improved energy homeostasis in the treated mice. These results provide the impetus to evaluate triheptanoin and the medium branched chain fatty acids as potential therapeutic agents for patients with MCAD deficiency.
三庚酸甘油酯(三庚酰基甘油)已被证明对长链脂肪酸氧化障碍患者具有补充代谢物的治疗价值,但对中链酰基辅酶 A 脱氢酶(MCAD)缺乏症患者禁用。为了寻找 MCAD 缺乏症患者的补充代谢物治疗方法,研究人员用假设不需要 MCAD 代谢的脂肪酸处理三位纯合 ACADM 突变患者的成纤维细胞,这些脂肪酸包括庚酸(C7;三庚酸甘油酯的活性成分)、2,6-二甲基庚酸(dMC7)、6-氨基-2,4-二甲基庚酸(AdMC7)或 4,8-二甲基壬酸(dMC9)。通过监测细胞耗氧量(OCR)和线粒体蛋白赖氨酸琥珀酰化的变化来评估它们作为补充代谢物脂肪酸的效果,细胞琥珀酰-CoA 水平用免疫荧光(IF)染色法进行评估。还使用靶向代谢组学方法定量分析了这些细胞中的克雷布斯循环中间产物。这四种脂肪酸诱导 OCR 参数的正向变化,这与它们的氧化催化和利用一致。观察到细胞中琥珀酰化赖氨酸的 IF 染色增加,表明在没有培养基葡萄糖、丙酮酸和脂质的情况下,这些脂肪酸是有效的琥珀酰-CoA 来源。MCAD 缺乏细胞能够代谢 C7 的能力通过提取物能够利用 C7-CoA 作为底物而不是 C8-CoA 来证实。为了评估 C7 在体内的治疗潜力,用三庚酸甘油酯处理 Acadm 小鼠 7 天。血浆中庚酰基、戊酰基和丙酰肉碱水平的剂量依赖性增加表明药物的代谢效率很高。酰基肉碱谱的模式与肝脏病理学的缓解一致,包括逆转肝脂肪变性、增加肝糖原含量和增加肝细胞蛋白琥珀酰化,所有这些都表明治疗小鼠的能量代谢得到改善。这些结果为评估三庚酸甘油酯和中链支链脂肪酸作为 MCAD 缺乏症患者潜在治疗药物提供了动力。
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