Prenatal and progressive coenzyme Q10 administration to mitigate muscle dysfunction in mitochondrial disease.

IF 8.9 1区 医学
Juan Diego Hernández-Camacho, Cristina Vicente-García, Lorena Ardila-García, Ana Padilla-Campos, Guillermo López-Lluch, Carlos Santos-Ocaña, Peter S Zammit, Jaime J Carvajal, Plácido Navas, Daniel J M Fernández-Ayala
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引用次数: 0

Abstract

Background: ADCK genes encode aarF domain-containing mitochondrial kinases involved in coenzyme Q (CoQ) biosynthesis and regulation. Haploinsufficiency of ADCK2 in humans leads to adult-onset physical incapacity with reduced mitochondrial CoQ levels in skeletal muscle, resulting in mitochondrial myopathy and alterations in fatty acid β-oxidation. The sole current treatment for CoQ deficiencies is oral administration of CoQ10, which causes only partial recovery with postnatal treatment, underscoring the importance of early diagnosis for successful intervention.

Methods: We used Adck2 heterozygous mice to examine the influence of this gene on muscle structure, function and regeneration throughout development, growth and ageing. This investigation involved techniques including immunohistochemistry, analysis of CoQ levels, mitochondrial respiratory content, muscle transcriptome analysis and functional tests.

Results: We demonstrated that Adck2 heterozygous mice exhibit defects from embryonic development, particularly in skeletal muscle (1102 genes deregulated). Adck2 heterozygous embryos were 7% smaller in size and displayed signs of delayed development. Prenatal administration of CoQ10 could mitigate these embryonic defects. Heterozygous Adck2 mice also showed a decrease in myogenic cell differentiation, with more severe consequences in 'aged' mice (41.63% smaller) (P < 0.01). Consequently, heterozygous Adck2 mice displayed accelerated muscle wasting associated with ageing in muscle structure (P < 0.05), muscle function (less grip strength capacity) (P < 0.001) and muscle mitochondrial respiration (P < 0.001). Furthermore, progressive CoQ10 administration conferred protective effects on mitochondrial function (P < 0.0001) and skeletal muscle (P < 0.05).

Conclusions: Our work uncovered novel aspects of CoQ deficiencies, revealing defects during embryonic development in mammals for the first time. Additionally, we identified the gradual establishment and progression of the deleterious Adck2 mouse phenotype. Importantly, CoQ10 supplementation demonstrated a protective effect when initiated during development.

产前和逐步服用辅酶Q10以缓解线粒体疾病的肌肉功能障碍。
背景:ADCK 基因编码含 aarF 结构域的线粒体激酶,参与辅酶 Q(CoQ)的生物合成和调节。人类 ADCK2 的单倍体缺陷会导致骨骼肌线粒体 CoQ 水平降低,导致线粒体肌病和脂肪酸 β 氧化改变,从而导致成年后的身体机能丧失。目前治疗 CoQ 缺乏症的唯一方法是口服 CoQ10,但这种方法只能在出生后的治疗中导致部分恢复,因此强调了早期诊断对成功干预的重要性:我们利用 Adck2 杂合子小鼠来研究该基因在整个发育、生长和衰老过程中对肌肉结构、功能和再生的影响。这项研究涉及的技术包括免疫组织化学、CoQ 水平分析、线粒体呼吸含量、肌肉转录组分析和功能测试:结果:我们发现 Adck2 杂合子小鼠从胚胎发育开始就表现出缺陷,尤其是在骨骼肌方面(1102 个基因失调)。Adck2杂合子胚胎的体积小7%,并表现出发育延迟的迹象。产前服用 CoQ10 可减轻这些胚胎缺陷。杂合子 Adck2 小鼠的成肌细胞分化也出现下降,"老龄 "小鼠的后果更为严重(小了 41.63%)(P 10):我们的研究发现了 CoQ 缺乏的新方面,首次揭示了哺乳动物胚胎发育过程中的缺陷。此外,我们还发现了 Adck2 小鼠有害表型的逐步建立和发展过程。重要的是,在发育过程中补充 CoQ10 具有保护作用。
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来源期刊
Journal of Cachexia, Sarcopenia and Muscle
Journal of Cachexia, Sarcopenia and Muscle Medicine-Orthopedics and Sports Medicine
自引率
12.40%
发文量
0
期刊介绍: The Journal of Cachexia, Sarcopenia, and Muscle is a prestigious, peer-reviewed international publication committed to disseminating research and clinical insights pertaining to cachexia, sarcopenia, body composition, and the physiological and pathophysiological alterations occurring throughout the lifespan and in various illnesses across the spectrum of life sciences. This journal serves as a valuable resource for physicians, biochemists, biologists, dieticians, pharmacologists, and students alike.
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