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Merck

Mosaic dysfunction of mitophagy in mitochondrial muscle disease.

Cell metabolism (2022-01-15)
Takayuki Mito, Amy E Vincent, Julie Faitg, Robert W Taylor, Nahid A Khan, Thomas G McWilliams, Anu Suomalainen
RESUMO

Mitophagy is a quality control mechanism that eliminates damaged mitochondria, yet its significance in mammalian pathophysiology and aging has remained unclear. Here, we report that mitophagy contributes to mitochondrial dysfunction in skeletal muscle of aged mice and human patients. The early disease stage is characterized by muscle fibers with central nuclei, with enhanced mitophagy around these nuclei. However, progressive mitochondrial dysfunction halts mitophagy and disrupts lysosomal homeostasis. Interestingly, activated or halted mitophagy occur in a mosaic manner even in adjacent muscle fibers, indicating cell-autonomous regulation. Rapamycin restores mitochondrial turnover, indicating mTOR-dependence of mitochondrial recycling in advanced disease stage. Our evidence suggests that (1) mitophagy is a hallmark of age-related mitochondrial pathology in mammalian muscle, (2) mosaic halting of mitophagy is a mechanism explaining mosaic respiratory chain deficiency and accumulation of pathogenic mtDNA variants in adult-onset mitochondrial diseases and normal aging, and (3) augmenting mitophagy is a promising therapeutic approach for muscle mitochondrial dysfunction.

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HEPES, BioPerformance Certified, ≥99.5% (titration), suitable for cell culture
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Citocromo c, ≥95% (SDS-PAGE)
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Catalase from bovine liver, lyophilized powder, ≥10,000 units/mg protein
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Anti-phospho-Ubiquitin (Ser65), from rabbit, purified by affinity chromatography
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Anti-Mouse IgG2a (γ2a), CF405S antibody produced in goat, ~2 mg/mL, affinity isolated antibody, buffered aqueous solution