Metabolic rescue ameliorates mitochondrial encephalo‐cardiomyopathy in murine and human iPSC models of Leigh syndrome

Yoon, Ju Yeon; Daneshgar, Nastaran; Chu, Yi; Chen, Biyi; Hefti, Marco M.; Vikram, Ajit; Irani, Kaikobad; Song, Long‐Sheng; Brenner, Charles; Abel, E. Dale; London, Barry; Dai, Dao Fu

doi:10.1002/ctm2.954

Cited by 14 publications

(19 citation statements)

References 49 publications

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“…The NAD + /NADH ratio is essential to maintaining redox balance of the cell, and reduced concentrations of NAD are linked to poor metabolic health in aging and chronic diseases [ 21 , 22 ]. Elevating NAD levels by targeted supplementation has improved health and reversed pathology in animal models of disease [ 23 , 24 ], and NAD enhancing supplements are currently being tested in clinical trials for multiple human conditions [ 25 , 26 , 27 ]. The therapeutic use of NAD+ precursors, such as nicotinamide riboside (NR), as a therapeutic target to compensate for deficits in complex I, is particularly appealing in PD [ 28 ].…”

Section: Introductionmentioning

confidence: 99%

ATP and NAD+ Deficiency in Parkinson’s Disease

et al. 2023

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The goal of this study is to identify a signature of bioenergetic and functional markers in the muscles of individuals with Parkinson’s disease (PD). Quantitative physiological properties of in vivo hand muscle (FDI, first dorsal interosseus) and leg muscle (TA, Tibialis Anterior) of older individuals with PD were compared to historical age/gender-matched controls (N = 30). Magnetic resonance spectroscopy and imaging (MRS) were used to assess in vivo mitochondrial and cell energetic dysfunction, including maximum mitochondrial ATP production (ATPmax), NAD concentrations linked to energy/stress pathways, and muscle size. Muscle function was measured via a single muscle fatigue test. TA ATPmax and NAD levels were significantly lower in the PD cohort compared to controls (ATPmax: 0.66 mM/s ± 0.03 vs. 0.76 ± 0.02; NAD: 0.75 mM ± 0.05 vs. 0.91 ± 0.04). Muscle endurance and specific force were also lower in both hand and leg muscles in the PD subjects. Exploratory analyses of mitochondrial markers and individual symptoms suggested that higher ATPmax was associated with a greater sense of motivation and engagement and less REM sleep behavior disorder (RBD). ATPmax was not associated with clinical severity or individual symptom(s), years since diagnosis, or quality of life. Results from this pilot study contribute to a growing body of evidence that PD is not a brain disease, but a systemic metabolic syndrome with disrupted cellular energetics and function in peripheral tissues. The significant impairment of both mitochondrial ATP production and resting metabolite levels in the TA muscles of the PD patients suggests that skeletal muscle mitochondrial function may be an important tool for mechanistic understanding and clinical application in PD patients. This study looked at individuals with mid-stage PD; future research should evaluate whether the observed metabolic perturbations in muscle dysfunction occur in the early stages of the disease and whether they have value as theragnostic biomarkers.

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Section: Introductionmentioning

confidence: 99%

ATP and NAD+ Deficiency in Parkinson’s Disease

et al. 2023

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Section: Discussionmentioning

confidence: 99%

“…To examine the role of microglia in LS encephalopathy, we used LS mouse model with Ndufs4 −/− , which developed multiple brain lesions, particularly in the brainstem and cerebellum, associated with increase in microglia (Quintana et al, 2010 ; Yoon et al, 2022 ). We showed that partial ablation of microglia by Pexidartinib may confer protective effect and extend lifespan of Ndufs4 −/− mice, but only when it was administered approximately at the onset of neurological symptoms during which activated microglia has been documented (Quintana et al, 2010 ; Aguilar et al, 2022 ; Yoon et al, 2022 ) (late Pexi, Figure 3 ). A plausible explanation for the detrimental effects of early Pexi in depleting microglia is that microglia play critical physiological roles in phagocytosis of cellular debris, secretion of signaling molecules (e.g., neurotrophins) and essential homeostasis during CNS development, maturation and in diseased state (Anderson and Vetter, 2019 ).…”

Section: Discussionmentioning

confidence: 99%

“…Another limitation is the inadequate maturity of iPSC-derived neurons, since in vitro maturation will not match the in-utero growth and development, including the degree of mitochondrial maturation (Dai et al, 2017 ). However, because LS is a disease of very early onset (the age of infant to toddler), iPSC approach has proven to be valuable to model LS (Inak et al, 2021 ; Yoon et al, 2022 ). The recent development of iPSC-derived brain organoids has enabled complex modeling of human diseases, such as those involving interactions of multiple cell types, as we reported here to show increased pro-inflammatory pathways in LS brain organoid.…”

Section: Discussionmentioning

confidence: 99%

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Activated microglia and neuroinflammation as a pathogenic mechanism in Leigh syndrome

Daneshgar

Leidinger

et al. 2023

Front. Neurosci.

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Neuroinflammation is one of the main mechanisms leading to neuronal death and dysfunction in neurodegenerative diseases. The role of microglia as primary mediators of inflammation is unclear in Leigh syndrome (LS) patients. This study aims to elucidate the role of microglia in LS progression by a detailed multipronged analysis of LS neuropathology, mouse and human induced pluripotent stem cells models of Leigh syndrome. We described brain pathology in three cases of Leigh syndrome and performed immunohistochemical staining of autopsy brain of LS patients. We used mouse model of LS (Ndufs4−/−) to study the effect of microglial partial ablation using pharmacologic approach. Genetically modified human induced pluripotent stem cell (iPS) derived neurons and brain organoid with Ndufs4 mutation were used to investigate the neuroinflammation in LS. We reported a novel observation of marked increased in Iba1+ cells with features of activated microglia, in various parts of brain in postmortem neuropathological examinations of three Leigh syndrome patients. Using an Ndufs4−/− mouse model for Leigh syndrome, we showed that partial ablation of microglia by Pexidartinib initiated at the symptom onset improved neurological function and significantly extended lifespan. Ndufs4 mutant LS brain organoid had elevated NLRP3 and IL6 pro-inflammatory pathways. Ndufs4-mutant LS iPSC neurons were more susceptible to glutamate excitotoxicity, which was further potentiated by IL-6. Our findings of LS human brain pathology, Ndufs4-deficient mouse and iPSC models of LS suggest a critical role of activated microglia in the progression of LS encephalopathy. This study suggests a potential clinical application of microglial ablation and immunosuppression during the active phase of Leigh syndrome.

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“…The mechanisms underlying its pathogenesis are not fully understood and no therapies are approved for the treatment of patients with LS. In a new study, Yoon and colleagues 1 shed light on the pathophysiological mechanisms of cardio‐encephalomyopathy in LS and demonstrates that nicotiname riboside (NR) provides significant amelioration in disease models of LS (Figure 1).…”

Section: Figurementioning

confidence: 99%