Accelerated expansion of pathogenic mitochondrial DNA heteroplasmies in Huntington’s disease

Wang, Yiqin; Guo, Xiaoxian; Ye, Kaixiong; Orth, Michael; Gu, Zhenglong

doi:10.1073/pnas.2014610118

Cited by 27 publications

(28 citation statements)

References 87 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…For example, colonic epithelium has shown that normal aging in associated with an increase in clonal fields lacking OXPHOS activity that are the result of mtDNA mutations (Taylor et al, 2003;Greaves et al, 2014). Similar findings have been observed in stomach, prostate, and small intestines of normally aged individuals, as well as blood of Huntington's disease patients (Fellous et al, 2009;Greaves et al, 2010;Wang et al, 2021).…”

Section: Clonal Expansions In Agingmentioning

confidence: 53%

The Complicated Nature of Somatic mtDNA Mutations in Aging

Sanchez‐Contreras

Kennedy

2022

Front. Aging

View full text Add to dashboard Cite

Mitochondria are the main source of energy used to maintain cellular homeostasis. This aspect of mitochondrial biology underlies their putative role in age-associated tissue dysfunction. Proper functioning of the electron transport chain (ETC), which is partially encoded by the extra-nuclear mitochondrial genome (mtDNA), is key to maintaining this energy production. The acquisition of de novo somatic mutations that interrupt the function of the ETC have long been associated with aging and common diseases of the elderly. Yet, despite over 30 years of study, the exact role(s) mtDNA mutations play in driving aging and its associated pathologies remains under considerable debate. Furthermore, even fundamental aspects of age-related mtDNA mutagenesis, such as when mutations arise during aging, where and how often they occur across tissues, and the specific mechanisms that give rise to them, remain poorly understood. In this review, we address the current understanding of the somatic mtDNA mutations, with an emphasis of when, where, and how these mutations arise during aging. Additionally, we highlight current limitations in our knowledge and critically evaluate the controversies stemming from these limitations. Lastly, we highlight new and emerging technologies that offer potential ways forward in increasing our understanding of somatic mtDNA mutagenesis in the aging process.

show abstract

Section: Clonal Expansions In Agingmentioning

confidence: 53%

The Complicated Nature of Somatic mtDNA Mutations in Aging

Sanchez‐Contreras

Kennedy

2022

Front. Aging

View full text Add to dashboard Cite

show abstract

“…We now turn our attention to potential maladaptive consequences of sustained allostatic load, namely evidence of mitochondrial and cellular allostatic overload. In vitro and in vivo studies have shown that one of the consequences of chronic metabolic stressors, OxPhos defects, and aging is mtDNA instability, manifested as the accumulation of mtDNA defects [50][51][52][53][54] . We also recently demonstrated that mtDNA instability can be induced by OxPhos defects in this cellular lifespan system 27 .…”

Section: Chronic Gc Stress Causes Mtdna Instabilitymentioning

confidence: 99%

“…We next turned our attention to potential maladaptive consequences of sustained allostatic load, namely evidence of allostatic overload. In vitro and in vivo studies have shown that chronic metabolic stressors, primary energetic defects, and aging result in mtDNA instability, which manifest as the accumulation of mtDNA defects (53)(54)(55)(56)(57).…”

Section: Chronic Gc Stress Causes Mtdna Instabilitymentioning

confidence: 99%

Cellular Allostatic Load is linked to Increased Energy Expenditure and Accelerated Biological Aging

Bobba-Alves

Sturm

Lin

et al. 2022

Preprint

View full text Add to dashboard Cite

Stress triggers energy-dependent, anticipatory responses that promote survival, a phenomenon termed allostasis. However, the chronic activation of allostatic responses results in allostatic load (AL) and in the maladaptive state known as allostatic overload. Epidemiological studies show that allostatic load predicts physical and cognitive decline, as well as earlier mortality; yet the manifestations of allostatic load and overload at the cellular level remain unclear. To define the energetic cost and potential detrimental effects of prolonged cellular allostatic load, we developed a longitudinal model of chronic glucocorticoid stress in primary human fibroblasts. Results replicated in three healthy donors demonstrated that chronic stress robustly increased cellular basal energy consumption by 62%. This hypermetabolic state relied on a bioenergetic shift away from glycolysis towards mitochondrial oxidative phosphorylation (OxPhos), supported by an upregulation of mitochondrial biogenesis and increased mitochondrial DNA (mtDNA) density. As in humans where chronic stress accelerates biological aging, chronic allostatic load altered extracellular cytokine and cell-free DNA, caused mtDNA instability, increased the rate of epigenetic aging based on DNA methylation clocks, accelerated telomere shortening, and reduced lifespan (i.e., Hayflick limit). Pharmacological blockade of mitochondrial nutrients uptake normalized OxPhos activity but exacerbated hypermetabolism, which further accelerated telomere shortening and reduced cellular lifespan. Together, these results highlight the increased energetic cost of cellular allostatic load and suggests a mechanism for the transduction of chronic stress into accelerated cellular aging to be examined in humans.

show abstract

“…Disruption of mitochondrial activity may be associated with PD, especially under the dysfunction of PINK1 and Parkin. PINK1 and Parkin are localized in the mitochondria ( Wang et al, 2021 ). PINK1 protects against mitochondrial dysfunction under stress by phosphorylating mitochondrial proteins.…”

Section: Human Neurological Diseases Caused By Dynamic Dysfunction Of Mitochondriamentioning

confidence: 99%

“…HTT mutants could accumulate in the body and trigger DRP1 dysfunction, leading to mitochondrial transport abnormalities and ultimately leading to neuronal apoptosis ( Song et al, 2011 ; Shirendeb et al, 2012 ). Of note, long CAG repeats in HTT could promote the age-dependent expansion of pathogenic mtDNA heteroplasmy in HD lymphoblasts ( Wang et al, 2021 ). Thus, they concluded that mtDNA quality is declining along with the HD’s process, indicating a role of HTT in mtDNA quality control.…”

Section: Human Neurological Diseases Caused By Dynamic Dysfunction Of Mitochondriamentioning

confidence: 99%

Players in Mitochondrial Dynamics and Female Reproduction

Zou

Zhang

et al. 2021

Front. Mol. Biosci.

View full text Add to dashboard Cite

Mitochondrial dynamics (fission and fusion) are essential physiological processes for mitochondrial metabolic function, mitochondrial redistribution, and mitochondrial quality control. Various proteins are involved in regulating mitochondrial dynamics. Aberrant expression of these proteins interferes with mitochondrial dynamics and induces a range of diseases. Multiple therapeutic approaches have been developed to treat the related diseases in recent years, but their curative effects are limited. Meanwhile, the role of mitochondrial dynamics in female reproductive function has attracted progressively more attention, including oocyte development and maturation, fertilization, and embryonic development. Here, we reviewed the significance of mitochondrial dynamics, proteins involved in mitochondrial dynamics, and disorders resulting from primary mitochondrial dynamic dysfunction. We summarized the latest therapeutic approaches of hereditary mitochondrial fusion–fission abnormalities and reviewed the recent advances in female reproductive mitochondrial dynamics.

show abstract

Accelerated expansion of pathogenic mitochondrial DNA heteroplasmies in Huntington’s disease

Cited by 27 publications

References 87 publications

The Complicated Nature of Somatic mtDNA Mutations in Aging

The Complicated Nature of Somatic mtDNA Mutations in Aging

Cellular Allostatic Load is linked to Increased Energy Expenditure and Accelerated Biological Aging

Players in Mitochondrial Dynamics and Female Reproduction

Contact Info

Product

Resources

About