Mitochondrial Microheteroplasmy and a Theory of Aging and Age-related Disease

Overview

Journal Rejuvenation Res

Specialties Geriatrics
Physiology

Date 2005 Sep 8

PMID 16144471

Citations 27

Authors

Rafal M Smigrodzki

Shaharyar M Khan

Affiliations

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Abstract

We implicate a recently described form of mitochondrial mutation, mitochondrial microheteroplasmy, as a candidate for the principal component of aging. Microheteroplasmy is the presence of hundreds of independent mutations in one organism, with each mutation usually found in 1-2% of all mitochondrial genomes. Despite the low abundance of single mutations, the vast majority of mitochondrial genomes in all adults are mutated. This mutational burden includes inherited mutations, de novo germline mutations, as well as somatic mutations acquired either during early embryonic development or later in adult life. We postulate that microheteroplasmy is sufficient to explain the pathomechanism of several age-associated diseases, especially in conditions with known mitochondrial involvement, such as diabetes (DM), cardiovascular disease, Parkinson's disease (PD), and Alzheimer's disease (AD) and cancer. The genetic properties of microheteroplasmy reconcile the results of disease models (cybrids, hypermutable PolG variants and mitochondrial toxins), with the relatively low levels of maternal inheritance in the aforementioned diseases, and provide an explanation of their delayed, progressive course.

Citing Articles

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Mechanisms of Mitochondrial Malfunction in Alzheimer's Disease: New Therapeutic Hope.

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Mitochondrial links between brain aging and Alzheimer's disease.

Wilkins H, Swerdlow R Transl Neurodegener. 2021; 10(1):33.

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