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Mol Aspects Med. 2005 Aug-Oct;26(4-5):363-78.

Mineral and vitamin deficiencies can accelerate the mitochondrial decay of aging.

Author information

1
Nutrition, Metabolisms and Genomics Center, Children's Hospital Oakland Research Institute, Oakland, CA 94609, U States. bames@chori.org

Abstract

Mitochondrial oxidative decay, which is a major contributor to aging, is accelerated by many common micronutrient deficiencies. One major mechanism is inhibition of the pathway of heme biosynthesis in mitochondria, which causes a deficit of heme-a. Heme-a, only found in Complex IV, is selectively diminished, resulting in oxidant leakage and accelerated mitochondrial decay, which leads to DNA damage, neural decay, and aging. We emphasize those deficiencies, which appear to cause damage through this mechanism, particularly minerals such as iron (25% of menstruating women ingest <50% of the RDA) or zinc (10% of the population ingest <50% of the RDA). Several vitamin deficiencies, such as biotin or pantothenic acid, also increase mitochondrial oxidants through this mechanism. Additionally, other minerals such as magnesium and manganese that play a role in mitochondrial metabolism, but do not affect heme directly, are discussed. An optimum intake of micronutrients could tune up metabolism and give a marked increase in health, particularly for the poor, elderly, and obese, at little cost.

PMID:
16102804
DOI:
10.1016/j.mam.2005.07.007
[Indexed for MEDLINE]

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