MOLECULAR-BASIS OF MITOCHONDRIAL-DNA DISEASE

被引：140

作者：

BROWN, MD

WALLACE, DC

机构：

[1] Department of Genetics and Molecular Medicine, Atlanta, 30333, Georgia, 1462 Clifton Road, N.E.

来源：

JOURNAL OF BIOENERGETICS AND BIOMEMBRANES | 1994年 / 26卷 / 03期

关键词：

MITOCHONDRIAL DNA; OXIDATIVE PHOSPHORYLATION; HUMAN DISEASE; BASE SUBSTITUTIONS; REARRANGEMENTS; GENOTYPE; PHENOTYPE; MISSENSE; TRANSFER RNA;

D O I：

10.1007/BF00763099

中图分类号：

Q6 [生物物理学];

学科分类号：

071011 ;

摘要：

Mitochondrial ATP production via oxidative phosphorylation (OXPHOS) is essential for normal function and maintenance of human organ systems. Since OXPHOS biogenesis depends on both nuclear- and mitochondrial-encoded gene products, mutations in both genomes can result in impaired electron transport and ATP synthesis, thus causing tissue dysfunction and, ultimately, human disease. Over 30 mitochondrial DNA (mtDNA) point mutations and over 100 mtDNA rearrangements have now been identified as etiological factors in human disease. Because of the unique characteristics of mtDNA genetics, genotype/phenotype associations are often complex and disease expression can be influenced by a number of factors, including the presence of nuclear modifying or susceptibility alleles. Accordingly, these mutations result in an extraordinarily broad spectrum of clinical phenotypes ranging from systemic, lethal pediatric disease to late-onset, tissue-specific neurodegenerative disorders. In spite of its complexity, an understanding of the molecular basis of mitochondrial DNA disease will be essential as the first step toward rationale and permanent curative therapy.

引用

页码：273 / 289

页数：17

共 112 条

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