Mitochondrial DNA alterations in cancer

被引:191
作者
Copeland, WC
Wachsman, JT
Johnson, FM
Penta, JS
机构
[1] NIEHS, Mol Genet Lab, Res Triangle Pk, NC 27709 USA
[2] NIEHS, Environm Toxicol Program, Res Triangle Pk, NC 27709 USA
[3] NIEHS, Off Clin Res, Res Triangle Pk, NC 27709 USA
来源
CANCER INVESTIGATION | 2002年 / 20卷 / 04期
关键词
cancer; mitochondrial DNA; mutation; reactive oxygen species;
D O I
10.1081/CNV-120002155
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
A number of studies have demonstrated the presence of mitochondrial DNA (mtDNA) mutations in cancer cells. In this article, we review mitochondrial genomic aberrations reported in solid tumors of the breast, colon, stomach, liver, kidney, bladder, head/neck, and lung. The tantalizing association of tumors with mDNA mutations implicates these mutations in the process of carcinogenesis. Alterations in expression of mtDNA transcripts in a variety of cancer types are also reviewed. In solid tumors, elevated expression Of mtDNA-genes coding for subunits of the mitochondrial electron respiratory chain may reflect mitochondrial adaptation to perturbations in cellular energy requirements. The role of mtDNA mutations and altered expression of mitochondrial genes in carcinogenesis is discussed. mitochondrial DNA mutations can initiate a cascade of events leading to a continuous increase in the production of reactive oxygen species (persistent oxidative stress), a condition that probably favors tumor development.
引用
收藏
页码:557 / 569
页数:13
相关论文
共 109 条
[1]   Detection of somatic mutations in the mitochondrial DNA control region of colorectal and gastric tumors by heteroduplex and single-strand conformation analysis [J].
Alonso, A ;
Martin, P ;
Albarran, C ;
Aguilera, B ;
Garcia, O ;
Guzman, A ;
Oliva, H ;
Sancho, M .
ELECTROPHORESIS, 1997, 18 (05) :682-685
[2]   SEQUENCE AND ORGANIZATION OF THE HUMAN MITOCHONDRIAL GENOME [J].
ANDERSON, S ;
BANKIER, AT ;
BARRELL, BG ;
DEBRUIJN, MHL ;
COULSON, AR ;
DROUIN, J ;
EPERON, IC ;
NIERLICH, DP ;
ROE, BA ;
SANGER, F ;
SCHREIER, PH ;
SMITH, AJH ;
STADEN, R ;
YOUNG, IG .
NATURE, 1981, 290 (5806) :457-465
[3]   ROLE OF MITOCHONDRIA IN CARCINOGENESIS [J].
BAGGETTO, LG .
EUROPEAN JOURNAL OF CANCER, 1993, 29A (01) :156-159
[4]   MITOCHONDRIAL MUTATIONS MAY INCREASE OXIDATIVE STRESS - IMPLICATIONS FOR CARCINOGENESIS AND AGING [J].
BANDY, B ;
DAVISON, AJ .
FREE RADICAL BIOLOGY AND MEDICINE, 1990, 8 (06) :523-539
[5]   MITOCHONDRIAL-DNA MUTATIONS IN NORMAL AND TUMOR-TISSUES FROM BREAST-CANCER PATIENTS [J].
BIANCHI, MS ;
BIANCHI, NO ;
BAILLIET, G .
CYTOGENETICS AND CELL GENETICS, 1995, 71 (01) :99-103
[6]   Oxidative DNA damage processing in nuclear and mitochondrial DNA [J].
Bohr, VA ;
Dianov, GL .
BIOCHIMIE, 1999, 81 (1-2) :155-160
[7]   In situ rat brain and liver spontaneous chemiluminescence after acute ethanol intake [J].
Boveris, A ;
Llesuy, S ;
Azzalis, LA ;
Giavarotti, L ;
Simon, KA ;
Junqueira, VBC ;
Porta, EA ;
Videla, LA ;
Lissi, EA .
TOXICOLOGY LETTERS, 1997, 93 (01) :23-28
[8]   SUPEROXIDE AND HYDROGEN-PEROXIDE IN RELATION TO MAMMALIAN-CELL PROLIFERATION [J].
BURDON, RH .
FREE RADICAL BIOLOGY AND MEDICINE, 1995, 18 (04) :775-794
[9]  
BURGART LJ, 1995, AM J PATHOL, V147, P1105
[10]  
Cavalli LR, 1997, CELL GROWTH DIFFER, V8, P1189
12345678910