A heteroplasmic, not homoplasmic, mitochondrial DNA mutation promotes tumorigenesis via alteration in reactive oxygen species generation and apoptosis

doi:10.1093/hmg/ddp069

Human Molecular Genetics Advance Access originally published online on February 10, 2009
Human Molecular Genetics 2009 18(9):1578-1589; doi:10.1093/hmg/ddp069

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A heteroplasmic, not homoplasmic, mitochondrial DNA mutation promotes tumorigenesis via alteration in reactive oxygen species generation and apoptosis

Jeong Soon Park¹^,, Lokendra Kumar Sharma¹^,, Hongzhi Li¹^,2, Ruihua Xiang¹, Deborah Holstein¹, Jun Wu¹, James Lechleiter¹, Susan L. Naylor¹, Janice J. Deng¹, Jianxin Lu² and Yidong Bai¹^,2^,*

¹ Department of Cellular and Structural Biology, University of Texas Health Science Center at San Antonio, San Antonio, TX 78229, USA and ² Zhejiang Provincial Key Laboratory of Medical Genetics, School of Laboratory Medicine and Life Science, Wenzhou Medical College, Wenzhou 325035, China

^* To whom correspondence should be addressed. Tel: +1 2105670561; Fax: +1 2105673803; Email: baiy{at}uthscsa.edu

Received December 18, 2008; Revised January 16, 2009; Accepted February 4, 2009

Mitochondrial alteration has been long proposed to play a majorrole in tumorigenesis. Recently, mitochondrial DNA (mtDNA) mutationshave been found in a variety of cancer cells. In this study,we examined the contribution of mtDNA mutation and mitochondrialdysfunction in tumorigenesis first using human cell lines carryinga frame-shift at NADH dehydrogenase (respiratory complex I)subunit 5 gene (ND5); the same homoplasmic mutation was alsoidentified in a human colorectal cancer cell line earlier. Withincreasing mutant ND5 mtDNA content, respiratory function includingoxygen consumption and ATP generation through oxidative phosphorylationdeclined progressively, while lactate production and dependenceon glucose increased. Interestingly, the reactive oxygen species(ROS) levels and apoptosis exhibited antagonistic pleiotropyassociated with mitochondrial defects. Furthermore, the anchorage-dependencephenotype and tumor-forming capacity of cells carrying wild-typeand mutant mtDNA were tested by growth assay in soft agar andsubcutaneous implantation of the cells in nude mice. Surprisingly,the cell line carrying the heteroplasmic ND5 mtDNA mutationshowed significantly enhanced tumor growth, while cells withhomoplasmic form of the same mutation inhibited tumor formation.Similar results were obtained from the analysis of a seriesof mouse cell lines carrying a nonsense mutation at ND5 gene.Our results indicate that the mtDNA mutations might play animportant role in the early stage of cancer development, possiblythrough alteration of ROS generation and apoptosis.

The authors wish it to be known that, in their opinion, thefirst two authors should be regarded as joint First Authors.

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