Mitochondrial mutational spectra in human cells and tissues

被引：148

作者：

Khrapko, K ^{[1
]}

Coller, HA ^{[1
]}

Andre, PC ^{[1
]}

Li, XC ^{[1
]}

Hanekamp, JS ^{[1
]}

Thilly, WG ^{[1
]}

机构：

[1] MIT, DIV TOXICOL, CTR ENVIRONM HLTH SCI, CAMBRIDGE, MA 02139 USA

来源：

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1997年 / 94卷 / 25期

关键词：

D O I：

10.1073/pnas.94.25.13798

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

We have found that human organs such as colon, lung, and muscle, as well as their derived tumors, share nearly all mitochondrial hotspot point mutations. Seventeen hotspots, primarily G --> A and A --> G transitions, have been identified in the mitochondrial sequence of base pairs 10,030-10,130. Mutant fractions increase with the number of cell generations in a human IS cell line, TK6, indicating that they are heritable changes. The mitochondrial point mutation rate appears to he more than two orders of magnitude higher than the nuclear point mutation rate in TK6 cells and in human tissues. The similarity of the hotspot sets in vivo and in vitro leads us to conclude that human mitochondrial point mutations in the sequence studied are primarily spontaneous in origin and arise either from DNA replication error or reactions of DNA with endogenous metabolites. The predominance of transition mutations and the high number of hotspots in this short sequence resembles spectra produced by DNA polymerases in vitro.

引用

页码：13798 / 13803

页数：6

共 36 条

[21]

LINNANE AW, 1990, BIOCHEM INT, V22, P1067

[22]

Muenscher C., 1993, FEBS (Federation of European Biochemical Societies) Letters, V317, P27

[23] PROGRESSIVE LOSS OF CYTOCHROME-C-OXIDASE IN THE HUMAN EXTRAOCULAR-MUSCLES IN AGING - A CYTOCHEMICAL-IMMUNOHISTOCHEMICAL STUDY [J].

MULLERHOCKER, J ;

SCHNEIDERBANGER, K ;

STEFANI, FH ;

KADENBACH, B .

MUTATION RESEARCH, 1992, 275 (3-6) :115-124

[24] MUTATIONAL SPECTRA IN HUMAN B-CELLS - SPONTANEOUS, OXYGEN AND HYDROGEN PEROXIDE-INDUCED MUTATIONS AT THE HPRT GENE [J].

OLLER, AR ;

THILLY, WG .

JOURNAL OF MOLECULAR BIOLOGY, 1992, 228 (03) :813-826

[25]

OLLER AR, 1989, MUTAT RES, V216, P83

[26]

Pallotti F, 1996, AM J HUM GENET, V59, P591

[27] AN ANALYSIS OF IN-VIVO HPRT MUTANT FREQUENCY IN CIRCULATING T-LYMPHOCYTES IN THE NORMAL HUMAN-POPULATION - A COMPARISON OF 4 DATASETS [J].

ROBINSON, DR ;

GOODALL, K ;

ALBERTINI, RJ ;

ONEILL, JP ;

FINETTE, B ;

SALATREPAT, M ;

MOUSTACCHI, E ;

TATES, AD ;

BEARE, DM ;

GREEN, MHL ;

COLE, J .

MUTATION RESEARCH-ENVIRONMENTAL MUTAGENESIS AND RELATED SUBJECTS, 1994, 313 (2-3) :227-247

[28] MUTATIONAL SPECTRUM INDUCED IN SACCHAROMYCES-CEREVISIAE BY THE CARCINOGEN N-2-ACETYLAMINOFLUORENE [J].

ROY, A ;

FUCHS, RPP .

MOLECULAR & GENERAL GENETICS, 1994, 245 (01) :69-77

[29] SPECTRA OF SPONTANEOUS MUTATIONS IN ESCHERICHIA-COLI STRAINS DEFECTIVE IN MISMATCH CORRECTION - THE NATURE OF INVIVO DNA-REPLICATION ERRORS [J].

SCHAAPER, RM ;

DUNN, RL .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1987, 84 (17) :6220-6224

[30] DELETION MUTANTS ARE FUNCTIONALLY DOMINANT OVER WILD-TYPE MITOCHONDRIAL GENOMES IN SKELETAL-MUSCLE FIBER SEGMENTS IN MITOCHONDRIAL DISEASE [J].

SHOUBRIDGE, EA ;

KARPATI, G ;

HASTINGS, KEM .

CELL, 1990, 62 (01) :43-49

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