Nucleotide changes in mitochondrial 16S rRNA gene from different mammalian cell lines

被引：6

作者：

Hashiguchi, K ^{[1
]}

Ikushima, T ^{[1
]}

机构：

[1] Kyoto Univ Educ, Div Biol, Mol Genet Lab, Fushimi Ku, Kyoto 6128522, Japan

来源：

GENES & GENETIC SYSTEMS | 1998年 / 73卷 / 05期

关键词：

D O I：

10.1266/ggs.73.317

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

The partial nucleotide sequences of mitochondrial 16S rRNA gene were analyzed in five rodent cell lines, prior to the analysis of mutation spectrum in the gene. Total DNA was isolated from V79 and CHO-K1 cell lines from Chinese hamster and murine cell lines, Balb Y SV and PCC4 AG Cap, and the 3' terminal regions including the peptidyl transferase domain which is the target for chloramphenicol, a selective inhibitor of mitochondrial protein synthesis, were amplified by polymerase chain reaction (PCR) using two sets of primers and directly sequenced. In Chinese hamster cells, C to T transition at one site was observed in CHO-K1, and either A was deleted at the sequence of AA in all three cell lines, relative to the V79-cell sequence registered in GenBank. One G to A transition mutation in heteroplasmic state was observed in mouse PCC4 AG Cap cells which have chloramphenicol resistant phenotype, whereas there was no change in the Balb Y SV cell line, relative to the L-cell sequence. These mutation sites were located outside the peptidyl transferase domain.

引用

页码：317 / 321

页数：5

共 14 条

[1] SEQUENCE AND GENE ORGANIZATION OF MOUSE MITOCHONDRIAL-DNA [J].

BIBB, MJ ;

VANETTEN, RA ;

WRIGHT, CT ;

WALBERG, MW ;

CLAYTON, DA .

CELL, 1981, 26 (02) :167-180

[2] PRIMARY AND SECONDARY STRUCTURES OF ESCHERICHIA-COLI MRE-600-23S RIBOSOMAL-RNA - COMPARISON WITH MODELS OF SECONDARY STRUCTURE FOR MAIZE CHLOROPLAST 23S RIBOSOMAL-RNA AND FOR LARGE PORTIONS OF MOUSE AND HUMAN 16S MITOCHONDRIAL RIBOSOMAL-RNAS [J].

BRANLANT, C ;

KROL, A ;

MACHATT, MA ;

POUYET, J ;

EBEL, JP ;

EDWARDS, K ;

KOSSEL, H .

NUCLEIC ACIDS RESEARCH, 1981, 9 (17) :4303-4324

[3] RAPID EVOLUTION OF ANIMAL MITOCHONDRIAL-DNA [J].

BROWN, WM ;

GEORGE, M ;

WILSON, AC .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1979, 76 (04) :1967-1971

[4]

GILLHAN NW, 1994, ORGANELLE GENES GENO

[5] SEQUENCE-ANALYSIS OF MITOCHONDRIAL CHLORAMPHENICOL RESISTANCE MUTATIONS IN CHINESE-HAMSTER CELLS [J].

HOWELL, N ;

KUBACKA, I .

MAMMALIAN GENOME, 1993, 4 (05) :271-275

[6] SEQUENCE-ANALYSIS OF MOUSE MITOCHONDRIAL CHLORAMPHENICOL-RESISTANT MUTANTS [J].

HOWELL, N ;

LEE, A .

SOMATIC CELL AND MOLECULAR GENETICS, 1989, 15 (03) :237-244

[7] BIMODAL INDUCTION OF SISTER-CHROMATID EXCHANGES BY LUMINOL, AN INHIBITOR OF POLY(ADP-RIBOSE) SYNTHETASE, DURING THE S-PHASE OF THE CELL-CYCLE [J].

IKUSHIMA, T .

CHROMOSOMA, 1990, 99 (05) :360-364

[8] ALTERED RIBOSOMAL-RNA GENES IN MITOCHONDRIA FROM MAMMALIAN-CELLS WIT CHLORAMPHENICOL RESISTANCE [J].

KEARSEY, SE ;

CRAIG, IW .

NATURE, 1981, 290 (5807) :607-608

[9] Molecular genetic aspects of human mitochondrial disorders [J].

Larsson, NG ;

Clayton, DA .

ANNUAL REVIEW OF GENETICS, 1995, 29 :151-178

[10]

Sambrook J., 2002, MOL CLONING LAB MANU

← 1 2 →