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CORRECTION OF CHROMOSOMAL INSTABILITY AND SENSITIVITY TO DIVERSE MUTAGENS BY A CLONED CDNA OF THE XRCC3 DNA-REPAIR GENE

被引:223
作者
TEBBS, RS
ZHAO, Y
TUCKER, JD
SCHEERER, JB
SICILIANO, MJ
HWANG, M
LIU, N
LEGERSKI, RJ
THOMPSON, LH
机构
[1] LAWRENCE LIVERMORE NATL LAB,BIOL & BIOTECHNOL RES PROGRAM,LIVERMORE,CA 94551
[2] UNIV TEXAS,CTR CANC,DEPT MOLEC GENET,HOUSTON,TX 77030
来源
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1995年 / 92卷 / 14期
关键词
IRS1SF; CROSS-LINKING AGENTS; GENETIC COMPLEMENTATION; CHROMOSOMAL ABERRATIONS;
D O I
10.1073/pnas.92.14.6354
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
The mutagen-sensitive CHO line irs1SF was previously isolated on the basis of hypersensitivity to ionizing radiation and was found to be chromosomally unstable as well as cross-sensitive to diverse kinds of DNA-damaging agents. The analysis of somatic cell hybrids formed between irs1SF and human lymphocytes implicated a human gene (defined as XRCC3; x-ray repair cross-complementing), which partially restored mitomycin C resistance to the mutant. A functional cDNA that confers mitomycin C resistance was transferred to irs1SF cells by transforming them with an expression cDNA library and obtaining primary and secondary transformants. Functional cDNA clones were recovered from a cosmid library prepared from a secondary transformant. Transformants also showed partial correction of sensitivity to cisplatin and gamma-rays, efficient correction of chromosomal instability, and substantially improved plating efficiency and growth rate. The XRCC3 cDNA insert is approximate to 2.5 kb and detects an approximate to 3.0-kb mRNA on Northern blots, The cDNA was mapped by fluorescence in situ hybridization to human chromosome 14q32.3, which was consistent with the chromosome concordance data of two independent hybrid clone panels.
引用
收藏
页码:6354 / 6358
页数:5
相关论文
共 30 条
[1]   CROSS-SENSITIVITY OF GAMMA-RAY-SENSITIVE HAMSTER MUTANTS TO CROSS-LINKING AGENTS [J].
CALDECOTT, K ;
JEGGO, P .
MUTATION RESEARCH, 1991, 255 (02) :111-121
[2]   REGIONAL ASSIGNMENT OF A HUMAN DNA-REPAIR GENE (XRCC5) TO 2Q35 BY X-RAY HYBRID MAPPING [J].
CHEN, DJ ;
MARRONE, BL ;
NGUYEN, T ;
STACKHOUSE, M ;
ZHAO, Y ;
SICILIANO, MJ .
GENOMICS, 1994, 21 (02) :423-427
[3]   DO WE KNOW THE CAUSE OF XERODERMA-PIGMENTOSUM [J].
CLEAVER, JE .
CARCINOGENESIS, 1990, 11 (06) :875-882
[4]   MUTANT RODENT CELL-LINES SENSITIVE TO ULTRAVIOLET-LIGHT, IONIZING-RADIATION AND CROSS-LINKING AGENTS - A COMPREHENSIVE SURVEY OF GENETIC AND BIOCHEMICAL CHARACTERISTICS [J].
COLLINS, AR .
MUTATION RESEARCH, 1993, 293 (02) :99-118
[5]   GENERATION OF SINGLE-NUCLEOTIDE REPAIR PATCHES FOLLOWING EXCISION OF URACIL RESIDUES FROM DNA [J].
DIANOV, G ;
PRICE, A ;
LINDAHL, T .
MOLECULAR AND CELLULAR BIOLOGY, 1992, 12 (04) :1605-1612
[6]   A CHINESE-HAMSTER OVARY CELL-LINE HYPERSENSITIVE TO IONIZING-RADIATION AND DEFICIENT IN REPAIR REPLICATION [J].
FULLER, LF ;
PAINTER, RB .
MUTATION RESEARCH, 1988, 193 (02) :109-121
[7]   NUCLEOTIDE EXCISION REPAIR .1. FROM ESCHERICHIA-COLI TO YEAST [J].
HOEIJMAKERS, JHJ .
TRENDS IN GENETICS, 1993, 9 (05) :173-177
[8]  
HOY CA, 1985, CANCER RES, V45, P1737
[9]   HUMAN NUCLEOTIDE EXCISION NUCLEASE REMOVES THYMINE DIMERS FROM DNA BY INCISING THE 22ND PHOSPHODIESTER BOND 5' AND THE 6TH PHOSPHODIESTER BOND 3' TO THE PHOTODIMER [J].
HUANG, JC ;
SVOBODA, DL ;
REARDON, JT ;
SANCAR, A .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (08) :3664-3668
[10]   BIOCHEMICAL AND GENETIC-ANALYSIS OF THE CHINESE-HAMSTER MUTANTS IRS1 AND IRS2 AND THEIR COMPARISON TO CULTURED ATAXIA TELANGIECTASIA CELLS [J].
JONES, NJ ;
STEWART, SA ;
THOMPSON, LH .
MUTAGENESIS, 1990, 5 (01) :15-23
123