DIFFERENT CAPACITIES FOR RECOMBINATION IN CLOSELY-RELATED HUMAN LYMPHOBLASTOID CELL-LINES WITH DIFFERENT MUTATIONAL RESPONSES TO X-IRRADIATION

被引:90
作者
XIA, F [1 ]
AMUNDSON, SA [1 ]
NICKOLOFF, JA [1 ]
LIBER, HL [1 ]
机构
[1] HARVARD UNIV,SCH PUBL HLTH,DEPT CANC BIOL,BOSTON,MA 02115
关键词
D O I
10.1128/MCB.14.9.5850
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
WIL2-NS and TK6 are two distinct human lymphoblast cell lines derived from a single male donor. WIL2-NS cells are significantly more resistant to the cytotoxic effects of S-irradiation but considerably more sensitive to induced mutation. In an effort to determine the mechanistic basis for these differences, we analyzed the physical structures of thymidine kinase (tk)-deficient mutants isolated after X-ray treatment of tk heterozygotes derived from TK6 and the more mutable WIL2-NS. Southern analysis showed that while 84% of TK6-derived mutants had arisen by loss of heterozygosity. (LOH), all 106 mutants from WIL2-NS derivatives arose with LOB at tk and all but one showed LOH at other linked loci on chromosome 17. We adapted a fluorescence in situ hybridization technique to distinguish between LOH due to deletion, which results in retention of only one fk allele, and LOH due to a mechanism involving the homologous chromosome (e.g., recombination), which results in the retention of two alleles. Among the LOH mutants derived that were analyzed in this way, 9 of 26 from WIL2-NS and 11 of 17 from TK6 cell lines arose by deletion. The remaining mutants retained two copies of the rk gene and thus arose by a mechanism involving the homologous allele. Since many of these mutants arising by a homologous mechanism retained partial heterozygosity of chromosome 17, they must have arisen by recombination or gene conversion, and not chromosome loss and reduplication. Finally, the recombinational capacities of WIL2-NS and TK6 were compared in transfection assays with plasmid recombination substrates. Intermolecular recombination frequencies were gl eater in WIL2-NS than in TK6. These data are consistent with a model suggesting that a recombinational repair system is functioning at a higher level in WIL2-NS than in TK6; the greater mutability of the tk locus in WIL2-NS results from more frequent inter- and intramolecular recombination events.
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收藏
页码:5850 / 5857
页数:8
相关论文
共 87 条
[31]   INVOLVEMENT OF DOUBLE-STRAND CHROMOSOMAL BREAKS FOR MATING-TYPE SWITCHING IN SACCHAROMYCES-CEREVISIAE [J].
KLAR, AJS ;
STRATHERN, JN ;
ABRAHAM, JA .
COLD SPRING HARBOR SYMPOSIA ON QUANTITATIVE BIOLOGY, 1984, 49 :77-88
[32]   DOUBLE-STRAND BREAKS CAN INITIATE MEIOTIC RECOMBINATION IN SACCHAROMYCES-CEREVISIAE [J].
KOLODKIN, AL ;
KLAR, AJS ;
STAHL, FW .
CELL, 1986, 46 (05) :733-740
[33]   MOLECULAR CHARACTERIZATION OF THYMIDINE KINASE MUTANTS OF HUMAN-CELLS INDUCED BY DENSELY IONIZING-RADIATION [J].
KRONENBERG, A ;
LITTLE, JB .
MUTATION RESEARCH, 1989, 211 (02) :215-224
[34]   HOMOLOGOUS RECOMBINATION BETWEEN PLASMIDS IN MAMMALIAN-CELLS CAN BE ENHANCED BY TREATMENT OF INPUT DNA [J].
KUCHERLAPATI, RS ;
EVES, EM ;
SONG, KY ;
MORSE, BS ;
SMITHIES, O .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1984, 81 (10) :3153-3157
[35]   EVIDENCE FOR INCREASED INVIVO MUTATION AND SOMATIC RECOMBINATION IN BLOOMS SYNDROME [J].
LANGLOIS, RG ;
BIGBEE, WL ;
JENSEN, RH ;
GERMAN, J .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (02) :670-674
[36]  
LEVY JA, 1968, CANCER-AM CANCER SOC, V22, P517, DOI 10.1002/1097-0142(196809)22:3<517::AID-CNCR2820220305>3.0.CO
[37]  
2-A
[38]   MOLECULAR MECHANISMS OF SPONTANEOUS AND INDUCED LOSS OF HETEROZYGOSITY IN HUMAN-CELLS INVITRO [J].
LI, CY ;
YANDELL, DW ;
LITTLE, JB .
SOMATIC CELL AND MOLECULAR GENETICS, 1992, 18 (01) :77-87
[39]   A COMPARISON OF MUTATION-INDUCTION AT THE TK AND HPRT LOCI IN HUMAN-LYMPHOBLASTOID CELLS - QUANTITATIVE DIFFERENCES ARE DUE TO AN ADDITIONAL CLASS OF MUTATIONS AT THE AUTOSOMAL TK LOCUS [J].
LIBER, HL ;
YANDELL, DW ;
LITTLE, JB .
MUTATION RESEARCH, 1989, 216 (01) :9-17
[40]   MUTATION ASSAY AT THE THYMIDINE KINASE LOCUS IN DIPLOID HUMAN-LYMPHOBLASTS [J].
LIBER, HL ;
THILLY, WG .
MUTATION RESEARCH, 1982, 94 (02) :467-485