SUGGESTIONS CONCERNING THE RELATIONSHIP BETWEEN MUTANT FREQUENCY AND MUTATION-RATE AT THE HPRT LOCUS IN HUMAN PERIPHERAL T-LYMPHOCYTES

被引：41

作者：

GREEN, MHL ^{[1
]}

ONEILL, JP ^{[1
]}

COLE, J ^{[1
]}

机构：

[1] UNIV VERMONT, CTR CANC, GENET LAB, BURLINGTON, VT 05401 USA

来源：

MUTATION RESEARCH-ENVIRONMENTAL MUTAGENESIS AND RELATED SUBJECTS | 1995年 / 334卷 / 03期

关键词：

MUTANT FREQUENCY; MUTATION RATE; HYPOXANTHINE GUANINE PHOSPHORIBOSYLTRANSFERASE; T-LYMPHOCYTES; HUMAN CELLS;

D O I：

10.1016/0165-1161(95)90070-5

中图分类号：

X [环境科学、安全科学];

学科分类号：

08 ; 0830 ;

摘要：

Mutant frequency is defined as the proportion of mutant cells in a population and is readily estimated. It should be distinguished from mutation rate, which relates to the rate at which mutation events arise, and is generally expressed as events per cell division. Since one mutation event may give rise to one or many mutant cells, depending on the generation in which it has arisen, the relationship of mutant frequency to the underlying mutation rate is complex. A large number of estimates of mutant frequency at the hprt locus in human lymphocytes are available, from our two laboratories among others, From our two extensive data sets, we have determined median hprt mutant frequencies of different age groups and used the method of Lea and Coulson (J. Genet., 49, 1949, 264-285) to attempt to estimate the underlying mutation rate at this locus. It is in principle possible to obtain estimates of mutation rate from the mutant frequency in newborns, from the increase in mutant frequency with age, and from the difference between the upper and lower quartile mutant frequencies. We discuss reasons for the discrepancies between these estimates and argue that the best estimate can probably be obtained from the increase in mutant frequency with age. We arrive at an estimate of mutation rate to 6-thioguanine resistance at the hprt locus of about 5 X 10(-7) mutation events per nominal cell division.

引用

页码：323 / 339

页数：17

共 55 条

[1] MOSAICISM OF PERIPHERAL-BLOOD LYMPHOCYTE POPULATIONS IN FEMALES HETEROZYGOUS FOR LESCH-NYHAN MUTATION [J].

ALBERTINI, RJ ;

DEMARS, R .

BIOCHEMICAL GENETICS, 1974, 11 (05) :397-411

[2] THE ROLE OF CD45 IN T-CELL ACTIVATION - RESOLVING THE PARADOXES [J].

ALEXANDER, D ;

SHIROO, M ;

ROBINSON, A ;

BIFFEN, M ;

SHIVNAN, E .

IMMUNOLOGY TODAY, 1992, 13 (12) :477-481

[3] ELEVATED FREQUENCIES OF 6-THIOGUANINE-RESISTANT LYMPHOCYTES IN MULTIPLE-SCLEROSIS PATIENTS TREATED WITH CYCLOPHOSPHAMIDE - A PROSPECTIVE-STUDY [J].

AMMENHEUSER, MM ;

WARD, JB ;

WHORTON, EB ;

KILLIAN, JM ;

LEGATOR, MS .

MUTATION RESEARCH, 1988, 204 (03) :509-520

[4] COMPARISON OF HPRT VARIANT FREQUENCIES AND CHROMOSOME ABERRATION FREQUENCIES IN LYMPHOCYTES FROM RADIOTHERAPY AND CHEMOTHERAPY PATIENTS - A PROSPECTIVE-STUDY [J].

AMMENHEUSER, MM ;

AU, WW ;

WHORTON, EB ;

BELLI, JA ;

WARD, JB .

ENVIRONMENTAL AND MOLECULAR MUTAGENESIS, 1991, 18 (02) :126-135

[5] A DIFFERENTIAL-AVIDITY MODEL FOR T-CELL SELECTION [J].

ASHTONRICKARDT, PG ;

TONEGAWA, S .

IMMUNOLOGY TODAY, 1994, 15 (08) :362-366

[6] SELECTIVE MECHANISMS IN BACTERIA [J].

ATWOOD, KC ;

SCHNEIDER, LK ;

RYAN, FJ .

COLD SPRING HARBOR SYMPOSIA ON QUANTITATIVE BIOLOGY, 1951, 16 :345-355

[7] AN IMPROVED PROCEDURE FOR THE INVITRO EXPANSION OF HUMAN T-LYMPHOCYTE CLONES FOR MUTANT ANALYSIS [J].

BEARE, DM ;

ALDRIDGE, KE ;

ODONOVAN, MR ;

COLE, J .

MUTATION RESEARCH, 1993, 291 (03) :207-212

[8]

BERNINI LF, 1990, PROG CLIN BIOL RES, V340, P57

[9] REVISITING AND REVISING SUPPRESSOR T-CELLS [J].

BLOOM, BR ;

SALGAME, P ;

DIAMOND, B .

IMMUNOLOGY TODAY, 1992, 13 (04) :131-136

[10] THE THYMIC MICROENVIRONMENT [J].

BOYD, RL ;

TUCEK, CL ;

GODFREY, DI ;

IZON, DJ ;

WILSON, TJ ;

DAVIDSON, NJ ;

BEAN, AGD ;

LADYMAN, HM ;

RITTER, MA ;

HUGO, P .

IMMUNOLOGY TODAY, 1993, 14 (09) :445-459

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