INCREASED POSTIMPLANTATION LOSS AND MALFORMATIONS AMONG THE F2 PROGENY OF MALE-RATS CHRONICALLY TREATED WITH CYCLOPHOSPHAMIDE

被引:77
作者
HALES, BF
CROSMAN, K
ROBAIRE, B
机构
[1] Department of Pharmacology and Therapeutics, Centre for the Study of Reproduction, McGill University, Montreal, Quebec
来源
TERATOLOGY | 1992年 / 45卷 / 06期
关键词
D O I
10.1002/tera.1420450612
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
Cyclophosphamide, administered to the male rat, produces increased pre- and postimplantation loss in the progeny as well as an increase in the numbers of malformed and growth retarded fetuses. The purpose of this study was to determine whether the adverse effects of chronic paternal cyclophosphamide exposure are transmissible to the next generation, the F2 progeny. Adult male rats were treated by gavage daily with saline or with cyclophosphamide (3.4 or 5.1 mg/kg) for 4 or 18 weeks and mated. The male and female offspring in each treatment group (F1 generation) were randomly mated. The resulting pregnant females were killed on day 20 of gestation to evaluate progeny outcome in the F2 generation. There was a significant increase in postimplantation loss among the offspring of the group whose fathers had been treated with cyclophosphamide at a dose of 5.1 mg/kg/day. Exposure to a dose of 5.1 mg/kg/day of cyclophosphamide also resulted in an F2 generation with a significantly decreased mean fetal weight per litter and a significant increase in the number of malformed fetuses. The malformations observed among the F2 progeny included open eyes, omphalocele, generalized edema, syndactyly, gigantism, and dwarfism. Thus, exposure of the father to cyclophosphamide does result in a specific and heritable alteration in the fertility of the surviving "apparently normal" F1 progeny. Interestingly, the adverse consequences of exposure of male rats to cyclophosphamide are similar in the F2 generation to those previously reported for the F1 progeny.
引用
收藏
页码:671 / 678
页数:8
相关论文
共 28 条
[11]   TUMORS AND MALFORMATIONS IN THE ADULT OFFSPRING OF CYCLOPHOSPHAMIDE-TREATED AND CONTROL MALE-RATS - PRELIMINARY COMMUNICATION [J].
FRANCIS, AJ ;
ANDERSON, D ;
EVANS, JG ;
JENKINSON, PC ;
GODBERT, P .
MUTATION RESEARCH, 1990, 229 (02) :239-246
[12]   EFFECT OF PHENOBARBITAL AND SKF 525-A ON TERATOGENICITY OF CYCLOPHOSPHAMIDE IN MICE [J].
GIBSON, JE ;
BECKER, BA .
TERATOLOGY, 1968, 1 (04) :393-&
[13]   REVERSIBILITY OF THE EFFECTS OF CHRONIC PATERNAL EXPOSURE TO CYCLOPHOSPHAMIDE ON PREGNANCY OUTCOME IN RATS [J].
HALES, BF ;
ROBAIRE, B .
MUTATION RESEARCH, 1990, 229 (02) :129-134
[14]  
HALES BF, 1982, CANCER RES, V42, P3016
[15]   EFFECTS OF ALKYLATING AGENTS ON FERTILITY [J].
JACKSON, H .
BRITISH MEDICAL BULLETIN, 1964, 20 (02) :107-&
[16]   MALFORMED FETUSES AND KARYOTYPE ABNORMALITIES IN THE OFFSPRING OF CYCLOPHOSPHAMIDE AND ALLYL ALCOHOL-TREATED MALE-RATS [J].
JENKINSON, PC ;
ANDERSON, D .
MUTATION RESEARCH, 1990, 229 (02) :173-184
[17]   INDUCTION OF CONGENITAL-MALFORMATION IN MICE BY PARENTAL IRRADIATION - TRANSMISSION TO LATER GENERATIONS [J].
LYON, MF ;
RENSHAW, R .
MUTATION RESEARCH, 1988, 198 (02) :277-283
[18]   PRENATAL LETHALITY IN A TRANSGENIC MOUSE LINE IS THE RESULT OF A CHROMOSOMAL TRANSLOCATION [J].
MAHON, KA ;
OVERBEEK, PA ;
WESTPHAL, H .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1988, 85 (04) :1165-1168
[19]   CYCLOPHOSPHAMIDE TERATOGENESIS - A REVIEW [J].
MIRKES, PE .
TERATOGENESIS CARCINOGENESIS AND MUTAGENESIS, 1985, 5 (02) :75-88
[20]   GENOTOXIC POTENCY IN MOUSE SPERMATOGONIAL STEM-CELLS OF TRIETHYLENEMELAMINE, MITOMYCIN-C, ETHYLNITROSOUREA, PROCARBAZINE, AND PROPYL METHANESULFONATE AS MEASURED BY F1-CONGENITAL DEFECTS [J].
NAGAO, T ;
FUJIKAWA, K .
MUTATION RESEARCH, 1990, 229 (02) :123-128
123