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Evaluation of chemically induced cytogenetic lesions in rabbit oocytes: II. A comparison of streptonigrin effects on somatic and germ cells
Authors:Russell J. DuFrain  L. Gayle Littlefield  James L. Wilmer  Edward L. Frome
Affiliation:Radiation Emergency Assistance Center/Training Site (REAC/TS), Medical and Health Sciences Division, Oak Ridge Associated Universities, P.O. Box 117, Oak Ridge, TN 37830, U.S.A.
Abstract:The dose-response relationships for streptonigrin (NSC-45383)-induced chromosome aberrations in rabbit somatic cells are compared with dose-response data derived from the analysis of inherited structural chromosome abnormalities in preimplantation embryos from female rabbits treated with streptonigrin prior to mating. The incidence of inherited aberrations assessed in over 1000 karyotype preparations from 361 6-day blastocysts obtained from 55 female rabbits is used to derive a measure of the transmissible cytogenetic damage induced in the oocytes. The cytogenetic damage assessed in 2300 lymphoblast metaphases from 23 rabbits and 2750 marrow-derived metaphases from 27 rabbits which were collected and prepared for examination 6 h after the initiation of streptonigrin dosing are used to obtain estimates of the somatic cell insult. A uniform maximum likelihood analysis technique is applied individually to the 3 sets of data to derive the coefficients of the dose-response relationships. The resulting equations are Y = 0.6 ± 28.0 (×10?5) + 8.2 ± 5.1 (×10?4χ for inherited aberrations in 6-day blastocysts, Y = 9.7 ± 3.3 (×10?3 + 1.9 ± (×10?3)χ for bone-marrow cells, and Y = 2.8 ± 0.7 (×10?2 + 4.8 ± 0.2 (×10?3)χ for the lymphoblasts. In the somatic tissues Y is the percentage of cells with chromosome breakage, while in the blastocyst data Y is the percentage of 6-day blastocysts with consistent structural chromosome aberrations, and in all equations χ is the total streptonigrin dose in μg/kg.The study shows that streptonigrin injections in the range of 30–90 μg/kg when given to sexually mature female rabbits cause dose-dependent increases in chromosome aberrations in 2 types of somatic cells and in the incidence of inherited aberrations recovered in 6-day blastocysts. The coefficients of damage recovered in blastocysts versus damage recovered in somatic cells have the ratio of 1:2.3:5.8 (blastocysts: bone marrow: lymphoblasts). The results are discussed in terms of risk assessment and kinetics of aberration loss during meiosis and early embryonic development. The conclusion drawn from the study is that somatic cell cytogenetic damage is in some way predictive of damage incurred by oocytes which can be passed on to preimplantation embryos, at least for agents like streptonigrin.
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