Comparison of Tumour Susceptibility Among Various Organs of Foetal, Young and Adult ICR/Jcl Mice

Overview

Journal Br J Cancer

Specialty Oncology

Date 1976 May 1

PMID 179560

Citations 5

Authors

T Nomura

Affiliations

Soon will be listed here.

Abstract

Urethane was found to be uniformly distributed in all the major organs of foetal, young and adult ICR/Jcl mice and then to disappear rapidly as measured by the incorporation of urethane-carbonyl-14C, thus permitting the accurate comparison of tumour susceptibility of cells in various organs of mice at different ages. Lung tumour frequency (tumours/lung) was significantly higher in mice treated with urethane when young (21 days old) and adult (63 days old) than in those treated in utero (Days 11-19 of gestation). When relative sensitivity of a lung cell was calculated as the ratio of average number of tumours per lung per mg of lung at the time of treatment, however, a lung cell of the foetus was more sensitive to urethane than that of the young and adult. Hepatomata were induced significantly only when male foetuses and neonates were exposed to urethane. The offspring exposed to urethane on Days 11-16, however, developed hepatomata in lower incidence than those exposed on Days 14-19, whereas the previous investigation by the author revealed that Days 11-13 correspond to the stage most sensitive to hepatocarcinogenesis. This contradiction was due to the occurrence of testicular hypogenesis (chemical castration) in all offspring of the former group. Differentiating female gonad and rapidly proliferating blood vessels of the placenta and deciduum were also sensitive to tumour induction by urethane. Thus, high tumour susceptibility of rapidly proliferating and undifferentiated cells suggests that some initiating events in the process of carcinogenesis may occur during or after DNA replication. Leukaemia induction in the young mice, but not in the foetus, remains to be elucidated.

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References

Nomura T . Sensitivity of a lung cell in the developing mouse embryo to tumor induction by urethan. Cancer Res. 1974; 34(12):3363-72. View

Shendrikova I, Anisimov V, Likhachev A . [Dynamics of the transplacental penetration of 7,12-dimethylbenz(a)anthracene (DMBA) in mice]. Vopr Onkol. 1973; 19(5):75-9. View

Nomura T, Takebe H, Okamoto E . Long retention of urethan transferred into newborn mice transplacentally, as a possible cause of high carcinogenesis. Gan. 1973; 64(1):29-40. View

Nomura T . An analysis of the changing urethan response of the developing mouse embryo in relation to mortality, malformation, and neoplasm. Cancer Res. 1974; 34(9):2217-31. View

Kimura K . Progression of pulmonary tumor in mice. 1. Histological studies of primary and transplanted pulmonary tumors. Acta Pathol Jpn. 1971; 21(1):13-56. DOI: 10.1111/j.1440-1827.1971.tb00108.x. View

Tomatis L, Turusov V, Guibbert D, Duperray B, Malaveille C, Pacheco H . Transplacental carcinogenic effect of 3-methylcholanthrene in mice and its quantitation in fetal tissues. J Natl Cancer Inst. 1971; 47(3):645-51. View

CIVIDALLI G, MIRVISH S, BERENBLUM I . The catabolism of urethan in young mice of varying age and strain, and in x-irradiated mice, in relation to urethan carcinogenesis. Cancer Res. 1965; 25(6):855-8. View

Gardner W . Hormonal aspects of experimental tumorigenesis. Adv Cancer Res. 1953; 1:173-232. DOI: 10.1016/s0065-230x(08)60004-4. View

Dunn T . Normal and pathologic anatomy of the reticular tissue in laboratory mice, with a classification and discussion of neoplasms. J Natl Cancer Inst. 1954; 14(6):1281-433. View

10.

BERENBLUM I, Haran-Ghera N, WINNICK R, WINNICK T . Distribution of C14-labeled urethans in tissues of the mouse and subcellular localization in lung and liver. Cancer Res. 1958; 18(2):181-5. View

11.

Pietra G, Rappaport H, SHUBIK P . The effects of carcinogenic chemicals in newborn mice. Cancer. 1961; 14:308-17. DOI: 10.1002/1097-0142(196103/04)14:2<308::aid-cncr2820140211>3.0.co;2-n. View

12.

De Benedictis G, Maiorano G, Chieco-Bianchi L, FIORE-DONATI L . Lung carcinogenesis by urethane in newborn, suckling, and adult Swiss mice. Br J Cancer. 1962; 16:686-9. PMC: 2071055. DOI: 10.1038/bjc.1962.78. View

13.

DOMSKY I, Lijinsky W, Spencer K, SHUBIK P . Rate of metabolism of 9,10-dimethyl-1,2-benzanthracene in newborn and adult mice. Proc Soc Exp Biol Med. 1963; 113:110-2. DOI: 10.3181/00379727-113-28292. View

14.

MIRVISH S, CIVIDALLI G, BERENBLUM I . SLOW ELIMINATION OF URETHAN IN RELATION TO ITS HIGH CARCINOGENICITY IN NEWBORN MICE. Proc Soc Exp Biol Med. 1964; 116:265-8. DOI: 10.3181/00379727-116-29220. View

15.

ANDERVONT H . Studies on the occurrence of spontaneous hepatomas in mice of strains C3H and CBA. J Natl Cancer Inst. 1950; 11(3):581-92. View

16.

Klein M . The transplacental effect of urethan on lung tumor genesis in mice. J Natl Cancer Inst. 1952; 12(5):1003-10. View

17.

Boyland E, Rhoden E . The distribution of urethane in animal tissues, as determined by a microdiffusion method, and the effect of urethane treatment on enzymes. Biochem J. 1949; 44(5):528-31. PMC: 1274907. DOI: 10.1042/bj0440528. View

18.

GRADY H, Stewart H . Histogenesis of induced pulmonary tumors in strain a mice. Am J Pathol. 2009; 16(4):417-432.5. PMC: 1965107. View

19.

Nomura T . Carcinogenicity of the food additive furylfuramide in foetal and young mice. Nature. 1975; 258(5536):610-11. DOI: 10.1038/258610a0. View

20.

Vesselinovitch S, Mihailovich N . The neonatal and infant age periods as biologic factors which modify multicarcinogenesis by urethan. Cancer Res. 1967; 27(8):1422-9. View