Sage Journals: Discover world-class research

Abstract

Routine carcinogenicity testings have been designed and conducted primarily for providing data to show whether or not the test compounds have a potential of inducing tumors in animals. Therefore, in the case of safety assessment or risk assessment of test compounds in humans, additional data are needed, at times, to learn how intensely the test compound can induce tumors in animals or by which mechanism the test compound can induce tumors in animals. The initiation/promotion experiment is performed as a proceeding for such requests. This paper describes the updating principle and procedures to evaluate initiation effects and promotion effects separately. However, it must be realized that our present knowledge about the initiation/promotion is still limited to some qualitative evidences. Actually, we know very little about mechanistic background and quantitative aspect of the initiation/promotion such as the site or mode of action of promoter action, the organ-specificity of promoter action, or threshold of the initiator action and promoter action. All these problems are necessary to be studied systematically in order that the initiation/promotion design can make a more important contribution to the evaluation of carcinogenicity of chemicals.

References

1. International Agency for Research on Cancer, Lyon, (1972): IARC Monographs on the Evaluation of Carcinogenic Risk of Chemicals to Man. Vol. 1, p 10, France.

2. Ryzin JV (1980): Quantitative risk assessment. J Occupational Med 22: 21–326.

3. Weisburger JH , and Williams GM (1981): Carcinogen testing: Current problems and new approaches. Science 214: 401–407.

4. Ward JM , Griesmer RA , and Weisburger EK (1979): The mouse liver tumor as an endpoint in carcinogenesis tests. Toxicol Applied Pharmacol 51: 389–397.

5. Stoner GD , and Shimkin MB (1982): Strain A mouse lung tumor bioassay. J Amer Coll Toxicol 1: 145–169.

6. Ward JM , and Reynolds CW (1983): Large granular lymphocyte leukemia. A heterogenous lymphocytic leukemia in F344 rats. Am J Path 111: 1–10.

7. Pitot HC , Goldworthy T , Campbell HA , and Polland A (1980): Quantitative evaluation of the promotion by 2,3,7,8,-tetrachlorbenzo-p-dioxin of hepatocarcinogenesis from dimethyl-nitrosamine. Cancer Res 40: 3616–3620.

8. Nakanishi K , Fukushima S , Hagiwara A , Tamano S , and Ito N (1982): Organ-specific promotion effects of phenobarbital sodium and sodium saccharin in the induction of liver and urinary bladder tumors in male F344 rats. JNCI 68: 497–500.

9. Fujiki H , Mori M , Nakayasu M , Terada M , and Sugimura T (1979): A possible naturally occurring tumor promoter, teleocidin B from Streptomyces. Biochem Biophys Res Commun 90: 976–983.

10.

10. Slaga TJ , Fischer SM , Weeks CE , Nelson K , Mamrack M , and Klein-Szanto AJP (1982): Specificity and mechanisms of promoter inhibitors in multistage promotion. Carcinogenesis, Vol. 7, Cocarcinogenesis and Biological Effects of Tumor Promoters, ed. by Hecker E. , Fusenig N.E. , Kunz W. , Marks F. , Thielmann H.W. , Raven Press, New York, pp. 19–34.

11.

11. Ito N , Fukushima S , Shirai T , Nakanishi K , Hasegawa R , and Imaida K (1983): Modifying factors in urinary bladder carcinogenesis. Environmental Health Perspectives 49: 217–222.

12.

12. Hiasa Y , Kitahori Y , Ohshima M , Fujita T , Yuasa T , Kononishi N , and Miyashiro A (1982): Promoting effects of phenobarbital and barbital on development thyroid tumors in rats treated with N-bis(2-hydroxypropyl)nitrosamine. Carcinogenesis 3: 1187–1190.

13.

13. Tsuda H , Sakata T , Tamano S , Okumura M , and Ito N (1983): Sequential observations on the appearance of neoplastic lesions in the liver and kidney after treatment with N-ethyl-N-hydroxyethylnitrosamine followed by partial hepatectomy and unilateral nephrectomy. Carcinogenesis 4: 523–528.

14.

14. Takahashi M: Personal communication.

15.

15. Kurokawa Y: Personal communication.

16.

16. Hayashi Y , and Hasegawa T : 1971): Experimental pancreatic tumor in rats after intravenous injection of 4-hydroxyaminoquinoline ***1-oxide. Gann 62: 329–330.

17.

17. Hayashi Y , and Katayama H : 1981): Promoting effect of testosterone propionate on experimental exocrine pancreatic tumors by 4-hydroxyaminoquinoline 1-oxide in rats. Toxicol Letters 9: 349–354.

18.

18. Berenblum I (1978): Established principles and unresolved problems in carcinogenesis. J Nat Cancer Inst 60: 723–726.

Initiation/Promotion Designs in Carcinogenicity Bioassays

Abstract

References