The Initiating and Promoting Elements in Tumor Production

Friedewald, William F.; Rous, Peyton

doi:10.1084/jem.80.2.101

Cited by 227 publications

(57 citation statements)

References 10 publications

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“…The horn seen grossly was of keratin and debris. These conical tumors have not been previously described, though they are similar to the " papillomes invagines " seen by Bang (1922) in tarred mice, and to the " frill horns " and " carcinomatoids" described by Rous and Kidd (1939) and by Friedewald and Rous (1944) in tarred and in benzpyrene painted rabbits.…”

supporting

confidence: 70%

The Life and Progression of Induced Skin Tumors in Mice

Shubik¹,

Baserga²,

Ritchie³

1953

Br J Cancer

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BY studying the life of various kinds of spontaneous and induced tumors in animals, it has been found that they sometimes undergo irreversible changes in character. For example, a papilloma induced in mouse skin by applications of carcinogen, may become a carcinoma, so changing its character; or a spontaneous tumor of the mouse breast responding to pregnancy by an increase in growth rate may change its character and no longer respond to this stimulus. Foulds (1949stimulus. Foulds ( , 1950stimulus. Foulds ( , 1951) made a special study of these changes in character, calling them " progressions ", and defining " progression " as an " irreversible, qualitative change " in a tumor.Foulds then went further, claiming that different characters of the same tumor could progress independently of one another. For example, he found that in spontaneous mammary tumours in mice one character, the growth rate, might progress, and the tumor grow faster, while another, the responsiveness to pregnancy remained unchanged.Foulds (1949) studied not only the spontaneous mammary tumors of mice, but also bladder tumors induced by feeding 2-acetylaminofluorene to mice (Foulds, 1950) and transplantable mammary fibroadenomata in rats (Foulds, 1951). In each case he found that the tumors did sometimes progress, and that progression could occur independently in different characters of the same tumor. These findings seemed so interesting as to make desirable further confirmation, and this paper records an investigation of the life of tumors induced in mouse skin by repeated applications of 9,10-dimethyl-1,2-benzanthracene. Two characters were studied, the morphology of the tumors and their growth rate.The paper falls into three parts. In the first is discussed the morphological classification of the tumors; in the second whether they progress, whether progression of one of these characters can occur without progression of the other, and certain other matters related; and in the third the significance of these findings is discussed. MATERIAL AND METHODS.One hundred Swiss virgin female mice bred at the Roscoe B. Jackson Memorial Laboratory, Bar Harbor, Maine, were used. The mice were housed in groups of 25 in plastic cages and given Rockland mouse diet and-water ad libitum.The carcinogen was a 0-5 per cent solution of 9,10-dimethyl-1,2-benzanthracene (Eastman Kodak) in mineral oil (Superla 34, Standard Oil), and was applied twice each week to an area 1' cm. square in the interscapular region which was

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confidence: 70%

The Life and Progression of Induced Skin Tumors in Mice

Shubik¹,

Baserga²,

Ritchie³

1953

Br J Cancer

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“…Progression from non-dysplastic papillomas to dysplastic papillomas to malignant skin tumors has been studied in the mouse (Berenblum, 1954;Berenblum and Shubik, 1949;Boutwell, 1964;DiGiovanni, 1992;Friedewald and Rous, 1944;Yuspa, 1998). In SENCAR mouse skin, ENU functions as a tumor initiator at lower doses, but as a complete carcinogen at higher doses (O'Connell et al, 1987).…”

Section: Enu Induces Neoplasia In Zebrafishmentioning

confidence: 99%

Ethylnitrosourea Induces Neoplasia in Zebrafish (Danio rerio)

Beckwith

Moore

Tsao-Wu

et al. 2000

Laboratory Investigation

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SUMMARY:The zebrafish (Danio rerio) has been successfully used to discover hundreds of genes involved in development and organogenesis. To address the potential of zebrafish as a cancer model, it is important to determine the susceptibility of zebrafish to tumors. Germ line mutations are most commonly induced for zebrafish mutant screens by exposing adult male zebrafish to the alkylating agent, ethylnitrosourea (ENU). To determine whether ENU induces tumors, we compared the incidence of tumors in ENU-treated fish with untreated controls. Interestingly, 18 of 18 (100%) fish mutagenized with either 2.5 or 3.0 mM ENU developed epidermal papillomas, which numbered 1 to 22 per fish, within 1 year of treatment. The induced epidermal lesions included epidermal hyperplasia, flat papillomas (0.2 to 1.2 mm), and pedunculated papillomas (1.2 to 8 mm in greatest dimension), but no skin cancers. Angiogenesis was evident in papillomas larger than approximately 1 mm. All but two papillomas contained the three cell types (keratinocytes, club, and mucous cells) of normal zebrafish epidermis; histologic variants lacked either club cells or mucous cells. Two cavernous hemangiomas and a single malignant peripheral nerve sheath tumor were also found in the treated fish. None of five untreated controls developed tumors. These studies establish the feasibility of the zebrafish as an experimental model for the study of skin tumors. (Lab Invest 2000, 80:379-385).

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“…Thus, Mottram's second stage (" Specific Cellular Reaction ") corresponds to the " Precarcinogenic Action " of Berenblum (1941b; and also to the "Initiating Process " of Friedewald and Rous (1944), while his third stage (" Developing Factor ") corresponds to Berenblum's " Epicarcinogenic Action " and Friedewald and Rous's " Promoting Process." (See Table of (a) whether a single application of a carcinogen is indeed adequate antecedent treatment to allow the " developing " effect of croton oil to be manifested; and (b) whether there is in fact an initial, non-specific, hyperplasia-producing, " sensitizing factor," operating prior to the specific carcinogenic action.…”

mentioning

confidence: 99%