Lung adenoma development and NK activity in mice treated with multiple carcinogens.

Y. S. Lee; J. S. Seo; H. T. Chung; K. J. Cho; J. J. Jan

doi:10.3346/jkms.1992.7.1.1

Lung adenoma development and NK activity in mice treated with multiple carcinogens.

Y. S. Lee
, J. S. Seo
, H. T. Chung
, K. J. Cho
, J. J. Jan

Department of Pharmaceutical Sciences

Research output: Contribution to journal › Article › peer-review

1 Scopus citations

Abstract

A wide-spectrum initiation model was investigated in mice. Sequential treatments with diethylnitrosamine, urethane and N-methylnitrosourea, with or without a promoter, phenobarbital, resulted in tumor formation in the lungs in 85-90% of animals, but did not produce any tumorous lesions in other organs. The lung tumors were adenomas and the mean number of adenomas was 2.2-2.6 per mouse. Phenobarbital combination had no additive effect on lung tumor incidence and multiplicity. Splenic NK cell activity showed inconsistent increment in the carcinogen plus phenobarbital-treated group during the experiment (P less than 0.05).

Original language	English
Pages (from-to)	1-5
Number of pages	5
Journal	Journal of Korean Medical Science
Volume	7
Issue number	1
DOIs	https://doi.org/10.3346/jkms.1992.7.1.1
State	Published - Mar 1992

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title = "Lung adenoma development and NK activity in mice treated with multiple carcinogens.",

abstract = "A wide-spectrum initiation model was investigated in mice. Sequential treatments with diethylnitrosamine, urethane and N-methylnitrosourea, with or without a promoter, phenobarbital, resulted in tumor formation in the lungs in 85-90\% of animals, but did not produce any tumorous lesions in other organs. The lung tumors were adenomas and the mean number of adenomas was 2.2-2.6 per mouse. Phenobarbital combination had no additive effect on lung tumor incidence and multiplicity. Splenic NK cell activity showed inconsistent increment in the carcinogen plus phenobarbital-treated group during the experiment (P less than 0.05).",

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year = "1992",

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AU - Lee, Y. S.

AU - Seo, J. S.

AU - Chung, H. T.

AU - Cho, K. J.

AU - Jan, J. J.

PY - 1992/3

Y1 - 1992/3

N2 - A wide-spectrum initiation model was investigated in mice. Sequential treatments with diethylnitrosamine, urethane and N-methylnitrosourea, with or without a promoter, phenobarbital, resulted in tumor formation in the lungs in 85-90% of animals, but did not produce any tumorous lesions in other organs. The lung tumors were adenomas and the mean number of adenomas was 2.2-2.6 per mouse. Phenobarbital combination had no additive effect on lung tumor incidence and multiplicity. Splenic NK cell activity showed inconsistent increment in the carcinogen plus phenobarbital-treated group during the experiment (P less than 0.05).

AB - A wide-spectrum initiation model was investigated in mice. Sequential treatments with diethylnitrosamine, urethane and N-methylnitrosourea, with or without a promoter, phenobarbital, resulted in tumor formation in the lungs in 85-90% of animals, but did not produce any tumorous lesions in other organs. The lung tumors were adenomas and the mean number of adenomas was 2.2-2.6 per mouse. Phenobarbital combination had no additive effect on lung tumor incidence and multiplicity. Splenic NK cell activity showed inconsistent increment in the carcinogen plus phenobarbital-treated group during the experiment (P less than 0.05).

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JF - Journal of Korean Medical Science

IS - 1

ER -

Lung adenoma development and NK activity in mice treated with multiple carcinogens.

Abstract

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