Histoculture drug response assay (HDRA) systems have been used in evaluating the cytotoxic effects of chemotherapeutic agents for many kinds of advanced cancers. We have adapted the HDRA system to estimate the antitumor effect of aromatase (estrogen synthetase) inhibitors on breast cancer. Small pieces of breast cancer tissue specimens were placed onto a collagen-matrix filled with medium containing testosterone (a substrate for aromatase) or testosterone plus an aromatase inhibitor. At the end of culture, [3H]-thymidine incorporation was measured in aliquots of the histocultured specimens after 10 days culture. The increment of thymidine incorporation in testosterone-treated specimens to that of control provides an index of existence of aromatase and estrogen-dependency, since converted estradiol from added testosterone by aromatase stimulates the incorporation. The decrease in the index of "testosterone + aromatase inhibitor"/"testosterone" indicates the antitumor effect of the aromatase inhibitor on breast cancer. Twenty-one 25 breast cancer surgical specimens were successfully cultured, and 6 showed the increased incorporation of [3H]-thymidine by testosterone. Aromatase inhibitor blocked this stimulation in these 6 specimens. These results suggested that this antitumor effect is related to the inhibition of aromatase and the aromatase inhibitor would be effective for individual patients with breast cancer which responds to testosterone in this histoculture assay system. The histoculture technique we used here is therefore expected to be useful in predicting the efficacy of aromatase inhibitors for individual patients with breast cancer.

Aromatase inhibitor

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Staurosporine, a prolyl endopeptidase inhibitor.

Agricultural and Biological Chemistry (1990)

Ken‐ichi Kimura Noboru Kawaguchi Makoto Yoshihama Gosei Kawanishi

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Prolyl endopeptidase

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Endopeptidase

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SNA-60-367, New Peptide Enzyme Inhibitors against Aromatase.

The Journal of Antibiotics (1997)

Ken‐ichi Kimura Shoji F. Nakayama Junji Nakamura TAKEKO TAKADA Makoto Yoshihama

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ChemInform Abstract: New Piericidin Antibiotics, 7-Demethylpiericidin A1 and 7-Demethyl-3′- rhamnopiericidin A1.

ChemInform (1996)

Ken‐ichi Kimura Hidetoshi Takahashi N. Miyata Makoto Yoshihama Masakazu Uramoto

Abstract ChemInform is a weekly Abstracting Service, delivering concise information at a glance that was extracted from about 100 leading journals. To access a ChemInform Abstract of an article which was published elsewhere, please select a “Full Text” option. The original article is trackable via the “References” option.

10.1002/chin.199652285

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New Types of Liposidomycins Produced by Streptomyces that Inhibit Bacterial Peptidoglycan Synthesis Structure Elucidation of Fatty Acid Components by Tandem Mass Spectrometry.

The Journal of Antibiotics (1999)

Yasuaki Esumi Yoshikatsu Suzuki Ken‐ichi Kimura Makoto Yoshihama Teruo Ichikawa

Moiety

Carboxylate

Tandem

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Citations (18)