Mode of Action of Estra‐1,3,5(10)‐triene‐3,17β‐diol 3‐Benzoate 17‐((4‐(4‐Bis(2‐chloroethyl)amino)phenyl)‐1‐oxobutoxy)acetate) on Human Breast Carcinoma Xenografts in Nude Mice

To elucidate the mode of action of busramustine (KM2210), 17β‐ and α‐busramustine, estradiol and chlorambucil were used for experimental chemo‐ and endocrino‐therapy against hormone‐dependent (T‐61) and independent (MX‐1) human breast carcinomas serially transplanted into BALB/cA female nude mice. B...

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Autores principales: Kubota, Tetsuro, Koh, Jun‐ichi, Yamada, Yoshinori, Oka, Shoichi, Enomoto, Koji, Ishibiki, Kyuya, Abe, Osahiko, Masui, Osamu, Asano, Kiro
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Blackwell Publishing Ltd 1988
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5917647/
https://www.ncbi.nlm.nih.gov/pubmed/3147278
http://dx.doi.org/10.1111/j.1349-7006.1988.tb01548.x
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author Kubota, Tetsuro
Koh, Jun‐ichi
Yamada, Yoshinori
Oka, Shoichi
Enomoto, Koji
Ishibiki, Kyuya
Abe, Osahiko
Masui, Osamu
Asano, Kiro
author_facet Kubota, Tetsuro
Koh, Jun‐ichi
Yamada, Yoshinori
Oka, Shoichi
Enomoto, Koji
Ishibiki, Kyuya
Abe, Osahiko
Masui, Osamu
Asano, Kiro
author_sort Kubota, Tetsuro
collection PubMed
description To elucidate the mode of action of busramustine (KM2210), 17β‐ and α‐busramustine, estradiol and chlorambucil were used for experimental chemo‐ and endocrino‐therapy against hormone‐dependent (T‐61) and independent (MX‐1) human breast carcinomas serially transplanted into BALB/cA female nude mice. Busramustine was administered po daily for 3 weeks at doses of 12.5–300 mg/kg for the β‐isomer and 25–300 mg/kg for the α‐isomer. Five to 50 mg of estradiol per kg was administered im once, and 3 to 6 mg of chlorambucil per kg was administered po daily for 3 weeks. All of the compounds were effective against estrogen receptor‐positive T‐61 with a clear dose‐response relationship, while estrogen receptor‐negative MX‐1 was sensitive to all of the agents except estradiol. Since the α‐isomer of busramustine was effective against both tumor lines, the mode of action of 17β‐busramustine may not be related to estrogenic action by estradiol released from the maternal compound. However, 17bT‐busramustine generated the estrogen receptor system of T‐61 tumor and resulted in the endometrial hyperplasia of tumor‐bearing nude mice, suggesting that this compound also has estrogenic action on transplanted human breast carcinoma and tumor‐bearing host mice, besides non‐estrogenic antitumor activity on human breast carcinoma xenografts.
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spelling pubmed-59176472018-05-11 Mode of Action of Estra‐1,3,5(10)‐triene‐3,17β‐diol 3‐Benzoate 17‐((4‐(4‐Bis(2‐chloroethyl)amino)phenyl)‐1‐oxobutoxy)acetate) on Human Breast Carcinoma Xenografts in Nude Mice Kubota, Tetsuro Koh, Jun‐ichi Yamada, Yoshinori Oka, Shoichi Enomoto, Koji Ishibiki, Kyuya Abe, Osahiko Masui, Osamu Asano, Kiro Jpn J Cancer Res Article To elucidate the mode of action of busramustine (KM2210), 17β‐ and α‐busramustine, estradiol and chlorambucil were used for experimental chemo‐ and endocrino‐therapy against hormone‐dependent (T‐61) and independent (MX‐1) human breast carcinomas serially transplanted into BALB/cA female nude mice. Busramustine was administered po daily for 3 weeks at doses of 12.5–300 mg/kg for the β‐isomer and 25–300 mg/kg for the α‐isomer. Five to 50 mg of estradiol per kg was administered im once, and 3 to 6 mg of chlorambucil per kg was administered po daily for 3 weeks. All of the compounds were effective against estrogen receptor‐positive T‐61 with a clear dose‐response relationship, while estrogen receptor‐negative MX‐1 was sensitive to all of the agents except estradiol. Since the α‐isomer of busramustine was effective against both tumor lines, the mode of action of 17β‐busramustine may not be related to estrogenic action by estradiol released from the maternal compound. However, 17bT‐busramustine generated the estrogen receptor system of T‐61 tumor and resulted in the endometrial hyperplasia of tumor‐bearing nude mice, suggesting that this compound also has estrogenic action on transplanted human breast carcinoma and tumor‐bearing host mice, besides non‐estrogenic antitumor activity on human breast carcinoma xenografts. Blackwell Publishing Ltd 1988-11 /pmc/articles/PMC5917647/ /pubmed/3147278 http://dx.doi.org/10.1111/j.1349-7006.1988.tb01548.x Text en
spellingShingle Article
Kubota, Tetsuro
Koh, Jun‐ichi
Yamada, Yoshinori
Oka, Shoichi
Enomoto, Koji
Ishibiki, Kyuya
Abe, Osahiko
Masui, Osamu
Asano, Kiro
Mode of Action of Estra‐1,3,5(10)‐triene‐3,17β‐diol 3‐Benzoate 17‐((4‐(4‐Bis(2‐chloroethyl)amino)phenyl)‐1‐oxobutoxy)acetate) on Human Breast Carcinoma Xenografts in Nude Mice
title Mode of Action of Estra‐1,3,5(10)‐triene‐3,17β‐diol 3‐Benzoate 17‐((4‐(4‐Bis(2‐chloroethyl)amino)phenyl)‐1‐oxobutoxy)acetate) on Human Breast Carcinoma Xenografts in Nude Mice
title_full Mode of Action of Estra‐1,3,5(10)‐triene‐3,17β‐diol 3‐Benzoate 17‐((4‐(4‐Bis(2‐chloroethyl)amino)phenyl)‐1‐oxobutoxy)acetate) on Human Breast Carcinoma Xenografts in Nude Mice
title_fullStr Mode of Action of Estra‐1,3,5(10)‐triene‐3,17β‐diol 3‐Benzoate 17‐((4‐(4‐Bis(2‐chloroethyl)amino)phenyl)‐1‐oxobutoxy)acetate) on Human Breast Carcinoma Xenografts in Nude Mice
title_full_unstemmed Mode of Action of Estra‐1,3,5(10)‐triene‐3,17β‐diol 3‐Benzoate 17‐((4‐(4‐Bis(2‐chloroethyl)amino)phenyl)‐1‐oxobutoxy)acetate) on Human Breast Carcinoma Xenografts in Nude Mice
title_short Mode of Action of Estra‐1,3,5(10)‐triene‐3,17β‐diol 3‐Benzoate 17‐((4‐(4‐Bis(2‐chloroethyl)amino)phenyl)‐1‐oxobutoxy)acetate) on Human Breast Carcinoma Xenografts in Nude Mice
title_sort mode of action of estra‐1,3,5(10)‐triene‐3,17β‐diol 3‐benzoate 17‐((4‐(4‐bis(2‐chloroethyl)amino)phenyl)‐1‐oxobutoxy)acetate) on human breast carcinoma xenografts in nude mice
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5917647/
https://www.ncbi.nlm.nih.gov/pubmed/3147278
http://dx.doi.org/10.1111/j.1349-7006.1988.tb01548.x
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