Raloxifene-stimulated experimental breast cancer with the paradoxical actions of estrogen to promote or prevent tumor growth: A unifying concept in anti-hormone resistance

Detalhes bibliográficos
Autor(a) principal: Balaburski, Gregor M.
Data de Publicação: 2010
Outros Autores: Dardes, Rita de Cássia de Maio [UNIFESP], Johnson, Michael, Haddad, Bassem, Zhu, Fang, Ross, Eric A., Sengupta, Surojeet, Klein-Szanto, Andres, Liu, Hong, Lee, Eun Sook, Kim, Helen, Jordan, V. Craig
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Repositório Institucional da UNIFESP
Texto Completo: http://repositorio.unifesp.br/handle/11600/32758
http://dx.doi.org/10.3892/ijo_00000687
Resumo: We have previously demonstrated that prolonged treatments with raloxifene (RAL) in vitro will result in phase II RAL resistance and RAL-induced tumor growth. Clinical interest prompted us to re-examine RAL resistance in vivo, particularly the effects of long-term treatments (a decade or more) on the evolution of RAL resistance. in this study, we have addressed the question of this being a reproducible phenomenon in wild-type estrogen receptor (ER)-positive human breast cell line MCF-7. MCF-7 cells cultured under estrogen-deprived conditions in the presence of 1 mu M RAL for more than a year develop RAL, resistance resulting in an independent cell line, MCF7-RAL. the MCF7-RAL cells grow in response to both estradiol E, and RAL. Fulvestrant (FUL) blocks RAL and E(2)-mediated growth. Transplantation of MCF7-RAL cells into athymic ovariectomized mice and treatment with physiologic doses of E(2) causes early E(2)-stimulated tumor growth. in contrast, continuous treatment of implanted animals with daily oral RAL (1.5 mg daily) causes growth of small tumors within 15 weeks. Continuous re-transplantation of the tumors growing in RAL-treated mice indicated that RAL, stimulated tumor growth. Tumors in the untreated mice did not grow. Bi-transplantation of MCF7-E(2) and MCF7-RAL tumors into the opposing mammary fat pads of the same ovariectomized animal demonstrated that MCF7-E(2) grew with E(2) stimulation and not with RAL. Conversely. MCF7-RAL tumors grew with RAL and not E(2) a characteristic of phase II resistance. Established phase II resistance of MCF7-RAL tumors was confirmed following up to 7 years of serial transplantation in RAL-treated athymic mice. the ER alpha was retained in these tumors. the cyclical nature of RAL resistance was confirmed and extended during a 2-year evolution of the resistant phases of the MCF7-RAL tumors. the MCF7-RAL tumors that initially were inhibited by E(2) grew in the presence of E(2) and subsequently grew with either RAL or E(2). RAL remained the major grow stimulus and RAL enhanced E(2)-stimulated growth. Subsequent transplantation of E(2) stimulated tumors and evaluations of the actions of RAL, demonstrated robust E(2)-stimulated growth that was blocked by RAL. These are the characteristics of the anti-estrogenic actions of RAL on E(2)-stimulated breast cancer growth with a minor component of phase I RAL resistance. Continuous transplantation of the phase I RAL-stimulated tumors for >8 months causes reversion to phase II resistance. These data and literature reports of the cyclical nature of anti-androgen/androgen responsiveness of prostate cancer growth, illustrate the generality of the evolution of anti-hormonal resistance in sex steroid-sensitive target tissues.
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spelling Balaburski, Gregor M.Dardes, Rita de Cássia de Maio [UNIFESP]Johnson, MichaelHaddad, BassemZhu, FangRoss, Eric A.Sengupta, SurojeetKlein-Szanto, AndresLiu, HongLee, Eun SookKim, HelenJordan, V. CraigGeorgetown UnivFox Chase Canc CtrUniversidade Federal de São Paulo (UNIFESP)Northwestern Univ2016-01-24T14:05:15Z2016-01-24T14:05:15Z2010-08-01International Journal of Oncology. Athens: Spandidos Publ Ltd, v. 37, n. 2, p. 387-398, 2010.1019-6439http://repositorio.unifesp.br/handle/11600/32758http://dx.doi.org/10.3892/ijo_0000068710.3892/ijo_00000687WOS:000280024500017We have previously demonstrated that prolonged treatments with raloxifene (RAL) in vitro will result in phase II RAL resistance and RAL-induced tumor growth. Clinical interest prompted us to re-examine RAL resistance in vivo, particularly the effects of long-term treatments (a decade or more) on the evolution of RAL resistance. in this study, we have addressed the question of this being a reproducible phenomenon in wild-type estrogen receptor (ER)-positive human breast cell line MCF-7. MCF-7 cells cultured under estrogen-deprived conditions in the presence of 1 mu M RAL for more than a year develop RAL, resistance resulting in an independent cell line, MCF7-RAL. the MCF7-RAL cells grow in response to both estradiol E, and RAL. Fulvestrant (FUL) blocks RAL and E(2)-mediated growth. Transplantation of MCF7-RAL cells into athymic ovariectomized mice and treatment with physiologic doses of E(2) causes early E(2)-stimulated tumor growth. in contrast, continuous treatment of implanted animals with daily oral RAL (1.5 mg daily) causes growth of small tumors within 15 weeks. Continuous re-transplantation of the tumors growing in RAL-treated mice indicated that RAL, stimulated tumor growth. Tumors in the untreated mice did not grow. Bi-transplantation of MCF7-E(2) and MCF7-RAL tumors into the opposing mammary fat pads of the same ovariectomized animal demonstrated that MCF7-E(2) grew with E(2) stimulation and not with RAL. Conversely. MCF7-RAL tumors grew with RAL and not E(2) a characteristic of phase II resistance. Established phase II resistance of MCF7-RAL tumors was confirmed following up to 7 years of serial transplantation in RAL-treated athymic mice. the ER alpha was retained in these tumors. the cyclical nature of RAL resistance was confirmed and extended during a 2-year evolution of the resistant phases of the MCF7-RAL tumors. the MCF7-RAL tumors that initially were inhibited by E(2) grew in the presence of E(2) and subsequently grew with either RAL or E(2). RAL remained the major grow stimulus and RAL enhanced E(2)-stimulated growth. Subsequent transplantation of E(2) stimulated tumors and evaluations of the actions of RAL, demonstrated robust E(2)-stimulated growth that was blocked by RAL. These are the characteristics of the anti-estrogenic actions of RAL on E(2)-stimulated breast cancer growth with a minor component of phase I RAL resistance. Continuous transplantation of the phase I RAL-stimulated tumors for >8 months causes reversion to phase II resistance. These data and literature reports of the cyclical nature of anti-androgen/androgen responsiveness of prostate cancer growth, illustrate the generality of the evolution of anti-hormonal resistance in sex steroid-sensitive target tissues.Department of Defense, Center of ExcellenceSPORE in Breast CancerGenuardi's FundFCCCLynn Sage Breast Cancer Research FoundationWeg Fund of Fox Chase Cancer CenterCancer Center Support Grant (CCSG)Georgetown Univ, Med Ctr, Lombardi Comprehens Canc Ctr, Washington, DC 20057 USAFox Chase Canc Ctr, Philadelphia, PA 19111 USAUniversidade Federal de São Paulo, Dept Gynecol, BR-04535001 São Paulo, BrazilNorthwestern Univ, Robert H Lurie Comprehens Canc Ctr, Feinberg Sch Med, Chicago, IL 60611 USAUniversidade Federal de São Paulo, Dept Gynecol, BR-04535001 São Paulo, BrazilDepartment of Defense, Center of Excellence: BC050277SPORE in Breast Cancer: CA89018FCCC: NIH P30 CA006927Cancer Center Support Grant (CCSG): NIH P30 CA051008Web of Science387-398engSpandidos Publ LtdInternational Journal of Oncologyraloxifenetamoxifenosteoporosisbreast cancerRaloxifene-stimulated experimental breast cancer with the paradoxical actions of estrogen to promote or prevent tumor growth: A unifying concept in anti-hormone resistanceinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/articleinfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UNIFESPinstname:Universidade Federal de São Paulo (UNIFESP)instacron:UNIFESP11600/327582022-11-04 14:18:41.664metadata only accessoai:repositorio.unifesp.br:11600/32758Repositório InstitucionalPUBhttp://www.repositorio.unifesp.br/oai/requestopendoar:34652022-11-04T17:18:41Repositório Institucional da UNIFESP - Universidade Federal de São Paulo (UNIFESP)false
dc.title.en.fl_str_mv Raloxifene-stimulated experimental breast cancer with the paradoxical actions of estrogen to promote or prevent tumor growth: A unifying concept in anti-hormone resistance
title Raloxifene-stimulated experimental breast cancer with the paradoxical actions of estrogen to promote or prevent tumor growth: A unifying concept in anti-hormone resistance
spellingShingle Raloxifene-stimulated experimental breast cancer with the paradoxical actions of estrogen to promote or prevent tumor growth: A unifying concept in anti-hormone resistance
Balaburski, Gregor M.
raloxifene
tamoxifen
osteoporosis
breast cancer
title_short Raloxifene-stimulated experimental breast cancer with the paradoxical actions of estrogen to promote or prevent tumor growth: A unifying concept in anti-hormone resistance
title_full Raloxifene-stimulated experimental breast cancer with the paradoxical actions of estrogen to promote or prevent tumor growth: A unifying concept in anti-hormone resistance
title_fullStr Raloxifene-stimulated experimental breast cancer with the paradoxical actions of estrogen to promote or prevent tumor growth: A unifying concept in anti-hormone resistance
title_full_unstemmed Raloxifene-stimulated experimental breast cancer with the paradoxical actions of estrogen to promote or prevent tumor growth: A unifying concept in anti-hormone resistance
title_sort Raloxifene-stimulated experimental breast cancer with the paradoxical actions of estrogen to promote or prevent tumor growth: A unifying concept in anti-hormone resistance
author Balaburski, Gregor M.
author_facet Balaburski, Gregor M.
Dardes, Rita de Cássia de Maio [UNIFESP]
Johnson, Michael
Haddad, Bassem
Zhu, Fang
Ross, Eric A.
Sengupta, Surojeet
Klein-Szanto, Andres
Liu, Hong
Lee, Eun Sook
Kim, Helen
Jordan, V. Craig
author_role author
author2 Dardes, Rita de Cássia de Maio [UNIFESP]
Johnson, Michael
Haddad, Bassem
Zhu, Fang
Ross, Eric A.
Sengupta, Surojeet
Klein-Szanto, Andres
Liu, Hong
Lee, Eun Sook
Kim, Helen
Jordan, V. Craig
author2_role author
author
author
author
author
author
author
author
author
author
author
dc.contributor.institution.none.fl_str_mv Georgetown Univ
Fox Chase Canc Ctr
Universidade Federal de São Paulo (UNIFESP)
Northwestern Univ
dc.contributor.author.fl_str_mv Balaburski, Gregor M.
Dardes, Rita de Cássia de Maio [UNIFESP]
Johnson, Michael
Haddad, Bassem
Zhu, Fang
Ross, Eric A.
Sengupta, Surojeet
Klein-Szanto, Andres
Liu, Hong
Lee, Eun Sook
Kim, Helen
Jordan, V. Craig
dc.subject.eng.fl_str_mv raloxifene
tamoxifen
osteoporosis
breast cancer
topic raloxifene
tamoxifen
osteoporosis
breast cancer
description We have previously demonstrated that prolonged treatments with raloxifene (RAL) in vitro will result in phase II RAL resistance and RAL-induced tumor growth. Clinical interest prompted us to re-examine RAL resistance in vivo, particularly the effects of long-term treatments (a decade or more) on the evolution of RAL resistance. in this study, we have addressed the question of this being a reproducible phenomenon in wild-type estrogen receptor (ER)-positive human breast cell line MCF-7. MCF-7 cells cultured under estrogen-deprived conditions in the presence of 1 mu M RAL for more than a year develop RAL, resistance resulting in an independent cell line, MCF7-RAL. the MCF7-RAL cells grow in response to both estradiol E, and RAL. Fulvestrant (FUL) blocks RAL and E(2)-mediated growth. Transplantation of MCF7-RAL cells into athymic ovariectomized mice and treatment with physiologic doses of E(2) causes early E(2)-stimulated tumor growth. in contrast, continuous treatment of implanted animals with daily oral RAL (1.5 mg daily) causes growth of small tumors within 15 weeks. Continuous re-transplantation of the tumors growing in RAL-treated mice indicated that RAL, stimulated tumor growth. Tumors in the untreated mice did not grow. Bi-transplantation of MCF7-E(2) and MCF7-RAL tumors into the opposing mammary fat pads of the same ovariectomized animal demonstrated that MCF7-E(2) grew with E(2) stimulation and not with RAL. Conversely. MCF7-RAL tumors grew with RAL and not E(2) a characteristic of phase II resistance. Established phase II resistance of MCF7-RAL tumors was confirmed following up to 7 years of serial transplantation in RAL-treated athymic mice. the ER alpha was retained in these tumors. the cyclical nature of RAL resistance was confirmed and extended during a 2-year evolution of the resistant phases of the MCF7-RAL tumors. the MCF7-RAL tumors that initially were inhibited by E(2) grew in the presence of E(2) and subsequently grew with either RAL or E(2). RAL remained the major grow stimulus and RAL enhanced E(2)-stimulated growth. Subsequent transplantation of E(2) stimulated tumors and evaluations of the actions of RAL, demonstrated robust E(2)-stimulated growth that was blocked by RAL. These are the characteristics of the anti-estrogenic actions of RAL on E(2)-stimulated breast cancer growth with a minor component of phase I RAL resistance. Continuous transplantation of the phase I RAL-stimulated tumors for >8 months causes reversion to phase II resistance. These data and literature reports of the cyclical nature of anti-androgen/androgen responsiveness of prostate cancer growth, illustrate the generality of the evolution of anti-hormonal resistance in sex steroid-sensitive target tissues.
publishDate 2010
dc.date.issued.fl_str_mv 2010-08-01
dc.date.accessioned.fl_str_mv 2016-01-24T14:05:15Z
dc.date.available.fl_str_mv 2016-01-24T14:05:15Z
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/article
format article
status_str publishedVersion
dc.identifier.citation.fl_str_mv International Journal of Oncology. Athens: Spandidos Publ Ltd, v. 37, n. 2, p. 387-398, 2010.
dc.identifier.uri.fl_str_mv http://repositorio.unifesp.br/handle/11600/32758
http://dx.doi.org/10.3892/ijo_00000687
dc.identifier.issn.none.fl_str_mv 1019-6439
dc.identifier.doi.none.fl_str_mv 10.3892/ijo_00000687
dc.identifier.wos.none.fl_str_mv WOS:000280024500017
identifier_str_mv International Journal of Oncology. Athens: Spandidos Publ Ltd, v. 37, n. 2, p. 387-398, 2010.
1019-6439
10.3892/ijo_00000687
WOS:000280024500017
url http://repositorio.unifesp.br/handle/11600/32758
http://dx.doi.org/10.3892/ijo_00000687
dc.language.iso.fl_str_mv eng
language eng
dc.relation.ispartof.none.fl_str_mv International Journal of Oncology
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv 387-398
dc.publisher.none.fl_str_mv Spandidos Publ Ltd
publisher.none.fl_str_mv Spandidos Publ Ltd
dc.source.none.fl_str_mv reponame:Repositório Institucional da UNIFESP
instname:Universidade Federal de São Paulo (UNIFESP)
instacron:UNIFESP
instname_str Universidade Federal de São Paulo (UNIFESP)
instacron_str UNIFESP
institution UNIFESP
reponame_str Repositório Institucional da UNIFESP
collection Repositório Institucional da UNIFESP
repository.name.fl_str_mv Repositório Institucional da UNIFESP - Universidade Federal de São Paulo (UNIFESP)
repository.mail.fl_str_mv
_version_ 1802764182444048384

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