ERα negative breast cancer cells restore response to endocrine therapy by combination treatment with both HDAC inhibitor and DNMT inhibitor
Identifieur interne : 000C97 ( Main/Merge ); précédent : 000C96; suivant : 000C98ERα negative breast cancer cells restore response to endocrine therapy by combination treatment with both HDAC inhibitor and DNMT inhibitor
Auteurs : Jiang Fan [République populaire de Chine] ; Wen-Jin Yin [République populaire de Chine] ; Jin-Song Lu [République populaire de Chine] ; Lei Wang [République populaire de Chine] ; Jiong Wu [République populaire de Chine] ; Feng-Ying Wu [République populaire de Chine] ; Gen-Hong Di [République populaire de Chine] ; Zhen-Zhou Shen [République populaire de Chine] ; Zhi-Min Shao [République populaire de Chine]Source :
- Journal of Cancer Research and Clinical Oncology [ 0171-5216 ] ; 2008.
English descriptors
- Teeft :
- Annealing temperature, Breast, Breast cancer, Breast cancer cell, Breast cancer patient, Cell culture medium, Cell cycle, Cell growth, Clin, Clin cancer, Clin oncol, Combination treatment, Constant concentration, Deacetylase, Dnmt, Dnmt inhibitor, Dose responsive, Endocrine, Endocrine therapy, Endogenous gene, Epigenetic event, Epigenetic modiwcations, Error bar, Estrogen, Estrogen receptor, Evect, Functional estrogen receptor, Functional estrogen receptor alpha, Growth inhibition, Growth inhibition evect, Growth rate, Hdac, Hdac inhibitor, Histone, Histone deacetylase, Histone deacetylase inhibition, Histone deacetylase inhibitor, Histone deacetylase inhibitor trichostatin, Human breast cancer cell, Inhibitor, Mrna expression, National natural science foundation, Negative breast cancer cell, Negative human breast cancer cell, Novel histone deacetylase inhibitor, Nude mouse, Oncol, Ovarectomy, Phase arrest, Predictive factor, Proliferation rate, Receptor, Representative quantitation, Same time, Sample buver, Standard error, Synergistic activation, Tamoxifen, Tamoxifen treatment, Treatment group, Trichostatin, Vehicle control, Xenograft, Xenograft volume.
Abstract
Abstract: Purpose: Estrogen receptor α (ERα) mediates the growth stimulation of estrogen in breast cancer cells and is a useful predictive factor for response to endocrine therapy. It is reported that ERα was induced in ERα negative breast cancer cells by both DNA methyltransferase-1 (DNMT1) inhibitor 5-aza-2′-deoxycytidine (AZA) and histone deacetylase (HDAC) inhibitor trichostatin A (TSA). However, whether the breast cancer cells with induced ERα restore response to endocrine therapy requires to be further researched. Patients and methods: Reverse transcriptase-polymerase chain reaction (RT-PCR) method was used to explore the change in the mRNA of ERα, PR and pS2 in the ERα negative breast cancer cells MDA-MB-435 treated with two chemicals (AZA + TSA). Water-soluble tetrazolium salt-8 (WST-8) method was used to study the proliferation rate of the breast cancer cells. Flow cytometer (FCW) was used to analyze the distribution of cell cycle of these breast cancer cells. Some xenograft models in nude mice were used to further study the results we found in vitro. Results: In this study we observed that the mRNA of ERα, PR and pS2 in the ERα negative breast cancer cells MDA-MB-435 was re-expressed by treatment with AZA + TSA. The proliferation assay analysis showed AZA + TSA suppressed the proliferation of MDA-MB-435 cells, which were further suppressed by addition of 4-OH Tamoxifen (4-OHT). On the contrary, the proliferation of cells treated with 4-OHT alone showed no difference compared with the vehicle control. Cell cycle analysis showed AZA + TSA treated cells showed S phase arrest, which was partially attenuated by addition of estradiol (E2); furthermore, the effect of E2 on stimulation of cell cycle could be reversed by 4-OHT in the treated cells with induced ERα. In vivo experiment xenograft volume of MDA-MB-435 cells treated with AZA + TSA was smaller than that of the control (P < 0.01), and the xenograft of AZA + TSA treated cells was further suppressed by ovarectomy (P < 0.01). Conclusions: Our data indicate that DNMT1 inhibitor AZA and HDAC inhibitor TSA play important roles in restoring sensitivity of the ERα negative breast cancer cells to endocrine therapy in vitro and in vivo.
Url:
DOI: 10.1007/s00432-008-0354-x
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uniqKey="Wang L" first="Lei" last="Wang">Lei Wang</name><affiliation wicri:level="1"><country xml:lang="fr">République populaire de Chine</country><wicri:regionArea>Department of Breast Surgery, Cancer Hospital/Cancer Institute, Fudan University, 399 Ling-Ling Road, 200032, Shanghai</wicri:regionArea><wicri:noRegion>Shanghai</wicri:noRegion></affiliation><affiliation></affiliation></author><author><name sortKey="Wu, Jiong" sort="Wu, Jiong" uniqKey="Wu J" first="Jiong" last="Wu">Jiong Wu</name><affiliation wicri:level="1"><country xml:lang="fr">République populaire de Chine</country><wicri:regionArea>Department of Breast Surgery, Cancer Hospital/Cancer Institute, Fudan University, 399 Ling-Ling Road, 200032, Shanghai</wicri:regionArea><wicri:noRegion>Shanghai</wicri:noRegion></affiliation><affiliation></affiliation></author><author><name sortKey="Wu, Feng Ying" sort="Wu, Feng Ying" uniqKey="Wu F" first="Feng-Ying" last="Wu">Feng-Ying Wu</name><affiliation wicri:level="1"><country xml:lang="fr">République populaire de Chine</country><wicri:regionArea>Department of Breast Surgery, Cancer Hospital/Cancer Institute, Fudan University, 399 Ling-Ling Road, 200032, Shanghai</wicri:regionArea><wicri:noRegion>Shanghai</wicri:noRegion></affiliation><affiliation></affiliation></author><author><name sortKey="Di, Gen Hong" sort="Di, Gen Hong" uniqKey="Di G" first="Gen-Hong" last="Di">Gen-Hong Di</name><affiliation wicri:level="1"><country xml:lang="fr">République populaire de Chine</country><wicri:regionArea>Department of Breast Surgery, Cancer Hospital/Cancer Institute, Fudan University, 399 Ling-Ling Road, 200032, Shanghai</wicri:regionArea><wicri:noRegion>Shanghai</wicri:noRegion></affiliation><affiliation wicri:level="1"><country wicri:rule="url">République populaire de Chine</country></affiliation></author><author><name sortKey="Shen, Zhen Zhou" sort="Shen, Zhen Zhou" uniqKey="Shen Z" first="Zhen-Zhou" last="Shen">Zhen-Zhou Shen</name><affiliation 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level="j" type="abbrev">J Cancer Res Clin Oncol</title><idno type="ISSN">0171-5216</idno><idno type="eISSN">1432-1335</idno><imprint><publisher ref="https://scientific-publisher.data.istex.fr/ark:/67375/H02-SWLMH5L1-1">Springer-Verlag</publisher><pubPlace>Berlin/Heidelberg</pubPlace><date type="published" when="2008">2008</date><biblScope unit="vol" from="134" to="134">134</biblScope><biblScope unit="issue" from="8" to="8">8</biblScope><biblScope unit="page" from="883">883</biblScope><biblScope unit="page" to="890">890</biblScope></imprint><idno type="ISSN">0171-5216</idno></series></biblStruct></sourceDesc><seriesStmt><idno type="ISSN">0171-5216</idno></seriesStmt></fileDesc><profileDesc><textClass><keywords scheme="Teeft" xml:lang="en"><term>Annealing temperature</term><term>Breast</term><term>Breast cancer</term><term>Breast cancer cell</term><term>Breast cancer patient</term><term>Cell culture medium</term><term>Cell cycle</term><term>Cell growth</term><term>Clin</term><term>Clin cancer</term><term>Clin oncol</term><term>Combination treatment</term><term>Constant concentration</term><term>Deacetylase</term><term>Dnmt</term><term>Dnmt inhibitor</term><term>Dose responsive</term><term>Endocrine</term><term>Endocrine therapy</term><term>Endogenous gene</term><term>Epigenetic event</term><term>Epigenetic modiwcations</term><term>Error bar</term><term>Estrogen</term><term>Estrogen receptor</term><term>Evect</term><term>Functional estrogen receptor</term><term>Functional estrogen receptor alpha</term><term>Growth inhibition</term><term>Growth inhibition evect</term><term>Growth rate</term><term>Hdac</term><term>Hdac inhibitor</term><term>Histone</term><term>Histone deacetylase</term><term>Histone deacetylase inhibition</term><term>Histone deacetylase inhibitor</term><term>Histone deacetylase inhibitor trichostatin</term><term>Human breast cancer cell</term><term>Inhibitor</term><term>Mrna expression</term><term>National natural science foundation</term><term>Negative breast cancer cell</term><term>Negative human breast cancer cell</term><term>Novel histone deacetylase inhibitor</term><term>Nude mouse</term><term>Oncol</term><term>Ovarectomy</term><term>Phase arrest</term><term>Predictive factor</term><term>Proliferation rate</term><term>Receptor</term><term>Representative quantitation</term><term>Same time</term><term>Sample buver</term><term>Standard error</term><term>Synergistic activation</term><term>Tamoxifen</term><term>Tamoxifen treatment</term><term>Treatment group</term><term>Trichostatin</term><term>Vehicle control</term><term>Xenograft</term><term>Xenograft volume</term></keywords></textClass></profileDesc></teiHeader><front><div type="abstract" xml:lang="en">Abstract: Purpose: Estrogen receptor α (ERα) mediates the growth stimulation of estrogen in breast cancer cells and is a useful predictive factor for response to endocrine therapy. It is reported that ERα was induced in ERα negative breast cancer cells by both DNA methyltransferase-1 (DNMT1) inhibitor 5-aza-2′-deoxycytidine (AZA) and histone deacetylase (HDAC) inhibitor trichostatin A (TSA). However, whether the breast cancer cells with induced ERα restore response to endocrine therapy requires to be further researched. Patients and methods: Reverse transcriptase-polymerase chain reaction (RT-PCR) method was used to explore the change in the mRNA of ERα, PR and pS2 in the ERα negative breast cancer cells MDA-MB-435 treated with two chemicals (AZA + TSA). Water-soluble tetrazolium salt-8 (WST-8) method was used to study the proliferation rate of the breast cancer cells. Flow cytometer (FCW) was used to analyze the distribution of cell cycle of these breast cancer cells. Some xenograft models in nude mice were used to further study the results we found in vitro. Results: In this study we observed that the mRNA of ERα, PR and pS2 in the ERα negative breast cancer cells MDA-MB-435 was re-expressed by treatment with AZA + TSA. The proliferation assay analysis showed AZA + TSA suppressed the proliferation of MDA-MB-435 cells, which were further suppressed by addition of 4-OH Tamoxifen (4-OHT). On the contrary, the proliferation of cells treated with 4-OHT alone showed no difference compared with the vehicle control. Cell cycle analysis showed AZA + TSA treated cells showed S phase arrest, which was partially attenuated by addition of estradiol (E2); furthermore, the effect of E2 on stimulation of cell cycle could be reversed by 4-OHT in the treated cells with induced ERα. In vivo experiment xenograft volume of MDA-MB-435 cells treated with AZA + TSA was smaller than that of the control (P < 0.01), and the xenograft of AZA + TSA treated cells was further suppressed by ovarectomy (P < 0.01). Conclusions: Our data indicate that DNMT1 inhibitor AZA and HDAC inhibitor TSA play important roles in restoring sensitivity of the ERα negative breast cancer cells to endocrine therapy in vitro and in vivo.</div></front></TEI></record>Pour manipuler ce document sous Unix (Dilib)
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