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题名Small molecule inhibition of TFF3 overcomes tamoxifen resistance and enhances taxane efficacy in ER+ mammary carcinoma
作者
发表日期2023-11-28
发表期刊Cancer Letters
ISSN/eISSN0304-3835
卷号579
摘要

Even though tamoxifen has significantly improved the survival of estrogen receptor positive (ER+) mammary carcinoma (MC) patients, the development of drug resistance with consequent disease recurrence has limited its therapeutic efficacy. Trefoil factor-3 (TFF3) has been previously reported to mediate anti-estrogen resistance in ER+MC. Herein, the efficacy of a small molecule inhibitor of TFF3 (AMPC) in enhancing sensitivity and mitigating acquired resistance to tamoxifen in ER+MC cells was investigated. AMPC induced apoptosis of tamoxifen-sensitive and resistant ER+MC cells and significantly reduced cell survival in 2D and 3D culture in vitro. In addition, AMPC reduced cancer stem cell (CSC)-like behavior in ER+MC cells in a BCL2-dependent manner. Synergistic effects of AMPC and tamoxifen were demonstrated in ER+MC cells and AMPC was observed to improve tamoxifen efficacy in tamoxifen-sensitive cells and to re-sensitize cells to tamoxifen in tamoxifen-resistant ER+MC in vitro and in vivo. Additionally, tamoxifen-resistant ER+MC cells were concomitantly resistant to anthracycline, platinum and fluoropyrimidine drugs, but not to Taxanes. Taxane treatment of tamoxifen-sensitive and resistant ER+MC cells increased TFF3 expression indicating a combination vulnerability for tamoxifen-resistant ER+MC cells. Taxanes increased CSC-like behavior of tamoxifen-sensitive and resistant ER+MC cells which was reduced by AMPC treatment. Taxanes synergized with AMPC to promote apoptosis and reduce CSC-like behavior in vitro and in vivo. Hence, AMPC restored the sensitivity of tamoxifen and enhanced the efficacy of Taxanes in tamoxifen-resistant ER+MC. In conclusion, pharmacological inhibition of TFF3 may serve as an effective combinatorial therapeutic strategy for the treatment of tamoxifen-resistant ER+MC.

关键词AMPC ER+ mammary carcinoma Tamoxifen resistance Taxanes TFF3
DOI10.1016/j.canlet.2023.216443
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收录类别SCIE
语种英语English
WOS研究方向Oncology
WOS类目Oncology
WOS记录号WOS:001109918800001
Scopus入藏号2-s2.0-85175871147
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文献类型期刊论文
条目标识符https://repository.uic.edu.cn/handle/39GCC9TT/13162
专题个人在本单位外知识产出
通讯作者Lobie, Peter E.
作者单位
1.Tsinghua Berkeley Shenzhen Institute and the Institute of Biopharmaceutical and Health Engineering,Tsinghua Shenzhen International Graduate School,Tsinghua University,Shenzhen,518055,China
2.Laboratory of Chemical Biology,Department of Studies in Organic Chemistry,University of Mysore,Mysore,570006,India
3.The First Affiliated Hospital of USTC,Division of Life Sciences and Medicine,University of Science and Technology of China,Hefei,Anhui,China
4.The CAS Key Laboratory of Innate Immunity and Chronic Disease,Division of Life Sciences and Medicine,University of Science and Technology of China,Hefei,Anhui,China
5.Shenzhen Bay Laboratory,Shenzhen,Guangdong,518055,China
推荐引用方式
GB/T 7714
Guo, Hui,Tan, Yan Qin,Huang, Xiaominget al. Small molecule inhibition of TFF3 overcomes tamoxifen resistance and enhances taxane efficacy in ER+ mammary carcinoma[J]. Cancer Letters, 2023, 579.
APA Guo, Hui., Tan, Yan Qin., Huang, Xiaoming., Zhang, Shuwei., Basappa, Basappa., .. & Lobie, Peter E. (2023). Small molecule inhibition of TFF3 overcomes tamoxifen resistance and enhances taxane efficacy in ER+ mammary carcinoma. Cancer Letters, 579.
MLA Guo, Hui,et al."Small molecule inhibition of TFF3 overcomes tamoxifen resistance and enhances taxane efficacy in ER+ mammary carcinoma". Cancer Letters 579(2023).
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