[No authors listed]
Tamoxifen is widely used as a highly effective drug for treating estrogenâreceptor (ER) alphaâpositive breast cancer. However, tamoxifen resistance developed during cancer treatment remains a significant challenge. Tongue cancer resistanceârelated protein1 (TCRP1), which is recognized as a novel drug target, is related to chemoâresistance in human cancers, moreover, it is often overexpressed in various cancer cells, such as in lung cancer, breast cancer, and tongue cancer. However, the effects of TCRP1 on tamoxifenâresistant breast cancer cells and tissues are far from clear. The present study revealed that TCRP1 induced tamoxifen resistance in breast cancer cells. Western blotting, quantitative realâtime polymerase chain reaction (RTâPCR) and immunohistochemical staining were performed to detect the expression level of TCRP1 in vivo and in vitro between primary breast cancer tissues and tamoxifenâresistant breast cancer tissues. The data revealed that the expression of TCRP1 was upregulated in the tamoxifenâresistant breast cancer tissues and human breast cancer cell line, MCFâ7. Further study revealed that knocking down TCRP1 inhibited the growth of MCFâ7 cells with tamoxifenâresistance (MCF7âR cells) and induced cell apoptosis. Moreover, TCRP1 promoted serumâ and glucocorticoidâinducible kinase 1 (SGK1) activation via phosphorylation of phosphoinositideâdependent kinase 1 (PDK1) in MCF7âR cells. In addition, it was also observed that knocking down TCRP1 inhibited tumorigenesis of MCFâ7 cells in nude mice. In conclusion, these data indicated that TCRP1 could induce tamoxifen resistance by regulating the PDK1/SGK1 signaling pathway. Thus, TCRP1 could be explored as a promising candidate for treating tamoxifenâresistant breast cancer in the future.
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