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ER-α36-mediated rapid estrogen signaling positively regulates ER-positive breast cancer stem/progenitor cells.

PLoS ONE. 2014; 
Deng H, Zhang XT, Wang ML, Zheng HY, Liu LJ, Wang ZY.
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PCR Cloning and Subcloning To establish stable cell lines with knocked-down expression of ER-a36 from T47D cells, we constructed an ER-a36 specific shRNA expression vector by cloning the DNA oligonucleotides 59-GATGCCAATAGG- TACTGAATTGATATCCGTTCAGTACCTATTGGCAT-39 targeting the sequence in the 39UTR of ER-a36 gene into the ER-a36 in Breast Cancer Stem Cells from GenScript Corp....1/Neo expression vector from GenScript Corp. Get A Quote

摘要

The breast cancer stem cells (BCSC) play important roles in breast cancer occurrence, recurrence and metastasis. However, the role of estrogen signaling, a signaling pathway important in development and progression of breast cancer, in regulation of BCSC has not been well established. Previously, we identified and cloned a variant of estrogen receptor α, ER-α36, with a molecular weight of 36 kDa. ER-α36 lacks both transactivation domains AF-1 and AF-2 of the 66 kDa full-length ER-α (ER-α66) and mediates rapid estrogen signaling to promote proliferation of breast cancer cells. In this study, we aim to investigate the function and the underlying mechanism of ER-α36-mediated rapid estrogen signaling in growt... More

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