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Merck

UHRF1 modulates breast cancer cell growth via estrogen signaling.

Medical oncology (Northwood, London, England) (2022-06-07)
Guosheng Luo, Quanhui Li, Miao Yu, Tianshi Wang, Yifeng Zang, Ziping Liu, Zhiguo Niu, Huijie Yang, Jianghua Lai
摘要

The ubiquitination process, which involves that binding of an ubiquitin protein to certain substrates, regulates several human biological processes and human cancers. Several studies report that the abnormal expression of quite a few E3 ubiquitin ligases could play critical role in carcinogenic process and cancer progression. In our current study, we identify UHRF1 (Ubiquitin Like with PHD And Ring Finger Domain 1) is an important regulator for breast cancer growth. UHRF1 depletion significantly decreases breast cancer growth in vitro and in vivo. Clinical data analysis reveals that UHRF1 is dramatically elevated in breast cancer, compared to normal breast tissue. UHRF1 correlates with poor survival in luminal type of breast cancer patients, but not in ER-negative groups. The molecular biological studies show that UHRF1 localizes in the nuclear and interact with ERα via its SRA domain, which subsequently inhibits K48-linked ubiquitination of ERα and enhances ERα stability. Our study provides a novel function of UHRF1 in regulation estrogen signaling in breast cancer and a promising target for breast cancer therapeutics.

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Anti-Actin-pan antibody produced in rabbit, affinity isolated antibody