Inhibition of prostate cancer cell growth in vivo with short hairpin RNA targeting SATB1
Qiang Wang, Shi‑Cheng Hu, Chun‑Sheng Yang, Jia‑Cun Chen, Jun‑Nian Zheng, Xiao‑Qing Sun, Jun‑Qi Wang
Journal:Oncology Letters
IF:1.39
DOI:10.3892/ol.2017.7006
PMID:29151908
Published:2017-09-20
research field:肿瘤学分子生物学基因治疗
Abstract
Despite previous advances, the treatment options for prostate cancer remain limited. For the purposes of gene knockdown, the utility of RNA interference has been demonstrated and is considered to have therapeutic potential. In the present study, a short hairpin RNA (shRNA) was used to assess the effect of special AT‑rich sequence binding protein (SATB1) downregulation on the growth and metastatic potential of prostate cancer in xenograft nude mice. A plasmid carrying shRNA targeting SATB1, pSilencer‑SATB1‑shRNA, was successfully engineered. Using this plasmid, significant downregulation of SATB1 mRNA and protein expression in the DU145 prostate cancer cells was observed. pSilencer‑SATB1‑shRNA was demonstrated to be markedly efficacious against prostate cancer xenografts in nude mice. These results may lead to a novel method of improving gene therapy efficacy against prostate cancer via regulating the function of SATB1.
本文使用的Yeasen产品


