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Inactivation of ID4 promotes a CRPC phenotype with constitutive AR activation through FKBP52.

Mol Oncol. 2019-04; 
JoshiJugal Bharat, PatelDivya, MortonDerrick J, SharmaPankaj, ZouJin, Hewa BostanthirigeDhanushka, GorantlaYamini, NagappanPeri, KomaragiriShravan Kumar, SivilsJeffrey C, XieHuan, PalaniappanRavi, WangGuangdi, CoxMarc B, ChaudharyJai
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Catalog Antibody … Co‐immunoprecipitation analysis using ID4‐specific antibody on L+ns cells was performed with the help of protein A coupled to magnetic beads (Protein A Mag beads; GenScript, Piscataway, NJ, USA) as per the manufacturer's instructions … Get A Quote

摘要

Castration-resistant prostate cancer (CRPC) is the emergence of prostate cancer cells that have adapted to the androgen-depleted environment of the prostate. In recent years, targeting multiple chaperones and co-chaperones (e.g., Hsp27, FKBP52) that promote androgen receptor (AR) signaling and/or novel AR regulatory mechanisms have emerged as promising alternative treatments for CRPC. We have shown that inactivation of inhibitor of differentiation 4 (ID4), a dominant-negative helix loop helix protein, promotes de?novo steroidogenesis and CRPC with a gene expression signature that resembles constitutive AR activity in castrated mice. In this study, we investigated the underlying mechanism through whi... More

關鍵詞

HLH , PSA ,FKBP51,FKBP52,Hsp27,Hsp90,ID4,MJC13,androgen receptor,castration-resistant,prostate ca
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