Pentagalloyl Glucose (PGG) Exhibits Anti-Cancer Activity against Aggressive Prostate Cancer by Modulating the ROR1 Mediated AKT-GSK3β Pathway

被引:0
作者
Sivaganesh, Vignesh [1 ,2 ]
Ta, Tram M. [1 ]
Peethambaran, Bela [1 ]
机构
[1] St Josephs Univ, Dept Biol, 600 S 43rd St, Philadelphia, PA 19104 USA
[2] Philadelphia Coll Osteopath Med, Dept Biomed Sci, 4170 City Ave, Philadelphia, PA 19131 USA
关键词
ROR1; receptor tyrosine kinase; pentagalloyl glucose; targeted therapy; prostate cancer; castration resistance; oncology; natural small molecule inhibitor; ACID-PHOSPHATASE; EXPRESSION; MECHANISMS; INHIBITOR; TARGET; CELLS; TRANSCRIPTION; PROGRESSION; RESISTANCE; APOPTOSIS;
D O I
10.3390/ijms25137003
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Androgen-receptor-negative, androgen-independent (ARneg-AI) prostate cancer aggressively proliferates and metastasizes, which makes treatment difficult. Hence, it is necessary to continue exploring cancer-associated markers, such as oncofetal Receptor Tyrosine Kinase like Orphan Receptor 1 (ROR1), which may serve as a form of targeted prostate cancer therapy. In this study, we identify that Penta-O-galloyl-beta-D-glucose (PGG), a plant-derived gallotannin small molecule inhibitor, modulates ROR1-mediated oncogenic signaling and mitigates prostate cancer phenotypes. Results indicate that ROR1 protein levels were elevated in the highly aggressive ARneg-AI PC3 cancer cell line. PGG was selectively cytotoxic to PC3 cells and induced apoptosis of PC3 (IC50 of 31.64 mu M) in comparison to normal prostate epithelial RWPE-1 cells (IC50 of 74.55 mu M). PGG was found to suppress ROR1 and downstream oncogenic pathways in PC3 cells. These molecular phenomena were corroborated by reduced migration, invasion, and cell cycle progression of PC3 cells. PGG minimally and moderately affected RWPE-1 and ARneg-AI DU145, respectively, which may be due to these cells having lower levels of ROR1 expression in comparison to PC3 cells. Additionally, PGG acted synergistically with the standard chemotherapeutic agent docetaxel to lower the IC50 of both compounds about five-fold (combination index = 0.402) in PC3 cells. These results suggest that ROR1 is a key oncogenic driver and a promising target in aggressive prostate cancers that lack a targetable androgen receptor. Furthermore, PGG may be a selective and potent anti-cancer agent capable of treating ROR1-expressing prostate cancers.
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页数:24
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