2-Phenyl-5-(pyrrolidin-1-yl)-1-(3,4,5-trimethoxybenzyl)-1H-benzimidazole, a benzimidazole derivative, inhibits growth of human prostate cancer cells by affecting tubulin and c-Jun N-terminal kinase
Journal
British Journal of Pharmacology
Journal Volume
160
Journal Issue
7
Pages
1677-1689
Date Issued
2010
Author(s)
Abstract
BACKGROUND AND PURPOSE The c-Jun N-terminal kinase (JNK) and tubulin are, frequently, targets for developing anti-cancer drugs. A major obstacle to successful development is P-glycoprotein (P-gp)-mediated resistance. Here, we have assessed a compound that inhibited growth of cancer cells, for effects on JNK and tubulin and as a substrate for P-gp. EXPERIMENTAL APPROACH Several pharmacological and biochemical assays were used to characterize signalling pathways of 2-phenyl-5-(pyrrolidin-1-yl)-1-(3,4,5-trimethoxybenzyl)-1H- benzimidazole (PPTMB), a benzimidazole analogue, in prostate cancer cells. KEY RESULTS PPTMB inhibited proliferation of several human prostate cancer cell lines. It displayed similar activity against a P-gp-rich cell line, indicating that PPTMB was not a substrate for P-gp. PPTMB induced G2/M arrest of the cell cycle and subsequent apoptosis, using flow cytometry. Tubulin polymerization assays and Western blot analysis showed that PPTMB directly acted on tubulin and caused disruption of microtubule dynamics, inducing mitotic arrest and sustained high levels of cyclin B1 expression and Cdk1 activation. Subsequently, mitochondria-related apoptotic cascades were induced, including Bcl-2 and Bcl-xL phosphorylation, Mcl-1 down-regulation, truncated Bad formation and activation of caspase-9 and -3. PPTMB stimulated JNK phosphorylation at Thr 183/Tyr 185. SP600125, a specific JNK inhibitor, significantly inhibited apoptotic signalling, indicating that JNK plays a key role in PPTMB action. PPTMB showed a 10-fold higher potency against prostate cancer cells than normal prostate cells. CONCLUSIONS AND IMPLICATIONS PPTMB is an effective anti-cancer agent. It disrupted microtubule dynamics, leading to mitotic arrest of the cell cycle and JNK activation, which in turn stimulated the mitochondria-related apoptotic cascades in prostate cancer cells. ? 2010 The Authors. Journal compilation ? 2010 The British Pharmacological Society.
Subjects
cell cycle progression; intrinsic apoptotic pathway; JNK; microtubule; prostate cancer
SDGs
Other Subjects
2 phenyl 5 (pyrrolidin 1 yl) 1 (3,4,5 trimethoxybenzyl) 1h benzimidazole; anthra[1,9 cd]pyrazol 6(2h) one; antineoplastic agent; benzimidazole derivative; caspase 3; caspase 9; cyclin B1; cyclin dependent kinase 1; glycoprotein P; mitogen activated protein kinase; paclitaxel; protein BAD; protein bcl 2; protein bcl xl; protein mcl 1; threonine; tubulin; tyrosine; unclassified drug; vincristine; apoptosis; article; cancer cell; cancer growth; cancer inhibition; cell cycle arrest; cell cycle G2 phase; cell cycle M phase; cell proliferation; cell strain LNCaP; competitive inhibition; controlled study; down regulation; drug potency; enzyme activation; enzyme substrate; flow cytometry; human; human cell; human tissue; male; microtubule; mitochondrion; mitosis; polymerization; priority journal; prostate cancer; protein expression; protein phosphorylation; signal transduction; Western blotting; Anisoles; Antineoplastic Agents; Apoptosis; Benzimidazoles; Blotting, Western; Cell Cycle; Cell Line, Tumor; Cell Proliferation; Drug Resistance, Neoplasm; Flow Cytometry; Humans; JNK Mitogen-Activated Protein Kinases; Male; Microtubules; Mitotic Spindle Apparatus; Molecular Structure; P-Glycoprotein; Prostatic Neoplasms; Substrate Specificity; Tubulin
Type
journal article