Literature DB >> 19395473

Polyethylene glycosylated curcumin conjugate inhibits pancreatic cancer cell growth through inactivation of Jab1.

Jun Li1, Yun Wang, Chaozhe Yang, Pengfei Wang, Denise K Oelschlager, Yong Zheng, De-An Tian, William E Grizzle, Donald J Buchsbaum, Mei Wan.   

Abstract

Jab1 (Jun activation domain binding protein 1), integrated into COP9 signalosome complex (CSN), induces protein instability of many tumor suppressors and cell cycle regulators and is therefore a novel target in cancer therapy. Curcumin, an inhibitor of Jab1/CSN-associated kinase(s), has been reported to suppress tumor growth; however, curcumin is highly hydrophobic, and this feature prevents its usage as an antitumor drug. To increase the solubility and targeted delivery, we generated a water-soluble polyethylene glycol (PEG)-conjugated curcumin system, in which curcumin is covalently linked to PEG(35kD). PEGylated curcumin showed much greater reduction of cell growth than free curcumin in pancreatic cancer cells. Cells treated with PEGylated curcumin had increased arrest at the mitotic phase with the formation of abnormal multinucleated cells, indicating that this compound affects cell cycle progression, which may contribute to cell growth inhibition. The stabilities of Jab1 target proteins were also examined. PEGylated curcumin increased protein stability of these proteins in pancreatic cancer cells and directly inhibited the activity of Jab1/CSN-associated kinases. Moreover, the inhibitory effect of PEGylated curcumin on cell proliferation was blunted in pancreatic cancer cells with Jab1 knockdown. The results suggest that PEGylated curcumin inhibits cell proliferation through suppression of Jab1/CSN activity. More importantly, the new compound sensitized pancreatic cancer cells to gemcitabine-induced apoptosis and cell proliferation inhibitory effects. Collectively, the PEGylated curcumin conjugate has much more potent effects on pancreatic cancer cell growth inhibition than free curcumin. The current study provides a biologic rationale to treat patients with pancreatic adenocarcinoma with the nontoxic phytochemical conjugated to PEG for systemic delivery.

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Year:  2009        PMID: 19395473     DOI: 10.1124/mol.109.054551

Source DB:  PubMed          Journal:  Mol Pharmacol        ISSN: 0026-895X            Impact factor:   4.436


  32 in total

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Authors:  Murali M Yallapu; Meena Jaggi; Subhash C Chauhan
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Journal:  Inflammation       Date:  2018-03       Impact factor: 4.092

4.  Therapeutic potential of curcumin in gastrointestinal diseases.

Authors:  Sigrid A Rajasekaran
Journal:  World J Gastrointest Pathophysiol       Date:  2011-02-15

5.  DM-1, sodium 4-[5-(4-hydroxy-3-methoxyphenyl)-3-oxo-penta-1,4-dienyl]-2-methoxy-phenolate: a curcumin analog with a synergic effect in combination with paclitaxel in breast cancer treatment.

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6.  Big punches come in nanosizes for chemoprevention.

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7.  Chemogenomic study of gemcitabine using Saccharomyces cerevisiae as model cell-molecular insights about chemoresistance.

Authors:  Lucas de Sousa Cavalcante; Tales A Costa-Silva; Tiago Antônio Souza; Susan Ienne; Gisele Monteiro
Journal:  Braz J Microbiol       Date:  2019-09-12       Impact factor: 2.476

8.  Nanochemoprevention by bioactive food components: a perspective.

Authors:  Imtiaz A Siddiqui; Hasan Mukhtar
Journal:  Pharm Res       Date:  2010-03-11       Impact factor: 4.200

9.  Therapeutic potential of curcumin and curcumin analogues in rheumatology.

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Journal:  Int J Rheum Dis       Date:  2015-07       Impact factor: 2.454

Review 10.  Emerging roles of Jab1/CSN5 in DNA damage response, DNA repair, and cancer.

Authors:  Yunbao Pan; Huiling Yang; Francois X Claret
Journal:  Cancer Biol Ther       Date:  2014-02-04       Impact factor: 4.742

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