Literature DB >> 23373735

Regulation of carboxylesterase-2 expression by p53 family proteins and enhanced anti-cancer activities among 5-fluorouracil, irinotecan and doxazolidine prodrug.

Da Xiao1, Dongfang Yang, Liangran Guo, Wei Lu, Margaret Charpentier, Bingfang Yan.   

Abstract

BACKGROUND AND
PURPOSE: For four decades, 5-fluorouracil (5-FU) has been a major anti-cancer medicine. This drug is increasingly used with other anti-cancer agents such as irinotecan. Irinotecan and many others such as PPD (pentyl carbamate of p-aminobenzyl carbamate of doxazolidine) require activation by carboxylesterase-2 (CES2). 5-FU, on the other hand, reportedly induces CES2 in colorectal tumour lines. The aims of this study were to determine the molecular basis for the induction and to ascertain interactive cell-killing activity between 5-FU and ester prodrugs. EXPERIMENTAL APPROACH: Colorectal and non-colorectal lines and xenografts were treated with 5-FU and the expression of CES2 was determined. Cell-killing activity of irinotecan and PPD were determined in the presence or absence of CES2 inhibitor. Several molecular experiments were used to determine the molecular basis for the induction. KEY
RESULTS: Without exceptions, robust induction was detected in cell lines expressing functional p53. High-level induction was also detected in xenografts. 5-FU pretreatment significantly increased cell-killing activity of irinotecan and PPD. Molecular experiments established that the induction was achieved by both transactivation and increased mRNA stability through p53. Either p63 or p73, functionally related to p53, did not support the transactivation. CONCLUSIONS AND IMPLICATIONS: The results in this study suggest that FOLFIRI, a common regimen combining irinotecan and 5-FU, should switch the dosing sequence, namely from 5-FU to irinotecan, to enhance hydrolytic activation of irinotecan. This modified order likely reduces the dose of anti-cancer agents, thus minimizing overall toxicity. The results also conclude that p53 family members act differently in regulating gene expression.
© 2013 The Authors. British Journal of Pharmacology © 2013 The British Pharmacological Society.

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Year:  2013        PMID: 23373735      PMCID: PMC3623067          DOI: 10.1111/bph.12125

Source DB:  PubMed          Journal:  Br J Pharmacol        ISSN: 0007-1188            Impact factor:   8.739


  45 in total

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Authors:  Michael H Wu; Bingfang Yan; Rod Humerickhouse; M Eileen Dolan
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8.  Hydrolysis of irinotecan and its oxidative metabolites, 7-ethyl-10-[4-N-(5-aminopentanoic acid)-1-piperidino] carbonyloxycamptothecin and 7-ethyl-10-[4-(1-piperidino)-1-amino]-carbonyloxycamptothecin, by human carboxylesterases CES1A1, CES2, and a newly expressed carboxylesterase isoenzyme, CES3.

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Journal:  Drug Metab Dispos       Date:  2004-07-28       Impact factor: 3.922

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3.  Carboxylesterase-2 is a highly sensitive target of the antiobesity agent orlistat with profound implications in the activation of anticancer prodrugs.

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5.  The Relationship between TP53 Gene Status and Carboxylesterase 2 Expression in Human Colorectal Cancer.

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6.  Prognostic Impact of Carboxylesterase 2 in Cholangiocarcinoma.

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7.  CES2, ABCG2, TS and Topo-I primary and synchronous metastasis expression and clinical outcome in metastatic colorectal cancer patients treated with first-line FOLFIRI regimen.

Authors:  Nicola Silvestris; Giovanni Simone; Giulia Partipilo; Emanuela Scarpi; Vito Lorusso; Anna Elisabetta Brunetti; Evaristo Maiello; Angelo Paradiso; Anita Mangia
Journal:  Int J Mol Sci       Date:  2014-09-05       Impact factor: 5.923

8.  High-throughput proteomics integrated with gene microarray for discovery of colorectal cancer potential biomarkers.

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9.  Combined use of irinotecan and p53 activator enhances growth inhibition of mesothelioma cells.

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  9 in total

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