CYP24A1 inhibition facilitates the anti-tumor effect of vitamin D3 on colorectal cancer cells

doi:10.3748/wjg.v19.i17.2621

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World Journal of Gastroenterology

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1007-9327

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Baishideng Publishing Group Inc, 7041 Koll Center Parkway, Suite 160, Pleasanton, CA 94566, USA

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Original Article

World J Gastroenterol. May 7, 2013; 19(17): 2621-2628
Published online May 7, 2013. doi: 10.3748/wjg.v19.i17.2621

CYP24A1 inhibition facilitates the anti-tumor effect of vitamin D3 on colorectal cancer cells

Péter Lakatos, Henrik Horváth, Zsolt Nagy, István Takács, Gábor Speer, Evelin Horváth, Péter Mátyus, Bernadett Balla, Dóra Kovács, János Wölfling, Péter Horváth, János P Kósa

János P Kósa, Péter Horváth, Bernadett Balla, Evelin Horváth, Gábor Speer, István Takács, Zsolt Nagy, Henrik Horváth, Péter Lakatos, 1^st Department of Internal Medicine, Semmelweis University, H-1083 Budapest, Hungary

János Wölfling, Dóra Kovács, Department of Organic Chemistry, University of Szeged, H-6720 Szeged, Hungary

Péter Mátyus, Department of Organic Chemistry, Semmelweis University, H-1092 Budapest, Hungary

Author contributions: Kósa JP and Lakatos P designed and coordinated the study; Kósa JP, Horváth P, Balla B and Horváth E carried out the cell culture and mRNA experiments; Wölfling J, Kovács D and Mátyus P designed and synthesized the compounds used; Speer G, Takács I, Nagy Z and Horvath H contributed to the data analysis; Kósa JP and Horváth P wrote the paper.

Supported by Research Grants ETT 022/2006 and ETT 151/2009 from the Ministry of Health, Hungary; TÁMOP-4.2.1/B-09/1/KONV-2010-0005 from Creating the Center of Excellence at the University of Szeged, supported by the European Union and co-financed by the European Regional Fund

Correspondence to: János P Kósa, PhD, 1^st Department of Internal Medicine, Semmelweis University, Koranyi 2/a, H-1083 Budapest, Hungary. jkosa@bel1.sote.hu

Telephone: +36-1-2100278 Fax: +36-1-2104874

Received: May 23, 2012
Revised: August 21, 2012
Accepted: August 25, 2012
Published online: May 7, 2013

Abstract

AIM: The effects of vitamin D3 have been investigated on various tumors, including colorectal cancer (CRC). 25-hydroxyvitamin-D3-24-hydroxylase (CYP24A1), the enzyme that inactivates the active vitamin D3 metabolite 1,25-dihydroxyvitamin D3 (1,25-D3), is considered to be the main enzyme determining the biological half-life of 1,25-D3. During colorectal carcinogenesis, the expression and concentration of CYP24A1 increases significantly, suggesting that this phenomenon could be responsible for the proposed efficacy of 1,25-D3 in the treatment of CRC. The aim of this study was to investigate the anti-tumor effects of vitamin D3 on the human CRC cell line Caco-2 after inhibition of the cytochrome P450 component of CYP24A1 activity.

METHODS: We examined the expression of CYP24A1 mRNA and the effects of 1,25-D3 on the cell line Caco-2 after inhibition of CYP24A1. Cell viability and proliferation were determined by means of sulforhodamine-B staining and bromodeoxyuridine incorporation, respectively, while cytotoxicity was estimated via the lactate dehydrogenase content of the cell culture supernatant. CYP24A1 expression was measured by real-time reverse transcription polymerase chain reaction. A number of tetralone compounds were synthesized to investigate their CP24A1 inhibitory activity.

RESULTS: In response to 1,25-D3, CYP24A1 mRNA expression was enhanced significantly, in a time- and dose-dependent manner. Caco-2 cell viability and proliferation were not influenced by the administration of 1,25-D3 alone, but were markedly reduced by co-administration of 1,25-D3 and KD-35, a CYP24A1-inhibiting tetralone. Our data suggest that the mechanism of action of co-administered KD-35 and 1,25-D3 does not involve a direct cytotoxic effect, but rather the inhibition of cell proliferation.

CONCLUSION: These findings demonstrate that the selective inhibition of CYP24A1 by compounds such as KD-35 may be a new approach for enhancement of the anti-tumor effect of 1,25-D3 on CRC.

Keywords: Colorectal cancer; CYP24A1 inhibition; Vitamin D3; Tetralone derivatives; Caco-2 cell culture