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Publication Date:
July 2007
ISSN:
1437-4331
DOI:
10.1515/CCLM.2007.143

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Clinical Chemistry and Laboratory Medicine (CCLM)

Published in Association with the International Federation of Clinical Chemistry and Laboratory Medicine and the European Federation of Clinical Chemistry and Laboratory Medicine

Editor-in-Chief: Plebani, Mario

Editorial Board Member: Lippi, Giuseppe / Gillery, Philippe / Kazmierczak, Steven / Lackner, Karl J. / Melichar, Bohuslav / Siest, Gérard / Whitfield, John B. / Abi Fadel, Marianne / Alvarez Menendez, Francisco V. / Azzazy, Hassan M.E. / Diamandis, Eleftherios P. / Eckardstein, Arnold / Favaloro, Emmanuel J. / Griesmacher, Andrea / Herrmann, Wolfgang / Hoffmann, Johannes J.M.L. / Hooijkaas, Herbert / Ichihara, Kiyoshi / Kaabachi, Naziha / Kim, Jeong-Ho / Korte, Wolfgang / Kroupis, Christos / Lai, Leslie Charles / Lam, Wai Kei Christopher / Marc, Janja / Miyoshi, Eiji / Özben, Tomris / Palicka, Vladimir / Panteghini, Mauro / Queralto, Jose M. / Scartezini, Marileia / Simundic, Ana-Maria / Tsongalis, Gregory J. / Wallemacq, Pierre E. / Yan, Shengkai / Young, Ian S. / Chiu, Rossa Wai Kwun / Ghosh, Debabrata / Kappelmayer, Janos / Lehmann, Sylvain / Sypniewska, Grazyna

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Increased IMPACT FACTOR 2011: 2.150
Rank 10 out of 32 in category Medical Laboratory Technology in the 2011 Thomson Reuters Journal Citation Report/Science Edition

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Polymorphisms in genes involved in DNA repair and metabolism of xenobiotics in individual susceptibility to sporadic diffuse gastric cancer

Annamaria Ruzzo1 / Emanuele Canestrari2 / Paolo Maltese3 / Francesca Pizzagalli4 / Francesco Graziano5 / Daniele Santini6 / Vincenzo Catalano7 / Rita Ficarelli8 / Davide Mari9 / Renato Bisonni10 / Paolo Giordani11 / Lucio Giustini12 / Paolo Lippe13 / Rosarita Silva14 / Rodolfo Mattioli15 / Umberto Torresi16 / Luciano Latini17 / Mauro Magnani18

1Institute of Biochemistry ‘G. Fornaini’, University of Urbino, Urbino, Italy

2Institute of Biochemistry ‘G. Fornaini’, University of Urbino, Urbino, Italy

3Institute of Biochemistry ‘G. Fornaini’, University of Urbino, Urbino, Italy

4Institute of Biochemistry ‘G. Fornaini’, University of Urbino, Urbino, Italy

5Medical Oncology Unit, Hospital of Urbino, Urbino, Italy

6Medical Oncology, University Campus Biomedico, Rome, Italy

7Medical Oncology, Hospital of Pesaro, Pesaro, Italy

8Medical Oncology, Hospital of Senigallia, Senigallia, Italy

9Medical Oncology, Hospital of Fabriano, Fabriano, Italy

10Medical Oncology, Hospital of Fermo, Fermo, Italy

11Medical Oncology, Hospital of Pesaro, Pesaro, Italy

12Medical Oncology, Hospital of Fermo, Fermo, Italy

13Medical Oncology, Hospital of Fermo, Fermo, Italy

14Medical Oncology, Hospital of Fabriano, Fabriano, Italy

15Medical Oncology, Hospital of Fano, Fano, Italy

16Medical Oncology, Hospital of Macerata, Macerata, Italy

17Medical Oncology, Hospital of Macerata, Macerata, Italy

18Institute of Biochemistry ‘G. Fornaini’, University of Urbino, Urbino, Italy

Corresponding author: Annamaria Ruzzo, Institute of Biochemistry ‘G. Fornaini’, University of Urbino, Urbino, Italy Phone: +39-0722-305252, Fax: +39-0722-320188

Citation Information: Clinical Chemical Laboratory Medicine. Volume 45, Issue 7, Pages 822–828, ISSN (Online) 14374331, ISSN (Print) 14346621, DOI: 10.1515/CCLM.2007.143, July 2007

Publication History:
Received:
2006-09-26
Accepted:
2007-02-20
Published Online:
2007-07-08

Abstract

Background: Gastric cancer is the second highest cause of cancer mortality in the world, despite declining rates of incidence in many industrialized countries. We carried out a case-control study to evaluate whether polymorphisms of DNA repair and glutathione S-transferase (GST) genes modulate the risk of developing diffuse gastric cancer.

Methods: ERCC1 118 T/C, XRCC1 399 G/A, XPD 312 G/A, XPD 751 A/C, XRCC3 241 C/T, MS 919 A/G, GSTP1 105 A/G, GSTM1-null/positive and GSTT1-null/positive genotypes were obtained for a series of 126 Helicobacter pylori-negative diffuse gastric cancer patients and 144 Helicobacter pylori-negative controls sampled from the population of Marche, an area with high gastric cancer risk in central Italy.

Results: GSTP1 105 A/G and GSTP1 105 G/G genotypes were identified as protective factors, with odds ratio (OR) of 0.4 (95% CI 0.17–0.81, p=0.01) and OR=0.58 (95% CI 0.33–1, p=0.05), respectively. GSTT1-null genotype was identified as a protective factor, with OR=0.48 (95% CI 0.22–0.99, p=0.04). There was no significant difference between cases and controls for XPD 751 A/C, ERCC1 118 T/C, XRCC3 241 C/T, XRCC1 399 G/A, XPD 312 G/A, GSTM1-null/positive and MS 919 A/G polymorphisms.

Conclusions: This study suggests that GSTP1 105A/G and GSTT1-null/positive genotypes might be associated with a reduced risk for sporadic diffuse gastric cancer.

Clin Chem Lab Med 2007;45:822–8.

Keywords: diffuse gastric cancer; DNA repair; GSTM1; GSTP1; GSTT1; polymorphisms

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