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The multidrug resistance 1 (MDR1) gene polymorphism G-rs3789243-A is not associated with disease susceptibility in Norwegian patients with colorectal adenoma and colorectal cancer; a case control study

Author: A Ernst
A Imhof
A Nakano
AH Schinkel
AT Toriola
B Sarkadi
C Hilgendorf
C Vache
CF Skjelbred
CF Skjelbred
CP Gross
D Serre
D Wang
DB Goldstein
DL Kroetz
Dorte Jensen
E Buc
E Giovannucci
E Giovannucci
E Giovannucci
E Osswald
Elin Kure
G Gondal
GT Ho
H Suzuki
H Takane
JN Hirschhorn
Julian Hamfjord
Lene Agerstjerne
M Kurzawski
M Ostergaard
Mette Østergaard
Mona Sæbø
N Albermann
N Morita
N Soranzo
O Fantappie
P Boffetta
P Zubor
RD Hansen
RK Russell
RW Johnstone
S Hoffmeyer
S Kury
S Turgut
SA Miller
SY Bae
T Mizutani
UL Larsen
Ulla Vogel
V Annese
V Medici
Vibeke Andersen
Y Moriya
Publication venue: BioMed Central
Publication date: 01/01/2009
Field of study

Abstract Background Smoking, dietary factors, and alcohol consumption are known life style factors contributing to gastrointestinal carcinogenesis. Genetic variations in carcinogen handling may affect cancer risk. The multidrug resistance 1(<it>MDR1/ABCB1</it>) gene encodes the transport protein P-glycoprotein (a phase III xenobiotic transporter). P-glycoprotein is present in the intestinal mucosal lining and restricts absorption of certain carcinogens, among these polycyclic aromatic hydrocarbons. Moreover, P-glycoprotein transports various endogenous substrates such as cytokines and chemokines involved in inflammation, and may thereby affect the risk of malignity. Hence, genetic variations that modify the function of P-glycoprotein may be associated with the risk of colorectal cancer (CRC). We have previously found an association between the <it>MDR1 </it>intron 3 G-rs3789243-A polymorphism and the risk of CRC in a Danish study population. The aim of this study was to investigate if this <it>MDR1 </it>polymorphism was associated with risk of colorectal adenoma (CA) and CRC in the Norwegian population. Methods Using a case-control design, the association between the <it>MDR1 </it>intron 3 G-rs3789243-A polymorphism and the risk of colorectal carcinomas and adenomas in the Norwegian population was assessed in 167 carcinomas, 990 adenomas, and 400 controls. Genotypes were determined by allelic discrimination. Odds ratio (OR) and 95 confidence interval (95% CI) were estimated by binary logistic regression. Results No association was found between the <it>MDR1 </it>polymorphism (G-rs3789243-A) and colorectal adenomas or cancer. Carriers of the variant allele of MDR1 intron 3 had odds ratios (95% CI) of 0.97 (0.72–1.29) for developing adenomas, and 0.70 (0.41–1.21) for colorectal cancer, respectively, compared to homozygous wild type carriers. Conclusion The <it>MDR1 </it>intron 3 (G-rs3789243-A) polymorphism was not associated with a risk of colorectal adenomas or carcinomas in the present Norwegian study group. Thus, this <it>MDR1 </it>polymorphism does not seem to play an important role in colorectal carcinogenesis in this population.</p

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