Polymorphism in the oxytocin promoter region in patients with lactase non-persistence is not related to symptoms

A Larcher; B Ohlsson; B Ohlsson; B Ohlsson; B Ohlsson; B Ohlsson; Bodil Ohlsson; CF Bernardes-Silva; CL Wu; D Louvel; D Xie; DP Xie; GF Longstreth; H-J Monstein; HJ Kim; J Borg; JH Bond; JM Park; Joyce Carlson; K Uvnäs-Moberg; K Uvnäs-Moberg; L Agreus; L Rinaman; LT Cavalli-Sforza; M Camilleri; M Feng; M Hashmonai; M Stefano Di; Magnus Simrén; MC Lomer; Mikael Truedsson; MK Koohi; N Cui; OU Petring; Q Yang; RD Leake; SR Anthoni; T Inoue; T Sahi; TK Nilsson; VV Rao

Polymorphism in the oxytocin promoter region in patients with lactase non-persistence is not related to symptoms

Authors: A Larcher
B Ohlsson
B Ohlsson
B Ohlsson
B Ohlsson
B Ohlsson
Bodil Ohlsson
CF Bernardes-Silva
CL Wu
D Louvel
D Xie
DP Xie
GF Longstreth
H-J Monstein
HJ Kim
J Borg
JH Bond
JM Park
Joyce Carlson
K Uvnäs-Moberg
K Uvnäs-Moberg
L Agreus
L Rinaman
LT Cavalli-Sforza
M Camilleri
M Feng
M Hashmonai
M Stefano Di
Magnus Simrén
MC Lomer
Mikael Truedsson
MK Koohi
N Cui
OU Petring
Q Yang
RD Leake
SR Anthoni
T Inoue
T Sahi
TK Nilsson
VV Rao
Publication date: 1 January 2009
Publisher: BioMed Central
Doi

Abstract

Abstract Background Oxytocin and the oxytocin receptor have been demonstrated in the gastrointestinal (GI) tract and have been shown to exert physiological effects on gut motility. The role for oxytocin in the pathophysiology of GI complaints is unknown. The aim of this study was to examine genetic variations or polymorphism of oxytocin (<it>OXT</it>) and its receptor (<it>OXTR</it>) genes in patients with GI complaints without visible organic abnormalities. Methods Genetic variants in the <it>OXT </it>promoter region, and in the <it>OXTR </it>gene in DNA samples from 131 rigorously evaluated patients with Irritable Bowel Syndrome (IBS), 408 homozygous subjects referred for lactase (LCT-13910 C>T, rs4988235) genotyping, and 299 asymptomatic blood donors were compared. One polymorphism related to the <it>OXT </it>gene (rs6133010 A>G) and 4 related to the <it>OXTR </it>gene (rs1465386 G>T, rs3806675 G>A, rs968389 A>G, rs1042778 G>T) were selected for genotyping using Applied Biosystems 7900 HT allele discrimination assays. Results There were no statistically significant differences in the genotype or allele frequencies in any of the SNPs when IBS patients were compared to healthy controls. Among subjects referred for lactase genotyping, the rs6133010 A>G <it>OXT </it>promoter A/G genotype tended to be more common in the 154 non-persistent (27.3%) subjects than in the 254 lactase persistant (18.1%) subjects and in the healthy controls (19.4%) (p = 0.08). When direct comparing, the A/G genotype was less common in the <it>OXT </it>promoter region in controls (p = 0.09) and in subjects with lactase persistence (p = 0.03) compared to subjects with lactase non-persistence. When healthy controls were viewed according to their own LCT-13910 genotypes, the C/C lactase non-persistent controls had a higher frequency for the <it>OXT </it>promoter A/G genotype than LCT-13910 T/T lactase persistent controls (41.2% vs 13.1%). No significant differences in frequencies of the investigated <it>OXTR </it>SNPs were noted in this study. Conclusion The results suggest that polymorphism in the promoter region of the <it>OXT </it>gene is most common in subjects with lactase non-persistence. This polymorphism may not be related to GI symptoms, as it is related to lactase non-persistence also in healthy controls.</p