García-González María Asunción, Lanas Angel, Quintero Enrique, Nicolás David, Parra-Blanco Adolfo, Strunk Mark, Benito Rafael, Angel Simón Miguel, Santolaria Santos, Sopeña Federico, Piazuelo Elena, Jiménez Pilar, Pascual Cristina, Mas Eva, Irún Pilar, Espinel Jesús, Campo Rafael, Manzano Marisa, Geijo Fernando, Pellisé Maria, González-Huix Ferrán, Nieto Miguel, Espinós Jorge, Titó Llúcia, Bujanda Luis, Zaballa Manuel
Instituto Aragonés de Ciencias de la Salud, Zaragoza, Spain.
Am J Gastroenterol. 2007 Sep;102(9):1878-92. doi: 10.1111/j.1572-0241.2007.01423.x. Epub 2007 Jul 19.
Recent studies have reported an association between cytokine gene polymorphisms and GC risk. However, results are inconsistent among studies from different geographic regions and ethnic groups. Our goal was to evaluate the influence of Helicobacter pylori (H. pylori) infection and host genetic factors on GC susceptibility in a population of Spanish white GC patients.
DNA from 404 unrelated patients with GC and 404 sex- and age-matched healthy controls was typed for several functional polymorphisms in pro- (IL-1B, TNFA, LTA, IL-12p40) and anti-inflammatory (IL-4, IL-1RN, IL-10, TGFB1) genes by PCR, RFLP, and TaqMan assays. H. pylori infection and CagA/VacA antibody status were also determined by western blot serology.
Logistic regression analysis identified H. pylori infection with cagA strains (OR 2.54, 95% CI 1.77-3.66), smoking habit (OR 1.91, 95% CI 1.25-2.93), and positive family history of GC (OR 3.67, 95% CI 2.01-6.71) as independent risk factors for GC. None of the cytokine gene polymorphisms analyzed in this study were associated with susceptibility to GC development, whether GC patients were analyzed as a group or categorized according to anatomic location or histological subtype. Some simultaneous combinations of proinflammatory genotypes reportedly associated with greater GC risk yielded no significant differences between patients and controls.
Our results show that, at least in some white populations, the contribution of the cytokine gene polymorphisms evaluated in this study (IL-1B, IL-1RN, IL-12p40, LTA, IL-10, IL-4, and TGF-B1) to GC susceptibility may be less relevant than previously reported.
近期研究报道了细胞因子基因多态性与胃癌(GC)风险之间的关联。然而,来自不同地理区域和种族群体的研究结果并不一致。我们的目标是评估幽门螺杆菌(H. pylori)感染和宿主遗传因素对西班牙白人GC患者群体中GC易感性的影响。
通过聚合酶链反应(PCR)、限制性片段长度多态性分析(RFLP)和TaqMan分析,对404例无亲缘关系的GC患者及404例性别和年龄匹配的健康对照的DNA进行促炎(IL-1B、TNFA、LTA、IL-12p40)和抗炎(IL-4、IL-1RN、IL-10、TGFB1)基因的几种功能多态性分型。还通过蛋白质印迹血清学检测H. pylori感染及CagA/VacA抗体状态。
逻辑回归分析确定,携带cagA菌株的H. pylori感染(比值比[OR] 2.54,95%置信区间[CI] 1.77 - 3.66)、吸烟习惯(OR 1.91,95% CI 1.25 - 2.93)以及GC家族史阳性(OR 3.67,95% CI 2.01 - 6.71)为GC的独立危险因素。本研究中分析的细胞因子基因多态性均与GC发生易感性无关,无论将GC患者作为一个整体分析,还是根据解剖位置或组织学亚型分类分析。一些据报道与更高GC风险相关的促炎基因型的同时组合,在患者和对照之间未产生显著差异。
我们的结果表明,至少在某些白人人群中,本研究评估的细胞因子基因多态性(IL-1B、IL-1RN、IL-12p40、LTA、IL-10、IL-4和TGF - B1)对GC易感性的影响可能比先前报道的要小。
