首页> 外文期刊>Microbial Pathogenesis >Decreased circulating interleukin-33 concentration in Helicobacter pylori-infected patients with peptic ulcer: Evaluation of its association with a Pheck for cytokine gene polymorphism, gender of patients and bacterial virulence factor CagA
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Decreased circulating interleukin-33 concentration in Helicobacter pylori-infected patients with peptic ulcer: Evaluation of its association with a Pheck for cytokine gene polymorphism, gender of patients and bacterial virulence factor CagA

机译:在幽门螺杆菌感染患者中循环白细胞介素-33浓度降低:与细胞因子基因多态性,患者性别和细菌毒力因子Caga评估其与pheck的关系

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IL-33 has powerful immunoregulatory activities such as reinforcement of Th2 cell responses. The aim was to assess the circulating IL-33 levels and IL-33 rs1929992 polymorphism in H. pylori-infected peptic ulcer (PU) patients and asymptomatic (AS) subjects. Blood samples were obtained from 100 PU patients, 100 AS subjects and 100 uninfected individuals. Circulating IL-33 levels were detected by ELISA. After DNA extraction, the IL-33 rs1929992 polymorphism was determined using PCR-RFLP method. Serum IL-33 quantities were significantly lower in PU patients compared with AS and uninfected groups. IL-33 levels were higher in AS subjects compared with uninfected group. In PU, AS and uninfected groups, IL-33 levels were significantly higher in women than men. In PU and AS groups, the CagA(+) H. pylori-infected subjects exhibit higher IL-33 levels compared with carriers of CagA(+) H. pylori strains. In PU patients, the frequency of genotype GG and allele G at IL-33 rs1929992 was significantly higher compared with all healthy subjects (AS(+) uninfected groups). The presence of genotypes GG and AG, and allele G in rs1929992 conferred greater risk for PU. In whole H. pylori-infected population (PU + AS groups), IL-33 levels in individuals with genotype AA or allele A at rs1929992 were higher than subjects with GG genotype or allele G. The reduced IL-33 production could contribute to the PU development during H. pylori infection. The IL-33 levels may be affected by individual gender, rs1929992 polymorphism, and the CagA status of bacteria. The rs1929992-related GG genotype and G allele may be associated with PU development.
机译:IL-33具有强大的免疫调节活动,如加固Th2细胞应答。目的是评估幽门螺杆菌感染的消化溃疡(PU)患者的循环IL-33水平和IL-33 RS1929992多态性和无症状的受试者。从100名PU患者,100岁的受试者和100个未感染的个体获得血样。 ELISA检测循环IL-33水平。在DNA提取后,使用PCR-RFLP方法测定IL-33 RS1929992多态性。 PU患者的血清IL-33量显着降低,与和未感染的群体相比。与未感染的群体相比,IL-33水平较高。在PU,作为未感染的群体,女性的IL-33水平比男性显着高。在PU和作为群体中,与Caga(+)H.幽门螺杆菌菌株的载体相比,Caga(+)H. pylori感染的受试者表现出更高的IL-33水平。在PU患者中,与所有健康受试者相比,IL-33 rs1929992的基因型GG和等位基因G的频率显着高于(AS(+)未感染的组)。基因型Gg和Ag的存在,以及Rs1929992中的等位基因G赋予PU的风险更大。在整个H.幽门螺杆菌群体(Pu +作为群体)中,在GG基因型或等位基因G的基因型AA或等位基因A中的个体中的IL-33水平高于GG基因型或等位基因G.降低的IL-33生产可能有助于H.幽门螺杆菌感染过程中的PU开发。 IL-33水平可能受到个体性别,Rs1929992多态性的影响和细菌的CAGA状态。 RS1929992相关的GG基因型和G等位基因可能与PU开发相关联。

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