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Association between Virulence Factors and TRAF1/4-1BB/Bcl-xL Expression in Gastric Mucosa Infected with Helicobacter pylori

机译:毒力因子与胃粘膜胃粘膜中胃粘膜中的毒力因子和TRAF1 / 4-1BB / BCL-XL表达的关联

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摘要

Objective. CagA+/vacAs1+/vacAm1+ Helicobacter pylori upregulates the expression of tumor necrosis factor receptor-associated factor 1 (TRAF1), tumor necrosis factor receptor superfamily member 9 (4-1BB), and B-cell lymphoma-extra large (Bcl-xL) in human gastric epithelial cells. We investigated the correlation between cagA/vacAs1/vacAm1 and TRAF1/4-1BB/Bcl-xL expression in gastric mucosal tissue of patients with gastric disorders. Methods. We collected gastric mucosa samples from 35 chronic, nonatrophic gastritis (CG) patients, 41 atrophic gastritis patients, 44 intestinal metaplasia with atypical hyperplasia (IM) patients, and 28 gastric carcinoma (Ca) patients. The expression of TRAF1, 4-1BB, and Bcl-xL was determined using western blotting. The expression of cagA, vacAs1, and vacAm1 in H. pylori was examined with polymerase chain reaction. Results. The expression of TRAF1, 4-1BB, and Bcl-xL was significantly upregulated in IM and Ca patients (P 0.05 compared with CG). There were more cases of cagA+/vacAs1+/vacAm1+ H. pylori infection in samples with elevated TRAF1, 4-1BB, or Bcl-xL expression (P 0.05). Additionally, there were a remarkably large number of samples with upregulated TRAF1/4-1BB/Bcl-xL expression in cases of cagA+/vacAs1+/vacAm1+ H. pylori infection (44 cases, 67.7%; P 0.05). Conclusions. The pathogenesis of IM and Ca may be promoted by cagA+/vacAs1+/vacAm1+ H. pylori, possibly via upregulated TRAF1, 4-1BB, and Bcl-xL in gastric mucosal tissue.
机译:客观的。 Caga + / Vacas1 + / vacam1 +幽门螺杆菌幽门螺杆菌上调肿瘤坏死因子受体相关因子1(Traf1),肿瘤坏死因子受体超家族成员9(4-1bb)和B细胞淋巴瘤 - 超大(Bcl-xl)的表达人胃上皮细胞。我们研究了Caga / Vacas1 / vacam1和TRAF1 / 4-1BB / BCL-XL在胃粘膜组织中的表达与胃疾病的胃粘膜组织之间的相关性。方法。我们收集了35例慢性,非营养性胃炎(CG)患者的胃粘膜样品,41例萎缩性胃炎患者,44例肠道细胞,非典型增生(IM)患者,28例胃癌(CA)患者。使用蛋白质印迹测定Traf1,4-1Bb和Bcl-XL的表达。用聚合酶链反应检查Caga,Vacas1和H.Pylori中的vacam1的表达。结果。在IM和CA患者中显着上调TRAF1,4-1BB和BCL-XL的表达(P <0.05与CG相比)。在具有升高的TRAF1,4-1BB或BCL-XL表达(P <0.05)的样品中,在样品中有更多的CAGA + / VACA1 + / VAC.幽门螺杆菌感染。另外,在Caga + / Vacas1 + / Vacam1 + H.幽门螺杆菌感染情况下,存在具有上调的TRAF1 / 4-1BB / BCL-XL表达的显着大量样品。幽门螺杆菌感染(44例,67.7%; P <0.05)。结论。可通过CAGA + / VACA1 / v + H.幽门螺杆菌促进IM和Ca的发病机制,可能通过胃粘膜组织中的上调的TRAF1,4-1BB和BCL-XL促进幽门螺杆菌。

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    Cent S Univ Dept Gastroenterol Xiangya Hosp 3 Changsha 410013 Hunan Peoples R China;

    Cent S Univ Xiangya Sch Med Dept Parasitol Changsha 410013 Hunan Peoples R China;

    Cent S Univ Dept Gastroenterol Xiangya Hosp 3 Changsha 410013 Hunan Peoples R China;

    Cent S Univ Dept Gastroenterol Xiangya Hosp 3 Changsha 410013 Hunan Peoples R China;

    Cent S Univ Dept Gastroenterol Xiangya Hosp 3 Changsha 410013 Hunan Peoples R China;

    Cent S Univ Dept Gastroenterol Xiangya Hosp 3 Changsha 410013 Hunan Peoples R China;

    Cent S Univ Dept Gastroenterol Xiangya Hosp 3 Changsha 410013 Hunan Peoples R China;

    Cent S Univ Dept Gastroenterol Xiangya Hosp 3 Changsha 410013 Hunan Peoples R China;

    Cent S Univ Dept Gastroenterol Xiangya Hosp 3 Changsha 410013 Hunan Peoples R China;

    Cent S Univ Dept Neurol Xiangya Hosp 3 Changsha 410013 Hunan Peoples R China;

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  • 正文语种 eng
  • 中图分类 消化系及腹部疾病;
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