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首页> 外文期刊>Journal of Clinical Microbiology >CagA and VacA Polymorphisms Do Not Correlate with Severity of Histopathological Lesions in Helicobacter pylori-Infected Greek Children
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CagA and VacA Polymorphisms Do Not Correlate with Severity of Histopathological Lesions in Helicobacter pylori-Infected Greek Children

机译:CagA和VacA多态性与幽门螺杆菌感染的希腊儿童的组织病理学病变的严重程度不相关。

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摘要

The presence of various numbers of EPIYA tyrosine phosphorylation motifs in the CagA protein of Helicobacter pylori has been suggested to contribute to pathogenesis in adults. In this prospective study, we characterized H. pylori isolates from symptomatic children, with reference to the diversity of functional EPIYA motifs in the CagA protein and vacA isotypes, and assessed the potential correlation with the histopathological manifestations of the infection. We analyzed 105 H. pylori isolates from 98 children and determined the diversity of EPIYA motifs in CagA by amplification and sequencing of the 3′ variable region of the cagA gene as well as vacA isotypes for the signal, middle, and intermediate regions. CagA phosphorylation and levels of secreted IL-8 were determined following in vitro infection of AGS gastric epithelial cells. Histopathological evaluation of H. pylori colonization, activity, and severity of the associated gastritis was performed according to the updated Sydney criteria. EPIYA A (GLKN[ST]EPIYAKVNKKK), EPIYA B (Q[V/A]ASPEPIY[A/T]QVAKKVNAKI), and EPIYA C (RS[V/A]SPEPIYATIDDLG) motifs were detected in the ABC (46.6%) and ABCC (17.1%) combinations. No isolates harboring more than two EPIYA C motifs in CagA were found. The presence of isogenic strains with variable numbers of CagA EPIYA C motifs within the same patient was detected in seven cases. Occurrence of increasing numbers of EPIYA C motifs correlated strongly with presence of a high-vacuolation (s1 or s2/i1/m1) phenotype and age. A weak positive correlation was observed between vacuolating vacA genotypes and presence of nodular gastritis. However, CagA- and VacA-dependent pathogenicities were not found to contribute to severity of histopathology manifestations in H. pylori-infected children.
机译:幽门螺杆菌的CagA蛋白中存在大量的EPYYA酪氨酸磷酸化基序,已被认为有助于成人的发病。在这项前瞻性研究中,我们表征了 H。从有症状的儿童中分离出幽门螺杆菌,并参考CagA蛋白和 vacA 同种型的功能性EPIYA基序的多样性,并评估其与感染的组织病理学表现的潜在相关性。我们分析了105H。通过对 cagA 基因的3'可变区和 vacA 的3'可变区进行扩增和测序,确定了98例儿童的幽门螺杆菌分离株,并确定了CagA中EPYYA的多样性。信号,中间和中间区域的同种型。在体外感染AGS胃上皮细胞后,测定CagA的磷酸化和分泌的IL-8水平。 H的组织病理学评估。根据最新的悉尼标准进行幽门螺杆菌的定植,活动和相关胃炎的严重程度。在ABC中检出了EPIYA A(GLKN [ST] EPIYAKVNKKK),EPIYA B(Q [V / A] ASPEPIY [A / T] QVAKKVNAKI)和EPIYA C(RS [V / A] SPEPIYATIDDLGLG)图案(46.6%)和ABCC(17.1%)组合。在CagA中未发现带有两个以上EPIYA C主​​题的分离株。在七名患者中,同一名患者中检测到了具有可变数量的CagA EPIYA C基序的同基因菌株。 EPIYA C基序数目的增加与高真空化(s1或s2 / i1 / m1)表型和年龄的存在密切相关。空泡 vacA 基因型与结节性胃炎的存在之间存在弱的正相关。但是,未发现CagA和VacA依赖的致病性导致 H的组织病理学表现的严重性。幽门螺杆菌感染的儿童

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