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首页> 外文期刊>Journal of Clinical Microbiology >Molecular Characterization of Campylobacter jejunifrom Patients with Guillain-Barré and Miller Fisher Syndromes
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Molecular Characterization of Campylobacter jejunifrom Patients with Guillain-Barré and Miller Fisher Syndromes

机译:格林-巴雷和米勒·费雪综合征患者空肠弯曲菌的分子特征

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摘要

Campylobacter jejuni has been identified as the predominant cause of antecedent infection in Guillain-Barrésyndrome (GBS) and Miller Fisher syndrome (MFS). The risk of developing GBS or MFS may be higher after infection with specific C. jejuni types. To investigate the putative clonality, 18 GBS- or MFS-related C. jejuni strains from The Netherlands and Belgium and 17 control strains were analyzed by serotyping (Penner and Lior), restriction fragment length polymorphism analysis of PCR products of the flaA gene, amplified fragment length polymorphism analysis, pulsed-field gel electrophoresis, and randomly amplified polymorphic DNA analysis. Serotyping revealed 10 different O serotypes and 7 different Lior serotypes, thereby indicating a lack of serotype clustering. Two new O serotypes, O:35 and O:13/65, not previously associated with GBS or MFS were found. Serotype O:19 was encountered in 2 of 18 strains, and none was of serotype O:41. The results of all genotypic methods also demonstrated substantial heterogeneity. No clustering of GBS- or MFS-related strains occurred and no molecular marker capable of separating pathogenic GBS or MFS from non-GBS- or non-MFS-related enteritis strains could be identified in this study. Sialic-acid-containing lipopolysaccharides (LPS) are thought to be involved in the triggering of GBS or MFS through molecular mimicry with gangliosides in human peripheral nerves. Therefore, further characterization of GBS- or MFS-related C. jejuni should target the genes involved in the synthesis of LPS and the incorporation of sialic acid.
机译:空肠弯曲杆菌已被确认为格林-巴利综合征(GBS)和米勒·费舍综合症(MFS)的前期感染的主要原因。感染特定的 C后,发生GBS或MFS的风险可能更高。空肠类型。为了调查推定的克隆性,使用18 GBS或MFS相关的 C。通过血清分型(Penner和Lior), flaA 基因PCR产物的限制性片段长度多态性分析,扩增的片段长度多态性分析,分析了荷兰和比利时的空肠菌株和17个对照菌株,脉冲场凝胶电泳和随机扩增多态性DNA分析。血清分型显示出10种不同的O血清型和7种不同的Lior血清型,从而表明缺乏血清型聚类。发现了两个以前未与GBS或MFS关联的新O型血清型:O:35和O:13/65。在18个菌株中有2个遇到O:19血清型,而O:41血清型均没有。所有基因型方法的结果也显示出实质性的异质性。在这项研究中,没有发生与GBS或MFS相关的菌株的聚类,也没有能够分离出与非GBS或非MFS相关的肠炎菌株的致病性GBS或MFS的分子标记。含唾液酸的脂多糖(LPS)被认为是通过分子模拟神经节苷脂在人周围神经中引发GBS或MFS的。因此,进一步表征了与GBS或MFS相关的 C。空肠应该靶向参与LPS合成和唾液酸掺入的基因。

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