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首页> 外文期刊>Expert Review of Molecular Diagnostics >Molecular mechanisms of the adaptive, innate and regulatory immune responses in the intestinal mucosa of celiac disease patients.
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Molecular mechanisms of the adaptive, innate and regulatory immune responses in the intestinal mucosa of celiac disease patients.

机译:腹腔疾病患者肠道黏膜适应性,先天性和调节性免疫反应的分子机制。

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摘要

Celiac disease is a complex genetic disorder that affects the small intestine of genetically predisposed individuals when they ingest gluten, a dietary protein. Although several genome screens have been successful in identifying susceptibility loci in celiac disease, the only genetic contributors identified so far are the human leukocyte antigen (HLA)-DQ2/DQ8 molecules. One of the most important aspects in the pathogenesis of celiac disease is the activation of a T-helper 1 immune response, when the antigen-presenting cells that express HLA-DQ2/DQ8 molecules present the toxic gluten peptides to reactive CD4(+) T-cells. Recently, new insights into the activation of an innate immune response have also been described. It is generally accepted that the immune response triggers destruction of the mucosa in the small intestine of celiac disease patients. Hence, the activation of a detrimental immune response in the intestine of celiac disease patients appears to be key in the initiation and progression of the disease. This review summarizes the immunologic pathways that have been studied in celiac disease thus far, and will point to new potential candidate genes and pathways involved in the etiopathogenesis of celiac disease, which should lead to novel alternatives for diagnosis and treatment.
机译:乳糜泻是一种复杂的遗传疾病,当食用具有蛋白质的麸质时,会影响遗传易感者的小肠。尽管已经成功进行了几项基因组筛选,以鉴定出乳糜泻的易感基因座,但到目前为止,唯一鉴定出的遗传因素是人白细胞抗原(HLA)-DQ2 / DQ8分子。腹腔疾病发病机理中最重要的方面之一是激活T-helper 1免疫反应,当表达HLA-DQ2 / DQ8分子的抗原呈递细胞向反应性CD4(+)T呈毒性面筋肽时-细胞。最近,还描述了对先天免疫应答激活的新见解。通常认为,免疫反应触发了乳糜泻患者小肠粘膜的破坏。因此,在腹腔疾病患者的肠中有害的免疫应答的激活似乎是疾病起始和进展的关键。这篇综述总结了迄今为止在乳糜泻中已研究的免疫途径,并指出了与乳糜泻的发病机制有关的新的潜在候选基因和途径,这将为诊断和治疗带来新的选择。

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