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The gut immune system, inflammatory bowel diseases, and the body immune homeostasis: modern treatment strategies

机译:肠道免疫系统,炎症性肠病和机体免疫稳态:现代治疗策略

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The digestive tract is nowadays conceived as a barrier organ constituted by a mucosal membrane separating the gut lumen from the inner milieu. The gut lumen is laden by a myriad of antigens brought about by the diet, but also pertaining to the overwhelming bacterial species of the gut microbiome. The mucosal cell population comprehends epithelial cells, and a variety of immune reactive cells. Of them, the mononuclear types effecting innate responses are endowed by membrane signaling receptors and, as a rule, are sensing the polysaccharides of bacterial cell walls; non-tolerated signals may then push the chain reaction on, to end in full activation of inflammation mediators. Acquired immunity is in turn mainly effected by T-cell types, some of them, behaving as autoreactive cells, may induce metastatic inflammation beyond bowel boundaries, partly explaining the so-called extra-intestinal manifestations of inflammatory bowel disease (IBD). The scenario is further complicated by the possible influence of epigenetic factors: diet, stress, smoking, drugs. Being IBD a low-penetrance disorder, for the full phenotype to develop, a critical mass of the above listed factors (typically, a disturbed membrane permeability, an immune stimulus, and an epigenetic factor) must occur. In the century since the full description of IBD, a variegated plethora of measures have been attempted. Some updated designs are now under scrutiny. Microbiota engineering, apoptosis modulation, and diet modification are just a few of the measures that we are arbitrarily describing here.
机译:如今,消化道被认为是由将肠腔与内部环境隔开的粘膜构成的屏障器官。饮食给肠道内的抗原带来无数种抗原,但也与肠道微生物组中绝大多数细菌有关。粘膜细胞群包括上皮细胞和各种免疫反应性细胞。其中,影响先天反应的单核类型是由膜信号受体所赋予的,通常是感知细菌细胞壁的多糖。然后,非耐受信号可能会推动链反应,从而最终激活炎症介质。获得性免疫反过来主要受T细胞类型的影响,其中一些表现为自身反应性细胞,可能会诱发肠外转移性炎症,部分解释了炎症性肠病(IBD)的所谓肠外表现。表观遗传因素的可能影响使情况变得更加复杂:饮食,压力,吸烟,药物。作为IBD的一种低渗透性疾病,要发展出完整的表型,就必须产生上述因素的临界质量(通常是膜通透性受损,免疫刺激和表观遗传因素)。自从对IBD进行全面描述以来的一个世纪,人们已经尝试了多种多样的措施。现在正在审查一些更新的设计。微生物群工程,细胞凋亡调节和饮食调节只是我们在此处任意描述的一些措施。

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