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Mechanisms of immunotherapy.

机译:免疫疗法的机制。

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Specific allergen injection immunotherapy is highly effective in IgE-mediated diseases, such as allergic rhinitis and venom anaphylaxis. Immunotherapy inhibits both early and late responses to allergen exposure. Immunotherapy is accompanied by increases in allergen-specific IgG, particularly the IgG4 isotype, which blocks not only IgE-dependent histamine release from basophils but also IgE-mediated antigen presentation to T cells. Immunotherapy acts on T cells to modify peripheral and mucosal T(H)2 responses to allergen in favor of T(H)1 responses. Recent studies have identified increased IL-10 production in peripheral blood and mucosal surfaces after immunotherapy. IL-10 has numerous potential antiallergic properties, including suppression of mast cell, eosinophil, and T-cell responses, as well as acting on B cells to favor heavy chain class switching to IgG4. These IL-10-producing cells might be so-called regulatory T cells and appear to be identified by the CD4(+)CD25(+) phenotype. Studies in mice suggest that dendritic cells play a vital role in induction of regulatory T cells. Novel approaches to immunotherapy currently being explored include the use of adjuvants, such as monophosphoryl lipid A or nucleotide immunostimulatory sequences derived from bacteria that potentiate T(H)1 responses. Alternative strategies include the use of allergen-derived peptides or modified recombinant allergen vaccines that act on T cells while minimizing the IgE-dependent mast cell activation that is dependent on the native allergen conformation.
机译:特异性变应原注射免疫疗法在IgE介导的疾病(例如变应性鼻炎和毒液过敏)中非常有效。免疫疗法抑制对过敏原暴露的早期和晚期反应。免疫疗法伴随着变应原特异性IgG的增加,尤其是IgG4同种型的增加,它不仅阻断了嗜碱性粒细胞的IgE依赖性组胺释放,而且阻止了IgE介导的抗原呈递给T细胞。免疫疗法作用于T细胞,以改变外周和粘膜对过敏原的T(H)2反应,从而有利于T(H)1反应。最近的研究已经确定免疫疗法后外周血和粘膜表面IL-10产生增加。 IL-10具有许多潜在的抗过敏特性,包括抑制肥大细胞,嗜酸性粒细胞和T细胞反应,以及作用于B细胞以促进重链类别转换为IgG4。这些产生IL-10的细胞可能是所谓的调节性T细胞,似乎由CD4(+)CD25(+)表型鉴定。小鼠研究表明,树突状细胞在诱导调节性T细胞方面起着至关重要的作用。目前正在探索的新型免疫疗法方法包括使用佐剂,例如单磷酰脂质A或衍生自能够增强T(H)1反应的细菌的核苷酸免疫刺激序列。替代策略包括使用对T细胞起作用的变应原衍生肽或修饰的重组变应原疫苗,同时使依赖于天然变应原构象的IgE依赖性肥大细胞活化减至最小。

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