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Peptide-based immunotherapy: a novel strategy for allergic disease.

机译:基于肽的免疫疗法:过敏性疾病的新策略。

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The T-cell component of the antigen-specific immune response is the target of various novel interventions to modify chronic immunologic disorders, such as allergic diseases. Recent clinical trials have evaluated the safety and efficacy of therapeutic vaccines consisting of short, synthetic, allergen-derived peptides, corresponding to T-cell epitopes from the eliciting antigen. The main advantage of such an approach is the reduction in systemic, immunoglobulin E-mediated adverse events compared with existing whole allergen immunotherapy, often referred to as 'allergy shots'. T-cell peptide epitopes, although capable of inducing immunologic tolerance, are short linear structures that have reduced ability to cross-link mast cell- and basophil-bound immunoglobulin E. The precise mechanism of tolerance induction remains incompletely defined. However, recent data indicate that peptide therapy induces/expands a population of antigen-specific regulatory T-cells. A novel form of treatment combining efficacy with a substantially decreased occurrence of adverse events is likely to have a major impact on the management and prevalence of allergic diseases. Furthermore, the principles of epitope-specific therapy hold promise for the development of therapeutic vaccines for the treatment of autoimmune diseases.
机译:抗原特异性免疫反应的T细胞成分是修饰慢性免疫系统疾病(例如变态反应性疾病)的各种新型干预措施的目标。最近的临床试验已经评估了由短的,合成的,变应原衍生的肽组成的治疗性疫苗的安全性和有效性,这些肽对应于来自引发抗原的T细胞表位。这种方法的主要优点是,与现有的全变应原免疫疗法(通常称为“过敏注射”)相比,减少了全身性免疫球蛋白E介导的不良事件。 T细胞肽表位虽然能够诱导免疫耐受,但是短的线性结构,具有降低与肥大细胞和嗜碱性粒细胞结合的免疫球蛋白E交联的能力。耐受诱导的精确机制仍未完全确定。但是,最近的数据表明,肽疗法可诱导/扩增抗原特异性调节性T细胞。结合疗效和不良事件的发生率大大降低的新型治疗方法可能会对过敏性疾病的控制和患病率产生重大影响。此外,表位特异性疗法的原理为开发用于治疗自身免疫性疾病的治疗性疫苗具有希望。

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