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Second-generation peptidomimetic inhibitors of antigen presentation effectively treat autoimmune diseases in HLA-DR-transgenic mouse models

机译:抗原呈递的第二代拟肽抑制剂可有效治疗HLA-DR转基因小鼠模型中的自身免疫性疾病

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摘要

Peptidomimetic compounds that bind to major histocompatibility complex class II molecules and are resistant to cathepsins can competitively inhibit the presentation of processed protein antigens. Therefore, compounds that bind to autoimmune disease-associated class II molecules are expected to compete with autoantigens for presentation and thereby interrupt the disease process. The first generation of such competitors developed for rheumatoid arthritis-associated HLA-DR molecules, although resistant to cathepsins, has remained sensitive to plasma proteases, and was thus unlikely to be effective in vivo. We have therefore produced a second generation of compounds that is resistant to cathepsins and stable in plasma while maintaining binding affinity for HLA-DR molecules associated with rheumatoid arthritis and multiple sclerosis. Selected compounds of this series are shown to inhibit antigen presentation in vivo, as well as effectively treat collagen induced arthritis and experimental autoimmune encephalomyelitis in HLA-DR transgenic mouse models.
机译:与主要的组织相容性复杂的II类分子结合并对组织蛋白酶具有抗性的拟肽化合物可以竞争性地抑制加工的蛋白质抗原的呈递。因此,与自身免疫疾病相关的II类分子结合的化合物有望与自身抗原竞争呈递,从而中断疾病进程。为类风湿性关节炎相关的HLA-DR分子开发的第一代此类竞争者尽管对组织蛋白酶具有抗性,但对血浆蛋白酶仍然敏感,因此不太可能在体内有效。因此,我们生产了第二代对组织蛋白酶具有抗性并且在血浆中稳定,同时又保持与类风湿性关节炎和多发性硬化症相关的HLA-DR分子的结合亲和力的化合物。在HLA-DR转基因小鼠模型中,该系列的选定化合物显示可抑制体内抗原呈递,并有效治疗胶原蛋白诱导的关节炎和实验性自身免疫性脑脊髓炎。

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