基于恶唑和咪唑的Ser-Leu二肽模拟物对MHC II类DR分子抗原呈递的有效抑制作用。

Drug design and discovery Pub Date : 2002-01-01
Ramakanth Sarabu, David R Bolin, Robert Campbell, Joel R Cooper, Donald Cox, Diana Gaizband, Raymond Makofske, Zoltan Nagy, Gary L Olson
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引用次数: 0

摘要

设计并制备了咪唑和恶唑衍生物1至4作为二肽模拟物,以取代Ro-25-9980 (Ac-(Cha)- rama - s - l - nh2)的Ser-Leu二肽序列,Ro-25-9980 (Ac-(Cha)- rama - s - l - nh2)是与类风湿关节炎(RA)相关的主要组织相容性复合体(MHC) II类DR分子结合的肽抑制剂。结合实验中最有效的类似物(IC50 = 30 nM)在DRB1*0401结合;16、Ac-(Cha)RAMA-(S)S-psi(恶唑)- l - nh2的效力是Ro 25-9980的1.6倍。讨论了由二肽模拟物1 ~ 4合成的多肽杂交种10 ~ 24的合成孔径(SAR)。在这些杂交种中,含有咪唑和恶唑模拟物的23和24,以及位置3至5的优化变体,在DRB1 1*0401结合中具有70至80 nM的结合亲和力,并且在DRB1*0101结合中也具有活性,同时抵抗组织蛋白酶b的蛋白水解。这表明它们有抑制自身免疫反应的潜力,并可作为治疗类风湿性关节炎的药物的线索。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Oxazole- and imidazole-based Ser-Leu dipeptide mimetics in potent inhibitors of antigen presentation by MHC class II DR molecules.

Imidazole and oxazole derivatives 1 to 4 were designed and prepared as dipeptide mimetics to replace the Ser-Leu dipeptide sequence of Ro-25-9980 (Ac-(Cha)-RAMA-S-L-NH2), a peptidic inhibitor of antigen binding to major histocompatibility complex (MHC) class II DR molecules linked to rheumatoid arthritis (RA). The most potent analog in binding assays (IC50 = 30 nM in DRB1*0401 binding; 1.6 times as potent as Ro 25-9980) was 16, Ac-(Cha)RAMA-(S)S-psi(oxazole)-L-NH2. The SAR of peptide hybrids 10 to 24, prepared by incorporating the dipeptide mimetics 1 to 4 is discussed. Of these hybrids, 23 and 24, analogs that incorporated the imidazole and oxazole mimetics as well as optimized variants at positions 3 to 5, were found to have 70 to 80 nM binding affinity comparable to the parent peptide in DRB 1*0401 binding and were also active in DRB1*0101 binding, while being resistant to proteolysis by cathepsin B. Both of these compounds showed inhibitory activity in an antigen-stimulated T-cell proliferation assay, indicating their potential to suppress autoimmune responses and as leads for therapeutic agents to treat RA.

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