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一种 Co(III) 配合物在 h-IAPP 的聚合体存在的情况下切割 h-IAPP 的可溶性低聚物。

A Co(III) complex cleaving soluble oligomers of h-IAPP in the presence of polymeric aggregates of h-IAPP.

机构信息

Department of Chemistry, Seoul National University, Seoul 151-742, Republic of Korea.

出版信息

Bioorg Med Chem Lett. 2012 Sep 1;22(17):5689-93. doi: 10.1016/j.bmcl.2012.06.089. Epub 2012 Jul 3.

Abstract

Soluble oligomers of human islet amyloid polypeptide (h-IAPP) are believed to be the pathogenic species for type 2 diabetes mellitus. In search of the peptide-cleavage agent cleaving oligomers of h-IAPP with low affinity for polymeric aggregates of h-IAPP, a chemical library was constructed by using the Ugi condensation. From the library, a Co(III) complex was discovered to cleave soluble oligomers of h-IAPP in the presence of polymeric aggregates of h-IAPP without being captured by the aggregates considerably. The peptide-cleavage agent inhibited apoptosis of INS-1 cell by h-IAPP even in the presence of preformed polymeric aggregates of h-IAPP. This suggests that target-selective peptide-cleavage agents may be applied clinically not only to diabetes but also to various other amyloid diseases.

摘要

可溶性人胰岛淀粉样多肽(h-IAPP)寡聚物被认为是 2 型糖尿病的致病物质。为了寻找对 h-IAPP 聚合物聚集体具有低亲和力的肽裂解剂来裂解 h-IAPP 的寡聚物,使用 Ugi 缩合反应构建了一个化学文库。从该文库中发现了一种 Co(III) 配合物,它可以在 h-IAPP 聚合物聚集体存在的情况下裂解可溶性 h-IAPP 寡聚物,而不会被聚集体大量捕获。即使在存在 h-IAPP 聚合物聚集体的情况下,该肽裂解剂也能抑制 h-IAPP 诱导的 INS-1 细胞凋亡。这表明,选择性的肽裂解剂不仅可以应用于糖尿病,还可以应用于各种其他淀粉样疾病的临床治疗。

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