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具有治疗 2 型糖尿病潜力的两栖动物宿主防御肽 - 最新综述。

Amphibian host-defense peptides with potential for Type 2 diabetes therapy - an updated review.

机构信息

Diabetes Research Centre, School of Biomedical Sciences, Ulster University, Coleraine, Northern Ireland BT52 1SA, UK.

Diabetes Research Centre, School of Biomedical Sciences, Ulster University, Coleraine, Northern Ireland BT52 1SA, UK.

出版信息

Peptides. 2024 May;175:171180. doi: 10.1016/j.peptides.2024.171180. Epub 2024 Feb 22.

DOI:10.1016/j.peptides.2024.171180
PMID:38401671
Abstract

Investigations conducted since 2018 have identified several host-defense peptides present in frog skin secretions whose properties suggest the possibility of their development into a new class of agent for Type 2 diabetes (T2D) therapy. Studies in vitro have described peptides that (a) stimulate insulin release from BRIN-BD11 clonal β-cells and isolated mouse islets, (b) display β-cell proliferative activity and protect against cytokine-mediated apoptosis and (c) stimulate production of the anti-inflammatory cytokine IL-10 and inhibit production of the pro-inflammatory cytokines TNF-α and IL-1β. Rhinophrynin-27, phylloseptin-3.2TR and temporin F are peptides with therapeutic potential. Studies in vivo carried out in db/db and high fat-fed mice have shown that twice-daily administration of [S4K]CPF-AM1 and [A14K]PGLa-AM1, analogs of peptides first isolated from the octoploid frog Xenopus amieti, over 28 days lowers circulating glucose and HbA1c concentrations, increases insulin sensitivity and improves glucose tolerance and lipid profile. Peptide treatment produced potentially beneficial changes in the expression of skeletal muscle genes involved in insulin signaling and islet genes involved in insulin secretion in these murine models of T2D. Lead compounds uncovered by the study of frog HDPs may provide a basis for the design of new types of agents that can be used, alone or in combination with existing therapies, for the treatment of T2D.

摘要

自 2018 年以来开展的研究已经确定了几种存在于青蛙皮肤分泌物中的宿主防御肽,其特性表明它们有可能开发成 2 型糖尿病 (T2D) 治疗的新型药物。体外研究描述了具有以下特性的肽:(a) 刺激 BRIN-BD11 克隆β细胞和分离的小鼠胰岛释放胰岛素,(b) 显示β细胞增殖活性,并防止细胞因子介导的细胞凋亡,(c) 刺激抗炎细胞因子 IL-10 的产生并抑制促炎细胞因子 TNF-α和 IL-1β的产生。 Rhinophrynin-27、phylloseptin-3.2TR 和 temporin F 是具有治疗潜力的肽。在 db/db 和高脂肪喂养的小鼠中进行的体内研究表明,每天两次给予 [S4K]CPF-AM1 和 [A14K]PGLa-AM1,这两种肽是从八倍体青蛙 Xenopus amieti 中首次分离出的肽的类似物,连续 28 天可降低循环葡萄糖和 HbA1c 浓度,增加胰岛素敏感性,改善葡萄糖耐量和脂质谱。在这些 T2D 小鼠模型中,肽治疗导致与胰岛素信号转导相关的骨骼肌基因和与胰岛素分泌相关的胰岛基因的表达发生了潜在的有益变化。通过研究青蛙 HDP 发现的先导化合物可能为设计新型药物提供基础,这些药物可单独或与现有疗法联合用于治疗 T2D。

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