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肽学:细胞生物学和免疫学中的短氨基酸模块

Peptidology: short amino acid modules in cell biology and immunology.

作者信息

Lucchese G, Stufano A, Trost B, Kusalik A, Kanduc D

机构信息

Department of Biochemistry and Molecular Biology "Ernesto Quagliariello", University of Bari, Bari, Italy.

出版信息

Amino Acids. 2007 Nov;33(4):703-7. doi: 10.1007/s00726-006-0458-z. Epub 2006 Nov 2.

Abstract

Short amino acid motifs, either linear sequences or discontinuous amino acid groupings, can interact with specific protein domains, so exerting a central role in cell adhesion, signal transduction, hormone activity, regulation of transcript expression, enzyme activity, and antigen-antibody interaction. Here, we analyze the literature for such critical short amino acid motifs to determine the minimal peptide length involved in biologically important interactions. We report the pentapeptide unit as a common minimal amino acid sequence critically involved in peptide-protein interaction and immune recognition. The present survey may have implications in defining the dimensional module for peptide-based therapeutical approaches such as the development of novel antibiotics, enzyme inhibitors/activators, mimetic agonists/antagonists of neuropeptides, thrombolitic agents, specific anti-viral agents, etc. In such a therapeutical context, it is of considerable interest that low molecular weight peptides can easily cross biological barriers, are less susceptible to protease attacks, and can be administered at high concentrations. In addition, small peptides are a rational target for strategies aimed at antigen-specific immunotherapeutical intervention. As an example, specific short peptide fragments might be used to elicit antibodies capable of reacting with the full-length proteins containing the peptide fragment's amino acid sequence, so abolishing the risk of cross-reactivity.

摘要

短氨基酸基序,无论是线性序列还是不连续的氨基酸分组,都能与特定的蛋白质结构域相互作用,从而在细胞黏附、信号转导、激素活性、转录表达调控、酶活性以及抗原 - 抗体相互作用中发挥核心作用。在此,我们分析了关于此类关键短氨基酸基序的文献,以确定参与生物学重要相互作用的最小肽长度。我们报道五肽单元是肽 - 蛋白质相互作用和免疫识别中关键涉及的常见最小氨基酸序列。本综述可能对定义基于肽的治疗方法的尺寸模块有启示,例如新型抗生素、酶抑制剂/激活剂、神经肽模拟激动剂/拮抗剂、溶栓剂、特异性抗病毒剂等的开发。在这样的治疗背景下,低分子量肽能够轻松穿越生物屏障、不易受到蛋白酶攻击且可高浓度给药,这一点相当有趣。此外,小肽是旨在进行抗原特异性免疫治疗干预策略的合理靶点。例如,特定的短肽片段可用于引发能够与包含该肽片段氨基酸序列的全长蛋白质发生反应的抗体,从而消除交叉反应的风险。

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