Systematic analysis and comparison of peptide specificity and selectivity between their cognate receptors and noncognate decoys

IF 2.3 4区生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY

Journal of Molecular Recognition Pub Date : 2022-12-29 DOI:10.1002/jmr.3006

Jianping Shu, Juelin Li, Shaozhou Wang, Jing Lin, Li Wen, Haiyang Ye, Peng Zhou

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引用次数: 8

Abstract

Protein–peptide interactions (PpIs) play an important role in cell signaling networks and have been exploited as new and attractive therapeutic targets. The affinity and specificity are two unity-of-opposite aspects of PpIs (and other biomolecular interactions); the former indicates the absolute binding strength between the peptide ligand and its cognate protein receptor in a PpI, while the latter represents the relative recognition selectivity of the peptide ligand for its cognate protein receptor in a PpI over those noncognate decoys that could be potentially encountered by the peptide in cell. Although the PpI binding affinity has been widely investigated over the past decades, the peptide recognition specificity (and selectivity) still remains largely unexplored to date. In this study, we classified PpI specificity into three types: (i) class-I specificity: peptide selectivity for its cognate wild-type protein receptor over the noncognate mutant decoys of this receptor, (ii) class-II specificity: peptide selectivity for its cognate protein receptor over other noncognate decoys that are homologous with this receptor, and (iii) class-III specificity: peptide selectivity for its cognate protein receptor over other noncognate decoys that are the cognate receptors of other peptides. We performed affinity and selectivity analysis for the three types of PpI specificity and revealed that the PpIs generally exhibit a moderate or modest specificity; peptide selectivity increases in the order: class-I < class-II < class-III. All the three types of PpI specificity were observed to have no statistically significant correlation with peptide length and hydrophobicity, but the class-I and class-II specificities can be influenced considerably by peptide secondary structures; the high specificity is preferentially associated with ordered structure types as compared to undefined structure types. In addition, the mutation distribution (for class-I specificity), sequence conservation (for class-II specificity), and structural similarity (for class-III specificity) seem also to address effects on peptide selectivity.

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系统分析和比较其同源受体和非同源诱饵的肽特异性和选择性

蛋白-肽相互作用(PpIs)在细胞信号网络中发挥着重要作用，并已被开发为新的和有吸引力的治疗靶点。亲和力和特异性是ppi(和其他生物分子相互作用)的两个对立统一方面;前者表示肽配体在PpI中与其同源蛋白受体之间的绝对结合强度，而后者表示肽配体在PpI中对其同源蛋白受体的相对识别选择性，而不是肽在细胞中可能遇到的非同源诱饵。虽然在过去的几十年里，PpI的结合亲和力已经得到了广泛的研究，但肽识别的特异性(和选择性)至今仍未得到很大的探索。在本研究中，我们将PpI特异性分为三种类型:(i) i类特异性:其同源野生型蛋白受体对该受体非同源突变诱饵的肽选择性，(ii) ii类特异性:其同源蛋白受体对其他与该受体同源的非同源诱饵的肽选择性，以及(iii) iii类特异性。多肽对其同源蛋白受体的选择性优于其他非同源诱饵，即其他多肽的同源受体。我们对三种类型的PpI特异性进行了亲和力和选择性分析，发现PpI通常表现出中等或中等的特异性;肽选择性依次增加:ⅰ类<ⅱ类<ⅲ类。三种类型PpI的特异性均与肽长度和疏水性无统计学意义相关，但ⅰ类和ⅱ类特异性受肽二级结构的影响较大;与未定义结构类型相比，高特异性优先与有序结构类型相关。此外，突变分布(针对i类特异性)、序列保守性(针对ii类特异性)和结构相似性(针对iii类特异性)似乎也能解决对肽选择性的影响。

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来源期刊

Journal of Molecular Recognition 生物-生化与分子生物学

CiteScore

4.60

自引率

3.70%

发文量

审稿时长

2.7 months

期刊介绍： Journal of Molecular Recognition (JMR) publishes original research papers and reviews describing substantial advances in our understanding of molecular recognition phenomena in life sciences, covering all aspects from biochemistry, molecular biology, medicine, and biophysics. The research may employ experimental, theoretical and/or computational approaches. The focus of the journal is on recognition phenomena involving biomolecules and their biological / biochemical partners rather than on the recognition of metal ions or inorganic compounds. Molecular recognition involves non-covalent specific interactions between two or more biological molecules, molecular aggregates, cellular modules or organelles, as exemplified by receptor-ligand, antigen-antibody, nucleic acid-protein, sugar-lectin, to mention just a few of the possible interactions. The journal invites manuscripts that aim to achieve a complete description of molecular recognition mechanisms between well-characterized biomolecules in terms of structure, dynamics and biological activity. Such studies may help the future development of new drugs and vaccines, although the experimental testing of new drugs and vaccines falls outside the scope of the journal. Manuscripts that describe the application of standard approaches and techniques to design or model new molecular entities or to describe interactions between biomolecules, but do not provide new insights into molecular recognition processes will not be considered. Similarly, manuscripts involving biomolecules uncharacterized at the sequence level (e.g. calf thymus DNA) will not be considered.