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基于蛋白质组学方法鉴定的巨型石斑鱼鱼卵蛋白中释放的生物活性肽的计算机分析。

In Silico Analysis of Bioactive Peptides Released from Giant Grouper () Roe Proteins Identified by Proteomics Approach.

机构信息

Department of Food Science, National Taiwan Ocean University, Keelung 20224, Taiwan.

Institute of Fish Processing Technology, College of Fisheries and Ocean Sciences, University of the Philippines Visayas, Miagao, Iloilo 5023, Philippines.

出版信息

Molecules. 2018 Nov 8;23(11):2910. doi: 10.3390/molecules23112910.

Abstract

Major proteins contained in dried giant grouper roe (GR) such as vitellogenin (from ; NCBI accession number: AAW29031.1), apolipoprotein A-1 precursor (from ; NCBI accession number: ACI01807.1) and apolipoprotein E (from ; NCBI accession number: AEB31283.1) were characterized through compiled proteomics techniques (SDS-PAGE, in-gel digestion, mass spectrometry and on-line Mascot database analysis). These proteins were subjected to in silico analysis using BLAST and BIOPEP-UWM database. Sequence similarity search by BLAST revealed that the aligned vitellogenin sequences from and share 70% identity, which indicates that the sequence sample has significant similarity with proteins in sequence databases. Moreover, prediction of potential bioactivities through BIOPEP-UWM database resulted in high numbers of peptides predominantly with dipeptidyl peptidase-IV (DPP-IV) and angiotensin-I-converting enzyme (ACE-I) inhibitory activities. Pepsin (pH > 2) was predicted to be the most promising enzyme for the production of bioactive peptides from GR protein, which theoretically released 82 DPP-IV inhibitory peptides and 47 ACE-I inhibitory peptides. Overall, this work highlighted the potentiality of giant grouper roe as raw material for the generation of pharmaceutical products. Furthermore, the application of proteomics and in silico techniques provided rapid identification of proteins and useful prediction of its potential bioactivities.

摘要

通过编译蛋白质组学技术(SDS-PAGE、胶内消化、质谱和在线 Mascot 数据库分析)对干巨型石斑鱼鱼卵(GR)中包含的主要蛋白质(如卵黄蛋白原(来自;NCBI 登录号:AAW29031.1)、载脂蛋白 A-1 前体(来自;NCBI 登录号:ACI01807.1)和载脂蛋白 E(来自;NCBI 登录号:AEB31283.1))进行了表征。这些蛋白质使用 BLAST 和 BIOPEP-UWM 数据库进行了计算机分析。BLAST 的序列相似性搜索表明,与 和 对齐的卵黄蛋白原序列具有 70%的同一性,这表明该序列样本与序列数据库中的蛋白质具有显著的相似性。此外,通过 BIOPEP-UWM 数据库预测潜在的生物活性导致大量的肽主要具有二肽基肽酶-IV(DPP-IV)和血管紧张素 I 转换酶(ACE-I)抑制活性。预测胃蛋白酶(pH>2)是从 GR 蛋白生产生物活性肽最有前途的酶,理论上可释放 82 个 DPP-IV 抑制肽和 47 个 ACE-I 抑制肽。总的来说,这项工作强调了巨型石斑鱼鱼卵作为药物产品原料的潜力。此外,蛋白质组学和计算机技术的应用提供了蛋白质的快速鉴定和其潜在生物活性的有用预测。

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