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体外胃蛋白酶特异性的统计建模。

Statistical modeling of in vitro pepsin specificity.

机构信息

STLO, INRAE, Institut Agro, 65 rue de Saint-Brieuc, 35042 Rennes, France.

IRMAR UMR6625, CNRS, Institut Agro, 65 rue de Saint-Brieuc, 35042 Rennes, France.

出版信息

Food Chem. 2021 Nov 15;362:130098. doi: 10.1016/j.foodchem.2021.130098. Epub 2021 May 13.

Abstract

The specificity of pepsin, the major protease of gastric digestion, has been previously investigated, but only regarding the primary sequence of the protein substrates. The present study aimed to consider in addition physicochemical and structural characteristics, at the molecular and sub-molecular scales. For six different proteins submitted to in vitro gastric digestion, the peptide bonds cleaved were determined from the peptides released and identified by LC-MS/MS. An original statistical approach, based on propensity scores calculated for each amino acid residue on both sides of the peptide bonds, concluded that preferential cleavage occurred after Leu and Phe, and before Ile. Moreover, reliable statistical models developed for predicting peptide bond cleavage, highlighted the predominant role of the amino acid residues at the N-terminal side of the peptide bonds, up to the seventh position (P7 and P7'). The significant influence of hydrophobicity, charge and structural constraints around the peptide bonds was also evidenced.

摘要

胃蛋白酶是胃消化的主要蛋白酶,其特异性此前已有研究,但仅涉及蛋白质底物的一级序列。本研究旨在考虑理化性质和结构特征,从分子和亚分子尺度进行研究。对于六种不同的蛋白质进行体外胃消化,通过 LC-MS/MS 释放和鉴定的肽来确定肽键的断裂。一种基于肽键两侧每个氨基酸残基计算倾向得分的原始统计方法得出结论,优先断裂发生在亮氨酸和苯丙氨酸之后,异亮氨酸之前。此外,为预测肽键断裂而开发的可靠统计模型强调了肽键 N 末端氨基酸残基的主要作用,可达第七位(P7 和 P7')。还证明了肽键周围疏水性、电荷和结构限制的显著影响。

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