人胃蛋白酶3b肽图序列分析、基因型及疏水性。

A T Jones, J N Keen, N B Roberts
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引用次数: 7

摘要

从金黄色葡萄球菌(V8)蛋白酶消化的人胃蛋白酶3b的氨基酸序列分析中鉴定出多肽。326个预期残基中只有137个来自分子的C和N端区域。通过对三个不同胃蛋白酶原A基因的核苷酸分析得出的氨基酸序列进行比较,鉴定出4个可能的取代序列中的2个。缬氨酸位于第30位,亮氨酸位于第291位,这表明胃液中主要的胃蛋白酶成分胃蛋白酶3b与胃蛋白酶原基因型PGA-3相对应。天然人胃蛋白酶3b在C4 (300 A)、C18 (300 A)或聚合物(1000 A)色谱柱上的反相色谱在C4柱上是最优的,用2-丙醇而不是乙腈梯度洗脱。蛋白质在盐酸胍、尿素或高pH中变性导致不可逆的柱滞留。变性胃蛋白酶3b的显著疏水性可以解释为什么肽图分析没有显示出该蛋白的中心部分。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Human pepsin 3b peptide map sequence analysis, genotype and hydrophobic nature.

Peptides from a Staphylococcus aureus (V8) proteinase digest of human pepsin 3b have been identified by amino acid sequence analysis. Only 137 out of 326 expected residues were detected from the C and N terminal regions of the molecule. Comparison with amino acid sequences derived from nucleotide analysis of three different pepsinogen A genes, identified 2 out of 4 possible substitutions. The presence of valine at position 30 and leucine at 291 indicates that the major pepsin component of gastric juice, pepsin 3b, corresponds to pepsinogen genotype PGA-3. Reversed-phase chromatography of native human pepsin 3b on C4 (300 A), C18 (300 A) or polymer (1000 A) columns was optimal on the C4 column and gradient elution with 2-propanol rather than acetonitrile. Denaturation of the protein in guanidinium hydrochloride, urea or high pH resulted in irreversible column retention. The marked hydrophobicity of denatured pepsin 3b may thus explain why the central segment of the protein was not revealed by peptide map analysis.

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