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胰岛素的乙酰化作用。

The acetylation of insulin.

作者信息

Lindsay D G, Shall S

出版信息

Biochem J. 1971 Mar;121(5):737-45. doi: 10.1042/bj1210737a.

Abstract

The acetylation of the free amino groups of insulin was studied by reaction of the hormone with N-hydroxysuccinimide acetate at pH6.9 and 8.5. The products formed were separated by chromatography on DEAE-Sephadex and were characterized by isoelectric focusing, by end-group analysis, by the incorporation of [(3)H]acetyl groups in the molecule, and by treatment with trypsin that had been treated with 1-chloro-4-phenyl-3-toluene-p-sulphonamidobutan-2-one (;tosylphenylalanyl chloromethyl ketone'). Three monosubstituted products, two disubstituted products and one trisubstituted derivative were prepared. The alpha-amino groups of the terminal residues and the in-amino group of the lysine-B29 were the sites of reaction. Acetylation of any of the free amino groups did not affect the biological activity of insulin. It was demonstrated, however, that substitution at the glycine-A1 amino group by the larger residues, acetoacetyl or thiazolidinecarbonyl, produced a decrease in biological activity. Modification of the lysine-B29 or phenylalanine-B1 amino groups with these larger reagents did not affect the biological activity. Modification of the phenylalanine-B1 amino group by any of the three substituents resulted in a large decrease in the affinity of insulin for anti-insulin antibodies raised in the guinea pig. Modification of the other two amino groups did not affect the reaction with antibody. These observations are correlated with the tertiary structure of insulin.

摘要

通过在pH6.9和8.5条件下使胰岛素与N-羟基琥珀酰亚胺乙酸酯反应,研究了胰岛素游离氨基的乙酰化作用。形成的产物通过DEAE-葡聚糖凝胶柱色谱法进行分离,并通过等电聚焦、端基分析、分子中[(3)H]乙酰基的掺入以及用经1-氯-4-苯基-3-甲苯-对磺酰胺基丁-2-酮(;甲苯磺酰苯丙氨酰氯甲基酮')处理的胰蛋白酶处理来进行表征。制备了三种单取代产物、两种双取代产物和一种三取代衍生物。末端残基的α-氨基和赖氨酸-B29的ε-氨基是反应位点。任何游离氨基的乙酰化均不影响胰岛素的生物活性。然而,已证明用较大的残基乙酰乙酰基或噻唑烷羰基取代甘氨酸-A1氨基会导致生物活性降低。用这些较大的试剂修饰赖氨酸-B29或苯丙氨酸-B1氨基并不影响生物活性。用三种取代基中的任何一种修饰苯丙氨酸-B1氨基会导致胰岛素对豚鼠体内产生的抗胰岛素抗体的亲和力大幅降低。修饰其他两个氨基并不影响与抗体的反应。这些观察结果与胰岛素的三级结构相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ffb8/1176661/e8de2ca90053/biochemj00659-0017-a.jpg

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