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溶菌酶的酶学与免疫化学性质。十六、通过直接连接构成抗原反应位点的相关构象相邻残基来构建该位点的一种新型合成方法。

Enzymic and immunochemical properties of lysozyme. XVI. A novel synthetic approach to an antigenic reactive site by direct linkage of the relevant conformationally adjacent residues constituting the site.

作者信息

Atassi M Z, Lee C L, Pai R C

出版信息

Biochim Biophys Acta. 1976 Apr 14;427(2):745-51. doi: 10.1016/0005-2795(76)90219-1.

DOI:10.1016/0005-2795(76)90219-1
PMID:57805
Abstract

Previous studies from this laboratory on the immunochemistry of specific chemical derivatives of native lysozyme and of the two disulfide peptide 62-68 (Cys 64-Cys 80) 74-97 (Cys 76-Cys 94) (i.e. (SS)2-peptide), have established an antigenic reactive site to comprise the spatially contiguous surface residues: Trp 72, Lys 97, Lys 96, Asn 93, Thr 89 and Asp 87. In the present work, the identity of the site was verified by an entirely different and novel approach. The aforementioned amino acids were linked directly into a single linear peptide with an intervening spacer where appropriate and substituting phenylalanine for tryptophan (i.e. Phe-Gly-Lys-Asn-Thr-Asp). This peptide (which does not exist in native lysozyme but simulates a surface region of the protein) possessed a remarkable inhibitory activity towards the reaction of lysozyme with its antisera. The immunochemical reactivity of the peptide was equal to the maximum expected reactivity of the site (i.e. a third of the total antigenic reactivity of lysozyme). These findings define quite conclusively and accurately the reactive site which is clearly composed of spatially adjacent residues that are distant in sequence reacting as if in direct linear linkage. The unequivocal establishment of this concept indicates that antigenic sites need not always be composed of residues in direct peptide linkage in the sequence. The nature of the site may depend on the protein. This unorthodox attack at the problem provides a novel and powerful approach for final delineation of the antigenic reactive sites (and perhaps other types of binding sites) in native proteins, following the completion of accurate narrowing down by chemical methods.

摘要

本实验室先前对天然溶菌酶的特定化学衍生物以及两种二硫键肽62 - 68(半胱氨酸64 - 半胱氨酸80)、74 - 97(半胱氨酸76 - 半胱氨酸94)(即(SS)2 - 肽)的免疫化学研究,已确定一个抗原反应位点,该位点由空间上相邻的表面残基组成:色氨酸72、赖氨酸97、赖氨酸96、天冬酰胺93、苏氨酸89和天冬氨酸87。在本研究中,通过一种完全不同且新颖的方法验证了该位点的特性。上述氨基酸在适当位置通过间隔基团直接连接成单个线性肽,并将色氨酸替换为苯丙氨酸(即苯丙氨酸 - 甘氨酸 - 赖氨酸 - 天冬酰胺 - 苏氨酸 - 天冬氨酸)。该肽(天然溶菌酶中不存在,但模拟了蛋白质的一个表面区域)对溶菌酶与其抗血清的反应具有显著的抑制活性。该肽的免疫化学反应性等同于该位点预期的最大反应性(即溶菌酶总抗原反应性的三分之一)。这些发现确凿且准确地定义了反应位点,该位点显然由序列上相隔较远但空间上相邻的残基组成,它们的反应就如同直接线性连接一样。这一概念的明确确立表明,抗原位点不一定总是由序列中直接肽键连接的残基组成。位点的性质可能取决于蛋白质。这种对该问题的非传统研究方法为在通过化学方法精确缩小范围后最终确定天然蛋白质中的抗原反应位点(或许还有其他类型的结合位点)提供了一种新颖且强大的方法。

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1
Enzymic and immunochemical properties of lysozyme. XVI. A novel synthetic approach to an antigenic reactive site by direct linkage of the relevant conformationally adjacent residues constituting the site.溶菌酶的酶学与免疫化学性质。十六、通过直接连接构成抗原反应位点的相关构象相邻残基来构建该位点的一种新型合成方法。
Biochim Biophys Acta. 1976 Apr 14;427(2):745-51. doi: 10.1016/0005-2795(76)90219-1.
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Biochim Biophys Acta. 1976 Feb 20;420(2):358-75. doi: 10.1016/0005-2795(76)90328-7.
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Delineation of the third antigenic site of lysozyme by application of a novel 'surface-simulation' synthetic approach directly linking the conformationally adjacent residues forming the site.通过应用一种新颖的“表面模拟”合成方法直接连接形成该位点的构象相邻残基,来描绘溶菌酶的第三个抗原位点。
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Boundary refinement of the lysozyme antigenic site around the disulphide bond 6-127 (site 1) by 'surface-simulation' synthesis.通过“表面模拟”合成对围绕二硫键6-127(位点1)的溶菌酶抗原位点进行边界优化。
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Enzymic and immunochemical properties of lysozyme. XI. Conformation and immunochemistry of the two-disulfide peptide and the tryptophan and lysine residues in its antigenic reactivity.溶菌酶的酶学和免疫化学性质。十一、二硫键肽的构象与免疫化学及其抗原反应性中的色氨酸和赖氨酸残基
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The precise and entire antigenic structure of lysozyme: implications of surface-simulation synthesis and the molecular features of protein antigenic sites.溶菌酶精确完整的抗原结构:表面模拟合成的意义及蛋白质抗原位点的分子特征
Adv Exp Med Biol. 1978;98:41-99. doi: 10.1007/978-1-4615-8858-0_4.
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Can an antibody-combining site be mimicked synthetically? The possible surface simulation synthesis of two antibody-combining sites complementary to two antigenic sites of lysozyme.抗体结合位点能否通过合成进行模拟?针对溶菌酶两个抗原位点的两个抗体结合位点的可能表面模拟合成。
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引用本文的文献

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Using THz Spectroscopy, Evolutionary Network Analysis Methods, and MD Simulation to Map the Evolution of Allosteric Communication Pathways in c-Type Lysozymes.利用太赫兹光谱、进化网络分析方法和分子动力学模拟绘制c型溶菌酶变构通讯途径的演变图谱。
Mol Biol Evol. 2016 Jan;33(1):40-61. doi: 10.1093/molbev/msv178. Epub 2015 Sep 3.
2
SUPERFICIAL--surface mapping of proteins via structure-based peptide library design.表面——通过基于结构的肽库设计对蛋白质进行表面图谱分析。
BMC Bioinformatics. 2005 Sep 9;6:223. doi: 10.1186/1471-2105-6-223.
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Design of peptide enzymes (pepzymes): surface-simulation synthetic peptides that mimic the chymotrypsin and trypsin active sites exhibit the activity and specificity of the respective enzyme.
肽酶(pepzyme)的设计:模拟胰凝乳蛋白酶和胰蛋白酶活性位点的表面模拟合成肽表现出相应酶的活性和特异性。
Proc Natl Acad Sci U S A. 1993 Sep 1;90(17):8282-6. doi: 10.1073/pnas.90.17.8282.
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Binding with lysozyme of antibodies against surface-simulation peptides representing the lysozyme antigenic sites.针对代表溶菌酶抗原位点的表面模拟肽的抗体与溶菌酶的结合。
Biochem J. 1982 Mar 1;201(3):669-72. doi: 10.1042/bj2010669.
5
Inhibition of rabbit tissue kininase by anti-(endo-oligopeptidase A) antibodies.抗(内肽酶A)抗体对兔组织激肽酶的抑制作用。
Biochem J. 1981 Jul 1;197(1):85-93. doi: 10.1042/bj1970085.
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Antibody combining sites can be mimicked synthetically. Surface-simulation synthesis of the phosphorylcholine-combining site of myeloma protein M-603.抗体结合位点可以通过合成来模拟。骨髓瘤蛋白M-603磷酸胆碱结合位点的表面模拟合成。
Biochem J. 1980 Jun 1;187(3):661-6. doi: 10.1042/bj1870661.
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Localization, synthesis, and activity of an antigenic site on influenza virus hemagglutinin.流感病毒血凝素抗原位点的定位、合成与活性
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Precise determination of protein antigenic structures has unravelled the molecular immune recognition of proteins and provided a prototype for synthetic mimicking of other protein binding sites.蛋白质抗原结构的精确测定揭示了蛋白质的分子免疫识别,并为其他蛋白质结合位点的合成模拟提供了原型。
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