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1
Consequences of molecular recognition in the S1-S2 intersubsite region of papain for catalytic-site chemistry. Change in pH-dependence characteristics and generation of an inverse solvent kinetic isotope effect by introduction of a P1-P2 amide bond into a two-protonic-state reactivity probe.木瓜蛋白酶S1 - S2亚位点间区域分子识别对催化位点化学的影响。通过将P1 - P2酰胺键引入双质子态反应性探针,pH依赖性特征的变化及反向溶剂动力学同位素效应的产生。
Biochem J. 1988 Mar 15;250(3):761-72. doi: 10.1042/bj2500761.
2
Identification of signalling and non-signalling binding contributions to enzyme reactivity. Alternative combinations of binding interactions provide for change in transition-state geometry in reactions of papain.确定信号和非信号结合对酶反应性的贡献。结合相互作用的不同组合导致木瓜蛋白酶反应中过渡态几何结构的变化。
Biochem J. 1989 Mar 15;258(3):755-64. doi: 10.1042/bj2580755.
3
Supracrystallographic resolution of interactions contributing to enzyme catalysis by use of natural structural variants and reactivity-probe kinetics.利用天然结构变异体和反应性探针动力学对有助于酶催化的相互作用进行超晶体学分辨率研究。
Biochem J. 1988 Dec 1;256(2):543-58. doi: 10.1042/bj2560543.
4
Substrate-derived two-protonic-state electrophiles as sensitive kinetic specificity probes for cysteine proteinases. Activation of 2-pyridyl disulphides by hydrogen-bonding.作为半胱氨酸蛋白酶敏感动力学特异性探针的底物衍生双质子态亲电试剂。通过氢键作用激活2-吡啶基二硫化物。
Biochem J. 1987 May 15;244(1):173-81. doi: 10.1042/bj2440173.
5
Evaluation of hydrogen-bonding and enantiomeric P2-S2 hydrophobic contacts in dynamic aspects of molecular recognition by papain.木瓜蛋白酶分子识别动态过程中氢键和对映体P2-S2疏水相互作用的评估。
Biochem J. 1992 Nov 1;287 ( Pt 3)(Pt 3):881-9. doi: 10.1042/bj2870881.
6
A re-appraisal of the structural basis of stereochemical recognition in papain. Insensitivity of binding-site-catalytic-site signalling to P2-chirality in a time-dependent inhibition.木瓜蛋白酶中立体化学识别结构基础的重新评估。在时间依赖性抑制中,结合位点 - 催化位点信号对P2手性不敏感。
Biochem J. 1990 Mar 15;266(3):645-51. doi: 10.1042/bj2660645.
7
Differences in the chemical and catalytic characteristics of two crystallographically 'identical' enzyme catalytic sites. Characterization of actinidin and papain by a combination of pH-dependent substrate catalysis kinetics and reactivity probe studies targeted on the catalytic-site thiol group and its immediate microenvironment.两个晶体学上“相同”的酶催化位点在化学和催化特性上的差异。通过结合pH依赖性底物催化动力学以及针对催化位点硫醇基团及其紧邻微环境的反应性探针研究,对猕猴桃蛋白酶和木瓜蛋白酶进行表征。
Biochem J. 1987 Oct 1;247(1):181-93. doi: 10.1042/bj2470181.
8
Ionization characteristics of the Cys-25/His-159 interactive system and of the modulatory group of papain: resolution of ambiguity by electronic perturbation of the quasi-2-mercaptopyridine leaving group in a new pyrimidyl disulphide reactivity probe.半胱氨酸-25/组氨酸-159相互作用系统及木瓜蛋白酶调节基团的电离特性:通过新型嘧啶基二硫化物反应性探针中准2-巯基吡啶离去基团的电子扰动解决歧义问题。
Biochem J. 1993 Feb 15;290 ( Pt 1)(Pt 1):289-96. doi: 10.1042/bj2900289.
9
The interplay of electrostatic fields and binding interactions determining catalytic-site reactivity in actinidin. A possible origin of differences in the behaviour of actinidin and papain.静电场与结合相互作用的相互影响决定了猕猴桃蛋白酶催化位点的反应活性。猕猴桃蛋白酶和木瓜蛋白酶行为差异的一个可能来源。
Biochem J. 1989 Apr 15;259(2):443-52. doi: 10.1042/bj2590443.
10
Evidence that binding to the s2-subsite of papain may be coupled with catalytically relevant structural change involving the cysteine-25-histidine-159 diad. Kinetics of the reaction of papain with a two-protonic-state reactivity probe containing a hydrophobic side chain.有证据表明,与木瓜蛋白酶的s2亚位点结合可能与涉及半胱氨酸-25-组氨酸-159二元组的催化相关结构变化相关联。木瓜蛋白酶与含有疏水侧链的双质子态反应性探针反应的动力学。
Biochem J. 1979 Nov 1;183(2):223-31. doi: 10.1042/bj1830223.

引用本文的文献

1
Molecular basis of specificity and deamidation of eIF4A by Burkholderia Lethal Factor 1.eIF4A 被伯克霍尔德菌致死因子 1 特异性脱酰胺的分子基础。
Commun Biol. 2022 Mar 28;5(1):272. doi: 10.1038/s42003-022-03186-2.
2
Protein arginine deiminase 4: evidence for a reverse protonation mechanism.蛋白质精氨酸脱亚氨酶4:反向质子化机制的证据
Biochemistry. 2007 Jun 5;46(22):6578-87. doi: 10.1021/bi700095s. Epub 2007 May 12.
3
Appendix: Analysis of pH-dependent kinetics in up to four reactive hydronic states.附录:多达四种反应性水合状态下pH依赖性动力学分析
Biochem J. 1988 Dec 1;256(2):556-8. doi: 10.1042/bj2560556.
4
Temperature-dependences of the kinetics of reactions of papain and actinidin with a series of reactivity probes differing in key molecular recognition features.木瓜蛋白酶和猕猴桃蛋白酶与一系列在关键分子识别特征上不同的反应性探针反应动力学的温度依赖性。
Biochem J. 2006 May 15;396(1):17-21. doi: 10.1042/BJ20051501.
5
Clarification of the pH-dependent kinetic behaviour of papain by using reactivity probes and analysis of alkylation and catalysed acylation reactions in terms of multihydronic state models: implications for electrostatics calculations and interpretation of the consequences of site-specific mutations such as Asp-158-Asn and Asp-158-Glu.利用反应性探针阐明木瓜蛋白酶的pH依赖性动力学行为,并根据多质子态模型分析烷基化和催化酰化反应:对静电计算以及对位点特异性突变(如Asp-158-Asn和Asp-158-Glu)后果的解释的意义。
Biochem J. 1993 Aug 15;294 ( Pt 1)(Pt 1):201-10. doi: 10.1042/bj2940201.
6
Structure of chymopapain M the late-eluted chymopapain deduced by comparative modelling techniques and active-centre characteristics determined by pH-dependent kinetics of catalysis and reactions with time-dependent inhibitors: the Cys-25/His-159 ion-pair is insufficient for catalytic competence in both chymopapain M and papain.糜蛋白酶M的结构:通过比较建模技术推导得出的晚期洗脱糜蛋白酶,以及通过pH依赖性催化动力学和与时间依赖性抑制剂反应确定的活性中心特征:半胱氨酸-25/组氨酸-159离子对对于糜蛋白酶M和木瓜蛋白酶的催化活性而言均不充分。
Biochem J. 1994 Jun 15;300 ( Pt 3)(Pt 3):805-20. doi: 10.1042/bj3000805.
7
Supracrystallographic resolution of interactions contributing to enzyme catalysis by use of natural structural variants and reactivity-probe kinetics.利用天然结构变异体和反应性探针动力学对有助于酶催化的相互作用进行超晶体学分辨率研究。
Biochem J. 1988 Dec 1;256(2):543-58. doi: 10.1042/bj2560543.
8
The interplay of electrostatic and binding interactions determining active centre chemistry and catalytic activity in actinidin and papain.静电相互作用与结合相互作用之间的相互影响决定了猕猴桃蛋白酶和木瓜蛋白酶的活性中心化学性质及催化活性。
Biochem J. 1989 Jan 1;257(1):309-10. doi: 10.1042/bj2570309.
9
Identification of signalling and non-signalling binding contributions to enzyme reactivity. Alternative combinations of binding interactions provide for change in transition-state geometry in reactions of papain.确定信号和非信号结合对酶反应性的贡献。结合相互作用的不同组合导致木瓜蛋白酶反应中过渡态几何结构的变化。
Biochem J. 1989 Mar 15;258(3):755-64. doi: 10.1042/bj2580755.
10
The interplay of electrostatic fields and binding interactions determining catalytic-site reactivity in actinidin. A possible origin of differences in the behaviour of actinidin and papain.静电场与结合相互作用的相互影响决定了猕猴桃蛋白酶催化位点的反应活性。猕猴桃蛋白酶和木瓜蛋白酶行为差异的一个可能来源。
Biochem J. 1989 Apr 15;259(2):443-52. doi: 10.1042/bj2590443.

本文引用的文献

1
Effect of cysteine-25 on the ionization of histidine-159 in papain as determined by proton nuclear magnetic resonance spectroscopy. Evidence for a his-159--Cys-25 ion pair and its possible role in catalysis.通过质子核磁共振光谱法测定半胱氨酸-25对木瓜蛋白酶中组氨酸-159电离的影响。组氨酸-159与半胱氨酸-25离子对的证据及其在催化中的可能作用。
Biochemistry. 1981 Jan 6;20(1):48-51. doi: 10.1021/bi00504a009.
2
Determination of a low pK for histidine-159 in the S-methylthio derivative of papain by proton nuclear magnetic resonance spectroscopy.通过质子核磁共振光谱法测定木瓜蛋白酶S-甲硫基衍生物中组氨酸-159的低pK值。
Biochemistry. 1981 Jan 6;20(1):44-8. doi: 10.1021/bi00504a008.
3
Solvent isotope effects on the rates of alkylation of thiolamine models of papain.溶剂同位素效应对半胱氨酸木瓜蛋白酶模型烷基化反应速率的影响。
FEBS Lett. 1980 Jul 11;116(1):116-21. doi: 10.1016/0014-5793(80)80541-2.
4
Is the thiolate--imidazolium ion pair the catalytically important form of papain?硫醇盐 - 咪唑鎓离子对是木瓜蛋白酶具有催化活性的重要形式吗?
FEBS Lett. 1980 Feb 11;110(2):319-22. doi: 10.1016/0014-5793(80)80101-3.
5
Solvent isotope effects on tautomerization equilibria of papain and model thiolamines.溶剂同位素对木瓜蛋白酶和模型硫醇胺互变异构平衡的影响。
FEBS Lett. 1980 Feb 11;110(2):313-8. doi: 10.1016/0014-5793(80)80100-1.
6
Half-time analysis of the integrated Michaelis equation. Simulation and use of the half-time plot and its direct linear variant in the analysis of some alpha-chymotrypsin, papain- and fumarase-catalysed reactions.米氏积分方程的半衰期分析。半衰期图及其直接线性变体在某些α-糜蛋白酶、木瓜蛋白酶和延胡索酸酶催化反应分析中的模拟与应用。
Biochem J. 1982 May 1;203(2):351-60. doi: 10.1042/bj2030351.
7
Precise structural information for transient enzyme-substrate complexes by a combined X-ray crystallographic-resonance Raman spectroscopic approach.
Biochemistry. 1982 Jun 22;21(13):3109-15. doi: 10.1021/bi00256a012.
8
Evidence for a close similarity in the catalytic sites of papain and ficin in near-neutral media despite differences in acidic and alkaline media. Kinetics of the reactions of papain and ficin with chloroacetate.尽管在酸性和碱性介质中存在差异,但木瓜蛋白酶和无花果蛋白酶在近中性介质中的催化位点具有高度相似性的证据。木瓜蛋白酶和无花果蛋白酶与氯乙酸反应的动力学。
Biochem J. 1982 Jan 1;201(1):101-4. doi: 10.1042/bj2010101.
9
Proteinase-catalyzed synthesis of peptide bonds.
Adv Enzymol Relat Areas Mol Biol. 1982;53:239-306. doi: 10.1002/9780470122983.ch7.
10
Evidence for a two-state transition in papain that may have no close analogue in ficin. Differences in the disposition of cationic sites and hydrophobic binding areas in the active centres of papain and ficin.木瓜蛋白酶中可能在无花果蛋白酶中没有类似情况的双态转变的证据。木瓜蛋白酶和无花果蛋白酶活性中心中阳离子位点和疏水结合区域分布的差异。
Biochem J. 1980 Dec 1;191(3):707-18. doi: 10.1042/bj1910707.

木瓜蛋白酶S1 - S2亚位点间区域分子识别对催化位点化学的影响。通过将P1 - P2酰胺键引入双质子态反应性探针,pH依赖性特征的变化及反向溶剂动力学同位素效应的产生。

Consequences of molecular recognition in the S1-S2 intersubsite region of papain for catalytic-site chemistry. Change in pH-dependence characteristics and generation of an inverse solvent kinetic isotope effect by introduction of a P1-P2 amide bond into a two-protonic-state reactivity probe.

作者信息

Brocklehurst K, Kowlessur D, Patel G, Templeton W, Quigley K, Thomas E W, Wharton C W, Willenbrock F, Szawelski R J

机构信息

Department of Biochemistry, St. Bartholomew's Hospital Medical College, University of London, U.K.

出版信息

Biochem J. 1988 Mar 15;250(3):761-72. doi: 10.1042/bj2500761.

DOI:10.1042/bj2500761
PMID:2839145
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1148922/
Abstract
  1. The pH-dependences of the second-order rate constant (k) for the reactions of papain (EC 3.4.22.2) with 2-(acetamido)ethyl 2'-pyridyl disulphide and with ethyl 2-pyridyl disulphide and of k for the reaction of benzimidazol-2-ylmethanethiol (as a minimal model of cysteine proteinase catalytic sites) with the former disulphide were determined in aqueous buffers at 25 degrees C at I 0.1. 2. Of these three pH-k profiles only that for the reaction of papain with 2-(acetamido)ethyl 2'-pyridyl disulphide has a rate maximum at pH approx. 6; the others each have a rate minimum in this pH region and a rate maximum at pH 4, which is characteristic of reactions of papain with other 2-pyridyl disulphides that do not contain a P1-P2 amide bond in the non-pyridyl part of the molecule. 3. The marked change in the form of the pH-k profile consequent upon introduction of a P1-P2 amide bond into the probe molecule for the reaction with papain but not for that with the minimal catalytic-site model is interpreted in terms of the induction by binding of the probe in the S1-S2 intersubsite region of the enzyme of a transition-state geometry in which nucleophilic attack by the -S- component of the catalytic site is assisted by association of the imidazolium ion component with the leaving group. 4. The greater definition of the rate maximum in the pH-k profile for the reaction of papain with an analogous 2-pyridyl disulphide reactivity probe containing both a P1-P2 amide bond and a potential occupant for the S2 subsite [2-(N'-acetyl-L-phenylalanylamino)ethyl 2'-pyridyl disulphide [Brocklehurst, Kowlessur, O'Driscoll, Patel, Quenby, Salih, Templeton, Thomas & Willenbrock (1987) Biochem. J. 244, 173-181]) suggests that a P2-S2 interaction substantially increases the population of transition states for the imidazolium ion-assisted reaction. 5. The overall kinetic solvent 2H-isotope effect at pL 6.0 was determined to be: for the reaction of papain with 2,2'-dipyridyl disulphide, 0.96 (i.e. no kinetic isotope effect), for its reaction with the probe containing only the P1-P2 amide bond, 0.75, for its reaction with the probe containing both the P1-P2 amide bond and the occupant for the S2 subsite, 0.61, and for kcat./Km for its catalysis of the hydrolysis of N-methoxycarbonylglycine 4-nitrophenyl ester, 0.67.(ABSTRACT TRUNCATED AT 400 WORDS)
摘要
  1. 在25℃、离子强度I = 0.1的水性缓冲液中,测定了木瓜蛋白酶(EC 3.4.22.2)与2-(乙酰氨基)乙基2'-吡啶基二硫化物、与乙基2-吡啶基二硫化物反应的二级速率常数(k)的pH依赖性,以及苯并咪唑-2-基甲硫醇(作为半胱氨酸蛋白酶催化位点的最小模型)与前一种二硫化物反应的k的pH依赖性。2. 在这三种pH-k曲线中,只有木瓜蛋白酶与2-(乙酰氨基)乙基2'-吡啶基二硫化物反应的曲线在pH约为6时具有速率最大值;其他曲线在该pH区域各有一个速率最小值,在pH 4时有一个速率最大值,这是木瓜蛋白酶与分子中非吡啶部分不含P1 - P2酰胺键的其他2-吡啶基二硫化物反应的特征。3. 将P1 - P2酰胺键引入与木瓜蛋白酶反应的探针分子中,pH-k曲线形式发生显著变化,而与最小催化位点模型反应时则没有这种变化,这可以解释为探针在酶的S1 - S2亚位点区域结合诱导了一种过渡态几何结构,其中催化位点的 -S- 组分的亲核攻击通过咪唑鎓离子组分与离去基团的缔合得到辅助。4. 木瓜蛋白酶与同时含有P1 - P2酰胺键和S2亚位点占据基团的类似2-吡啶基二硫化物反应性探针[2-(N'-乙酰-L-苯丙氨酰氨基)乙基2'-吡啶基二硫化物[布罗克赫斯特、科维勒苏尔、奥德里斯科尔、帕特尔、昆比、萨利赫、坦普尔顿、托马斯和威伦布罗克(1987年)《生物化学杂志》244卷,173 - 181页]]反应的pH-k曲线中速率最大值的定义更明确,这表明P2 - S2相互作用显著增加了咪唑鎓离子辅助反应的过渡态数量。5. 测定了在pL 6.0时的整体动力学溶剂2H同位素效应:对于木瓜蛋白酶与2,2'-二吡啶基二硫化物的反应,为0.96(即无动力学同位素效应),对于其与仅含P1 - P2酰胺键的探针的反应,为0.75,对于其与同时含P1 - P2酰胺键和S2亚位点占据基团的探针的反应,为0.61,对于其催化N-甲氧基羰基甘氨酸4-硝基苯酯水解的kcat./Km,为0.67。(摘要截短于400字)