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通过pH停流装置评估甘氨酰甘氨酸、血浆和组织提取物的氨基甲酸酯反应。

The carbamate reaction of glycylglycine, plasma, and tissue extracts evaluated by a pH stopped flow apparatus.

作者信息

Gros G, Forster R E, Lin L

出版信息

J Biol Chem. 1976 Jul 25;251(14):4398-407.

PMID:6479
Abstract

We have used a stopped flow rapid reaction pH apparatus to investigate the carbamate equilibrium in glycylglycine solutions and in three biological tissues, human plasma, sheep muscle, and sheep brain, as well as to investigate the kinetics of carbamate formation in glyclyglycine solution and in human plasma. The rapid reaction apparatus was equipped with a pH sensitive glass electrode in order to follow the time course of pH from 0.005 to 100 s after rapid mixing of a solution of amine or protein and CO2. Two phases of the pH curve were observed: a fast phase representing carbamate formation, and a slow phase due to the hydration of CO2 which was uncatalyzed since a carbonic anhydrase inhibitor was added to the biological solutions. From the time course of pH change during the fast phase K2, the R-NH2 ionization constant, and Kc, the carbamate equilibrium constant as well as the velocity constant for the formation of carbamate, ka could be calculated from data at different pH and pCO2. The carbamate formed in glycylglycine solutions over a wide range of pH and pCO2 was found consistent with the theory of carbamate formation and with published data. At ionic strength 0.16 and 37 degrees pK is 7.67. pKc 4.58. The heat of the carbamate reaction (deltaH) was calculated to be -3.2 kcal/mol between 20 degrees and 37 degrees. Kt of glycylglycine depends quantitatively on ionic strength as predicted by the Debye-Huckel theory. With ionic strength 0.16 ku was found to be 2,500 M1 S1 at 37 degrees. The activation energy of carbamate formation is 6.7 kcal/mol. Carbamate measurements in human plasma at pCO2 from 38 to 359 Torr. pH from 6.9 to 8.3, temperature 37 degrees, and ionic strength 0.15 provided evidence that two kinds of amino groups participate in carbamate formation. From the equilibrium constants computed for the two species they could be identified as alpha- and epsilon-amino groups. On the basis of a protein molecular weight of 69.000. 0.6 alpha-amino groups/molecule with pKz=7.0 and pKc=4.2, and 5.9 epsilon-amino groups/molecule with pKz=9.0 and pKc=4.3 contribute to carbamate formation. The velocity constant ka was estimated to be 4,950 M1 S1 for the alpha-amino groups and 13,800 M1 S1 for the epsilon-amino groups. Under physiological conditions (pCO2=40 Torr. pH=7.4). The concentration of carbamate in plasma is 0.6 mM and the half-time of carbamate formation is 0.05 s. In extracts prepared from sheep brain at 37 degrees pH=7 and pCO2=35 Torr. the carbamate formation was estimated to be 0.8 mM. With pCO2=70 Torr and the same pH and temperature the carbamate concentration in muscle approximates 0.3 mM and increases to 7 mM as pH rises to 8. It is concluded that, as in plasma, a considerable number of epsilon-amino groups appear to be available for carbamate formation in these tissues.

摘要

我们使用了停流快速反应pH装置来研究甘氨酰甘氨酸溶液以及三种生物组织(人血浆、羊肌肉和羊脑)中的氨基甲酸酯平衡,同时研究甘氨酰甘氨酸溶液和人血浆中氨基甲酸酯形成的动力学。该快速反应装置配备了一个pH敏感玻璃电极,以便在胺或蛋白质溶液与二氧化碳快速混合后的0.005至100秒内跟踪pH的时间进程。观察到pH曲线有两个阶段:一个快速阶段代表氨基甲酸酯的形成,一个缓慢阶段是由于二氧化碳的水合作用,由于向生物溶液中添加了碳酸酐酶抑制剂,该过程未被催化。根据快速阶段pH变化的时间进程,可以从不同pH和pCO₂下的数据计算出K₂(R-NH₂电离常数)、Kc(氨基甲酸酯平衡常数)以及氨基甲酸酯形成的速度常数ka。在广泛的pH和pCO₂范围内,甘氨酰甘氨酸溶液中形成的氨基甲酸酯与氨基甲酸酯形成理论和已发表的数据一致。在离子强度0.16和37℃时,pK为7.67,pKc为4.58。氨基甲酸酯反应的热(ΔH)在20℃至37℃之间计算为-3.2千卡/摩尔。甘氨酰甘氨酸的Kt如德拜-休克尔理论所预测的那样定量地取决于离子强度。在离子强度0.16时,37℃下ku为2500 M⁻¹ s⁻¹。氨基甲酸酯形成的活化能为6.7千卡/摩尔。在pCO₂为38至359托、pH为6.9至8.3、温度为37℃和离子强度为0.15的条件下人血浆中的氨基甲酸酯测量结果表明,有两种氨基参与氨基甲酸酯的形成。根据为这两种物质计算的平衡常数,可以将它们鉴定为α-和ε-氨基。基于蛋白质分子量69000,有0.6个α-氨基/分子,pK₂ = 7.0,pKc = 4.2,以及5.9个ε-氨基/分子,pK₂ = 9.0,pKc = 4.3参与氨基甲酸酯的形成。α-氨基的速度常数ka估计为4950 M⁻¹ s⁻¹,ε-氨基的速度常数ka估计为13800 M⁻¹ s⁻¹。在生理条件下(pCO₂ = 40托,pH = 7.4),血浆中氨基甲酸酯的浓度为0.6 mM,氨基甲酸酯形成的半衰期为0.05秒。在37℃、pH = 7和pCO₂ = 35托条件下从羊脑制备的提取物中,氨基甲酸酯的形成估计为0.8 mM。在pCO₂ = 70托以及相同的pH和温度下,肌肉中的氨基甲酸酯浓度约为0.3 mM,当pH升至8时增加到7 mM。得出的结论是,与血浆中一样,在这些组织中似乎有相当数量的ε-氨基可用于氨基甲酸酯的形成。

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