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多克隆抗体催化的酰胺水解

Polyclonal antibody-catalysed amide hydrolysis.

作者信息

Gallacher G, Searcey M, Jackson C S, Brocklehurst K

机构信息

Department of Biochemistry, Queen Mary and Westfield College, University of London, U.K.

出版信息

Biochem J. 1992 Jun 15;284 ( Pt 3)(Pt 3):675-80. doi: 10.1042/bj2840675.

Abstract
  1. The activated amide (4-nitroanilide), N-(4-nitrophenyl) N'-butyl-1,4-phenylenediacetamide (III) was synthesized. 2. A polyclonal antibody preparation (PCA 270-29) was elicited in a multigeneration cross-bred sheep (no. 270) and isolated 29 weeks into the immunization schedule by procedures described previously for PCA 270-22 [Gallacher, Jackson, Searcey, Badman, Goel, Topham, Mellor & Brocklehurst (1991) Biochem J. 271, 871-881]. These involved the use of an amide conjugate bonded through the carboxy group of 4-nitrophenyl 4'-carboxymethylphenyl phosphate and an amino group of keyhole-limpet haemocyanin as the immunogen. 3. PCA 270-29 was shown to catalyse the hydrolysis of both the carbonate ester substrate 4-nitrophenyl 4'-(3-aza-2-oxoheptyl)phenyl carbonate (I) and the amide substrate (III). Both catalyses obeyed the Michaelis-Menten equation with the following values of the parameters at 25 degrees C: for the hydrolysis of (I) at pH 8.0, Km = 3.96 +/- 0.28 microM and k(cat.) = 0.135 +/- 0.004 s-1 (k(non-cat.) = 1.99 x 10(-4) s-1); for the hydrolysis of (III) at pH 9.0, Km = 5.4 +/- 1.4 microM and k(cat.) = (5.95 +/- 0.75) x 10(-5) s-1 (k(non-cat.) = approx. 2 x 10(-7) s-1). 4. The finding that PCA 270-29 is almost equally effective as a catalyst for the hydrolysis of the amide (III) as for that of the carbonate ester (I) when allowance is made for the different intrinsic reactivities of the two types of substrate is discussed. The catalytic characteristics of PCA 270-29, the first example of a polyclonal catalytic antibody preparation shown to catalyse the hydrolysis of an amide and the first example of an antibody preparation (monoclonal or polyclonal) with such catalytic character to be produced by use of a phosphate immunogen, are compared with those of the small number of other antibody-mediated hydrolyses of amides in the literature.
摘要
  1. 合成了活化酰胺(4-硝基苯胺),即N-(4-硝基苯基) N'-丁基-1,4-苯二乙酰胺(III)。2. 在多代杂交绵羊(编号270)中诱导产生了多克隆抗体制剂(PCA 270-29),并在免疫计划进行到第29周时,按照先前针对PCA 270-22所述的程序进行分离[加拉赫、杰克逊、西西、巴德曼、戈尔、托普姆、梅勒和布罗克赫斯特(1991年)《生物化学杂志》。271, 871 - 881]。这些程序涉及使用通过4-硝基苯基4'-羧甲基苯基磷酸的羧基与钥孔血蓝蛋白的氨基键合的酰胺缀合物作为免疫原。3. 结果表明,PCA 270-29能催化碳酸酯底物4-硝基苯基4'-(3-氮杂-2-氧代庚基)苯基碳酸酯(I)和酰胺底物(III)的水解。两种催化反应均符合米氏方程,并在25℃下具有以下参数值:对于(I)在pH 8.0时的水解反应,Km = 3.96±0.28 μM,k(cat.) = 0.135±0.004 s-1(k(non-cat.) = 1.99×10-4 s-1);对于(III)在pH 9.0时的水解反应,Km = 5.4±1.4 μM,k(cat.) = (5.95±0.75)×10-5 s-1(k(non-cat.) = 约2×10-7 s-1)。4. 讨论了在考虑两种底物不同的固有反应活性时,PCA 270-29作为酰胺(III)水解催化剂与碳酸酯(I)水解催化剂几乎同样有效的这一发现。将PCA 270-29的催化特性与文献中少量其他抗体介导的酰胺水解反应的催化特性进行了比较。PCA 270-29是首个被证明能催化酰胺水解的多克隆催化抗体制剂的例子,也是首个通过使用磷酸盐免疫原产生具有这种催化特性的抗体(单克隆或多克隆)制剂的例子。

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