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苯甲酸酰肼对髓过氧化物酶的抑制作用。

Inhibition of myeloperoxidase by benzoic acid hydrazides.

作者信息

Kettle A J, Gedye C A, Hampton M B, Winterbourn C C

机构信息

Department of Pathology, Christchurch School of Medicine, New Zealand.

出版信息

Biochem J. 1995 Jun 1;308 ( Pt 2)(Pt 2):559-63. doi: 10.1042/bj3080559.

Abstract

Myeloperoxidase is the most abundant protein in neutrophils and catalyses the conversion of H2O2 and chloride into HOCl. To help clarify the role of this enzyme in bacterial killing and inflammation, a specific and potent inhibitor needs to be identified. We have studied a series of benzoic acid hydrazides and found that in general they inhibit the peroxidation activity of myeloperoxidase with an IC50 value of less than 10 microM. The IC50 values of derivatives with substituents containing oxygen or nitrogen were related to their Hammett substituent constants. This indicates that myeloperoxidase oxidizes the hydrazide group of these compounds, and the degree to which they inhibit the enzyme is dependent on the ease of their oxidation. Unsubstituted benzoic acid hydrazide and its 4-chloro derivative were poor inhibitors of peroxidation. Thus it is likely that hydrogen-bonding of the enzyme to substituents containing oxygen or nitrogen increases the binding affinity of the hydrazides and enhances their oxidation by myeloperoxidase. 4-Aminobenzoic acid hydrazide (ABAH) was the most potent inhibitor of peroxidation. It irreversibly inhibited HOCl production by the purified enzyme, having an IC50 value of 0.3 microM. With neutrophils stimulated with opsonized zymosan or phorbol myristate acetate, ABAH inhibited HOCl production by up to 90% and the IC50 values were 16 microM and 2.2 microM respectively. In the presence of superoxide dismutase, these values decreased to 6.4 microM and 0.6 microM respectively. ABAH had no effect on superoxide radical (O2-.) production and degranulation by neutrophils, nor did it inhibit catalase or glutathione peroxidase. Thus ABAH is an effective and selective inhibitor that should be useful for determining the contribution of myeloperoxidase to oxidant-mediated reactions of neutrophils.

摘要

髓过氧化物酶是中性粒细胞中含量最丰富的蛋白质,可催化过氧化氢和氯离子转化为次氯酸。为了阐明这种酶在细菌杀伤和炎症中的作用,需要鉴定一种特异性且强效的抑制剂。我们研究了一系列苯甲酸酰肼,发现它们一般能抑制髓过氧化物酶的过氧化活性,半数抑制浓度(IC50)值小于10微摩尔。含有氧或氮取代基的衍生物的IC50值与它们的哈米特取代基常数有关。这表明髓过氧化物酶氧化这些化合物的酰肼基团,它们抑制该酶的程度取决于其氧化的难易程度。未取代的苯甲酸酰肼及其4-氯衍生物是过氧化作用的弱抑制剂。因此,酶与含氧或氮取代基之间的氢键作用可能增加了酰肼的结合亲和力,并增强了髓过氧化物酶对它们的氧化作用。4-氨基苯甲酸酰肼(ABAH)是最有效的过氧化作用抑制剂。它能不可逆地抑制纯化酶产生次氯酸,IC50值为0.3微摩尔。在用调理酵母聚糖或佛波酯肉豆蔻酸酯刺激的中性粒细胞中,ABAH可将次氯酸的产生抑制高达90%,IC50值分别为16微摩尔和2.2微摩尔。在超氧化物歧化酶存在的情况下,这些值分别降至6.4微摩尔和0.6微摩尔。ABAH对中性粒细胞产生超氧阴离子自由基(O2-.)和脱颗粒没有影响,也不抑制过氧化氢酶或谷胱甘肽过氧化物酶。因此,ABAH是一种有效且选择性的抑制剂,对于确定髓过氧化物酶在中性粒细胞氧化介导反应中的作用应该是有用的。

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