van Dalen Christine J, Winterbourn Christine C, Kettle Anthony J
Centre for Public Health Research, Massey University, Wellington, New Zealand.
Biochem J. 2006 Mar 15;394(Pt 3):707-13. doi: 10.1042/BJ20051470.
Eosinophil peroxidase is a haem enzyme of eosinophils that is implicated in oxidative tissue injury in asthma. It uses hydrogen peroxide to oxidize thiocyanate and bromide to their respective hypohalous acids. Nitrite is also a substrate for eosinophil peroxidase. We have investigated the mechanisms by which the enzyme oxidizes nitrite. Nitrite was very effective at inhibiting hypothiocyanous acid ('cyanosulphenic acid') and hypobromous acid production. Spectral studies showed that nitrite reduced the enzyme to its compound II form, which is a redox intermediate containing Fe(IV) in the haem active site. Compound II does not oxidize thiocyanate or bromide. These results demonstrate that nitrite is readily oxidized by compound I, which contains Fe(V) at the active site. However, it reacts more slowly with compound II. The observed rate constant for reduction of compound II by nitrite was determined to be 5.6x10(3) M(-1) x s(-1). Eosinophils were at least 4-fold more effective at promoting nitration of a heptapeptide than neutrophils. This result is explained by our finding that nitrite reacts 10-fold faster with compound II of eosinophil peroxidase than with the analogous redox intermediate of myeloperoxidase. Nitration by eosinophils was increased 3-fold by superoxide dismutase, which indicates that superoxide interferes with nitration. We propose that at sites of eosinophilic inflammation, low concentrations of nitrite will retard oxidant production by eosinophil peroxidase, whereas at higher concentrations nitrogen dioxide will be a major oxidant formed by these cells. The efficiency of protein nitration will be decreased by the diffusion-controlled reaction of superoxide with nitrogen dioxide.
嗜酸性粒细胞过氧化物酶是嗜酸性粒细胞的一种血红素酶,与哮喘中的氧化组织损伤有关。它利用过氧化氢将硫氰酸盐和溴化物氧化为各自的次卤酸。亚硝酸盐也是嗜酸性粒细胞过氧化物酶的一种底物。我们研究了该酶氧化亚硝酸盐的机制。亚硝酸盐在抑制次硫氰酸(“氰亚磺酸”)和次溴酸生成方面非常有效。光谱研究表明,亚硝酸盐将该酶还原为其化合物II形式,这是一种在血红素活性位点含有Fe(IV)的氧化还原中间体。化合物II不会氧化硫氰酸盐或溴化物。这些结果表明,亚硝酸盐很容易被活性位点含有Fe(V)的化合物I氧化。然而,它与化合物II的反应较慢。亚硝酸盐还原化合物II的观测速率常数被确定为5.6×10³ M⁻¹×s⁻¹。嗜酸性粒细胞在促进七肽硝化方面比中性粒细胞至少有效4倍。我们的这一发现解释了这一结果,即亚硝酸盐与嗜酸性粒细胞过氧化物酶的化合物II反应的速度比与髓过氧化物酶的类似氧化还原中间体快10倍。超氧化物歧化酶使嗜酸性粒细胞的硝化作用增加了3倍,这表明超氧化物会干扰硝化作用。我们提出,在嗜酸性粒细胞炎症部位,低浓度的亚硝酸盐会抑制嗜酸性粒细胞过氧化物酶产生氧化剂,而在较高浓度下,二氧化氮将是这些细胞形成的主要氧化剂。超氧化物与二氧化氮的扩散控制反应将降低蛋白质硝化的效率。