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组胺和肌肽氯胺分子间及分子内快速氯转移反应的证据:对预防次氯酸介导损伤的意义。

Evidence for rapid inter- and intramolecular chlorine transfer reactions of histamine and carnosine chloramines: implications for the prevention of hypochlorous-acid-mediated damage.

作者信息

Pattison David I, Davies Michael J

机构信息

The Heart Research Institute, 114 Pyrmont Bridge Road, Camperdown, Sydney, New South Wales 2050, Australia.

出版信息

Biochemistry. 2006 Jul 4;45(26):8152-62. doi: 10.1021/bi060348s.

Abstract

Hypochlorous acid (HOCl) is a powerful oxidant generated from H(2)O(2) and Cl(-) by the heme enzyme myeloperoxidase, which is released from activated leukocytes. HOCl possesses potent antibacterial properties, but excessive production can lead to host tissue damage that is implicated in a wide range of human diseases (e.g., atherosclerosis). Histamine and carnosine have been proposed as protective agents against such damage. However, as recent studies have shown that histidine-containing compounds readily form imidazole chloramines that can rapidly chlorinate other targets, it was hypothesized that similar reactions may occur with histamine and carnosine, leading to propagation, rather than prevention, of HOCl-mediated damage. In this study, the reactions of HOCl with histamine, histidine, carnosine, and other compounds containing imidazole and free amine sites were examined. In all cases, rapid formation (k, 1.6 x 10(5) M(-)(1) s(-)(1)) of imidazole chloramines was observed, followed by chlorine transfer to yield more stable, primary chloramines (R-NHCl). The rates of most of these secondary reactions are dependent upon substrate concentrations, consistent with intermolecular mechanisms (k, 10(3)-10(4) M(-)(1) s(-)(1)). However, for carnosine, the imidazole chloramine transfer rates are independent of the concentration, indicative of intramolecular processes (k, 0.6 s(-)(1)). High-performance liquid chromatography studies show that in all cases the resultant R-NHCl species can slowly chlorinate N-alpha-acetyl-Tyr. Thus, the current data indicate that the chloramines formed on the imidazole and free amine groups of these compounds can oxidize other target molecules but with limited efficiency, suggesting that histamine and particularly carnosine may be able to limit HOCl-mediated oxidation in vivo.

摘要

次氯酸(HOCl)是一种由血红素酶髓过氧化物酶催化H₂O₂和Cl⁻生成的强氧化剂,髓过氧化物酶由活化的白细胞释放。HOCl具有强大的抗菌特性,但过量产生会导致宿主组织损伤,这与多种人类疾病(如动脉粥样硬化)有关。组胺和肌肽已被提出作为针对此类损伤的保护剂。然而,最近的研究表明,含组氨酸的化合物容易形成咪唑氯胺,后者可迅速氯化其他靶点,因此推测组胺和肌肽可能会发生类似反应,导致HOCl介导的损伤扩散而非预防。在本研究中,检测了HOCl与组胺、组氨酸、肌肽以及其他含有咪唑和游离胺位点的化合物的反应。在所有情况下,均观察到咪唑氯胺的快速形成(k,1.6×10⁵ M⁻¹ s⁻¹),随后发生氯转移以生成更稳定的一级氯胺(R-NHCl)。这些二级反应中的大多数速率取决于底物浓度,这与分子间机制一致(k,10³ - 10⁴ M⁻¹ s⁻¹)。然而,对于肌肽,咪唑氯胺的转移速率与浓度无关,表明是分子内过程(k,0.6 s⁻¹)。高效液相色谱研究表明,在所有情况下,生成的R-NHCl物种可缓慢氯化N-α-乙酰酪氨酸。因此,目前的数据表明,这些化合物的咪唑和游离胺基团上形成的氯胺可氧化其他靶分子,但效率有限,这表明组胺尤其是肌肽可能能够在体内限制HOCl介导的氧化。

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