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NADPH oxidase, Nramp1 and Nitric Oxide Synthase 2 in the host antimicrobial response

机译:NADPH氧化酶,Nramp1和一氧化氮合酶2在宿主中的抗菌反应

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Using highly conserved, complex enzyme system, leukocytes utilize the toxic nature of free radical intermediates, derived from oxygen and nitrogen, to control microbial pathogens as part of the innate immune response. Upon activation. NADPH oxidase generates superoxide anion radicals, which in turn give rise to further reactive oxygen intermediates. Similarly, activated nitric oxide synthase 2 catalyses the production of nitric oxide radicals, which leads to the formation of reactive nitrogen intermediates. Nitrogen- and and oxygen-centered reactive intermediates can interact to form further reactive species. In addition, presence of the cationic transporter, Nramp1, may exacerbate the effects of these toxic compounds on invading microbes. While each of these antimicrobial systems can operate independently, the combination of their activities is synergistic in the successful containment of almost all invading pathogens. These systems are activated and modulated by microbial products and a series of temporally expressed cytokines. They also feed directly into the initiation of the adaptive immune response, which culminates in lasting specific immunity. The effector molecules, generated in the early innate immune response, are not specific to the invading pathogen and may also cause damage to the host. It is the critical balance of these processes in the initial stages of infection that determines the outcome of infectious disease.
机译:使用高度保守的复杂酶系统,白细胞利用源自氧和氮的自由基中间体的毒性,来控制微生物病原体,作为先天免疫反应的一部分。激活后。 NADPH氧化酶产生超氧阴离子自由基,进而产生更多的活性氧中间体。类似地,活化的一氧化氮合酶2催化一氧化氮自由基的产生,这导致反应性氮中间体的形成。以氮和氧为中心的反应中间体可以相互作用形成其他反应物种。此外,阳离子转运蛋白Nramp1的存在可能会加剧这些有毒化合物对入侵微生物的影响。虽然这些抗菌系统中的每一个都可以独立运行,但它们的活性组合在成功遏制几乎所有入侵病原体方面具有协同作用。这些系统被微生物产物和一系列暂时表达的细胞因子激活和调节。它们还直接进入适应性免疫反应的开始,最终导致持久的特异性免疫。在先天先天免疫应答中产生的效应子分子对入侵的病原体不是特异性的,并且还可能对宿主造成损害。这些过程在感染初期的关键平衡决定了传染病的后果。

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