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Roles of DUOX-mediated hydrogen peroxide in metabolism, host defense, and signaling

机译:DUOX介导的过氧化氢在代谢,宿主防御和信号传导中的作用

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Significance: Among the NADPH oxidases, the dual oxidases, DUOX1 and DUOX2, constitute a distinct subfamily initially called thyroid oxidases, based on their high level of expression in thyroid tissue. Genetic alterations causing inherited hypothyroidism clearly demonstrate their physiological implication in thyroid hormonogenesis. However, a growing list of biological functions triggered by DUOX-dependent reactive oxygen species (ROS) in highly differentiated mucosae have recently emerged. Recent Advances: A role of DUOX enzymes as ROS providers for lactoperoxidase-mediated killing of invading pathogens has been well established and a role in bacteria chemorepulsion has been proposed. Control of DUOX expression and activity by inflammatory molecules and immune receptor activation consolidates their contributions to innate immune defense of mucosal surfaces. Recent studies conducted in ancestral organisms have identified effectors of DUOX redox signaling involved in wound healing including epithelium regeneration and leukocyte recruitment. Moreover, local generation of hydrogen peroxide (H2O2) by DUOX has also been suggested to constitute a positive feedback loop to promote receptor signaling activation. Critical Issues: A correct balance between H 2O2 generation and detoxification mechanisms must be properly maintained to avoid oxidative damages. Overexpression of DUOX genes has been associated with an increasing number of chronic inflammatory diseases. Furthermore, H2O2-mediated DNA damage supports a mutagenic function promoting tumor development. Future Directions: Despite the high sequence similarity shared between DUOX1 and DUOX2, the two isoforms present distinct regulations, tissue expression and catalytic functions. The phenotypic characterization of novel DUOX/DUOXA invalidated animal models will be very useful for defining their medical importance in pathological conditions. Antioxid. Redox Signal. 20, 2776-2793.
机译:意义:在NADPH氧化酶中,双重氧化酶DUOX1和DUOX2构成了一个独特的亚科,最初被称为甲状腺氧化酶,因为它们在甲状腺组织中的表达水平很高。引起遗传性甲状腺功能减退的遗传改变清楚地表明了它们在甲状腺激素生成中的生理意义。然而,近来出现了由高度分化的粘膜中由DUOX依赖性活性氧(ROS)触发的生物学功能的日益增长的清单。最新进展:DUOX酶作为ROS提供者在乳过氧化物酶介导的入侵病原体杀灭中的作用已得到充分确立,并已提出了在细菌化学趋化作用中的作用。通过炎症分子和免疫受体激活控制DUOX的表达和活性,巩固了它们对粘膜表面固有免疫防御的作用。在祖先生物中进行的最新研究已经确定了DUOX氧化还原信号传导的效应因子,涉及伤口愈合,包括上皮再生和白细胞募集。此外,还建议由DUOX局部产生过氧化氢(H2O2)构成一个正反馈回路,以促进受体信号激活。关键问题:必须适当地维持H 2O2产生和排毒机制之间的正确平衡,以避免氧化损害。 DUOX基因的过表达与越来越多的慢性炎症疾病有关。此外,H2O2介导的DNA损伤支持促进肿瘤发展的诱变功能。未来方向:尽管DUOX1和DUOX2之间具有高度的序列相似性,但这两种同工型仍具有不同的调控,组织表达和催化功能。新型DUOX / DUOXA无效动物模型的表型表征对于定义其在病理条件下的医学重要性将非常有用。抗氧化。氧化还原信号。 20,2776-2793。

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