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Hydrogen Sulfide—Clues from Evolution and Implication for Neonatal Respiratory Diseases

机译:来自演化和新生儿呼吸疾病的硫化氢线索

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摘要

Reactive oxygen species (ROS) have been the focus of redox research in the realm of oxidative neonatal respiratory diseases such as bronchopulmonary dysplasia (BPD). Over the years, nitric oxide (NO) and carbon monoxide (CO) have been identified as important gaseous signaling molecules involved in modulating the redox homeostasis in the developing lung. While animal data targeting aspects of these redox pathways have been promising in treating and/or preventing experimental models of neonatal lung disease, none are particularly effective in human neonatal clinical trials. In recent years, hydrogen sulfide (H2S) has emerged as a novel gasotransmitter involved in a magnitude of cellular signaling pathways and functions. The importance of H2S signaling may lie in the fact that early life-forms evolved in a nearly anoxic, sulfur-rich environment and were dependent on H2S for energy. Recent studies have demonstrated an important role of H2S and its synthesizing enzymes in lung development, which normally takes place in a relatively hypoxic intrauterine environment. In this review, we look at clues from evolution and explore the important role that the H2S signaling pathway may play in oxidative neonatal respiratory diseases and discuss future opportunities to explore this phenomenon in the context of neonatal chronic lung disease.
机译:反应性氧(ROS)一直是氧化性新生儿呼吸疾病境界氧化还原研究的重点,如支气管扩漏患者(BPD)。多年来,已经鉴定了一氧化氮(NO)和一氧化碳(CO)作为在显影肺中调节氧化还原稳态的重要气态信号传导分子。虽然这些氧化还原途径的动物数据在治疗和/或预防新生儿肺病的实验模型方面一直很有前途,但在人类新生儿临床试验中没有特别有效。近年来,硫化氢(H2S)作为一种新的汽油转体,其涉及细胞信号传导途径和功能的大小。 H2S信号传导的重要性可能位于较早氧化,富含硫的环境中的早期生命形式,并依赖于能量的H2S。最近的研究表明H2S的重要作用及其在肺部发育中的合成酶,通常在相对缺氧的宫内环境中进行。在这篇综述中,我们从演化中看线索,探讨H2S信号通路可能在氧化新生儿呼吸系统疾病中发挥的重要作用,并讨论在新生儿慢性肺病的背景下探索这种现象的未来机会。

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