首页> 美国卫生研究院文献>Translational Psychiatry >Klotho: a humeral mediator in CSF and plasma that influences longevity and susceptibility to multiple complex disorders including depression
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Klotho: a humeral mediator in CSF and plasma that influences longevity and susceptibility to multiple complex disorders including depression

机译:Klotho:CSF和血浆中的肱骨介质影响寿命和对多种复杂疾病(包括抑郁症)的敏感性

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摘要

Klotho is a hormone secreted into human cerebrospinal fluid (CSF), plasma and urine that promotes longevity and influences the onset of several premature senescent phenotypes in mice and humans, including atherosclerosis, cardiovascular disease, stroke and osteoporosis. Preliminary studies also suggest that Klotho possesses tumor suppressor properties. Klotho's roles in these phenomena were first suggested by studies demonstrating that a defect in the Klotho gene in mice results in a significant decrease in lifespan. The Klotho-deficient mouse dies prematurely at 8–9 weeks of age. At 4–5 weeks of age, a syndrome resembling human ageing emerges consisting of atherosclerosis, osteoporosis, cognitive disturbances and alterations of hippocampal architecture. Several deficits in Klotho-deficient mice are likely to contribute to these phenomena. These include an inability to defend against oxidative stress in the central nervous system and periphery, decreased capacity to generate nitric oxide to sustain normal endothelial reactivity, defective Klotho-related mediation of glycosylation and ion channel regulation, increased insulin/insulin-like growth factor signaling and a disturbed calcium and phosphate homeostasis accompanied by altered vitamin D levels and ectopic calcification. Identifying the mechanisms by which Klotho influences multiple important pathways is an emerging field in human biology that will contribute significantly to understanding basic physiologic processes and targets for the treatment of complex diseases. Because many of the phenomena seen in Klotho-deficient mice occur in depressive illness, major depression and bipolar disorder represent illnesses potentially associated with Klotho dysregulation. Klotho's presence in CSF, blood and urine should facilitate its study in clinical populations.
机译:Klotho是一种分泌到人脑脊液(CSF),血浆和尿液中的激素,可延长寿命并影响小鼠和人体内几种早衰表型的发作,包括动脉粥样硬化,心血管疾病,中风和骨质疏松症。初步研究还表明,Klotho具有抑癌特性。研究表明,老鼠体内Klotho基因的缺陷会导致寿命的显着降低,这首先表明了Klotho在这些现象中的作用。 Klotho缺陷小鼠在8–9周龄时过早死亡。在4-5周龄时,出现一种类似于人类衰老的综合征,包括动脉粥样硬化,骨质疏松,认知障碍和海马结构改变。 Klotho缺陷小鼠中的一些缺陷可能是造成这些现象的原因。这些包括无法抵抗中枢神经系统和周围神经系统的氧化应激,降低产生一氧化氮的能力以维持正常的内皮反应性,糖基化和离子通道调节的Klotho相关介导缺陷,胰岛素/胰岛素样生长因子信号增强以及钙和磷稳态的紊乱,并伴有维生素D水平和异位钙化的改变。识别Klotho影响多种重要途径的机制是人类生物学中的一个新兴领域,它将为理解基本的生理过程和复杂疾病的治疗目标做出重要贡献。因为在Klotho缺陷小鼠中发现的许多现象都发生在抑郁症中,所以严重的抑郁症和躁郁症代表了与Klotho失调相关的潜在疾病。 Klotho在脑脊液,血液和尿液中的存在应有助于其在临床人群中的研究。

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