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首页> 外文期刊>CNS neuroscience & therapeutics. >Pleiotropic Role of PPAR iγ/i in Intracerebral Hemorrhage: An Intricate System Involving Nrf2, RXR , and NF ‐iκ/iB
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Pleiotropic Role of PPAR iγ/i in Intracerebral Hemorrhage: An Intricate System Involving Nrf2, RXR , and NF ‐iκ/iB

机译:PPAR γ在脑出血中的多效性作用:涉及Nrf2,RXR和NF ‐i B的复杂系统

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Summary Intracerebral hemorrhage ( ICH ) is a subtype of stroke involving formation of hematoma within brain parenchyma, which accounts for 8–15% of all strokes in Western societies and 20–30% among Asian populations, and has a 1‐year mortality rate 50%. The high mortality and severe morbidity make ICH a major public health problem. Only a few evidence‐based targeted treatments are used for ICH management, and interventions focus primarily on supportive care and comorbidity prevention. Even in patients who survive the ictus, extravasated blood (including plasma components) and subsequent intrahematoma hemolytic products trigger a series of adverse events within the brain parenchyma, leading to secondary brain injury, edema and severe neurological deficits or death. Although the hematoma in humans gradually resolves within months, full restoration of neurological function can be slow and often incomplete, leaving survivors with devastating neurological deficits. During past years, peroxisome proliferator‐activated receptor gamma ( PPAR γ ) transcription factor and its agonists received recognition as important players in regulating not only glucose and lipid metabolism (which underlies its therapeutic effect in type 2 diabetes mellitus), and more recently, as an instrumental pleiotropic regulator of antiinflammation, antioxidative regulation, and phagocyte‐mediated cleanup processes. PPAR γ agonists have emerged as potential therapeutic target for stroke. The use of PPAR γ as a therapeutic target appears to have particularly strong compatibility toward pathogenic components of ICH . In addition to its direct genomic effect, PPAR γ may interact with transcription factor, NF ‐ κ B, which may underlie many aspects of the antiinflammatory effect of PPAR γ . Furthermore, PPAR γ appears to regulate expression of Nrf2, another transcription factor and master regulator of detoxification and antioxidative regulation. Finally, the synergistic costimulation of PPAR γ and retinoid X receptor, RXR , may play an additional role in the therapeutic modulation of PPAR γ function. In this article, we outline the main components of the role of PPAR γ in ICH pathogenesis.
机译:总结脑出血是脑实质内涉及血肿形成的中风的一种亚型,在西方社会占所有中风的8-15%,在亚洲人口中占20-30%,其一年死亡率> 50%。高死亡率和严重的发病率使ICH成为主要的公共卫生问题。仅少数基于证据的靶向治疗用于ICH治疗,干预措施主要集中在支持治疗和合并症的预防上。即使在存活的患者中,渗出的血液(包括血浆成分)和随后的血肿内溶血产物也会在脑实质内引发一系列不良事件,导致继发性脑损伤,水肿和严重的神经功能缺损或死亡。尽管人类的血肿可在数月内逐渐消退,但神经功能的完全恢复可能很缓慢,而且常常不完全,从而使幸存者遭受毁灭性的​​神经功能缺陷。在过去的几年中,过氧化物酶体增殖物激活受体γ(PPARγ)转录因子及其激动剂不仅在调节葡萄糖和脂质代谢(这是其对2型糖尿病的治疗作用的基础)上,而且在调节糖代谢方面起着重要的作用。一种抗炎,抗氧化调节和吞噬细胞介导的清除过程的仪器多效性调节剂。 PPARγ激动剂已成为中风的潜在治疗靶标。使用PPARγ作为治疗靶点似乎对ICH的致病成分具有特别强的相容性。除了直接的基因组效应外,PPARγ还可能与转录因子NFκB相互作用,这可能是PPARγ抗炎作用的许多方面的基础。此外,PPARγ似乎调节Nrf2的表达,Nrf2是另一种转录因子,是排毒和抗氧化调节的主要调节剂。最后,PPARγ和类维生素X受体RXR的协同协同刺激可能在PPARγ功能的治疗性调节中起额外作用。在本文中,我们概述了PPARγ在ICH发病机理中的主要作用。

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