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首页> 外文期刊>Oxidative Medicine and Cellular Longevity >Rh-CSF1 Attenuates Oxidative Stress and Neuronal Apoptosis via the CSF1R/PLCG2/PKA/UCP2 Signaling Pathway in a Rat Model of Neonatal HIE
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Rh-CSF1 Attenuates Oxidative Stress and Neuronal Apoptosis via the CSF1R/PLCG2/PKA/UCP2 Signaling Pathway in a Rat Model of Neonatal HIE

机译:RH-CSF1通过CSF1R / PLCG2 / PKA / UCP2信号传导途径衰减氧化应激和神经元细胞凋亡,在新生儿HIE的大鼠模型中

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Oxidative stress (OS) and neuronal apoptosis are major pathological processes after hypoxic-ischemic encephalopathy (HIE). Colony stimulating factor 1 (CSF1), binding to CSF1 receptor (CSF1R), has been shown to reduce neuronal loss after hypoxic-ischemia- (HI-) induced brain injury. In the present study, we hypothesized that CSF1 could alleviate OS-induced neuronal degeneration and apoptosis through the CSF1R/PLCG2/PKA/UCP2 signaling pathway in a rat model of HI. A total of 127 ten-day old Sprague Dawley rat pups were used. HI was induced by right common carotid artery ligation with subsequent exposure to hypoxia for 2.5?h. Exogenous recombinant human CSF1 (rh-CSF1) was administered intranasally at 1?h and 24?h after HI. The CSF1R inhibitor, BLZ945, or phospholipase C-gamma 2 (PLCG2) inhibitor, U73122, was injected intraperitoneally at 1?h before HI induction. Brain infarct volume measurement, cliff avoidance test, righting reflex test, double immunofluorescence staining, western blot assessment, 8-OHdG and MitoSOX staining, Fluoro-Jade C staining, and TUNEL staining were used. Our results indicated that the expressions of endogenous CSF1, CSF1R, p-CSF1R, p-PLCG2, p-PKA, and uncoupling protein2 (UCP2) were increased after HI. CSF1 and CSF1R were expressed in neurons and astrocytes. Rh-CSF1 treatment significantly attenuated neurological deficits, infarct volume, OS, neuronal apoptosis, and degeneration at 48?h after HI. Moreover, activation of CSF1R by rh-CSF1 significantly increased the brain tissue expressions of p-PLCG2, p-PKA, UCP2, and Bcl2/Bax ratio, but reduced the expression of cleaved caspase-3. The neuroprotective effects of rh-CSF1 were abolished by BLZ945 or U73122. These results suggested that rh-CSF1 treatment attenuated OS-induced neuronal degeneration and apoptosis after HI, at least in part, through the CSF1R/PLCG2/PKA/UCP2 signaling pathway. Rh-CSF1 may serve as therapeutic strategy against brain damage in patients with HIE.
机译:氧化应激(OS)和神经元凋亡是缺氧缺血性脑病(HIE)后的主要病理过程。已经证明了与CSF1受体(CSF1R)结合的菌落刺激因子1(CSF1),以减少缺氧缺血(HI-)诱导的脑损伤后的神经元损失。在本研究中,我们假设CSF1可以通过CSF1R / PLCG2 / PKA / UCP2信号传导途径缓解OS诱导的神经元变性和凋亡。共使用127个十天的Sprague Dawley大鼠幼犬。嗨,通过正确的颈动脉结扎诱导,随后暴露于缺氧2.5?h。外源性重组人CSF1(RH-CSF1)在HI后1℃和24℃鼻内施用。 CSF1R抑制剂,BLZ945或磷脂酶C-Gamma 2(PLCG2)抑制剂U73122在HI诱导之前在1〜H腹膜内注射。使用脑梗塞体积测量,悬崖避免试验,抗反射试验,双免疫荧光染色,蛋白质印迹评估,8-OHDG和MITOSOX染色,氟 - 玉染色和TUNEL染色。我们的结果表明,在HI之后增加了内源CSF1,CSF1,P-CSF1R,P-PLCG2,P-PKA和解偶联蛋白2(UCP2)的表达。 CSF1和CSF1R在神经元和星形胶质细胞中表达。 RH-CSF1治疗显着减弱了神经系统缺陷,梗塞体积,OS,神经元细胞凋亡,并在HI后48℃下变性。此外,通过RH-CSF1激活CSF1R显着增加了P-PLCG2,P-PKA,UCP2和BCL2 / BAX比的脑组织表达,但是降低了切割的Caspase-3的表达。 BLZ945或U73122废除了RH-CSF1的神经保护作用。这些结果表明Rh-CSF1治疗在HI,至少部分地通过CSF1R / PLCG2 / PKA / UCP2信号传导途径缓解OS诱导的OS诱导的神经元变性和细胞凋亡。 RH-CSF1可作为HIE患者脑损伤的治疗策略。

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