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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Pre-conditioning with Remote Photobiomodulation Modulates the Brain Transcriptome and Protects Against MPTP Insult in Mice
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Pre-conditioning with Remote Photobiomodulation Modulates the Brain Transcriptome and Protects Against MPTP Insult in Mice

机译:具有远程光致调节的预调节调节脑转录组,并防止小鼠的MPTP损伤

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Transcranial photobiomodulation (PBM), which involves the application of low-intensity red to near-infrared light (600-1100 nm) to the head, provides neuroprotection in animal models of various neurodegenerative diseases. However, the absorption of light energy by the human scalp and skull may limit the utility of transcranial PBM in clinical contexts. We have previously shown that targeting light at peripheral tissues (i.e. "remote PBM") also provides protection of the brain in an MPTP mouse model of Parkinson's disease, suggesting remote PBM might be a viable alternative strategy for overcoming penetration issues associated with transcranial PBM. This present study aimed to determine an effective pre-conditioning regimen of remote PBM for inducing neuroprotection and elucidate the molecular mechanisms by which remote PBM enhances the resilience of brain tissue. Balb/c mice were irradiated with 670-nm light (4 J/cm(2) per day) targeting dorsum and hindlimbs for 2, 5 or 10 days, followed by injection of the parkinsonian neurotoxin MPTP (50 mg/kg) over two consecutive days. Despite no direct irradiation of the head, 10 days of pre-conditioning with remote PBM significantly attenuated MPTP-induced loss of midbrain tyrosine hydroxylase-positive dopaminergic cells and mitigated the increase in FOS-positive neurons in the caudate-putamen complex. Interrogation of the midbrain transcriptome by RNA microarray and pathway enrichment analysis suggested upregulation of cell signaling and migration (including CXCR4(+) stem cell and adipocytokine signaling), oxidative stress response pathways and modulation of the blood-brain barrier following remote PBM. These findings establish remote PBM preconditioning as a viable neuroprotective intervention and provide insights into the mechanisms underlying this phenomenon. (C) 2019 IBRO. Published by Elsevier Ltd. All rights reserved.
机译:涉及将低强度红色施加到近红外光(600-1100nm)到头部的颅颅光学调节(PBM),为各种神经变性疾病的动物模型提供神经保护。然而,人头皮和颅骨吸收光能可以限制临床环境中经颅PBM的效用。我们之前已经表明,在外周组织(即“偏远PBM”)下靶向光线,也为帕金森病的MPTP小鼠模型中的大脑提供了保护,旨在为克服与经颅PBM相关的渗透问题是可行的替代策略。本研究旨在确定用于诱导神经保护的远程PBM的有效预调节方案,并阐明远程PBM增强脑组织的弹性的分子机制。用670纳米灯(每天4J / cm(2))照射BALB / C小鼠,靶向背部和2,5或10天,然后注射帕金森尼神经毒素MPTP(50mg / kg)超过两个连续多日。尽管头部没有直接照射,但远程PBM预调节10天显着减弱MPTP诱导的中脑羟化羟化酶阳性多巴胺能细胞的丧失,并减轻了浮石复合物中的FOS阳性神经元的增加。通过RNA微阵列和途径富集分析的中脑转录组的询问提出了细胞信号传导和迁移的上调(包括CXCR4(+)干细胞和脂肪蛋白信号传导),偏远PBM后氧化应激响应途径和血脑屏障的调节。这些发现建立了远程PBM预处理作为一种可行的神经保护干预,并向这一现象的基础提供了洞察力。 (c)2019年IBRO。 elsevier有限公司出版。保留所有权利。

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