首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Endotoxin-mediated regulation of nuclear factor-kappaB nuclear translocation and activation in the hippocampus of the central nervous system: modulation by intracerebroventricular treatment with thymulin and the immunomodulatory role of the IkappaB-alpha/pIkappaB-alpha pathway.
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Endotoxin-mediated regulation of nuclear factor-kappaB nuclear translocation and activation in the hippocampus of the central nervous system: modulation by intracerebroventricular treatment with thymulin and the immunomodulatory role of the IkappaB-alpha/pIkappaB-alpha pathway.

机译:内毒素介导的中枢神经系统海马中核因子-κB核转运和激活的调节:胸腺素通过脑室内处理进行调节,以及IkappaB-alpha / pIkappaB-alpha途径的免疫调节作用。

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摘要

The transcription factor nuclear factor kappaB (NF-kappaB) is one member of a ubiquitously expressed family of Rel-related transcription factors that serve as critical regulators of many proinflammatory genes and immunomodulators. Nevertheless, the immunomodulatory potential of thymulin and its effect on NF-kappaB in vivo, and particularly in the central nervous system (CNS), is not well characterized. In this study, the role of endotoxin (ET/LPS) in regulating NF-kappaB was deciphered in various compartments of the CNS. Stereotaxic localization reverberated specific intracerebroventricular (ICV) injection of ET into the CNS, with or without pretreatment with ICV thymulin. Treatment with ET (1 microg for 45 min; ICV) upregulated the expression and nuclear localization of NF-kappaB(1) (p50), NF-kappaB(2) (p52), RelA (p65), RelB (p68) and c-Rel (p75) in the hippocampus (HC), an effect abrogated, in a dose-dependent manner, by ICV pretreatment (30 min) with thymulin. Thymulin modulated the phosphorylation of IkappaB-alpha in the HC by upregulating the cytosolic accumulation of IkappaB-alpha and downregulating its phosphorylation (pIkappaB-alpha). Further analysis of the DNA-binding activity revealed an upregulated activity in the HC relative to saline-constitutive expression of the RelA (p65) subunit, the specificity of which was determined by a mutant oligonucleotide of RelA and a cold, non-specific competitor. ET did not induce the DNA-binding activity of NF-kappaB in the diencephalon (DE) or substantia nigra (SN) at various time points, when compared with baseline levels of expression. Intraperitoneal (IP) injections of ET (25 microg for 15 min) in vivo upregulated the expression of NF-kappaB subunits in the liver and reduced the cytosolic accumulation of IkappaB-alpha by inducing pIkappaB-alpha. Furthermore, IP pretreatment with thymulin followed by ICV injection of ET attenuated and reduced the DNA-binding activity of NF-kappaB in the HC. These results indicate that ICV injection of ET regulates the nuclear translocation and activation of NF-kappaB subunits within specific compartments in the brain, an effect particularly localized to the hippocampus. Additionally, thymulin attenuated the ET-induced response, with particular involvement of the transduction pathway implicating IkappaB-alpha, the major cytosolic inhibitor of NF-kappaB. The in vivo molecular regulation of thymulin via the NF-kappaB pathway is critical to understanding the alleviating anti-inflammatory role of this nonapeptide and paving the way to unraveling pathways associated with neuroimmune interactions mediating proinflammatory signals in the CNS.
机译:转录因子核因子κB(NF-kappaB)是普遍表达的Rel相关转录因子家族的成员之一,Rel相关转录因子充当许多促炎基因和免疫调节剂的关键调节剂。然而,在体内,特别是在中枢神经系统(CNS)中,胸腺素的免疫调节潜能及其对NF-κB的作用尚未得到很好的表征。在这项研究中,在中枢神经系统的各个区室中破译了内毒素(ET / LPS)在调节NF-κB中的作用。立体定向定位可以将ET特定的脑室内(ICV)注射到CNS中,无论是否经过ICV胸腺素预处理。 ET(1 microg持续45分钟; ICV)处理可上调NF-kappaB(1)(p50),NF-kappaB(2)(p52),RelA(p65),RelB(p68)和c的表达和核定位-海马(HC)中的Rel(p75),这种作用通过剂量依赖性的百里香素ICV预处理(30分钟)而消失。 Thymulin通过上调IkappaB-alpha的胞质积累并下调其磷酸化(pIkappaB-alpha)来调节HC中IkappaB-alpha的磷酸化。 DNA结合活性的进一步分析显示,相对于RelA(p65)亚基的盐水组成型表达,HC中的活性上调,其特异性由RelA的突变寡核苷酸和冷的非特异性竞争者确定。与基线表达水平相比,ET在不同时间点均未诱导二脑(DE)或黑质(SN)中NF-κB的DNA结合活性。体内腹膜内(IP)注射ET(25微克,持续15分钟)通过诱导pIkappaB-α上调了肝脏中NF-kappaB亚基的表达,并减少了IkappaB-α的胞质积累。此外,用百里香素进行IP预处理,然后用ICV注射ET可以减弱并降低HC中NF-κB的DNA结合活性。这些结果表明,ICV注射ET调节了大脑特定隔室内的核易位和NF-κB亚基的激活,这种作用特别局限在海马体中。此外,百里香素减弱了ET诱导的反应,尤其是涉及NF-κB的主要胞质抑制剂IkappaB-α的转导途径。胸腺素通过NF-κB途径的体内分子调节对于理解这种九肽的抗炎作用以及为揭示与中枢神经系统中介导促炎信号的神经免疫相互作用相关的途径铺平道路至关重要。

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