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Localization, Occurrence, and CSF Changes of SP-G, a New Surface Active Protein with Assumable Immunoregulatory Functions in the CNS

机译:SP-G的定位,发生和CSF变化,一种新的表面活性蛋白,CNS中具有明显的免疫调节功能

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Conventional surfactant proteins (A, B, C, and D) are important players of the innate immunity in the central nervous system and serve as effective regulators of cerebrospinal fluid rheology, probably being involved in clearance of detrimental metabolites like beta-amyloid and phospho-tau. Recently, a novel surfactant protein, SP-G, was described in kidneys and peripheral endocrine and exocrine glands. So far, its presence and possible functions in the central nervous system are unknown. Therefore, our study aimed to elucidate the presence of SP-G in the brain and its concentration in normal and pathologic samples of cerebrospinal fluid in order to gain first insight into its regulation and possible functions. A total of 121 samples of human cerebrospinal fluid (30 controls, 60 hydrocephalus patients, 7 central nervous system infections, and 24 brain hemorrhage patients) and 21 rat brains were included in our study. CSF samples were quantified using a commercially available ELISA system. Results were analyzed statistically using SPSS 22, performing Spearman Rho correlation and ANOVA with Dunnett's post hoc analysis. Rat brains were investigated via immunofluorescence to determine SP-G presence and colocalization with common markers like aquaporin-4, glial fibrillary acidic protein, platelet endothelial adhesion molecule 1, and neuronal nuclear antigen. SP-G occurs associated with brain vessels, comparable to other conventional SPs, and is present in a set of cortical neurons. SP-G is furthermore actively produced by ependymal and choroid plexus epithelium and secreted into the cerebrospinal fluid. Its concentrations are low in control subjects and patients suffering from aqueductal stenosis, higher in normal pressure hydrocephalus (p<0.01), and highest in infections of the central nervous system and brain hemorrhage (p<0.001). Interestingly, SP-G did correlate with total CSF protein in patients with CNS infections and hemorrhage, but not with cell count. Based on the changes in CSF levels of SP-G in hydrocephalus, brain hemorrhage, and CNS infections as well as its abundance at CSF flow-related anatomical structures closely associated with immunological barrier systems, importance for CSF rheology, brain waste clearance, and host defense is assumable. Thus, SP-G is a potential new CSF biomarker, possibly not only reflecting aspects of CNS innate immune responses, but also rheo-dynamically relevant changes of CSF composition, associated with CSF malabsorbtion. However, further studies are warranted to validate our findings and increase insight into the physiological importance of SP-G in the CNS.
机译:常规的表面活性剂蛋白(A,B,C和D)是中枢神经系统先天免疫的重要参与者,并用作脑脊液流变学的有效调节剂,可能参与β-淀粉样和磷酸盐等有害代谢物的清除TAU。最近,新型表面活性剂蛋白SP-G描述于肾脏和外周内分泌和外分泌腺中。到目前为止,其在中枢神经系统中的存在和可能的功能是未知的。因此,我们的研究旨在阐明大脑中Sp-g的存在及其在脑脊液的正常和病理样品中的浓度,以便首先洞察其调节和可能的功能。在我们的研究中,共有121个人脑脊液(30次对照,60例对照,60例,7例,中枢神经系统感染和24例脑出血患者)和21只大鼠大脑。使用市售的ELISA系统量化CSF样品。结果在统计上使用SPSS 22分析了SPEARMANT RHO相关性和ANOVA与Dunnett的后HOC分析。通过免疫荧光研究了大鼠血液,以确定SP-G存在和分致基质,普通标记物如水素-4,胶质纤维酸性蛋白,血小板内皮粘附分子1和神经元核抗原等常见标记。 SP-G与脑血管相关,与其他常规SPS相当,并且存在于一组皮质神经元中。此外,SP-G通过外膜和脉络膜上皮积极地产生并分泌到脑脊液中。其浓度在对照受试者和患者患有渡槽狭窄的患者中,正常压力脑积水(P <0.01),中枢神经系统和脑出血的感染最高(P <0.001)。有趣的是,SP-G与CNS感染和出血的患者中的总CSF蛋白质相关,但没有细胞计数。基于脑积水,脑出血和CNS感染中SP-G的CSF水平的变化以及与免疫屏障系统密切相关的CSF流动相关解剖结构的丰度,CSF流变学,脑废隙和主持人的重要性防御是假设的。因此,SP-G是潜在的新CSF生物标志物,可能不仅反映了CNS先天免疫应答的方面,而且还反映了与CSF MalabsorBTION相关的CSF组合物的RHEO-动态相关变化。然而,有必要进一步研究来验证我们的调查结果并增加对CNS中SP-G的生理重要性的洞察力。

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