血清胶质纤维酸性蛋白可预测穿透性弹道式脑损伤后脑组织胶质纤维酸性蛋白降解产物及治疗效果。
Serum Glial Fibrillary Acidic Protein Predicts Tissue Glial Fibrillary Acidic Protein Break-Down Products and Therapeutic Efficacy after Penetrating Ballistic-Like Brain Injury.
作者信息
Boutté Angela M, Deng-Bryant Ying, Johnson David, Tortella Frank C, Dave Jitendra R, Shear Deborah A, Schmid Kara E
机构信息
Brain Trauma Neuroprotection and Neurorestoration Branch, Center for Military Psychiatry and Neuroscience, Walter Reed Army Institute of Research , Silver Spring, Maryland.
出版信息
J Neurotrauma. 2016 Jan 1;33(1):147-56. doi: 10.1089/neu.2014.3672. Epub 2015 Jun 8.
Acute traumatic brain injury (TBI) is associated with neurological dysfunction, changes in brain proteins, and increased serum biomarkers. However, the relationship between these brain proteins and serum biomarkers, and the ability of these serum biomarkers to indicate a neuroprotective/therapeutic response, remains elusive. Penetrating ballistic-like brain injury (PBBI) was used to systematically analyze several key TBI biomarkers, glial fibrillary acidic protein (GFAP) and its break-down products (BDPs)-ubiquitin C-terminal hydrolase-L1 (UCH-L1), α-II spectrin, and α-II spectrin BDPs (SBDPs)-in brain tissues and serum during an extended acute-subacute time-frame. In addition, neurological improvement and serum GFAP theranostic value was evaluated after neuroprotective treatment. In brain tissues, total GFAP increased more than three-fold 2 to 7 d after PBBI. However, this change was primarily due to GFAP-BDPs which increased to 2.7-4.8 arbitrary units (AU). Alpha-II spectrin was nearly ablated 3 d after PBBI, but somewhat recovered after 7 d. In conjunction with α-II spectrin loss, SBDP-145/150 increased approximately three-fold 2 to 7 d after PBBI (vs. sham, p<0.05). UCH-L1 protein levels were slightly decreased 7 d after PBBI but otherwise were unaffected. Serum GFAP was elevated by 3.2- to 8.8-fold at 2 to 4 h (vs. sham; p<0.05) and the 4 h increase was strongly correlated to 3 d GFAP-BDP abundance (r=0.66; p<0.05). Serum GFAP showed such a strong injury effect that it also was evaluated after therapeutic intervention with cyclosporin A (CsA). Administration of 2.5 mg/kg CsA significantly reduced serum GFAP elevation by 22.4-fold 2 h after PBBI (vs. PBBI+vehicle; p<0.05) and improved neurological function 1 d post-injury. Serum biomarkers, particularly GFAP, may be correlative tools of brain protein changes and feasible theranostic markers of TBI progression and recovery.
急性创伤性脑损伤(TBI)与神经功能障碍、脑蛋白变化及血清生物标志物升高有关。然而,这些脑蛋白与血清生物标志物之间的关系,以及这些血清生物标志物指示神经保护/治疗反应的能力,仍不清楚。采用贯穿性弹道样脑损伤(PBBI)在延长的急性-亚急性时间范围内,系统分析脑组织和血清中的几种关键TBI生物标志物,即胶质纤维酸性蛋白(GFAP)及其降解产物(BDPs)——泛素C末端水解酶-L1(UCH-L1)、α-II血影蛋白和α-II血影蛋白BDPs(SBDPs)。此外,在进行神经保护治疗后,评估神经功能改善情况及血清GFAP的诊疗价值。在脑组织中,PBBI后2至7天,总GFAP增加了三倍多。然而,这种变化主要是由于GFAP-BDPs增加到2.7 - 4.8任意单位(AU)。α-II血影蛋白在PBBI后3天几乎消失,但7天后有所恢复。与α-II血影蛋白丢失同时发生的是,PBBI后2至7天,SBDP-145/150增加了约三倍(与假手术组相比,p<0.05)。PBBI后7天,UCH-L1蛋白水平略有下降,但其他方面未受影响。血清GFAP在2至4小时时升高了3.2至8.8倍(与假手术组相比;p<0.05),4小时时的升高与3天的GFAP-BDP丰度密切相关(r=0.66;p<0.05)。血清GFAP显示出如此强烈的损伤效应,以至于在使用环孢素A(CsA)进行治疗干预后也对其进行了评估。给予2.5 mg/kg CsA可使PBBI后2小时血清GFAP升高显著降低22.4倍(与PBBI+赋形剂组相比;p<0.05)并改善损伤后1天的神经功能。血清生物标志物,尤其是GFAP,可能是脑蛋白变化的相关工具,也是TBI进展和恢复的可行诊疗标志物。
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