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神经营养蛋白S100B:作为脑损伤标志物的价值及可能的治疗意义。

The neurotrophic protein S100B: value as a marker of brain damage and possible therapeutic implications.

作者信息

Kleindienst Andrea, Hesse Felicitas, Bullock M Ross, Buchfelder Michael

机构信息

Department of Neurosurgery, Friedrich-Alexander-University, Erlangen-Nuremberg, Germany.

出版信息

Prog Brain Res. 2007;161:317-25. doi: 10.1016/S0079-6123(06)61022-4.

Abstract

We provide a critical analysis of the value of S100B as a marker of brain damage and possible therapeutic implications. The early assessment of the injury severity and the consequent prognosis are of major concern for physicians treating patients suffering from traumatic brain injury (TBI). A reliable indicator to accurately determine the extent of the brain damage has to meet certain requirements: (i) to originate in the central nervous system (CNS) with no contribution from extracerebral sources; (ii) a passive release from damaged neurons and/or glial cells without any stimulated active release; (iii) a lack of specific effects on neurons and/or glial cells interfering with the initial injury; (iv) an unlimited passage through the blood-brain barrier (BBB). The measurement of putative biochemical markers, such as the S100B protein, has been proposed in this role. Over the past decade, numerous studies have reported a positive correlation of S100B serum levels with a poor outcome following TBI. However, some studies raise doubt whether the serum measurement of S100B is a valid biochemical marker of brain damage. We summarize the specific properties of S100B and analyze whether they support or counteract the necessary requirements to designate this protein as an indicator of brain damage. Finally, we report recent experimental findings suggesting a possible therapeutic potential of S100B.

摘要

我们对S100B作为脑损伤标志物的价值及可能的治疗意义进行了批判性分析。对于治疗创伤性脑损伤(TBI)患者的医生来说,早期评估损伤严重程度及随之而来的预后是主要关注点。一个能准确确定脑损伤程度的可靠指标必须满足某些要求:(i)起源于中枢神经系统(CNS),无来自脑外来源的影响;(ii)从受损神经元和/或胶质细胞被动释放,无任何刺激后的主动释放;(iii)对神经元和/或胶质细胞无特异性影响,不干扰初始损伤;(iv)能无限通过血脑屏障(BBB)。有人提出测量诸如S100B蛋白等假定的生化标志物可发挥这一作用。在过去十年中,众多研究报告了TBI后S100B血清水平与不良预后呈正相关。然而,一些研究对S100B的血清测量是否为脑损伤的有效生化标志物提出了质疑。我们总结了S100B的具体特性,并分析它们是支持还是抵消了将该蛋白指定为脑损伤指标的必要要求。最后,我们报告了最近的实验结果,提示S100B可能具有治疗潜力。

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