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偏头痛患者 S100B 和神经元特异性烯醇化酶水平升高:是否存在神经退行性变的证据?

Elevated S100B and neuron specific enolase levels in patients with migraine-without aura: evidence for neurodegeneration?

机构信息

Department of Neurology, Medical Faculty, Akdeniz University, 07070, Antalya, Turkey.

出版信息

Cell Mol Neurobiol. 2011 May;31(4):579-85. doi: 10.1007/s10571-011-9651-z. Epub 2011 Feb 4.

Abstract

Although migraine has mainly been considered as a benign disease, there is cumulative evidence of silent changes in the brain, brainstem, or cerebellum and subtle subclinical cerebellar dysfunction. In this study, in order to investigate a possible neuronal and/or glial damage at the cellular level in migraine, we measured and compared serum levels of S100B which is a protein marker of glial damage or activation, and neuron specific enolase (NSE) which is a marker of neuronal damage, in migraine patients and control subjects. Serum levels of S100B and NSE were measured in blood samples from 41 patients with migraine-without aura taken during a migraine attack (ictal) and in the attack-free period between migraine attacks (interictal) and 35 age- and sex-matched controls. Patients with migraine-without aura had significantly higher ictal serum levels of S100B and NSE (P < 0.05, for both) than control subjects; whereas in the interictal phase, there was a significant increment only in S100B levels (P < 0.05) compared to controls. On the other hand, serum levels of S100B and NSE in ictal and interictal blood samples did not differ significantly. The findings of increased ictal serum S100B and NSE levels together with increased interictal levels of S100B suggested that migraine might be associated with glial and/or neuronal damage in the brain and a prolonged disruption of blood-brain barrier. Increased interictal serum levels of S100B might point out to an insidious and slow damaging process in migraine patients.

摘要

尽管偏头痛主要被认为是一种良性疾病,但有越来越多的证据表明,大脑、脑干或小脑会发生无声的变化,以及细微的亚临床小脑功能障碍。在这项研究中,为了研究偏头痛患者在细胞水平上是否存在神经元和/或神经胶质损伤,我们测量并比较了偏头痛患者和对照组患者发作期(痉挛期)和无发作期(间歇期)血清中 S100B(一种神经胶质损伤或激活的蛋白标志物)和神经元特异性烯醇化酶(NSE)(一种神经元损伤标志物)的水平。从 41 例无先兆偏头痛患者的偏头痛发作期(痉挛期)和发作间期(间歇期)的血液样本中测量了血清 S100B 和 NSE 的水平,同时选取了 35 名年龄和性别匹配的对照者。与对照组相比,无先兆偏头痛患者的痉挛期血清 S100B 和 NSE 水平明显升高(均 P < 0.05);而在间歇期,S100B 水平明显升高(P < 0.05),与对照组相比。另一方面,痉挛期和间歇期血清 S100B 和 NSE 水平无明显差异。痉挛期血清 S100B 和 NSE 水平升高,以及间歇期 S100B 水平升高的发现表明,偏头痛可能与大脑中的神经胶质和/或神经元损伤以及血脑屏障的长期破坏有关。间歇期血清 S100B 水平升高可能表明偏头痛患者存在隐匿和缓慢的损伤过程。

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