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首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >BDNF and serum S100B levels according the spectrum of structural pathology in chronic pain patients
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BDNF and serum S100B levels according the spectrum of structural pathology in chronic pain patients

机译:根据慢性疼痛患者的结构病理谱的BDNF和血清S100B水平

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Central sensitivity syndrome (CSS) consists of adaptive pathophysiological changes associated with neuroplasticity in some chronic pain disorders. It could be grouped in two main conceptual conditions: one includes those chronic pain patients without overt structural pathology such as fibromyalgia, and the other subgroup includes conditions with recognizable structural abnormalities, both somatic (osteoarthritis) and visceral (endometriosis). In order to understand the role of neuromodulators in GCS we aim to determine whether brain-derived neurotrophic factor (BDNF) and S100B are associated to specific chronic pain disorders. Serum BDNF and S100B were measured in chronic pain women with different diagnosis: 88 with osteoarthritis, 36 with endometriosis, 117 with fibromyalgia, 33 with chronic tension type headache and in 41 healthy controls. ANCOVA analysis followed by heteroscedasticity-consistent covariance matrix was performed to evaluate BDNF and S100B levels, adjusted for depression severity, pain levels and use of analgesics according different pathologies. Serum BDNF concentrations were higher and not different in patients with fibromyalgia and headache, the CSS group without structural pathology. In contrast, the concentrations of S100B were higher in patients with osteoarthritis and endometriosis, in comparison to controls, fibromyalgia and tensional headache patients. This study supports the hypothesis that BDNF and S100B neuromodulators present different serum levels according to the background disease associated to the chronic pain. These have the potential to be studied as markers of active disease or treatment evolution.
机译:中央敏感性综合征(CSS)包括与一些慢性疼痛障碍中神经塑性相关的适应性病理生理学变化。它可以分为两个主要概念条件:其中包括那些没有明显结构病理学的慢性疼痛患者,如纤维肌痛,其他亚组包括具有可识别结构异常的条件,体细胞体(骨关节炎)和内膜病(子宫内膜异位症)。为了理解神经调节剂在GC的作用,我们的目的是确定脑衍生的神经营养因子(BDNF)和S100B是否与特异性慢性疼痛障碍相关联。血清BDNF和S100b在慢性疼痛女性中测量,慢性疼痛妇女不同诊断:88例骨关节炎,36例,子宫内膜异位症,117种纤维肌痛,33例,慢性张力型头痛和41例健康对照。 ancova分析随后进行异源性 - 一致的协方差基质,进行评估BDNF和S100b水平,调整抑郁严重程度,疼痛水平和镇痛药的使用根据不同病理学。在没有结构病变的CSS组,血清BDNF浓度较高,患者患者没有差异。相反,与对照,纤维肌痛和严重头痛患者相比,骨关节炎和子宫内膜异位症患者的S100b浓度较高。该研究支持BDNF和S100B神经调节剂根据与慢性疼痛相关的背景疾病存在不同血清水平的假设。这些有可能被研究为有源疾病或治疗进化的标志物。

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