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人脑脊液中地西泮结合抑制剂样免疫反应性(DBI-LI)。与神经系统疾病的相关性。

Diazepam binding inhibitor-like immunoreactivity (DBI-LI) in human CSF. Correlations with neurological disorders.

作者信息

Ferrero P, Benna P, Costa P, Tarenzi L, Baggio G, Bergamasco B, Bergamini L

机构信息

Department of Neurology, University of Turin, Italy.

出版信息

J Neurol Sci. 1988 Nov;87(2-3):327-49. doi: 10.1016/0022-510x(88)90257-2.

Abstract

Cerebrospinal fluid (CSF) levels of the anxiogenic neuropeptide diazepam binding inhibitor (DBI) were determined by radioimmunoassay in 281 patients who underwent evaluation for neurological problems. Serial dilution curves and reverse-phase high pressure liquid chromatography showed that the immunoreactive material in CSF behaved just as authentic DBI extracted from human brain. Furthermore in the assay there was no evidence of interference from CSF samples deprived of DBI by immunoaffinity. In 82 patients with no evidence of major lesions in the central nervous system, who acted as controls, the CSF DBI content was shown to be age- and sex-related. No correlation was observed with the CSF protein concentration. In patients with different types of dementia, the levels of CSF DBI were significantly increased in a group with normal pressure hydrocephalus. No significant differences were found between Alzheimer's disease, multi-infarct dementia, or dementia with Parkinson's disease and controls. In non-demented patients with Parkinson's disease the levels of DBI were increased in a subgroup with depressive disturbances whereas no differences was observed in the non-depressed cases. The content of DBI was markedly reduced in 5 cases with olivopontocerebellar atrophy and in 4 with spinocerebellar ataxia. In all the other disorders studied the levels of DBI were similar to or slightly lower (multiple sclerosis) than those of the controls. The origin of DBI in cerebrospinal fluid is uncertain; a number of various possibilities are discussed concerning the proposed role of DBI as modulator of brain GABAergic transmission.

摘要

采用放射免疫分析法测定了281例接受神经系统问题评估患者的脑脊液中致焦虑神经肽地西泮结合抑制剂(DBI)的水平。系列稀释曲线和反相高压液相色谱显示,脑脊液中的免疫反应性物质与从人脑提取的 authentic DBI 的行为一致。此外,在该检测中,没有证据表明免疫亲和去除DBI的脑脊液样本存在干扰。在82例无中枢神经系统重大病变证据的患者(作为对照)中,脑脊液DBI含量显示与年龄和性别相关。未观察到与脑脊液蛋白浓度的相关性。在不同类型痴呆患者中,正常压力脑积水组的脑脊液DBI水平显著升高。阿尔茨海默病、多发性梗死性痴呆或帕金森病痴呆患者与对照组之间未发现显著差异。在非痴呆帕金森病患者中,抑郁障碍亚组的DBI水平升高,而未抑郁患者未观察到差异。5例橄榄桥脑小脑萎缩患者和4例脊髓小脑共济失调患者的DBI含量明显降低。在所有其他研究的疾病中,DBI水平与对照组相似或略低(多发性硬化症)。脑脊液中DBI的来源尚不确定;关于DBI作为脑γ-氨基丁酸能传递调节剂的拟议作用,讨论了多种可能性。

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