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首页> 外文期刊>Journal of Neuroimmunology: Official Bulletin of the Research Committee on Neuroimmunology of the World Federation of Neurology >Intercellular adhesion molecule-1 in cerebrospinal fluid--the evaluation of blood-derived and brain-derived fractions in neurological diseases.
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Intercellular adhesion molecule-1 in cerebrospinal fluid--the evaluation of blood-derived and brain-derived fractions in neurological diseases.

机译:脑脊液中的细胞间粘附分子-1-神经疾病中血液和脑源性成分的评估。

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摘要

The soluble intercellular adhesion molecule-1 (sICAM-1) was measured in paired CSF and serum samples from 128 patients with different neurological diseases. The reference range of blood-derived sICAM-1 fractions in CSF was characterized with reference to the albumin CSF/serum quotients. The low mean concentrations of sICAM-1 of normal controls (n=33) in CSF (1.5 ng/ml; C.V.=40%) compared to serum (285.1 ng/ml; C.V.=32%) indicate that about 60% to 80% of sICAM-1 in normal lumbar CSF derives from blood. This calculation is based on the theoretically expected molecular size-dependent blood-CSF gradient between 300:1 to 250:1. In patients with non-inflammatory diseases (n=21) the sICAM-1 CSF/serum quotient increased non-linearly with increasing albumin CSF/serum quotient (blood-CSF barrier dysfunction) displaying the shape of a saturation-like curve in contrast to hyperbolic curves of other blood-derived proteins in CSF. This non-linear relation between sICAM-1 and albumin quotients does not allow a linear index evaluation reported in earlier studies. In bacterial meningitis (n=31) and viral meningoencephalitis (n=28) in addition to the increased blood-derived fraction, the brain-derived fraction of sICAM-1 in CSF was up to 12-fold higher than that in controls. The sICAM-1 CSF/serum quotients in MS (n=15) did not differ from non-inflammatory controls, i.e., there was no brain-dependent sICAM-1 fluctuation in CSF in contrast to the known fluctuations in blood. Earlier published reports on sICAM-1 have been controversial due to less sensitive assays and unsuitable linear evaluation concepts for blood-CSF barrier dysfunction.
机译:在成对的CSF和来自128名患有不同神经疾病的患者的血清样本中测量了可溶性细胞间粘附分子-1(sICAM-1)。参考白蛋白CSF /血清商来表征CSF中血液来源的sICAM-1组分的参考范围。与血清(285.1 ng / ml; CV = 32%)相比,CSF(1.5 ng / ml; CV = 40%)中正常对照(n = 33)的sICAM-1平均浓度低,表明大约60%至80正常腰椎CSF中sICAM-1的百分比来自血液。该计算基于理论上预期的分子大小依赖性血液CSF梯度在300:1至250:1之间。在患有非炎性疾病的患者(n = 21)中,sICAM-1 CSF /血清商数随白蛋白CSF /血清商数(血液-CSF屏障功能障碍)的增加而呈非线性增加,而饱和状态曲线的形状与CSF中其他血液衍生蛋白质的双曲线。 sICAM-1和白蛋白商之间的这种非线性关系不允许在较早的研究中进行线性指数评估。在细菌性脑膜炎(n = 31)和病毒性脑膜脑炎(n = 28)中,除了血液来源的分数增加外,脑脊液中sICAM-1的大脑来源分数比对照组高12倍。 MS中的sICAM-1 CSF /血清商(n = 15)与非炎性对照无差异,即与已知的血液波动相反,CSF中没有大脑依赖性的sICAM-1波动。较早发表的有关sICAM-1的报告一直存在争议,原因是分析灵敏度较低,并且对血脑脊液屏障功能障碍的线性评估概念不合适。

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