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正常和异常脑脊液/血清蛋白浓度梯度下血脑脊髓液屏障对血清蛋白通透性的异质性模型

Heterogeneous models for blood-cerebrospinal fluid barrier permeability to serum proteins in normal and abnormal cerebrospinal fluid/serum protein concentration gradients.

作者信息

Livrea P, Trojano M, Simone I L, Zimatore G B, Pisicchio L, Logroscino G, Cibelli G

出版信息

J Neurol Sci. 1984 Jun;64(3):245-58. doi: 10.1016/0022-510x(84)90173-4.

Abstract

Cerebrospinal fluid (CSF)/serum concentration gradients (Q) of individual proteins (albumin, IgG, alpha 2-macroglobulin) have been studied in controls and in patients in whom the lumbar CSF flow is altered (medullary compression) or the blood-CSF barrier (BCB) function impaired (acute idiopathic polyneuropathy and acute meningoencephalitis). The analysis of relationships among protein Q has been performed by total and multiple regressions and the actual BCB permeability to individual proteins has been interpreted according to the accepted theoretical porous or vesicular BCB models. The exponential Q-IgG vs. Q-albumin total regression, and the poor Q-alpha 2-macroglobulin vs. Q-albumin regression found in controls, together with the different multiple regressions among proteins and the high Q-IgG vs. Q-albumin partial regression coefficients found in medullary compression, acute idiopathic polyneuropathy and acute meningoencephalitis, indicated that different permeability mechanisms can be postulated. Heterogeneous, fairly independent permeability BCB mechanisms maintain the normal CSF/serum protein concentration gradient. Pinocytotic vesicles or pores of radius exceeding 1000-1500 A, probably located at the capillary endothelium, account for the main serum-derived CSF protein fraction(s) with large hydrodynamic radius (R). A more selective endothelial vesicular transport with a radius of 250 A transfers a negligible amount of protein from serum into CSF. Proteins with small R also enter the CSF through a set of selective pores of radius 120 A, probably at the level of the choroidal epithelium. Pinocytotic vesicles with a radius of 250 A and increased rate of formation induce the accumulation of proteins below an obstruction of lumbar CSF flow. An increased formation rate of vesicles with a radius of 450 A can explain the increased capillary permeability in nerve roots in acute idiopathic polyneuropathy. Loss of selectivity was the main feature of BCB in acute meningoencephalitis, and it seemed to be due to pores or vesicles with a radius larger than 1000-1500 A. The heterogeneity of BCB mechanisms must be taken into account when the intrathecal synthesis of a protein, also derived from serum (for example IgG), has to be measured.

摘要

已对对照组以及腰椎脑脊液流动改变(髓质受压)或血脑脊液屏障(BCB)功能受损(急性特发性多神经病和急性脑膜脑炎)的患者个体蛋白质(白蛋白、免疫球蛋白G、α2-巨球蛋白)的脑脊液(CSF)/血清浓度梯度(Q)进行了研究。通过全回归和多重回归分析了蛋白质Q之间的关系,并根据公认的理论多孔或囊泡BCB模型解释了BCB对个体蛋白质的实际通透性。对照组中免疫球蛋白G的Q与白蛋白的Q指数全回归以及α2-巨球蛋白的Q与白蛋白的回归较差,以及蛋白质之间不同的多重回归和髓质受压、急性特发性多神经病和急性脑膜脑炎中免疫球蛋白G的Q与白蛋白的部分回归系数较高,表明可以假设不同的通透机制。异质性、相当独立的通透性BCB机制维持正常的脑脊液/血清蛋白质浓度梯度。半径超过1000 - 1500埃的胞饮小泡或孔隙,可能位于毛细血管内皮,构成了具有较大流体动力学半径(R)的主要血清源性脑脊液蛋白质部分。半径为250埃的更具选择性的内皮囊泡转运将可忽略量的蛋白质从血清转运到脑脊液中。小R的蛋白质也通过一组半径为120埃的选择性孔隙进入脑脊液,可能在脉络丛上皮水平。半径为250埃且形成速率增加的胞饮小泡会导致蛋白质在腰椎脑脊液流动受阻下方积聚。半径为450埃的小泡形成速率增加可以解释急性特发性多神经病中神经根毛细血管通透性增加的原因。选择性丧失是急性脑膜脑炎中BCB的主要特征,似乎是由于半径大于1000 - 1500埃的孔隙或小泡所致。当必须测量同样源自血清的蛋白质(例如免疫球蛋白G)的鞘内合成时,必须考虑BCB机制的异质性。

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