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Increased cerebrospinal fluid concentrations of soluble Fas(CD95/Apo-1) in hydrocephalus

机译:脑脊液中可溶性Fas浓度升高脑积水中的(CD95 / Apo-1)

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摘要

BACKGROUND AND AIMS—The ventricular enlargement observed in children with chronically raised intracranial pressure (ICP) causes a secondary loss of brain tissue. In animal studies of hydrocephalus, programmed cell death (apoptosis) has been found as a major mechanism of neuronal injury. One of the regulators of the apoptotic cell death programme is the receptor mediated Fas/Fas ligand interaction.
METHODS—The apoptosis regulating cytokines soluble Fas (sFas) and soluble Fas ligand (sFasL) were studied in the cerebrospinal fluid (CSF) of 31 hydrocephalic children undergoing shunt surgery for symptomatic hydrocephalus and 18controls.
RESULTS—High concentrations of sFas were observed in children with hydrocephalus (median 252 ng/ml); in controls sFas was below the detection limit (0.5 ng/ml). sFasL was undetectable in all but one sample.
CONCLUSION—High concentrations of sFas in the CSF of children with hydrocephalus suggest intrinsic sFas production, potentially antagonising pressure mediated Fas activation.

机译:背景与目的:在慢性颅内压(ICP)升高的儿童中观察到的心室扩大会导致脑组织的继发性丧失。在脑积水的动物研究中,已发现程序性细胞死亡(细胞凋亡)是神经元损伤的主要机制。凋亡介导的凋亡机制之一是受体介导的Fas / Fas配体相互作用。 )31例因症状性脑积水而接受分流手术的脑积水儿童和18例对照者。
结果—脑积水儿童的sFas浓度较高(中位数为252 ng / ml);对照中sFas低于检测极限(0.5 ng / ml)。 sFasL在除一个样本外的所有样本中均无法检出。
结论—脑积水儿童脑脊液中高浓度的sFas提示内在的sFas产生,可能拮抗压力介导的Fas激活。

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