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脑脊液中新蝶呤是脑源性的,与非炎症性情感和精神分裂症谱系障碍中的血脑屏障功能障碍无关。

Cerebrospinal fluid neopterin is brain-derived and not associated with blood-CSF barrier dysfunction in non-inflammatory affective and schizophrenic spectrum disorders.

机构信息

Division of Biological Chemistry, Biocenter, Innsbruck Medical University, Innrain 80, A-6020 Innsbruck, Austria.

出版信息

J Psychiatr Res. 2013 Oct;47(10):1417-22. doi: 10.1016/j.jpsychires.2013.05.027. Epub 2013 Jun 19.

DOI:10.1016/j.jpsychires.2013.05.027
PMID:23790260
Abstract

Many psychiatric patients have a minor blood-CSF barrier dysfunction and increased Cerebrospinal fluid (CSF) neopterin concentrations. The source of normal CSF neopterin, a biomarker in inflammatory and non-inflammatory neurological diseases, has never been shown explicitly, a precondition for sensitive detection of pathologically increased CSF neopterin. Neopterin concentrations (ELISA) in CSF and serum of normal controls (n = 26) are evaluated by inter-individual variation propagation. Normal CSF neopterin is brain-derived: The inter-individual variation of CSF neopterin in the control group does not depend on serum neopterin concentration variation (coefficient of variation, CV-CSF = 9.7% < CV-serum = 24.5%). Additionally individual normal CSF neopterin concentrations are invariant to the variation of the albumin quotient, QAlb, i.e. CSF neopterin does not derive from leptomeninges. Subsequently CSF neopterin was interpreted with reference to its absolute concentration in CSF (cut off = 5.5 nmol/l). Patients (N = 44), retrospectively selected from a larger group with schizophrenic and affective spectrum disorder, are characterized by the absence of any clinical and neurochemical signs of inflammation. In this group 30% had an increased CSF neopterin concentration and 30% had an increased QAlb with only 7% combined pathologies. Increased CSF neopterin did not correlate with the blood-CSF barrier dysfunction. In the discussion we point to possible sources of both independent pathologies, connected either with reduced CSF flow rate (QAlb) or microglial activation (neopterin). With CSF neopterin analysis earlier in vitro studies about microglia activation in schizophrenic spectrum disorders or corresponding therapeutic efforts could get a more direct, in-vivo analytical tool.

摘要

许多精神病患者存在轻微的血脑屏障功能障碍和脑脊液(CSF)中新蝶呤浓度升高。正常 CSF 中新蝶呤的来源,一种在炎症性和非炎症性神经疾病中的生物标志物,从未被明确表明,这是敏感检测病理性升高的 CSF 中新蝶呤的前提条件。通过个体间变异传播来评估正常对照(n = 26)的 CSF 和血清中新蝶呤浓度(ELISA)。正常 CSF 中新蝶呤是源自大脑的:对照组 CSF 中新蝶呤的个体间变异不依赖于血清中新蝶呤浓度的变异(变异系数,CV-CSF = 9.7% < CV-血清 = 24.5%)。此外,个体正常 CSF 中新蝶呤浓度不受白蛋白商 QAlb 变化的影响,即 CSF 中新蝶呤不是来自软脑膜。随后,根据 CSF 中新蝶呤的绝对浓度(截值 = 5.5 nmol/L)对其进行解释。从具有精神分裂症和情感谱障碍的较大组中回顾性选择的患者(N = 44),其特征是没有任何炎症的临床和神经化学迹象。在该组中,有 30%的患者 CSF 中新蝶呤浓度升高,有 30%的患者 QAlb 升高,只有 7%的患者同时存在两种病理学。CSF 中新蝶呤升高与血脑屏障功能障碍无关。在讨论中,我们指出了这两种独立病理学的可能来源,它们可能与 CSF 流量(QAlb)降低或小胶质细胞激活(新蝶呤)有关。通过 CSF 中新蝶呤分析,早期关于精神分裂症谱障碍中小胶质细胞激活的体外研究或相应的治疗努力可能会获得更直接的体内分析工具。

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