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首页> 外文期刊>Molecular Psychiatry >Increased macrophages and changed brain endothelial cell gene expression in the frontal cortex of people with schizophrenia displaying inflammation
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Increased macrophages and changed brain endothelial cell gene expression in the frontal cortex of people with schizophrenia displaying inflammation

机译:增加巨噬细胞和改变脑内皮细胞基因表达,在脑卒中脑前皮层中显示出炎症

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Elevated pro-inflammatory cytokines exist in both blood and brain of people with schizophrenia but how this affects molecular indices of the blood-brain barrier (BBB) is unclear. Eight mRNAs relating to BBB function, a microglia and three immune cell markers were measured by qPCR in the prefrontal cortex from 37 people with schizophrenia/schizoaffective disorder and 37 matched controls. This cohort was previously grouped into "high inflammation" and "low inflammation" subgroups based on cortical inflammatory-related transcripts. Soluble intercellular adhesion molecule-1 (sICAM1) was measured in the plasma of 78 patients with schizophrenia/schizoaffective disorder and 73 healthy controls. We found thatsICAM1 was significantly elevated in schizophrenia. An efflux transporter, ABCG2, was lower, while mRNAs encoding VE-cadherin and ICAM1 were higher in schizophrenia brain. The "high inflammation" schizophrenia subgroup had lower ABCG2 and higher ICAM1, VE-cadherin, occludin and interferon-induced transmembrane protein mRNAs compared to both "low inflammation" schizophrenia and "low inflammation" control subgroups. ICAM1 immunohistochemistry showed enrichment in brain endothelium regardless of diagnosis and was localised to astrocytes in some brains. Microglia mRNA was not altered in schizophrenia nor did it correlate with ICAM1 expression. Immune cell mRNAs were elevated in "high inflammation" schizophrenia compared to both "low inflammation" schizophrenia and controls. CD163+ perivascular macrophages were identified by immunohistochemistry in brain parenchyma in over 40% of "high inflammation" schizophrenia brains. People with high levels of cytokine expression and schizophrenia display changes consistent with greater immune cell transmigration into brain via increased ICAM1, which could contribute to other neuropathological changes found in this subgroup of people.
机译:升高的促炎细胞因子存在于有精神分裂症的人的血液和脑中存在,但这将如何影响血脑屏障(BBB)的分子指数尚不清楚。通过37人从精神分裂症/ SchizoAfective病症和37种匹配的对照,通过QPCR测量与BBB功能有关的八个MRNA和三种免疫细胞标记物测量。该队列以前基于皮质炎症相关的转录物分组成“高炎症”和“低炎症”亚组。在78例精神分裂症/ SchizoAfferceive病症和73例健康对照中测量可溶性细胞间粘附分子-1(SICAM1)。我们发现Sechizopheria显着升高。流出转运蛋白ABCG2较低,而在精神分裂症脑中编码Ve-Cadherin和ICAM1的MRNA也较高。与“低炎症”精神分裂症和“低炎症”对照亚组相比,“高炎症”精神分裂症亚组具有较低的ABCG2和更高的ICAM1,Ve-Cadherin,occludin和干扰素诱导的跨膜蛋白MRNA。 ICAM1免疫组织化学在脑内皮中均有浓缩,无论诊断如何,都在一些脑中定位于星形胶质细胞。微胶质细胞mRNA未在精神分裂症中改变,也没有与ICAM1表达相关。与“低炎症”精神分裂症和对照相比,免疫细胞mRNA在“高炎症”精神分裂症中升高。通过在40%的“高炎症”精神分裂症中,通过免疫组织化学鉴定CD163 +羽毛血管巨噬细胞。细胞因子表达和精神分裂症表达和精神分裂症展示的人通过增加的ICAM1增加了更大的免疫细胞迁移到脑中,这可能导致该亚组中发现的其他神经病理学变化。

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