首页> 美国卫生研究院文献>The Journal of Neurology and Psychopathology >Evidence for the role of demyelination HLA-DR alleles and cytokines in the pathogenesis of parvovirus B19 meningoencephalitis and its sequelae
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Evidence for the role of demyelination HLA-DR alleles and cytokines in the pathogenesis of parvovirus B19 meningoencephalitis and its sequelae

机译:脱髓鞘HLA-DR等位基因和细胞因子在细小病毒B19脑膜脑炎及其后遗症发病机理中的作用的证据

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摘要

>Objective: To review the clinical and pathological features of parvovirus B19 meningoencephalitis and its sequelae in 12 previously published cases, and to perform additional tests to determine the pathogenesis of the disease. >Methods: Cases were reviewed and available serum and cerebrospinal fluid (CSF) tested for antiganglioside antibodies and a range of cytokines. In situ hybridisation for parvovirus B19 DNA was performed on postmortem brain tissue in two cases. HLA-DRB1 typing was undertaken on genomic DNA extracted from peripheral blood leucocytes. >Results: Cerebellar involvement was suggested either clinically or pathologically in four cases. In the two cases with postmortem histology, there was marked atrophy of the molecular and granular layers of the cerebellum with focal loss of Purkinje cells. Brain scanning by MRI or CT was done in six cases during the acute phase. Three were abnormal with evidence of demyelination. Three had markedly enlarged ventricles, in two of which there was high signal intensity from the white matter on both T1 and T2 weighted images. The three cases with abnormal brain scans had long term neurological sequelae (mental retardation, personality change, altered affect). In situ hybridisation on available postmortem brain tissue was negative in the two cases tested. All cases in which HLA-DR alleles were determined carried at least one of the following alleles: HLA-DRB1*01, *04, *07, *09, *15, *16. Available serum and CSF was tested for antiganglioside antibodies (all negative) and for a panel of cytokines, which had a similar profile in both serum (n = 5) and CSF (n = 1) during the acute phase. Cytokines that were consistently detectable were IL-6 (mean 726.20 pg/ml), TNFα (50.64 pg/ml), IFNγ (39.64 pg/ml), GM-CSF (216.12 pg/ml), and MCP-1 (154.43 pg/ml); IL-1ß, IL-5, and IL-13 were undetectable. >Conclusions: HLA-DR associations, an increased cytokine response, and benefit from immunomodulatory treatment (in one case) support a role for the immune response in the pathogenesis of parvovirus B19 meningoencephalitis.
机译:>目的:回顾细小病毒B19脑膜脑炎及其后遗症在12例先前发表的病例中的临床和病理学特征,并进行其他测试以确定该病的发病机制。 >方法:对病例进行了审查,并对可用的血清和脑脊液(CSF)进行了抗神经节苷脂抗体和一系列细胞因子的检测。在两种情况下,在死后脑组织上进行细小病毒B19 DNA的原位杂交。对从外周血白细胞提取的基因组DNA进行HLA-DRB1分型。 >结果:有4例在临床或病理上均提示小脑受累。在死后组织学检查的两个病例中,小脑的分子层和颗粒层明显萎缩,浦肯野细胞灶性丢失。在急性期有6例通过MRI或CT进行了脑部扫描。 3例异常,脱髓鞘。三个显着增大的心室,其中两个在T1和T2加权图像上都有来自白质的高信号强度。 3例脑部扫描异常的患者有长期的神经系统后遗症(智力低下,人格改变,情感改变)。在测试的两个案例中,可用死后大脑组织的原位杂交均为阴性。确定HLA-DR等位基因的所有情况均携带以下至少一个等位基因:HLA-DRB1 * 01,* 04,* 07,* 09,* 15,* 16。测试了可用血清和CSF的抗神经节苷脂抗体(全部阴性)和一组细胞因子,在急性期血清(n = 5)和CSF(n = 1)具有相似的特征。始终可检测到的细胞因子是IL-6(平均726.20 pg / ml),TNFα(50.64 pg / ml),IFNγ(39.64 pg / ml),GM-CSF(216.12 pg / ml)和MCP-1(154.43 pg) / ml); IL-1ß,IL-5和IL-13无法检测到。 >结论: HLA-DR关联,细胞因子应答增加以及免疫调节治疗(一种情况)的获益支持了细小病毒B19脑膜脑炎发病机理中免疫应答的作用。

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