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首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >Detection by 4-parameter microscopic imaging and increase of rare mononuclear blood leukocyte types expressing the Fc gamma RIII receptor (CD16) for immunoglobulin G in human sporadic amyotrophic lateral sclerosis (ALS).
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Detection by 4-parameter microscopic imaging and increase of rare mononuclear blood leukocyte types expressing the Fc gamma RIII receptor (CD16) for immunoglobulin G in human sporadic amyotrophic lateral sclerosis (ALS).

机译:通过4参数显微镜成像进行检测,并增加人零食性肌萎缩性侧索硬化症(ALS)中表达免疫球蛋白G的FcγRIII受体(CD16)的罕见单核白细胞类型。

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摘要

By using quantitative multiparameter microscopic imaging we demonstrate concentration of two peripheral mononuclear blood leukocyte types expressing the Fc gamma RIII receptor for immunoglobulin G in a clinical subgroup of amyotrophic lateral sclerosis (ALS, n = 9) showing bulbar palsy (ALSBP) and/or predominant involvement of the upper motor neuron (ALSC). Triple fluorescence staining and overlay with phase contrast images (4 parameters) reveals that cell type 1 co-expresses Fc gamma RIII (CD16), CD8 and CD57 surface antigens (ALSC 50 +/- 33.6 cells/microliters, P = 0.0012; ALSBP 16.5 +/- 32.4, P = 0.029). This cell type is not observed in healthy individuals (n = 8) and is only insignificantly increased (P > 0.05) in neurological disease controls (stroke, n = 3, 2.1 +/- 3.7; polymyositis, n = 6, 1.5 +/- 4.0 cells/microliters) and in ALS cases with peripheral symptoms (ALSP n = 12: 7.6 +/- 8.7). Cell type 2 co-expresses Fc gamma RIII (CD16) and CD8, but is negative for CD57 (ALSC 60.1 +/- 19.3; ALSBP 24.2 +/- 28.0 cells/microliters). These findings are consistent with previous reports on IgG isotype changes and immune-cell invasion of the motor system in ALS.
机译:通过使用定量多参数显微成像,我们证明了肌萎缩性侧索硬化症(ALS,n = 9)的临床亚组中两种表达免疫球蛋白G的FcγRIII受体的外周单核白细胞的浓度,显示了延髓性麻痹(ALSBP)和/或优势性涉及上运动神经元(ALSC)。三重荧光染色和相衬图像叠加(4个参数)显示,细胞类型1共表达FcγRIII(CD16),CD8和CD57表面抗原(ALSC 50 +/- 33.6细胞/微升,P = 0.0012; ALSBP 16.5 +/- 32.4,P = 0.029)。在健康个体中未观察到这种细胞类型(n = 8),而在神经系统疾病对照(中风,n = 3,2.1 +/- 3.7;多发性肌炎,n = 6,1.5 + /)中,这种细胞类型仅显着增加(P> 0.05)。 -4.0细胞/微升),并且在有周围症状的ALS病例中(ALSP n = 12:7.6 +/- 8.7)。 2型细胞共表达FcγRIII(CD16)和CD8,但CD57阴性(ALSC 60.1 +/- 19.3; ALSBP 24.2 +/- 28.0细胞/微升)。这些发现与以前关于ALS中IgG同种型变化和运动系统的免疫细胞入侵的报道一致。

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