用特应性皮炎或寻常型银屑病患者的外周血单核细胞重组的 NOD/Scid IL2Rγ 空鼠反映了各自的表型。

Marietta Schindler , Paula Schuster-Winkelmann , Veronika Weß , Sophia Czell , Franziska Rueff , Andreas Wollenberg , Matthias Siebeck , Roswitha Gropp
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引用次数: 0

摘要

用溃疡性结肠炎或克罗恩病患者捐赠的 PBMC 重组的 NSG(NOD/Scid IL2Rγnull)小鼠高度反映了各自的病理表型。为了确定这些发现是否适用于特应性皮炎(AD)和寻常型银屑病(PV),我们首先对从特应性皮炎和寻常型银屑病患者体内分离的 PBMCs 进行了免疫学分析。随后,用这些 PBMCs 重建 NSG 小鼠。层次聚类和网络分析揭示了 AD 和 PV 患者的独特特征,活化的 CD4+ T 细胞(CD69、CD25)在 AD 网络中占据中心位置,而 CD4+ CD134+ 细胞则是 PV 网络的主要枢纽。在皮肤应用 DMSO 后,用 AD 供体的 PBMC 重组的 NSG 小鼠(即 NSG-AD 小鼠)和用 PV 供体的 PBMC 重组的 NSG 小鼠(即 NSG-PV 小鼠)的临床、皮肤和组织学评分都有所提高。免疫组化分析、脾脏人类白细胞频率和细胞因子表达水平表明,CD4+ CD69+细胞、表达M1和TSLP受体的单核细胞、切换B细胞和单核细胞趋化蛋白3是NSG-AD小鼠炎症的驱动因素。相反,NSG-PV 小鼠炎症的特征是表皮成纤维细胞、表达 CD1a 的单核细胞频率和 IL-17 水平的增加。因此,NSG-AD小鼠和NSG-PV小鼠的病理表型不同,部分反映了各自的人类疾病。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
NOD/Scid IL2Rγnull Mice Reconstituted with PBMCs from Patients with Atopic Dermatitis or Psoriasis Vulgaris Reflect the Respective Phenotype

NSG (NOD/Scid IL2Rγnull) mice reconstituted with PBMCs donated by patients with ulcerative colitis or Crohn’s disease highly reflect the respective pathological phenotype. To determine whether these findings could be applicable to atopic dermatitis (AD) and psoriasis vulgaris (PV), PBMCs isolated from patients with AD and PV were first subjected to immunological profiling. Subsequently, NSG mice were reconstituted with these PBMCs. Hierarchical clustering and network analysis revealed a distinct profile of patients with AD and PV with activated CD4+ T cells (CD69, CD25) occupying a central position in the AD network and CD4+ CD134+ cells acting as the main hub in the PV network. After dermal application of DMSO, both NSG mice reconstituted with PBMCs from donors with AD (ie, NSG-AD mice) and NSG mice reconstituted with PBMCs from donors with PV (ie, NSG-PV mice) exhibited increased clinical, skin, and histological scores. Immunohistochemical analysis, frequencies of splenic human leukocytes, and cytokine expression levels indicated that CD4+ CD69+ cells, M1 and TSLP receptor–expressing monocytes, switched B cells, and monocyte chemoattractant protein 3 were the driving factors of inflammation in NSG-AD mice. In contrast, inflammation in NSG-PV mice was characterized by an increase in fibroblasts in the epidermis, frequencies of CD1a-expressing monocytes, and IL-17 levels. Therefore, the pathological phenotypes of NSG-AD mice and NSG-PV mice differ and partially reflect the respective human diseases.

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