Center for Gene Therapy, The Research Institute at Nationwide Children's Hospital, Columbus, Ohio, USA.
J Neuroinflammation. 2010 Jul 16;7:39. doi: 10.1186/1742-2094-7-39.
Recently, using a mouse model of mucopolysaccharidosis (MPS) IIIB, a lysosomal storage disease with severe neurological deterioration, we showed that MPS IIIB neuropathology is accompanied by a robust neuroinflammatory response of unknown consequence. This study was to assess whether MPS IIIB lymphocytes are pathogenic.
Lymphocytes from MPS IIIB mice were adoptively transferred to naïve wild-type mice. The recipient animals were then evaluated for signs of disease and inflammation in the central nervous system.
Our results show for the first time, that lymphocytes isolated from MPS IIIB mice caused a mild paralytic disease when they were injected systemically into naïve wild-type mice. This disease is characterized by mild tail and lower trunk weakness with delayed weight gain. The MPS IIIB lymphocytes also trigger neuroinflammation within the CNS of recipient mice characterized by an increase in transcripts of IL2, IL4, IL5, IL17, TNFalpha, IFNalpha and Ifi30, and intraparenchymal lymphocyte infiltration.
Our data suggest that an autoimmune response directed at CNS components contributes to MPS IIIB neuropathology independent of lysosomal storage pathology. Adoptive transfer of purified T-cells will be needed in future studies to identify specific effector T-cells in MPS IIIB neuroimmune pathogenesis.
最近,我们使用黏多糖贮积症 IIIB(MPS IIIB)的小鼠模型(一种伴有严重神经功能恶化的溶酶体贮积病),发现 MPS IIIB 神经病理学伴有未知后果的强烈神经炎症反应。本研究旨在评估 MPS IIIB 淋巴细胞是否具有致病性。
将 MPS IIIB 小鼠的淋巴细胞过继转移到新生野生型小鼠体内。然后评估受体动物中枢神经系统中是否存在疾病和炎症的迹象。
我们的研究结果首次表明,从 MPS IIIB 小鼠分离的淋巴细胞在被系统注射到新生野生型小鼠体内时,会引起轻微的麻痹性疾病。这种疾病的特征是尾巴和下躯干轻微无力,体重增加延迟。MPS IIIB 淋巴细胞还会引发受体内的神经炎症,表现为白细胞介素 2(IL2)、白细胞介素 4(IL4)、白细胞介素 5(IL5)、白细胞介素 17(IL17)、肿瘤坏死因子-α(TNFalpha)、干扰素-α(IFNalpha)和 Ifi30 转录物的增加,以及实质内淋巴细胞浸润。
我们的数据表明,针对中枢神经系统成分的自身免疫反应是导致 MPS IIIB 神经病理学的原因之一,与溶酶体贮积病无关。在未来的研究中,需要进行纯化 T 细胞的过继转移,以鉴定 MPS IIIB 神经免疫发病机制中的特定效应 T 细胞。
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