首页> 外文期刊>The journal of immunology >Tissue-Resident Ecto-5′ Nucleotidase (CD73) Regulates Leukocyte Trafficking in the Ischemic Brain
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Tissue-Resident Ecto-5′ Nucleotidase (CD73) Regulates Leukocyte Trafficking in the Ischemic Brain

机译:驻留于组织的Ecto-5'核苷酸酶(CD73)调节缺血性脑中的白细胞运输。

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Ectoenzymes expressed on the surface of vascular cells and leukocytes modulate the ambient nucleotide milieu. CD73 is an ecto-5′ nucleotidase that catalyzes the terminal phosphohydrolysis of AMP and resides in the brain on glial cells, cells of the choroid plexus, and leukocytes. Though CD73 tightens epithelial barriers, its role in the ischemic brain remains undefined. When subjected to photothrombotic arterial occlusion, CD73?/? mice exhibited significantly larger (49%) cerebral infarct volumes than wild-type mice, with concordant increases in local accumulation of leukocyte subsets (neutrophils, T lymphocytes, macrophages, and microglia). CD73?/? mice were rescued from ischemic neurologic injury by soluble 5′-nucleotidase. In situ, CD73?/? macrophages upregulated expression of costimulatory molecules far more than wild-type macrophages, with a sharp increase of the CD80/CD86 ratio. To define the CD73-bearing cells responsible for ischemic cerebroprotection, mice were subjected to irradiative myeloablation, marrow reconstitution, and then stroke following engraftment. Chimeric mice lacking CD73 in tissue had larger cerebral infarct volumes and more tissue leukosequestration than did mice lacking CD73 on circulating cells. These data show a cardinal role for CD73 in suppressing ischemic tissue leukosequestration. This underscores a critical role for CD73 as a modulator of brain inflammation and immune function.
机译:在血管细胞和白细胞表面表达的电子酶调节周围核苷酸环境。 CD73是一种ecto-5'核苷酸酶,可催化AMP的末端磷酸水解,并位于大脑中的神经胶质细胞,脉络丛细胞和白细胞上。尽管CD73加强了上皮屏障,但其在缺血性脑中的作用仍不确定。当遭受光血栓性动脉闭塞时,CD73α/β是阳性的。与野生型小鼠相比,小鼠表现出明显更大的脑梗死体积(49%),并且白细胞亚群(中性粒细胞,T淋巴细胞,巨噬细胞和小胶质细胞)的局部积累也相应增加。 CD73?/?通过可溶性5'-核苷酸酶使小鼠免于缺血性神经系统损伤。 CD73?/?巨噬细胞上调共刺激分子的表达远超过野生型巨噬细胞,CD80 / CD86比值急剧增加。为了确定负责缺血性脑保护的带有CD73的细胞,对小鼠进行辐照性骨髓消融,骨髓重建,然后在植入后中风。与在循环细胞上缺乏CD73的小鼠相比,组织中缺乏CD73的嵌合小鼠具有更大的脑梗死体积和更多的组织白细胞富集。这些数据显示了CD73在抑制局部缺血性白细胞形成中的主要作用。这突显了CD73作为大脑炎症和免疫功能调节剂的关键作用。

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