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首页> 外文期刊>Journal of Leukocyte Biology: An Official Publication of the Reticuloendothelial Society >P-selectin mediates IL-13-induced eosinophil transmigration but not eotaxin generation in vivo: a comparative study with IL-4-elicited responses.
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P-selectin mediates IL-13-induced eosinophil transmigration but not eotaxin generation in vivo: a comparative study with IL-4-elicited responses.

机译:P-选择素在体内介导IL-13诱导的嗜酸性粒细胞迁移,但不介导嗜酸性粒细胞生成:IL-4引起的反应的比较研究。

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The study investigated the role of P-selectin in the responses of eosinophil transmigration and eotaxin generation in vivo elicited by interleukin (IL)-13, as compared with IL-4. Two murine models of leukocyte transmigration were used, migration into cytokine-stimulated peritoneal cavities and through stimulated cremasteric venules, as observed by intravital microscopy. In mice lacking P-selectin, eosinophil infiltration elicited by the cytokines in the peritonitis model was totally inhibited. In the cremaster muscle, however, although spontaneous leukocyte-rolling flux and stimulated leukocyte firm adhesion were inhibited by approximately 97% and approximately 48%, respectively, stimulated transmigration was unaffected. However, IL-13-induced leukocyte transmigration was totally blocked in P-selectin-deficient mice treated with an anti-alpha(4) integrin monoclonal antibody (mAb; PS/2). In comparison, treatment of wild-type mice with the anti-alpha(4) integrin mAb resulted in only partial suppression of IL-13-induced leukocyte transmigration. Significant levels of eotaxin were detected in response to IL-13/IL-4 in both tissues in P-selectin-deficient animals. In conclusion, the regulatory role of P-selectin in leukocyte transmigration elicited by IL-13 appears to be tissue-specific, a phenomenon that is independent of the ability of the cytokine to stimulate eotaxin generation.
机译:该研究调查了白介素(IL)-13与IL-4相比,P-选择素在体内嗜酸性粒细胞迁移和嗜酸性粒细胞生成趋化因子的反应中的作用。如在活体显微镜下所观察到的,使用了两种鼠类白细胞迁移模型,它们迁移到细胞因子刺激的腹膜腔中并通过刺激的睾丸小静脉迁移。在缺乏P-选择蛋白的小鼠中,腹膜炎模型中由细胞因子引起的嗜酸性粒细胞浸润被完全抑制。然而,在提睾肌中,尽管自发性白细胞滚动通量和刺激的白细胞牢固粘附分别被抑制了约97%和约48%,但刺激的迁移并未受到影响。但是,IL-13诱导的白细胞迁移在用抗alpha(4)整合素单克隆抗体(mAb; PS / 2)治疗的P-选择素缺陷型小鼠中被完全阻断。相比之下,用抗alpha(4)整合素单抗治疗野生型小鼠只导致部分抑制IL-13诱导的白细胞迁移。在缺乏P-选择蛋白的动物的两个组织中都检测到了对IL-13 / IL-4应答的严重的趋化因子水平。总之,IL-13引起的白细胞转运中P-选择蛋白的调节作用似乎是组织特异性的,这种现象与细胞因子刺激嗜酸性粒细胞趋化因子的能力无关。

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