首页> 外文期刊>Tissue antigens. >The expression analysis of ICOS-L on activated T cells and immature dendritic cells as well as malignant B cells and Grave's-disease-derived thyroid tissues by two novel mAbs against human ICOS-L.
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The expression analysis of ICOS-L on activated T cells and immature dendritic cells as well as malignant B cells and Grave's-disease-derived thyroid tissues by two novel mAbs against human ICOS-L.

机译:通过两种针对人ICOS-L的单克隆抗体,ICOS-L在活化的T细胞和未成熟树突状细胞以及恶性B细胞和Grave's疾病衍生的甲状腺组织上的表达分析。

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摘要

ICOS-L, a newly identified member of B7 superfamily, plays an important role in immune responses. In this article, we report on two novel mouse anti-human ICOS-L monoclonal antibodies (mAbs) named as 11C4 and 12B11, whose specificities were verified by methods of flow cytometry, western blotting, and epitope competition assay. The two mAbs bound to distinct ICOS-L epitopes on B cells. Interestingly, mAb 11C4 could well recognize ICOS-L molecule on activated T cells and Jurkat cell lines, which is different from commercial anti-ICOS-L mAb (clone number MIH12) and the other mAb 12B11. In addition, we found that the expression of ICOS-L molecule was only detected on the surface of immature monocyte-derived dendritic cells (Mo-DCs) and was sharply decreased after induction of mature Mo-DCs activated by tumor necrosis factor-alpha or CD40. Furthermore, we showed that 11C4 could effectively suppress the maturation of Mo-DCs in vitro as evidenced by the low expression of CD80, CD86, CD83, and human leukocyte antigen-DR, which suggested that ICOS-L may be involved in the maturation of Mo-DCs. Using immunohistochemistry staining with mAb 11C4, the expression of ICOS-L was found in B lymphoma tissues and thyroid tissues from the Grave's disease but not in thyroid adenoma and normal thyroid tissues.
机译:B7超家族的新成员ICOS-L在免疫应答中起重要作用。在本文中,我们报告了两种名为11C4和12B11的新型小鼠抗人ICOS-L单克隆抗体(mAbs),它们的特异性已通过流式细胞仪,蛋白质印迹和表位竞争分析方法进行了验证。这两个mAb与B细胞上独特的ICOS-L表位结合。有趣的是,mAb 11C4可以很好地识别激活的T细胞和Jurkat细胞系上的ICOS-L分子,这与市售的抗ICOS-L mAb(克隆号MIH12)和其他mAb 12B11不同。此外,我们发现ICOS-L分子的表达仅在未成熟的单核细胞衍生的树突状细胞(Mo-DCs)的表面上检测到,并在诱导由肿瘤坏死因子-α激活的成熟Mo-DCs后急剧下降。 CD40。此外,我们显示11C4可以在体外有效抑制Mo-DC的成熟,CD80,CD86,CD83和人白细胞抗原-DR的低表达证明了这一点,这表明ICOS-L可能参与了Mo-DC的成熟。 Mo-DC。使用mAb 11C4进行的免疫组织化学染色,在Grave's病的B淋巴瘤组织和甲状腺组织中发现了ICOS-L的表达,而在甲状腺腺瘤和正常甲状腺组织中未发现ICOS-L的表达。

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