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首页> 外文期刊>Leukemia >A bispecific single-chain antibody that mediates target cell-restricted, supra-agonistic CD28 stimulation and killing of lymphoma cells
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A bispecific single-chain antibody that mediates target cell-restricted, supra-agonistic CD28 stimulation and killing of lymphoma cells

机译:一种双特异性单链抗体,介导靶细胞限制的超激动CD28刺激和淋巴瘤细胞的杀伤

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摘要

We have previously reported that r28M, a recombinant bispecific single-chain antibody directed to a melanoma-associated proteoglycan (NG2) and the costimulatory CD28 molecule on T cells, induced T-cell activation, which resulted in tumor-cell killing. T-cell activation did not require a primary signal through the T-cell antigen receptor (TCR)/CD3 complex and depended on the presence of NG2-positive tumor cells. Here, we further investigate this phenomenon of a target cell-restricted, supra-agonistic CD28 stimulation with bispecific antibodies. To this end, we exchanged the NG2 targeting part of r28M with a single-chain antibody directed to the B-cell associated antigen CD20. The resulting bispecific single-chain antibody, termed r2820, induced supra-agonistic T-cell activation, which required the presence of autologous normal or malignant B cells, respectively. Once activated, T cells were capable of destroying lymphoma target cells.These findings demonstrate that supra-agonistic CD28 stimulation with bispecific single-chain antibodies is a robust and readily reproducible phenomenon. In the context of experimental tumor therapy, it may provide a valuable alternative to the unrestricted T-cell activation induced by 'super-agonistic', monospecific CD28 antibodies.
机译:我们以前曾报道过,r28M是针对黑素瘤相关蛋白聚糖(NG2)和共刺激CD28分子在T细胞上的重组双特异性单链抗体,可诱导T细胞活化,从而导致肿瘤细胞被杀死。 T细胞活化不需要通过T细胞抗原受体(TCR)/ CD3复合物的主要信号,而是取决于NG2阳性肿瘤细胞的存在。在这里,我们进一步研究了用双特异性抗体对靶细胞进行限制,超激动的CD28刺激的现象。为此,我们用针对B细胞相关抗原CD20的单链抗体交换了r28M的NG2靶向部分。产生的称为r2820的双特异性单链抗体诱导了超激动性T细胞活化,这需要分别存在自体正常或恶性B细胞。一旦激活,T细胞就能破坏淋巴瘤靶细胞。这些发现表明,双特异性单链抗体对超激动CD28的刺激是一种强大且易于再现的现象。在实验性肿瘤治疗的背景下,它可以为“超激动性”单特异性CD28抗体诱导的不受限制的T细胞活化提供有价值的替代方法。

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