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convertible CARs: A chimeric antigen receptor system for flexible control of activity and antigen targeting

机译:可换股车:一种嵌合抗原受体系统,可灵活控制活性和抗原靶向

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摘要

We have developed a chimeric antigen receptor (CAR) platform that functions as a modular system to address limitations of traditional CAR therapies. An inert form of the human NKG2D extracellular domain (iNKG2D) was engineered as the ectodomain of the CAR to generate convertibleCARTM-T cells. These cells were specifically directed to kill antigen-expressing target cells only in the presence of an activating bispecific adapter comprised of an iNKG2D-exclusive ULBP2-based ligand fused to an antigen-targeting antibody (MicAbodyTM). Efficacy against Raji tumors in NSG mice was dependent upon doses of both a rituximab-based MicAbody and convertibleCAR-T cells. We have also demonstrated that the exclusive ligand-receptor partnering enabled the targeted delivery of a mutant form of IL-2 to selectively promote the expansion of convertibleCAR-T cells in vitro and in vivo. By altering the Fv domains of the MicAbody or the payload fused to the orthogonal ligand, convertibleCAR-T cells can be readily targeted or regulated. Landgraf et al. developed a chimeric antigen receptor (CAR) platform that functions as a modular system. convertibleTM-T cells are designed to kill antigen-expressing target cells only in the presence of ligands fused to antigen-targeting antibodies (MicAbodyTM). This method provides a wide dosing window while minimizing toxicity.
机译:我们开发了一种嵌合抗原受体(汽车)平台,其用作模块化系统,以解决传统汽车疗法的局限性。人NKG2D细胞外结构域(INKG2D)的惰性形式被设计为轿厢的外胚瘤,以产生转化性artm-T细胞。具体地涉及这些细胞仅在由融合到抗原靶向抗体(MicaBodyTM)的基于InkG2D-独立的ULBP2的配体的激活双特异性衔接子存在下仅杀死抗原表达靶细胞。针对NSG小鼠的Raji肿瘤的功效依赖于Rituximab基脊髓型和转化性的剂量。我们还证明了独家配体受体合作使突变形式的IL-2的靶向递送能够在体外和体内选择性地促进转化性CopliBlecar-T细胞的膨胀。通过改变脊髓孢子的FV结构域或融合到正交配体的有效载荷,可以容易地靶向或调节转换器-T细胞。 Landgraf等人。开发出作为模块化系统的嵌合抗原受体(汽车)平台。转化性MM-T细胞设计成仅在融合与抗原靶向抗体(MicaBodyTM)的配体存在下杀死抗原表达的靶细胞。该方法提供了一个宽的计量窗口,同时最小化毒性。

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