首页> 外文期刊>Journal of immunotherapy >A novel CD19-directed recombinant bispecific antibody derivative with enhanced immune effector functions for human leukemic cells.
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A novel CD19-directed recombinant bispecific antibody derivative with enhanced immune effector functions for human leukemic cells.

机译:一种新型的CD19定向重组双特异性抗体衍生物,具有增强的人类白血病细胞免疫效应功能。

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摘要

A novel bispecific antibody-derived recombinant protein targeting leukemias and lymphomas was designed, a single-chain Fv triple body (sctb) consisting of 1 polypeptide chain with 3 scFvs connected in tandem. The distal scFvs were specific for the tumor antigen CD19, and the central scFv for the trigger molecule CD16 (FcgammaRIII) on natural killer (NK) cells and macrophages. We had previously built a disulphide stabilized (ds) bsscFv [19 x 16] with monovalent binding for CD19 from ds components. The sctb ds[19 x 16 x 19] also used ds components and displayed 3-fold greater avidity for CD19 than the bsscFv (KD = 13 vs. 42 nM), whereas both had equal affinity for CD16 (KD = 58 nM). Plasma half-lives in mice were 4 and 2 hours for the sctb and the bsscFv, respectively. In antibody-dependent cellular cytotoxicity reactions with human mononuclear cells as effectors, the sctb promoted equal lysis of leukemic cell lines and primary cells from leukemia and lymphoma patients at 10-fold to 40-fold lower concentrations than the bsscFv. This new format may also be applicable to a variety of other tumor antigens and effector molecules. With half-maximum effective concentrations (EC50) in the low picomolar range, the sctb ds[19 x 16 x 19] is an attractive candidate for further preclinical evaluation.
机译:设计了一种针对白血病和淋巴瘤的新型双特异性抗体衍生重组蛋白,该单链Fv三体(sctb)由1条多肽链和3条scFv串联而成。远端scFv对肿瘤抗原CD19具有特异性,而中央scFv对自然杀伤(NK)细胞和巨噬细胞上的触发分子CD16(FcgRIII)具有特异性。我们以前已经构建了一个二硫键稳定的(ds)bsscFv [19 x 16],与ds组分的CD19具有单价结合。 sctb ds [19 x 16 x 19]也使用ds成分,对CD19的亲和力比bsscFv高3倍(KD = 13 vs. 42 nM),而两者对CD16的亲和力均相同(KD = 58 nM)。对于sctb和bsscFv,小鼠的血浆半衰期分别为4小时和2小时。在以人单核细胞为效应子的抗体依赖性细胞毒性反应中,sctb促进白血病和淋巴瘤患者白血病细胞系和原代细胞的均等裂解,其浓度比bsscFv低10到40倍。这种新形式也可能适用于多种其他肿瘤抗原和效应分子。由于在半皮摩尔范围内的最大有效浓度(EC50)为一半,因此sctb ds [19 x 16 x 19]是进行进一步临床前评估的有吸引力的候选药物。

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