The potential of bispecific T cell-engaging antibodies is hindered by manufacturing challenges and short serum half-life. We circumvented these limitations by treating mice with in vitro-transcribed pharmacologically optimized, nucleoside-modified mRNA encoding the antibody. We achieved sustained endogenous synthesis of the antibody, which eliminated advanced tumors as effectively as the corresponding purified bispecific antibody. Because manufacturing of pharmaceutical mRNA is fast, this approach could accelerate the clinical development of novel bispecific antibodies.

译文

双特异性T细胞结合抗体的潜力受到制造挑战和血清半衰期短的阻碍。我们通过用体外转录的药理优化的核苷修饰的编码抗体的mRNA处理小鼠来规避这些限制。我们实现了抗体的持续内源性合成,与相应的纯化双特异性抗体一样有效地消除了晚期肿瘤。由于药物mRNA的制造速度很快,因此该方法可以加速新型双特异性抗体的临床开发。

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