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Functional diversification of hybridoma-produced antibodies by CRISPR/HDR genomic engineering

机译:通过CRISPR / HDR基因组工程实现杂交瘤产生的抗体的功能多样化

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摘要

Hybridoma technology is instrumental for the development of novel antibody therapeutics and diagnostics. Recent preclinical and clinical studies highlight the importance of antibody isotype for therapeutic efficacy. However, since the sequence encoding the constant domains is fixed, tuning antibody function in hybridomas has been restricted. Here, we demonstrate a versatile CRISPR/HDR platform to rapidly engineer the constant immunoglobulin domains to obtain recombinant hybridomas, which secrete antibodies in the preferred format, species, and isotype. Using this platform, we obtained recombinant hybridomas secreting Fab′ fragments, isotype-switched chimeric antibodies, and Fc-silent mutants. These antibody products are stable, retain their antigen specificity, and display their intrinsic Fc-effector functions in vitro and in vivo. Furthermore, we can site-specifically attach cargo to these antibody products via chemoenzymatic modification. We believe that this versatile platform facilitates antibody engineering for the entire scientific community, empowering preclinical antibody research.
机译:杂交瘤技术对新型抗体疗法和诊断方法的开发至关重要。最近的临床前和临床研究强调了抗体同种型对于治疗功效的重要性。但是,由于编码恒定域的序列是固定的,因此杂交瘤中调节抗体的功能受到限制。在这里,我们展示了一个多功能的CRISPR / HDR平台,可以快速工程化恒定的免疫球蛋白结构域以获得重组杂交瘤,该杂交瘤分泌出优选形式,种类和同种型的抗体。使用该平台,我们获得了分泌Fab'片段,同种型嵌合抗体和Fc-沉默突变体的重组杂交瘤。这些抗体产物稳定,保留其抗原特异性,并在体外和体内显示其固有的Fc效应子功能。此外,我们可以通过化学酶修饰将货物固定在这些抗体产品上。我们相信,该多功能平台可促进整个科学界的抗体工程设计,从而为临床前抗体研究提供支持。

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