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Prevalence of Pre-existing Antibodies to CRISPR-Associated Nuclease Cas9 in the USA Population

机译:在美国人群中与CRISPR相关的核酸酶Cas9的既有抗体的患病率

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摘要

The repurposing of the CRISPR/Cas microbial adaptive immune system for gene editing has resulted in an exponential rise in new technologies and promising approaches for treating numerous human diseases. While some of the approaches being currently developed involve ex vivo editing by CRISPR/Cas9, many more potential applications will require in vivo editing. The in vivo use of this technology comes with challenges, one of which is the immune response to Cas9, a protein of microbial origin. Thus, the prevalence of pre-existing antibodies to Cas9 could also be a relevant parameter. There are many avenues for how CRISPR/Cas9 technologies will be applied in vivo, including the mode of delivery. These may be expected to invoke different immunological pathways. Nonetheless, as with all protein therapeutics, it may be desirable to monitor for anti-Cas9 antibodies during clinical development. This will require the development of robust and reliable assays. Here, we describe ELISA-based assays that are capable of detecting antibodies to Cas9 from Staphylococcus aureus (SaCas9) and Streptococcs pyogenes (SpCas9) in human sera. Furthermore, using these assays to screen for pre-existing antibodies in 200 human serum samples, we found the prevalence of anti-SaCas9 and anti-SpCas9 antibodies to be 10% and 2.5%, respectively.
机译:CRISPR / Cas微生物适应性免疫系统用于基因编辑的重新利用已导致用于治疗多种人类疾病的新技术和有前途的方法呈指数增长。尽管目前正在开发的一些方法涉及CRISPR / Cas9的体外编辑,但在体内编辑中还需要更多潜在的应用程序。这项技术在体内的使用带来了挑战,其中之一是对Cas9(一种微生物来源的蛋白质)的免疫反应。因此,已经存在的针对Cas9的抗体的流行也可能是一个相关参数。 CRISPR / Cas9技术如何在活体内应用的途径有很多,包括交付方式。这些可能会引起不同的免疫途径。但是,与所有蛋白质治疗剂一样,可能需要在临床开发过程中监测抗Cas9抗体。这将需要开发强大而可靠的检测方法。在这里,我们描述了基于ELISA的检测方法,该检测方法能够检测人血清中来自金黄色葡萄球菌(SaCas9)和化脓链球菌(SpCas9)的Cas9抗体。此外,使用这些分析方法筛选200个人血清样品中预先存在的抗体,我们发现抗SaCas9和抗SpCas9抗体的患病率分别为10%和2.5%。

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