Inflammatory Non-CpG Antisense Oligonucleotides Are Signaling Through TLR9 in Human Burkitt Lymphoma B Bjab Cells.

IF 4 2区 医学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
Adam J Pollak, Patrick Cauntay, Todd Machemer, Suzanne Paz, Sagar Damle, Scott P Henry, Sebastien A Burel
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引用次数: 3

Abstract

Nucleic acid-based phosphorothioate containing antisense oligonucleotides (PS-ASOs) have the potential to activate cellular innate immune responses, and the level of activation can vary quite dramatically with sequence. Minimizing the degree of proinflammatory effect is one of the main selection criteria for compounds intended to move into clinical trials. While a recently developed human peripheral blood mononuclear cell (hPBMC)-based assay showed excellent ability to detect innate immune active PS-ASOs, which can then be discarded from the developmental process, this assay is highly resource intensive and easily affected by subject variability. This compelled us to develop a more convenient high-throughput assay. In this study, we describe a new in vitro assay, utilizing a cultured human Bjab cell line, which was developed and validated to identify PS-ASOs that may cause innate immune activation. The assay was calibrated to replicate results from the hPBMC assay. The Bjab assay was designed to be high throughput and more convenient by using RT-qPCR readout of mRNA of the chemokine Ccl22. The Bjab assay was also shown to be highly reproducible and to provide a large dynamic range in determining the immune potential of PS-ASOs through comparison to known benchmark PS-ASO controls that were previously shown to be safe or inflammatory in clinical trials. In addition, we demonstrate that Bjab cells can be used to provide mechanistic information on PS-ASO TLR9-dependent innate immune activation.

炎症性非cpg反义寡核苷酸在人伯基特淋巴瘤Bjab细胞中通过TLR9信号传导
含有反义寡核苷酸的核酸基硫代磷酸酯(PS-ASOs)具有激活细胞先天免疫应答的潜力,其激活水平随序列的变化而变化。将促炎作用的程度降到最低是化合物进入临床试验的主要选择标准之一。虽然最近开发的基于人外周血单个核细胞(hbmc)的检测显示出出色的检测先天免疫活性ps - aso的能力,然后可以从发育过程中丢弃,但这种检测是高度资源密集型的,容易受到受试者差异的影响。这迫使我们开发一种更方便的高通量测定方法。在这项研究中,我们描述了一种新的体外实验,利用培养的人Bjab细胞系,开发并验证了鉴定可能导致先天免疫激活的PS-ASOs。校准该测定以复制hPBMC测定的结果。通过RT-qPCR读取趋化因子Ccl22的mRNA, Bjab检测具有高通量和更方便的特点。Bjab试验还被证明具有高度可重复性,并通过与已知的PS-ASO基准对照进行比较,在确定PS-ASO的免疫潜力方面提供了很大的动态范围,这些对照在临床试验中被证明是安全的或具有炎症性的。此外,我们证明Bjab细胞可用于提供PS-ASO tlr9依赖性先天免疫激活的机制信息。
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来源期刊
Nucleic acid therapeutics
Nucleic acid therapeutics BIOCHEMISTRY & MOLECULAR BIOLOGY-CHEMISTRY, MEDICINAL
CiteScore
7.60
自引率
7.50%
发文量
47
审稿时长
>12 weeks
期刊介绍: Nucleic Acid Therapeutics is the leading journal in its field focusing on cutting-edge basic research, therapeutic applications, and drug development using nucleic acids or related compounds to alter gene expression. The Journal examines many new approaches for using nucleic acids as therapeutic agents or in modifying nucleic acids for therapeutic purposes including: oligonucleotides, gene modification, aptamers, RNA nanoparticles, and ribozymes.
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