来自自身免疫小鼠的抗多磷酸单克隆抗体

IF 3.4 3区 医学 Q2 HEMATOLOGY
Josepha C. Sedzro , Stephanie A. Smith , Alexander Scott , Yuqi Wang , Richard J. Travers , Rachel Hemp , Chase N. Morse , James H. Morrissey
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引用次数: 0

摘要

背景无机聚磷酸盐(polyPs)是一种线性磷酸盐链,可加速血液凝固。方法从自身免疫性 NZBWF1/J 雌性小鼠的脾脏细胞中制备杂交瘤,并筛选抗聚磷酸盐抗体。使用酶联免疫吸附试验和牵引试验对与 polyP 结合的抗体进行了进一步鉴定,并使用平板结合、表面等离子体共振和基于血浆的凝血试验对这些抗体进行了鉴定。在氯化铁诱导的小鼠颈动脉血栓形成模型中对抗血栓形成的潜力进行了评估。在分析这些抗多聚酶抗体时,我们发现分泌型白细胞肽酶抑制剂(SLPI)是这些抗体的常见杂质,而且 SLPI 与多聚酶结合。我们从纯化的免疫球蛋白 G 中定量去除 SLPI。PP2069 和 PP2099 免疫球蛋白 G 对多聚果糖都有很高的亲和力,但也与其他多聚阴离子(如 DNA、肝素和某些其他糖胺聚糖)结合,这表明其特异性有限。这两种抗体在体外都能抑制多聚酶引发的血浆凝结。然而,在小鼠血栓模型中进行体内试验时,PP2069 和 PP2099 都没有表现出明显的抗血栓作用。本文研究的两种抗多聚酶单克隆抗体不仅能与多聚酶产生高亲和力,还能与 DNA 和肝素产生交叉反应。这两种抗体都不能在小鼠模型中防止血栓形成,但它们在体外研究多聚酶时可能会有一些用处。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Antipolyphosphate monoclonal antibodies derived from autoimmune mice

Background

Inorganic polyphosphates (polyPs) are linear chains of phosphates that accelerate blood clotting. Targeting polyP in vivo has been shown to reduce thrombosis.

Objectives

To identify and characterize anti-polyP monoclonal antibodies that could be used as analytical tools and as antithrombotic agents.

Methods

Hybridomas were prepared from spleen cells from autoimmune NZBWF1/J female mice and screened for anti-polyP antibodies. Antibodies that bound polyP using enzyme-linked immunosorbent assay and pull-down assays were further characterized with plate binding, surface plasmon resonance, and plasma-based clotting assays. Antithrombotic potential was evaluated in a murine ferric chloride–induced carotid artery thrombosis model.

Results

Of 4 antibodies that bound polyP in our pull-down assay, 2 (PP2069 and PP2099) were available for further characterization. While analyzing these anti-polyP antibodies, we found secretory leukocyte peptidase inhibitor (SLPI) to be a common contaminant of these antibodies and that SLPI binds polyP. We removed SLPI quantitatively from our purified immunoglobulin G. Both PP2069 and PP2099 immunoglobulin G displayed high affinity for polyP but also bound to other polyanions such as DNA, heparin, and certain other glycosaminoglycans, indicating limited specificity. Both antibodies inhibited polyP-initiated plasma clotting in vitro. When tested in vivo in a mouse thrombosis model, however, neither PP2069 nor PP2099 exhibited a significant antithrombotic effect.

Conclusion

Autoimmune mice spontaneously produce antibodies against polyP. The 2 examples of anti-polyP monoclonal antibodies studied here not only bound to polyP with high affinity but also cross-reacted with DNA and heparin. Neither antibody protected against thrombosis in a mouse model, but they might have some utility for in vitro studies of polyP.

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来源期刊
CiteScore
5.60
自引率
13.00%
发文量
212
审稿时长
7 weeks
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