Phagocytosed Polyhedrin-Cytokine Cocrystal Nanoparticles Provide Sustained Secretion of Bioactive Cytokines from Macrophages.

Q2 Agricultural and Biological Sciences
生物设计研究(英文) Pub Date : 2021-05-14 eCollection Date: 2021-01-01 DOI:10.34133/2021/9816485
Astrid Wendler, Nicholas James, Michael H Jones, Christian Pernstich
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引用次数: 4

Abstract

Many cells possess the ability to engulf and incorporate particles by phagocytosis. This active process is characteristic of microorganisms as well as higher order species. In mammals, monocytes, macrophages, and microglia are among the so-called professional phagocytes. In addition, cells such as fibroblast and chondrocytes are classified as nonprofessional phagocytes. Professional phagocytes play important roles in both the innate and adaptive immune responses, wound healing, and tissue homeostasis. Consequently, these cells are increasingly studied as targets and vectors of therapeutic intervention to treat a range of diseases. Professional phagocytes are notoriously difficult to transfect limiting their study and manipulation. Consequently, efforts have shifted towards the development of nanoparticles to deliver a cargo to phagocytic cells via phagocytosis. However, this approach carries significant technical challenges, particularly for protein cargos. We have focused on the development of nanoscale cocrystalline protein depots, known as PODS®, that contain protein cargos, including cytokines. Here, we show that PODS are readily phagocytosed by nonprofessional as well as professional phagocytic cells and have attributes, such as highly sustained release of cargo, that suggest potential utility for the study and exploitation of phagocytic cells for drug delivery. Monocytes and macrophages that ingest PODS retain normal characteristics including a robust chemotactic response. Moreover, the PODS-cytokine cargo is secreted by the loaded cell at a level sufficient to modulate the behavior of surrounding nonphagocytic cells. The results presented here demonstrate the potential of PODS nanoparticles as a novel molecular tool for the study and manipulation of phagocytic cells and for the development of Trojan horse immunotherapy strategies to treat cancer and other diseases.

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吞噬细胞的多角体细胞因子共晶纳米粒子提供从巨噬细胞中持续分泌生物活性细胞因子。
许多细胞具有通过吞噬作用吞噬和结合颗粒的能力。这种活性过程是微生物和高等物种的特征。在哺乳动物中,单核细胞、巨噬细胞和小胶质细胞属于所谓的专业吞噬细胞。此外,成纤维细胞和软骨细胞等细胞被归类为非专业吞噬细胞。专业吞噬细胞在先天和适应性免疫反应、伤口愈合和组织稳态中发挥着重要作用。因此,这些细胞越来越多地被研究为治疗一系列疾病的治疗干预的靶点和载体。众所周知,专业吞噬细胞很难转染,限制了它们的研究和操作。因此,努力转向开发纳米颗粒,通过吞噬作用将货物输送到吞噬细胞。然而,这种方法带来了重大的技术挑战,尤其是对于蛋白质货物。我们专注于开发纳米级共晶蛋白质库,称为PODS®,含有蛋白质货物,包括细胞因子。在这里,我们发现PODS很容易被非专业和专业吞噬细胞吞噬,并且具有高度持续释放货物等特性,这表明其在研究和开发吞噬细胞用于药物递送方面具有潜在的实用性。摄取PODS的单核细胞和巨噬细胞保持正常特征,包括强大的趋化反应。此外,负载细胞以足以调节周围非吞噬细胞行为的水平分泌PODS细胞因子货物。本文的结果证明了PODS纳米颗粒作为一种新型分子工具的潜力,可用于研究和操纵吞噬细胞,并开发治疗癌症和其他疾病的特洛伊木马免疫疗法策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
3.90
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0.00%
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