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在细胞因子风暴的微生理系统中,用 DS-IkL 减轻中性粒细胞迁移和心脏毒性。

Mitigating neutrophil trafficking and cardiotoxicity with DS-IkL in a microphysiological system of a cytokine storm.

机构信息

Department of Biomedical Engineering, University of California, Davis, 451 E. Health Sciences Drive, Room 2315, Davis, CA 95616, USA.

出版信息

Lab Chip. 2023 Jun 28;23(13):3050-3061. doi: 10.1039/d2lc01070d.

Abstract

A feature of severe COVID-19 is the onset of an acute and intense systemic inflammatory response referred to as the "cytokine storm". The cytokine storm is characterized by high serum levels of inflammatory cytokines and the subsequent transport of inflammatory cells to damaging levels in vital organs (, myocarditis). Immune trafficking and its effect on underlying tissues (, myocardium) are challenging to observe at a high spatial and temporal resolution in mouse models. In this study, we created a vascularized organ-on-a-chip system to mimic cytokine storm-like conditions and tested the effectiveness of a novel multivalent selectin-targeting carbohydrate conjugate (composed of DS - dermatan sulfate and IkL - a selectin-binding peptide, termed DS-IkL) in blocking infiltration of polymorphonuclear leukocytes (PMN). Our data shows that cytokine storm-like conditions induce endothelial cells to produce additional inflammatory cytokines and facilitate infiltration of PMNs into tissue. Treatment of tissues with DS-IkL (60 μM) reduced PMN accumulation in the tissue by >50%. We then created cytokine storm-like conditions in a vascularized cardiac tissue-chip and found that PMN infiltration increases the spontaneous beating rate of the cardiac tissue, and this effect is eliminated by treatment with DS-IkL (60 μM). In summary, we demonstrate the utility of an organ-on-a-chip platform to mimic COVID-19 related cytokine storm and that blocking leukocyte infiltration with DS-IkL could be a viable strategy to mitigate associated cardiac complications.

摘要

严重 COVID-19 的一个特征是急性和强烈的全身性炎症反应的发作,称为“细胞因子风暴”。细胞因子风暴的特征是炎症细胞因子的血清水平升高,随后炎症细胞向重要器官(如心肌炎)转移到损害水平。在小鼠模型中,免疫细胞的运输及其对潜在组织(如心肌)的影响很难在高时空分辨率下观察到。在这项研究中,我们创建了一个血管化的器官芯片系统来模拟细胞因子风暴样条件,并测试了一种新型多价选择素靶向碳水化合物缀合物(由 DS-硫酸皮肤素和 IkL-选择素结合肽组成,称为 DS-IkL)在阻断多形核白细胞(PMN)浸润中的有效性。我们的数据表明,细胞因子风暴样条件诱导内皮细胞产生额外的炎症细胞因子,并促进 PMN 渗透到组织中。用 DS-IkL(60 μM)处理组织可使组织中 PMN 的积累减少 >50%。然后,我们在血管化的心脏组织芯片中创建了细胞因子风暴样条件,发现 PMN 浸润会增加心脏组织的自发跳动率,而用 DS-IkL(60 μM)处理可消除这种作用。总之,我们证明了器官芯片平台模拟 COVID-19 相关细胞因子风暴的实用性,并且用 DS-IkL 阻断白细胞浸润可能是减轻相关心脏并发症的一种可行策略。

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