嵌入式巨噬细胞在三维芯片血管中诱导血管内凝血

IF 3 4区 医学 Q3 ENGINEERING, BIOMEDICAL Biomedical Microdevices Pub Date : 2023-12-12 DOI:10.1007/s10544-023-00684-w
H.H.T. Middelkamp, H.J. Weener, T. Gensheimer, K. Vermeul, L.E. de Heus, H.J. Albers, A. van den Berg, A.D. van der Meer
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引用次数: 0

摘要

巨噬细胞是一种先天性免疫细胞,可预防感染并帮助伤口愈合和血管发炎。虽然这些细胞是天然的辅助细胞,但它们也会导致慢性疾病,例如在动脉粥样硬化早期浸润血管内皮层和促进血管炎症。炎症途径与血小板和内皮细胞等血栓形成的主要参与者之间存在相互影响,这种现象被称为 "血栓炎症"。人们对嵌入的巨噬细胞在血管疾病血栓炎症中的作用尚不完全了解。芯片血管是一种微流控血管细胞培养模型,已被广泛用于研究血管疾病的各个方面,如通透性、免疫细胞粘附和血栓形成。片上血管模型中的血液灌流试验得益于该模型的多个独特方面,如控制微血管结构和明确的流动模式,以及进行实时成像的能力。然而,由于其简化的性质,芯片上血管模型尚未用于捕捉血栓炎症中重要的复杂细胞串联。我们利用诱导多能干细胞衍生的内皮细胞和极化的 THP-1 单核细胞,开发并系统地建立了嵌入(脂质)巨噬细胞的三维芯片上血管。我们为这些三维芯片血管建立了人体全血灌注试验。在含有脂质巨噬细胞的片上血管模型中,我们观察到纤维蛋白沉积增加。我们预计这种先进的体外血管模型未来将用于早期动脉粥样硬化或其他血管疾病的药物开发。
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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Embedded macrophages induce intravascular coagulation in 3D blood vessel-on-chip

Macrophages are innate immune cells that prevent infections and help in wound healing and vascular inflammation. While these cells are natural helper cells, they also contribute to chronic diseases, e.g., by infiltrating the endothelial layer in early atherosclerosis and by promoting vascular inflammation. There is a crosstalk between inflammatory pathways and key players in thrombosis, such as platelets and endothelial cells – a phenomenon known as ‘thromboinflammation’. The role of the embedded macrophages in thromboinflammation in the context of vascular disease is incompletely understood. Blood vessels-on-chips, which are microfluidic vascular cell culture models, have been used extensively to study aspects of vascular disease, like permeability, immune cell adhesion and thrombosis. Blood perfusion assays in blood vessel-on-chip models benefit from multiple unique aspects of the models, such as control of microvessel structure and well-defined flow patterns, as well as the ability to perform live imaging. However, due to their simplified nature, blood vessels-on-chip models have not yet been used to capture the complex cellular crosstalk that is important in thromboinflammation. Using induced pluripotent stem cell-derived endothelial cells and polarized THP-1 monocytes, we have developed and systematically set up a 3D blood vessel-on-chip with embedded (lipid-laden) macrophages, which is created using sequential cell seeding in viscous finger patterned collagen hydrogels. We have set up a human whole blood perfusion assay for these 3D blood vessels-on-chip. An increased deposition of fibrin in the blood vessel-on-chip models containing lipid-laden macrophages was observed. We anticipate the future use of this advanced vascular in vitro model in drug development for early atherosclerosis or aspects of other vascular diseases.

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来源期刊
Biomedical Microdevices
Biomedical Microdevices 工程技术-工程:生物医学
CiteScore
6.90
自引率
3.60%
发文量
32
审稿时长
6 months
期刊介绍: Biomedical Microdevices: BioMEMS and Biomedical Nanotechnology is an interdisciplinary periodical devoted to all aspects of research in the medical diagnostic and therapeutic applications of Micro-Electro-Mechanical Systems (BioMEMS) and nanotechnology for medicine and biology. General subjects of interest include the design, characterization, testing, modeling and clinical validation of microfabricated systems, and their integration on-chip and in larger functional units. The specific interests of the Journal include systems for neural stimulation and recording, bioseparation technologies such as nanofilters and electrophoretic equipment, miniaturized analytic and DNA identification systems, biosensors, and micro/nanotechnologies for cell and tissue research, tissue engineering, cell transplantation, and the controlled release of drugs and biological molecules. Contributions reporting on fundamental and applied investigations of the material science, biochemistry, and physics of biomedical microdevices and nanotechnology are encouraged. A non-exhaustive list of fields of interest includes: nanoparticle synthesis, characterization, and validation of therapeutic or imaging efficacy in animal models; biocompatibility; biochemical modification of microfabricated devices, with reference to non-specific protein adsorption, and the active immobilization and patterning of proteins on micro/nanofabricated surfaces; the dynamics of fluids in micro-and-nano-fabricated channels; the electromechanical and structural response of micro/nanofabricated systems; the interactions of microdevices with cells and tissues, including biocompatibility and biodegradation studies; variations in the characteristics of the systems as a function of the micro/nanofabrication parameters.
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