Endothelial cell apicobasal polarity coordinates distinct responses to luminally versus abluminally delivered TNF-α in a microvascular mimetic.

IF 1.5 4区生物学 Q4 CELL BIOLOGY

Integrative Biology Pub Date : 2020-11-18 DOI:10.1093/intbio/zyaa022

Alec T Salminen, Jeffrey Tithof, Yara Izhiman, Elysia A Masters, Molly C McCloskey, Thomas R Gaborski, Douglas H Kelley, Anthony P Pietropaoli, Richard E Waugh, James L McGrath

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引用次数: 7

Abstract

Endothelial cells (ECs) are an active component of the immune system and interact directly with inflammatory cytokines. While ECs are known to be polarized cells, the potential role of apicobasal polarity in response to inflammatory mediators has been scarcely studied. Acute inflammation is vital in maintaining healthy tissue in response to infection; however, chronic inflammation can lead to the production of systemic inflammatory cytokines and deregulated leukocyte trafficking, even in the absence of a local infection. Elevated levels of cytokines in circulation underlie the pathogenesis of sepsis, the leading cause of intensive care death. Because ECs constitute a key barrier between circulation (luminal interface) and tissue (abluminal interface), we hypothesize that ECs respond differentially to inflammatory challenge originating in the tissue versus circulation as in local and systemic inflammation, respectively. To begin this investigation, we stimulated ECs abluminally and luminally with the inflammatory cytokine tumor necrosis factor alpha (TNF-α) to mimic a key feature of local and systemic inflammation, respectively, in a microvascular mimetic (μSiM-MVM). Polarized IL-8 secretion and polymorphonuclear neutrophil (PMN) transmigration were quantified to characterize the EC response to luminal versus abluminal TNF-α. We observed that ECs uniformly secrete IL-8 in response to abluminal TNF-α and is followed by PMN transmigration. The response to abluminal treatment was coupled with the formation of ICAM-1-rich membrane ruffles on the apical surface of ECs. In contrast, luminally stimulated ECs secreted five times more IL-8 into the luminal compartment than the abluminal compartment and sequestered PMNs on the apical EC surface. Our results identify clear differences in the response of ECs to TNF-α originating from the abluminal versus luminal side of a monolayer for the first time and may provide novel insight into future inflammatory disease intervention strategies.

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内皮细胞顶基底极性协调了在微血管模拟物中对发光或不发光递送TNF-α的不同反应。

内皮细胞(ECs)是免疫系统的活性成分，直接与炎症细胞因子相互作用。虽然已知内皮细胞是极化细胞，但对顶基底极性在炎症介质反应中的潜在作用几乎没有研究。急性炎症对于维持健康组织以应对感染至关重要;然而，即使在没有局部感染的情况下，慢性炎症也会导致全身炎症细胞因子的产生和白细胞运输的失调。血液循环中细胞因子水平升高是脓毒症发病机制的基础，脓毒症是重症监护死亡的主要原因。由于内皮细胞构成循环(腔内界面)和组织(腔内界面)之间的关键屏障，我们假设内皮细胞对来自组织和循环的炎症挑战的反应不同，分别是局部和全身炎症。为了开始这项研究，我们在微血管模拟(μSiM-MVM)中分别用炎症细胞因子肿瘤坏死因子α (TNF-α)在光照和光照下刺激ECs，以模拟局部和全身炎症的关键特征。我们量化了极化IL-8分泌和多形核中性粒细胞(PMN)的迁移，以表征EC对腔内TNF-α的反应。我们观察到ECs均匀地分泌IL-8以响应腔内TNF-α，然后是PMN转运。对腹腔处理的反应伴随着在内皮细胞顶端表面形成富含icam -1的膜褶。相比之下，光刺激的内皮细胞向腔室分泌的IL-8是腔室的5倍，并将pmn隔离在内皮细胞的顶端表面。我们的研究结果首次明确了内皮细胞对来自单层管腔侧和来自单层管腔侧的TNF-α的反应存在明显差异，并可能为未来炎症疾病干预策略提供新的见解。

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

Integrative Biology 生物-细胞生物学

CiteScore

4.90

自引率

0.00%

发文量

审稿时长

1 months

期刊介绍： Integrative Biology publishes original biological research based on innovative experimental and theoretical methodologies that answer biological questions. The journal is multi- and inter-disciplinary, calling upon expertise and technologies from the physical sciences, engineering, computation, imaging, and mathematics to address critical questions in biological systems. Research using experimental or computational quantitative technologies to characterise biological systems at the molecular, cellular, tissue and population levels is welcomed. Of particular interest are submissions contributing to quantitative understanding of how component properties at one level in the dimensional scale (nano to micro) determine system behaviour at a higher level of complexity. Studies of synthetic systems, whether used to elucidate fundamental principles of biological function or as the basis for novel applications are also of interest.