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层流切应力通过 TNFα 和 IL-1β 的激活引起内皮细胞 E-选择素表达模式的改变。

Laminar shear stress elicit distinct endothelial cell E-selectin expression pattern via TNFα and IL-1β activation.

机构信息

Department of Chemical Engineering, University of Michigan, Ann Arbor, Michigan 48109, USA.

出版信息

Biotechnol Bioeng. 2013 Mar;110(3):999-1003. doi: 10.1002/bit.24746. Epub 2012 Oct 18.

DOI:10.1002/bit.24746
PMID:23055258
Abstract

The ability to discriminate cell adhesion molecule expression between healthy and inflamed endothelium is critical for therapeutic intervention in many diseases. This study explores the effect of laminar flow on TNFα-induced E-selectin surface expression levels in human umbilical vein endothelial cells (HUVECs) relative to IL-1β-induced expression via flow chamber assays. HUVECs grown in static culture were either directly (naïve) activated with cytokine in the presence of laminar shear or pre-exposed to 12 h of laminar shear (shear-conditioned) prior to simultaneous shear and cytokine activation. Naïve cells activated with cytokine in static served as control. Depending on the cell shear history, fluid shear is found to differently affect TNFα-induced relative to IL-1β-induced HUVEC expression of E-selectin. Specifically, E-selectin surface expression by naïve HUVECs is enhanced in the 8-12 h activation time range with simultaneous exposure to shear and TNFα (shear-TNFα) relative to TNFα static control whereas enhanced E-selectin expression is observed in the 4-24 h range for shear-IL-1β treatment relative to IL-1β static control. While exposure of HUVECs to shear preconditioning mutes shear-TNFα-induced E-selectin expression, it enhances or down-regulates shear-IL-1β-induced expression dependent on the activation period. Under dual-cytokine-shear conditions, IL-1β signaling dominates. Overall, a better understanding of E-selectin expression pattern by human ECs relative to the combined interaction of cytokines, shear profile and history can help elucidate many disease pathologies.

摘要

区分健康和炎症内皮细胞细胞黏附分子表达的能力对于许多疾病的治疗干预至关重要。本研究通过流室实验探讨了层流对 TNFα 诱导的人脐静脉内皮细胞(HUVEC)表面 E-选择素表达水平相对于 IL-1β 诱导表达的影响。在静态培养中生长的 HUVEC 要么直接(初始)在层流剪切存在的情况下用细胞因子激活,要么在同时进行剪切和细胞因子激活之前预先暴露于 12 小时的层流剪切(剪切预处理)。用细胞因子在静态中激活的初始细胞作为对照。根据细胞剪切历史,发现流体剪切会以不同的方式影响 TNFα 诱导的相对于 IL-1β 诱导的 HUVEC 表达 E-选择素。具体而言,与 TNFα 静态对照相比,同时暴露于剪切和 TNFα 下(剪切-TNFα),初始 HUVEC 的 E-选择素表面表达在 8-12 小时的激活时间范围内增强,而剪切-IL-1β 处理在 4-24 小时的范围内观察到 E-选择素表达增强与 IL-1β 静态对照相比。尽管 HUVEC 暴露于剪切预处理会使剪切-TNFα 诱导的 E-选择素表达沉默,但它会增强或下调剪切-IL-1β 诱导的表达,具体取决于激活时间。在双重细胞因子-剪切条件下,IL-1β 信号占主导地位。总体而言,更好地了解人类 ECs 的 E-选择素表达模式相对于细胞因子、剪切谱和历史的综合相互作用,有助于阐明许多疾病病理。

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