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Screening Assays to Characterize Novel Endothelial Regulators Involved in the Inflammatory Response

机译:筛选测定法表征涉及炎症反应的新型内皮调节剂

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摘要

The endothelial layer is essential for maintaining homeostasis in the body by controlling many different functions. Regulation of the inflammatory response by the endothelial layer is crucial to efficiently fight against harmful inputs and aid in the recovery of damaged areas. When the endothelial cells are exposed to an inflammatory environment, such as the outer component of gram-negative bacteria membrane, lipopolysaccharide (LPS), they express soluble pro-inflammatory cytokines, such as Ccl5, Cxcl1 and Cxcl10, and trigger the activation of circulating leukocytes. In addition, the expression of adhesion molecules E-selectin, VCAM-1 and ICAM-1 on the endothelial surface enables the interaction and adhesion of the activated leukocytes to the endothelial layer, and eventually the extravasation towards the inflamed tissue. In this scenario, the endothelial function must be tightly regulated because excessive or defective activation in the leukocyte recruitment could lead to inflammatory-related disorders. Since many of these disorders do not have an effective treatment, novel strategies with a focus on the vascular layer must be investigated. We propose comprehensive assays that are useful to the search of novel endothelial regulators that modify leukocyte function. We analyze endothelial activation by using specific expression targets involved in leukocyte recruitment (such as, cytokines, chemokines, and adhesion molecules) with several techniques, including: real-time quantitative polymerase chain reaction (RT-qPCR), western-blot, flow cytometry and adhesion assays. These approaches determine endothelial function in the inflammatory context and are very useful to perform screening assays to characterize novel endothelial inflammatory regulators that are potentially valuable for designing new therapeutic strategies.
机译:内皮层是通过控制许多不同功能来维持体内动态平衡所必需的。内皮层对炎症反应的调节对于有效抵抗有害输入并帮助恢复受损区域至关重要。当内皮细胞暴露于炎性环境(例如革兰氏阴性细菌膜的外部成分,脂多糖)时,它们会表达可溶性促炎性细胞因子,例如Ccl5,Cxcl1和Cxcl10,并触发循环的激活。白细胞。另外,在内皮表面上粘附分子E-选择蛋白,VCAM-1和ICAM-1的表达使得活化的白细胞与内皮层相互作用和粘附,并最终向发炎组织外渗。在这种情况下,必须严格调节内皮功能,因为白细胞募集的过度激活或缺陷激活可能导致炎症相关疾病。由于许多这些疾病没有有效的治疗方法,因此必须研究针对血管层的新策略。我们提出了全面的检测方法,可用于寻找可修改白细胞功能的新型内皮调节剂。我们使用几种技术,通过参与白细胞募集的特定表达靶标(例如细胞因子,趋化因子和粘附分子)来分析内皮激活,这些技术包括:实时定量聚合酶链反应(RT-qPCR),蛋白质印迹,流式细胞仪和粘附测定。这些方法确定了炎性背景下的内皮功能,对于进行筛选试验以表征新型内皮炎性调节剂非常有用,这些新型调节剂对于设计新的治疗策略可能具有潜在价值。

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