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An integrated adipose-tissue-on-chip nanoplasmonic biosensing platform for investigating obesity-associated inflammation

机译:一种用于研究肥胖相关炎症的芯片组织片内纳米型纳米型膨胀平台

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摘要

Although many advanced biosensing techniques have been proposed for cytokine profiling, there are no clinically available methods that integrate high-resolution immune cell monitoring and in situ multiplexed cytokine detection together in a biomimetic tissue microenvironment. The primary challenge arises due to the lack of suitable label-free sensing techniques and difficulty for sensor integration. In this work, we demonstrated a novel integration of a localized-surface plasmon resonance (LSPR)-based biosensor with a biomimetic microfluidic 'adipose-tissue-on-chip' platform for an in situ label-free, high-throughput and multiplexed cytokine secretion analysis of obese adipose tissue. Using our established adipose-tissue-on-chip platform, we were able to monitor the adipose tissue initiation, differentiation, and maturation and simulate the hallmark formation of crown-like structures (CLSs) during pro-inflammatory stimulation. With integrated antibody-conjugated LSPR barcode sensor arrays, our platform enables simultaneous multiplexed measurements of pro-inflammatory (IL-6 and TNF-alpha) and anti-inflammatory (IL-10 and IL-4) cytokines secreted by the adipocytes and macrophages. As a result, our adipose-tissue-on-chip platform is capable of identifying stage-specific cytokine secretion profiles from a complex milieu during obesity progression, highlighting its potential as a high-throughput preclinical readout for personalized obesity treatment strategies.
机译:虽然已经提出了许多先进的生物腐蚀性技术用于细胞因子分析,但没有临床上可用的方法,其将高分辨率免疫细胞监测和在仿生组织微环境中聚合在一起。由于缺乏合适的无标签传感技术和传感器集成难度,主要挑战产生。在这项工作中,我们展示了局部表面等离子体共振(LSPR)的生物传感器与仿生微流体的“脂肪组织片”平台的新型集成,用于原位标记,高通量和多重细胞因子肥胖脂肪组织的分泌分析。使用我们建立的脂肪组织片上平台,我们能够在促炎症刺激期间监测脂肪组织起始,分化和成熟,并模拟冠状结构(CLSS)的标志性形成。通过集成的抗体缀合的LSPR条形码传感器阵列,我们的平台可以同时复用测量由脂肪细胞和巨噬细胞分泌的促炎(IL-6和TNF-α)和抗炎(IL-10和IL-4)细胞因子。结果,我们的脂肪组织片上平台能够在肥胖进展期间从复杂的Milieu鉴定特异性细胞因子分泌物,突出显示其作为个性化肥胖治疗策略的高通量临床前读数。

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