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肾小球肾炎药物疗效测试平台的开发

Development of Drug Efficacy Testing Platform for Glomerulonephritis.

作者信息

Kwon Eun-Jeong, Choi Yunyeong, Kim Shin Young, Park Seokwoo, Yun Giae, Min Sei Hong, Kim Sejoong

机构信息

Department of Internal Medicine, Seoul National University Bundang Hospital, Seongnam-si 13620, Republic of Korea.

Department of Internal Medicine, Seoul National University College of Medicine, Seoul 03080, Republic of Korea.

出版信息

Micromachines (Basel). 2024 Feb 24;15(3):317. doi: 10.3390/mi15030317.

Abstract

We developed a 3D glomeruli tissue chip for glomerulonephritis (GN) testing, featuring a gravity-driven glomerular filtration barrier (GFB) with human podocytes and endothelial cells with a bidirectional flow in the bottom channel. Using puromycin-induced GN, we observed decreased cell viability, increased albumin permeability, and reduced WT1 and nephrin compared to the normal GFB. Tacrolimus restored cell viability, reduced albumin permeability, and increased WT1 expression. Using serum from five membranous nephropathy (MN) patients, we created MN models using a GFB-mimicking chip. A notable decline in cell viability was observed in the serum-induced MN1 and MN2 models. However, tacrolimus restored it. Albumin permeability was reduced in the MN1, MN2, and MN5 models by tacrolimus treatment. MN1 displayed the best clinical response to tacrolimus, exhibiting increased expression of WT1 in chip-based evaluations after tacrolimus treatment. We successfully evaluated the efficacy of tacrolimus using puromycin-induced and serum-induced GN models on a chip that mimicked the structure and function of the GFB. The GFB-mimicking chip holds promise as a personalized platform for assessing drug efficacy using patient serum samples.

摘要

我们开发了一种用于肾小球肾炎(GN)检测的3D肾小球组织芯片,其特点是具有重力驱动的肾小球滤过屏障(GFB),带有人类足细胞和内皮细胞,底部通道有双向流动。使用嘌呤霉素诱导的GN,我们观察到与正常GFB相比,细胞活力下降、白蛋白通透性增加以及WT1和nephrin减少。他克莫司恢复了细胞活力,降低了白蛋白通透性,并增加了WT1表达。使用来自五名膜性肾病(MN)患者的血清,我们使用模拟GFB的芯片创建了MN模型。在血清诱导的MN1和MN2模型中观察到细胞活力显著下降。然而,他克莫司使其恢复。通过他克莫司治疗,MN1、MN2和MN5模型中的白蛋白通透性降低。MN1对他克莫司表现出最佳临床反应,在他克莫司治疗后的芯片评估中WT1表达增加。我们在模拟GFB结构和功能的芯片上,使用嘌呤霉素诱导和血清诱导的GN模型成功评估了他克莫司的疗效。模拟GFB的芯片有望成为使用患者血清样本评估药物疗效的个性化平台。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5eca/10971927/90548795d0f8/micromachines-15-00317-g001.jpg

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