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亚砷酸盐暴露于人肾近端小管细胞(HRPT)可产生可逆转的上皮间质转化(EMT):体内外研究。

Arsenite Exposure to Human RPCs (HRTPT) Produces a Reversible Epithelial Mesenchymal Transition (EMT): In-Vitro and In-Silico Study.

机构信息

Department of Pathology, School of Medicine and Health Sciences, University of North Dakota, Grand Forks, ND 58203, USA.

Department of Biomedical Engineering, School of Electrical Engineering and Computer Science, University of North Dakota, Grand Forks, ND 58203, USA.

出版信息

Int J Mol Sci. 2023 Mar 7;24(6):5092. doi: 10.3390/ijms24065092.

Abstract

The human kidney is known to possess renal progenitor cells (RPCs) that can assist in the repair of acute tubular injury. The RPCs are sparsely located as single cells throughout the kidney. We recently generated an immortalized human renal progenitor cell line (HRTPT) that co-expresses PROM1/CD24 and expresses features expected on RPCs. This included the ability to form nephrospheres, differentiate on the surface of Matrigel, and undergo adipogenic, neurogenic, and osteogenic differentiation. These cells were used in the present study to determine how the cells would respond when exposed to nephrotoxin. Inorganic arsenite (iAs) was chosen as the nephrotoxin since the kidney is susceptible to this toxin and there is evidence of its involvement in renal disease. Gene expression profiles when the cells were exposed to iAs for 3, 8, and 10 passages (subcultured at 1:3 ratio) identified a shift from the control unexposed cells. The cells exposed to iAs for eight passages were then referred with growth media containing no iAs and within two passages the cells returned to an epithelial morphology with strong agreement in differential gene expression between control and cells recovered from iAs exposure. Results show within three serial passages of the cells exposed to iAs there was a shift in morphology from an epithelial to a mesenchymal phenotype. EMT was suggested based on an increase in known mesenchymal markers. We found RPCs can undergo EMT when exposed to a nephrotoxin and undergo MET when the agent is removed from the growth media.

摘要

已知人类肾脏中存在肾祖细胞(RPCs),它们可以帮助修复急性肾小管损伤。这些 RPC 作为单个细胞稀疏地分布在整个肾脏中。我们最近生成了一种永生化的人类肾祖细胞系(HRTPT),该细胞系共同表达 PROM1/CD24,并表现出预期的 RPC 特征。这包括形成肾小体、在 Matrigel 表面分化以及进行脂肪生成、神经生成和成骨分化的能力。这些细胞在本研究中用于确定当它们暴露于肾毒素时会如何反应。选择无机砷酸盐(iAs)作为肾毒素,因为肾脏容易受到这种毒素的影响,并且有证据表明它参与了肾脏疾病。当细胞暴露于 iAs 3、8 和 10 个传代(以 1:3 的比例传代)时,基因表达谱发生了变化,与未暴露于 iAs 的对照细胞相比发生了变化。然后,将暴露于 iAs 的细胞用不含 iAs 的生长培养基孵育,在两个传代内,细胞恢复到上皮形态,与从 iAs 暴露中恢复的对照细胞的差异基因表达具有强烈的一致性。结果表明,在暴露于 iAs 的细胞连续传代三次内,形态从上皮样向间充质表型发生转变。基于已知的间充质标志物的增加,提示 EMT。我们发现,当 RPC 暴露于肾毒素时,它们可以经历 EMT,当从生长培养基中去除该试剂时,它们可以经历 MET。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1934/10048886/efe8255e7deb/ijms-24-05092-g001.jpg

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