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Renal carcinoma/kidney progenitor cell chimera organoid as a novel tumorigenesis gene discovery model. | LitMetric

Renal carcinoma/kidney progenitor cell chimera organoid as a novel tumorigenesis gene discovery model.

Dis Model Mech

Biocenter Oulu, Laboratory of Developmental Biology, InfoTech Oulu, Center for Cell Matrix Research, Faculty of Biochemistry and Molecular Medicine, Oulu University, FI-90014 Oulu, Finland

Published: December 2017

AI Article Synopsis

  • - The study focuses on using 3D organoids, specifically renal organoids, to better model and understand kidney cancer by comparing gene profiles from embryonic mouse tissue and tumor biopsies from kidney cancer patients.
  • - Researchers identified specific genes related to kidney development and cancer that affect cell migration and viability when silenced, using siRNA techniques on renal cell carcinoma (RCC) cells.
  • - Findings suggest that combining kidney tissue with cancer cells in 3D organoids helps reveal how cancer cells impact kidney tissue development, indicating potential for new gene screens related to kidney cancer and improved modeling of tumor behaviors.

Article Abstract

Three-dimensional (3D) organoids provide a new way to model various diseases, including cancer. We made use of recently developed kidney-organ-primordia tissue-engineering technologies to create novel renal organoids for cancer gene discovery. We then tested whether our novel assays can be used to examine kidney cancer development. First, we identified the transcriptomic profiles of quiescent embryonic mouse metanephric mesenchyme (MM) and of MM in which the nephrogenesis program had been induced The transcriptome profiles were then compared to the profiles of tumor biopsies from renal cell carcinoma (RCC) patients, and control samples from the same kidneys. Certain signature genes were identified that correlated in the developmentally induced MM and RCC, including components of the caveolar-mediated endocytosis signaling pathway. An efficient siRNA-mediated knockdown (KD) of , , , , , or gene expression was achieved in mouse RCC (Renca) cells. The live-cell imaging analysis revealed inhibition of cell migration and cell viability in the gene-KD Renca cells in comparison to Renca controls. Upon siRNA treatment, the transwell invasion capacity of Renca cells was also inhibited. Finally, we mixed E11.5 MM with yellow fluorescent protein (YFP)-expressing Renca cells to establish chimera organoids. Strikingly, we found that the , and -KD Renca-YFP+ cells as a chimera with the MM in 3D organoid rescued, in part, the RCC-mediated inhibition of the nephrogenesis program during epithelial tubules formation. Altogether, our research indicates that comparing renal ontogenesis control genes to the genes involved in kidney cancer may provide new growth-associated gene screens and that 3D RCC-MM chimera organoids can serve as a novel model with which to investigate the behavioral roles of cancer cells within the context of emergent complex tissue structures.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5769601PMC
http://dx.doi.org/10.1242/dmm.028332DOI Listing

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