AI Article Synopsis

  • The kidney's tubular epithelium can suffer damage from various factors, including immune disorders and nephrotoxins, making it essential to explore reliable cell models for research.
  • Primary renal epithelial cells are limited in their ability to model kidney diseases that originate during embryonic development, highlighting the need for better cellular systems.
  • Induced pluripotent stem cells (iPSCs), which can differentiate into any cell type, can be created from kidney cells using just two transcription factors, allowing for improved disease modeling and drug testing for kidney-related conditions.

Article Abstract

The tubular epithelium of the kidney is susceptible to injury from a number of different causes, including inflammatory and immune disorders, oxidative stress, and nephrotoxins, among others. Primary renal epithelial cells remain one of the few tools for studying the biochemical and physiological characteristics of the renal tubular system. Nevertheless, differentiated primary cells are not suitable for recapitulation of disease properties that might arise during embryonic kidney formation and further maturation. Thus, cellular systems resembling kidney characteristics are in urgent need to model disease as well as to establish reliable drug-testing platforms. Induced pluripotent stem cells (iPSCs) bear the capacity to differentiate into every cell lineage comprising the adult organism. Thus, iPSCs bring the possibility for recapitulating embryonic development by directed differentiation into specific lineages. iPSC differentiation ultimately allows for both disease modeling in vitro and the production of cellular products with potential for regenerative medicine. Here, we describe the rapid, reproducible, and highly efficient generation of iPSCs derived from endogenous kidney tubular renal epithelial cells with only two transcriptional factors, OCT4 and SOX2. Kidney-derived iPSCs may provide a reliable cellular platform for the development of kidney differentiation protocols allowing drug discovery studies and the study of kidney pathology.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3397840PMC
http://dx.doi.org/10.1074/jbc.M112.350413DOI Listing

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