Induced pluripotent stem cells model personalized variations in liver disease resulting from α1-antitrypsin deficiency.
Edgar N TafalengSouvik ChakrabortyBing HanPamela HaleWanquan WuAlejandro Soto-GutierrezCarol A Feghali-BostwickAndrew A WilsonDarrell N KottonMasaki NagayaStephen C StromJayanta Roy-ChowdhuryDonna B StolzDavid H PerlmutterIra J FoxPublished in: Hepatology (Baltimore, Md.) (2015)
iHeps model the individual disease phenotypes of ATD patients with more rapid degradation of misfolded ATZ and lack of globular inclusions in cells from patients who have escaped liver disease. The results support the concept that "proteostasis" mechanisms, such as intracellular degradation pathways, play a role in observed variations in clinical phenotype and show that iPSCs can potentially be used to facilitate predictions of disease susceptibility for more precise and timely application of therapeutic strategies.