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Eckert, Christoph; Kim, Yong Ook; Julich, Henrike; Heier, Eva-Carina; Klein, Niklas; Krause, Elmar; Tschernig, Thomas; Kornek, Miroslaw; Lammert, Frank; Schuppan, Detlef; Lukacs-Kornek, Veronika

Podoplanin discriminates distinct stromal cell populations and a novel progenitor subset in the liver

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  • Medientyp: E-Artikel
  • Titel: Podoplanin discriminates distinct stromal cell populations and a novel progenitor subset in the liver
  • Beteiligte: Eckert, Christoph; Kim, Yong Ook; Julich, Henrike; Heier, Eva-Carina; Klein, Niklas; Krause, Elmar; Tschernig, Thomas; Kornek, Miroslaw; Lammert, Frank; Schuppan, Detlef; Lukacs-Kornek, Veronika
  • Erschienen: American Physiological Society, 2016
  • Erschienen in: American Journal of Physiology-Gastrointestinal and Liver Physiology, 310 (2016) 1, Seite G1-G12
  • Sprache: Englisch
  • DOI: 10.1152/ajpgi.00344.2015
  • ISSN: 0193-1857; 1522-1547
  • Entstehung:
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  • Beschreibung: Podoplanin/gp38+ stromal cells present in lymphoid organs play a central role in the formation and reorganization of the extracellular matrix and in the functional regulation of immune responses. Gp38+ cells are present during embryogenesis and in human livers of primary biliary cirrhosis. Since little is known about their function, we studied gp38+ cells during chronic liver inflammation in models of biliary and parenchymal liver fibrosis and steatohepatitis. Gp38+ cells were analyzed using flow cytometry and confocal microscopy, and the expression of their steady state and inflammation-associated genes was evaluated from healthy and inflamed livers. Gp38+ cells significantly expanded in all three models of liver injury and returned to baseline levels during regression of inflammation. Based on CD133 and gp38 expression in the CD45−CD31−Asgpr1− liver cell fraction, numerous subsets could be identified that were negative for CD133 (gp38hiCD133−, gp38lowCD133−, and gp38−CD133−). Moreover, among the CD133+ cells, previously identified as progenitor population in injured liver, two subpopulations could be distinguished based on their gp38 expression (gp38−CD133+ and CD133+gp38+). Importantly, the distribution of the identified subsets in inflammation illustrated injury-specific changes. Moreover, the gp38+CD133+ cells exhibited liver progenitor cell characteristics similar to the gp38−CD133+ population, thus representing a novel subset within the classical progenitor cell niche. Additionally, these cells expressed distinct sets of inflammatory genes during liver injury. Our study illuminates a novel classification of the stromal/progenitor cell compartment in the liver and pinpoints a hitherto unrecognized injury-related alteration in progenitor subset composition in chronic liver inflammation and fibrosis.
  • Zugangsstatus: Freier Zugang