Necrotic cell-derived high mobility group box 1 attracts antigen-presenting cells but inhibits hepatocyte growth factor-mediated tropism of mesenchymal stem cells for apoptotic cell death

Tissue damage due to apoptotic or necrotic cell death typically initiates distinct cellular responses, leading either directly to tissue repair and regeneration or to immunological processes first, to clear the site, for example, of potentially damage-inducing agents. Mesenchymal stem cells (MSC) as...

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Published in:	Cell death and differentiation Vol. 22; no. 7; pp. 1219 - 1230
Main Authors:	Vogel, S, Börger, V, Peters, C, Förster, M, Liebfried, P, Metzger, K, Meisel, R, Däubener, W, Trapp, T, Fischer, J C, Gawaz, M, Sorg, R V
Format:	Journal Article
Language:	English
Published:	London Nature Publishing Group UK 01-07-2015 Nature Publishing Group
Subjects:	13 13/100 13/106 13/31 38 631/250/1933 Animals Apoptosis Biochemistry Biomedical and Life Sciences Cell Biology Cell Cycle Analysis Chemotaxis Dendritic Cells - physiology Hepatocyte Growth Factor - secretion HMGB1 Protein - secretion Humans Inflammation Life Sciences Male Mesenchymal Stromal Cells - physiology Mice Monocytes - physiology Myocytes, Cardiac - physiology Myocytes, Cardiac - secretion Necrosis Neurons - physiology Neurons - secretion Original Paper Regeneration Stem Cells
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Summary:	Tissue damage due to apoptotic or necrotic cell death typically initiates distinct cellular responses, leading either directly to tissue repair and regeneration or to immunological processes first, to clear the site, for example, of potentially damage-inducing agents. Mesenchymal stem cells (MSC) as well as immature dendritic cells (iDC) and monocytes migrate to injured tissues. MSC have regenerative capacity, whereas monocytes and iDC have a critical role in inflammation and induction of immune responses, including autoimmunity after tissue damage. Here, we investigated the influence of apoptotic and necrotic cell death on recruitment of MSC, monocytes and iDC, and identified hepatocyte growth factor (HGF) and the alarmin high mobility group box 1 (HMGB1) as key factors differentially regulating these migratory responses. MSC, but not monocytes or iDC, were attracted by apoptotic cardiomyocytic and neuronal cells, whereas necrosis induced migration of monocytes and iDC, but not of MSC. Only apoptotic cell death resulted in HGF production and HGF-mediated migration of MSC towards the apoptotic targets. In contrast, HMGB1 was predominantly released by the necrotic cells and mediated recruitment of monocytes and iDC via the receptor of advanced glycation end products. Moreover, necrotic cardiomyocytic and neuronal cells caused an HMGB1/toll-like receptor-4-dependent inhibition of MSC migration towards apoptosis or HGF, while recruitment of monocytes and iDC by necrosis or HMGB1 was not affected by apoptotic cells or HGF. Thus, the type of cell death differentially regulates recruitment of either MSC or monocytes and iDC through HGF and HMGB1, respectively, with a dominant, HMGB1-mediated role of necrosis in determining tropism after tissue injury.
Bibliography:	ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23 Current address: Department of Cardiology and Cardiovascular Diseases, Eberhard Karls University, Tübingen, Germany Current address: Department of Neurology, Heinrich Heine University Hospital, Düsseldorf, Germany Current address: Institute for Transfusion Medicine, University Hospital Essen, Essen, Germany
ISSN:	1350-9047 1476-5403
DOI:	10.1038/cdd.2014.225