Literature DB >> 23897677

Mesenchymal stem cells inhibit cutaneous radiation-induced fibrosis by suppressing chronic inflammation.

Jason A Horton1, Kathryn E Hudak, Eun Joo Chung, Ayla O White, Bradley T Scroggins, Jeffrey F Burkeen, Deborah E Citrin.   

Abstract

Exposure to ionizing radiation (IR) can result in the development of cutaneous fibrosis, for which few therapeutic options exist. We tested the hypothesis that bone marrow-derived mesenchymal stem cells (BMSC) would favorably alter the progression of IR-induced fibrosis. We found that a systemic infusion of BMSC from syngeneic or allogeneic donors reduced skin contracture, thickening, and collagen deposition in a murine model. Transcriptional profiling with a fibrosis-targeted assay demonstrated increased expression of interleukin-10 (IL-10) and decreased expression of IL-1β in the irradiated skin of mice 14 days after receiving BMSC. Similarly, immunoassay studies demonstrated durable alteration of these and several additional inflammatory mediators. Immunohistochemical studies revealed a reduction in infiltration of proinflammatory classically activated CD80(+) macrophages and increased numbers of anti-inflammatory regulatory CD163(+) macrophages in irradiated skin of BMSC-treated mice. In vitro coculture experiments confirmed that BMSC induce expression of IL-10 by activated macrophages, suggesting polarization toward a regulatory phenotype. Furthermore, we demonstrated that tumor necrosis factor-receptor 2 (TNF-R2) mediates IL-10 production and transition toward a regulatory phenotype during coculture with BMSC. Taken together, these data demonstrate that systemic infusion of BMSC can durably alter the progression of radiation-induced fibrosis by altering macrophage phenotype and suppressing local inflammation in a TNF-R2-dependent fashion. © AlphaMed Press.

Entities:  

Keywords:  Chronic inflammation; Dermal fibrosis; Ionizing radiation; Mesenchymal stem cell

Mesh:

Substances:

Year:  2013        PMID: 23897677      PMCID: PMC7511998          DOI: 10.1002/stem.1483

Source DB:  PubMed          Journal:  Stem Cells        ISSN: 1066-5099            Impact factor:   6.277


  52 in total

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5.  Mesenchymal stem cell therapy for cutaneous radiation syndrome.

Authors:  Sadanori Akita; Kozo Akino; Akiyoshi Hirano; Akira Ohtsuru; Shunichi Yamashita
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6.  The development of classically and alternatively activated macrophages has different effects on the varied stages of radiation-induced pulmonary injury in mice.

Authors:  Hui Zhang; Guang Han; Hui Liu; Ji Chen; Xuemei Ji; Fuxiang Zhou; Yunfeng Zhou; Conghua Xie
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Review 8.  New insights into mesenchymal stromal cell-mediated T-cell suppression through galectins.

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Journal:  Scand J Immunol       Date:  2011-02       Impact factor: 3.487

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10.  Mouse bone marrow-derived mesenchymal stromal cells turn activated macrophages into a regulatory-like profile.

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Journal:  PLoS One       Date:  2010-02-16       Impact factor: 3.240

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  49 in total

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2.  Therapeutic potential of gingival fibroblasts for cutaneous radiation syndrome: comparison to bone marrow-mesenchymal stem cell grafts.

Authors:  Christine Linard; Frederique Tissedre; Elodie Busson; Valerie Holler; Thomas Leclerc; Carine Strup-Perrot; Ludovic Couty; Bruno L'homme; Marc Benderitter; Antoine Lafont; Jean Jacques Lataillade; Bernard Coulomb
Journal:  Stem Cells Dev       Date:  2015-02-26       Impact factor: 3.272

3.  Antifibrotic Activity of Human Placental Amnion Membrane-Derived CD34+ Mesenchymal Stem/Progenitor Cell Transplantation in Mice With Thioacetamide-Induced Liver Injury.

Authors:  Po-Huang Lee; Chi-Tang Tu; Chih-Chiang Hsiao; Ming-Song Tsai; Cheng-Maw Ho; Nai-Chen Cheng; Tzu-Min Hung; Daniel Tzu-Bi Shih
Journal:  Stem Cells Transl Med       Date:  2016-07-12       Impact factor: 6.940

Review 4.  Pharmacological management of ionizing radiation injuries: current and prospective agents and targeted organ systems.

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5.  Loss of CD73 prevents accumulation of alternatively activated macrophages and the formation of prefibrotic macrophage clusters in irradiated lungs.

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6.  Cellular Therapies for Treatment of Radiation Injury: Report from a NIH/NIAID and IRSN Workshop.

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7.  Cellular Therapies for Treatment of Radiation Injury after a Mass Casualty Incident.

Authors:  Carmen Rios; Jean-René Jourdain; Andrea L DiCarlo
Journal:  Radiat Res       Date:  2017-06-13       Impact factor: 2.841

Review 8.  Mechanisms of Normal Tissue Injury From Irradiation.

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Journal:  Semin Radiat Oncol       Date:  2017-10       Impact factor: 5.934

Review 9.  Altering the response to radiation: sensitizers and protectors.

Authors:  Deborah E Citrin; James B Mitchell
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Review 10.  Radiation-induced fibrosis: mechanisms and implications for therapy.

Authors:  Jeffrey M Straub; Jacob New; Chase D Hamilton; Chris Lominska; Yelizaveta Shnayder; Sufi M Thomas
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