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Mesenchymal stromal cells mediate aspergillus hyphal extract-induced allergic airway inflammation by inhibition of the th17 signaling pathway

  • Melissa J. Lathrop
  • , Elice M. Brooks
  • , Nick R. Bonenfant
  • , Dino Sokocevic
  • , Zachary D. Borg
  • , Meagan Goodwin
  • , Roberto Loi
  • , Fernanda Cruz
  • , Chad W. Dunaway
  • , Chad Steele
  • , Daniel J. Weiss
  • University of Vermont
  • University of Cagliari
  • Museu Nacional/UFRJ
  • University of Alabama at Birmingham

Research output: Contribution to journalArticlepeer-review

69 Scopus citations

Abstract

Systemic administration of mesenchymal stromal cells (MSCs) suppresses airway inflammation and methacholine-induced airway hyper-responsiveness (AHR) in mouse models of T helper cell (Th) type 2-mediated eosinophilic allergic airway inflammation (AAI); however, the efficacy of MSCs in mouse models of severe Th17-mediated neutrophilic AAI has not yet been demonstrated. We assessed MSC effects in a mouse model of mixed Th2/Th17 AAI produced by mucosal exposure to Aspergillus fumigatus hyphal extract (AHE). Following sensitization produced by oropharyngeal AHE administration, systemic (tail vein) administration of syngeneicMSCsonthe first day of challenge significantly reduced acute AHR predominantly through reduction of Th17-mediated airway inflammation. In parallel experiments, MSCs also mitigated AHR when administered during recurrent challenge 10 weeks after initial sensitization and challenge through reduction in systemic Th17-mediated inflammation. Investigation into potential mechanistic actions of MSCs in this model demonstrated that although T regulatory cells were increased in all AHE-treated mice,MSC administration did not alter T regulatory cell numbers in either the acute or recurrent model. Differential induction of interleukin-17a secretion was observed in ex vivo restimulation of mediastinal lymph node mixed-cell cytokine analyses. Although the mechanisms by which MSCs act to decrease inflammation and AHR in this model are not yet fully elucidated, decrease in Th17-mediated airway inflammation appears to play a significant role. These results provide a basis for further investigations of MSC administration as a potential therapeutic approach for severe refractory neutrophilic asthma.

Original languageEnglish
Pages (from-to)194-205
Number of pages12
JournalStem Cells Translational Medicine
Volume3
Issue number2
DOIs
StatePublished - Feb 2014
Externally publishedYes

Keywords

  • Cell therapy
  • Lung asthma
  • Mesenchymal stromal cell
  • Mouse

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