PLoS ONE (Jan 2013)

IL-17A mediates early post-transplant lesions after heterotopic trachea allotransplantation in Mice.

  • Philippe H Lemaître,
  • Benoît Vokaer,
  • Louis-Marie Charbonnier,
  • Yoichiro Iwakura,
  • Marc Estenne,
  • Michel Goldman,
  • Oberdan Leo,
  • Myriam Remmelink,
  • Alain Le Moine

DOI
https://doi.org/10.1371/journal.pone.0070236
Journal volume & issue
Vol. 8, no. 7
p. e70236

Abstract

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Primary graft dysfunction (PGD) and bronchiolitis obliterans (BO) are the leading causes of morbidity and mortality after lung transplantation. Reports from clinical and rodent models suggest the implication of IL-17A in either PGD or BO. We took advantage of the heterotopic trachea transplantation model in mice to study the direct role of IL-17A in post-transplant airway lesions. Across full MHC barrier, early lesions were controlled in IL-17A(-/-) or anti-IL17 treated recipients. In contrast, IL-17A deficiency did not prevent subsequent obliterative airway disease (OAD). Interestingly, this early protection occurred also in syngeneic grafts and was accompanied by a decrease in cellular stress, as attested by lower HSP70 mRNA levels, suggesting the involvement of IL-17A in ischemia-reperfusion injury (IRI). Furthermore, persistence of multipotent CK14(+) epithelial stem cells underlined allograft protection afforded by IL-17A deficiency or neutralisation. Recipient-derived γδ(+) and CD4(+) T cells were the major source of IL-17A. However, lesions still occurred in the absence of each subset, suggesting a high redundancy between the innate and adaptive IL-17A producing cells. Notably, a double depletion significantly diminished lesions. In conclusion, this work implicated IL-17A as mediator of early post-transplant airway lesions and could be considered as a potential therapeutic target in clinical transplantation.