Donor pretreatment with nebulized complement C3a receptor antagonist mitigates brain-death induced immunological injury post–lung transplant

Qi Cheng, Kunal Patel, Biao Lei, Lindsay Rucker, D. Patterson Allen, Peng Zhu, Chentha Vasu, Paulo N. Martins, Martin Goddard, Satish N. Nadig, Carl Atkinson*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

20 Scopus citations

Abstract

Donor brain death (BD) is an inherent part of lung transplantation (LTx) and a key contributor to ischemia-reperfusion injury (IRI). Complement activation occurs as a consequence of BD in other solid organ Tx and exacerbates IRI, but the role of complement in LTx has not been investigated. Here, we investigate the utility of delivering nebulized C3a receptor antagonist (C3aRA) pretransplant to BD donor lungs in order to reduce post-LTx IRI. BD was induced in Balb/c donors, and lungs nebulized with C3aRA or vehicle 30 minutes prior to lung procurement. Lungs were then cold stored for 18 hours before transplantation into C57Bl/6 recipients. Donor lungs from living donors (LD) were removed and similarly stored. At 6 hours and 5 days post-LTx, recipients of BD donor lungs had exacerbated IRI and acute rejection (AR), respectively, compared to recipients receiving LD lungs, as determined by increased histopathological injury, immune cells, and cytokine levels. A single pretransplant nebulized dose of C3aRA to the donor significantly reduced IRI as compared to vehicle-treated BD donors, and returned IRI and AR grades to that seen following LD LTx. These data demonstrate a role for complement inhibition in the amelioration of IRI post-LTx in the context of donor BD.

Original languageEnglish (US)
Pages (from-to)2417-2428
Number of pages12
JournalAmerican Journal of Transplantation
Volume18
Issue number10
DOIs
StatePublished - Oct 2018

Funding

These studies were supported by grants from the NIH (NHLBI 1R01090144 to CA), NIH (NIBIB K08EB19495 to SN), Lee Patterson Allen Foundation Award (CA and SN), NIH Institutional Postdoctoral Training Grant, NIH-HL-007260 (KP), and South Carolina Clinical & Translational Research Institute, Medical University of South Carolina’s CTSA, NIH/NCATS Grant Number UL1TR000062. These studies were supported by grants from the NIH (NHLBI 1R01090144 to CA), NIH (NIBIB K08EB19495 to SN), Lee Patterson Allen Foundation Award (CA and SN), NIH Institutional Postdoctoral Training Grant, NIH-HL-007260 (KP), and South Carolina Clinical & Translational Research Institute, Medical University of South Carolina's CTSA, NIH/NCATS Grant Number UL1TR000062.

Keywords

  • animal models: murine
  • basic (laboratory) research/science
  • complement biology
  • immunobiology
  • immunosuppression/immune modulation
  • ischemia reperfusion injury (IRI)
  • lung transplantation/pulmonology

ASJC Scopus subject areas

  • Transplantation
  • Pharmacology (medical)
  • Immunology and Allergy

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