Type 1 Innate Lymphoid Cells Alleviate Acute Liver Injury Following Transplantation via Interferon-γ Mediated Pathway

H. Kojima, K. Kadono, H. Hirao, K. J. Dery, J. Kupiec-Weglinski, Y. Zhai

Dumont-UCLA Transplant Center, Los Angeles, CA

Meeting: 2022 American Transplant Congress

Abstract number: 192

Keywords: Inflammation, Interferon (IFN), Ischemia, Liver transplantation

Topic: Basic Science » Basic Science » 08 - Innate Immunity; Chemokines, Cytokines, Complement

Session Information

Session Name: Innate Immunity, Chemokines, Cytokines, and Complement

Session Type: Rapid Fire Oral Abstract

Date: Sunday, June 5, 2022

Session Time: 5:30pm-7:00pm

Presentation Time: 6:40pm-6:50pm

Location: Hynes Room 309

*Purpose: Innate lymphoid cells (ILCs), a heterogeneous population of non-B non-T lymphocytes, have been found in recent years to plays key regulatory roles in tissue inflammatory response against infectious and non-infectious agents. The question of whether they are involved in the pathophysiology of liver ischemia-reperfusion injury (IRI), particularly in the setting of orthotopic liver transplantation (OLT), is largely unknown.

*Methods: Mouse liver grafts were subjected to the extended cold storage (4°C/18 hours) to mimic the marginal donor livers in human OLT. To evaluate the role of recipient ILCs in OLT, we transplanted the cold-stored WT B6 grafts into: WT, or Rag2 knockout (KO, lack T and B cells), or Rag2-common-γ-chain double KO (Rag2-γc DKO, lack ILCs/NK and T and B cells) recipient mice (all in B6 background). Liver IRI was evaluated at 6h post Tx. Additionally, we treated Rag2 KO recipient mice with anti-CD90.2 (0.5 mg at 72h and 0.25 mg at 24h prior to OLT, intraperitoneal injection), or anti-NK1.1 (0.25 mg at 48h prior to OLT, intravenous injection; i.v.), or anti-interferon-γ (IFN-γ) antibodies (0.5mg immediately after reperfusion, i.v.) to deplete all ILCs, or type 1 ILCs (ILC1s), or to neutralize IFN-γ, respectively.

*Results: Compared with WT controls, Rag2 KO recipients were protected from liver IRI; Rag2-γc DKO recipients, however, developed significantly higher levels of liver IRI, as documented by levels of serum ALT/AST and Suzuki’s histological grading. Depletion of total ILCs with anti-CD90.2 increased liver injuries in Rag2 KO mice and diminished the differences between Rag2 KO and Rag2-γc DKO recipients. Quantitative RT-PCR analysis of intrahepatic gene transcripts revealed no differences in the signature gene expression profiles of ILC2, ILC3, ILCreg, but ILC1. Levels of T-box transcriptional factor (T-bet) and IFN-γ were significantly higher in OLTs of Rag2 KO recipients as compared with those of Rag2-γc DKO and Rag2 KO treated with anti-CD90.2 Abs. In addition, depletion of ILC1s by anti-NK1.1 Abs and neutralization of IFN-γ exacerbated IRI of OLTs in Rag2 KO recipients.

*Conclusions: Recipient’s ILCs, in particular ILC1s/NK cells protect OLTs from IRI via IFN-γ. This study demonstrates, for the first time, unique roles of ILC1s in liver IRI, and provides us a novel therapeutic target for future clinical application in transplant recipients.

To cite this abstract in AMA style:

Kojima H, Kadono K, Hirao H, Dery KJ, Kupiec-Weglinski J, Zhai Y. Type 1 Innate Lymphoid Cells Alleviate Acute Liver Injury Following Transplantation via Interferon-γ Mediated Pathway [abstract]. Am J Transplant. 2022; 22 (suppl 3). https://atcmeetingabstracts.com/abstract/type-1-innate-lymphoid-cells-alleviate-acute-liver-injury-following-transplantation-via-interferon-%ce%b3-mediated-pathway/. Accessed November 21, 2024.

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