Extended survival of 9- and 10-gene-edited pig heart xenografts with ischemia minimization and CD154 costimulation blockade-based immunosuppression

Ryan Chaban; Ikechukwu Ileka; Gannon McGrath; Kohei Kinoshita; Zahra Habibabady; Madelyn Ma; Victoria Diaz; Akihiro Maenaka; Anthony Calhoun; Megan Dufault; Ivy Rosales; Christiana M Laguerre; Seyed-Amir Sanatkar; Lars Burdorf; David L Ayares; William Eyestone; Prachi Sardana; Kasinath Kuravi; Lori Sorrells; Seth Lederman; Caroline G Lucas; Randall S Prather; Kevin D Wells; Kristin M Whitworth; David K C Cooper; Richard N Pierson 3rd

doi:10.1016/j.healun.2024.07.022

Extended survival of 9- and 10-gene-edited pig heart xenografts with ischemia minimization and CD154 costimulation blockade-based immunosuppression

J Heart Lung Transplant. 2024 Dec;43(12):1932-1944. doi: 10.1016/j.healun.2024.07.022. Epub 2024 Aug 7.

Authors

Ryan Chaban¹, Ikechukwu Ileka², Gannon McGrath², Kohei Kinoshita², Zahra Habibabady², Madelyn Ma², Victoria Diaz², Akihiro Maenaka², Anthony Calhoun², Megan Dufault², Ivy Rosales², Christiana M Laguerre², Seyed-Amir Sanatkar², Lars Burdorf³, David L Ayares⁴, William Eyestone⁴, Prachi Sardana⁴, Kasinath Kuravi⁴, Lori Sorrells⁴, Seth Lederman⁵, Caroline G Lucas⁶, Randall S Prather⁶, Kevin D Wells⁶, Kristin M Whitworth⁶, David K C Cooper², Richard N Pierson 3rd⁷

Affiliations

¹ Center for Transplantation Sciences and Department of Surgery, Massachusetts General Hospital and Harvard Medical School, Boston, Massachusetts; Department of Cardiovascular Surgery, University Hospital of Mainz, Mainz, Germany.
² Center for Transplantation Sciences and Department of Surgery, Massachusetts General Hospital and Harvard Medical School, Boston, Massachusetts.
³ Center for Transplantation Sciences and Department of Surgery, Massachusetts General Hospital and Harvard Medical School, Boston, Massachusetts; Revivicor, Inc., Blacksburg, Virginia.
⁴ Revivicor, Inc., Blacksburg, Virginia.
⁵ Tonix Pharma LLC, Chatham, New Jersey.
⁶ National Swine Resource and Research Center (NSRRC), Animal Science Research Center, University of Missouri, Columbia, Missouri.
⁷ Center for Transplantation Sciences and Department of Surgery, Massachusetts General Hospital and Harvard Medical School, Boston, Massachusetts. Electronic address: rpierson@mgh.harvard.edu.

PMID: 39097214
PMCID: PMC11568940 (available on 2025-12-01)
DOI: 10.1016/j.healun.2024.07.022

Abstract

Background: Xenotransplantation has made significant advances recently using pigs genetically engineered to remove carbohydrate antigens, either alone or with addition of various human complement, coagulation, and anti-inflammatory ''transgenes''. Here we evaluated results associated with gene-edited (GE) pig hearts transplanted in baboons using an established costimulation-based immunosuppressive regimen and a cold-perfused graft preservation technique.

Methods: Eight baboons received heterotopic abdominal heart transplants from 3-GE (GalKO.β4GalNT2KO.hCD55, n = 3), 9-GE (GalKO.β4GalNT2KO.GHRKO.hCD46.hCD55. TBM.EPCR.hCD47. HO-1, n = 3) or 10-G (9-GE+CMAHKO, n = 2) pigs using Steen's cold continuous perfusion for ischemia minimization. Immunosuppression (IS) included induction with anti-thymocyte globulin and αCD20, ongoing αCD154, MMF, and tapered corticosteroid.

Results: All three 3-GE grafts functioned well initially, but failed within 5 days. One 9-GE graft was lost intraoperatively due to a technical issue and another was lost at POD 13 due to antibody mediated rejection (AMR) in a baboon with a strongly positive pre-operative cross-match. One 10-GE heart failed at POD113 with combined cellular and antibody mediated rejection. One 9-GE and one 10-GE hearts had preserved graft function with normal myocardium on protocol biopsies, but exhibited slowly progressive graft hypertrophy until elective necropsy at POD393 and 243 respectively. Elevated levels of IL-6, MCP-1, C-reactive protein, and human thrombomodulin were variably associated with conditioning, the transplant procedure, and clinically significant postoperative events.

Conclusion: Relative to reference genetics without thrombo-regulatory and anti-inflammatory gene expression, 9- or 10-GE pig hearts exhibit promising performance in the context of a clinically applicable regimen including ischemia minimization and αCD154-based IS, justifying further evaluation in an orthotopic model.

Keywords: costimulation pathway blockade; genetic engineering; heart transplantation; swine; xenotransplantation.

MeSH terms

Animals
Animals, Genetically Modified
CD40 Ligand*
Gene Editing / methods
Graft Rejection / prevention & control
Graft Survival*
Heart Transplantation* / methods
Heterografts
Immunosuppression Therapy* / methods
Papio*
Swine
Transplantation, Heterologous / methods

Substances

CD40 Ligand

Abstract

MeSH terms

Substances

Grants and funding