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Adjuvant Immunotherapy for Liver Transplant Recipients with Hepatocellular Carcinoma Using Donor Liver Derived Natural Killer Cells

M. Ohira1, R. Hotta1, Y. Imaoka1, K. Sato1, N. Tanimine1, H. Tahara1, K. Ide1, T. Kobayashi1, Y. Tanaka1, A. Tzakis2, S. Nishida2, H. Ohdan1

1Hiroshima University, Hiroshima, Japan, 2University of Miami, Miami, FL

Meeting: 2020 American Transplant Congress

Abstract number: 251

Keywords: Hepatocellular carcinoma, Liver transplantation, Natural killer cells, Tumor recurrence

Session Information

Session Name: Liver: Hepatocellular Carcinoma and Other Malignancies II

Session Type: Oral Abstract Session

Date: Saturday, May 30, 2020

Session Time: 3:15pm-4:45pm

 Presentation Time: 3:27pm-3:39pm

Location: Virtual

*Purpose: Development of an effective adjuvant therapy to prevent HCC recurrence after liver transplantation (LT) is an important medical requirement. Immunosuppressive regimens currently used after LT reduce the proportion of adaptive components of cellular immunity while maintaining innate components. Natural killer (NK) cells play a central role in innate immunity against neoplastic cells; therefore, their augmentation is a promising immunotherapeutic approach against HCC recurrence after LT.

*Methods: We propose that adoptive transfer of IL-2-stimulated TRAIL+ NK cells extracted from donor liver graft perfusate can mount an anti-tumor response without causing toxicity to intact recipient tissues.

*Results: We have successfully performed NK-cell immunotherapy in 44 living donor LT (LDLT) recipients with HCC in Japan. The median follow-up period is 77.5 months. In the series of LDLT with HCC, among the 101 patients who met the Milan criteria (MC) on preoperative imaging (NK group n=37; control group n=64), 38 patients (37%) had HCC exceeding MC on postoperative pathology. Of these 38 patients, the recurrent free survival (RFS) rates were significantly improved in the NK group (n=16) as compared to those in the control group (n=22). Their 5 year-RFS were 75% and 48%, respectively (p=0.042). After infusion of NK cells, the NK cytotoxicity and the proportion of TRAIL+ NK cells in the peripheral blood of patients increased significantly (p<0.05). The inoculated donor NK cells could be confirmed up to 1 month through the analysis of peripheral blood chimerism. We also applied the proposed approach to the deceased donor LT (DDLT) recipients in collaboration with the US since 2009. This phase I study included 17 subjects with a median follow-up of 43 months. No study-related adverse events were noted in either of the studies. In the series of DDLT with HCC, among the 17 patients who met MC on preoperative imaging, 9 patients (53%) had HCC exceeding MC on postoperative pathology. None of the patients have shown any symptom of HCC recurrence. Interestingly, the number of HLA mismatch between donor and recipient was associated with tumor recurrence after NK cell therapy.

*Conclusions: In conclusions, the administration of IL-2-stimulated NK cells derived from both living and deceased donor liver allografts was safely applied and is, therefore, a potential novel adjuvant immune treatment after LT in HCC patients.

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To cite this abstract in AMA style:

Ohira M, Hotta R, Imaoka Y, Sato K, Tanimine N, Tahara H, Ide K, Kobayashi T, Tanaka Y, Tzakis A, Nishida S, Ohdan H. Adjuvant Immunotherapy for Liver Transplant Recipients with Hepatocellular Carcinoma Using Donor Liver Derived Natural Killer Cells [abstract]. Am J Transplant. 2020; 20 (suppl 3). https://atcmeetingabstracts.com/abstract/adjuvant-immunotherapy-for-liver-transplant-recipients-with-hepatocellular-carcinoma-using-donor-liver-derived-natural-killer-cells/. Accessed May 9, 2025.

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