Synapse - Genetic ablation of adhesion ligands mitigates rejection of allogeneic cellular immunotherapies

Genetic ablation of adhesion ligands mitigates rejection of allogeneic cellular immunotherapies Journal Article

Authors:	Hammer, Q.; Perica, K.; Mbofung, R. M.; van Ooijen, H.; Martin, K. E.; Momayyezi, P.; Varady, E.; Pan, Y.; Jelcic, M.; Groff, B.; Abujarour, R.; Krokeide, S. Z.; Lee, T.; Williams, A.; Goodridge, J. P.; Valamehr, B.; Önfelt, B.; Sadelain, M.; Malmberg, K. J.
Article Title:	Genetic ablation of adhesion ligands mitigates rejection of allogeneic cellular immunotherapies
Abstract:	Allogeneic cellular immunotherapies hold promise for broad clinical implementation but face limitations due to potential rejection of donor cells by the host immune system. Silencing of beta-2 microglobulin (B2M) B2M ) expression is commonly employed to evade T cell-mediated rejection by the host, although the absence of B2M is expected to trigger missing-self responses by host natural killer (NK) cells. Here, we demonstrate that genetic deletion of the adhesion ligands CD54 and CD58 in B2M-deficient chimeric antigen receptor (CAR) T cells and multi-edited induced pluripotent stem cell (iPSC)-derived CAR NK cells reduces their susceptibility to rejection by host NK cells in vitro and in vivo. . The absence of adhesion ligands limits rejection in a unidirectional manner in B2M-deficient and B2M-sufficient settings without affecting the antitumor functionality of the engineered donor cells. Thus, these data suggest that genetic ablation of adhesion ligands effectively alleviates rejection by host immune cells, facilitating the implementation of universal immunotherapy.
Keywords:	design; expression; pluripotent stem-cells; costimulation; natural-killer-cells; self; nk cells; escape; platform; icam-1
Journal Title:	Cell Stem Cell
Volume:	31
Issue:	9
ISSN:	1934-5909
Publisher:	Cell Press
Date Published:	2024-09-05
Language:	English
ACCESSION:	WOS:001317257900001
DOI:	10.1016/j.stem.2024.06.011
PROVIDER:	wos
PUBMED:	38981470
Notes:	Article -- Source: Wos

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583 Sadelain
19 Perica

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