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Data from Combining AFM13, a Bispecific CD30/CD16 Antibody, with Cytokine-Activated Blood and Cord Blood–Derived NK Cells Facilitates CAR-like Responses Against CD30+ Malignancies

Authors :
Katayoun Rezvani
Todd A. Fehniger
Elizabeth J. Shpall
Oswaldo Keith Okamoto
Wolfgang Fischer
Martin Treder
Joachim Koch
Yago L. Nieto
Richard E. Champlin
Luis Muniz-Feliciano
Ken Chen
Natalie W. Fowlkes
Natalia Baran
Yifei Shen
Qi Miao
Vakul Mohanty
Vandana Nandivada
Rong Cai
Sonny O. Ang
Enli Liu
Pamela Wong
Nadima Uprety
Emily L. Ensley
Mayra Shanley
Hila Shaim
Li Li
Timothy Schappe
Mayela Carolina Mendt
Francesca Wei Inng Lim
Sweta Desai
Ana Karen Nunez Cortes
May Daher
Ethan McClain
Carly C. Neal
Luciana Garcia Melo
Mark Foster
Rafet Basar
Michelle Becker-Hapak
Melissa M. Berrien-Elliott
Pinaki P. Banerjee
Mecit Kaplan
Nancy D. Marin
Lucila N. Kerbauy
Publication Year :
2023
Publisher :
American Association for Cancer Research (AACR), 2023.

Abstract

Purpose:Natural killer (NK)-cell recognition and function against NK-resistant cancers remain substantial barriers to the broad application of NK-cell immunotherapy. Potential solutions include bispecific engagers that target NK-cell activity via an NK-activating receptor when simultaneously targeting a tumor-specific antigen, as well as enhancing functionality using IL12/15/18 cytokine pre-activation.Experimental Design:We assessed single-cell NK-cell responses stimulated by the tetravalent bispecific antibody AFM13 that binds CD30 on leukemia/lymphoma targets and CD16A on various types of NK cells using mass cytometry and cytotoxicity assays. The combination of AFM13 and IL12/15/18 pre-activation of blood and cord blood–derived NK cells was investigated in vitro and in vivo.Results:We found heterogeneity within AFM13-directed conventional blood NK cell (cNK) responses, as well as consistent AFM13-directed polyfunctional activation of mature NK cells across donors. NK-cell source also impacted the AFM13 response, with cNK cells from healthy donors exhibiting superior responses to those from patients with Hodgkin lymphoma. IL12/15/18-induced memory-like NK cells from peripheral blood exhibited enhanced killing of CD30+ lymphoma targets directed by AFM13, compared with cNK cells. Cord-blood NK cells preactivated with IL12/15/18 and ex vivo expanded with K562-based feeders also exhibited enhanced killing with AFM13 stimulation via upregulation of signaling pathways related to NK-cell effector function. AFM13–NK complex cells exhibited enhanced responses to CD30+ lymphomas in vitro and in vivo.Conclusions:We identify AFM13 as a promising combination with cytokine-activated adult blood or cord-blood NK cells to treat CD30+ hematologic malignancies, warranting clinical trials with these novel combinations.

Details

Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....26f8e65e1e920150dcbd7408adbc0a3d