Interleukin-21 Engineering Enhances NK Cell Activity Against Glioblastoma Via CEBPD

Overview

Journal Cancer Cell

Publisher Cell Press

Specialty Oncology

Date 2024 Aug 13

PMID 39137729

Authors

Mayra Shanley

May Daher

Jinzhuang Dou

SuFang Li

Rafet Basar

Hind Rafei

Merve Dede

Joy Gumin

Jezreel Pantaleon Garcia

Ana Karen Nunez Cortes

Shan He

Corry M Jones

Sunil Acharya

Natalie W Fowlkes

Donghai Xiong

Sanjay Singh

Hila Shaim

Samantha Claire Hicks

Bin Liu

Abhinav Jain

Mohammad Fayyad Zaman

Qi Miao

Ye Li

Nadima Uprety

Enli Liu

Luis Muniz-Feliciano

Gary M Deyter

Vakul Mohanty

Patrick Zhang

Scott E Evans

Elizabeth J Shpall

Frederick F Lang

Ken Chen

Katayoun Rezvani

Affiliations

Soon will be listed here.

Abstract

Glioblastoma (GBM) is an aggressive brain cancer with limited therapeutic options. Natural killer (NK) cells are innate immune cells with strong anti-tumor activity and may offer a promising treatment strategy for GBM. We compared the anti-GBM activity of NK cells engineered to express interleukin (IL)-15 or IL-21. Using multiple in vivo models, IL-21 NK cells were superior to IL-15 NK cells both in terms of safety and long-term anti-tumor activity, with locoregionally administered IL-15 NK cells proving toxic and ineffective at tumor control. IL-21 NK cells displayed a unique chromatin accessibility signature, with CCAAT/enhancer-binding proteins (C/EBP), especially CEBPD, serving as key transcription factors regulating their enhanced function. Deletion of CEBPD resulted in loss of IL-21 NK cell potency while its overexpression increased NK cell long-term cytotoxicity and metabolic fitness. These results suggest that IL-21, through C/EBP transcription factors, drives epigenetic reprogramming of NK cells, enhancing their anti-tumor efficacy against GBM.

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