Regulation of NKG2D Stress Ligands and Its Relevance in Cancer Progression

Author:

Jones Amber B.,Rocco AbbeyORCID,Lamb Lawrence S.,Friedman Gregory K.ORCID,Hjelmeland Anita B.

Abstract

Under cellular distress, multiple facets of normal homeostatic signaling are altered or disrupted. In the context of the immune landscape, external and internal stressors normally promote the expression of natural killer group 2 member D (NKG2D) ligands that allow for the targeted recognition and killing of cells by NKG2D receptor-bearing effector populations. The presence or absence of NKG2D ligands can heavily influence disease progression and impact the accessibility of immunotherapy options. In cancer, tumor cells are known to have distinct regulatory mechanisms for NKG2D ligands that are directly associated with tumor progression and maintenance. Therefore, understanding the regulation of NKG2D ligands in cancer will allow for targeted therapeutic endeavors aimed at exploiting the stress response pathway. In this review, we summarize the current understanding of regulatory mechanisms controlling the induction and repression of NKG2D ligands in cancer. Additionally, we highlight current therapeutic endeavors targeting NKG2D ligand expression and offer our perspective on considerations to further enhance the field of NKG2D ligand biology.

Funder

National Institute of Neurological Disorders and Stroke

University of Alabama at Birmingham

Rally Foundation

CureSearch for Children's Cancer

The V Foundation

Hyundai Hope on Wheels

Andrew McDonough B+ Foundation

Pediatric Cancer Research Foundation

National Pediatric Cancer Foundation

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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