Litcius/Paper detail

Recent advances in the development of AHR antagonists in immuno-oncology

Lijun Sun

2021RSC Medicinal Chemistry39 citationsDOIOpen Access PDF

Abstract

The arylhydrocarbon receptor (AHR) is a ligand activated transcription factor that controls the expression of a number of immunosuppressive signaling molecules, including the immune checkpoint proteins PD-1/L1 and cytokine IL-10. AHR activation also stimulates the formation and recruitment of tolerogenic dendritic cells, tumor associated macrophages, and regulatory T cells in the tumor microenvironment, which restrains antitumoral immune response. Overexpression of AHR has been observed in a number of different types of cancer and suggested to contribute to immune dysfunction and cancer progression. One prominent endogenous ligand of AHR is the oncometabolite kynurenine, a product of tryptophan metabolism catalyzed by the dioxygenases IDO1 and TDO that are often aberrantly activated in cancer. AHR has gained significant interest as a drug target for the development of novel small molecule cancer immunotherapies, as evidenced by the advancement of two clinical candidates into phase 1 clinical trials in patients with advanced cancer. Discussed in this Review is a brief background of AHR in immuno-oncology and the recent progress in the discovery and development of AHR antagonists.

Topics & Concepts

Immune systemCancer researchTumor microenvironmentCancerTranscription factorCytokineImmune checkpointImmunotherapyKynurenineBiologyCancer cellImmunologyMedicineInternal medicineBiochemistryGeneAmino acidTryptophanTryptophan and brain disordersImmune cells in cancerCancer, Stress, Anesthesia, and Immune Response
Recent advances in the development of AHR antagonists in immuno-oncology | Litcius