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MerTK <sup>+</sup> macrophages promote melanoma progression and immunotherapy resistance through AhR-ALKAL1 activation

Naming Wu, Jun Li, Lu Li, Yang Liu, Liyun Dong, Chen Shen, Shanshan Sha, Yangxue Fu, E Dong, Fang Zheng, Zheng Tan, Juan Tao

2024Science Advances23 citationsDOIOpen Access PDF

Abstract

Despite our increasing understanding of macrophage heterogeneity, drivers of macrophage phenotypic and functional polarization in the microenvironment are not fully elucidated. Here, our single-cell RNA sequencing data identify a subpopulation of macrophages expressing high levels of the phagocytic receptor MER proto-oncogene tyrosine kinase (MerTK + macrophages), which is closely associated with melanoma progression and immunotherapy resistance. Adoptive transfer of the MerTK + macrophages into recipient mice notably accelerated tumor growth regardless of macrophage depletion. Mechanistic studies further revealed that ALK And LTK Ligand 1 (ALKAL1), a target gene of aryl hydrocarbon receptor (AhR), facilitated MerTK phosphorylation, resulting in heightened phagocytic activity of MerTK + macrophages and their subsequent polarization toward an immunosuppressive phenotype. Specifically targeted delivery of AhR antagonist to tumor-associated macrophages with mannosylated micelles could suppress MerTK expression and improved the therapeutic efficacy of anti–programmed cell death ligand 1 therapy. Our findings shed light on the regulatory mechanism of MerTK + macrophages and provide strategies for improving the efficacy of melanoma immunotherapy.

Topics & Concepts

MERTKGAS6Cancer researchImmunotherapyMacrophage polarizationMelanomaTumor microenvironmentBiologyMacrophageImmunologyAdoptive cell transferReceptor tyrosine kinaseImmune systemT cellKinaseCell biologyIn vitroBiochemistryPhagocytosis and Immune RegulationImmune cells in cancerCAR-T cell therapy research