Monitoring Melanoma Patients on Treatment Reveals a Distinct Macrophage Population Driving Targeted Therapy Resistance

Overview

Journal Cell Rep Med

Publisher Cell Press

Specialties Biology
General Medicine

Date 2024 Jun 28

PMID 38942020

Authors

Jelena Vasilevska

Phil Fang Cheng

Julia Lehmann

Egle Ramelyte

Julia Martinez Gomez

Florentia Dimitriou

Federica Sella

Daria Ferretti

Adrian Salas-Bastos

Whitney Shannon Jordaan

Mitchell Paul Levesque

Reinhard Dummer

Lukas Sommer

Affiliations

Soon will be listed here.

Abstract

Resistance to targeted therapy remains a major clinical challenge in melanoma. To uncover resistance mechanisms, we perform single-cell RNA sequencing on fine-needle aspirates from resistant and responding tumors of patients undergoing BRAFi/MEKi treatment. Among the genes most prominently expressed in resistant tumors is POSTN, predicted to signal to a macrophage population associated with targeted therapy resistance (TTR). Accordingly, tumors from patients with fast disease progression after therapy exhibit high POSTN expression levels and high numbers of TTR macrophages. POSTN polarizes human macrophages toward a TTR phenotype and promotes resistance to targeted therapy in a melanoma mouse model, which is associated with a phenotype change in intratumoral macrophages. Finally, polarized TTR macrophages directly protect human melanoma cells from MEKi-induced killing via CD44 receptor expression on melanoma cells. Thus, interfering with the protective activity of TTR macrophages may offer a strategy to overcome resistance to targeted therapy in melanoma.

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