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Single-cell dissection of Merkel cell carcinoma heterogeneity unveils transcriptomic plasticity and therapeutic vulnerabilities

Bhaba Krishna Das, Aarthi Kannan, Graham J. Velasco, Mikaela D Kunika, Nils Lambrecht, Quy Nguyen, Haibo Zhao, Jie Wu, Ling Gao

2023Cell Reports Medicine18 citationsDOIOpen Access PDF

Abstract

Merkel cell carcinoma (MCC), a rare but aggressive skin cancer, remains a challenge in the era of precision medicine. Immune checkpoint inhibitors (ICIs), the only approved therapy for advanced MCC, are impeded by high primary and acquired resistance. Hence, we dissect transcriptomic heterogeneity at single-cell resolution in a panel of patient tumors, revealing phenotypic plasticity in a subset of treatment-naive MCC. The tumor cells in a "mesenchymal-like" state are endowed with an inflamed phenotype that portends a better ICI response. This observation is also validated in the largest whole transcriptomic dataset available from MCC patient tumors. In contrast, ICI-resistant tumors predominantly express neuroepithelial markers in a well-differentiated state with "immune-cold" landscape. Importantly, a subtle shift to "mesenchymal-like" state reverts copanlisib resistance in primary MCC cells, highlighting potential strategies in patient stratification for therapeutics to harness tumor cell plasticity, augment treatment efficacy, and avert resistance.

Topics & Concepts

Merkel cell carcinomaCancer researchTranscriptomeImmune checkpointMesenchymal stem cellPhenotypeMedicineImmune systemBiologyImmunotherapyCarcinomaPathologyImmunologyGeneGeneticsGene expressionPolyomavirus and related diseasesEnergy Harvesting in Wireless NetworksBacteriophages and microbial interactions