What question did this study set out to answer?

This research aims to understand how CD45+ immune cells influence the lung tumor microenvironment and cancer outcomes.

February 12, 2026Open Access

Divergent CD45+ immune landscapes shape the lung tumor microenvironment

Key Points

This research aims to understand how CD45+ immune cells influence the lung tumor microenvironment and cancer outcomes.
Conducted single-cell RNA sequencing of CD45+ immune cells from various lung sources.
Analyzed immune composition and transcriptional programs in different tumor models.
Studied differentiation trajectories and metabolic states of immune cells.
Performed ligand-receptor analyses to assess intercellular communication.
Identified four main immune cell types: B cells, T cells, NK cells, and macrophages undergoing remodeling.
LLC1 tumors displayed B cell expansion and reduced T and NK cells with inflammatory responses.
Kras LA2 tumors maintained immune balance but showed signs of metabolic adaptation and enhanced antigen presentation.
Subclustering revealed specific immune cell subsets with distinct characteristics.

Abstract

Background The lung tumor microenvironment (TME) plays a crucial role in the progression and metastasis of lung cancer. It consists of various cell types that interact in complex ways to influence tumor behavior. CD45 + cells, as a component of the TME, have complex and multifaceted roles in lung cancer. The balance between the anti-tumor and pro-tumor functions of CD45 + cells can significantly affect lung cancer outcomes. Understanding these roles is essential for developing targeted therapies that harness the beneficial effects of CD45 + cells while mitigating their harmful effects. Methods We performed single-cell RNA sequencing of sorted CD45 + immune cells from healthy lungs, orthotopic LLC1 tumors, and Kras LA2 (Kras) genetically engineered tumors. Analyses included immune composition, transcriptional programs, differentiation trajectories, metabolic states, and ligand-receptor-based intercellular communication networks. Results Four major immune compartments, B cells, T cells, NK cells, and macrophages, underwent model-specific remodeling. LLC1 tumors showed B cell expansion and T and NK cell reduction, with inflammatory, stress-response, and NF−κB/TNF-dominant programs. Kras LA2 tumors retained a balanced immune composition but exhibited metabolic rewiring, elevated antigen-presentation signatures, and selective intercellular signaling. Subclustering revealed specialized changes across B cell (resting, mature, pre-Bcr, late pro-B, plasma), T cell (Cd4 + , Cd8 + , memory, activated, Treg, Th17), NK cell (Fcgr3 high , Fcgr3 low , Xcl1 + ), and macrophage (Ace + , Bcr + , Ccr2 + , Cd3 + , metabolic, MHCII + ) subsets. Ligand-receptor analyses highlighted dense inflammatory networks in LLC1 tumors versus metabolically tuned signaling in Kras LA2 tumors. Conclusion Distinct CD45 + immune landscapes, characterized by inflammatory suppression in LLC1 and metabolic adaptation in Kras LA2 tumors, shape lung tumor biology. This atlas identifies genotype-specific immune vulnerabilities with potential relevance for precision immunotherapy in non-small cell lung cancer.

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Divergent CD45+ immune landscapes shape the lung tumor microenvironment

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Abstract

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