What question did this study set out to answer?

This research aims to explore the variations in tumor and immune cell characteristics in CLL patients receiving ibrutinib treatment.

April 24, 2026

Single-Cell RNA-seq Analysis Reveals Distinct Tumor and Immunosuppressive T-Cell Phenotypes in Patients with CLL Treated with Ibrutinib

Key Points

This research aims to explore the variations in tumor and immune cell characteristics in CLL patients receiving ibrutinib treatment.
Utilized single-cell RNA-sequencing analysis to assess transcriptional profiles.
Examined the tumor and immune cell environments in patients.
Identified T-cell and monocyte phenotypes associated with treatment resistance.
Observed distinct transcriptional changes in circulating immune cells linked to ibrutinib resistance.
Identified increased signs of T-cell exhaustion in the immune milieu of treated patients.
Monocyte polarization was associated with long-term treatment effects, indicating its role in resistance.

Abstract

At single-cell level, our findings demonstrate a picture of transcriptional heterogeneity in the tumor compartment and immune milieu. Overall, these findings highlight transcriptional changes in circulating immune cells associated with ibrutinib resistance, suggesting that T-cell exhaustion and monocyte polarization accompany and may contribute to resistance during long-term BTKi therapy.

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