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Dual targeting of CDK4/6 and CDK7 augments tumor response and antitumor immunity in breast cancer models
Sungsoo Kim, Eugene Son, Ha-Ram Park, Minah Kim, Hee Won Yang
Sungsoo Kim, Eugene Son, Ha-Ram Park, Minah Kim, Hee Won Yang
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Research Article Cell biology Oncology

Dual targeting of CDK4/6 and CDK7 augments tumor response and antitumor immunity in breast cancer models

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Abstract

Cyclin-dependent kinase 4/6 inhibitors (CDK4/6i) have transformed the treatment landscape for hormone receptor+ (HR+) breast cancer. However, their long-term efficacy is limited by acquired resistance, and CDK4/6i monotherapy remains ineffective in triple-negative breast cancer (TNBC). Here, we demonstrate that dual inhibition of CDK4/6 and CDK7 is a promising strategy to overcome therapeutic resistance in both HR+ and TNBC models. Kinetic analyses revealed that CDK7 inhibitors (CDK7i) primarily impair RNA polymerase II–mediated transcription rather than directly targeting cell cycle CDKs. This transcriptional suppression attenuated E2F-driven transcriptional amplification, a key mechanism for developing CDK4/6i resistance following the degradation of the retinoblastoma protein. Consequently, combining CDK7i at minimal effective concentrations with CDK4/6i potently inhibited the growth of drug-resistant tumors. Furthermore, dual CDK4/6 and CDK7 inhibition stimulated immune-related signaling and cytokine production in cancer cells, promoting antitumor immune responses within the tumor microenvironment. These findings provide mechanistic insights into CDK inhibition and support the therapeutic potential of combining CDK7i with CDK4/6i for breast cancer treatment.

Authors

Sungsoo Kim, Eugene Son, Ha-Ram Park, Minah Kim, Hee Won Yang

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Figure 7

Immune cell dynamics in the TME following CDK4/6i and CDK7i treatment.

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Immune cell dynamics in the TME following CDK4/6i and CDK7i treatment.
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(A and B) UMAP plots of single-cell transcriptomes from AT3OVA tumors in total (A), control (B, left), and combination-treated (50 mg/kg palbociclib and 2 mg/kg SY5609) (B, right) groups (n = 2 mice/group). (C) Stacked bar plot showing relative proportions of immune, cancer, and stromal cells in control and combination groups. (D) Quantification of major immune cell populations in control and combination groups. (E and F) UMAP plots of T cell subpopulations in total (E), control (F, top), and combination-treated (F, bottom) tumors. (G) Quantification of CD8+ and CD4+ T cell subtypes in control and combination groups. (H) Quantification of activated B (CD69+ or CD83+) and NK (GZMB+ or PRFN1+) cells in control and combination groups.

Copyright © 2026 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)

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