PD-1 blockade and CDK4/6 inhibition augment nonoverlapping features of T cell activation in cancer

Lestat R. Ali; Ana C. Garrido-Castro; Patrick J. Lenehan; Naima Bollenrucher; Courtney T. Stump; Michael Dougan; Shom Goel; Geoffrey I. Shapiro; Sara M. Tolaney; Stephanie K. Dougan

Journal ArticleOPEN ACCESS

PD-1 blockade and CDK4/6 inhibition augment nonoverlapping features of T cell activation in cancer

Journal of Experimental Medicine (2023) 220(4)

DOI: 10.1084/jem.20220729

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Abstract

We performed single-cell RNA-sequencing and T cell receptor clonotype tracking of breast and ovarian cancer patients treated with the CDK4/6 inhibitor ribociclib and PD-1 blockade. We highlight evidence of two orthogonal treatment-associated phenomena: expansion of T cell effector populations and promotion of T cell memory formation. Augmentation of the antitumor memory pool by ribociclib boosts the efficacy of subsequent PD-1 blockade in mouse models of melanoma and breast cancer, pointing toward sequential therapy as a potentially safe and synergistic strategy in patients.

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Ali, L. R., Garrido-Castro, A. C., Lenehan, P. J., Bollenrucher, N., Stump, C. T., Dougan, M., … Dougan, S. K. (2023). PD-1 blockade and CDK4/6 inhibition augment nonoverlapping features of T cell activation in cancer. Journal of Experimental Medicine, 220(4). https://doi.org/10.1084/jem.20220729

PD-1 blockade and CDK4/6 inhibition augment nonoverlapping features of T cell activation in cancer

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