Targeting CXCL16 and STAT1 augments immune checkpoint blockade therapy in triple-negative breast cancer.
Bhavana PalakurthiShaneann R FrossIan H GuldnerEmilija AleksandrovicXiyu LiuAnna K MartinoQingfei WangRyan A NeffSamantha M GolombCheryl M LewisYan PengErin N HoweSiyuan ZhangPublished in: Nature communications (2023)
Chemotherapy prior to immune checkpoint blockade (ICB) treatment appears to improve ICB efficacy but resistance to ICB remains a clinical challenge and is attributed to highly plastic myeloid cells associating with the tumor immune microenvironment (TIME). Here we show by CITE-seq single-cell transcriptomic and trajectory analyses that neoadjuvant low-dose metronomic chemotherapy (MCT) leads to a characteristic co-evolution of divergent myeloid cell subsets in female triple-negative breast cancer (TNBC). Specifically, we identify that the proportion of CXCL16 + myeloid cells increase and a high STAT1 regulon activity distinguishes Programmed Death Ligand 1 (PD-L1) expressing immature myeloid cells. Chemical inhibition of STAT1 signaling in MCT-primed breast cancer sensitizes TNBC to ICB treatment, which underscores the STAT1's role in modulating TIME. In summary, we leverage single-cell analyses to dissect the cellular dynamics in the tumor microenvironment (TME) following neoadjuvant chemotherapy and provide a pre-clinical rationale for modulating STAT1 in combination with anti-PD-1 for TNBC patients.
Keyphrases
- single cell
- induced apoptosis
- neoadjuvant chemotherapy
- locally advanced
- rna seq
- cell proliferation
- low dose
- bone marrow
- signaling pathway
- cell cycle arrest
- acute myeloid leukemia
- dendritic cells
- rectal cancer
- endoplasmic reticulum stress
- high throughput
- clinical trial
- prognostic factors
- oxidative stress
- immune response
- ejection fraction
- gene expression
- high dose
- sentinel lymph node