Chemotherapy Coupled to Macrophage Inhibition Induces T-cell and B-cell Infiltration and Durable Regression in Triple-Negative Breast Cancer

Swarnima Singh; Nigel Lee; Diego A. Pedroza; Igor L. Bado; Clark Hamor; Licheng Zhang; Sergio Aguirre; Jingyuan Hu; Yichao Shen; Yitian Xu; Yang Gao; Na Zhao; Shu Hsia Chen; Ying Wooi Wan; Zhandong Liu; Jeffrey T. Chang; Daniel Hollern; Charles M. Perou; Xiang H.F. Zhang; Jeffrey M. Rosen

doi:10.1158/0008-5472.CAN-21-3714

Chemotherapy Coupled to Macrophage Inhibition Induces T-cell and B-cell Infiltration and Durable Regression in Triple-Negative Breast Cancer

Swarnima Singh, Nigel Lee, Diego A. Pedroza, Igor L. Bado, Clark Hamor, Licheng Zhang, Sergio Aguirre, Jingyuan Hu, Yichao Shen, Yitian Xu, Yang Gao, Na Zhao, Shu Hsia Chen, Ying Wooi Wan, Zhandong Liu, Jeffrey T. Chang, Daniel Hollern, Charles M. Perou, Xiang H.F. Zhang, Jeffrey M. Rosen

Graduate School of Biomedical Sciences

Research output: Contribution to journal › Article › peer-review

39 Scopus citations

Abstract

Immunosuppressive elements within the tumor microenvironment, such as tumor-associated macrophages (TAM), can present a barrier to successful antitumor responses by cytolytic T cells. Here we employed preclinical syngeneic p53 null mouse models of triple-negative breast cancer (TNBC) to develop a treatment regimen that harnessed the immunostimulatory effects of low-dose cyclophosphamide coupled with the pharmacologic inhibition of TAMs using either a small-molecule CSF1R inhibitor or an anti-CSF1R antibody. This therapeutic combination was effective in treating several highly aggressive TNBC murine mammary tumor and lung metastasis models. Single-cell RNA sequencing characterized tumor-infiltrating lymphocytes including Th cells and antigen-presenting B cells that were highly enriched in responders to combination therapy. In one model that exhibited long-term posttreatment tumor regression, high-dimensional imaging techniques identified the close spatial localization of B220^þ/CD86^þ-activated B cells and CD4^þ T cells in tertiary lymphoid structures that were present up to 6 weeks posttreatment. The transcriptional and metabolic heterogeneity of TAMs was also characterized in two closely related claudin-low/mesenchymal subtype tumor models with differential treatment responses. A murine TAM signature derived from the T12 model was highly conserved in human claudin-low breast cancers, and high expression of the TAM signature correlated with reduced overall survival in patients with breast cancer. This TAM signature may help identify human patients with claudin-low breast cancer that will benefit from the combination of cyclophosphamide and anti-CSF1R therapy. These studies illustrate the complexity of the tumor immune microenvironment and highlight different immune responses that result from rational immunotherapy combinations. Significance: Immunostimulatory chemotherapy combined with pharmacologic inhibition of TAMs results in durable treatment responses elicited by Th cells and B cells in claudin-low TNBC models.

Original language	English (US)
Pages (from-to)	2281-2297
Number of pages	17
Journal	Cancer Research
Volume	82
Issue number	12
DOIs	https://doi.org/10.1158/0008-5472.CAN-21-3714
State	Published - Jun 15 2022

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1158/0008-5472.CAN-21-3714

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Singh, S., Lee, N., Pedroza, D. A., Bado, I. L., Hamor, C., Zhang, L., Aguirre, S., Hu, J., Shen, Y., Xu, Y., Gao, Y., Zhao, N., Chen, S. H., Wan, Y. W., Liu, Z., Chang, J. T., Hollern, D., Perou, C. M., Zhang, X. H. F., & Rosen, J. M. (2022). Chemotherapy Coupled to Macrophage Inhibition Induces T-cell and B-cell Infiltration and Durable Regression in Triple-Negative Breast Cancer. Cancer Research, 82(12), 2281-2297. https://doi.org/10.1158/0008-5472.CAN-21-3714

Singh, S, Lee, N, Pedroza, DA, Bado, IL, Hamor, C, Zhang, L, Aguirre, S, Hu, J, Shen, Y, Xu, Y, Gao, Y, Zhao, N, Chen, SH, Wan, YW, Liu, Z, Chang, JT, Hollern, D, Perou, CM, Zhang, XHF & Rosen, JM 2022, 'Chemotherapy Coupled to Macrophage Inhibition Induces T-cell and B-cell Infiltration and Durable Regression in Triple-Negative Breast Cancer', Cancer Research, vol. 82, no. 12, pp. 2281-2297. https://doi.org/10.1158/0008-5472.CAN-21-3714

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title = "Chemotherapy Coupled to Macrophage Inhibition Induces T-cell and B-cell Infiltration and Durable Regression in Triple-Negative Breast Cancer",

abstract = "Immunosuppressive elements within the tumor microenvironment, such as tumor-associated macrophages (TAM), can present a barrier to successful antitumor responses by cytolytic T cells. Here we employed preclinical syngeneic p53 null mouse models of triple-negative breast cancer (TNBC) to develop a treatment regimen that harnessed the immunostimulatory effects of low-dose cyclophosphamide coupled with the pharmacologic inhibition of TAMs using either a small-molecule CSF1R inhibitor or an anti-CSF1R antibody. This therapeutic combination was effective in treating several highly aggressive TNBC murine mammary tumor and lung metastasis models. Single-cell RNA sequencing characterized tumor-infiltrating lymphocytes including Th cells and antigen-presenting B cells that were highly enriched in responders to combination therapy. In one model that exhibited long-term posttreatment tumor regression, high-dimensional imaging techniques identified the close spatial localization of B220{\th}/CD86{\th}-activated B cells and CD4{\th} T cells in tertiary lymphoid structures that were present up to 6 weeks posttreatment. The transcriptional and metabolic heterogeneity of TAMs was also characterized in two closely related claudin-low/mesenchymal subtype tumor models with differential treatment responses. A murine TAM signature derived from the T12 model was highly conserved in human claudin-low breast cancers, and high expression of the TAM signature correlated with reduced overall survival in patients with breast cancer. This TAM signature may help identify human patients with claudin-low breast cancer that will benefit from the combination of cyclophosphamide and anti-CSF1R therapy. These studies illustrate the complexity of the tumor immune microenvironment and highlight different immune responses that result from rational immunotherapy combinations. Significance: Immunostimulatory chemotherapy combined with pharmacologic inhibition of TAMs results in durable treatment responses elicited by Th cells and B cells in claudin-low TNBC models.",

author = "Swarnima Singh and Nigel Lee and Pedroza, {Diego A.} and Bado, {Igor L.} and Clark Hamor and Licheng Zhang and Sergio Aguirre and Jingyuan Hu and Yichao Shen and Yitian Xu and Yang Gao and Na Zhao and Chen, {Shu Hsia} and Wan, {Ying Wooi} and Zhandong Liu and Chang, {Jeffrey T.} and Daniel Hollern and Perou, {Charles M.} and Zhang, {Xiang H.F.} and Rosen, {Jeffrey M.}",

note = "Publisher Copyright: {\textcopyright} 2022 American Association for Cancer Research",

year = "2022",

month = jun,

day = "15",

doi = "10.1158/0008-5472.CAN-21-3714",

language = "English (US)",

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AU - Singh, Swarnima

AU - Lee, Nigel

AU - Pedroza, Diego A.

AU - Bado, Igor L.

AU - Hamor, Clark

AU - Zhang, Licheng

AU - Aguirre, Sergio

AU - Hu, Jingyuan

AU - Shen, Yichao

AU - Xu, Yitian

AU - Gao, Yang

AU - Zhao, Na

AU - Chen, Shu Hsia

AU - Wan, Ying Wooi

AU - Liu, Zhandong

AU - Chang, Jeffrey T.

AU - Hollern, Daniel

AU - Perou, Charles M.

AU - Zhang, Xiang H.F.

AU - Rosen, Jeffrey M.

PY - 2022/6/15

Y1 - 2022/6/15

N2 - Immunosuppressive elements within the tumor microenvironment, such as tumor-associated macrophages (TAM), can present a barrier to successful antitumor responses by cytolytic T cells. Here we employed preclinical syngeneic p53 null mouse models of triple-negative breast cancer (TNBC) to develop a treatment regimen that harnessed the immunostimulatory effects of low-dose cyclophosphamide coupled with the pharmacologic inhibition of TAMs using either a small-molecule CSF1R inhibitor or an anti-CSF1R antibody. This therapeutic combination was effective in treating several highly aggressive TNBC murine mammary tumor and lung metastasis models. Single-cell RNA sequencing characterized tumor-infiltrating lymphocytes including Th cells and antigen-presenting B cells that were highly enriched in responders to combination therapy. In one model that exhibited long-term posttreatment tumor regression, high-dimensional imaging techniques identified the close spatial localization of B220þ/CD86þ-activated B cells and CD4þ T cells in tertiary lymphoid structures that were present up to 6 weeks posttreatment. The transcriptional and metabolic heterogeneity of TAMs was also characterized in two closely related claudin-low/mesenchymal subtype tumor models with differential treatment responses. A murine TAM signature derived from the T12 model was highly conserved in human claudin-low breast cancers, and high expression of the TAM signature correlated with reduced overall survival in patients with breast cancer. This TAM signature may help identify human patients with claudin-low breast cancer that will benefit from the combination of cyclophosphamide and anti-CSF1R therapy. These studies illustrate the complexity of the tumor immune microenvironment and highlight different immune responses that result from rational immunotherapy combinations. Significance: Immunostimulatory chemotherapy combined with pharmacologic inhibition of TAMs results in durable treatment responses elicited by Th cells and B cells in claudin-low TNBC models.

AB - Immunosuppressive elements within the tumor microenvironment, such as tumor-associated macrophages (TAM), can present a barrier to successful antitumor responses by cytolytic T cells. Here we employed preclinical syngeneic p53 null mouse models of triple-negative breast cancer (TNBC) to develop a treatment regimen that harnessed the immunostimulatory effects of low-dose cyclophosphamide coupled with the pharmacologic inhibition of TAMs using either a small-molecule CSF1R inhibitor or an anti-CSF1R antibody. This therapeutic combination was effective in treating several highly aggressive TNBC murine mammary tumor and lung metastasis models. Single-cell RNA sequencing characterized tumor-infiltrating lymphocytes including Th cells and antigen-presenting B cells that were highly enriched in responders to combination therapy. In one model that exhibited long-term posttreatment tumor regression, high-dimensional imaging techniques identified the close spatial localization of B220þ/CD86þ-activated B cells and CD4þ T cells in tertiary lymphoid structures that were present up to 6 weeks posttreatment. The transcriptional and metabolic heterogeneity of TAMs was also characterized in two closely related claudin-low/mesenchymal subtype tumor models with differential treatment responses. A murine TAM signature derived from the T12 model was highly conserved in human claudin-low breast cancers, and high expression of the TAM signature correlated with reduced overall survival in patients with breast cancer. This TAM signature may help identify human patients with claudin-low breast cancer that will benefit from the combination of cyclophosphamide and anti-CSF1R therapy. These studies illustrate the complexity of the tumor immune microenvironment and highlight different immune responses that result from rational immunotherapy combinations. Significance: Immunostimulatory chemotherapy combined with pharmacologic inhibition of TAMs results in durable treatment responses elicited by Th cells and B cells in claudin-low TNBC models.

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Chemotherapy Coupled to Macrophage Inhibition Induces T-cell and B-cell Infiltration and Durable Regression in Triple-Negative Breast Cancer

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