Leukocyte Complexity Predicts Breast Cancer Survival and Functionally Regulates Response to Chemotherapy

David G. DeNardo; Donal J. Brennan; Elton Rexhepaj; Brian Ruffell; Stephen L. Shiao; Stephen F. Madden; William M. Gallagher; Nikhil Wadhwani; Scott D. Keil; Sharfaa A. Junaid; Hope S. Rugo; E. Shelley Hwang; Karin Jirström; Brian L. West; Lisa M. Coussens

doi:10.1158/2159-8274.cd-10-0028

Leukocyte Complexity Predicts Breast Cancer Survival and Functionally Regulates Response to Chemotherapy

David G. DeNardo(University College Dublin), Donal J. Brennan(University College Dublin), Elton Rexhepaj(University College Dublin), Brian Ruffell(University College Dublin), Stephen L. Shiao(University College Dublin), Stephen F. Madden(University College Dublin), William M. Gallagher(University College Dublin), Nikhil Wadhwani(University College Dublin), Scott D. Keil(University College Dublin), Sharfaa A. Junaid(University College Dublin), Hope S. Rugo(University College Dublin), E. Shelley Hwang(University College Dublin), Karin Jirström(University College Dublin), Brian L. West(University College Dublin), Lisa M. Coussens(University College Dublin)

Cancer Discovery

April 8, 2011

10.1158/2159-8274.cd-10-0028

Cited by 1,717

Abstract

UNLABELLED: Immune-regulated pathways influence multiple aspects of cancer development. In this article we demonstrate that both macrophage abundance and T-cell abundance in breast cancer represent prognostic indicators for recurrence-free and overall survival. We provide evidence that response to chemotherapy is in part regulated by these leukocytes; cytotoxic therapies induce mammary epithelial cells to produce monocyte/macrophage recruitment factors, including colony stimulating factor 1 (CSF1) and interleukin-34, which together enhance CSF1 receptor (CSF1R)-dependent macrophage infiltration. Blockade of macrophage recruitment with CSF1R-signaling antagonists, in combination with paclitaxel, improved survival of mammary tumor-bearing mice by slowing primary tumor development and reducing pulmonary metastasis. These improved aspects of mammary carcinogenesis were accompanied by decreased vessel density and appearance of antitumor immune programs fostering tumor suppression in a CD8+ T-cell-dependent manner. These data provide a rationale for targeting macrophage recruitment/response pathways, notably CSF1R, in combination with cytotoxic therapy, and identification of a breast cancer population likely to benefit from this novel therapeutic approach. SIGNIFICANCE: These findings reveal that response to chemotherapy is in part regulated by the tumor immune microenvironment and that common cytotoxic drugs induce neoplastic cells to produce monocyte/macrophage recruitment factors, which in turn enhance macrophage infiltration into mammary adenocarcinomas. Blockade of pathways mediating macrophage recruitment, in combination with chemotherapy, significantly decreases primary tumor progression, reduces metastasis, and improves survival by CD8+ T-cell-dependent mechanisms, thus indicating that the immune microenvironment of tumors can be reprogrammed to instead foster antitumor immunity and improve response to cytotoxic therapy.

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