Abstract
Innate and type 1 cell-mediated cytotoxic immunity function as important extracellular control mechanisms that maintain cellular homeostasis. Interleukin-12 (IL12) is an important cytokine that links innate immunity with type 1 cell-mediated cytotoxic immunity. We recently observed in vitro that tumor-derived Wnt-inducible signaling protein-1 (WISP1) exerts paracrine action to suppress IL12 signaling. The objective of this retrospective study was three fold: 1) to determine whether a gene signature associated with type 1 cell-mediated cytotoxic immunity was correlated with overall survival, 2) to determine whether WISP1 expression is increased in invasive breast cancer, and 3) to determine whether a gene signature consistent with inhibition of IL12 signaling correlates with WISP1 expression. Clinical information and mRNA expression for genes associated with anti-tumor immunity were obtained from the invasive breast cancer arm of the Cancer Genome Atlas study. Patient cohorts were identified using hierarchical clustering. The immune signatures associated with the patient cohorts were interpreted using model-based inference of immune polarization. Reverse phase protein array, tissue microarray, and quantitative flow cytometry in breast cancer cell lines were used to validate observed differences in gene expression. We found that type 1 cell-mediated cytotoxic immunity was correlated with increased survival in patients with invasive breast cancer, especially in patients with invasive triple negative breast cancer. Oncogenic transformation in invasive breast cancer was associated with an increase in WISP1. The gene expression signature in invasive breast cancer was consistent with WISP1 as a paracrine inhibitor of type 1 cell-mediated immunity through inhibiting IL12 signaling and promoting type 2 immunity. Moreover, model-based inference helped identify appropriate immune signatures that can be used as design constraints in genetically engineering better pre-clinical models of breast cancer.
Highlights
The discovery of molecular targeted therapies revolutionized the treatment of breast cancer
We used model-based inference to demonstrate that a gene signature consistent with effective type 1 cell-mediated cytotoxic immunity is a predictor of overall survival independent of molecular pathology
We found that GATA3 expression was correlated with WISP1 and that GATA3 was up-regulated in invasive breast cancer compared to normal tissue
Summary
The discovery of molecular targeted therapies revolutionized the treatment of breast cancer. Trastuzumab was developed to inhibit the growth of breast cancer cells that overexpress HER2, an oncogenic member of the epidermal growth factor family of receptors [1] Based upon their demonstrated clinical impact, a pre-operative biopsy sample is used to guide treatment based upon expression of the hormone receptors for estrogen (ER) and progesterone (PR) and the epidermal growth factor receptor HER2 [2]. While these molecular targeted therapies have improved survival, de novo and acquired resistance to these therapies present challenges for achieving a durable clinical response [3,4].
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