Identification of Cell Type-Specific Differences in Erythropoietin Receptor Signaling in Primary Erythroid and Lung Cancer Cells.

Ruth Merkle,Max Schelker,Christoph Plass,Ursula Klingmüller,Oliver Mücke,Florian Salopiata,Daniel B Lipka,Jens Timmer,Marcel Schilling,Helge Hass,Bernhard Steiert,Wolf D Lehmann,Andreas Raue,Martin E Böhm,Marvin Wäsch,Nao Iwamoto,Sofia Depner,Clemens Kreutz,Feilim Mac Gabhann

doi:10.1371/journal.pcbi.1005049

Abstract

Lung cancer, with its most prevalent form non-small-cell lung carcinoma (NSCLC), is one of the leading causes of cancer-related deaths worldwide, and is commonly treated with chemotherapeutic drugs such as cisplatin. Lung cancer patients frequently suffer from chemotherapy-induced anemia, which can be treated with erythropoietin (EPO). However, studies have indicated that EPO not only promotes erythropoiesis in hematopoietic cells, but may also enhance survival of NSCLC cells. Here, we verified that the NSCLC cell line H838 expresses functional erythropoietin receptors (EPOR) and that treatment with EPO reduces cisplatin-induced apoptosis. To pinpoint differences in EPO-induced survival signaling in erythroid progenitor cells (CFU-E, colony forming unit-erythroid) and H838 cells, we combined mathematical modeling with a method for feature selection, the L1 regularization. Utilizing an example model and simulated data, we demonstrated that this approach enables the accurate identification and quantification of cell type-specific parameters. We applied our strategy to quantitative time-resolved data of EPO-induced JAK/STAT signaling generated by quantitative immunoblotting, mass spectrometry and quantitative real-time PCR (qRT-PCR) in CFU-E and H838 cells as well as H838 cells overexpressing human EPOR (H838-HA-hEPOR). The established parsimonious mathematical model was able to simultaneously describe the data sets of CFU-E, H838 and H838-HA-hEPOR cells. Seven cell type-specific parameters were identified that included for example parameters for nuclear translocation of STAT5 and target gene induction. Cell type-specific differences in target gene induction were experimentally validated by qRT-PCR experiments. The systematic identification of pathway differences and sensitivities of EPOR signaling in CFU-E and H838 cells revealed potential targets for intervention to selectively inhibit EPO-induced signaling in the tumor cells but leave the responses in erythroid progenitor cells unaffected. Thus, the proposed modeling strategy can be employed as a general procedure to identify cell type-specific parameters and to recommend treatment strategies for the selective targeting of specific cell types.

Highlights

Lung carcinoma is one of the leading causes of cancer-related deaths worldwide
We show that the same signal transduction network induced by erythropoietin (EPO), a hormone that is frequently employed to treat anemia in cancer patients, regulates survival of both cell types
We previously showed that the non-small-cell lung carcinoma (NSCLC) cell line H838 expresses the EPO receptor (EPOR) at the mRNA and protein level, albeit at rather low levels [10]

Summary

Introduction

Lung carcinoma is one of the leading causes of cancer-related deaths worldwide. The main types of lung cancer are small-cell lung carcinoma (SCLC) and non-small-cell lung carcinoma (NSCLC). Because lung cancer metastasizes already at early stages independent of the tumor size [2], most of the patients receive chemotherapeutic agents such as cisplatin. Expression of the EPO receptor (EPOR) has been detected in some tumors and cancer cells including NSCLC cells [7,8,9,10]. Co-expression of EPO and the EPOR has been shown to be associated with poor survival of NSCLC patients, even at stage I [11]. Because of these ambivalent effects, the treatment of lung cancer patients with EPO in the context of cancer-related anemia is controversially discussed [12, 13]

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