Priming of Anti-tumor Immune Mechanisms by Radiotherapy Is Augmented by Inhibition of Heat Shock Protein 90.

Anne Ernst,Kirsten Lauber,Christoph A Reichel,Udo S Gaipl,Nikko Brix,Senji Shirasawa,Heidi Kapfhammer,Gabriele Zuchtriegel,Julia Krombach,Benjamin Frey,Nicolas Winssinger,Takehiko Sasazuki,Claus Belka,Roman Hennel,Markus Sperandio,Bernd Uhl

doi:10.3389/fonc.2020.01668

Abstract

Radiotherapy is an essential part of multi-modal cancer therapy. Nevertheless, for certain cancer entities such as colorectal cancer (CRC) the indications of radiotherapy are limited due to anatomical peculiarities and high radiosensitivity of the surrounding normal tissue. The development of molecularly targeted, combined modality approaches may help to overcome these limitations. Preferably, such strategies should not only enhance radiation-induced tumor cell killing and the abrogation of tumor cell clonogenicity, but should also support the stimulation of anti-tumor immune mechanisms – a phenomenon which moved into the center of interest of preclinical and clinical research in radiation oncology within the last decade. The present study focuses on inhibition of heat shock protein 90 (HSP90) whose combination with radiotherapy has previously been reported to exhibit convincing therapeutic synergism in different preclinical cancer models. By employing in vitro and in vivo analyses, we examined if this therapeutic synergism also applies to the priming of anti-tumor immune mechanisms in model systems of CRC. Our results indicate that the combination of HSP90 inhibitor treatment and ionizing irradiation induced apoptosis in colorectal cancer cells with accelerated transit into secondary necrosis in a hyperactive Kras-dependent manner. During secondary necrosis, dying cancer cells released different classes of damage-associated molecular patterns (DAMPs) that stimulated migration and recruitment of monocytic cells in vitro and in vivo. Additionally, these dying cancer cell-derived DAMPs enforced the differentiation of a monocyte-derived antigen presenting cell (APC) phenotype which potently triggered the priming of allogeneic T cell responses in vitro. In summary, HSP90 inhibition – apart from its radiosensitizing potential – obviously enables and supports the initial steps of anti-tumor immune priming upon radiotherapy and thus represents a promising partner for combined modality approaches. The therapeutic performance of such strategies requires further in-depth analyses, especially for but not only limited to CRC.

Highlights

Radiotherapy is a cornerstone of multi-modal cancer treatment
We show that the combination of radiotherapy and heat shock protein 90 (HSP90) inhibitors (HSP90i) treatment induced apoptosis and accelerated transit into secondary necrosis in CRC cells with concomitant release of damage-associated molecular pattern (DAMP)
Apoptotic HCT116 Kirsten Rat Sarcoma virus protein (Kras)+/− Bcl-2-associated X protein (Bax)+/+ cells did not transit into secondary necrosis, and neither monocyte attraction nor DAMP release were observed. These results clearly suggest that DAMP release and attraction of monocytic cells after combined treatment with HSP90i and irradiation occur in the phase of post-apoptotic, secondary necrosis

Summary

Introduction

Radiotherapy is a cornerstone of multi-modal cancer treatment. Its therapeutic efficacy is primarily considered to derive from direct tumor cell killing and the abrogation of tumor cell clonogenicity [1, 2]. There is growing evidence for a relevant contribution of the immune system to local as well as distant tumor control, and the concept of cancer in situ vaccination by radiotherapy is receiving increasing acceptance [3, 4]. In this regard, the mode of cancer cell death induced by radiotherapy appears to be of fundamental importance. The priming of anti-tumor immune mechanisms has predominantly been observed in the context of necrotic forms of cell death due to the release of damage-associated molecular patterns (DAMPs) paralleled by the stimulation of an intra-tumoral type I interferon response [5, 6]. We and others have shown that DAMPs released from irradiated, dying tumor cells stimulate the activation of endothelial cells and the recruitment of antigen presenting cells (APCs) which crossprime CD8+ T cells in a type I interferon-dependent manner involving the cGAS/STING axis [8, 9, 11,12,13,14]

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Results

Conclusion