Systemic oncolytic adenovirus delivered in mesenchymal carrier cells modulate tumor infiltrating immune cells and tumor microenvironment in mice with neuroblastoma.

Lidia Franco-Luzón,Lorena García-García,Manuel Ramírez,Cristina Alcántara-Sánchez,Ana Luis Huertas,Louis Chesler,África González-Murillo,Maryam Tabasi

doi:10.18632/oncotarget.27401

Abstract

Celyvir (autologous mesenchymal cells -MSCs- that carry an oncolytic adenovirus) is a new therapeutic strategy for metastatic tumors developed by our research group over the last decade. There are limitations for studying the immune effects of human oncolytic adenoviruses in murine models since these viruses do not replicate naturally in these animals. The use of xenografts in immunodeficient mice prevent assessing important clinical aspects of this therapy such as the antiadenoviral immune response or the possible intratumoral immune changes, both of tumor infiltrating leukocytes and of the microenvironment. In our strategy, the presence of MSCs in the medicinal product adds an extra level of complexity. We present here a murine model that overcomes many of these limitations. We found that carrier cells outcompeted intravenous administration of naked particles in delivering the oncolytic virus into the tumor masses. The protection that MSCs could provide to the oncolytic adenovirus did not preclude the development of an antiadenoviral immune response. However, the presence of circulating antiadenoviral antibodies did not prevent changes detected at the tumor masses: increased infiltration and changes in the quality of immune cells per unit of tumor volume, and a less protumoral and more inflammatory profile of the tumor microenvironment. We believe that the model described here will enable the study of crucial events related to the immune responses affecting both the medicinal product and the tumor.

Highlights

Celyvir is a new therapeutic strategy for metastatic tumors developed by our research group over the last decade
Nowadays it is assumed that oncolytic virotherapy can be considered as a form of cancer immunotherapy [4], since the reported clinical benefits have been associated with antitumor immune phenomena initiated by infection and oncolysis
Murine mesenchymal stem cells (MSC) were infected with MAV-1 dlE102 (mAd) and viral replication was assessed by quantitative PCR

Summary

Introduction

Celyvir (autologous mesenchymal cells -MSCsthat carry an oncolytic adenovirus [1] inside) is a new therapeutic strategy for metastatic tumors developed by our research group over the last decade. Results of preclinical models and human trials demonstrate that the localized effect of oncolytic viruses is capable of activating an inflammatory immune infiltrate in tumors. This point is of vital importance, since it is known that tumor infiltration by T lymphocytes is a prerequisite for the success of immunotherapies based on inhibitors of immune checkpoints [5]. Celyvir, appears as a strategy capable of achieving tumor infiltration by lymphocytes in any type of tumor, in principle. In addition to its action on tumor infiltrating leukocytes, oncolytic virotherapies can act on the tolerant state of the tumor microenvironment [6]

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Results

Conclusion