Local Delivery of Interleukin 7 with an Oncolytic Adenovirus Activates Tumor-infiltrating Lymphocytes and Causes Tumor Regression

Overview

Journal Oncoimmunology

Specialty Allergy & Immunology

Date 2022 Jul 18

PMID 35845722

Authors

Tatiana V Kudling

James H A Clubb

Dafne C A Quixabeira

Joao M Santos

Riikka Havunen

Alexander Kononov

Camilla Heinio

Victor Cervera-Carrascon

Santeri Pakola

Saru Basnet

Susanna Gronberg-Vaha-Koskela

Victor Arias

Ivan Gladwyn-Ng

Katri Aro

Leif Back

Jari Rasanen

Ilkka Ilonen

Kristian Borenius

Mikko Rasanen

Otto Hemminki

Antti Rannikko

Anna Kanerva

Johanna Tapper

Akseli Hemminki

Affiliations

Soon will be listed here.

Abstract

Cytokines have proven to be effective for cancer therapy, however whilst low-dose monotherapy with cytokines provides limited therapeutic benefit, high-dose treatment can lead to a number of adverse events. Interleukin 7 has shown promising results in clinical trials, but anti-cancer effect was limited, in part due to a low concentration of the cytokine within the tumor. We hypothesized that arming an oncolytic adenovirus with Interleukin 7, enabling high expression localized to the tumor microenvironment, would overcome systemic delivery issues and improve therapeutic efficacy. We evaluated the effects of Ad5/3-E2F-d24-hIL7 (TILT-517) on tumor growth, immune cell activation and cytokine profiles in the tumor microenvironment using three clinically relevant animal models and tumor cultures. Our data showed that local treatment of tumor bearing animals with Ad5/3- E2F-d24-hIL7 significantly decreased cancer growth and increased frequency of tumor-infiltrating cells. Ad5/3-E2F-d24-hIL7 promoted notable upregulation of pro-inflammatory cytokines, and concomitant activation and migration of CD4+ and CD8 + T cells. Interleukin 7 expression within the tumor was positively correlated with increased number of cytotoxic CD4+ cells and IFNg-producing CD4+ and CD8+ cells. These findings offer an approach to overcome the current limitations of conventional IL7 therapy and could therefore be translated to the clinic.

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