Recombinant Adenoviral Vectors Have Adjuvant Activity and Stimulate T Cell Responses Against Tumor Cells

Overview

Journal Gene Ther

Date 2000 Sep 12

PMID 10981668

Citations 19

Authors

S B Geutskens

M M van der Eb

A C Plomp

L E Jonges

S J Cramer

N G Ensink

P J Kuppen

R C Hoeben

Affiliations

Soon will be listed here.

Abstract

The host-immune response against adenoviruses forms a major obstacle for their use as gene therapy vectors for treatment of genetic defects. None the less, they are the preferred vectors for in vivo gene transfer in experimental gene therapy protocols for cancer. In this article we demonstrate the antitumor efficacy of adenovirus-mediated transfer of human interleukin-2 cDNA in the rat-CC531 model for hepatic metastases of colorectal cancer: intratumoral administration of 10 plaque-forming units of the hlL-2-expressing adenoviral vector, AdCAIL-2, resulted in a cessation of tumor growth in 80% of the injected tumors. In control groups receiving AdCnull, a vector with the same viral backbone, but lacking transgene expression, none of the tumors responded. However, intratumoral treatment with this vector significantly enhanced tumor regression induced by systemic IL-2 protein treatment, which was used as a positive control. In addition we show, by performing delayed-type of hypersensitivity assays, that AdCnull when injected intratumorally enhances recognition of tumor antigens by T lymphocytes to the same extent as intratumoral treatment with the IL-2-expressing vector. The replication-deficient adenoviruses appear to have a therapeutic advantage in cytokine-mediated immunotherapy: even adenovirus vectors that do not express a transgene, show adjuvant activity and stimulate an antitumor immune response.

Citing Articles

Precise Gene Knock-In Tools with Minimized Risk of DSBs: A Trend for Gene Manipulation.

Liu Y, Kong J, Liu G, Li Z, Xiao Y Adv Sci (Weinh). 2024; 11(28):e2401797.

PMID: 38728624 PMC: 11267366. DOI: 10.1002/advs.202401797.

Clinical progress in genome-editing technology and in vivo delivery techniques.

Khirallah J, Eimbinder M, Li Y, Xu Q Trends Genet. 2023; 39(3):208-216.

PMID: 36669950 PMC: 9974761. DOI: 10.1016/j.tig.2022.12.001.

Therapeutic in vivo delivery of gene editing agents.

Raguram A, Banskota S, Liu D Cell. 2022; 185(15):2806-2827.

PMID: 35798006 PMC: 9454337. DOI: 10.1016/j.cell.2022.03.045.

CRISPR/Cas9-mediated genome editing: From basic research to translational medicine.

Jacinto F, Link W, Ferreira B J Cell Mol Med. 2020; 24(7):3766-3778.

PMID: 32096600 PMC: 7171402. DOI: 10.1111/jcmm.14916.

Pre-surgical neoadjuvant oncolytic virotherapy confers protection against rechallenge in a murine model of breast cancer.

Martin N, Roy D, Workenhe S, van den Wollenberg D, Hoeben R, Mossman K Sci Rep. 2019; 9(1):1865.

PMID: 30755678 PMC: 6372691. DOI: 10.1038/s41598-018-38385-7.