Affilin-based retargeting of adenoviral vectors to the epidermal growth factor receptor

Frederik Wienen; Robin Nilson; Ellen Allmendinger; David Graumann; Erik Fiedler; Eva Bosse-Doenecke; Stefan Kochanek; Lea Krutzke

doi:10.1016/j.bioadv.2022.213208

Affilin-based retargeting of adenoviral vectors to the epidermal growth factor receptor

Biomater Adv. 2023 Jan:144:213208. doi: 10.1016/j.bioadv.2022.213208. Epub 2022 Nov 23.

Authors

Frederik Wienen¹, Robin Nilson¹, Ellen Allmendinger¹, David Graumann¹, Erik Fiedler², Eva Bosse-Doenecke², Stefan Kochanek¹, Lea Krutzke³

Affiliations

¹ Department of Gene Therapy, University of Ulm, Helmholtzstraße 8/1, 89081 Ulm, Germany.
² Navigo Proteins GmbH, Heinrich-Damerow-Str. 1, 06120 Halle, Germany.
³ Department of Gene Therapy, University of Ulm, Helmholtzstraße 8/1, 89081 Ulm, Germany. Electronic address: lea.krutzke@uni-ulm.de.

PMID: 36442453
DOI: 10.1016/j.bioadv.2022.213208

Abstract

Introduction: Treatment of head and neck squamous cell carcinomas (HNSCC) by oncolytic adenoviral vectors holds promise as an efficient anti-cancer therapy. The epidermal growth factor receptor (EGFR) represents an attractive target receptor since it is frequently overexpressed in many types of HNSCC.

Methods: To achieve EGFR-specific targeting by human adenovirus type 5 (HAdV-5) based vectors, the EGFR affinity ligand Affilin was covalently attached in a position specific manner either to the fiber or the hexon protein of the vector capsid. In vitro and in vivo studies investigated EGFR-specific cancer cell transduction, susceptibility to natural sequestration mechanisms, pharmacokinetics and biodistribution profiles of Affilin-decorated vectors.

Results: Affilin-decorated vectors showed strongly enhanced and EGFR-specific cancer cell transduction in vitro and less susceptibility to known sequestration mechanisms of HAdV-5 particles. However, in vivo neither systemic nor intratumoral vector administration resulted in an improved transduction of EGFR-positive tumors. Comprehensive analyses indicated hampered EGFR-targeting by Affilin-decorated vectors was caused by rapid vector particle consumption due to binding to the murine EGFR, insufficient tumor vascularization and poor target accessibility for Affilin in the solid tumor caused by a pronounced tumor stroma.

Conclusion: In vitro studies yielded proof-of-concept results demonstrating that covalent attachment of a receptor-specific Affilin to the adenoviral capsid provides an effective and versatile tool to address cancer-specific target receptors by adenoviral vectors. Regarding EGFR as the vector target, off-target tissue transduction and low receptor accessibility within the tumor tissue prevented efficient tumor transduction by Affilin-decorated vectors, rendering EGFR a difficult-to-target receptor for adenoviral vectors.

Keywords: Adenovirus; Affilin; Cancer; Covalent linkage; Epidermal growth factor receptor; Gene therapy; Oncolytic virus; Retargeting ligand.

MeSH terms

Adenoviruses, Human* / metabolism
Animals
ErbB Receptors / genetics
ErbB Receptors / metabolism
Genetic Therapy / methods
Head and Neck Neoplasms* / therapy
Humans
Mice
Oncolytic Virotherapy*
Squamous Cell Carcinoma of Head and Neck* / therapy
Tissue Distribution
Transduction, Genetic

Substances

ErbB Receptors