# Oncolytic adenoviruses encoding bispecific T cell engagers or a novel trispecific T cell engager for dual-targeting of c-MET and EGFR

**Authors:** Martin A. Boos, Oliver Seifert, Stefanie Sawall, Jessica Genz, Annika Huber, Ilse Hofmann, Roland E. Kontermann, Guy Ungerechts, Dirk M. Nettelbeck

PMC · DOI: 10.1016/j.omton.2025.201106 · 2025-12-09

## TL;DR

Researchers developed a new approach using oncolytic viruses to target two tumor proteins, EGFR and c-MET, using bispecific and trispecific T cell engagers to combat tumor diversity.

## Contribution

The study introduces novel bispecific and trispecific T cell engagers encoded by oncolytic adenoviruses for dual-targeting tumor antigens.

## Key findings

- Bispecific TCEs scDb-cMET and taFv-EGFR showed efficacy in vitro.
- The trispecific Db-TriTE scDb-cMET-scFv-EGFR demonstrated superior dual-targeting and cytotoxicity.
- Oncolytic adenoviruses encoding TCEs induced T cell activation and cytotoxicity in co-cultures.

## Abstract

This study reports a strategy to overcome immune escape of tumors during viro-immunotherapy due to tumor heterogeneity. We pursued a dual-targeting approach of epidermal growth factor receptor (EGFR) and cellular mesenchymal epithelial transition factor (c-MET) facilitated by two bispecific T cell engagers (TCEs) or one trispecific TCE encoded by oncolytic adenoviruses (oAds). Different bi- and trispecific TCE formats were generated and characterized. We showed efficacy of bispecific TCEs single-chain diabody (scDb)-cMET and tandem scFv (taFv)-EFGR in vitro, encouraging the design of the diabody-based trispecific TCE (Db-TriTE) scDb-cMET-scFv-EGFR. The Db-TriTE exhibited effective dual-targeting, i.e., the induction of cytotoxicity for single-positive cells of both targets and superior efficacy on double-positive cells. Therefore, a panel of oAds was produced to test different TCE (co-)expression strategies. Our results showed no or minor attenuation of viruses harboring the transgenes for one of the analyzed insertion strategies, expression of TCEs, and specific induction of both T cell activation and cytotoxicity in co-cultures of infected tumor cells with peripheral blood mononuclear cells (PBMCs). Importantly, we demonstrated dual-targeting by oAds encoding the two bispecific TCEs or the Db-TriTE with the latter featuring superior genomic stability and the overall highest efficacy. Taken together, we report novel bi- and trispecific TCEs and proof of principle for their application as dual-targeted viro-antibody therapy.

Targeting two distinct antigens via bi- or trispecific T cell engagers encoded by oncolytic adenoviruses is explored to address the problem of tumor heterogeneity. Different antibody formats and expression strategies are investigated in vitro, establishing a promising platform for next-generation, dual-targeted viro-immunotherapy.

## Linked entities

- **Genes:** EGFR (epidermal growth factor receptor) [NCBI Gene 1956], MET (MET proto-oncogene, receptor tyrosine kinase) [NCBI Gene 4233]

## Full-text entities

- **Genes:** EGFR (epidermal growth factor receptor) [NCBI Gene 1956] {aka ERBB, ERBB1, ERRP, HER1, NISBD2, NNCIS}, MET (MET proto-oncogene, receptor tyrosine kinase) [NCBI Gene 4233] {aka AUTS9, DA11, DFNB97, HGFR, RCCP2, c-Met}
- **Diseases:** cytotoxicity (MESH:D064420), tumor (MESH:D009369)
- **Chemicals:** TCE (-)

## Figures

7 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12804148/full.md

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Source: https://tomesphere.com/paper/PMC12804148