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. 2024 Dec 26;187(26):7470-7491.e32.
doi: 10.1016/j.cell.2024.10.016. Epub 2024 Nov 5.

Multimodal targeting chimeras enable integrated immunotherapy leveraging tumor-immune microenvironment

Affiliations

Multimodal targeting chimeras enable integrated immunotherapy leveraging tumor-immune microenvironment

Feng Lin et al. Cell. .

Abstract

Although immunotherapy has revolutionized cancer treatment, its efficacy is affected by multiple factors, particularly those derived from the complexity and heterogeneity of the tumor-immune microenvironment (TIME). Strategies that simultaneously and synergistically engage multiple immune cells in TIME remain highly desirable but challenging. Herein, we report a multimodal and programmable platform that enables the integration of multiple therapeutic modules into single agents for tumor-targeted co-engagement of multiple immune cells within TIME. We developed the triple orthogonal linker (T-Linker) technology to integrate various therapeutic small molecules and biomolecules as multimodal targeting chimeras (Multi-TACs). The EGFR-CD3-PDL1 Multi-TAC facilitated T-dendritic cell co-engagement to target solid tumors with excellent efficacy, as demonstrated in vitro, in several humanized mouse models and in patient-derived tumor models. Furthermore, Multi-TACs were constructed to coordinate T cells with other immune cell types. The highly modular and programmable feature of our Multi-TACs may find broad applications in immunotherapy and beyond.

Keywords: T cell engager; antibody conjugates; bioorthogonal chemistry; dendritic cell engager; integrated immunotherapy; multi-cell co-engagement; multispecific drugs; triple orthogonal linker; tumor-immune microenvironment.

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Conflict of interest statement

Declaration of interests P.R.C., F.L., J. Lin, and H. Zhang are listed as inventors on a patent application (PCT/CN2021/130337) filed on this work through Peking University.

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