Enzyme‐Activatable Near‐Infrared Hemicyanines as Modular Scaffolds for in vivo Photodynamic Therapy

Author:

Cheng Zhiming12,Benson Sam12,Mendive‐Tapia Lorena12,Nestoros Eleni12,Lochenie Charles12,Seah Deborah12,Chang Kai Yee1,Feng Yi13,Vendrell Marc12ORCID

Affiliation:

1. Centre for Inflammation Research The University of Edinburgh EH16 4UU Edinburgh UK

2. IRR Chemistry Hub, Institute for Regeneration and Repair The University of Edinburgh EH16 4UU Edinburgh UK

3. Cancer Research UK Scotland Centre, Institute of Genetics and Cancer The University of Edinburgh EH4 2XR Edinburgh UK

Abstract

AbstractPhotodynamic therapy is an anti‐cancer treatment that requires illumination of photosensitizers to induce local cell death. Current near‐infrared organic photosensitizers are built from large and non‐modular structures that cannot be tuned to improve safety and minimize off‐target toxicity. This work describes a novel chemical platform to generate enzyme‐activatable near‐infrared photosensitizers. We optimized the Se‐bridged hemicyanine scaffold to include caging groups and biocompatible moieties, and generated cathepsin‐triggered photosensitizers for effective ablation of human glioblastoma cells. Furthermore, we demonstrated that enzyme‐activatable Se‐bridged hemicyanines are effective photosensitizers for the safe ablation of microtumors in vivo, creating new avenues in the chemical design of targeted anti‐cancer photodynamic therapy agents.

Funder

Engineering and Physical Sciences Research Council

European Research Council

Cancer Research UK

Horizon 2020 Framework Programme

Publisher

Wiley

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