Lysosomes Targeting pH Activable Imaging‐Guided Photodynamic Agents

Author:

Figliola Carlotta1ORCID,Anton Halina2ORCID,Sutter Christophe1,Chériaux Camille1,Sutter Alexandra1ORCID,Mazan Valérie3ORCID,Elhabiri Mourad3ORCID,Didier Pascal2ORCID,Jacquemin Denis45ORCID,Ulrich Gilles1ORCID

Affiliation:

1. Institut de Chimie pour l'Energie l'Environnement et la Santé (ICPEES) UMR CNRS 7515 Université de Strasbourg 25 rue Becquerel 67087 Strasbourg Cedex 02 France

2. Laboratoire de Bioimagerie et Pathologies UMR CNRS 7021 Faculté de Pharmacie Université de Strasbourg 74 Route du Rhin 67401 Illkirch Cedex France

3. Laboratoire d'Innovation Moléculaire et Applications (LIMA) UMR CNRS 7042 Université de Strasbourg 25 rue Becquerel 67087 Strasbourg Cedex 02 France

4. Nantes Université CNRS, CEISAM UMR 6230 44000 Nantes France

5. Institut Universitaire de France (IUF) 75005 Paris France

Abstract

AbstractPhotodynamic therapy (PDT) is a photochemistry‐based medical treatment combining light at a specific wavelength and a photosensitizer (PS) in the presence of oxygen. Application of PDT as a conventional treatment is limited and clearly the approval in clinics of new PS is challenging. The selective accumulation of the PS in the targeted malignant cells is of paramount importance to reduce the side effects that are typical of the current worldwide approved PS. Here we report a new series of aniline‐ and iodine‐substituted BODIPY derivatives (13) as promising lysosome‐targeting and pH‐responsive theranostic PS, which displayed a significant in vitro light‐induced cytotoxicity, efficient imaging properties and low dark toxicity (for 2 and 3). These compounds were obtained in few reproducible synthetic steps and good yields. Spectroscopic and electrochemical measurements along with computational calculations confirmed the quenching of the emissive properties of the PS, while both fluorescence and 1O2 emission were obtained only under acidic conditions inducing amine protonation. The pKa values and pH‐dependent emissive properties of 13 being established, their cellular uptake and activation in the lysosomal vesicles (pH≈4‐5) were confirmed by their co‐localization with the commercial LysoTracker deep red and light‐induced cytotoxicity (IC50 between 0.16 and 0.06 μM) against HeLa cancer cells.

Publisher

Wiley

Subject

Organic Chemistry,Molecular Biology,Molecular Medicine,Biochemistry

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