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Theranostic Properties of Crystalline Aluminum Phthalocyanine Nanoparticles as a Photosensitizer

The study of phthalocyanines, known photosensitizers, for biomedical applications has been of high research interest for several decades. Of specific interest, nanophotosensitizers are crystalline aluminum phthalocyanine nanoparticles (AlPc NPs). In crystalline form, they are water-insoluble and ato...

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Autores principales: Makarov, Vladimir I., Pominova, Daria V., Ryabova, Anastasiya V., Romanishkin, Igor D., Voitova, Arina V., Steiner, Rudolf W., Loschenov, Victor B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9611939/
https://www.ncbi.nlm.nih.gov/pubmed/36297557
http://dx.doi.org/10.3390/pharmaceutics14102122
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author Makarov, Vladimir I.
Pominova, Daria V.
Ryabova, Anastasiya V.
Romanishkin, Igor D.
Voitova, Arina V.
Steiner, Rudolf W.
Loschenov, Victor B.
author_facet Makarov, Vladimir I.
Pominova, Daria V.
Ryabova, Anastasiya V.
Romanishkin, Igor D.
Voitova, Arina V.
Steiner, Rudolf W.
Loschenov, Victor B.
author_sort Makarov, Vladimir I.
collection PubMed
description The study of phthalocyanines, known photosensitizers, for biomedical applications has been of high research interest for several decades. Of specific interest, nanophotosensitizers are crystalline aluminum phthalocyanine nanoparticles (AlPc NPs). In crystalline form, they are water-insoluble and atoxic, but upon contact with tumors, immune cells, or pathogenic microflora, they change their spectroscopic properties (acquire the ability to fluoresce and become phototoxic), which makes them upcoming agents for selective phototheranostics. Aqueous colloids of crystalline AlPc NPs with a hydrodynamic size of 104 ± 54 nm were obtained using ultrasonic dispersal and centrifugation. Intracellular accumulation and localization of AlPc were studied on HeLa and THP-1 cell cultures and macrophages (M0, M1, M2) by fluorescence microscopy. Crystallinity was assessed by XRD spectroscopy. Time-resolved spectroscopy was used to obtain characteristic fluorescence kinetics of AlPc NPs upon interaction with cell cultures. The photodynamic efficiency and fluorescence quantum yield of AlPc NPs in HeLa and THP-1 cells were evaluated. After entering the cells, AlPc NPs localized in lysosomes and fluorescence corresponding to individual AlPc molecules were observed, as well as destruction of lysosomes and a rapid decrease in fluorescence intensity during photodynamic action. The photodynamic efficiency of AlPc NPs in THP-1 cells was almost 1.8-fold that of the molecular form of AlPc (Photosens). A new mechanism for the occurrence of fluorescence and phototoxicity of AlPc NPs in interaction with cells is proposed.
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spelling pubmed-96119392022-10-28 Theranostic Properties of Crystalline Aluminum Phthalocyanine Nanoparticles as a Photosensitizer Makarov, Vladimir I. Pominova, Daria V. Ryabova, Anastasiya V. Romanishkin, Igor D. Voitova, Arina V. Steiner, Rudolf W. Loschenov, Victor B. Pharmaceutics Article The study of phthalocyanines, known photosensitizers, for biomedical applications has been of high research interest for several decades. Of specific interest, nanophotosensitizers are crystalline aluminum phthalocyanine nanoparticles (AlPc NPs). In crystalline form, they are water-insoluble and atoxic, but upon contact with tumors, immune cells, or pathogenic microflora, they change their spectroscopic properties (acquire the ability to fluoresce and become phototoxic), which makes them upcoming agents for selective phototheranostics. Aqueous colloids of crystalline AlPc NPs with a hydrodynamic size of 104 ± 54 nm were obtained using ultrasonic dispersal and centrifugation. Intracellular accumulation and localization of AlPc were studied on HeLa and THP-1 cell cultures and macrophages (M0, M1, M2) by fluorescence microscopy. Crystallinity was assessed by XRD spectroscopy. Time-resolved spectroscopy was used to obtain characteristic fluorescence kinetics of AlPc NPs upon interaction with cell cultures. The photodynamic efficiency and fluorescence quantum yield of AlPc NPs in HeLa and THP-1 cells were evaluated. After entering the cells, AlPc NPs localized in lysosomes and fluorescence corresponding to individual AlPc molecules were observed, as well as destruction of lysosomes and a rapid decrease in fluorescence intensity during photodynamic action. The photodynamic efficiency of AlPc NPs in THP-1 cells was almost 1.8-fold that of the molecular form of AlPc (Photosens). A new mechanism for the occurrence of fluorescence and phototoxicity of AlPc NPs in interaction with cells is proposed. MDPI 2022-10-06 /pmc/articles/PMC9611939/ /pubmed/36297557 http://dx.doi.org/10.3390/pharmaceutics14102122 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Makarov, Vladimir I.
Pominova, Daria V.
Ryabova, Anastasiya V.
Romanishkin, Igor D.
Voitova, Arina V.
Steiner, Rudolf W.
Loschenov, Victor B.
Theranostic Properties of Crystalline Aluminum Phthalocyanine Nanoparticles as a Photosensitizer
title Theranostic Properties of Crystalline Aluminum Phthalocyanine Nanoparticles as a Photosensitizer
title_full Theranostic Properties of Crystalline Aluminum Phthalocyanine Nanoparticles as a Photosensitizer
title_fullStr Theranostic Properties of Crystalline Aluminum Phthalocyanine Nanoparticles as a Photosensitizer
title_full_unstemmed Theranostic Properties of Crystalline Aluminum Phthalocyanine Nanoparticles as a Photosensitizer
title_short Theranostic Properties of Crystalline Aluminum Phthalocyanine Nanoparticles as a Photosensitizer
title_sort theranostic properties of crystalline aluminum phthalocyanine nanoparticles as a photosensitizer
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9611939/
https://www.ncbi.nlm.nih.gov/pubmed/36297557
http://dx.doi.org/10.3390/pharmaceutics14102122
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