Issue 25, 2022
From the journal:

Nanoscale

Fluorescence lifetime microscopy unveils the supramolecular organization of liposomal Doxorubicin

Paolo Tentori,ab   Giovanni Signore,c   Andrea Camposeo, ORCID logo d   Annalisa Carretta,a   Gianmarco Ferri,a   Pasqualantonio Pingue,ad   Stefano Luin,a   Daniela Pozzi, ORCID logo e   Enrico Gratton,f   Fabio Beltram,ab   Giulio Caracciolo ORCID logo e  and  Francesco Cardarelli ORCID logo *ad  

* Corresponding authors

a Laboratorio NEST, Scuola Normale Superiore, Pisa, Italy. E-mail:
E-mail: francesco.cardarelli@sns.it

b Center for Nanotechnology Innovation @NEST, Pisa, Italy

c Fondazione Pisana per la Scienza (FPS), Pisa, Italy

d NEST, Istituto Nanoscienze-CNR, Piazza S. Silvestro, 12, I-56127, Pisa, Italy

e Department of Molecular Medicine, Sapienza University of Rome, Rome, Italy

f Laboratory for Fluorescence Dynamics, Department of Biomedical Engineering, University of California at Irvine, Irvine, California, USA

Abstract

The supramolecular organization of Doxorubicin (DOX) within the standard Doxoves® liposomal formulation (DOX®) is investigated using visible light and phasor approach to fluorescence lifetime imaging (phasor-FLIM). First, the phasor-FLIM signature of DOX® is resolved into the contribution of three co-existing fluorescent species, each with its characteristic mono-exponential lifetime, namely: crystallized DOX (DOXc, 0.2 ns), free DOX (DOXf, 1.0 ns), and DOX bound to the liposomal membrane (DOXb, 4.5 ns). Then, the exact molar fractions of the three species are determined by combining phasor-FLIM with quantitative absorption/fluorescence spectroscopy on DOXc, DOXf, and DOXb pure standards. The final picture on DOX® comprises most of the drug in the crystallized form (∼98%), with the remaining fractions divided between free (∼1.4%) and membrane-bound drug (∼0.7%). Finally, phasor-FLIM in the presence of a DOX dynamic quencher allows us to suggest that DOXf is both encapsulated and non-encapsulated, and that DOXb is present on both liposome-membrane leaflets. We argue that the present experimental protocol can be applied to the investigation of the supramolecular organization of encapsulated luminescent drugs/molecules all the way from the production phase to their state within living matter.

Graphical abstract: Fluorescence lifetime microscopy unveils the supramolecular organization of liposomal Doxorubicin

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Article information

DOI
https://doi.org/10.1039/D2NR00311B
Article type
Communication
Submitted
17 Jan 2022
Accepted
10 May 2022
First published
17 Jun 2022
This article is Open Access
Creative Commons BY-NC license

Nanoscale, 2022,14, 8901-8905

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Fluorescence lifetime microscopy unveils the supramolecular organization of liposomal Doxorubicin

P. Tentori, G. Signore, A. Camposeo, A. Carretta, G. Ferri, P. Pingue, S. Luin, D. Pozzi, E. Gratton, F. Beltram, G. Caracciolo and F. Cardarelli, Nanoscale, 2022, 14, 8901 DOI: 10.1039/D2NR00311B

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