A BODIPY‐Based Molecular Rotor in Giant Unilamellar Vesicles: A Case Study by Polarization‐Resolved Time‐Resolved Emission and Transient Absorption Spectroscopy

Author:

Jha Keshav Kumar12ORCID,Prabhakaran Amrutha3ORCID,Spantzel Lukas4,Sia Rengel Cane5,Pérez Iván4,Arellano‐Reyes Ruben Arturo3,Elmanova Anna12,Dasgupta Anindita67,Eggeling Christian678,Börsch Michael4ORCID,Guthmuller Julien5,Presselt Martin12,Keyes Tia E.3,Dietzek‐Ivanšić Benjamin12

Affiliation:

1. Leibniz Institute of Photonic Technology Jena Research Department Functional Interfaces Albert-Einstein-Straße 9 07745 Jena Germany

2. Institute of Physical Chemistry and Abbe Center of Photonics Friedrich Schiller University Jena Helmholtzweg 4 07743 Jena Germany

3. School of Chemical Sciences National Centre for Sensor Research Dublin City University Dublin 9 Ireland

4. Single-Molecule Microscopy Group and Center of Medical Optics and Photonics Jena University Hospital Nonnenplan 2–4 07743 Jena Germany

5. Institute of Physics and Applied Computer Science Faculty of Applied Physics and Mathematics Gdańsk University of Technology Narutowicza 11/12 80233 Gdańsk Poland

6. Leibniz Institute of Photonic Technology Jena Member of the Leibniz Centre for Photonics in Infection Research (LPI), Jena, Germany) Research Department Biophysical Imaging Albert-Einstein-Straße 9 07745 Jena Germany

7. Institute of Applied Optics and Biophysics Friedrich Schiller University Jena Helmholtzweg 4 07743 Jena Germany

8. Jena Center for Soft Matter Philosophenweg 7 07743 Jena Germany

Abstract

AbstractBODIPY and BODIPY‐derived systems are widely applied as fluorophores and as probes for viscosity detection in solvents and biological media. Their orientational and rotational dynamics in biological media are thus of vital mechanistic importance and extensively investigated. In this contribution, polarization‐resolved confocal microscopy is used to determine the orientation of an amphiphilic BODIPY‐cholesterol derivative in homogeneous giant unilamellar vesicles (GUV) made from 1,2‐dioleoyl‐sn‐glycero‐3‐phosphocholine (DOPC). The BODIPY‐moiety of the molecule is placed near the polar headgroups, and the cholesterol moiety is embedded in the membrane along the acyl chain of the lipids. The rotational relaxation of fluorophore is conventionally investigated by time‐resolved emission anisotropy (TEA); and this method is also used here. However, TEA depends on the emission of the fluorophore and may not be useful to probe rotational dynamics of the non‐emissive triplet states. Thus, we employ femtosecond transient absorption anisotropy (TAA), that relies on the absorption of the molecule to complement the studies of the amphiphilic BODIPY in DCM and GUV. The photoinduced anisotropy of the BODIPY molecule in DCM decays tri‐exponentially, the decay components (sub‐5 ps, 43 ps and 440 ps) of anisotropy are associated with the non‐spherical shape of the BODIPY molecule. However, the anisotropy decay in homogenous GUVs follows a biexponential decay; which arises from the wobbling‐in‐a‐cone motion of the non‐spherical molecule in the high viscous lipid bilayer media. The observations for the BODIPY‐chol molecule in the GUV environment by TAA will extend to the investigation of non‐emissive molecules in cellular environment since GUV structure and size resembles the membrane of a biological cell.

Funder

European Commission

Deutsche Forschungsgemeinschaft

Science Foundation Ireland

Universitätsklinikum Jena

Publisher

Wiley

Subject

Organic Chemistry,Physical and Theoretical Chemistry,Analytical Chemistry

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