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Interleaflet organization of membrane nanodomains: What can(not) be resolved by FRET?
- 1.0572784 - ÚFCH JH 2024 RIV US eng J - Článek v odborném periodiku
Chmelová, Barbora - Davidović, David - Šachl, Radek
Interleaflet organization of membrane nanodomains: What can(not) be resolved by FRET?
Biophysical Journal. Roč. 122, č. 11 (2023), s. 2053-2067. ISSN 0006-3495. E-ISSN 1542-0086
Grant CEP: GA ČR(CZ) GC20-01401J
Výzkumná infrastruktura: e-INFRA CZ - 90140
Institucionální podpora: RVO:61388955
Klíčová slova: resonance * energy transfer * lipid nanodomains
Obor OECD: Physical chemistry
Impakt faktor: 3.4, rok: 2022
Způsob publikování: Omezený přístup
Plasma membranes as well as their simplified model systems show an inherent nanoscale heterogeneity. As a result of strong interleaflet interactions, these nanoheterogeneities (called here lipid nanodomains) can be found in perfect registration (i.e., nanodomains in the inner leaflet are registered with the nanodomains in the outer leaflet). Alternatively, they might be interleaflet independent, antiregistered, or located asymmetrically in one bilayer leaflet only. To distinguish these scenarios from each other appears to be an experimental challenge. In this work, we analyzed the potential of Förster resonance energy transfer to characterize interleaflet organization of nanodomains. We generated in silico time-resolved fluorescence decays for a large set of virtual as well as real donor/acceptor pairs distributed over the bilayer containing registered, independent, antiregistered, or asymmetrically distributed nanodomains. In this way, we were able to identify conditions that gave satisfactory or unsatisfactory resolution. Overall, Förster resonance energy transfer appears as a robust method that, when using donor/acceptor pairs with good characteristics, yields otherwise difficult-to-reach characteristics of membrane lipid nanodomains.
Trvalý link: https://hdl.handle.net/11104/0343351
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