Lipid Monolayer on Cell Surface Protein Templates Functional Extracellular Lipid Assembly

Author:

Dwivedi Anupma1ORCID,Mazumder Anisha1ORCID,Pullmannová Petra1ORCID,Paraskevopoulou Anna12ORCID,Opálka Lukáš1ORCID,Kováčik Andrej12ORCID,Macháček Miloslav3ORCID,Jančálková Pavla1ORCID,Svačinová Petra2ORCID,Peterlik Herwig4ORCID,Maixner Jaroslav5ORCID,Vávrová Kateřina1ORCID

Affiliation:

1. Skin Barrier Research Group, Faculty of Pharmacy Charles University Heyrovského 1203 Hradec Králové 50005 Czech Republic

2. Department of Pharmaceutical Technology, Faculty of Pharmacy Charles University Heyrovského 1203 Hradec Králové 50005 Czech Republic

3. Department of Biochemical Sciences, Faculty of Pharmacy Charles University Heyrovského 1203 Hradec Králové 50005 Czech Republic

4. Faculty of Physics University of Vienna Boltzmanngasse 5 Vienna 1090 Austria

5. Faculty of Chemical Technology University of Chemistry and Technology Prague Technická 5 Prague 16628 Czech Republic

Abstract

AbstractWhen the ancestors of men moved from aquatic habitats to the drylands, their evolutionary strategy to restrict water loss is to seal the skin surface with lipids. It is unknown how these rigid ceramide‐dominated lipids with densely packed chains squeeze through narrow extracellular spaces and how they assemble into their complex multilamellar architecture. Here it is shown that the human corneocyte lipid envelope, a monolayer of ultralong covalently bound lipids on the cell surface protein, templates the functional barrier assembly by partly fluidizing and rearranging the free extracellular lipids in its vicinity during the sculpting of a functional skin lipid barrier. The lipid envelope also maintains the fluidity of the extracellular lipids during mechanical stress. This local lipid fluidization does not compromise the permeability barrier. The results provide new testable hypotheses about epidermal homeostasis and the pathophysiology underlying diseases with impaired lipid binding to corneocytes, such as congenital ichthyosis. In a broader sense, this lipoprotein‐mediated fluidization of rigid (sphingo)lipid patches may also be relevant to lipid rafts and cellular signaling events and inspire new functional materials.

Funder

Grantová Agentura České Republiky

Univerzita Karlova v Praze

Publisher

Wiley

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