Author:
Mao Hong,Szafranska Karolina,Kruse Larissa,Holte Christopher,Wolfson Deanna L.,Ahluwalia Balpreet Singh,Whitchurch Cynthia B.,Cole Louise,Lockwood Glen P.,Diekmann Robin,Le Couteur David,Cogger Victoria C.,McCourt Peter A. G.
Abstract
AbstractXanthines such as caffeine and theobromine are among the most consumed psychoactive stimulants in the world, either as natural components of coffee, tea and chocolate, or as added ingredients. The present study assessed if xanthines affect liver sinusoidal endothelial cells (LSEC). Cultured primary rat LSEC were challenged with xanthines at concentrations typically obtained from normal consumption of xanthine-containing beverages, food or medicines; and at higher concentrations below the in vitro toxic limit. The fenestrated morphology of LSEC were examined with scanning electron and structured illumination microscopy. All xanthine challenges had no toxic effects on LSEC ultrastructure as judged by LSEC fenestration morphology, or function as determined by endocytosis studies. All xanthines in high concentrations (150 μg/mL) increased fenestration frequency but at physiologically relevant concentrations, only theobromine (8 μg/mL) showed an effect. LSEC porosity was influenced only by high caffeine doses which also shifted the fenestration distribution towards smaller pores. Moreover, a dose-dependent increase in fenestration number was observed after caffeine treatment. If these compounds induce similar changes in vivo, age-related reduction of LSEC porosity can be reversed by oral treatment with theobromine or with other xanthines using targeted delivery.
Funder
Tromsø Research Foundation/Trond Mohn, the University of Tromsø - The Arctic University of Norway
The Research Council of Norway FRIMED
FRIMED2/FORSKER21
Nano2021
Marie Sklodowska-Curie
DeLIVER, EU EIC-2021-Pathfinder “DeLIVERY”
The Engelhorn Foundation
UiT The Arctic University of Norway
Publisher
Springer Science and Business Media LLC
Cited by
3 articles.
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