학술논문
Lacteal junction zippering protects against diet-induced obesity
Document Type
Academic Journal
Author
Zhang, Feng; Zarkada, Georgia; Han, Jinan; Li, Jinyu; Dubrac, Alexandre; Ola, Roxana; Genet, Gael; Boye, Kevin; Michon, Pauline; Kiinzel, Steffen E.; Camporez, Joao Paulo; Singh, Abhishek K.; Fong, Guo-Hua; Simons, Michael; Tso, Patrick; Fernandez-Hernando, Carlos; Shulman, Gerald I.; Sessa, William C.; Eichmann, Anne
Source
Science. August 10, 2018, Vol. 361 Issue 6402, p599, 5 p.
Subject
Language
English
ISSN
0036-8075
Abstract
Excess dietary lipid uptake causes obesity, a major global health problem. Enterocyte-absorbed lipids are packaged into chylomicrons, which enter the bloodstream through intestinal lymphatic vessels called lacteals. Here, we show that preventing lacteal chylomicron uptake by inducible endothelial genetic deletion of Neuropilinl (Nrp1) and Vascular endothelial growth factor receptor 1 (Vegfr1; also known as Flt1) renders mice resistant to diet-induced obesity. Absence of NRP1 and FLT1 receptors increased VEGF-A bioavailability and signaling through VEGFR2, inducing lacteal junction zippering and chylomicron malabsorption. Restoring permeable lacteal junctions by VEGFR2 and vascular endothelial (VE)--cadherin signaling inhibition rescued chylomicron transport in the mutant mice. Zippering of lacteal junctions by disassembly of cytoskeletal VE-cadherin anchors prevented chylomicron uptake in wild-type mice. These data suggest that lacteal junctions may be targets for preventing dietary fat uptake.