Transcellular Barriers to Glucose Delivery in the Body
Research output: Contribution to journal › Review › Research › peer-review
Standard
Transcellular Barriers to Glucose Delivery in the Body. / Klip, Amira; De Bock, Katrien; Bilan, Philip J.; Richter, Erik A.
In: Annual Review of Physiology, Vol. 86, 2024, p. 149-173.Research output: Contribution to journal › Review › Research › peer-review
Harvard
APA
Vancouver
Author
Bibtex
}
RIS
TY - JOUR
T1 - Transcellular Barriers to Glucose Delivery in the Body
AU - Klip, Amira
AU - De Bock, Katrien
AU - Bilan, Philip J.
AU - Richter, Erik A.
N1 - Publisher Copyright: © 2024 Annual Reviews Inc.. All rights reserved.
PY - 2024
Y1 - 2024
N2 - Glucose is the universal fuel of most mammalian cells, and it is largely replenished through dietary intake. Glucose availability to tissues is paramount for the maintenance of homeostatic energetics and, hence, supply should match demand by the consuming organs. In its journey through the body, glucose encounters cellular barriers for transit at the levels of the absorbing intestinal epithelial wall, the renal epithelium mediating glucose reabsorption, and the tight capillary endothelia (especially in the brain). Glucose transiting through these cellular barriers must escape degradation to ensure optimal glucose delivery to the bloodstream or tissues. The liver, which stores glycogen and generates glucose de novo, must similarly be able to release it intact to the circulation. We present the most up-to-date knowledge on glucose handling by the gut, liver, brain endothelium, and kidney, and discuss underlying molecular mechanisms and open questions. Diseases associated with defects in glucose delivery and homeostasis are also briefly addressed. We propose that the universal problem of sparing glucose from catabolism in favor of translocation across the barriers posed by epithelia and endothelia is resolved through common mechanisms involving glucose transfer to the endoplasmic reticulum, from where glucose exits the cells via unconventional cellular mechanisms.
AB - Glucose is the universal fuel of most mammalian cells, and it is largely replenished through dietary intake. Glucose availability to tissues is paramount for the maintenance of homeostatic energetics and, hence, supply should match demand by the consuming organs. In its journey through the body, glucose encounters cellular barriers for transit at the levels of the absorbing intestinal epithelial wall, the renal epithelium mediating glucose reabsorption, and the tight capillary endothelia (especially in the brain). Glucose transiting through these cellular barriers must escape degradation to ensure optimal glucose delivery to the bloodstream or tissues. The liver, which stores glycogen and generates glucose de novo, must similarly be able to release it intact to the circulation. We present the most up-to-date knowledge on glucose handling by the gut, liver, brain endothelium, and kidney, and discuss underlying molecular mechanisms and open questions. Diseases associated with defects in glucose delivery and homeostasis are also briefly addressed. We propose that the universal problem of sparing glucose from catabolism in favor of translocation across the barriers posed by epithelia and endothelia is resolved through common mechanisms involving glucose transfer to the endoplasmic reticulum, from where glucose exits the cells via unconventional cellular mechanisms.
KW - endothelium
KW - epithelium
KW - glucose
KW - glucose-6-phosphatase
KW - GLUT
KW - SLGT
U2 - 10.1146/annurev-physiol-042022-031657
DO - 10.1146/annurev-physiol-042022-031657
M3 - Review
C2 - 38345907
AN - SCOPUS:85185114456
VL - 86
SP - 149
EP - 173
JO - Annual Review of Physiology
JF - Annual Review of Physiology
SN - 0066-4278
ER -
ID: 385895989