Low Glucose Enhances Na+/Glucose Transport in Bovine Brain Artery Endothelial Cells • Editorial Comment

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Stroke. 1998;29:844-849

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(Stroke. 1998;29:844-849.)
© 1998 American Heart Association, Inc.

Original Contributions

Low Glucose Enhances Na⁺/Glucose Transport in Bovine Brain Artery Endothelial Cells

Tomoyuki Nishizaki, MD, PhD; Toshiyuki Matsuoka, MD

From the Department of Physiology, Kobe University School of Medicine, Kobe, Japan.

Correspondence to T. Nishizaki, MD, PhD, Department of Physiology, Kobe University School of Medicine, 7–5-1 Kusunoki-cho, Chuo-ku, Kobe 650, Japan.

Background and Purpose—Brain arteries are structurallycharacterized by the tight junctions of the endothelium andby no vasa vasorum that feed arteries themselves. This raisesthe question of how brain arteries are provided with glucose.A possible explanation is that glucose uptake into arteriesmay be mediated by both GLUT1, a facilitative glucose transporter,and a Na⁺/glucose cotransporter (SGLT)-like glucose transporter.The functional role for the SGLT-like glucose transporter, however,is unknown. In the present study we investigated SGLT-like glucose transporter–operatedglucose uptake into brain arterial endothelial cells by recordingglucose-evoked Na⁺ currents and monitoring uptake of [³H]-2-deoxy-D-glucose ([³H]-2-DOG).

Methods—Endothelial cells were cultured from bovine cerebralcortical arteries. Whole-cell patches were made to cells, andglucose-evoked currents were recorded. Cells were incubatedwith [³H]-2-DOG, and the uptake was determined by a liquid scintillationcounter.

Results—Glucose and ${alpha}$ -methyl-D-glucoside ( ${alpha}$ MeDG), a specificcompound for the SGLTs, evoked Na⁺ currents in a whole-cellvoltage-clamp configuration, and the currents were enhanced incells with over 30 minutes' preincubation in glucose-free media. Glucose-inducedcurrents were inhibited by ${alpha}$ MeDG, by the selective SGLT inhibitorphlorizin, by dinitrophenol (DNP), an inhibitor of energy metabolism,or by deletion of Na⁺ from extracellular solution, which indicatesthat glucose uptake into endothelial cells was mediated by a Na⁺-and energy-dependent glucose transporter. Notably, the currentswere desensitized, reduced in a glucose concentration–dependentmanner, and markedly inhibited by either a second applicationof glucose or the addition of glucose to the patch electrodefilling solution; they were potentiated, however, by treatmentwith cytochalasin B, a GLUT1 to GLUT5 inhibitor. Consistentwith the results of patch-clamp recordings, uptake of [³H]-2-DOGinto endothelial cells was enhanced by glucose-free insult,and the enhancement was mediated by an SGLT-like glucose transporter.

Conclusions— The results presented demonstrate that an SGLT-likeglucose transporter takes part in glucose uptake into brain arteryendothelial cells and that the uptake is regulated by intracellularglucose concentrations; glucose-free insult and the ensuinglow cytosolic glucose enhance activity of the SGLT-like glucosetransporter. The SGLT-like glucose transporter in the brain arterialendothelium thus may be important in the maintenance of an adequateglucose concentration in the arterial wall under conditionsof stress, such as hypoglycemia.

Editorial Comment

Nabil J. Alkayed, MD, PhD; Patricia D. Hurn, PhD

Guest Editors, Anesthesiology/Critical Care Medicine, Johns Hopkins Medical Institutions, Baltimore, Maryland

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