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Diabetes, Vol 49, Issue 6 1016-1021, Copyright © 2000 by American Diabetes Association
Diabetes downregulates GLUT1 expression in the retina and its microvessels but not in the cerebral cortex or its microvessels
GA Badr, J Tang, F Ismail-Beigi and TS Kern
Department of Medicine, Case Western Reserve University, Cleveland, Ohio, USA.
Capillaries in the retina are more susceptible to develop microvascular
lesions in diabetes than capillaries in the embryologically similar
cerebral cortex. Because available evidence implicates hyperglycemia in the
pathogenesis of diabetic retinopathy, differences in glucose transport into
the retina and brain might contribute to this observed tissue difference in
susceptibility to diabetes-induced microvascular disease. Thus, we compared
levels of GLUT1 and GLUT3 expression in the retina, cerebrum, and their
respective microvessels by Western blot analysis. In nondiabetic animals,
the content of GLUT1 protein in retina and its microvessels was multifold
greater than that of cerebral cortex gray matter and its microvessels.
Streptozotocin-induced diabetes of a 2-week or 2-month duration reduced
GLUT1 expression in the retina and its microvasculature by approximately
50%, but it resulted in no reduction in GLUT1 expression in cerebrum or its
microvessels. The density of capillaries in retinas of diabetic animals did
not change from normal, and so the observed decrease in GLUT1 expression in
the retina and retinal capillaries of diabetic animals cannot be attributed
to fewer vessels. Despite the diabetes-induced reduction of GLUT1
expression in retina, neural retina of diabetic rats still possessed more
GLUT1 than the cerebrum. Retinal pigment epithelium (RPE) possessed more
GLUT1 than neural retina or its microvessels, and expression of the
transporter in the RPE was not affected by diabetes. GLUT3 levels were
greater in cerebral gray matter than in retina, and they were unaffected by
diabetes in either tissue. The effect of diabetes on GLUT1 expression
differs between retina and cerebral cortex, suggesting that glucose
transport is regulated differently in these embryologically similar
tissues. Because diabetes results in downregulation of GLUT1 expression in
retinal microvessels, but not in RPE, the fraction of the glucose entering
the retina in diabetes is likely to be greater across the RPE than across
the retinal vasculature.

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Copyright © 2000 by the American Diabetes Association.
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