Nerve Microvessel Changes in Diabetes are Prevented by Aldose
Reductase Inhibition
Timothy J Benstead and Virgilio E Sangalang

Abstract:
Background: Despite the potential importance
of endoneurial microvessel abnormalities in diabetic neuropathy,
the pathogenesis of these abnormalities is incompletely understood.
We wished to evaluate the effect of experimental diabetes on
endoneurial microvessels and determine if an aldose reductase
inhibitor alters any of the changes induced by diabetes. Methods:
We compared streptozocin diabetic rats with and without aldose
reductase inhibitor treatment to non-diabetic rats after 10
months of diabetes. Transverse microvessels from the mid-sciatic
level were studied by electron microscopic morphometric evaluation.
Results: Microvessel endothelial, pericyte, basement
membrane and total mural area were greater in untreated diabetic
animals than non-diabetic animals. Aldose reductase inhibitor
treated diabetic animals had greater endothelial area and possibly
pericyte area but not basement membrane or total mural area.
Conclusions: This study demonstrates that endoneurial
microvessel abnormalities can be detected in experimental diabetic
neuropathy. Microvessel basement membrane thickening will be
prevented by an aldose reductase inhibitor. One mechanism by
which abnormal polyol pathway activity may contribute to diabetic
neuropathy could be through damage to microvessels.
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Can.
J. Neurol. Sci. 1995; 22: 192-197
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