Search
Close
Search
Advanced Search
Search Menu
AI Discovery Assistant

Abstract

The epidemic of diabetic kidney disease is predicted to rise significantly in the next decade and will continue to represent the leading cause of end-stage renal failure. The interaction between metabolic and haemodynamic insults represents an important driver of the relentless decline in renal function that we observe in patients with diabetes. Studies have described different cellular pathophysiological mechanisms of diabetic glomerulopathy; increased oxidative stress appears to be the major alteration that drives the activation of many other cellular pathways which in turn will result in the phenotypic alterations seen in diabetic glomerulopathy. The glomerulus should be seen as a delicate network of cells that interact closely with one another in regulating the process of water and small solute filtration. In diabetes, this equilibrium is disrupted and its correction should aim at reinstating the balanced equilibrium as seen in physiology. Future therapeutic challenges will be represented by a tissue-specific personalized ‘ad hoc’ therapeutical approach which will depend on patients' characteristic and stage/progression of disease.

blood pressure, diabetes, kidney disease, metabolism, proteinuria
© The Author 2012. Published by Oxford University Press on behalf of ERA-EDTA. All rights reserved. For Permissions, please e-mail: [email protected]
Topic:
Issue Section:
Cutting-Edge Renal Science > CLINICAL SCIENCE AND OUTCOME RESEARCH IN NEPHROLOGY
You do not currently have access to this article.
Download all slides

Comments

0 Comments
Comments (0)
Submit a comment
You have entered an invalid code
Thank you for submitting a comment on this article. Your comment will be reviewed and published at the journal's discretion. Please check for further notifications by email.