A Highly Selective, Non-Hydantoin, Non-Carboxylic Acid Inhibitor of Aldose Reductase with Potent Oral Activity in Diabetic Rat Models: 6-(5-Chloro-3-methylbenzofuran- 2-sulfonyl)-2-H-pyridazin-3-one

Banavara L. Mylari,Sandra J. Armento,David A. Beebe,Edward L. Conn,James B. Coutcher,Michael S. Dina,Melissa T. Ogorman,Michael C. Linhares,William H. Martin,Peter J. Oates,David A. Tess,Gregory J. Withbroe,William James Zembrowski

A Highly Selective, Non-Hydantoin, Non-Carboxylic Acid Inhibitor of Aldose Reductase with Potent Oral Activity in Diabetic Rat Models: 6-(5-Chloro-3-methylbenzofuran- 2-sulfonyl)-2-H-pyridazin-3-one

2003

Banavara L. Mylari
Sandra J. Armento
David A. Beebe
Edward L. Conn
James B. Coutcher
Michael S. Dina
Melissa T. Ogorman
Michael C. Linhares
William H. Martin
Peter J. Oates
David A. Tess
Gregory J. Withbroe
William James Zembrowski

We report here on the discovery path that led to a structurally unprecedented non-hydantoin, non-carboxylic acid aldose reductase inhibitor, 24, which shows remarkably potent oral activity in normalizing elevated sorbitol levels and, more significantly, fructose levels in the sciatic nerve of chronically diabetic rats, with ED90 values of 0.8 and 3 mpk, respectively. It is well absorbed in rats (oral bioavailability, 98%) and has a long plasma t1/2 (26 ± 3 h).

Keywords:

Aldose reductase
Aldehyde Reductase
Sorbitol
Biochemistry
Sulfonyl
Aldose reductase inhibitor
Fructose
Hydantoin
Enzyme inhibitor
Chemistry

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