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DOI: 10.1126/science.272.5262.728
OpenAccess: Closed
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Amelioration of Vascular Dysfunctions in Diabetic Rats by an Oral PKC β Inhibitor

Hiromichi Ishii,Michael R. Jirousek,Daisuke Koya,Chikako Takagi,Pu Xia,Allen C. Clermont,Sven–Erik Bursell,Timothy S. Kern,Lawrence M. Ballas,William F. Heath,Lawrence E. Stramm,Edward P. Feener,George L. King

Protein kinase C
Diabetes mellitus
Internal medicine
1996
The vascular complications of diabetes mellitus have been correlated with enhanced activation of protein kinase C (PKC). LY333531, a specific inhibitor of the beta isoform of PKC, was synthesized and was shown to be a competitive reversible inhibitor of PKC beta 1 and beta 2, with a half-maximal inhibitory constant of approximately 5 nM; this value was one-fiftieth of that for other PKC isoenzymes and one-thousandth of that for non-PKC kinases. When administered orally, LY333531 ameliorated the glomerular filtration rate, albumin excretion rate, and retinal circulation in diabetic rats in a dose-responsive manner, in parallel with its inhibition of PKC activities.
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    Amelioration of Vascular Dysfunctions in Diabetic Rats by an Oral PKC β Inhibitor” is a paper by Hiromichi Ishii Michael R. Jirousek Daisuke Koya Chikako Takagi Pu Xia Allen C. Clermont Sven–Erik Bursell Timothy S. Kern Lawrence M. Ballas William F. Heath Lawrence E. Stramm Edward P. Feener George L. King published in 1996. It has an Open Access status of “closed”. You can read and download a PDF Full Text of this paper here.