Author: Shen G.X.¹

Source: Current Drug Targets - Cardiovascular & Hematological Disorders, Volume 3, Number 4, December 2003 , pp. 301-307(7)

Publisher: Bentham Science Publishers

Abstract:

Protein kinase C (PKC) represents a family of phospholipid-dependent serine / threonine kinase. PKC was detected in almost all types of cells and tissues in the body. The activation of PKC is involved in the signal regulation of many physiological and pathological processes. PKC has multiple isoforms (;, I, II, , , , , , , and ). PKC-mediated cellular processes are tissue- and isoform-specific. Investigations on selective or isoform-specific PKC inhibitors have attracted great attention during last two decades. Recent studies demonstrated that LY333531, a PKC--specific inhibitor, reduced the development of diabetic vascular complications in animal models and prevented hyperglycemia-induced impairment of endothelialdependent vasodilation in healthy subjects. Results from phase I clinical trial suggested low risk of the inhibitor. Phase III clinical trials on the safety and the preventive effects of the PKC--specific inhibitor on diabetic complications are under progress. The efficacy of ISSI-3521, a PKC- antisense inhibitor, on slowing the growth and metastasis of solid tumors is currently being examined in clinical trials. Partial responses in the prevention of the progress of malignancies were found in early phases of clinical trials for UCN-01 and CGP41251, two partially isoform-specific PKC inhibitors. Recent findings suggest that isoform-specific PKC inhibitors are potentially beneficial to the prevention or treatment of some common diseases, including cancers and diabetic vascular complications. Safety and efficacy studies of the PKC inhibitors will be required through large-scale long-term clinical trials.

Keywords: protein kinase c; inhibitors for pkc isoforms; gene therapy; cancer therapy; diabetic vascular complications

Document Type: Review article

DOI: 10.2174/1568006033481375

Affiliations: 1: Diabetes Research Group, University of Manitoba, 835-715 McDermot Ave, Winnipeg, Manitoba R3E 3P4, Canada.

Share this item with others: These icons link to social bookmarking sites where readers can share and discover new web pages.

• Website © 2009 Ingenta. Article copyright remains with the publisher, society or author(s) as specified within the article.
• Terms and Conditions
• Privacy Policy
• Information for advertisers

Click here for Page Help

Browse

Search

Electronic content Journal or book title

 

• Search History
  • Ti: IMAGINATIV... (tka)
    (84 hits)
  • Ti: hepatic cy... (tka)
    (187 hits)
  • Current search history
  • Saved searches
  • Search alerts

Shopping cart

Tools

• Print
• Article access options
• Subscribe
  • Activate Personal Subscription
• Export
  • EndNote
  • BibT_EX
• Linking
  • IngentaConnect
  • OpenURL
  • DOI
• Alerting Options
  • Receive New Issue Alert
  • Latest TOC RSS Feed
  • Recent Issues RSS Feed
• Bookmark
  • Marked List
  • Add to Marked List
  • Social Bookmarking Links

Sign in

Text size: A | A | A | A