Comparison of vasodilatory properties of 14,15-EET analogs: structural requirements for dilation.

نویسندگان

  • J R Falck
  • U Murali Krishna
  • Y Krishna Reddy
  • P Srinagesh Kumar
  • K Malla Reddy
  • Sarah B Hittner
  • Christine Deeter
  • Kamalesh K Sharma
  • Kathryn M Gauthier
  • William B Campbell
چکیده

Epoxyeicosatrienoic acids (EETs) are endothelium-derived eicosanoids that activate potassium channels, hyperpolarize the membrane, and cause relaxation. We tested 19 analogs of 14,15-EET on vascular tone to determine the structural features required for activity. 14,15-EET relaxed bovine coronary arterial rings in a concentration-related manner (ED(50) = 10(-6) M). Changing the carboxyl to an alcohol eliminated dilator activity, whereas 14,15-EET-methyl ester and 14,15-EET-methylsulfonimide retained full activity. Shortening the distance between the carboxyl and epoxy groups reduced the agonist potency and activity. Removal of all three double bonds decreased potency. An analog with a Delta8 double bond had full activity and potency. However, the analogs with only a Delta5 or Delta11 double bond had reduced potency. Conversion of the epoxy oxygen to a sulfur or nitrogen resulted in loss of activity. 14(S),15(R)-EET was more potent than 14(R),15(S)-EET, and 14,15-(cis)-EET was more potent than 14,15-(trans)-EET. These studies indicate that the structural features of 14,15-EET required for relaxation of the bovine coronary artery include a carbon-1 acidic group, a Delta8 double bond, and a 14(S),15(R)-(cis)-epoxy group.

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عنوان ژورنال:
  • American journal of physiology. Heart and circulatory physiology

دوره 284 1  شماره 

صفحات  -

تاریخ انتشار 2003