Time-dependent hyperreactivity to phenylephrine in aorta from untreated diabetic rats: role of prostanoids and calcium mobilization

Diabetes alters vascular smooth muscle contractility. Changes in reactivity to phenylephrine (Phe) in aortas from controls and untreated 1- and 4-week streptozotocin (STZ)-induced diabetic rats were investigated. In 1-week diabetic (DB1) aortas, the maximum response (E-max) and sensitivity (pD(2)) to Phe were similar to controls (CT1), but in 4-week diabetic (D134) aortas, the E-max for Phe was increased compared to CT4 aortas (E-max, DB4: 125+/-8.4% vs. CT4: 89.8+/-4.5%, P<.001). Endothelial denudation increased the response to Phe, and E-max was increased in the DB4 aortas compared to CT4 (E-max, DB4: 156+/-4.2% vs. CT4: 125+/-3.8%, P<.001). Pretreatment of CT4 and DB4 aortas with indomethacin reduced Emax and pD2 for Phe. After indomethacin treatment, no differences in E x and pD2 to Phe were observed in either group. SQ 29548 did not alter the Phe actions in CT4 aortas. However, in DB4 aortas, E-max was reduced to control level. CT4 and DB4 aortas incubated in free-Ca2+ solution plus Phe, contracted upon addition of CaCl2, this response was increased in DB4 aortas. No changes were observed for acetylcholine (ACh) or sodium nitroprusside (SNP) responses. Nitric oxide (NO) release in response to Phe determined by acute L-NAME administration showed no differences in the percentage increase of the contraction in CT1 and DB1 aortas, but was enhanced in DB4 aortas. Results suggested that diabetes induces time-dependent changes in the vascular reactivity to Phe. This response is not related to a reduction of endothelium-derived NO but might be due to an increase in prostaglandin H-2 (PGH(2))/thromboxane A(2) (TxA(2)) and/or an enhanced extracellular Ca2+ influx. (C) 2002 Elsevier Science Inc. All rights reserved.