Graham Drew A, Rush James W E
Department of Kinesiology, Faculty of Applied Health Sciences, Univ. of Waterloo, 200 Univ. Ave. West, Waterloo, ON, Canada N2L 3G1.
J Appl Physiol (1985). 2009 Oct;107(4):1059-67. doi: 10.1152/japplphysiol.90785.2008. Epub 2009 Aug 20.
Cyclooxygenase (COX)-derived vasoconstrictory prostanoids contribute to impaired endothelium-dependent vasorelaxation in aging male (m) spontaneously hypertensive rats (SHR); however, vasomotor responses in aging female (f) SHR and sex differences in aging SHR are unknown. Examining mechanisms governing dysfunction in aging fSHR will contribute to understanding sex-dependent vascular complications in advanced hypertension. Aortic endothelium-dependent relaxation dose responses (ACh) of 16- and 30-wk-old mSHR and fSHR and normotensive Wistar-Kyoto rats were examined in the absence (no drug control) and presence of COX inhibition [indomethacin (Indo)] and thromboxane/prostaglandin receptor inhibition (SQ-29548). No drug control-treated 16-wk mSHR exhibited considerable blunting of the peak relaxation response to ACh (e.g., 77 +/- 4% relaxation to 10(-5) mol/l) vs. Wistar-Kyoto controls (89 +/- 6%), and greater dysfunction occurred in 30-wk mSHR (63 +/- 2%). Interestingly, ACh relaxations of fSHR were unimpaired at 16 wk (101 +/- 2% to 10(-5) mol/l), but blunted in 30 wk (76 +/- 4%). Indo and SQ-29548 restored robust ACh vasorelaxation in all groups (e.g., 113 +/- 3 and 112 +/- 3%, respectively, in Indo- and SQ-29548-treated 30-wk fSHR). Aortic COX-1 protein expression was elevated by 75% in 30-wk vs. 16-wk fSHR, whereas group-averaged ACh-stimulated aortic PGI(2) release (assessed as 6- keto-PGF(1alpha)) was 30% greater in 30-wk vs. 16-wk fSHR (9,926 +/- 890 vs. 7,621 +/- 690 pg.ml(-1).mg dry wt(-1)), although this did not reach significance (P = 0.0758). Dramatic deterioration of endothelium-dependent vasomotor function in fSHR across this age range involves COX and thromboxane/prostaglandin receptor, supporting a mechanism of impairment similar to that which occurs in aging mSHR.
环氧化酶(COX)衍生的血管收缩性前列腺素会导致衰老雄性自发性高血压大鼠(SHR)的内皮依赖性血管舒张功能受损;然而,衰老雌性SHR的血管运动反应以及衰老SHR中的性别差异尚不清楚。研究衰老雌性SHR功能障碍的机制将有助于理解晚期高血压中性别依赖性血管并发症。在不存在(无药物对照)以及存在COX抑制[吲哚美辛(Indo)]和血栓素/前列腺素受体抑制(SQ - 29548)的情况下,检测了16周龄和30周龄雄性SHR、雌性SHR以及正常血压的Wistar - Kyoto大鼠的主动脉内皮依赖性舒张剂量反应(乙酰胆碱)。与Wistar - Kyoto对照(89±6%)相比,无药物对照处理的16周龄雄性SHR对乙酰胆碱的峰值舒张反应明显减弱(例如,对10⁻⁵mol/l的乙酰胆碱舒张率为77±4%),30周龄雄性SHR出现了更严重的功能障碍(63±2%)。有趣的是,16周龄雌性SHR的乙酰胆碱舒张功能未受损(对10⁻⁵mol/l的乙酰胆碱舒张率为101±2%),但在30周龄时减弱(76±4%)。吲哚美辛和SQ - 29548使所有组的乙酰胆碱血管舒张功能恢复(例如,吲哚美辛和SQ - 29548处理的30周龄雌性SHR分别为113±3%和112±3%)。与16周龄雌性SHR相比,30周龄雌性SHR的主动脉COX - 1蛋白表达升高了75%,而30周龄雌性SHR中乙酰胆碱刺激的主动脉前列环素(PGI₂)释放(以6 - 酮 - PGF₁α评估)的组平均水平比16周龄雌性SHR高30%(9926±890对7621±690 pg·ml⁻¹·mg干重⁻¹),尽管这未达到显著水平(P = 0.0758)。在这个年龄范围内,雌性SHR内皮依赖性血管运动功能的显著恶化涉及COX和血栓素/前列腺素受体,支持了一种与衰老雄性SHR中发生的类似的损伤机制。
