内皮素A受体阻断可减少去氧皮质酮盐性高血压模型中的血管超氧化物生成。
ETA receptor blockade decreases vascular superoxide generation in DOCA-salt hypertension.
作者信息
Callera Glaucia E, Touyz Rhian M, Teixeira Simone A, Muscara Marcelo N, Carvalho Maria Helena C, Fortes Zuleica B, Nigro Dorothy, Schiffrin Ernesto L, Tostes Rita C
机构信息
Department of Pharmacology, Institute of Biomedical Sciences, University of Sao Paulo, Sao Paulo, Brazil.
出版信息
Hypertension. 2003 Oct;42(4):811-7. doi: 10.1161/01.HYP.0000088363.65943.6C. Epub 2003 Aug 11.
Development and progression of end-organ damage in hypertension have been associated with increased oxidative stress. Superoxide anion accumulation has been reported in deoxycorticosterone acetate (DOCA)-salt hypertension, in which endothelin-1 plays an important role in cardiovascular damage. We hypothesized that blockade of ETA receptors in DOCA-salt rats would decrease oxidative stress. Both systolic blood pressure (SBP, 210+/-9 mm Hg; P<0.05) and vascular superoxide generation in vivo were increased in DOCA-salt (44.9+/-10.3% of ethidium bromide-positive nuclei; P<0.05) versus control uninephrectomized (UniNx) rats (118+/-3 mm Hg; 18.5+/-3%, respectively). In DOCA-salt rats, the ETA antagonist BMS 182874 (40 mg/kg per day PO) lowered SBP (170+/-4 versus UniNx, 120+/-3 mm Hg) and normalized superoxide production (21.7+/-6 versus UniNx, 11.9+/-7%). Vitamin E (200 mg/kg per day PO) decreased superoxide formation in DOCA-salt rats (18.8+/-7%) but did not alter SBP. Oxidative stress in nonstimulated circulating polymorphonuclear cells (PMNs) or in PMNs treated with zymosan, an inducer of superoxide release, was similar in DOCA-salt and UniNx groups. Superoxide formation by PMNs was unaffected by treatment with BMS 182874. Western blot analysis showed increased nitrotyrosine-containing proteins in mesenteric vessels from DOCA-salt compared with UniNX. Treatment with either BMS 182874 or vitamin E abolished the differences in vascular nitrotyrosine-containing proteins between DOCA-salt and UniNX. Maximal relaxation to acetylcholine was decreased in DOCA-salt aortas (75.8+/-4.2% versus UniNx, 95.4+/-1.9%, P<0.05). BMS 182874 treatment increased acetylcholine-induced relaxation in DOCA-salt aortas to 93.5+/-4.5%. These in vivo findings indicate that increased vascular superoxide production is associated with activation of the endothelin system through ETA receptors in DOCA-salt hypertension, in apparently blood pressure-independent fashion.
高血压终末器官损害的发生和进展与氧化应激增加有关。在醋酸脱氧皮质酮(DOCA)-盐性高血压中已报道有超氧阴离子蓄积,其中内皮素-1在心血管损害中起重要作用。我们推测,阻断DOCA-盐大鼠的ETA受体可降低氧化应激。与对照单肾切除(UniNx)大鼠(收缩压118±3 mmHg;超氧化物生成占溴化乙锭阳性细胞核的18.5±3%)相比,DOCA-盐大鼠的收缩压(SBP,210±9 mmHg;P<0.05)和体内血管超氧化物生成均增加(超氧化物生成占溴化乙锭阳性细胞核的44.9±10.3%;P<0.05)。在DOCA-盐大鼠中,ETA拮抗剂BMS 182874(每天口服40 mg/kg)可降低收缩压(与UniNx相比为170±4 mmHg,UniNx为120±3 mmHg)并使超氧化物生成恢复正常(与UniNx相比为21.7±6%,UniNx为11.9±7%)。维生素E(每天口服200 mg/kg)可降低DOCA-盐大鼠的超氧化物生成(18.8±7%),但不改变收缩压。在DOCA-盐组和UniNx组中,未刺激的循环多形核白细胞(PMN)或用酵母聚糖(一种超氧化物释放诱导剂)处理的PMN中的氧化应激相似。BMS 182874处理对PMN的超氧化物生成无影响。蛋白质印迹分析显示,与UniNX相比,DOCA-盐组肠系膜血管中含硝基酪氨酸的蛋白质增加。用BMS 182874或维生素E处理可消除DOCA-盐组和UniNX组之间血管中含硝基酪氨酸蛋白质的差异。DOCA-盐主动脉对乙酰胆碱的最大舒张反应降低(与UniNx相比为75.8±4.2%,UniNx为95.4±1.9%,P<0.05)。BMS 182874处理可使DOCA-盐主动脉中乙酰胆碱诱导的舒张反应增加至93.5±4.5%。这些体内研究结果表明,在DOCA-盐性高血压中,血管超氧化物生成增加与通过ETA受体激活内皮素系统有关,且显然与血压无关。
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