塞来昔布对环氧化酶-2的选择性抑制作用会升高血压并促进白细胞黏附。
Selective cyclo-oxygenase-2 inhibition with celecoxib elevates blood pressure and promotes leukocyte adherence.
作者信息
Muscará M N, Vergnolle N, Lovren F, Triggle C R, Elliott S N, Asfaha S, Wallace J L
机构信息
Department of Pharmacology & Therapeutics, University of Calgary, 3330 Hospital Drive NW, Calgary, Alberta, T2N 4N1, Canada.
出版信息
Br J Pharmacol. 2000 Apr;129(7):1423-30. doi: 10.1038/sj.bjp.0703232.
Abstract
- Selective inhibitors of cyclo-oxygenase-2 have been shown to be effective anti-inflammatory drugs with reduced gastrointestinal toxicity relative to conventional nonsteroidal anti-inflammatory drugs (NSAIDs). In the present study, we examined the possibility that selective COX-2 inhibition, by blocking prostacyclin synthesis, would increase blood pressure and cause leukocyte adherence and platelet aggregation. 2. Normal rats and rats with hypertension induced by chronic administration of Nomega-nitro-L-arginine methylester were given celecoxib (10 mg kg(-1)) daily for 3 weeks. Celecoxib significantly elevated of blood pressure in both the normal and hypertensive rats (mean increase of >33 mm Hg after 3 weeks). 3. In normal rats, celecoxib had no effect on serum 6-keto prostaglandin (PG)F(1alpha) levels. Hypertensive rats exhibited a significant increase (82%) in serum 6-keto PGF(1alpha) levels, and this was reduced to the levels of normal rats by treatment with celecoxib. 4. Rats treated with celecoxib exhibited significant increases in weight gain (20%), plasma arginine-vasopressin levels (148%) and plasma urea (69%) relative to vehicle-treated controls. Plasma creatinine levels were unaffected by treatment with celecoxib, while plasma renin levels were significantly decreased (30%) relative to controls. 5. Superfusion of mesenteric venules with celecoxib (3 microM) in vivo resulted in significant increases in leukocyte adherence to the endothelium in both normal and hypertensive rats. 6. These studies suggest that suppression of COX-2 significantly influences vascular and/or renal function, leading to elevated blood pressure and leukocyte adherence.
摘要
- 与传统非甾体抗炎药(NSAIDs)相比,环氧化酶-2选择性抑制剂已被证明是有效的抗炎药物,且胃肠道毒性较低。在本研究中,我们探讨了选择性抑制COX-2通过阻断前列环素合成增加血压、导致白细胞黏附和血小板聚集的可能性。2. 正常大鼠和经慢性给予Nω-硝基-L-精氨酸甲酯诱导高血压的大鼠,每天给予塞来昔布(10 mg·kg⁻¹),持续3周。塞来昔布使正常大鼠和高血压大鼠的血压均显著升高(3周后平均升高>33 mmHg)。3. 在正常大鼠中,塞来昔布对血清6-酮-前列腺素(PG)F₁α水平无影响。高血压大鼠血清6-酮-PGF₁α水平显著升高(82%),而用塞来昔布治疗后降至正常大鼠水平。4. 与给予赋形剂的对照组相比,用塞来昔布治疗的大鼠体重增加(20%)、血浆精氨酸加压素水平(148%)和血浆尿素(69%)显著升高。塞来昔布治疗对血浆肌酐水平无影响,而血浆肾素水平相对于对照组显著降低(30%)。5. 体内用塞来昔布(3 μM)对肠系膜小静脉进行灌流,导致正常大鼠和高血压大鼠的白细胞与内皮的黏附均显著增加。6. 这些研究表明,COX-2的抑制显著影响血管和/或肾功能,导致血压升高和白细胞黏附。
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