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首页> 外文期刊>Histology and histopathology >The effect of oestradiol and neta on immunohistochemical staining of iNOS and eNOS in coronary arteries of ovariectomized rats.
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The effect of oestradiol and neta on immunohistochemical staining of iNOS and eNOS in coronary arteries of ovariectomized rats.

机译:雌二醇和neta对去卵巢大鼠冠状动脉iNOS和eNOS免疫组织化学染色的影响。

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AIM: The postmenopausal period is associated with increased risk for coronary atherosclerosis, and the effect of hormone replacement therapy in reducing this risk is controversial. Previous studies reported that nitric oxide synthetase (NOS) level might be important for the development of atherosclerosis, but no study has shown the interaction between hormone replacement therapy and endothelial NOS and inducible NOS intensity on coronary arteries yet. Our goal was to find out the immunostaining intensity of endothelial NOS and inducible NOS in ovariectomized rats which received oestradiol and norethisterone treatment. METHODS: We performed bilateral ovariectomy in 15, female, 90-day-old Wistar rats with an average weight of 250 grams. After waiting for 4 weeks for the menopausal state, they were divided into 3 groups to receive either placebo, 0.1 mg/day 17-beta-oestradiol (group E2), or 0.1 mg/day 17-beta-oestradiol + 0.1 mg/day norethisterone acetate (group E2-NETA) for 5 weeks. Another group included 5, normal, adult, female intact rats and served as controls. At the end of the treatment, all rats were sacrificed and coronary arteries were stained with inducible NOS and endothelial NOS polyclonal antibodies using streptavidin-biotin technique. RESULTS: The immunostaining of inducible NOS was prominent in perivascular connective tissue of the ovariectomized group but not in the control group. The inducible NOS immunostaining immunoreactivity was not detected in either treated groups. Immunostaining intensity of endothelial NOS did not differ in any 4 groups with similar staining. CONCLUSION: The present findings indicate that hormone replacement therapy down-regulates iNOS expression in coronary arteries of ovariectomized rats, and reduced iNOS may likely be involved in estrogen's beneficial effects.
机译:目的:绝经后时期与冠状动脉粥样硬化的风险增加有关,激素替代疗法在降低这种风险中的作用尚存争议。先前的研究报道,一氧化氮合成酶(NOS)的水平可能对动脉粥样硬化的发展很重要,但尚无研究表明激素替代疗法与内皮NOS和可诱导的NOS强度在冠状动脉上的相互作用。我们的目标是找出接受雌二醇和炔诺酮治疗的去卵巢大鼠的内皮NOS和诱导型NOS的免疫染色强度。方法:我们对15只雌性90日龄Wistar大鼠进行了双侧卵巢切除术,平均体重为250克。等待更年期4周后,将他们分为3组,分别接受安慰剂,0.1 mg /天的17-β-雌二醇(E2组)或0.1 mg /天的17-β-雌二醇+ 0.1 mg /天醋酸炔诺酮(E2-NETA组)治疗5周。另一组包括5只正常,成年,雌性完整大鼠,并作为对照。在治疗结束时,处死所有大鼠,并使用链霉亲和素-生物素技术用诱导型NOS和内皮型NOS多克隆抗体对冠状动脉进行染色。结果:卵巢切除组的血管周结缔组织中可诱导的NOS的免疫染色明显,而对照组则没有。在两个治疗组中均未检测到可诱导的NOS免疫染色免疫反应性。内皮NOS的免疫染色强度在染色相似的任何4组中没有差异。结论:本研究结果表明,激素替代疗法下调了去卵巢大鼠冠状动脉中iNOS的表达,而iNOS的减少可能与雌激素的有益作用有关。

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