[艾多昔芬对人乳内动脉的血管舒张作用]

Wei Geng-Ze, Yu Jun, Zhu Yun-Long, Lin Shu-Xin, Kang Yun-Fan, Wang Rong, Zhou Jing-Jun, Zhang Qing-Hong

Department of Physiology, Fourth Military Medical University, Xi'an 710032, China.

Sheng Li Xue Bao. 2004 Feb 25;56(1):16-20.

The purpose of this study was to investigate the vasorelaxing effect and mechanism of idoxifene (a new estrogen receptor modulator) on human internal mammary artery (HIMA). HIMA segments were harvested from men during coronary artery bypass grafting surgery. Patients with diabetes mellitus, hypercholesterolemia, hypertension, or smoking habit were excluded. The vasorelaxing effect of idoxifene on artery rings from HIMA with and without endothelium was measured by means of perfusion in vitro. Cumulative dose-response to idoxifene in the range of 0.01-10 micromol/L was observed in the presence and absence of NO synthase inhibitor L-NAME. It was also studied whether the vasodilation effect of idoxifene on HIMA was blocked by methylene blue (MB), an inhibitor of guanylate cyclase (GC). The results obtained from idoxifene were compared with those from 17beta-estradiol (E(2)). It was found that idoxifene caused a concentration-dependent relaxation on HIMA. The dose range was from 0.03 micromol/L (minimal vasodilatory concentration) to 3 mmol/L (maximal vasodilatory concentration). It was also found that the vasorelaxation effect of idoxifene on HIMA was dependent on endothelium. E(2) (0.1-100 micromol/L) also resulted in an endothelium-dependent vasorelaxation, but the vessels were 15-fold less sensitive to E(2) than to idoxifene in their vasorelaxation responses. The EC(50) for E(2) was 4.65+/-0.34 micromol/L, compared with 0.32+/-0.02 micromol/L for idoxifene. The mean maximal vasodilatory value of E(2) was 88.3+/-5.7%, compared with 88.6+/-7.2% for idoxifene. Pretreatment with L-NAME (100micromol/L) abolished idoxifene-induced vasodilation virtually by blocking nitric oxide production. The vasorelaxing effect of idoxifene disappeared in the presence of MB (10 micromol/L). These findings demonstrate that idoxifene results in an endothelium-dependent vasorelaxation of HIMA, like estrogen. The effect of idoxifene is more potent than that of traditional estrogen, and is possibly mediated by NO-GC-cGMP pathway.

本研究旨在探讨艾多昔芬（一种新型雌激素受体调节剂）对人乳内动脉（HIMA）的血管舒张作用及其机制。在冠状动脉搭桥手术中从男性患者获取HIMA节段。排除患有糖尿病、高胆固醇血症、高血压或有吸烟习惯的患者。通过体外灌注法测定艾多昔芬对有内皮和无内皮的HIMA动脉环的血管舒张作用。在存在和不存在一氧化氮合酶抑制剂L-NAME的情况下，观察了0.01 - 10微摩尔/升范围内艾多昔芬的累积剂量反应。还研究了艾多昔芬对HIMA的血管舒张作用是否被鸟苷酸环化酶（GC）抑制剂亚甲蓝（MB）阻断。将艾多昔芬得到的结果与17β-雌二醇（E₂）的结果进行比较。发现艾多昔芬对HIMA产生浓度依赖性舒张作用。剂量范围为0.03微摩尔/升（最小血管舒张浓度）至3毫摩尔/升（最大血管舒张浓度）。还发现艾多昔芬对HIMA的血管舒张作用依赖于内皮。E₂（0.1 - 100微摩尔/升）也导致内皮依赖性血管舒张，但血管对E₂的血管舒张反应的敏感性比对艾多昔芬低15倍。E₂的半数有效浓度（EC₅₀）为4.65±0.34微摩尔/升，而艾多昔芬为0.32±0.02微摩尔/升。E₂的平均最大血管舒张值为88.3±5.7%，而艾多昔芬为88.6±7.2%。用L-NAME（100微摩尔/升）预处理实际上通过阻断一氧化氮生成消除了艾多昔芬诱导的血管舒张。在存在MB（10微摩尔/升）的情况下，艾多昔芬的血管舒张作用消失。这些发现表明，艾多昔芬与雌激素一样，可导致HIMA的内皮依赖性血管舒张。艾多昔芬的作用比传统雌激素更强，并且可能由NO-GC-cGMP途径介导。