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血管外膜源性舒张因子的作用机制 被引量:1
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作者 罗碧辉 曾昭华 +6 位作者 张震洪 何文凯 何兆初 梁丽英 Robert MKW Lee Yu-Jin Gao 苏诚坚 《中国病理生理杂志》 CAS CSCD 北大核心 2007年第10期2065-2066,2073,共3页
目的:验证血管外周脂肪组织释放血管外膜源性舒张因子(ADRF),并对ADRF的作用机制做初步探讨。方法:检测WKY大鼠带完整血管外周脂肪组织的血管环和不带血管外周脂肪组织的裸血管环的收缩力;并用液体转移方法鉴证血管外周脂肪组织释放ADRF... 目的:验证血管外周脂肪组织释放血管外膜源性舒张因子(ADRF),并对ADRF的作用机制做初步探讨。方法:检测WKY大鼠带完整血管外周脂肪组织的血管环和不带血管外周脂肪组织的裸血管环的收缩力;并用液体转移方法鉴证血管外周脂肪组织释放ADRF,使用工具药对ADRF作用途径进行观察。结果:与配对裸血管相比,带完整血管外周脂肪组织的胸主动脉在苯肾上腺素(PHE,10-6mol/L)诱发的血管收缩力下降20.5%;把孵育带完整血管外周脂肪组织的胸主动脉的生理池液体转移到配对裸血管,引起裸血管舒张20.8%;在无钙液中,有无血管外周脂肪组织的血管之间PHE诱发的收缩力无区别;钙激活的钾通道(KCa)阻断剂四乙胺和ATP敏感性钾通道(KATP)阻断剂格列苯脲均有效阻断ADRF的血管舒张作用。结论:血管外周脂肪组织释放一种引起血管舒张的ADRF,ADRF通过激活KCa、KATP发挥作用,且需钙离子参与。 展开更多
关键词 血管外膜源性舒张因子 脂肪组织 血管舒张 钾通道
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自发性高血压大鼠血管外周脂肪组织对血管调节功能的影响 被引量:1
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作者 张震洪 曾昭华 +3 位作者 罗碧辉 何文凯 何兆初 苏诚坚 《中国实用医刊》 2011年第11期1-4,共4页
目的观察自发性高血压大鼠(SHR)血管外周脂肪组织释放血管舒张因子功能的改变。方法把26周龄SHR和WKY两组大鼠相邻的两段胸主动脉环分为血管外周脂肪亚组和裸血管亚组,予1×10^-6mmol/L苯肾上腺素(PHE)刺激,比较两亚组血管... 目的观察自发性高血压大鼠(SHR)血管外周脂肪组织释放血管舒张因子功能的改变。方法把26周龄SHR和WKY两组大鼠相邻的两段胸主动脉环分为血管外周脂肪亚组和裸血管亚组,予1×10^-6mmol/L苯肾上腺素(PHE)刺激,比较两亚组血管收缩力的差异;用液体转移的方法,观察WKY孵育血管外周脂肪组织的培养液对裸血管张力的影响。结果WKY组血管外脂肪亚组的收缩力低于裸血管亚组的收缩力(P〈0.05),而SHR两血管亚组的收缩力差异无统计学意义(P〉0.05);把WKY孵育的血管外脂肪的培养液转移到裸血管诱发其快速舒张。结论WKY的血管外周脂肪组织释放一种可转移性血管舒张因子,降低血管对苯肾上腺素的反应性,调节血管功能。而SHR的血管外周脂肪组织这种血管调节作用减弱;血管外周脂肪组织这种功能异常可能是高血压病血管功能畀常的病理基础之一。 展开更多
关键词 血管外周脂肪组织 血管外膜源性舒张因子 高血压
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The functional change of perivascular adipose tissue in hypertensive rats and its mechanisms
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作者 张震洪 曾昭华 +3 位作者 罗碧辉 何文凯 何兆初 苏诚坚 《South China Journal of Cardiology》 CAS 2012年第1期46-52,58,共8页
Background Recent studies have showed that perivascular adipose tissue (PVAT) may secrete the adventitial-derived relaxing factor (ADRF) to affect vascular function.However,the functional change of ADRF in hyperte... Background Recent studies have showed that perivascular adipose tissue (PVAT) may secrete the adventitial-derived relaxing factor (ADRF) to affect vascular function.However,the functional change of ADRF in hypertensive status is seldom studied;and the mechanisms of ADRF remain unclear.Our study examined the ADRF secreted by perivascular adipose tissue of control rats with normal blood pressure (Wistar Kyoto rats,WKY) and discussed the mechanisms of ADRF;We observed the functional change in ADRF of perivascular adipose tissue in spontaneously hypertensive rats (SHRs).Method The two adjacent thoracic aorta rings of SHR and WKY rats were divided into naked vessel subgroup and PVAT subgroup.The differences of vascular contractility between the two subgroups induced by 10-6 mmol/L phenylephrine were compared.The effect of PVAT culture medium of WKY on the vascular tension of Fat (-) vessels was observed by liquid transfer measure.The mechanism of ADRF was determined by tool drugs.Results In WKY group,vascular contractility of Fat (+) subgroup was lower than that of the Fat (-) subgroup (P 0.05);while in SHR group,there was no difference between the two subgroups (P 0.05).Transferring the incubation solution of WKY Fat (+) subgroup to the matched Fat (-) subgroup induced rapid vasodilation.When incubating blood vessels in calcium free PSS solution,there was no significant difference of phenylephrine-induced vasoconstriction between Fat (-) and Fat (+) subgroup.Both glibenclamide,the blocker of ATP-sensitive potassium (KATP) channel and Tetraethy-lammonium chloride (TEA),the inhibitor of calcium-dependent potassium (KCa) channel,effectively inhibited vasodilation function of ADRF.Conclusions Perivascular adipose tissue in WKY releases ADRF which can cause vasodilation,while this function was inhibited in SHR.ADRF acts through the activation of KCa and KATP channels and calcium ion is involved. 展开更多
关键词 adventitial-derived relaxing factor hypertension calcium-dependent potassium (KCa) channel adenosine triphosphate-dependent potassium (KATP) channel CALCIUM
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