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机构地区:[1]遵义医学院生理学教研室,贵州遵义563003 [2]遵义医学院珠海校区生理学教研室,广东珠海519041
出 处:《遵义医学院学报》2005年第6期511-514,共4页Journal of Zunyi Medical University
基 金:珠海市科技局基金 资助项目:(PC2003010057)
摘 要:目的探讨大鼠第三脑室前腹侧区(AV3V)肾素-血管紧张素系统(RAS)对近球小管Na+,K+-AT- Pase活性的影响及作用途径。方法用小动物脑立体定位仪在大鼠AV3V埋植钢管供中枢注射,放射免疫法测定血浆血管紧张素Ⅱ(AngⅡ)及血清内源性洋地黄样物质(EDLS)浓度,立体显微镜下手工微分离近球小管,液体闪烁计数器测定标记磷酸Ⅱ的方法检测近球小管Na+,K+-ATPase活性。结果①与AV3V注射人工脑脊液(aCSF) 的结果比较,AV3V注射AngⅡ后,血浆AngⅡ水平无显著变化,血清EDLS水平显著升高,近球小管Na+,K+-AT- Pase活性显著下降。②在AV3V注射沙拉新后,血浆AngⅡ水平无显著变化,血清EDLS水平显著降低,近球小管 Na+,K+-ATPase活性显著增加。结论 AngⅡ作用于AV3V的AngⅡ受体,引起近球小管Na+,K+-ATPase活性降低,AngⅡ的这一作用可能与促进EDLS的释放有关。Objective The present study was designed to explore both the effect and the access of the intrinsic brain renin-angiotensin system (RAS) in the anteroventral part of the third ventricle (AV3V) on Na+ , K^+ -ATPase activity of proximal tubule. Methods Studies were performed on anesthetized Wistar rats and AV3V microinjection waa carried out by a stainless steel tube planted on the accurate site in the rat brain through a stereotactic apparatus. Ang Ⅱ and EDLS levels in plasm or serum were assessed by radioimmunoassay (ILIA). Renal proximal tubules were isolated by means of manual microdissection then a single tubule was incubated and the hydrolytic activity of Na^+, K^+-ATPase was determined using a radiochemical assay based on the measurement of Pi released from [ γ-32p] ATP by liquid scintillation counter(LSC). Resuits Serum endogenous digitalis - like substance ( EDLS ) level increased obviously on 60th minute after administration of Ang Ⅱ ( P 〈 0.01 vs aCSF). In contrast, a statistically significant decrease of the activity of Na^+ K^+ -ATPasc from rats proximal tubule was measured ( P 〈 0.01 vs aCSF). These effects could be antagonized by microinjection of saralasin, an angiotensin receptor antagonist, into the AV3V. The alterations of plasma Ang Ⅱ level were not significantly different in all groups after administration of the same volume of Ang Ⅱ, Sat. or aCSF ( P 〉 0.05) . There was a negative linear correlation between the serum EDLS level and proximal tubule Na^+, K^+-aATPase activity (r = -0. 905, P 〈 0.01 ). Conclusions The central Ang Ⅱ may stimulate and modulate EDLS release, acting directly upon AV3V which is an important receptive site for Ang H, consequently the Na^+, K^+-ATPase activity of renal cortex is alternated.
关 键 词:AV3V 近球小管 血管紧张素Ⅱ NA^+ K^+-ATPase 内源性洋地黄样物质
分 类 号:R331[医药卫生—人体生理学]
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