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大蝎毒素对兔离体耳中央动脉和分支动脉的不同作用。

Differential actions of charybdotoxin on central and daughter branch arteries of the rabbit isolated ear.

作者信息

Berman R S, Griffith T M

机构信息

Department of Diagnostic Radiology, University of Wales College of Medicine, Cardiff.

出版信息

Br J Pharmacol. 1997 Feb;120(4):639-46. doi: 10.1038/sj.bjp.0700962.

Abstract
  1. By use of rabbit isolated perfused intact ears and isolated perfused segments of central and first generation daughter branch ear arteries, we investigated the actions of charybdotoxin (ChTX), a blocker of calcium-activated K+ channels (KCa channels), and N omega-nitro-L-arginine methyl ester (L-NAME) on pressure-flow and diameter-flow relationships. 2. ChTX (1 nM) induced an upwards shift in the pressure-flow curve in the rabbit intact isolated ear preconstricted with 5-hydroxytryptamine (5-HT; 100 nM) with subsequent administration of L-NAME (100 microM) inducing a further upwards shift. L-NAME itself induced an upwards shift in the pressure-flow curve, but subsequent administration of ChTX was without significant effect. 3. Microangiographic analysis revealed a tendency of ChTX (1 nM) to decrease vessel diameter in the central ear artery (G0) with little effect on the first two generations of daughter branch arteries (G1 and G2) in the intact ear. Subsequent addition of L-NAME (100 microM) did not significantly further decrease vessel diameter in G0, but did decrease vessel diameter in G1 and G2. L-NAME itself showed a tendency to decrease vessel diameter in G0, G1 and G2 vessels with subsequent addition of ChTX being without significant effect. 4. In an isolated G0 preparation which was preconstricted with 5-HT (100 nM), ChTX (1 nM) caused an upwards shift in the pressure-flow curve which was augmented by subsequent addition of L-NAME (100 microM). L-NAME (100 microM) itself caused an upwards shift in the pressure-flow curve but subsequent addition of ChTX (1 nM) had no significant effect. 5. In comparison, in an isolated G1 preparation which was preconstricted with 5-HT (100 nM), ChTX (1 nM) had no significant effect on the pressure-flow curve relative to control, but subsequent addition of L-NAME (100 microM) caused an upwards shift. L-NAME (100 microM) itself induced an upwards shift in the pressure-flow curve with subsequent addition of ChTX (1 nM) being without significant effect. 6. ChTX (10 pM-10 nM) caused a concentration-dependent increase in perfusion pressure in isolated G0 and G1 preparations at fixed flow rates of 2 ml min-1 and 0.5 ml min-1, respectively. These responses were enhanced in the presence of L-NAME (100 microM) in G1 but not G0 preparations. 7. We conclude that at 1 nM, ChTX exhibits differential actions on central and daughter branch arteries of the intact ear of the rabbit, which are also apparent in the corresponding arteries when studied in isolation. The action of 1 nM ChTX in G0 vessels may reflect inhibition of either the release or action of nitric oxide as it was blocked in the presence of L-NAME. At higher concentrations of ChTX, there would appear to be a direct constrictor effect on vascular smooth muscle which is apparent in both G0 and G1 vessels. This observed heterogeneity could reflect different distributions of KCa channels between central and daughter branch arteries at either the endothelial or smooth muscle levels, or both.
摘要
  1. 通过使用兔离体灌注的完整耳朵以及中央耳动脉和第一代分支耳动脉的离体灌注节段,我们研究了钙激活钾通道(KCa通道)阻滞剂查卡毒素(ChTX)和Nω-硝基-L-精氨酸甲酯(L-NAME)对压力-流量和管径-流量关系的作用。2. ChTX(1 nM)使预先用5-羟色胺(5-HT;100 nM)预收缩的兔离体完整耳朵的压力-流量曲线向上移位,随后给予L-NAME(100 μM)导致进一步向上移位。L-NAME本身使压力-流量曲线向上移位,但随后给予ChTX无显著影响。3. 微血管造影分析显示,ChTX(1 nM)有使完整耳朵中央耳动脉(G0)管径减小的趋势,而对前两代分支耳动脉(G1和G2)影响很小。随后加入L-NAME(100 μM)并未使G0的管径进一步显著减小,但使G1和G2的管径减小。L-NAME本身有使G0、G1和G2血管管径减小的趋势,随后加入ChTX无显著影响。4. 在预先用5-HT(100 nM)预收缩的离体G0标本中,ChTX(1 nM)使压力-流量曲线向上移位,随后加入L-NAME(100 μM)使其增强。L-NAME(100 μM)本身使压力-流量曲线向上移位,但随后加入ChTX(1 nM)无显著影响。5. 相比之下,在预先用5-HT(100 nM)预收缩的离体G1标本中,ChTX(l nM)相对于对照对压力-流量曲线无显著影响,但随后加入L-NAME(100 μM)导致曲线向上移位。L-NAME(100 μM)本身使压力-流量曲线向上移位,随后加入ChTX(1 nM)无显著影响。6. ChTX(10 pM - 10 nM)分别在固定流速2 ml/min和0.5 ml/min下使离体G0和G1标本的灌注压力呈浓度依赖性增加。在G1标本中,L-NAME(100 μM)存在时这些反应增强,但在G0标本中未增强。7. 我们得出结论,1 nM时,ChTX对兔完整耳朵的中央耳动脉和分支耳动脉表现出不同作用,在离体研究相应动脉时也很明显。1 nM ChTX在G0血管中的作用可能反映了一氧化氮释放或作用的抑制,因为在L-NAME存在时被阻断。在较高浓度的ChTX时,似乎对血管平滑肌有直接收缩作用,在G0和G1血管中均明显。这种观察到的异质性可能反映了中央耳动脉和分支耳动脉在内皮或平滑肌水平或两者的KCa通道分布不同。

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