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血管活性肠肽对兔和豚鼠子宫肌层平滑肌的作用机制

Mechanism of action of vasoactive intestinal polypeptide on myometrial smooth muscle of rabbit and guinea-pig.

作者信息

Bolton T B, Lang R J, Ottesen B

出版信息

J Physiol. 1981 Sep;318:41-55. doi: 10.1113/jphysiol.1981.sp013849.

Abstract
  1. The action of vasoactive intestinal peptide (VIP) on the electrical and mechanical activity of strips of longitudinal myometrial smooth muscle from rabbits and guinea-pigs treated with oestradiol was studied in the sucrose-gap apparatus. 2. In myometrial strips which spontaneously exhibited regular contractions, or which were induced to contract rhythmically to the application of oxytocin, VIP reduced both the frequency and the force of contraction. 3. Contractions were associated with bursts of action potential discharge. In guinea-pig, the membrane potential reached its most negative value shortly following a burst and a slow decay of negativity followed ("generator potential'). VIP inhibited the decay of this negativity and increased the duration of the period between bursts. In rabbit myometrical strips, electrical discharges occurred less regularly but VIP also had an inhibitory action. The inhibitory action of VIP was not affected by the beta-adrenoreceptor blocker propranolol, by tetrodotoxin, or by apamin. 4. Using the double sucrose-gap apparatus, bursts of action potentials and contractions were elicited with depolarizing electrical pulses in the absence of oxytocin. Changes in membrane resistance were also estimated by eliciting hyperpolarizing electrotronic potentials. VIP hyperpolarized the membrane and inhibited contractions as depolarizing pulses now failed to reach threshold for action potential discharge or fewer action potentials were discharged. A small (about 10%) reduction in membrane resistance was freqeuently observed during the hyperpolarization. 5. If a single action potential was elicited in the presence of VIP, the tension generated by the muscle was less than in its absence. 6. In a calcium-free high-potassium (126 mM) solution, readmitting calcium produced contraction; VIP inhibited this contraction. Activation of beta-receptors by means of isoprenaline had a similar effect but unlike isoprenaline the action of VIP was not blocked by propranolol. 7. It is suggested that the primary action of VIP is on the calcium economy of the myometrial smooth muscle cell, possibly to accelerate sequestration and/or extrusion of calcium from the cell. In some way this is associated with inhibition of the generator potential, hyperpolarization, and with a small increase in permeability of the membrane to potassium.
摘要
  1. 采用蔗糖间隙装置研究了血管活性肠肽(VIP)对经雌二醇处理的兔和豚鼠子宫肌层纵行平滑肌条电活动和机械活动的作用。2. 在自发出现规则收缩或经催产素诱导产生节律性收缩的子宫肌条中,VIP可降低收缩频率和收缩力。3. 收缩与动作电位发放的爆发相关。在豚鼠中,动作电位爆发后不久膜电位达到最负值,随后出现缓慢的负性衰减(“发生器电位”)。VIP抑制这种负性衰减并增加爆发之间的时间间隔。在兔子宫肌条中,放电不太规则,但VIP也有抑制作用。VIP的抑制作用不受β-肾上腺素能受体阻滞剂普萘洛尔、河豚毒素或蜂毒明肽的影响。4. 使用双蔗糖间隙装置,在无催产素的情况下用去极化电脉冲引发动作电位爆发和收缩。还通过引发超极化电子电位来估计膜电阻的变化。VIP使膜超极化并抑制收缩,因为此时去极化脉冲未能达到动作电位发放阈值或发放的动作电位减少。在超极化期间经常观察到膜电阻有小幅(约10%)降低。5. 如果在有VIP的情况下引发单个动作电位,肌肉产生的张力比没有VIP时小。6. 在无钙的高钾(126 mM)溶液中,重新加入钙会产生收缩;VIP抑制这种收缩。通过异丙肾上腺素激活β受体有类似效果,但与异丙肾上腺素不同,VIP的作用不受普萘洛尔阻断。7. 提示VIP的主要作用在于子宫肌层平滑肌细胞的钙代谢,可能是加速钙从细胞内的隔离和/或排出。这在某种程度上与发生器电位的抑制、超极化以及膜对钾的通透性小幅增加有关。

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