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介导狨猴膀胱平滑肌收缩和舒张的嘌呤受体亚型。

Purinoceptor subtypes mediating contraction and relaxation of marmoset urinary bladder smooth muscle.

作者信息

McMurray G, Dass N, Brading A F

机构信息

University Department of Pharmacology, Oxford.

出版信息

Br J Pharmacol. 1998 Apr;123(8):1579-86. doi: 10.1038/sj.bjp.0701774.

Abstract
  1. The effects of adenosine triphosphate (ATP), adenosine diphosphate (ADP), alpha,beta-methylene-ATP (alpha,beta-MeATP) and 2-methylthio-ATP (2-MeSATP) on longitudinally orientated smooth muscle strips from marmoset urinary bladder were investigated by use of standard organ bath techniques. 2. After being mounted in superfusion organ baths, 66.7% (n=249) of marmoset detrusor smooth muscle strips developed spontaneous tone, 48.2% of all strips examined developed tone equivalent to greater than 0.1 g mg(-1) of tissue and were subsequently utilized in the present investigation. 3. On exposure to ATP, muscle strips exhibited a biphasic response, a rapid and transient contraction followed by a more prolonged relaxation. Both responses were found to be concentration-dependent. ADP and 2-MeSATP elicited a similar response (contraction followed by relaxation), whereas application of alpha,beta-MeATP only produced a contraction. The potency order for each effect was alpha,beta-MeATP> >2-MeSATP> ATP>ADP (contractile response) and ATP=2-MeSATP> or = ADP> > alpha,beta-MeATP (relaxational response). 4. Desensitization with alpha,beta-MeATP (10 microM) abolished the contractile phase of the response to ATP, but had no effect on the level of relaxation evoked by this agonist. On the other hand, the G-protein inactivator, GDPbetaS (100 microM) abolished only the relaxation response to ATP. Suramin (general P2 antagonist, 100 microM) shifted both the contractile and relaxation ATP concentration-response curves to the right, whereas cibacron blue (P2Y antagonist, 10 microM) only antagonized the relaxation response to ATP. In contrast, the adenosine receptor antagonist, 8-phenyltheophylline (10 microM), had no effect on the relaxation response curve to ATP. 5. Incubation with tetrodotoxin (TTX, 3 microM) or depolarization of the muscle strip with 40 mM K+ Krebs failed to abolish the relaxation to ATP. In addition, neither Nomega-nitro-L-arginine (L-NOARG, 10 microM) nor methylene blue (10 microM) had any effect on the relaxation response curve. However, tos-phe-chloromethylketone (TPCK, 3 microM), an inhibitor of cyclicAMP-dependent protein kinase A (PKA), significantly (P<0.01) shifted the curve for the ATP-induced relaxation to the right. 6. It is proposed that marmoset detrusor smooth muscle contains two receptors for ATP, a classical P2X-type receptor mediating smooth muscle contraction, and a P2Y (G-protein linked) receptor mediating smooth muscle relaxation. The results also indicate that the ATP-evoked relaxation may occur through the activation of cyclicAMP-dependent PKA.
摘要
  1. 采用标准器官浴技术,研究了三磷酸腺苷(ATP)、二磷酸腺苷(ADP)、α,β-亚甲基三磷酸腺苷(α,β-MeATP)和2-甲硫基三磷酸腺苷(2-MeSATP)对狨猴膀胱纵向平滑肌条的影响。2. 将平滑肌条安装在灌注器官浴中后,66.7%(n = 249)的狨猴逼尿肌平滑肌条出现自发张力,在所有检测的条带中,48.2%的条带产生的张力相当于大于0.1 g mg(-1)的组织,随后用于本研究。3. 暴露于ATP时,肌肉条表现出双相反应,先是快速短暂的收缩,随后是更持久的舒张。发现这两种反应均呈浓度依赖性。ADP和2-MeSATP引发类似反应(收缩后舒张),而应用α,β-MeATP仅产生收缩。每种效应的效力顺序为α,β-MeATP >> 2-MeSATP > ATP > ADP(收缩反应)和ATP = 2-MeSATP ≥ ADP >> α,β-MeATP(舒张反应)。4. 用α,β-MeATP(10 μM)脱敏消除了对ATP反应的收缩期,但对该激动剂引起的舒张水平无影响。另一方面,G蛋白失活剂GDPβS(100 μM)仅消除了对ATP的舒张反应。苏拉明(通用P2拮抗剂,100 μM)将收缩和舒张ATP浓度-反应曲线均向右移动,而西巴氯铵(P2Y拮抗剂,10 μM)仅拮抗对ATP的舒张反应。相比之下,腺苷受体拮抗剂8-苯基茶碱(10 μM)对ATP舒张反应曲线无影响。5. 用河豚毒素(TTX,3 μM)孵育或用40 mM K+ Krebs使肌肉条去极化未能消除对ATP的舒张反应。此外,Nω-硝基-L-精氨酸(L-NOARG,10 μM)和亚甲蓝(10 μM)对舒张反应曲线均无任何影响。然而,环磷酸腺苷依赖性蛋白激酶A(PKA)的抑制剂tos-苯丙氨酸氯甲基酮(TPCK,3 μM)使ATP诱导的舒张曲线显著(P < 0.01)向右移动。6. 提出狨猴逼尿肌平滑肌含有两种ATP受体,一种是介导平滑肌收缩的经典P2X型受体,另一种是介导平滑肌舒张的P2Y(G蛋白偶联)受体。结果还表明,ATP诱发的舒张可能通过环磷酸腺苷依赖性PKA的激活而发生。

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