4,4'-二异硫氰基芪-2,2'-二磺酸盐(DIDS)对大鼠输精管中P2X嘌呤受体的阻断作用
Blockade by 4,4'-diisothiocyanatostilbene-2,2'-disulphonate (DIDS) of P2X-purinoceptors in rat vas deferens.
作者信息
Bültmann R, Starke K
机构信息
Pharmakologisches Institut, Universität Freiburg, Germany.
出版信息
Br J Pharmacol. 1994 Jun;112(2):690-4. doi: 10.1111/j.1476-5381.1994.tb13131.x.
Abstract
- The possibility of an antagonist effect of 4,4'-diisothiocyanatostilbene-2,2'-disulphonate (DIDS) at P2X-purinoceptors was studied in rat vas deferens. 2. DIDS reduced contractions elicited by alpha,beta-methylene ATP 3 microM, IC50 1.6 microM, but did not change contractions elicited by K+ 35 mM. DIDS 3.2 microM slightly shifted the concentration-response curve of alpha,beta-methylene ATP to the right and reduced the maximum. DIDS 10 microM markedly decreased and DIDS 32 microM abolished contractions over the entire range of the alpha, beta-methylene ATP concentration-response curve. DIDS 32 microM also abolished contractions elicited by ATP but did not change contractions elicited by noradrenaline. The antagonist effect of DIDS was only slowly reversible. 3. The presence of either suramin 320 microM or alpha,beta-methylene ATP 10 microM during the exposure to DIDS protected the tissue from the long-lasting blocking effect of DIDS. 4. 4,4'-Diisothiocyanatodihydrostilbene-2,2'-disulphonate (H2DIDS) was equipotent with DIDS whereas several analogues in which one or both of the isothiocyanate residues were replaced were less effective or without effect against alpha,beta-methylene ATP. 5. DIDS attenuated the purinergic component of neurogenic contractions elicited by electrical field stimulation, IC50 3.9 microM, but did not change the adrenergic component. 6. It is concluded that DIDS causes a selective, long-lasting, non-equilibrium blockade of P2X-purinoceptors in rat vas deferens. Due to this effect it also selectively blocks the purinergic component of neurogenic contractions.
摘要
- 在大鼠输精管中研究了4,4'-二异硫氰基芪-2,2'-二磺酸盐(DIDS)对P2X嘌呤受体的拮抗作用。2. DIDS可降低由3 microM α,β-亚甲基ATP引起的收缩,IC50为1.6 microM,但不改变由35 mM K+引起的收缩。3.2 microM的DIDS使α,β-亚甲基ATP的浓度-反应曲线轻微右移并降低最大值。10 microM的DIDS显著降低,32 microM的DIDS在α,β-亚甲基ATP浓度-反应曲线的整个范围内消除收缩。32 microM的DIDS也消除了由ATP引起的收缩,但不改变由去甲肾上腺素引起的收缩。DIDS的拮抗作用仅缓慢可逆。3. 在暴露于DIDS期间,320 microM的苏拉明或10 microM的α,β-亚甲基ATP的存在可保护组织免受DIDS的持久阻断作用。4. 4,4'-二异硫氰基二氢芪-2,2'-二磺酸盐(H2DIDS)与DIDS等效,而其中一个或两个异硫氰酸酯残基被取代的几种类似物对α,β-亚甲基ATP的作用较小或无作用。5. DIDS减弱了电场刺激引起的神经源性收缩的嘌呤能成分,IC50为3.9 microM,但不改变肾上腺素能成分。6. 得出结论,DIDS在大鼠输精管中引起P2X嘌呤受体的选择性、持久、非平衡阻断。由于这种作用,它还选择性地阻断神经源性收缩的嘌呤能成分。
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2
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3
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