von Kügelgen I, Späth L, Starke K
Pharmakologisches Institut, Freiburg, Federal Republic of Germany.
Naunyn Schmiedebergs Arch Pharmacol. 1992 Aug;346(2):187-96. doi: 10.1007/BF00165300.
Effects of adenosine and nucleotides on the release of previously stored [3H]-noradrenaline were studied in rabbit brain cortex slices. The slices were stimulated twice, in most experiments by 6 electrical field pulses delivered at 100 Hz. Adenosine and the nucleotides AMP, ADP, ATP, AMPS, ADP beta S, ATP gamma S, beta,gamma-imido-ATP and beta,gamma-methylene-ATP all reduced the evoked overflow of tritiated compounds. For purines for which concentration-response curves were determined, the order of potency was adenosine greater than ATP approximately ATP gamma S approximately beta,gamma-imido-ATP approximately ADP greater than beta,gamma-methylene-ATP. AMP 30 mumol/l and AMPS 30 mumol/l were approximately equieffective with 30 mumol/l of adenosine and ATP gamma S, and ADP beta S 30 mumol/l was approximately equieffective with 30 mumol/l of ADP. alpha,beta-Methylene-ADP, 2-methylthio-ATP, UTP and GTP gamma S did not change the evoked overflow of tritium. alpha,beta-Methylene-ATP caused an increase; however, the increase was small and became significant only after 59 min of exposure to alpha,beta-methylene-ATP or when the slices were stimulated by 30 pulses, 10 Hz. Neither adenosine deaminase (100 U/l) nor the blocker of 5'-nucleotidase, alpha,beta-methylene-ADP (10 mumol/l), attenuated the inhibition caused by ATP, ATP gamma S and beta,gamma-methylene-ATP, despite the fact that adenosine deaminase abolished the effect of adenosine. 8-Cyclopentyl-1,3-dipropylxanthine (DPCPX, 10 nmol/l) shifted the concentration-response curves of adenosine, ATP gamma S, beta,gamma-imido-ATP and beta,gamma-methylene-ATP to the right by very similar degrees. 8-(p-Sulphophenyl)-theophylline (30 and 300 mumol/l) also markedly antagonized the inhibition produced by ATP gamma S. alpha,beta-Methylene-ATP (10 and 30 mumol/l) and suramin (100 mumol/l) did not modify the effects of adenosine, ATP gamma S and beta,gamma-methylene-ATP. It is concluded that nucleotides themselves can inhibit the release of noradrenaline in the rabbit brain cortex. The nucleotides and adenosine seem to act at the same site, i.e., the A1 subtype of the P1-purinoceptor. The results support the notion that metabolically stable, phosphate chain-modified nucleotides such as ATP gamma S, beta,gamma-imido-ATP and beta,gamma-methylene-ATP can be potent P1 agonists. No evidence was found for presynaptic P2x-, P2y- or P3-purinoceptors.
在兔脑皮层切片中研究了腺苷和核苷酸对先前储存的[3H]-去甲肾上腺素释放的影响。在大多数实验中,切片接受两次刺激,通过以100Hz施加6个电场脉冲。腺苷以及核苷酸AMP、ADP、ATP、AMPS、ADPβS、ATPγS、β,γ-亚氨基-ATP和β,γ-亚甲基-ATP均降低了诱发的氚化化合物的溢出。对于测定浓度-反应曲线的嘌呤,效力顺序为腺苷>ATP≈ATPγS≈β,γ-亚氨基-ATP≈ADP>β,γ-亚甲基-ATP。30μmol/l的AMP和30μmol/l的AMPS与30μmol/l的腺苷和ATPγS大致等效,30μmol/l的ADPβS与30μmol/l的ADP大致等效。α,β-亚甲基-ADP、2-甲硫基-ATP、UTP和GTPγS未改变诱发的氚溢出。α,β-亚甲基-ATP引起增加;然而,增加幅度较小,仅在暴露于α,β-亚甲基-ATP 59分钟后或当切片由10Hz的30个脉冲刺激时才变得显著。腺苷脱氨酶(100U/l)和5'-核苷酸酶的阻断剂α,β-亚甲基-ADP(10μmol/l)均未减弱ATP、ATPγS和β,γ-亚甲基-ATP引起的抑制作用,尽管腺苷脱氨酶消除了腺苷的作用。8-环戊基-1,3-二丙基黄嘌呤(DPCPX,10nmol/l)使腺苷、ATPγS、β,γ-亚氨基-ATP和β,γ-亚甲基-ATP的浓度-反应曲线向右移动的程度非常相似。8-(对-磺苯基)-茶碱(30和300μmol/l)也显著拮抗ATPγS产生的抑制作用。α,β-亚甲基-ATP(10和30μmol/l)和苏拉明(100μmol/l)未改变腺苷、ATPγS和β,γ-亚甲基-ATP的作用。结论是核苷酸本身可抑制兔脑皮层中去甲肾上腺素的释放。核苷酸和腺苷似乎作用于同一部位,即P1嘌呤受体的A1亚型。结果支持这样的观点,即代谢稳定的、磷酸链修饰的核苷酸如ATPγS、β,γ-亚氨基-ATP和β,γ-亚甲基-ATP可以是有效的P1激动剂。未发现突触前P2x、P2y或P3嘌呤受体的证据。
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