染料木黄酮对兔门静脉平滑肌中ATP敏感性钾通道的抑制作用。

Inhibitory effects of genistein on ATP-sensitive K+ channels in rabbit portal vein smooth muscle.

作者信息

Ogata R, Kitamura K, Ito Y, Nakano H

机构信息

Department of Gynecology and Obstetrics, Faculty of Medicine, Kyushu University, Fukuoka, Japan.

出版信息

Br J Pharmacol. 1997 Dec;122(7):1395-404. doi: 10.1038/sj.bjp.0701532.

DOI:10.1038/sj.bjp.0701532

PMID:9421287

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1565089/

Abstract

Effects on the pinacidil-induced outward current of inhibitors of tyrosine kinases and phosphatases were investigated by use of a patch-clamp method in smooth muscle cells of the rabbit portal vein. 2. A specific tyrosine kinase inhibitor, genistein, inhibited the pinacidil-induced current in a concentration-dependent manner with an IC50 of 5.5 microM. Superfusion of Ca2+-free solution did not affect this inhibitory effect of genistein. At higher concentrations, genistein inhibited the voltage-dependent Ba2+ and K+ currents with IC50 values of > 100 microM and 75 microM respectively. Tyrphostin B46 (30 microM), a tyrosine kinase inhibitor, also inhibited the pinacidil-induced current by 70% of the control. 3. Sodium orthovanadate (100 microM), an inhibitor of tyrosine phosphatase, slightly but significantly enhanced both the pinacidil-induced and delayed rectifier K+ currents. Daidzein (100 microM), an inactive analogue of genistein, did not inhibit these currents. 4. Neither herbimycin A (1 microM), lavendustin A (30 microM), tyrphostin 23 (10 microM), which are also tyrosine kinase inhibitors, nor wortmannin (10 microM), a phosphatidylinositol 3-kinase inhibitor, had an effect on either the pinacidil-induced or delayed rectifier K+ currents. Epidermal growth factor (EGF; 1 microg ml(-1)) did not induce an outward current or enhance the pinacidil-induced current. 5. Pinacidil alone, in the cell-attached configuration, or pinacidil with GDP, in the inside-out configuration, activated a 42 pS channel in the smooth muscle cells of the rabbit portal vein. Genistein (30 microM) reduced the channel's open probability without inducing a change in unitary conductance at any holding potential (-30 to +20 mV). 6. In the inside-out configuration, genistein at 30 microM did not change the mean channel open time, but reduced the burst duration. At 100 microM genistein abolished channel opening. The inhibitory potencies with which 30 and 100 microM genistein acted on the unitary current of the ATP-sensitive K+ channel were similar to those seen in the whole-cell voltage-clamp configuration. 7. Although direct inhibitory actions of genistein on the ATP-sensitive K+ channels are not ruled out, our results suggest that a protein tyrosine kinase may play a role in the regulation of ATP-sensitive K+ channel activity in the rabbit portal vein.

摘要

采用膜片钳方法在兔门静脉平滑肌细胞中研究了酪氨酸激酶和磷酸酶抑制剂对吡那地尔诱导的外向电流的影响。2. 一种特异性酪氨酸激酶抑制剂染料木黄酮以浓度依赖性方式抑制吡那地尔诱导的电流，IC50为5.5微摩尔。无钙溶液灌流不影响染料木黄酮的这种抑制作用。在较高浓度时，染料木黄酮分别以>100微摩尔和75微摩尔的IC50值抑制电压依赖性Ba2+和K+电流。酪氨酸激酶抑制剂酪氨酸磷酸化酶B46（30微摩尔）也使吡那地尔诱导的电流抑制至对照的70%。3. 酪氨酸磷酸酶抑制剂原钒酸钠（100微摩尔）轻微但显著增强了吡那地尔诱导的电流和延迟整流钾电流。染料木黄酮的无活性类似物大豆苷元（100微摩尔）不抑制这些电流。4. 同样作为酪氨酸激酶抑制剂的赫曲霉素A（1微摩尔）、拉文达ustin A（30微摩尔）、酪氨酸磷酸化酶23（10微摩尔）以及磷脂酰肌醇-3激酶抑制剂渥曼青霉素（10微摩尔）对吡那地尔诱导的电流或延迟整流钾电流均无影响。表皮生长因子（EGF；1微克/毫升）未诱导外向电流或增强吡那地尔诱导的电流。5. 在细胞贴附模式下单独的吡那地尔或在内外翻模式下与GDP一起的吡那地尔激活了兔门静脉平滑肌细胞中的一个42皮安的通道。染料木黄酮（30微摩尔）降低了通道的开放概率，而在任何钳制电位（-30至+20毫伏）下均未引起单位电导的变化。6. 在内外翻模式下，30微摩尔的染料木黄酮不改变平均通道开放时间，但缩短了爆发持续时间。在100微摩尔时，染料木黄酮使通道开放消失。30微摩尔和100微摩尔染料木黄酮对ATP敏感性钾通道单位电流的抑制效力与在全细胞膜片钳模式下观察到的相似。7. 尽管不能排除染料木黄酮对ATP敏感性钾通道的直接抑制作用，但我们的结果表明，一种蛋白酪氨酸激酶可能在兔门静脉ATP敏感性钾通道活性的调节中起作用。

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染料木黄酮对兔门静脉平滑肌中ATP敏感性钾通道的抑制作用。

Inhibitory effects of genistein on ATP-sensitive K+ channels in rabbit portal vein smooth muscle.

作者信息

Ogata R, Kitamura K, Ito Y, Nakano H

机构信息

Department of Gynecology and Obstetrics, Faculty of Medicine, Kyushu University, Fukuoka, Japan.

出版信息

Br J Pharmacol. 1997 Dec;122(7):1395-404. doi: 10.1038/sj.bjp.0701532.

DOI:10.1038/sj.bjp.0701532

PMID:9421287

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1565089/

Abstract

Effects on the pinacidil-induced outward current of inhibitors of tyrosine kinases and phosphatases were investigated by use of a patch-clamp method in smooth muscle cells of the rabbit portal vein. 2. A specific tyrosine kinase inhibitor, genistein, inhibited the pinacidil-induced current in a concentration-dependent manner with an IC50 of 5.5 microM. Superfusion of Ca2+-free solution did not affect this inhibitory effect of genistein. At higher concentrations, genistein inhibited the voltage-dependent Ba2+ and K+ currents with IC50 values of > 100 microM and 75 microM respectively. Tyrphostin B46 (30 microM), a tyrosine kinase inhibitor, also inhibited the pinacidil-induced current by 70% of the control. 3. Sodium orthovanadate (100 microM), an inhibitor of tyrosine phosphatase, slightly but significantly enhanced both the pinacidil-induced and delayed rectifier K+ currents. Daidzein (100 microM), an inactive analogue of genistein, did not inhibit these currents. 4. Neither herbimycin A (1 microM), lavendustin A (30 microM), tyrphostin 23 (10 microM), which are also tyrosine kinase inhibitors, nor wortmannin (10 microM), a phosphatidylinositol 3-kinase inhibitor, had an effect on either the pinacidil-induced or delayed rectifier K+ currents. Epidermal growth factor (EGF; 1 microg ml(-1)) did not induce an outward current or enhance the pinacidil-induced current. 5. Pinacidil alone, in the cell-attached configuration, or pinacidil with GDP, in the inside-out configuration, activated a 42 pS channel in the smooth muscle cells of the rabbit portal vein. Genistein (30 microM) reduced the channel's open probability without inducing a change in unitary conductance at any holding potential (-30 to +20 mV). 6. In the inside-out configuration, genistein at 30 microM did not change the mean channel open time, but reduced the burst duration. At 100 microM genistein abolished channel opening. The inhibitory potencies with which 30 and 100 microM genistein acted on the unitary current of the ATP-sensitive K+ channel were similar to those seen in the whole-cell voltage-clamp configuration. 7. Although direct inhibitory actions of genistein on the ATP-sensitive K+ channels are not ruled out, our results suggest that a protein tyrosine kinase may play a role in the regulation of ATP-sensitive K+ channel activity in the rabbit portal vein.

摘要

采用膜片钳方法在兔门静脉平滑肌细胞中研究了酪氨酸激酶和磷酸酶抑制剂对吡那地尔诱导的外向电流的影响。2. 一种特异性酪氨酸激酶抑制剂染料木黄酮以浓度依赖性方式抑制吡那地尔诱导的电流，IC50为5.5微摩尔。无钙溶液灌流不影响染料木黄酮的这种抑制作用。在较高浓度时，染料木黄酮分别以>100微摩尔和75微摩尔的IC50值抑制电压依赖性Ba2+和K+电流。酪氨酸激酶抑制剂酪氨酸磷酸化酶B46（30微摩尔）也使吡那地尔诱导的电流抑制至对照的70%。3. 酪氨酸磷酸酶抑制剂原钒酸钠（100微摩尔）轻微但显著增强了吡那地尔诱导的电流和延迟整流钾电流。染料木黄酮的无活性类似物大豆苷元（100微摩尔）不抑制这些电流。4. 同样作为酪氨酸激酶抑制剂的赫曲霉素A（1微摩尔）、拉文达ustin A（30微摩尔）、酪氨酸磷酸化酶23（10微摩尔）以及磷脂酰肌醇-3激酶抑制剂渥曼青霉素（10微摩尔）对吡那地尔诱导的电流或延迟整流钾电流均无影响。表皮生长因子（EGF；1微克/毫升）未诱导外向电流或增强吡那地尔诱导的电流。5. 在细胞贴附模式下单独的吡那地尔或在内外翻模式下与GDP一起的吡那地尔激活了兔门静脉平滑肌细胞中的一个42皮安的通道。染料木黄酮（30微摩尔）降低了通道的开放概率，而在任何钳制电位（-30至+20毫伏）下均未引起单位电导的变化。6. 在内外翻模式下，30微摩尔的染料木黄酮不改变平均通道开放时间，但缩短了爆发持续时间。在100微摩尔时，染料木黄酮使通道开放消失。30微摩尔和100微摩尔染料木黄酮对ATP敏感性钾通道单位电流的抑制效力与在全细胞膜片钳模式下观察到的相似。7. 尽管不能排除染料木黄酮对ATP敏感性钾通道的直接抑制作用，但我们的结果表明，一种蛋白酪氨酸激酶可能在兔门静脉ATP敏感性钾通道活性的调节中起作用。

染料木黄酮对兔门静脉平滑肌中ATP敏感性钾通道的抑制作用。

Inhibitory effects of genistein on ATP-sensitive K+ channels in rabbit portal vein smooth muscle.

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染料木黄酮对兔门静脉平滑肌中ATP敏感性钾通道的抑制作用。

Inhibitory effects of genistein on ATP-sensitive K+ channels in rabbit portal vein smooth muscle.

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