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佛波酯对海马钙通道电流的蛋白激酶C依赖性和非依赖性作用。

Protein kinase C-dependent and -independent effects of phorbol esters on hippocampal calcium channel current.

作者信息

Doerner D, Abdel-Latif M, Rogers T B, Alger B E

机构信息

Department of Physiology, University of Maryland School of Medicine, Baltimore 21201.

出版信息

J Neurosci. 1990 May;10(5):1699-706. doi: 10.1523/JNEUROSCI.10-05-01699.1990.

DOI:10.1523/JNEUROSCI.10-05-01699.1990
PMID:2159060
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6570075/
Abstract

Despite their widespread use in investigations of protein kinase C (PKC), concern is often expressed regarding the specificity of action of phorbol esters. We have extensively compared the effects of PDBu, a phorbol ester that activates PKC, with those of its inactive analog, 4 alpha-PDBu, on calcium (Ca) channel regulation in acutely isolated guinea pig hippocampal neurons and found that PKC-dependent and -independent actions could be clearly distinguished. While both phorbol esters depressed whole-cell barium current through Ca channels (IBa), PDBu was approximately 100-fold more potent than 4 alpha-PDBu. PKC-independent effects began to appear in the range of 5-10 microM, doses that, while high, have been used in some investigations. Moreover, only PDBu (1) was active when applied intracellularly, (2) had effects that were blocked by the PKC inhibitor H-7, and (3) induced PKC translocation with potency similar to its potency in depressing IBa. The finding that 4 alpha-PDBu acted only extracellularly was unexpected and suggested either that it acted via an extracellular binding site or that its orientation in the membrane was crucial to its effects on Ca channels. Finally, (4) PDBu alone caused a hyperpolarizing shift in the voltage dependence of the high-voltage-activated, rapidly inactivating (N type) component of Ca current. This result extends our previous finding that the N-type current component was depressed by PDBu to a greater extent than the L-type component and may represent an important new mode of neurotransmitter regulation of ion channels in the brain via PKC.

摘要

尽管佛波酯在蛋白激酶C(PKC)研究中被广泛应用,但人们常常对其作用特异性表示担忧。我们已全面比较了激活PKC的佛波酯PDBu与其无活性类似物4α-PDBu对急性分离的豚鼠海马神经元钙(Ca)通道调节的影响,发现PKC依赖性和非依赖性作用可被清晰区分。虽然两种佛波酯均通过Ca通道(IBa)降低全细胞钡电流,但PDBu的效力约为4α-PDBu的100倍。PKC非依赖性作用在5 - 10微摩尔范围内开始显现,此剂量虽高,但在一些研究中已被使用。此外,只有PDBu(1)在细胞内应用时具有活性,(2)其作用可被PKC抑制剂H - 7阻断,且(3)诱导PKC转位的效力与其降低IBa的效力相似。4α-PDBu仅在细胞外起作用这一发现出乎意料,表明它可能通过细胞外结合位点起作用,或者其在膜中的取向对其对Ca通道的作用至关重要。最后,(4)单独使用PDBu会使钙电流的高电压激活、快速失活(N型)成分的电压依赖性发生超极化偏移。这一结果扩展了我们之前的发现,即PDBu对N型电流成分的抑制程度大于L型成分,并且可能代表了大脑中通过PKC对离子通道进行神经递质调节的一种重要新方式。

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