大鼠脑突触体膜中多种类型的大电导电压依赖性钙激活钾通道。
Multiple types of voltage-dependent Ca2+-activated K+ channels of large conductance in rat brain synaptosomal membranes.
作者信息
Farley J, Rudy B
机构信息
Department of Psychology, Princeton University, New Jersey 08544.
出版信息
Biophys J. 1988 Jun;53(6):919-34. doi: 10.1016/S0006-3495(88)83173-4.
K+-selective ion channels from a mammalian brain synaptosomal membrane preparation were inserted into planar phospholipid bilayers on the tips of patch-clamp pipettes, and single-channel currents were measured. Multiple distinct classes of K+ channels were observed. We have characterized and described the properties of several types of voltage-dependent, Ca2+-activated K+ channels of large single-channel conductance (greater than 50 pS in symmetrical KCl solutions). One class of channels (Type I) has a 200-250-pS single-channel conductance. It is activated by internal calcium concentrations greater than 10(-7) M, and its probability of opening is increased by membrane depolarization. This channel is blocked by 1-3 mM internal concentrations of tetraethylammonium (TEA). These channels are similar to the BK channel described in a variety of tissues. A second novel group of voltage-dependent, Ca2+-activated K+ channels was also studied. These channels were more sensitive to internal calcium, but less sensitive to voltage than the large (Type I) channel. These channels were minimally affected by internal TEA concentrations of 10 mM, but were blocked by a 50 mM concentration. In this class of channels we found a wide range of relatively large unitary channel conductances (65-140 pS). Within this group we have characterized two types (75-80 pS and 120-125 pS) that also differ in gating kinetics. The various types of voltage-dependent, Ca2+-activated K+ channels described here were blocked by charybdotoxin added to the external side of the channel. The activity of these channels was increased by exposure to nanomolar concentrations of the catalytic subunit of cAMP-dependent protein kinase. These results indicate that voltage-dependent, charybdotoxin-sensitive Ca2+-activated K+ channels comprise a class of related, but distinguishable channel types. Although the Ca2+-activated (Type I and II) K+ channels can be distinguished by their single-channel properties, both could contribute to the voltage-dependent Ca2+-activated macroscopic K+ current (IC) that has been observed in several neuronal somata preparations, as well as in other cells. Some of the properties reported here may serve to distinguish which type contributes in each case. A third class of smaller (40-50 pS) channels was also studied. These channels were independent of calcium over the concentration range examined (10(-7)-10(-3) M), and were also independent of voltage over the range of pipette potentials of -60 to +60 mV. Type III channels were unaffected by internal TEA concentrations <50 mM. Our results also indicate that the study of K+ channels in lipid bilayers may allow the identification and characterization of novel K+ channels from brain regions otherwise inaccessible to conventional recording techniques.
将来自哺乳动物脑突触体膜制剂的钾离子选择性离子通道插入膜片钳微电极尖端的平面磷脂双分子层中,并测量单通道电流。观察到多种不同类型的钾通道。我们已经对几种大的单通道电导(在对称氯化钾溶液中大于50皮安)的电压依赖性、钙激活钾通道的特性进行了表征和描述。一类通道(I型)具有200 - 250皮安的单通道电导。它由内部钙浓度大于10⁻⁷M激活,其开放概率因膜去极化而增加。该通道被内部浓度为1 - 3毫摩尔的四乙铵(TEA)阻断。这些通道类似于在多种组织中描述的BK通道。还研究了另一组新型的电压依赖性、钙激活钾通道。这些通道对内部钙更敏感,但比对大的(I型)通道对电压更不敏感。这些通道在内部TEA浓度为10毫摩尔时影响最小,但在50毫摩尔浓度时被阻断。在这类通道中,我们发现了范围广泛的相对较大的单通道电导(65 - 140皮安)。在这一组中,我们已经表征了两种类型(75 - 80皮安和120 - 125皮安),它们在门控动力学上也有所不同。这里描述的各种电压依赖性、钙激活钾通道被添加到通道外侧的蝎毒素阻断。这些通道的活性通过暴露于纳摩尔浓度的环磷酸腺苷依赖性蛋白激酶催化亚基而增加。这些结果表明,电压依赖性、蝎毒素敏感的钙激活钾通道构成了一类相关但可区分的通道类型。尽管钙激活的(I型和II型)钾通道可以通过它们的单通道特性来区分,但两者都可能对在几种神经元胞体制剂以及其他细胞中观察到的电压依赖性钙激活宏观钾电流(IC)有贡献。这里报道的一些特性可能有助于区分在每种情况下哪种类型起作用。还研究了第三类较小的(40 - 50皮安)通道。在研究的钙浓度范围(10⁻⁷ - 10⁻³M)内,这些通道与钙无关,并且在微电极电位为 - 60至 + 60毫伏的范围内也与电压无关。III型通道不受内部TEA浓度<50毫摩尔的影响。我们的结果还表明,在脂质双分子层中研究钾通道可能允许从传统记录技术无法到达的脑区鉴定和表征新型钾通道。
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