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[3H]色胺与酸性脂质重构组分的结合

[3H]tryptamine binding to reconstituted fraction of acidic lipids.

作者信息

Karasawa A, Ogihara M, Ishitani R

出版信息

J Pharmacobiodyn. 1987 Feb;10(2):78-84. doi: 10.1248/bpb1978.10.78.

DOI:10.1248/bpb1978.10.78
PMID:3598846
Abstract

The possible involvement of sulphatides (CS), phosphatidylserine (PS) and phosphatidylinositol (PI) in [3H]tryptamine binding to various reconstituted fractions of these acidic lipids was examined by Sephadex LH20 column chromatography. The results indicated that each of the four systems, PS, PS-CS, PS-PI and PS-CS-PI, had the same binding capacity for [3H]tryptamine, whereas other systems (CS, PI and CS-PI systems) had no binding capacity. Furthermore, competitive inhibition experiments revealed that among these four reconstituted systems, the PS-CS system exhibited the highest affinity for 5-methoxytryptamine. Kinetic studies suggested that at least two binding components (or sites) are implicated in the binding of [3H]tryptamine to the reconstituted system of PS and CS with apparent KD values of 3 and 10 nM. Displacement studies with various compounds indicated that only tryptamine and 5-methoxytryptamine inhibited the [3H]tryptamine binding to this fraction, while other indoleamine analogues and neurotransmitters had no effect. In addition, we subjected whole rat brain synaptic plasma membranes to treatment with several kinds of lipid-modifying reagents and examined the [3H]tryptamine binding capacities of the membranes by a radioreceptor-binding assay. [3H]Tryptamine binding was decreased by treatment with Azure A and phospholipase A2, while phospholipase D had no effect. All these observations led to the inference that PS and CS may be involved in the tryptamine binding activities as recognition sites.

摘要

通过葡聚糖LH20柱色谱法研究了硫苷脂(CS)、磷脂酰丝氨酸(PS)和磷脂酰肌醇(PI)在[3H]色胺与这些酸性脂质的各种重组组分结合中的可能作用。结果表明,PS、PS-CS、PS-PI和PS-CS-PI这四个系统对[3H]色胺具有相同的结合能力,而其他系统(CS、PI和CS-PI系统)没有结合能力。此外,竞争性抑制实验表明,在这四个重组系统中,PS-CS系统对5-甲氧基色胺表现出最高的亲和力。动力学研究表明,至少有两个结合成分(或位点)参与了[3H]色胺与PS和CS重组系统的结合,其表观解离常数KD值分别为3和10 nM。用各种化合物进行的置换研究表明,只有色胺和5-甲氧基色胺抑制[3H]色胺与该组分的结合,而其他吲哚胺类似物和神经递质则没有作用。此外,我们用几种脂质修饰试剂处理大鼠全脑突触质膜,并通过放射受体结合试验检测膜的[3H]色胺结合能力。用天青A和磷脂酶A2处理后,[3H]色胺结合减少,而磷脂酶D没有作用。所有这些观察结果得出推论,PS和CS可能作为识别位点参与色胺结合活性。

相似文献

1
[3H]tryptamine binding to reconstituted fraction of acidic lipids.[3H]色胺与酸性脂质重构组分的结合
J Pharmacobiodyn. 1987 Feb;10(2):78-84. doi: 10.1248/bpb1978.10.78.
2
[3H]5-hydroxytryptamine binding to reconstituted fraction with sulphatides, phosphatidylserine and phosphatidylinositol.[3H]5-羟色胺与含有硫脂、磷脂酰丝氨酸和磷脂酰肌醇的重组组分的结合。
Jpn J Pharmacol. 1985 Aug;38(4):411-7. doi: 10.1254/jjp.38.411.
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Butanol extracts from myelin fragments: tryptamine binding to lipid fractions.髓磷脂碎片的丁醇提取物:色胺与脂质部分的结合。
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Effect of phospholipase A2 on temperature-induced high-affinity [3H]tryptamine binding sites in rat brain.磷脂酶A2对大鼠脑中温度诱导的高亲和力[3H]色胺结合位点的影响。
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Butanol extracts from myelin fragments: identification of 5-hydroxytryptamine binding components.髓磷脂碎片的丁醇提取物:5-羟色胺结合成分的鉴定
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Glutaraldehyde pretreatment blocks temperature-induced high-affinity [3H]tryptamine binding.戊二醛预处理可阻断温度诱导的高亲和力[³H]色胺结合。
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Effects of protein-modifying reagents on brain tryptamine binding sites: possible involvement of a thiol group in temperature-induced high-affinity [3H]tryptamine binding sites.蛋白质修饰试剂对脑色胺结合位点的影响:巯基可能参与温度诱导的高亲和力[3H]色胺结合位点的形成。
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Implication of acidic lipids in 5-hydroxytryptamine receptor mechanisms.酸性脂质在5-羟色胺受体机制中的作用
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Temperature-sensitive high affinity [3H]tryptamine binding sites in rat brain.
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Characterization of [3H]tryptamine binding sites in brain.
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