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大鼠脊髓中¹²⁵I-博尔顿-亨特标记的P物质结合位点的表征及节段分布

Characterization and segmental distribution of 125I-Bolton-Hunter-labeled substance P binding sites in rat spinal cord.

作者信息

Charlton C G, Helke C J

出版信息

J Neurosci. 1985 May;5(5):1293-9. doi: 10.1523/JNEUROSCI.05-05-01293.1985.

Abstract

Substance P (SP) is widely distributed in the spinal cord and has been implicated as a neurotransmitter in several spinal cord neuronal systems. To investigate SP receptors in the spinal cord, 125I-Bolton-Hunter-SP (125I-BH-SP) was used to identify and characterize spinal cord binding sites for the peptide. The binding of 125I-BH-SP had the following characteristics: high affinity; time, temperature, and membrane concentration dependent; reversible; and saturable. The IC50 of SP in whole spinal cord was 0.46 nM as compared with 0.95, 60, and 150 nM for physalaemin, eledoisin, and kassinin. Four putative antagonists of SP were less than 0.0001 times as potent as SP in inhibiting 125I-BH-SP binding. IC50s were 5, 7.5, 7.0, and 45 microM for D-Pro2, D-Trp7,9-SP; D-Pro2, D-Phe7, D-Trp9-SP; D-Arg1, D-Pro2, D-Trp7,9, Leu11-SP; and D-Pro4, D-Trp7,9,10-SP(4-11), respectively. The lumbosacral section bound 3 times more SP than the cervical and thoracic sections, although IC50 for the cervical section was 0.06 of that for the lumbosacral and thoracic sections. The data suggest more than one class of binding site for SP in the spinal cord and indicate a direct role for SP in spinal cord functions.

摘要

P物质(SP)广泛分布于脊髓,并在多个脊髓神经元系统中被认为是一种神经递质。为了研究脊髓中的SP受体,使用125I-博尔顿-亨特-SP(125I-BH-SP)来识别和表征该肽在脊髓中的结合位点。125I-BH-SP的结合具有以下特点:高亲和力;依赖时间、温度和膜浓度;可逆;可饱和。与催唾肽、蛙皮素和十肽胃泌素相比,SP在整个脊髓中的IC50为0.46 nM,而催唾肽、蛙皮素和十肽胃泌素的IC50分别为0.95、60和150 nM。四种假定的SP拮抗剂在抑制125I-BH-SP结合方面的效力比SP低0.0001倍以下。D-脯氨酸2、D-色氨酸7,9-SP;D-脯氨酸2、D-苯丙氨酸7、D-色氨酸9-SP;D-精氨酸1、D-脯氨酸2、D-色氨酸7,9、亮氨酸11-SP;以及D-脯氨酸4、D-色氨酸7,9,10-SP(4-11)的IC50分别为5、7.5、7.0和45 microM。腰骶部结合的SP比颈部和胸部多3倍,尽管颈部的IC50是腰骶部和胸部的0.06倍。数据表明脊髓中存在不止一类SP结合位点,并表明SP在脊髓功能中起直接作用。

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