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神经降压素8 - 13类似物Asp13 - NT8 - 13和Asp12 - NT8 - 13对肥大细胞分泌的抑制作用。

Inhibitory effects of the neurotensin8-13 analogs Asp13-NT8-13 and Asp12-NT8-13 on mast cell secretion.

作者信息

Miller L A, Cochrane D E, Carraway R E, Feldberg R S

机构信息

Tufts University, Medford, MA 02155.

出版信息

Agents Actions. 1993 Jan;38(1-2):1-7. doi: 10.1007/BF02027206.

DOI:10.1007/BF02027206
PMID:7683173
Abstract

Pretreatment of isolated mast cells with analogs of neurotensin 8-13 (NT8-13), in which the amino acids Leu13 or Ile12 are replaced with an aspartic acid (Asp13-NT8-13 or Asp12-NT8-13), inhibits the secretion of histamine in response to NT. A 10 min pretreatment with either analog (10 microM) inhibited NT-induced histamine release by 90% (Asp13-NT8-13) or by 98% (Asp12-NT8-13). At concentrations that are inhibitory, Asp13-NT8-13 and Asp12-NT8-13 alone elicit very little release (< 5% at 10 microM). In the continued presence of the analogs, the inhibitory effect lasts for more than 45 min; removal of the analogs resulted in restoration of sensitivity to NT within 10 min. Pretreatment with analog Asp13-NT8-13 resulted in a 39% inhibition of stimulation by substance P and a 52% inhibition of stimulation by histamine-releasing peptide (HRP). In contrast, pretreatment with analog Asp12-NT8-13 gave no inhibition of release by SP or HRP. Neither analog inhibited histamine release in response to bradykinin (BK), NT1-12, compound 48/80 (48/80), the calcium ionophore A23187, or anti-IgE stimulation of passively sensitized mast cells. Although Asp12-NT8-13 and Asp13-NT8-13 differ slightly in regard to the peptides they inhibit, both probably act at a step early in the stimulus-secretion coupling sequence; most likely before the rise in the level of free intracellular calcium that has been shown to accompany secretion in mast cells. It is suggested that these analogs exert their inhibitory effect on NT by competing with NT for a binding site on the mast cell membrane.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

用神经降压素8 - 13(NT8 - 13)类似物预处理分离的肥大细胞,其中亮氨酸13或异亮氨酸12被天冬氨酸取代(Asp13 - NT8 - 13或Asp12 - NT8 - 13),可抑制肥大细胞对神经降压素(NT)产生的组胺分泌。用任一类似物(10微摩尔)进行10分钟预处理,可使NT诱导的组胺释放抑制90%(Asp13 - NT8 - 13)或98%(Asp12 - NT8 - 13)。在具有抑制作用的浓度下,单独的Asp13 - NT8 - 13和Asp12 - NT8 - 13引起的释放非常少(10微摩尔时<5%)。在持续存在类似物的情况下,抑制作用持续超过45分钟;去除类似物后,10分钟内对NT的敏感性恢复。用类似物Asp13 - NT8 - 13预处理可使P物质刺激引起的组胺释放抑制39%,组胺释放肽(HRP)刺激引起的组胺释放抑制52%。相反,用类似物Asp12 - NT8 - 13预处理对P物质或HRP引起的组胺释放无抑制作用。两种类似物均不抑制缓激肽(BK)、NT1 - 12、化合物48/80(48/80)、钙离子载体A23187或被动致敏肥大细胞的抗IgE刺激所引起的组胺释放。尽管Asp12 - NT8 - 13和Asp13 - NT8 - 13在它们所抑制的肽方面略有不同,但两者可能都作用于刺激 - 分泌偶联序列的早期步骤;很可能在已证明与肥大细胞分泌相伴发生的细胞内游离钙水平升高之前。提示这些类似物通过与NT竞争肥大细胞膜上的结合位点而对NT发挥抑制作用。(摘要截短于250字)

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引用本文的文献

1
Blockade of mast cell histamine secretion in response to neurotensin by SR 48692, a nonpeptide antagonist of the neurotensin brain receptor.通过神经降压素脑受体的非肽拮抗剂SR 48692对肥大细胞组胺分泌的反应进行阻断,该反应是针对神经降压素的。
Br J Pharmacol. 1995 Apr;114(7):1466-70. doi: 10.1111/j.1476-5381.1995.tb13371.x.

本文引用的文献

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