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γ-促黑素/促肾上腺皮质激素样肽对大鼠脑血流动力学影响的构效分析

Structure-activity analysis for the effects of gamma-MSH/ACTH-like peptides on cerebral hemodynamics in rats.

作者信息

Van Bergen P, Van Der Vaart J G, Kasbergen C M, Versteeg D H, De Wildt D J

机构信息

Department of Medical Pharmacology, Rudolf Magnus Institute for Neurosciences, Utrecht University, Netherlands.

出版信息

Eur J Pharmacol. 1996 Dec 30;318(2-3):357-68. doi: 10.1016/s0014-2999(96)00806-0.

Abstract

In a previous structure-activity analysis we have shown that the gamma-melanocyte-stimulating hormones (gamma-MSHs) and structurally related adrenocorticotropic hormone (ACTH) fragments share an amino-acid sequence which is determinant for the effects of these peptides on peripheral hemodynamics, viz. a pressor and a tachycardiac response, in conscious rats. We now investigated whether these structural features are also important for the effects of these peptides on cerebral hemodynamics in urethane-anesthetized rats. After intracarotid and intravenous administration, the 'mother' peptides, Lys-gamma2-MSH and gamma2-MSH, and, with a 10-fold lower potency, ACTH-(4-10), caused a dose-dependent pressor and tachycardiac response, as well as an increase in extra- and intracranial blood flow and microcirculatory cerebrocortical blood flow. Removal of C-terminal amino acids resulted in gamma-MSH-fragments which were devoid of effects on peripheral and central hemodynamics. Fragments of gamma2-MSH which were shortened at the N-terminal side (gamma-MSH-(4-12) and gamma-MSH-(5-12)) were less potent than gamma2-MSH, but had an intrinsic activity similar to that of gamma2-MSH with respect to the pressor and tachycardiac effect. However, the potency and intrinsic activity of these shortened fragments on intracerebral hemodynamic parameters were the same as those of gamma2-MSH. This suggests that different mechanisms (e.g., site of action and/or melanocortin receptor subtype) are involved in the cerebral hemodynamic effects of the melanocortins and in their peripheral hemodynamic effects. Surprisingly, removal of an additional residue, His5, resulting in the fragment gamma-MSH-(6-12), led to full restoration of potency with respect to extracranial blood flow, blood pressure and heart rate. Neither the structurally related analog, [Nle4,D-Phe7]alpha-MSH (NDP-MSH), nor ACTH-(1-24) was able to induce a pressor effect or cerebral hemodynamic effects. In contrast, both compounds had a depressor effect. It is concluded that the C-terminal amino acids in the structure of gamma-MSH/ACTH-like peptides are essential for efficacy for the central hemodynamic effects, i.e., the increase in intracerebral (microcirculatory) blood flow. However, in contrast to what holds for the peripheral hemodynamic features, the N-terminal sequence has hardly any influence on potency or efficacy. The results with NDP-MSH and ACTH-(1-24) and the other fragments lead us to postulate that it is not one of the five known subtypes of melanocortin receptors which mediates the hemodynamic effects of the melanocortins, but an additional, still unidentified subtype. A clue for the elucidation of such a receptor might be found in the structural features of gamma-MSH-(6-12) that appear to be very important determinants for the effectiveness to alter peripheral and central hemodynamics.

摘要

在先前的构效关系分析中,我们已经表明,γ-促黑素(γ-MSHs)以及结构相关的促肾上腺皮质激素(ACTH)片段共享一个氨基酸序列,该序列决定了这些肽对清醒大鼠外周血流动力学的影响,即升压和心动过速反应。我们现在研究这些结构特征对于这些肽对氨基甲酸乙酯麻醉大鼠脑血流动力学的影响是否也很重要。在颈内动脉和静脉给药后,“母”肽Lys-γ2-MSH和γ2-MSH,以及效力低10倍的ACTH-(4 - 十),引起剂量依赖性的升压和心动过速反应,以及颅外和颅内血流量和脑皮质微循环血流量增加。去除C末端氨基酸会产生对外周和中枢血流动力学无影响的γ-MSH片段。在N末端缩短的γ2-MSH片段(γ-MSH-(4 - 12)和γ-MSH-(5 - 12))的效力低于γ2-MSH,但在升压和心动过速作用方面具有与γ2-MSH相似的内在活性。然而,这些缩短片段对脑血流动力学参数的效力和内在活性与γ2-MSH相同。这表明不同的机制(例如,作用部位和/或黑皮质素受体亚型)参与了黑皮质素的脑血流动力学效应及其外周血流动力学效应。令人惊讶的是,去除额外的残基His5,产生片段γ-MSH-(6 - 12),导致在颅外血流量、血压和心率方面效力完全恢复。结构相关类似物[Nle4,D-Phe7]α-MSH(NDP-MSH)和ACTH-(1 - 24)均不能诱导升压效应或脑血流动力学效应。相反,这两种化合物都有降压作用。结论是,γ-MSH/ACTH样肽结构中的C末端氨基酸对于中枢血流动力学效应(即脑内(微循环)血流量增加)的效力至关重要。然而,与外周血流动力学特征不同,N末端序列对效力或功效几乎没有影响。NDP-MSH和ACTH-(1 - 24)以及其他片段的结果使我们推测,介导黑皮质素血流动力学效应的不是五种已知的黑皮质素受体亚型之一,而是一种额外的、尚未确定的亚型。在γ-MSH-(6 - 12)的结构特征中可能找到阐明这种受体的线索,这些特征似乎是改变外周和中枢血流动力学有效性的非常重要的决定因素。

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