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[合成阳离子肽对软体动物和大鼠肌肉组织中生物胺激活腺苷酸环化酶信号系统的影响]

[Effect of synthetic cationic peptides on activation of the adenylyl cyclase signaling system by biogenic amines in muscle tissue of molluscs and rats].

作者信息

Shpakov A O, Korol'kov V I, Vlasova E N, Afonina M P, Vlasov G P

机构信息

Institute of Macromolecular Compounds RAS, St. Petersburg.

出版信息

Tsitologiia. 2001;43(5):483-90.

PMID:11517665
Abstract

The hormone-sensitive adenylyl cyclase signaling system (ACS), made of serpentine receptor, heterotrimeric G-protein and enzyme adenylyl cyclase (AC), regulates a wide spectrum of growth and metabolic processes in the cell. Molecular mechanisms of functional coupling of ACS components still remain obscure. We examined the influence of synthetic cationic peptides Ac-Ala-His(Ala)2-His-Ala-NH2 (I), Ac-Ala-His-(Ala)3-His-(Ala)2-His-Ala-NH2 (II), and Ac-(Pro)2-His-(Ala)2-His-(Ala)3-His-(Ala)2-His-Ala-NH2 (III) on the basal AC activity and that stimulated by nonhormonal (NaF) and hormonal reagents (serotonin--molluscs, beta-isoproterenol--rats) in smooth muscles of the freshwater bivalve molluscs Anodonta cygnea and in skeletal muscles of rats. Peptides II and III (the latter more effective) were shown to decrease hormone-stimulated AC activity in both tissues, in a dose-dependent manner. Peptide III strongly reduced NaF stimulating effect to AC, which suggests the involvement of this peptide in the functional coupling of both receptors with G-proteins, and of G-proteins with AC. A correlation was found between the efficacy of peptide action on the functional activity of ACS components and peptide length. As shown by IR-spectroscopy, in water all peptides can form helical structures. However, alpha-helicity of peptides I and II was higher than that of peptide III, which does not conform to a power series in efficacy of these peptides. Thus, it is the length of cationic peptides that plays a key role in hormonal regulation of the functional activity of ACS, especially on the step of receptor-G-protein coupling.

摘要

由蛇形受体、异源三聚体G蛋白和腺苷酸环化酶(AC)组成的激素敏感性腺苷酸环化酶信号系统(ACS),调节细胞内广泛的生长和代谢过程。ACS各组分功能偶联的分子机制仍不清楚。我们研究了合成阳离子肽Ac-Ala-His(Ala)2-His-Ala-NH2(I)、Ac-Ala-His-(Ala)3-His-(Ala)2-His-Ala-NH2(II)和Ac-(Pro)2-His-(Ala)2-His-(Ala)3-His-(Ala)2-His-Ala-NH2(III)对淡水双壳贝类河蚬平滑肌和大鼠骨骼肌中基础AC活性以及由非激素试剂(NaF)和激素试剂(5-羟色胺——软体动物,β-异丙肾上腺素——大鼠)刺激的AC活性的影响。结果显示,肽II和III(后者更有效)能以剂量依赖的方式降低两种组织中激素刺激的AC活性。肽III强烈降低NaF对AC的刺激作用,这表明该肽参与了受体与G蛋白以及G蛋白与AC的功能偶联。发现肽对ACS组分功能活性的作用效果与肽长度之间存在相关性。红外光谱显示,在水中所有肽都能形成螺旋结构。然而,肽I和II的α-螺旋度高于肽III,这与这些肽的功效幂级数不符。因此,阳离子肽的长度在ACS功能活性的激素调节中起关键作用,尤其是在受体-G蛋白偶联步骤中。

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Molecular mechanisms of interaction of polycationic peptides with G proteins.
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2
Inhibition of the hormonal stimulation of the functional activity of the adenylate cyclase signaling system by synthetic cationic peptides.
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