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血红素肽可能是脑血管紧张素AT4受体的内源性配体。

Haemorphin peptides may be endogenous ligands for brain angiotensin AT4 receptors.

作者信息

Moeller I, Chai S Y, Smith I, Lew R, Mendelsohn F A

机构信息

Howard Florey Institute of Experimental Physiology and Medicine, University of Melbourne, Parkville, Victoria, Australia.

出版信息

Clin Exp Pharmacol Physiol Suppl. 1998 Nov;25:S68-71. doi: 10.1111/j.1440-1681.1998.tb02304.x.

DOI:10.1111/j.1440-1681.1998.tb02304.x
PMID:9809196
Abstract
  1. Angiotensin IV (AngIV), the (3-8) fragment of AngII, was previously believed to be an inactive metabolite. However, specific binding sites, termed AT4 receptors, have been identified in the brain and peripheral organs and the peptide has been reported to enhance memory recall in passive avoidance studies and to dilate pial and renal cortical vessels. 2. AT4 receptors are distinct from AngII AT1 and AT2 receptors with respect to function, ligand specificity and distribution. 3. In the brain, AT4 receptors are abundant in cerebral and cerebellar cortex, hippocampal formation and cholinergic systems, as well as sensory and motor systems. However, the peptide AngIV is low or undetectable in the central nervous system. This led us to search for an alternative peptide ligand of the AT4 receptor. 4. The decapeptide LVVYPWTQRF was isolated from cerebral cortex and binds with high affinity to brain AT4 receptors. This peptide sequence corresponds to an internal sequence of beta-globin and has previously been named LVV-haemorphin 7. 5. Haemorphin may represent a new class of endogenous neuropeptides, some of which interact potently with the brain AT4 receptor to elicit a range of actions.
摘要
  1. 血管紧张素IV(AngIV)是血管紧张素II的(3 - 8)片段,以前被认为是一种无活性的代谢产物。然而,在大脑和外周器官中已鉴定出特定的结合位点,称为AT4受体,并且据报道该肽在被动回避研究中可增强记忆回忆,并能扩张软脑膜和肾皮质血管。2. AT4受体在功能、配体特异性和分布方面与血管紧张素II的AT1和AT2受体不同。3. 在大脑中,AT4受体在大脑皮质、小脑皮质、海马结构和胆碱能系统以及感觉和运动系统中大量存在。然而,肽AngIV在中枢神经系统中含量很低或无法检测到。这促使我们寻找AT4受体的替代肽配体。4. 十肽LVVYPWTQRF是从大脑皮质中分离出来的,它与大脑AT4受体具有高亲和力结合。该肽序列对应于β-珠蛋白的内部序列,以前被命名为LVV-血啡肽7。5. 血啡肽可能代表一类新的内源性神经肽,其中一些与大脑AT4受体强烈相互作用以引发一系列作用。

相似文献

1
Haemorphin peptides may be endogenous ligands for brain angiotensin AT4 receptors.血红素肽可能是脑血管紧张素AT4受体的内源性配体。
Clin Exp Pharmacol Physiol Suppl. 1998 Nov;25:S68-71. doi: 10.1111/j.1440-1681.1998.tb02304.x.
2
The globin fragment LVV-hemorphin-7 is an endogenous ligand for the AT4 receptor in the brain.珠蛋白片段LVV-血啡肽-7是大脑中AT4受体的内源性配体。
J Neurochem. 1997 Jun;68(6):2530-7. doi: 10.1046/j.1471-4159.1997.68062530.x.
3
Autoradiographic identification of kidney angiotensin IV binding sites and angiotensin IV-induced renal cortical blood flow changes in rats.大鼠肾脏血管紧张素IV结合位点的放射自显影鉴定及血管紧张素IV诱导的肾皮质血流变化
Peptides. 1998;19(2):269-77. doi: 10.1016/s0196-9781(97)00291-x.
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Distribution of AT4 receptors in the Macaca fascicularis brain.
Brain Res. 1996 Mar 18;712(2):307-24. doi: 10.1016/0006-8993(95)01482-9.
5
A globin fragment, LVV-hemorphin-7, induces [3H]thymidine incorporation in a neuronal cell line via the AT4 receptor.一种珠蛋白片段,LVV-血啡肽-7,通过AT4受体诱导神经元细胞系中[3H]胸苷掺入。
J Neurochem. 1999 Jul;73(1):301-8. doi: 10.1046/j.1471-4159.1999.0730301.x.
6
Angiotensin II- and IV-induced changes in cerebral blood flow. Roles of AT1, AT2, and AT4 receptor subtypes.血管紧张素II和IV诱导的脑血流变化。AT1、AT2和AT4受体亚型的作用。
Regul Pept. 1997 Jan 29;68(2):131-8. doi: 10.1016/s0167-0115(96)02116-7.
7
Effect of I.C.V. injection of AT4 receptor ligands, NLE1-angiotensin IV and LVV-hemorphin 7, on spatial learning in rats.脑室内注射AT4受体配体NLE1 - 血管紧张素IV和LVV - 血啡肽7对大鼠空间学习的影响。
Neuroscience. 2004;124(2):341-9. doi: 10.1016/j.neuroscience.2003.12.006.
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Autoradiographic identification of brain angiotensin IV binding sites and differential c-Fos expression following intracerebroventricular injection of angiotensin II and IV in rats.
Brain Res. 1995 Jun 5;682(1-2):13-21. doi: 10.1016/0006-8993(95)00289-3.
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Angiotensin AT4 ligands are potent, competitive inhibitors of insulin regulated aminopeptidase (IRAP).血管紧张素AT4配体是胰岛素调节氨肽酶(IRAP)的强效竞争性抑制剂。
J Neurochem. 2003 Jul;86(2):344-50. doi: 10.1046/j.1471-4159.2003.01852.x.
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Distribution of angiotensin IV binding sites (AT4 receptor) in the human forebrain, midbrain and pons as visualised by in vitro receptor autoradiography.
J Chem Neuroanat. 2000 Dec;20(3-4):339-48. doi: 10.1016/s0891-0618(00)00112-5.

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