Camanni F, Ghigo E, Arvat E
Department of Internal Medicine, University of Turin, Italy.
Front Neuroendocrinol. 1998 Jan;19(1):47-72. doi: 10.1006/frne.1997.0158.
Growth hormone-releasing peptides (GHRPs) are a series of hepta (GHRP-1)- and hexapeptides (GHRP-2, GHRP-6, Hexarelin) that have been shown to be effective releasers of GH in animals and humans. More recently, a series of nonpeptidyl GH secretagogues (L-692,429, L-692,585, MK-0677) were discovered using GHRP-6 as a template. Some cyclic peptides as well as penta-, tetra-, and pseudotripeptides have also been described. This review summarizes recent developments in our understanding of the GHRPs, as well as the current nonpeptide pharmacologic analogs. GHRPs and their analogs have no structural homology with GHRH and act via specific receptors present at either the pituitary or the hypothalamic level. The GHRP receptor has recently been cloned and it does not show sequence homology with other G-protein-coupled receptors known so far. This evidence strongly suggests the existence of a natural GHRP-like ligand which, however, has not yet been found. Although the exact mechanism of action of GHRPs has not been fully established, there is probably a dual site of action on both the pituitary and the hypothalamus, possibly involving regulatory factors in addition to GHRH and somatostatin. Moreover, the possibility that GHRPs act via an unknown hypothalamic factor (U factor) is still open. The marked GH-releasing activity of GHRPs is reproducible and dose-related after intravenous, subcutaneous, intranasal, and even oral administration. The GH-releasing effect of GHRPs is the same in both sexes, but undergoes age-related variations. It increases from birth to puberty and decreases in aging. The GH-releasing activity of GHRPs is synergistic with that of GHRH and not affected by opioid receptor antagonists, while it is only blunted by inhibitory influences that are known to nearly abolish the effect of GHRH, such as neurotransmitters, glucose, free fatty acids, glucocorticoids, rhGH, and even exogenous somatostatin. GHRPs maintain their GH-releasing effect in somatotrope hypersecretory states, such as acromegaly, anorexia nervosa, and hyperthyroidism. On the other hand, GHRPs and their analogs have been reported to be effective in idiopathic short stature, in some situations of GH deficiency, in obesity, and in hypothyroidism, while in patients with pituitary stalk disconnection and in Cushing's syndrome the somatotrope responsiveness to GHRPs is almost absent. A potential role in the treatment of short stature, aging, catabolic states, and dilated cardiomyopathy has been envisaged.
生长激素释放肽(GHRPs)是一系列七肽(GHRP-1)和六肽(GHRP-2、GHRP-6、Hexarelin),已被证明在动物和人类中是有效的生长激素释放剂。最近,以GHRP-6为模板发现了一系列非肽类生长激素促分泌素(L-692,429、L-692,585、MK-0677)。还描述了一些环肽以及五肽、四肽和假三肽。本综述总结了我们对GHRPs以及当前非肽类药理学类似物认识的最新进展。GHRPs及其类似物与生长激素释放激素(GHRH)没有结构同源性,通过垂体或下丘脑水平存在的特异性受体发挥作用。GHRP受体最近已被克隆,它与迄今为止已知的其他G蛋白偶联受体没有序列同源性。这一证据强烈表明存在一种天然的GHRP样配体,然而,尚未找到。尽管GHRPs的确切作用机制尚未完全明确,但可能在垂体和下丘脑都有作用位点,可能除了GHRH和生长抑素外还涉及调节因子。此外,GHRPs通过一种未知下丘脑因子(U因子)发挥作用的可能性仍然存在。GHRPs显著的生长激素释放活性在静脉内、皮下、鼻内甚至口服给药后都是可重复的且与剂量相关。GHRPs的生长激素释放作用在两性中相同,但存在与年龄相关的变化。从出生到青春期增加,在衰老过程中减少。GHRPs的生长激素释放活性与GHRH的活性具有协同作用,不受阿片受体拮抗剂的影响,而只有已知几乎能消除GHRH作用的抑制性影响(如神经递质、葡萄糖、游离脂肪酸、糖皮质激素、重组人生长激素,甚至外源性生长抑素)才能使其减弱。GHRPs在生长激素分泌过多状态(如肢端肥大症、神经性厌食症和甲状腺功能亢进症)中维持其生长激素释放作用。另一方面,据报道GHRPs及其类似物在特发性身材矮小、某些生长激素缺乏情况、肥胖症和甲状腺功能减退症中有效,而在垂体柄离断患者和库欣综合征患者中,生长激素细胞对GHRPs的反应性几乎不存在。已经设想了其在治疗身材矮小、衰老、分解代谢状态和扩张型心肌病方面的潜在作用。
