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在月经周期正常的女性中,六元瑞林是一种比生长激素释放激素更强的生长激素释放肽,但在神经性厌食症患者中并非如此。

Hexarelin is a stronger GH-releasing peptide than GHRH in normal cycling women but not in anorexia nervosa.

作者信息

Giusti M, Foppiani L, Ponzani P, Cuttica C M, Falivene M R, Valenti S

机构信息

DISEM, Cattedra di Endocrinologia, University of Genova, Italy.

出版信息

J Endocrinol Invest. 1997 May;20(5):257-63. doi: 10.1007/BF03350297.

Abstract

Anorexia nervosa (AN) is a chronic disease in which an enhanced GH response to GHRH, a paradoxic increase after TRH and LHRH, and low IGF1 levels may be present according to the patient's clinical state. It is well known that the GH hypersecretory state commonly found in the "acute phase" of AN is restored with weight gain. The new synthetic hexapeptide, Hexarelin (HEX), which is chemically similar to GH-releasing peptide 6, has recently been shown to possess a stronger GH-releasing activity than GHRH in humans and to share a synergistic effect with GHRH when administered intravenously. Indeed, HEX shows a slight cortisol and PRL-releasing activity. The aim of the study was to evaluate the effect of i.v. administration of old (GHRH) and new (HEX) GH-releasing peptides on GH, PRL and cortisol secretion in 9 AN patients in the "recovery phase" of the disease, after partial but significant weight gain. For controls we studied 7 normal cycling women. No significant difference in GH secretion after GHRH was found between AN and controls. GHRH was not able to release cortisol or PRL either in AN or controls. HEX produced a significantly (p < 0.05) higher GH peak in controls than in AN, while GH AUC was slightly but not significantly higher. Indeed, only in controls, HEX was a stronger GH-releasing peptide than GHRH. These findings could be explained by the fact that, in AN, GH secretion is already stimulated both by reduced IGF1 levels and by increased GHRH/somatostatin ratio. As reported in the literature, the action of HEX action is only slightly influenced by variations in somatostatin tone. It therefore appears likely that the absolute or relative GHRH increase present in AN could partially mimic the unknown hypothalamic factor necessary for HEX action on the hypophisis and that, following a structural modification of pituitary HEX receptors, GHRH would become able to bind to HEX receptors on somatotropic cells. Consequently, the pituitary cells would already be over-activated and so unable to respond maximally to HEX stimulation. Indeed, in AN, GHRH might play a role of negative modulation in the control of HEX action. Finally, in our study HEX was able to produce a persistent PRL release in controls but not in AN, thus suggesting that its action could be partially dependent on the estrogen milieu, while it stimulated cortisol secretion only transiently in the patients studied.

摘要

神经性厌食症(AN)是一种慢性疾病,根据患者的临床状态,可能存在生长激素(GH)对生长激素释放激素(GHRH)反应增强、促甲状腺激素释放激素(TRH)和促黄体生成素释放激素(LHRH)后出现反常增加以及胰岛素样生长因子1(IGF1)水平降低的情况。众所周知,AN“急性期”常见的GH分泌亢进状态会随着体重增加而恢复。新型合成六肽Hexarelin(HEX)在化学结构上与生长激素释放肽6相似,最近的研究表明,在人体中,它具有比GHRH更强的GH释放活性,静脉注射时与GHRH具有协同作用。实际上,HEX还具有轻微的皮质醇和催乳素(PRL)释放活性。本研究旨在评估静脉注射旧的(GHRH)和新的(HEX)GH释放肽对9例处于疾病“康复期”且体重已有部分但显著增加的AN患者的GH、PRL和皮质醇分泌的影响。作为对照,我们研究了7名正常月经周期的女性。AN患者和对照组在注射GHRH后GH分泌无显著差异。GHRH在AN患者和对照组中均不能释放皮质醇或PRL。与AN患者相比,HEX在对照组中产生的GH峰值显著更高(p<0.05),而GH曲线下面积(AUC)虽略高但无显著差异。实际上,仅在对照组中,HEX是比GHRH更强的GH释放肽。这些发现可以解释为,在AN患者中,IGF1水平降低和GHRH/生长抑素比值增加均已刺激了GH分泌。正如文献报道,HEX的作用仅受生长抑素水平变化的轻微影响。因此,AN患者中存在的GHRH绝对或相对增加可能部分模拟了HEX作用于垂体所需的未知下丘脑因子,并且在垂体HEX受体发生结构改变后,GHRH将能够与促生长细胞上的HEX受体结合。因此,垂体细胞可能已经过度激活,从而无法对HEX刺激产生最大反应。实际上,在AN患者中,GHRH可能在控制HEX作用方面发挥负调节作用。最后,在我们的研究中,HEX能够在对照组中产生持续的PRL释放,但在AN患者中则不能,这表明其作用可能部分依赖于雌激素环境,而在我们研究的患者中,它仅短暂刺激了皮质醇分泌。

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