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使用促性腺激素释放激素的强效长效激动剂治疗性早熟。

Use of a potent, long acting agonist of gonadotropin-releasing hormone in the treatment of precocious puberty.

作者信息

Boepple P A, Mansfield M J, Wierman M E, Rudlin C R, Bode H H, Crigler J F, Crawford J D, Crowley W F

出版信息

Endocr Rev. 1986 Feb;7(1):24-33. doi: 10.1210/edrv-7-1-24.

DOI:10.1210/edrv-7-1-24
PMID:2937629
Abstract

Studies utilizing the administration of GnRH in various GnRH-deficient models have revealed the critical importance of the dose and mode of delivery of this releasing factor in determining the subsequent pituitary response. Chronic administration of long acting GnRH agonists (GnRHa), like continuous infusion of high doses of the native peptide, results in suppression of pituitary gonadotropin secretion. This selective and reversible suppression of gonadotropin secretion suggested several therapeutic applications for these analogs, particularly in the treatment of central precocious puberty (CPP), a disorder for which the previously available therapies lacked uniform efficacy and were associated with potential side effects. In our series, 74 children with CPP have been treated during the last 5 yr with the potent GnRH agonist, [D-Trp6, Pro9-ethylamide(NEt)]GnRH. Having selected a dose and route of administration that produced uniform suppression of spontaneous and stimulated pituitary gonadotropin secretion, GnRHa therapy resulted in a fall of gonadal sex steroid levels into the prepubertal range, a halting or regression of secondary sexual development, and a complete cessation of menses. Growth velocity slowed during therapy, with this slowing more pronounced during prolonged treatment periods and among those patients with more advanced chronological and skeletal ages. Skeletal maturation was retarded to a greater degree than linear growth, with resultant increases in the predictions for adult stature. Moreover, these benefits have been achieved in the absence of significant side effects. Complete reversal of the suppression of gonadarche has followed discontinuation of therapy; however, patterns of growth and skeletal maturation after discontinuation of GnRHa administration remain to be characterized. Thus, the impact of GnRHa therapy on final height must await further longitudinal study. The selective nature of GnRHa suppression of gonadarche also permits an investigation of the natural history of adrenarche and its discrete influences upon skeletal growth and maturation. In addition, GnRHa therapy of CPP provides a unique opportunity to study the effects of gonadal sex steroids on GH secretion and somatomedin-C (Sm-C) generation during sexual maturation. Finally, the detailed characterization of children with precocious puberty has helped to define more precisely a subset of patients whose precocity occurs in the absence of demonstrable gonadotropin secretion.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

在各种促性腺激素释放激素(GnRH)缺乏模型中使用GnRH进行的研究表明,这种释放因子的剂量和给药方式对于决定随后垂体的反应至关重要。长期给予长效GnRH激动剂(GnRHa),如持续输注高剂量的天然肽,会导致垂体促性腺激素分泌受到抑制。促性腺激素分泌的这种选择性和可逆性抑制提示了这些类似物的几种治疗应用,特别是在治疗中枢性性早熟(CPP)方面,此前可用的治疗方法缺乏一致的疗效且存在潜在的副作用。在我们的系列研究中,过去5年间有74例CPP患儿接受了强效GnRH激动剂[D-色氨酸6,脯氨酸9-乙酰胺(NEt)]GnRH的治疗。选择了能一致抑制自发性和刺激性垂体促性腺激素分泌的剂量和给药途径后,GnRHa治疗使性腺性甾体激素水平降至青春期前范围,第二性征发育停止或消退,月经完全停止。治疗期间生长速度减慢,在长期治疗期间以及那些实际年龄和骨龄较大的患者中这种减慢更为明显。骨骼成熟比线性生长受到更大程度的延迟,导致对成人身高的预测增加。此外,这些益处是在没有明显副作用的情况下实现的。停止治疗后,性腺初现的抑制作用完全逆转;然而,停止GnRHa给药后的生长和骨骼成熟模式仍有待确定。因此,GnRHa治疗对最终身高的影响必须等待进一步的纵向研究。GnRHa对性腺初现抑制的选择性性质也使得能够对肾上腺初现的自然史及其对骨骼生长和成熟的离散影响进行研究。此外,CPP的GnRHa治疗为研究性腺性甾体激素在性成熟过程中对生长激素分泌和生长调节素-C(Sm-C)生成的影响提供了独特的机会。最后,对性早熟儿童的详细特征描述有助于更精确地定义一组性早熟发生时无明显促性腺激素分泌的患者亚组。(摘要截取自400字)

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