Nicolson A, Toogood A A, Rahim A, Shalet S M
Department of Endocrinology, Christie Hospital, Manchester, UK.
Clin Endocrinol (Oxf). 1996 Mar;44(3):311-6. doi: 10.1046/j.1365-2265.1996.671492.x.
The few previous studies in which reassessment of GH status has been carried out in young adults treated with GH therapy for childhood GH deficiency concentrated on determining the incidence of 'transient GH deficiency'. As the benefits of GH replacement therapy in adults become increasingly appreciated, it is likely that GH therapy started in childhood for GH deficiency will be continued into adult life in many of those with severe GH deficiency. The aim of this study is to determine how many patients who received GH replacement therapy in childhood until completion of growth have GH deficiency severe enough to be considered for GH replacement therapy in adult life.
Retrospective analysis of the peak GH responses to provocative stimuli performed at the time of diagnosis of GH deficiency in childhood and at the completion of growth after GH replacement therapy had been stopped.
Eighty-eight adults (49 male, 39 female) who had received GH therapy in childhood for a diagnosis of GH deficiency. The aetiology of the GH deficiency included craniopharyngioma, radiation induced associated with either a cerebral tumour or acute lymphoblastic leukaemia, histiocytosis-X and idiopathic.
In childhood the original diagnosis of GH deficiency was based biochemically on the failure of the peak GH response to reach 20 mU/l during two provocative tests in 59 of the 88 patients and to a single test in the remaining 29. A total of 147 tests were performed, the most common being an insulin tolerance test (ITT, n = 72) and an arginine stimulation test (AST, n = 53). At reassessment in young adult life 146 tests were performed (74 ITT, 64 AST). Severe GH deficiency was defined arbitrarily as a peak GH response of less than 9 mU/l to a single (n = 33) or to two (n = 55) pharmacological stimuli.
By definition all patients were considered GH deficient at the time of initial diagnosis. A peak GH response of less than 9 mU/l was seen in 64.8% at initial assessment and 60.2% at reassessment. Analysis in aetiological terms, however, showed that between assessments the incidence of severe GH deficiency increased in the group of radiation induced (48.8 vs. 55.8%) but decreased in the idiopathic group (78.1 vs. 53.1%). Out of the 55 patients who underwent two tests at reassessment, 47.3% of those with a GH peak less than 9 mU/l at one test had a GH peak greater than 9 mU/l at the second test. Fifteen of the 55 patients had additional pituitary hormone deficiencies and all 15 had a GH peak below 9 mU/l in both tests.
Our study suggests that all children who have received GH replacement therapy in childhood should undergo reassessment of GH status in young adult life. Between 40 and 60% of such patients merit consideration for GH therapy in adult life depending on the definition of severe GH deficiency in use. Patients with isolated GH deficiency should undergo two provocative tests of GH secretion, but those with additional anterior pituitary hormone deficiencies require only one test at reassessment.
之前有少数研究对因儿童生长激素缺乏症接受生长激素治疗的年轻人进行了生长激素状态的重新评估,这些研究主要集中于确定“暂时性生长激素缺乏”的发生率。随着生长激素替代疗法在成人中的益处越来越受到重视,许多因生长激素缺乏症在儿童期开始接受生长激素治疗的患者很可能会在成年后继续接受该治疗。本研究的目的是确定有多少在儿童期接受生长激素替代治疗直至生长结束的患者,其生长激素缺乏严重到在成年后仍需考虑接受生长激素替代治疗。
对儿童期生长激素缺乏症诊断时以及生长激素替代治疗停止后生长结束时对刺激物的生长激素峰值反应进行回顾性分析。
88名成年人(49名男性,39名女性),他们在儿童期因生长激素缺乏症接受过生长激素治疗。生长激素缺乏的病因包括颅咽管瘤、与脑肿瘤或急性淋巴细胞白血病相关的辐射诱导、组织细胞增多症X和特发性。
在儿童期,88名患者中有59名通过生化检查,基于两次激发试验中生长激素峰值反应未达到20 mU/l,另外29名基于单次试验,做出了生长激素缺乏的初始诊断。共进行了147次试验,最常见的是胰岛素耐量试验(ITT,n = 72)和精氨酸刺激试验(AST,n = 53)。在成年后的重新评估中进行了146次试验(74次ITT,64次AST)。严重生长激素缺乏被任意定义为对单次(n = 33)或两次(n = 55)药物刺激的生长激素峰值反应低于9 mU/l。
根据定义,所有患者在初始诊断时都被认为存在生长激素缺乏。初始评估时64.8%的患者生长激素峰值反应低于9 mU/l,重新评估时为60.2%。然而,按病因分析显示,两次评估之间,辐射诱导组严重生长激素缺乏的发生率增加(48.8%对55.8%),而特发性组则下降(78.1%对53.1%)。在重新评估时接受两次试验的55名患者中,一次试验生长激素峰值低于9 mU/l的患者中有47.3%在第二次试验时生长激素峰值高于9 mU/l。55名患者中有1个有额外的垂体激素缺乏,所有15名患者在两次试验中生长激素峰值均低于9 mU/l。
我们的研究表明,所有在儿童期接受过生长激素替代治疗的儿童在成年后都应重新评估生长激素状态。根据所使用的严重生长激素缺乏的定义,这类患者中有40%至60%在成年后值得考虑接受生长激素治疗。孤立性生长激素缺乏的患者应进行两次生长激素分泌激发试验,但有额外垂体前叶激素缺乏的患者在重新评估时仅需进行一次试验。
