Rogol Alan D, Blethen Sandra L, Sy Judy P, Veldhuis Johannes D
Genentech, Inc, South San Francisco, CA.
Clin Endocrinol (Oxf). 2003 Feb;58(2):229-37. doi: 10.1046/j.1365-2265.2003.01701.x.
To compare the relative utility of GH secretion via pharmacological stimulation, overnight serial sampling, IGF-I levels and auxological variables as predictors of change in height standard deviation score (deltaHt SDS) during GH treatment.
A multicentre observational study.
Prepubertal children (n = 825) with idiopathic growth failure who were subsequently treated with GH were divided into two groups, based on their maximum GH response to pharmacological stimulation testing: (1) idiopathic GH deficiency (IGHD), defined by a maximum GH response < 10 microg/l (n = 300); and (2) idiopathic short stature (ISS), with a maximum GH response > or = 10 microg/l (n = 525) (GH conversion factor: 3 IU = 1 mg).
Overnight spontaneous GH secretion was measured in all patients. The following characteristics of spontaneous GH secretion were studied: maximum or peak GH, mean peak GH, number of GH peaks, pooled GH, mean GH, and approximate entropy of GH secretion.
Although children with IGHD had lower indices of spontaneous GH secretion, there were no differences between IGHD and ISS groups in baseline Ht SDS, growth rate or IGF-I level. The dose and duration of GH therapy were similar. There was no statistically significant difference in the mean (+/- SD) change in Ht SDS (deltaHt SDS) in the two groups (IGHD 1.3 +/- 0.9 and ISS 1.2 +/- 0.8). Measures of spontaneous secretion, such as peak GH, mean of GH peaks, mean area under GH peaks, and mean GH, as well as IGF-I concentrations, were all statistically significantly correlated with deltaHt SDS in IGHD children (P < 0.0001). A significant correlation was also observed for pooled GH (P = 0.002) and approximate entropy (P = 0.01). Children with the most severe ISS (Ht SDS < -3.33) demonstrated a more disorganized pattern of GH secretion compared to children who were not as short (Ht SDS -2.33 to -1.64), as indicated by a higher approximate entropy (0.673 +/- 0.193 vs. 0.607 +/- 0.161, P < 0.004). This increased disorder in GH secretion was accompanied by lower IGF-I levels (104 +/- 99 microg/l vs. 137 +/- 74 microg/l, P < 0.001), even though pooled GH concentrations were indistinguishable between the two groups (2.2 +/- 1.3 microg/l vs. 2.0 +/- 1.0 microg/l). Children with IGHD demonstrated lower approximate entropy than did those with ISS (0.551 +/- 0.235 vs. 0.631 +/- 0.182, P < 0.0001). Duration of GH treatment, height deficit and genetic potential (midparental Ht SDS) were the most important variables influencing deltaHt SDS in children receiving GH therapy. Maximum stimulated GH, IGF-I and indices of spontaneous GH secretion also correlated with deltaHt SDS, but their relative importance varied among diagnostic groups.
Patients with GH deficiency demonstrate a reduced capacity for GH secretion, while those with idiopathic short stature exhibit a more disorderly and less functional secretory pattern. Although effective in predicting a response to GH treatment in patients with severe GH deficiency, overnight serial sampling is less practical than other methods currently available. In addition, serial sampling was less useful as a predictor of growth response to exogenous GH in patients with idiopathic short stature.
比较通过药物刺激的生长激素(GH)分泌、夜间连续采样、胰岛素样生长因子-I(IGF-I)水平及体格学变量作为GH治疗期间身高标准差评分变化(ΔHt SDS)预测指标的相对效用。
一项多中心观察性研究。
825例特发性生长障碍的青春期前儿童,随后接受GH治疗,根据其对药物刺激试验的最大GH反应分为两组:(1)特发性GH缺乏(IGHD),定义为最大GH反应<10μg/L(n = 300);(2)特发性身材矮小(ISS),最大GH反应≥10μg/L(n = 525)(GH转换因子:3IU = 1mg)。
对所有患者测量夜间自发性GH分泌。研究自发性GH分泌的以下特征:最大或峰值GH、平均峰值GH、GH峰值数量、总GH、平均GH以及GH分泌的近似熵。
尽管IGHD儿童的自发性GH分泌指标较低,但IGHD组和ISS组在基线身高标准差评分、生长速率或IGF-I水平方面无差异。GH治疗的剂量和持续时间相似。两组的身高标准差评分平均变化(ΔHt SDS)(±标准差)无统计学显著差异(IGHD组为1.3±0.9,ISS组为1.2±0.8)。在IGHD儿童中,自发性分泌指标,如峰值GH、GH峰值均值、GH峰值下平均面积、平均GH以及IGF-I浓度,均与ΔHt SDS呈统计学显著相关(P<0.0001)。总GH(P = 0.002)和近似熵(P = 0.01)也观察到显著相关性。与身高不是很矮的儿童(身高标准差评分-2.33至-1.64)相比,最严重的ISS儿童(身高标准差评分<-3.33)的GH分泌模式更紊乱,表现为近似熵更高(0.673±0.193对0.607±0.161,P<0.004)。尽管两组的总GH浓度无差异(2.2±1.3μg/L对2.0±1.0μg/L),但这种GH分泌紊乱增加伴随着较低的IGF-I水平(104±99μg/L对137±74μg/L,P<0.001)。IGHD儿童的近似熵低于ISS儿童(0.551±0.235对0.631±0.182,P<0.0001)。GH治疗持续时间、身高缺陷和遗传潜力(父母平均身高标准差评分)是影响接受GH治疗儿童ΔHt SDS的最重要变量。最大刺激GH、IGF-I和自发性GH分泌指标也与ΔHt SDS相关,但其相对重要性在不同诊断组中有所不同。
GH缺乏患者的GH分泌能力降低,而特发性身材矮小患者表现出更紊乱且功能较差的分泌模式。尽管夜间连续采样对预测严重GH缺乏患者对GH治疗的反应有效,但它不如目前可用的其他方法实用。此外,连续采样作为特发性身材矮小患者对外源性GH生长反应的预测指标不太有用。
