Blum Werner F, Crowe Brenda J, Quigley Charmian A, Jung Heike, Cao Dachuang, Ross Judith L, Braun LeeAnn, Rappold Gudrun
Lilly Research Laboratories, Eli Lilly & Company, Saalburgstrasse 153, D-61350 Bad Homburg, Germany.
J Clin Endocrinol Metab. 2007 Jan;92(1):219-28. doi: 10.1210/jc.2006-1409. Epub 2006 Oct 17.
The short stature homeobox-containing gene, SHOX, located on the distal ends of the X and Y chromosomes, encodes a homeodomain transcription factor responsible for a significant proportion of long-bone growth. Patients with mutations or deletions of SHOX, including those with Turner syndrome (TS) who are haplo-insufficient for SHOX, have variable degrees of growth impairment, with or without a spectrum of skeletal anomalies consistent with dyschondrosteosis.
Our objective was to determine the efficacy of GH in treating short stature associated with short stature homeobox-containing gene deficiency (SHOX-D).
Fifty-two prepubertal subjects (24 male, 28 female; age, 3.0-12.3 yr) with a molecularly proven SHOX gene defect and height below the third percentile for age and gender (or height below the 10th percentile and height velocity below the 25th percentile) were randomized to either a GH-treatment group (n = 27) or an untreated control group (n = 25) for 2 yr. To compare the GH treatment effect between subjects with SHOX-D and those with TS, a third study group, 26 patients with TS aged 4.5-11.8 yr, also received GH. Between-group comparisons of first-year and second-year height velocity, height sd score, and height gain (cm) were performed using analysis of covariance accounting for diagnosis, sex, and baseline age.
The GH-treated SHOX-D group had a significantly greater first-year height velocity than the untreated control group (mean +/- se, 8.7 +/- 0.3 vs. 5.2 +/- 0.2 cm/yr; P < 0.001) and similar first-year height velocity to GH-treated subjects with TS (8.9 +/- 0.4 cm/yr; P = 0.592). GH-treated subjects also had significantly greater second-year height velocity (7.3 +/- 0.2 vs. 5.4 +/- 0.2 cm/yr; P < 0.001), second-year height sd score (-2.1 +/- 0.2 vs.-3.0 +/- 0.2; P < 0.001) and second-year height gain (16.4 +/- 0.4 vs. 10.5 +/- 0.4 cm; P < 0.001) than untreated subjects.
This large-scale, randomized, multicenter clinical trial in subjects with SHOX-D demonstrates marked, highly significant, GH-stimulated increases in height velocity and height SDS during the 2-yr study period. The efficacy of GH treatment in subjects with SHOX-D was equivalent to that seen in subjects with TS. We conclude that GH is effective in improving the linear growth of patients with various forms of SHOX-D.
矮小同源框基因(SHOX)位于X和Y染色体的远端,编码一种同源结构域转录因子,对大部分长骨生长起重要作用。SHOX发生突变或缺失的患者,包括特纳综合征(TS)患者,其SHOX基因单倍体不足,有不同程度的生长障碍,伴有或不伴有与软骨发育不全一致的一系列骨骼异常。
我们的目的是确定生长激素(GH)治疗与矮小同源框基因缺陷(SHOX-D)相关的矮小症的疗效。
52名青春期前受试者(24名男性,28名女性;年龄3.0 - 12.3岁),经分子检测证实存在SHOX基因缺陷,身高低于年龄和性别的第3百分位数(或身高低于第10百分位数且身高生长速度低于第25百分位数),被随机分为GH治疗组(n = 27)或未治疗对照组(n = 25),治疗2年。为比较SHOX-D患者与TS患者的GH治疗效果,第三个研究组,26名年龄在4.5 - 11.8岁的TS患者,也接受了GH治疗。使用协方差分析对诊断、性别和基线年龄进行校正,比较第一年和第二年的身高生长速度、身高标准差评分和身高增长(厘米)的组间差异。
GH治疗的SHOX-D组第一年的身高生长速度显著高于未治疗的对照组(均值±标准误,8.7±0.3 vs. 5.2±0.2厘米/年;P < 0.001),且与接受GH治疗的TS患者第一年的身高生长速度相似(8.9±0.4厘米/年;P = 0.592)。GH治疗的受试者第二年的身高生长速度(7.3±0.2 vs. 5.4±0.2厘米/年;P < 0.001)、第二年的身高标准差评分(-2.1±0.2 vs. -3.0±0.2;P < 0.001)和第二年的身高增长(16.4±0.4 vs. 10.5±0.4厘米;P < 0.001)也显著高于未治疗的受试者。
这项针对SHOX-D患者的大规模、随机、多中心临床试验表明,在2年的研究期间,GH刺激显著提高了身高生长速度和身高标准差评分。GH治疗SHOX-D患者的疗效与TS患者相当。我们得出结论,GH对改善各种形式SHOX-D患者的线性生长有效。
