Murray R D, Skillicorn C J, Howell S J, Lissett C A, Rahim A, Shalet S M
Department of Endocrinology, Christie Hospital, Manchester, UK.
Clin Endocrinol (Oxf). 1999 Jun;50(6):749-57. doi: 10.1046/j.1365-2265.1999.00722.x.
Previous studies of GH replacement in adults have used unselected cohorts of GH deficient (GHD) adults and weight-based dosing regimens resulting in supraphysiological serum IGF-I levels and a high frequency of side-effects and withdrawal from these studies. By choosing patients with a high level of morbidity at baseline and using a low dose GH titration regimen we aimed to avoid over-replacement and increase the efficacy of treatment.
An open study of GH replacement, initiating treatment with a dose of 0. 8 U/day and titrating the dose by 0.4 U increments to normalize the IGF-I SDS between - 2.0 and + 2.0 SD of the age-related normal range.
65 severely GHD patients (peak GH < 9 mU/l to provocative testing), 25 males, of mixed adult and childhood-onset and mean age 38.7 (range 17-72) years. Inclusion criterion was that of subjectively poor quality of life on clinical interview.
Height, weight, waist and hip circumference were measured to allow calculation of body mass index (BMI) and waist-hip ratio (WHR). Bone mineral density (BMD) was measured by dual X-ray absorptiometry (DEXA). Serum haemoglobin A1C (HbA1C), lipid profile and insulin like growth factor 1 (IGF-I) were measured. The Psychological General Well-Being Schedule (PGWB) and Adult Growth Hormone Deficiency Assessment (AGHDA) self-rating questionnaires (SRQ) were used to assess quality of life.
Baseline characteristics were consistent with those previously described in severely GHD adults; mean IGF-I SDS - 2.4 (+/- 2.7), BMI 28.8 (+/- 5. 4) kg/m2, total cholesterol 6.17 (+/- 1.2) mmol/l, reduced BMD z-scores at the lumbar spine (- 0.8 +/- 1.2) and femoral neck (- 0. 44 +/- 1.4), and SRQ scores considerably lower than reported in previous studies of GH deficient adults and normal controls. Following initiation of GH serum IGF-I SDS was increased significantly from baseline to a mean level of 0.15 +/- 2.7 (P < 0. 001) and 0.31 +/- 2.0 (P < 0.001) at three and eight months, respectively. The mean PGWB score increased from 59.7 +/- 19.9 to 75. 8 +/- 15.0 (P < 0.001) and 73.7 +/- 19.5 (P = 0.001) at three and eight months, respectively. An increase of 14 points represents the largest improvement in quality of life, using this index, that has been reported in GHD adults. The mean AGHDA score also demonstrated considerable improvement, falling from 15.3 +/- 6.0 to 10.4 +/- 6.2 (P < 0.001) and 9.8 +/- 6.5 (P < 0.001) at three and eight months, respectively. The changes observed in both the PGWB and AGHDA scores between baseline and at both three and eight months were shown to correlate significantly with the respective baseline score. A significantly greater improvement was observed in the PGWB following GH replacement in those with a baseline PGWB score of < 60 than in those with a score > 60. This observation was significant at both three (27.1 vs 6.7, P = 0.0001) and eight (25.6 vs 3.3, P = 0.0003) months. All PGWB subscales showed significant improvement though that of vitality was of greatest magnitude. A strong correlation was observed between the generic and disease-specific SRQ (r = - 0.73, P < 0.001).
The observed improvement in quality of life in GH deficient adults is proportional to the degree of impairment before commencing therapy. The use of low-dose titration and selection of a population with greater morbidity reduces the occurrence of over-replacement and increases the efficacy of treatment. This allows direction of resources to those in greatest need.
以往针对成年人生长激素(GH)替代治疗的研究采用的是未经过筛选的生长激素缺乏(GHD)成年人群体,并采用基于体重的给药方案,导致血清胰岛素样生长因子-I(IGF-I)水平超过生理范围,且副作用发生率高,许多患者退出研究。通过选择基线时发病率高的患者并采用低剂量GH滴定方案,我们旨在避免替代过度并提高治疗效果。
一项关于GH替代治疗的开放性研究,起始剂量为0.8 U/天,并以每次增加0.4 U的幅度滴定剂量,以使IGF-I标准差评分(SDS)在年龄相关正常范围的-2.0至+2.0标准差之间恢复正常。
65例严重GHD患者(激发试验时峰值GH<9 mU/l),25例男性,成年期和儿童期发病混合型,平均年龄38.7岁(范围17 - 72岁)。纳入标准是临床访谈中主观生活质量差。
测量身高、体重、腰围和臀围,以计算体重指数(BMI)和腰臀比(WHR)。采用双能X线吸收法(DEXA)测量骨密度(BMD)。检测血清糖化血红蛋白(HbA1C)、血脂谱和胰岛素样生长因子1(IGF-I)。使用心理总体幸福感量表(PGWB)和成人生长激素缺乏评估(AGHDA)自评问卷(SRQ)评估生活质量。
基线特征与先前报道的严重GHD成年人一致;平均IGF-I SDS为-2.4(±2.7),BMI为28.8(±5.4)kg/m²,总胆固醇为6.17(±1.2)mmol/l,腰椎(-0.8±1.2)和股骨颈(-0.44±1.4)的骨密度z评分降低,且SRQ评分显著低于先前GHD成年人及正常对照研究报告的结果。开始使用GH治疗后,血清IGF-I SDS在3个月和8个月时分别从基线显著升高至平均水平0.15±2.7(P<0.001)和0.31±2.0(P<0.001)。PGWB平均评分在3个月和8个月时分别从59.7±19.9提高到75.8±15.0(P<0.001)和73.7±19.5(P = 0.001)。使用该指标,14分的提高代表了GHD成年人中报道的最大生活质量改善。AGHDA平均评分也有显著改善,在3个月和8个月时分别从15.3±6.0降至10.4±6.2(P<0.001)和9.8±6.5(P<0.001)。PGWB和AGHDA评分在基线与3个月及8个月时的变化均与各自的基线评分显著相关。基线PGWB评分<60的患者在接受GH替代治疗后,PGWB改善程度显著大于评分>60的患者。这一观察结果在3个月(27.1对6.7,P = 0.0001)和8个月(25.6对3.3,P = 0.0003)时均具有显著性。所有PGWB子量表均显示出显著改善,其中活力子量表改善幅度最大。通用型和疾病特异性SRQ之间存在强相关性(r = -0.73,P<0.001)。
观察到GHD成年人生活质量的改善与开始治疗前的受损程度成正比。采用低剂量滴定并选择发病率较高的人群可减少替代过度的发生并提高治疗效果。这使得资源能够导向最有需求的人群。
