Fors H, Bjarnason R, Wirént L, Albertsson-Wikland K, Bosaeust L, Bengtsson B A, Johannsson G
Göteborg Paediatric Growth Research Center, Sahlgrenska University Hospital, Sweden.
Clin Endocrinol (Oxf). 2001 Nov;55(5):617-24. doi: 10.1046/j.1365-2265.2001.01386.x.
The need for continued GH replacement in patients with childhood-onset GH deficiency (GHD) into adulthood has been recognized. The consequences of discontinuing GH treatment on bone mineralization in adolescent patients with GHD and short stature were examined over a period of 2 years.
Forty adolescents (aged 16-21 years) treated with GH for more than 3 years and 16 closely matched healthy controls were studied. After a baseline visit, GH treatment was discontinued. The patients were then re-examined with the same protocol after 1 and 2 years. Twenty-one patients had continuing severe GHD into adulthood, while 19 patients were regarded as having sufficient endogenous GH secretion (GHS).
At baseline, there were no differences between the groups in total bone mineral content (BMC) or bone mineral density (BMD). After 2 years without GH treatment, BMC increased similarly in the GHD and GHS groups. BMC of the lumbar spine (L2-L4) increased only in the GHD group. Lumbar spine BMD increased in the GHD and the GHS groups. No changes were observed in the femoral neck region. Biochemical measurements showed that carboxy-terminal cross-linked telopeptide of type I collagen (ICTP) and bone specific alkaline phosphates (ALP) were higher in the GHD and GHS groups at baseline compared with controls. Osteocalcin, carboxy-terminal propeptide of type I procollagen (PICP), ICTP and ALP decreased during the 2 years off treatment in both the GHD and GHS groups. PICP was also lower after 2 years in the GHD group compared with both the GHS group and controls.
After discontinuation of GH therapy in adolescents at or near final height, there was a continued increase in BMC and BMD both for adolescents with growth hormone deficiency and for those classified as growth hormone sufficient. These groups did not differ from controls at baseline or after 2 years. In the growth hormone deficiency group, biochemical markers for bone formation decreased to levels below those in the growth hormone sufficient and healthy control groups. Although the number of patients and controls in this study were small, the results indicate that the present treatment of Swedish GH-deficient children to final height results in normal BMD.
儿童期生长激素缺乏症(GHD)患者成年后仍需持续进行生长激素替代治疗已得到认可。本研究在2年的时间里,对青春期GHD和身材矮小患者停用生长激素治疗对骨矿化的影响进行了研究。
研究了40名接受生长激素治疗超过3年的青少年(年龄16 - 21岁)以及16名年龄匹配的健康对照者。在基线访视后,停用生长激素治疗。然后在1年和2年后按照相同方案对患者进行复查。21名患者成年后仍存在严重GHD,而19名患者被认为具有足够的内源性生长激素分泌(GHS)。
基线时,两组在总骨矿物质含量(BMC)或骨矿物质密度(BMD)方面无差异。在停用生长激素治疗2年后,GHD组和GHS组的BMC均有相似程度的增加。仅GHD组腰椎(L2 - L4)的BMC增加。GHD组和GHS组的腰椎BMD均增加。股骨颈区域未观察到变化。生化检测显示,与对照组相比,GHD组和GHS组在基线时I型胶原羧基末端交联肽(ICTP)和骨特异性碱性磷酸酶(ALP)水平较高。在GHD组和GHS组停止治疗的2年期间,骨钙素、I型前胶原羧基末端前肽(PICP)、ICTP和ALP均下降。2年后,GHD组的PICP水平低于GHS组和对照组。
在接近最终身高的青少年停用生长激素治疗后,生长激素缺乏的青少年和被归类为生长激素充足的青少年的BMC和BMD均持续增加。这些组在基线时或2年后与对照组无差异。在生长激素缺乏组中,骨形成的生化标志物降至低于生长激素充足组和健康对照组的水平。尽管本研究中的患者和对照数量较少,但结果表明,目前瑞典对生长激素缺乏儿童治疗至最终身高可使骨密度正常。