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澳大利亚囊性纤维化儿童和青少年的青春期发育及其对骨密度的影响。

Pubertal development and its influences on bone mineral density in Australian children and adolescents with cystic fibrosis.

作者信息

Buntain Helen M, Greer Ristan M, Wong Joseph C H, Schluter Philip J, Batch Jennifer, Lewindon Peter, Bell Scott C, Wainwright Claire E

机构信息

Department of Respiratory Medicine, Royal Children's Hospital, Herston, Queensland, Australia.

出版信息

J Paediatr Child Health. 2005 Jul;41(7):317-22. doi: 10.1111/j.1440-1754.2005.00635.x.

DOI:10.1111/j.1440-1754.2005.00635.x
PMID:16014134
Abstract

BACKGROUND

Pubertal delay is thought to contribute to suboptimal peak bone mass acquisition in young people with cystic fibrosis (CF), leading to an increased fracture incidence. This study aims to compare pubertal development in young people with CF with that of a local healthy population and assess the influence it has on areal bone mineral density (aBMD).

METHODS

Tanner stage, age of menarche, bone age (BA), sex hormone levels and aBMD were examined in 85 individuals with CF (aged 5.3-18.1 years, 39 females) and 100 local controls (5.6-17.9 years, 54 females).

RESULTS

Tanner stage and age of menarche were not significantly different between controls and CF. Tanner stage-adjusted mean values for follicle stimulating hormone (FSH), luteinizing hormone (LH) and testosterone (T) were lower in males with CF (FSH: P = 0.004, LH: P = 0.01 and T: P = 0.002). Bone age was delayed in adolescents with CF compared to controls (chronological age-BA: controls = 0.13 years (SE = 0.16), CF = 0.95 years (SE = 0.22), P = 0.003). Areal bone mineral density (adjusted for age, sex, height and lean tissue mass) was not significantly different between CF and controls. Moderate negative correlations were found between delayed BA and weight (r = -0.41, P < 0.001) and height (r = -0.41, P < 0.001).

CONCLUSIONS

There was no evidence of clinical pubertal delay or low aBMD (adjusted for short stature and lean tissue mass) in young people with CF when compared with a local population, despite lower nutritional markers, height and weight and delayed skeletal maturation.

摘要

背景

青春期延迟被认为会导致囊性纤维化(CF)青少年的骨峰值获取不理想,从而增加骨折发生率。本研究旨在比较CF青少年与当地健康人群的青春期发育情况,并评估其对骨面积密度(aBMD)的影响。

方法

对85例CF患者(年龄5.3 - 18.1岁,女性39例)和100名当地对照者(年龄5.6 - 17.9岁,女性54例)进行坦纳分期、初潮年龄、骨龄(BA)、性激素水平及aBMD检测。

结果

对照者与CF患者的坦纳分期和初潮年龄无显著差异。CF男性患者经坦纳分期调整后的促卵泡生成素(FSH)、促黄体生成素(LH)和睾酮(T)均值较低(FSH:P = 0.004,LH:P = 0.01,T:P = 0.002)。与对照者相比,CF青少年的骨龄延迟(实际年龄 - BA:对照者 = 0.13岁(标准误 = 0.16),CF患者 = 0.95岁(标准误 = 0.22),P = 0.003)。CF患者与对照者之间的骨面积密度(经年龄、性别、身高和瘦组织质量调整)无显著差异。骨龄延迟与体重(r = -0.41,P < 0.001)和身高(r = -0.41,P < 0.001)之间存在中度负相关。

结论

尽管CF青少年的营养指标、身高和体重较低且骨骼成熟延迟,但与当地人群相比,并无临床青春期延迟或低aBMD(经身材矮小和瘦组织质量调整)的证据。

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