Jorge Alexander A L, Marchisotti Frederico G, Montenegro Luciana R, Carvalho Luciani R, Mendonca Berenice B, Arnhold Ivo J P
Hospital das Clinicas, Laboratorio de Hormonios, Avenida Dr Eneas de Carvalho Aguiar 155 PAMB, 2 andar Bloco 6, 05403-900, São Paulo, Brazil.
J Clin Endocrinol Metab. 2006 Mar;91(3):1076-80. doi: 10.1210/jc.2005-2005. Epub 2005 Nov 15.
A polymorphism in GHR gene, the presence or absence of exon 3, has been shown to influence the 1- and 2-yr growth responses to human recombinant GH (hGH) therapy in children without GH deficiency (GHD).
The objective of this study was to assess the influence of GHR-exon-3 genotype on the short and long-term response to hGH therapy in children with GHD.
The study was conducted in the university hospital.
Genotype and retrospective analysis was performed on data of 75 children with GHD.
INTERVENTION consisted of hGH treatment at a mean dose of 33 mug/kg.d and GHR-exon-3 genotype by multiplex PCR.
The main outcome measures were GHR genotype: full-length (fl) and exon 3-deleted (d3) alleles, growth velocity in 58 children who remained prepubertal during the first year, and adult height in 44 patients with GHD after 7.5 +/- 3.0 yr of treatment.
Clinical and laboratory data at the start of treatment and hGH doses were indistinguishable among patients with different GHR-exon-3 genotypes (fl/fl vs. fl/d3 or d3/d3). Patients carrying at least one GHRd3 allele had a significantly better growth velocity in the first year of hGH replacement (12.3 +/- 2.6 vs. 10.6 +/- 2.3 cm/yr; P < 0.05) and achieved a taller adult height (final height sd score, -0.8 +/- 1.1 vs. -1.7 +/- 1.2; P < 0.05) when compared with patients homozygous for GHRfl alleles.
Patients with GHD who are homozygous for GHR exon 3 fl were less responsive to short- and long-term hGH therapy. Approximately half of the population is homozygous for GHRfl, and future studies adjusting hGH therapy to genotype may improve outcome.
生长激素受体(GHR)基因中的一种多态性,即外显子3的有无,已被证明会影响非生长激素缺乏(GHD)儿童对重组人生长激素(hGH)治疗的1年和2年生长反应。
本研究的目的是评估GHR外显子3基因型对GHD儿童hGH治疗短期和长期反应的影响。
该研究在大学医院进行。
对75例GHD儿童的数据进行了基因型和回顾性分析。
干预措施包括平均剂量为33μg/kg·d的hGH治疗以及通过多重聚合酶链反应检测GHR外显子3基因型。
主要观察指标为GHR基因型:全长(fl)和外显子3缺失(d3)等位基因、58例在第一年仍处于青春期前儿童的生长速度以及44例接受7.5±3.0年治疗的GHD患者的成人身高。
不同GHR外显子3基因型(fl/fl与fl/d3或d3/d3)患者在治疗开始时的临床和实验室数据以及hGH剂量无差异。与GHRfl等位基因纯合子患者相比,携带至少一个GHRd3等位基因的患者在hGH替代治疗的第一年生长速度明显更快(12.3±2.6 vs. 10.6±2.3 cm/年;P<0.05),且成人身高更高(最终身高标准差评分,-0.8±1.1 vs. -1.7±1.2;P<0.05)。
GHR外显子3 fl纯合的GHD患者对短期和长期hGH治疗反应较差。大约一半的人群是GHRfl纯合子,未来根据基因型调整hGH治疗的研究可能会改善治疗效果。
