生长激素受体基因多态性与特发性矮小遗传易感性的关系

目的探讨人生长激素受体(GHR)基因的单核苷酸多态性(SNP)与中国汉族人群特发性矮小(ISS)遗传易感性的关系。方法采用病例对照法,在199例ISS患儿(ISS组)和469名身高正常成人(对照组)中,对GHR基因16个SNP位点进行基因分型和比较,筛查阳性SNP位点(特异基因型频率差异有统计学意义),分析阳性SNP位点基因型与ISS发病风险及血清胰岛素样生长因子1(IGF-1)等相关临床变量的关系。结果在ISS组和对照组中,发现3个阳性SNP位点rs6182(P=0.027)、rs4410646(P=0.01)和rs10044169(P=0.024)。①rs6182(G/T):在T显性模式下,TT和GT基因型的ISS发病风险降低(OR=0.624,95%CI:0.402~0.969,P=0.021)。②rs4410646(A/C):在C显性模式下AA基因型的ISS发病风险降低(OR=0.674,95%CI:0.475~0.958,P=0.016);该位点的多因素Logistics回归分析显示,以CC基因型为参照,血清IGF-1与基因型AA(OR=1.011,95%CI:1.002~1.020,P=0.018...

单纯促性腺激素释放激素类似物或联合重组人生长激素治疗青春期矮小患儿的疗效分析

目的 比较分析单纯促性腺激素释放激素类似物（GnRHa）或联合重组人生长激素（rhGH）治疗青春期非生长激素缺乏矮小（NGHDSS）患儿的助长疗效,探讨科学有效的青春期助长治疗方案.方法 42例青春期NGHDSS患儿（男性14,女性28）,采用GnRHa联合rhGH治疗者（联合组）30例,单独GnRHa 治疗者（单治组）12例.GnRHa初始剂量100ug·kg-1·d-1（28 d）,维持剂量60-80μg·kg-1·d-1（28d）;rhGH初始剂量0.15 IU·ks-1·d-1（28 d）,维持剂量0.10～0.15 IU·ks-1·d-1（28 d）,疗程均为1-2年.主要观察各组年生长速率（GV）、对年龄的身高标准差分值（HtSDSCA）、对骨龄的身高标准差分值（HtSDSBA）、预测身高标准差分值（PAHSDS）的动态变化.结果 （1）1年疗效：联合组治疗前后比较,GV、HtSDSCA、HtSDSBA、PAHSDS变化均有统计学意义（均P〈0.05）.单治组患儿治疗前后比较,GV、HtSDSCA、HtSDSBA、PAHSDS变化均无统计学意义（均P〉0.05）.2组间比较,GV、HtSDSBA、PAHSDS均有显著性差异（均P〈0.05）.（2）2年疗效：联合组治疗前后比较,GV、HtSDSCA、HtSDSBA、PAHSDS变化均有统计学意义（均P〈0.05）.单治组治疗前后比较,GV、HtSDSCA、HtSDSBA、PAHSDS变化均无统计学意义（均P〉0.05）.2组间比较,GV、HtSDSBA、HtSDSCA、PAHSDS均有显著性差异（均P〈0.05）.结论 采用GnRHa联合rhGH治疗青春发育初期的NGHDSS患儿能有效促进近期生长速率,其疗效明显优于单独GnRHa治疗,但对成年终身的贡献尚待研究.

血清8-异构前列腺素变化与川崎病的相关性

目的:探讨血清8-异构前列腺素与川崎病(KD)的相关性。方法:检测35例川崎病患儿和25例发热对照组患儿急性期及恢复期血清中8-异构前列腺素的浓度并进行相互比较,同时川崎病患儿行超声心动图检查,比较合并冠状动脉损害组患儿与无冠状动脉损害组患儿血清8-异构前列腺素水平。结果:KD急性期和KD恢复期与发热对照组比较血清8-异构前列腺素水平升高明显,且KD恢复期患儿血清8-异构前列腺素水平较发热对照组急性期升高明显,差异有统计学意义。KD急性期合并CAL组患儿血清8-异构前列腺素较NCAL组明显升高,差异有统计学意义(P<0.05)。急性期KD冠脉扩张程度和血清8-异构前列腺素含量呈正相关(R=0.937,P<0.05)。结论:8-异构前列腺素为标志的氧化应激可能参与KD患儿急性期血管炎的发病,与KD冠状动脉损伤的程度有相关性,对于评估KD冠状动脉损伤发生的概率及远期预后有一定价值。

ASSOCIATION ANALYSIS OF POLYMORPHISMS IN SIX GENES WITHIN THE GH/IGF-1 AXIS IN PATIENTS WITH IDIOPATHIC SHORT STATURE IN THE CHINESE HAN POPULATION

Objective To investigate relationships of polymorphisms in six genes （ GHR, IGF-1, IGF-1R, IGFBP-3, JAK2, and STAT5b） in the growth hormone （GH）/insulin-like growth factor-1 （IGF-1） axis with idiopathic short stature （ISS） in the Chinese Han population. Methods A case- control study was carried out on a cohort of 198 ISS patients and 306 healthy controls. A total of 106 tagging single nucleotide polymorphisms （tagSNPs） from the six genes were selected from the HapMap （haplotype map of the human genome ） Han Chinese in the Beijing subset. Results of genotyping conducted by high- throughput lllumina GoldenGateTM Assay were analyzed by statistical software. Results Both individual tagSNPs and haplotypes showed an association with 1SS in the Han Chinese population （ P 〈 O. 05 ）. For each single test, both allele and genotype were tested. By allele frequency analysis, six positive SNP sites （ rsNo. 1, rsNo. 2, rsNo. 3, rsNo. 4, rsNo. 5, and rsNo. 6） of 3 genes （ JAK2, 1GF-1R, and GHR） were found having associations with ISS. By genotype frequency analysis, there were significant differences between the patient and control groups in the following SNP sites： 4 sites in JAK2 gene （ rsNo. 1, rsNo. 2, rsNo. 3, and rsNo. 4） and 1 site in GHR gene （ rsNo. 6）. The risk which affected ISS was found related to the JAK2 gene in 4 sites （ increase in rsNo. 1 and decrease in rsNo. 2, rsNo. 3, and rsNo. 4 ） and to the GHR gene in 1 site （decrease in rsNo. 6）. They were four haplotypes in gene of IGF-1R as ＂TGC＂, ＂CGCT＂, ＂TA＂, and ＂ CA＂, one haplotype in IGFBP-3 as ＂TA＂, and one haplotype in JAK2 as ＂CTG＂, which revealed high significance for risks of affecting ISS. At last, multivariate logistic regression analysis of specific site rsNo. 6 of the GHR gene revealed that the serum IGF-1 was related to genotypes AA and AC, with genotype CC as the reference （ P =0. 015）. Conclusion Genetic variances in six genes within the GH/IGF-1 axis may be important etiological factors for ISS in the Chinese Han population.