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FGF-2 Gene Polymorphism in Osteoporosis among Guangxi’s Zhuang Chinese

机译:广西壮族人群骨质疏松症中FGF-2基因多态性

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摘要

Osteoporosis is a complex multifactorial disorder of gradual bone loss and increased fracture risk. While previous studies have shown the importance of many genetic factors in determining peak bone mass and fragility fractures and in suggesting involvement of fibroblast growth factor-2 (FGF-2) in bone metabolism and bone mass, the relationship of FGF-2 genetic diversity with bone mass/osteoporosis has not yet been revealed. The current study investigated the potential relevance of FGF-2 gene polymorphism in osteoporosis among a Zhuang ethnic Chinese cohort of 623, including 237 normal bone mass controls, 227 osteopenia, and 159 osteoporosis of different ages. Bone density was examined by calcaneus ultrasound attenuation measurement, and single nucleotide polymorphisms (SNPs) and linkage disequilibrium analyses were performed on five SNP loci of FGF-2 gene. Significant differences were found in bone mass in males between the 45-year-old and ≥70-year-old groups (p < 0.01), and in females among 55, 60, 65 and 70-year-old groups (p < 0.05). Males had higher bone mass values than females in the same age (over 55-year-old) (p < 0.05). The proportions of individuals with normal bone mass decreased with age (65.2% to 40% in males, and 50% to 0% in females), whereas prevalence of osteoporosis increased with age (15.4% to 30% in men, and 7.7% to 82% in women). Out of five FGF-2 SNP loci, the TA genotype of rs308442 in the osteoporosis group (40.2%) was higher than in the control group (29.5%) (p < 0.05). The TA genotype was significantly correlated with the risk of osteoporosis (odds ratio OR = 1.653), 95% confidence interval (CI): 1.968–1.441). Strong linkage disequilibrium in FGF-2 gene was also detected between rs12644427 and rs3747676, between rs12644427 and rs3789138, and between rs3747676 and rs3789138 (D’ > 0.8, and r2 > 0.33). Thus, the rs308442 locus of FGF-2 gene is closely correlated to osteoporosis in this Zhuang ethnic Chinese cohort, and the TA may be the risk genotype of osteoporosis.
机译:骨质疏松症是一种复杂的多因素疾病,逐渐导致骨质流失和骨折风险增加。尽管先前的研究表明许多遗传因素在确定峰值骨量和脆性骨折以及暗示成纤维细胞生长因子2(FGF-2)参与骨代谢和骨量方面的重要性,但FGF-2遗传多样性与骨量/骨质疏松症尚未发现。当前的研究调查了623名壮族华裔队列中FGF-2基因多态性与骨质疏松症的潜在相关性,其中包括237名正常骨量对照,227名骨质减少和159名不同年龄的骨质疏松症。通过跟骨超声衰减测量检查骨密度,并对FGF-2基因的五个SNP位点进行单核苷酸多态性(SNP)和连锁不平衡分析。在45岁和≥70岁组之间,男性的骨量存在显着差异(p <0.01),而在55、60、65和70岁组中,女性的骨量存在显着差异(p <0.05) )。在同一年龄段(55岁以上),男性的骨量值高于女性(p <0.05)。骨量正常的个体比例随着年龄的增长而下降(男性为65.2%至40%,女性为50%至0%),而骨质疏松的患病率随年龄而增加(男性为15.4%至30%,男性为7.7%女性占82%)。在五个FGF-2 SNP位点中,骨质疏松组的rs308442的TA基因型(40.2%)高于对照组(29.5%)(p <0.05)。 TA基因型与骨质疏松症的风险显着相关(比值比OR = 1.653),95%置信区间(CI):1.968–1.441)。在rs12644427和rs3747676之间,rs12644427和rs3789138之间以及rs3747676和rs3789138之间也检测到了FGF-2基因的强连锁不平衡(D'> 0.8,r 2 > 0.33)。因此,该壮族人群FGF-2基因的rs308442基因座与骨质疏松症密切相关,TA可能是骨质疏松症的危险基因型。

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