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IGF1基因启动子中的微卫星多态性与白种女性自然绝经时间

A microsatellite polymorphism in IGF1 gene promoter and timing of natural menopause in Caucasian women.

作者信息

Kaczmarek Maria, Pacholska-Bogalska Joanna, Kwaśniewski Wojciech, Kotarski Jan, Halerz-Nowakowska Barbara, Goździka-Józefiak Anna

机构信息

1. Department of Human Biological Development, Institute of Anthropology, Faculty of Biology, Adam Mickiewicz University in Poznań, Poland.

2. Department of Animal Physiology, Institute of Experimental Biology, Faculty of Biology, Adam Mickiewicz University in Poznań, Poland.

出版信息

Int J Med Sci. 2015 Jan 1;12(1):32-41. doi: 10.7150/ijms.9840. eCollection 2015.

Abstract

BACKGROUND

Genes involved in the IGF-1 aging pathways in the human ovary can be considered strong candidates for predictors of the natural menopause timing. This study evaluates the association between a cytosine-adenine (CA) microsatellite polymorphism in the IGF1 gene promoter P1 and age at natural menopause.

METHODS

Genomic DNA was extracted from the peripheral blood, PCR was performed using primers designed to amplify the polymorphic (CA) n repeat of the human IGF1 gene, an allele dose effect for the most common (CA)19 repeats allele, Cox proportional hazard regression models and the Kaplan-Meier cumulative survivorship method with the log-rank test were used to determine statistical significance of studied associations in a sample of 257 Polish women aged 40-58 years.

RESULTS

Crude Cox proportional hazard regression analysis confirmed the association between the IGF1 gene polymorphism and the menopause timing (p=0.038). This relationship remained statistically significant after controlling for other menopause confounders in multivariate modelling. Out of the input variables, the (CA)n polymorphism in the IGF1 gene promoter, age at menarche and smoking status were independent covariates of the natural menopause timing (χ2=12.845; df=3; p=0.034). The onset of menopause at a younger age was likely associated with the IGF1 genotype variant not carrying the (CA)19 repeats allele, menarche before the age of 12 and a current cigarette smoker status (HR=1.6).

CONCLUSION

This study provides evidence that a common cytosine-adenine (CA) microsatellite repeat polymorphism in the P1 promoter region of the IGF1 gene is an independent predictive factor for age at natural menopause in Caucasian women also after adjusting for other menopause covariates.

摘要

背景

人类卵巢中参与胰岛素样生长因子-1(IGF-1)衰老途径的基因可被视为自然绝经时间预测指标的有力候选基因。本研究评估了IGF1基因启动子P1中胞嘧啶-腺嘌呤(CA)微卫星多态性与自然绝经年龄之间的关联。

方法

从外周血中提取基因组DNA,使用设计用于扩增人类IGF1基因多态性(CA)n重复序列的引物进行聚合酶链反应(PCR),针对最常见的(CA)19重复等位基因进行等位基因剂量效应分析,采用Cox比例风险回归模型以及带有对数秩检验的Kaplan-Meier累积生存法,以确定在257名年龄在40 - 58岁的波兰女性样本中所研究关联的统计学意义。

结果

粗Cox比例风险回归分析证实了IGF1基因多态性与绝经时间之间的关联(p = 0.038)。在多变量建模中控制其他绝经混杂因素后,这种关系仍具有统计学意义。在输入变量中,IGF1基因启动子中的(CA)n多态性、初潮年龄和吸烟状况是自然绝经时间的独立协变量(χ2 = 12.845;自由度 = 3;p = 0.034)。绝经年龄较小可能与不携带(CA)19重复等位基因的IGF1基因型变体、12岁之前的初潮以及当前吸烟者状态相关(风险比 = 1.6)。

结论

本研究提供了证据表明,在调整其他绝经协变量后,IGF1基因P1启动子区域常见的胞嘧啶-腺嘌呤(CA)微卫星重复多态性是白种女性自然绝经年龄的独立预测因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9c0f/4278873/1defb36b2a4f/ijmsv12p0032g001.jpg

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