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The genetic architecture of age at menarche and its causal effects on other traits

全基因组关联研究 生物 遗传建筑学 数量性状位点 初潮 遗传学 遗传关联 特质 候选基因 因果推理 基因 进化生物学 单核苷酸多态性 基因型 医学 内分泌学 病理 计算机科学 程序设计语言
作者
Guijuan Feng,Qian Xu,Qi-Gang Zhao,Bai‐Xue Han,Shanshan Yan,Jie Zhu,Yu‐Fang Pei
出处
期刊:Journal of Human Genetics [Springer Nature]
标识
DOI:10.1038/s10038-024-01287-w
摘要

Age at menarche (AAM) is a sign of puberty of females. It is a heritable trait associated with various adult diseases. However, the genetic mechanism that determines AAM and links it to disease risk is poorly understood. Aiming to uncover the genetic basis for AAM, we conducted a joint association study in up to 438,089 women from 3 genome-wide association studies of European and East Asian ancestries. A series of bioinformatical analyses and causal inference were then followed to explore in-depth annotations at the associated loci and infer the causal relationship between AAM and other complex traits/diseases. This largest meta-analysis identified a total of 21 novel AAM associated loci at the genome wide significance level (P < 5.0 × 10−8), 4 of which were European ancestry-specific loci. Functional annotations prioritized 33 candidate genes at newly identified loci. Significant genetic correlations were observed between AAM and 67 complex traits. Further causal inference demonstrated the effects of AAM on 13 traits, including forced vital capacity (FVC), high blood pressure, age at first live birth, etc, indicating that earlier AAM causes lower FVC, worse lung function, hypertension and earlier age at first (last) live birth. Enrichment analysis identified 5 enriched tissues, including the hypothalamus middle, hypothalamo hypophyseal system, neurosecretory systems, hypothalamus and retina. Our findings may provide useful insights that elucidate the mechanisms determining AAM and the genetic interplay between AAM and some traits of women.

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