Abstract
BackgroundAge at menarche has been associated with various health outcomes. We aimed to identify potential causal effects of age at menarche on health-related traits in a hypothesis-free manner.MethodsWe conducted a Mendelian randomization phenome-wide association study (MR-pheWAS) of age at menarche with 17,893 health-related traits in UK Biobank (n = 181,318) using PHESANT. The exposure of interest was the genetic risk score for age at menarche. We conducted a second MR-pheWAS after excluding SNPs associated with BMI from the genetic risk score, to examine whether results might be due to the genetic overlap between age at menarche and BMI. We followed up a subset of health-related traits to investigate MR assumptions and seek replication in independent study populations.ResultsOf the 17,893 tests performed in our MR-pheWAS, we identified 619 associations with the genetic risk score for age at menarche at a 5% false discovery rate threshold, of which 295 were below a Bonferroni-corrected P value threshold. These included potential effects of younger age at menarche on lower lung function, higher heel bone-mineral density, greater burden of psychosocial/mental health problems, younger age at first birth, higher risk of childhood sexual abuse, poorer cardiometabolic health, and lower physical activity. After exclusion of variants associated with BMI, the genetic risk score for age at menarche was related to 37 traits at a 5% false discovery rate, of which 29 were below a Bonferroni-corrected P value threshold. We attempted to replicate findings for bone-mineral density, lung function, neuroticism, and childhood sexual abuse using 5 independent cohorts/consortia. While estimates for lung function, higher bone-mineral density, neuroticism, and childhood sexual abuse in replication cohorts were consistent with UK Biobank estimates, confidence intervals were wide and often included the null.ConclusionsThe genetic risk score for age at menarche was related to a broad range of health-related traits. Follow-up analyses indicated imprecise evidence of an effect of younger age at menarche on greater bone-mineral density, lower lung function, higher neuroticism score, and greater risk of childhood sexual abuse in the smaller replication samples available; hence, these findings need further exploration when larger independent samples become available.
Highlights
Age at menarche has been associated with various health outcomes
Steiger filtering found that 27 of the 360 single nucleotide polymorphisms (SNPs) included in the GRS for age at menarche explained more of the variation in adult body mass index (BMI) than age at menarche
After excluding SNPs associated with childhood BMI, the GRS including the remaining 353 SNPs (GRS-child BMI) explained 6.0% of the variance in age at menarche (F-statistic = 1012), and after excluding childhood and/or adult BMI associated SNPs, the GRS including the remaining 154 SNPs (GRS-BMI) explained 3.0% of the variance (F-statistic = 489)
Summary
Age at menarche has been associated with various health outcomes. We aimed to identify potential causal effects of age at menarche on health-related traits in a hypothesis-free manner. Mendelian randomization has previously been used to explore effects of age at menarche on cardiometabolic traits [9, 11, 12], depression [13, 14], breast cancer [15, 16], educational level [17], lung function [18], osteoporosis [19], fracture risk [20], and reproductive/behavioral outcomes [21] These have focused on hypothesized effects by exploring whether associations that have been widely examined in the literature have causal evidence from Mendelian randomization analyses. The large sample size used here supports more precise estimates than these previous studies as well as the potential for novel etiological understanding
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