Association of maternal and fetal LEPR common variants with maternal glycemic traits during pregnancy

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作者
Rong Lin
Hongfang Ju
Ziyu Yuan
Liangliang Zeng
Yuantian Sun
Zhenyu Su
Yajun Yang
Yi Wang
Li Jin
机构
[1] Hainan Medical College,Department of Biology
[2] Taizhou People’s Hospital,Department of Gynaecology and Obstetrics
[3] Fudan-Taizhou Institute of Health Sciences,Ministry of Education Key Laboratory of Contemporary Anthropology and State Key Laboratory of Genetic Engineering, Collaborative Innovation Center for Genetics and Development, School of Life Sciences
[4] Fudan University,CAS
[5] Chinese Academy of Sciences,MPG Partner Institute for Computational Biology, Shanghai Institute for Biological Sciences
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Recent studies suggested that maternal and placental leptin receptor (LEPR) may be involved in maternal glucose metabolism in pregnancy. To identify maternal and fetal LEPR common variants influencing gestational glycemic traits, we performed association study of 24-28-week maternal fasting glucose, glucose 1 hour after the consumption of a 50-g oral glucose load, fasting insulin and indices of beta-cell function (HOMA-β) and insulin resistance (HOMA-IR) in 1,112 unrelated women and their children. Follow-up of 36 LEPR loci identified 3 maternal loci (rs10889567, rs1137101 and rs3762274) associated with fasting glucose, these 3 fetal loci associated with fasting insulin and HOMA1-IR, as well as these 3 maternal-fetal loci combinations associated with HOMA2-β. We also demonstrated association of maternal locus rs7554485 with HOMA2-β and HOMA2-IR, maternal locus rs10749754 with fasting glucose, fetal locus rs10749754 with HOMA2-IR. However, these associations were no longer statistically significant after Bonferroni correction. In conclusion, our results first revealed multiple associations between maternal and fetal LEPR common variants and gestational glycemic traits. These associations did not survive Bonferroni correction. These corrections are overly conservative for association studies. We therefore believe the influence of these nominally significant variants on gestational glycometabolism will be confirmed by additional studies.
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