Literature DB >> 29967039

Gene-Centric Analysis of Preeclampsia Identifies Maternal Association at PLEKHG1.

Kathryn J Gray1,2,3, Vesela P Kovacheva4, Hooman Mirzakhani5, Andrew C Bjonnes2,3, Berta Almoguera6, Andrew T DeWan7, Elizabeth W Triche8, Audrey F Saftlas9, Josephine Hoh10, Dale L Bodian11, Elisabeth Klein11, Kathi C Huddleston11, Sue Ann Ingles12, Charles J Lockwood13, Hakon Hakonarson14, Thomas F McElrath15, Jeffrey C Murray16, Melissa L Wilson12, Errol R Norwitz17, S Ananth Karumanchi18,19, Brian T Bateman5, Brendan J Keating20, Richa Saxena5,2,3.   

Abstract

The genetic susceptibility to preeclampsia, a pregnancy-specific complication with significant maternal and fetal morbidity, has been poorly characterized. To identify maternal genes associated with preeclampsia risk, we assembled 498 cases and 1864 controls of European ancestry from preeclampsia case-control collections in 5 different US sites (with additional matched population controls), genotyped samples on a cardiovascular gene-centric array composed of variants from ≈2000 genes selected based on prior genetic studies of cardiovascular and metabolic diseases and performed case-control genetic association analysis on 27 429 variants passing quality control. In silico replication testing of 9 lead signals with P<10-4 was performed in independent European samples from the SOPHIA (Study of Pregnancy Hypertension in Iowa) and Inova cohorts (212 cases, 456 controls). Multiethnic assessment of lead signals was then performed in samples of black (26 cases, 136 controls), Hispanic (132 cases, 468 controls), and East Asian (9 cases, 80 controls) ancestry. Multiethnic meta-analysis (877 cases, 3004 controls) revealed a study-wide statistically significant association of the rs9478812 variant in the pleiotropic PLEKHG1 gene (odds ratio, 1.40 [1.23-1.60]; Pmeta=5.90×10-7). The rs9478812 effect was even stronger in the subset of European cases with known early-onset preeclampsia (236 cases diagnosed <37 weeks, 1864 controls; odds ratio, 1.59 [1.27-1.98]; P=4.01×10-5). PLEKHG1 variants have previously been implicated in genome-wide association studies of blood pressure, body weight, and neurological disorders. Although larger studies are required to further define maternal preeclampsia heritability, this study identifies a novel maternal risk locus for further investigation.
© 2018 American Heart Association, Inc.

Entities:  

Keywords:  genetic association studies; hypertension; population control; preeclampsia; pregnancy

Mesh:

Substances:

Year:  2018        PMID: 29967039      PMCID: PMC6043396          DOI: 10.1161/HYPERTENSIONAHA.117.10688

Source DB:  PubMed          Journal:  Hypertension        ISSN: 0194-911X            Impact factor:   10.190


  79 in total

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Review 5.  Neurodevelopmental Outcomes of Prenatal Preeclampsia Exposure.

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6.  Genes for Preeclampsia: An Opportunity for Blood Pressure Genomics.

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Review 7.  Pregnancy, preeclampsia and maternal aging: From epidemiology to functional genomics.

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9.  Risk of pre-eclampsia in patients with a maternal genetic predisposition to common medical conditions: a case-control study.

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