Influence of genetic variation, genetic ancestry, and obesity on gestational diabetes mellitus risk
遗传变异、遗传血统和肥胖对妊娠期糖尿病风险的影响
基本信息
- 批准号:10359742
- 负责人:
- 金额:$ 14.03万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2020
- 资助国家:美国
- 起止时间:2020-03-01 至 2023-09-30
- 项目状态:已结题
- 来源:
- 关键词:Academic Medical CentersAffectAfrican AmericanAfrican American populationAfrican ancestryAlgorithmsAmericanAreaAsianAsian AmericansAsian ancestryAwardBioinformaticsBiologyBody mass indexCandidate Disease GeneCategoriesCentral obesityClassificationClinical DataComplications of Diabetes MellitusCountryDataDatabasesDevelopmentDevelopment PlansDiabetes MellitusDietElectronic Health RecordEnvironmental Risk FactorEthnic OriginEtiologyEuropeanFunctional disorderFutureGene ExpressionGenesGeneticGenetic Predisposition to DiseaseGenetic VariationGenetic studyGenomeGestational DiabetesGlucoseGoalsHigh PrevalenceHispanic AmericansHispanic PopulationsHyperglycemiaIndividualInsulinInsulin ResistanceInvestigationKidney DiseasesKnowledgeKoreansLeadLightLinkLow PrevalenceMeasuresMendelian randomizationMentored Research Scientist Development AwardMentorsMethodsNational Institute of Diabetes and Digestive and Kidney DiseasesNative American AncestryNative AmericansNeuropathyNon-Insulin-Dependent Diabetes MellitusObesityPatient Self-ReportPhenotypePhysiologyPlant RootsPopulationPredictive ValuePregnancyPregnancy ComplicationsPregnancy OutcomePregnant WomenPrevalencePreventionQuantitative Trait LociRaceRegulationReportingReproducibilityResearchResearch PersonnelResearch PriorityResourcesRetinal DiseasesRiskRisk FactorsRoleSamplingStreamStructure of beta Cell of isletTestingThinnessTimeTissue-Specific Gene ExpressionTissuesTrainingTraining ProgramsUnited KingdomVariantWaist-Hip RatioWeightWomanWomen&aposs Healthbiobankbiomedical informaticscase controlcausal variantcost effectivegenetic architecturegenetic epidemiologygenetic variantgenome wide association studyhigh riskinnovationinstrumentmultidisciplinarypersonalized approachpersonalized interventionpersonalized strategiespopulation basedportabilitypreventracial disparityrepositoryscreeningtrait
项目摘要
PROJECT SUMMARY/ABSTRACT
Gestational diabetes mellitus (GDM), is among the most common pregnancy complications in the US. Shared
pathophysiology with type-2 diabetes (T2D), evidence of familial aggregation, and evidence of racial disparity
all support a role for genetic predisposition. Asian American (AAM) and Hispanic American (HA) women have
lower prevalence of obesity on average than African American (AA) women, yet have higher GDM prevalence:
10.2%, 6.8%, 4.5% and 4.4% in AAM, HA, European American (EA) and AA women, respectively. Current
studies are limited to candidate gene investigations with most investigating five to ten known T2D loci and only
one genome-wide association study (GWAS) (468 cases; 1242 controls), in a South-Korean population. AAMs
and HAs are the fastest growing populations in the US. Despite evident racial disparity suggesting a genetic
etiology, no study has evaluated whether this is in part is rooted in differences associated with genetic
ancestry. The overall goals of this proposal are to expand comprehensive genetic investigations of GDM and
related traits by leveraging electronic health records (EHR) and bio-repositories to better understand the
etiology which may inform personalized strategies for screening and prevention. We aim to develop, refine and
validate reproducible and portable bioinformatics-algorithms to identity GDM cases and controls using de-
identified EHR data at Vanderbilt. We will evaluate whether reported race/ethnicity modifies the association
between maternal BMI and GDM in the Vanderbilt EHR database, the synthetic derivative (SD) (>8000 cases;
Aim 1.1). In approximately 2,200 cases and 4,400 controls with genetic data, we will perform a Mendelian
randomization study to test whether genetic instruments of central obesity (waist to hip ratio) or overall obesity
(BMI) are more strongly associated with GDM (Aim 1.2). We will perform the first two-stage trans-ethnic GWAS
of GDM in the US in EA, AA, HA, and AAM women from the SD and replicate associated variants (P < 1x10-6)
in over 1000 GDM cases and many controls from the UK Biobank and Mount Sinai BioME EHR-linked bio-
repository (Aim 2.1). By integrating GWAS data and expression quantitative trait loci (eQTL) data from various
tissues with methods such as S-PrediXcan, we will prioritize candidate causal genes for GDM (Aim 2.2).
Finally, we will explore whether genetically inferred Asian/Native American ancestry proportion is associated
with increased risk of GDM (Aim 3.1) and T2D (Aim 3.2) in HAs. The well-tailored mentored training program
supports the stated research aims and provides the candidate with the protected time to gain appropriate
training in areas in which he lacks fully independent expertise, including phenotyping in the EHR setting,
biomedical informatics and knowledge of gestational diabetes and classification of pregnancy outcomes.
Successful completion of this award will facilitate the candidate's development into an independent multi-
disciplinary researcher ideally prepared to contribute significantly to the fields of gestational diabetes, diabetes
and associated complications, genetic epidemiology, racial disparity and women's health research.
项目概要/摘要
妊娠糖尿病(GDM)是美国最常见的妊娠并发症之一。共享
2 型糖尿病 (T2D) 的病理生理学、家族聚集的证据以及种族差异的证据
所有这些都支持遗传倾向的作用。亚裔美国人 (AAM) 和西班牙裔美国人 (HA) 女性
平均肥胖患病率低于非裔美国 (AA) 女性,但 GDM 患病率较高:
AAM、HA、欧洲裔美国人 (EA) 和 AA 女性的比例分别为 10.2%、6.8%、4.5% 和 4.4%。当前的
研究仅限于候选基因调查,大多数调查五到十个已知的 T2D 位点,并且仅
一项针对韩国人群的全基因组关联研究 (GWAS)(468 例病例;1242 名对照)。空空导弹
HA 和 HA 是美国增长最快的人口。尽管明显的种族差异表明遗传因素
病因学方面,尚无研究评估这是否部分源于与遗传相关的差异
祖先。该提案的总体目标是扩大 GDM 的全面遗传研究和
通过利用电子健康记录 (EHR) 和生物存储库来更好地了解相关特征
病因学可为筛查和预防的个性化策略提供信息。我们的目标是开发、完善和
验证可重复且可移植的生物信息学算法,以使用 de- 来识别 GDM 病例和对照
确定了范德比尔特大学的 EHR 数据。我们将评估所报告的种族/民族是否会改变关联
范德比尔特 EHR 数据库中母亲 BMI 和 GDM 之间的合成衍生物 (SD)(>8000 例;
目标 1.1)。在大约 2,200 个病例和 4,400 个具有遗传数据的对照中,我们将进行孟德尔分析
随机化研究测试中心性肥胖(腰臀比)或整体肥胖的遗传因素
(BMI) 与 GDM 的相关性更强(目标 1.2)。我们将进行首个两阶段跨种族 GWAS
美国 EA、AA、HA 和 AAM 女性中来自 SD 的 GDM 的发生率以及复制相关变异 (P < 1x10-6)
在超过 1000 个 GDM 病例以及来自 UK Biobank 和 Mount Sinai BioME EHR 相关生物的许多对照中
存储库(目标 2.1)。通过整合 GWAS 数据和来自不同来源的表达数量性状位点 (eQTL) 数据
通过 S-PrediXcan 等方法对组织进行分析,我们将优先考虑 GDM 的候选致病基因(目标 2.2)。
最后,我们将探讨基因推断的亚洲/美洲原住民血统比例是否相关
HA 中 GDM(目标 3.1)和 T2D(目标 3.2)的风险增加。精心定制的指导培训计划
支持既定的研究目标,并为候选人提供受保护的时间来获得适当的研究成果
在他缺乏完全独立专业知识的领域接受培训,包括电子病历环境中的表型分析,
生物医学信息学和妊娠糖尿病知识以及妊娠结局的分类。
成功完成该奖项将有助于候选人发展成为独立的多学科人士
学科研究员理想地准备为妊娠糖尿病、糖尿病领域做出重大贡献
及相关并发症、遗传流行病学、种族差异和妇女健康研究。
项目成果
期刊论文数量(1)
专著数量(0)
科研奖励数量(0)
会议论文数量(0)
专利数量(0)
Incidental urinary tract injury and the formation of vesicovaginal fistula at the time of hysterectomy for benign indications.
良性子宫切除术时意外的尿路损伤和膀胱阴道瘘的形成。
- DOI:
- 发表时间:2023-02
- 期刊:
- 影响因子:1.8
- 作者:Butler, Brandy M;Adam, Rony A;Giri, Ayush
- 通讯作者:Giri, Ayush
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{{ truncateString('Ayush Giri', 18)}}的其他基金
Understanding causal mechanisms in preeclampsia through genetic instrumental variables
通过遗传工具变量了解先兆子痫的因果机制
- 批准号:
10345097 - 财政年份:2022
- 资助金额:
$ 14.03万 - 项目类别:
Understanding causal mechanisms in preeclampsia through genetic instrumental variables
通过遗传工具变量了解先兆子痫的因果机制
- 批准号:
10546467 - 财政年份:2022
- 资助金额:
$ 14.03万 - 项目类别:
Influence of genetic variation, genetic ancestry, and obesity on gestational diabetes mellitus risk
遗传变异、遗传血统和肥胖对妊娠期糖尿病风险的影响
- 批准号:
10113596 - 财政年份:2020
- 资助金额:
$ 14.03万 - 项目类别:
Influence of genetic variation, genetic ancestry, and obesity on gestational diabetes mellitus risk
遗传变异、遗传血统和肥胖对妊娠期糖尿病风险的影响
- 批准号:
9891814 - 财政年份:2020
- 资助金额:
$ 14.03万 - 项目类别:
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