Early childhood nutrition and adult metabolomic and cardiometabolic profiles
幼儿营养和成人代谢组学和心脏代谢特征
基本信息
- 批准号:9254217
- 负责人:
- 金额:$ 55.91万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2014
- 资助国家:美国
- 起止时间:2014-04-10 至 2019-03-31
- 项目状态:已结题
- 来源:
- 关键词:AcuteAddressAdultAffectAgeAttenuatedBiological AssayBiological MarkersBirthBlood capillariesBlood specimenCaloriesCentral AmericaCharacteristicsChildChild MalnutritionChildhoodChronicClinicalCohort StudiesCollaborationsCollectionCommunicable DiseasesCommunitiesConceptionsCountryDataData AnalysesDatabasesDevelopmentDiabetes MellitusDiagnosisDietary InterventionDiseaseElementsEnsureEpidemicEtiologyEventExposure toFailureFutureGlucoseGrowthGuatemalaGuatemalanHealthHigh PrevalenceHumanIncomeInfectionInflammationInstitutesInterventionIntervention TrialLaboratoriesLifeLife Cycle StagesLinkLipidsLong-Term EffectsLongevityMalignant NeoplasmsMalnutritionMethodsNutritionalObesityPanamaPaperPerinatalPositioning AttributePrevalenceProspective cohortProspective cohort studyProteinsPublishingRandomized Controlled TrialsRecording of previous eventsResearchResearch PersonnelResolutionRisk FactorsRoleSamplingSupplementationSurveysTestingTimeUniversitiesUpdateWorkburden of illnesscardiometabolic riskcohortcombatdisability-adjusted life yearsdisorder riskearly childhoodeffective interventionexperienceimprovedinnovationlow and middle-income countriesmembermetabolomemetabolomicsmodifiable riskmultidisciplinarynovel markernutritionpublic health relevanceresearch facilityresponsesocioeconomicsstudy population
项目摘要
DESCRIPTION (provided by applicant): Nutrition and infection are key determinants of child growth and survival. Chronic inflammation, which results in part from an increased lifetime burden of infectious disease, is an underlying determinant of adult cardiometabolic disease. The modifiability of this risk by improving nutrition in early life is unknown. Our principal objectiveis to determine whether improvements in early-life nutrition can attenuate the development of cardiometabolic risk. We will collect new data from the INCAP (Guatemala) Nutrition Supplementation Trial cohort. From 1969-77, 2392 children received atole, a high protein and calorie supplement, or fresco, a low calorie drink, for up to 8 y. Children who received atole in the first 3 y of life grew better in childhood and recovered more quickly from diarrheal illness episodes than did children who received fresco. We have followed this cohort prospectively. We propose to re-contact the surviving members of the cohort. The cohort will be 38-53 y old, an ideal age to assess cardiometabolic risk. We will conduct clinical examinations, including (for the first time in this cohort) collection of biomarkers of cardiometabolic risk. We will assay the samples for established and novel biomarkers, including highly innovative metabolomic profiling. We will update and enhance the extensive life-course data that we collected in previous surveys. We will link the new data to our existing rich database to address critical questions regarding the long-term effects on cardiometabolic health of both chronic under-nutrition and an effective intervention to combat under-nutrition, in the context of a community-randomized trial that controls for otherwise intractable questions of endogeneity. The study will be unique in its ability to address unanswered questions relating to early life determinants of adult health. This prospectively-studied cohort has reached an age where the prevalence of cardiometabolic risk is non-negligible. The highly productive research team has extensive experience with survey work among this cohort, demonstrated capacity to link data across study waves, and extensive experience with the appropriate field methods, laboratory methods, and statistical approaches to data analysis. The resulting extensive repository of data and samples will enhance the value of the cohort for future research. Taken together, these elements ensure that the study will be well positioned to successfully address critical understudied questions in human health and development.
描述(由申请人提供):营养和感染是儿童生长和生存的关键决定因素。慢性炎症,部分原因是终身感染性疾病负担增加,是成人心脏代谢疾病的潜在决定因素。通过改善生命早期的营养来改变这种风险是未知的。我们的主要目的是确定早期营养的改善是否可以减轻心脏代谢风险的发展。我们将从INCAP(危地马拉)营养补充试验队列中收集新数据。从1969年到1977年,2392名儿童接受了atole(一种高蛋白质和卡路里的补充剂)或fresco(一种低卡路里的饮料),最长8年。在生命的前3年接受atole的儿童在童年时期生长得更好,并且比接受fresco的儿童更快地从腹泻疾病中恢复过来。我们前瞻性地跟踪了这一队列。我们建议重新联系幸存者。该队列将为38-53岁,这是评估心脏代谢风险的理想年龄。我们将进行临床检查,包括(本队列首次)收集心脏代谢风险的生物标志物。我们将分析样本中已建立和新的生物标志物,包括高度创新的代谢组学分析。我们将更新和加强我们在以前的调查中收集的广泛的生命过程数据。我们将把新的数据与我们现有的丰富数据库联系起来,以解决有关慢性营养不良对心脏代谢健康的长期影响以及有效干预以对抗营养不良的关键问题,在社区随机试验的背景下,控制其他棘手的内分泌问题。这项研究将是独一无二的,它能够解决与成人健康的早期生活决定因素有关的悬而未决的问题。该前瞻性研究队列已达到心脏代谢风险患病率不可忽略的年龄。高效的研究团队在这一群体中的调查工作方面拥有丰富的经验,证明了跨研究波链接数据的能力,以及在适当的实地方法,实验室方法和数据分析统计方法方面的丰富经验。由此产生的广泛的数据和样本库将提高队列对未来研究的价值。总之,这些因素确保了研究将能够成功地解决人类健康和发展中研究不足的关键问题。
项目成果
期刊论文数量(0)
专著数量(0)
科研奖励数量(0)
会议论文数量(0)
专利数量(0)
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ARYEH DAVID STEIN其他文献
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{{ truncateString('ARYEH DAVID STEIN', 18)}}的其他基金
Adult epigenetics and telomere length in relation to improved nutrition in early life
成人表观遗传学和端粒长度与改善早期营养有关
- 批准号:
10562425 - 财政年份:2023
- 资助金额:
$ 55.91万 - 项目类别:
Early childhood nutrition and adult metabolomic and cardiometabolic profiles
幼儿营养和成人代谢组学和心脏代谢特征
- 批准号:
9058129 - 财政年份:2014
- 资助金额:
$ 55.91万 - 项目类别:
Early childhood nutrition and adult metabolomic and cardiometabolic profiles
幼儿营养和成人代谢组学和心脏代谢特征
- 批准号:
8630478 - 财政年份:2014
- 资助金额:
$ 55.91万 - 项目类别:
Education and Health Across the Life course in Guatemala
危地马拉终生教育和健康
- 批准号:
7007346 - 财政年份:2004
- 资助金额:
$ 55.91万 - 项目类别:
Education and Health Across the Life course in Guatemala
危地马拉终生教育和健康
- 批准号:
6849299 - 财政年份:2004
- 资助金额:
$ 55.91万 - 项目类别:
Education and Health Across the Life course in Guatemala
危地马拉终生教育和健康
- 批准号:
6736658 - 财政年份:2004
- 资助金额:
$ 55.91万 - 项目类别:
Zinc, Mental Health and School Performance in Mexico
墨西哥的锌、心理健康和学校表现
- 批准号:
7233666 - 财政年份:2004
- 资助金额:
$ 55.91万 - 项目类别:
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