Intrauterine exposure to tobacco smoke, DNA methylation, and vision disorders in preschool children

学龄前儿童宫内烟草烟雾暴露、DNA 甲基化和视力障碍

• 批准号: 10220040
• 负责人: Xuejuan Jiang
• 金额: $ 40.01万
• 依托单位: UNIVERSITY OF SOUTHERN CALIFORNIA
• 依托单位国家: 美国
• 财政年份: 2019
• 资助国家: 美国
• 起止时间: 2019-09-01 至 2024-07-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/10220040
• 关键词: African American; Age; Amblyopia; Bilateral; Biological; Biological Assay; Biological Markers; Biological Process; Birth; Blood; Blood specimen; California; Chemicals; Child; Childhood; Cigarette; Cornea; Cotinine; Cytosine; DNA Methylation; Data; Development; Disease; Disease Outcome; Dose; Early identification; Electronic Nicotine Delivery Systems; Electronic cigarette; Epidemiology; Epigenetic Process; Etiology; Exposure to; Eye diseases; Fetal Development; Fetus; Genetic Diseases; Genetic study; Guanine; Health; Hyperopia; Impairment; Individual; Inherited; Investigation; Knowledge; Late pregnancy; Length; Life; Light; Link; Los Angeles; Low Birth Weight Infant; Measures; Mediating; Metabolism; Methods; Modification; Monitor; Mothers; Neonatal; Neonatal Screening; Nested Case-Control Study; Newborn Infant; Nicotine; Not Hispanic or Latino; Outcome; Patient Self-Report; Phenotype; Play; Population; Population Heterogeneity; Population Study; Predisposition; Pregnancy; Preschool Child; Provider; Public Health; Refractive Errors; Reporting; Research; Resources; Retinal Diseases; Risk; Risk Factors; Role; Scientist; Smoke; Smoking; Source; Spottings; Strabismus; Susceptibility Gene; Systems Development; Testing; Third Pregnancy Trimester; Tobacco; Tobacco smoke; Variant; Vision Disorders; Visual Acuity; aged; base; case control; cognitive function; early childhood; early screening; environmental tobacco smoke; environmental tobacco smoke exposure; fetal; genomic locus; high risk; improved; in vivo; inorganic phosphate; insight; intrauterine environment; maternal cigarette smoking; multi-ethnic; neuron development; nicotine replacement; novel; prevent; public health relevance; response; screening; screening program; smoking during pregnancy; tool; treatment response; uptake; vision development; visual motor

Project Summary Vision disorders in early childhood, such as strabismus, amblyopia and high hyperopia, can significantly impair the development of visual, motor, and cognitive functions. There is a need for better understanding of their disease etiology which remains mostly unknown and methods for early identification of these disorders, which still remain undetected in many children until their older ages when response to treatment is worse. Maternal smoking during pregnancy (MSP), especially sustained smoking that persisted into third trimester, has been consistently associated with several pediatric vision disorders including hyperopia, strabismus, and bilateral amblyopia, and nicotine is considered as a key chemical responsible for the effects. The broad impact of MSP on multiple vision disorders indicates that disturbance of intrauterine environment and fetal development may play an important role in the development of vision disorders that occur very early in life. However, intrauterine exposure to tobacco smoke or nicotine are not well captured by self-reported MSP, due to under-reporting, exposure to overlooked sources of smoke or nicotine (e.g., environmental tobacco smoke, nicotine replacement therapy), and variation in the uptake and metabolism of tobacco smoke by the mother and in the fetal response to intrauterine disturbance. Objective and reliable measures of biologically effective dose of intrauterine exposure to tobacco smoke or early biological effects of this exposure are needed. There have been major advances in identifying specific genomic loci that are differentially methylated in newborns in response to MSP and accumulating evidence linking alterations to DNA methylation at birth with childhood diseases and outcomes such as low birth weight. These led us to hypothesize that epigenetic changes can alter the development of the vision system in the fetus, leading to the development of vision disorders in early childhood. To test this hypothesis, we propose to conduct a case-control study nested within the Multiethnic Pediatric Eye Disease Study (MEPEDS) and retrieve neonatal dried blood spots (DBSs) that had been collected by the California State’s Genetic Disease Screening Program from MEPEDS children at their birth. Using these biospecimens, we will 1) assess the relationship of cotinine level in DBS and tobacco dosimeter based on DNA methylation marks, in comparison to self-reported MSP, with strabismus, bilateral decreased visual acuity, and hyperopia in 1508 preschool children; and 2) investigate epigenetic susceptibility loci for hyperopia by comparing DNA methylation in neonatal DBS from 508 cases and an equal number of random controls. Findings from this proposed study will have a great impact on assessing population and individual risks from intrauterine exposure to different sources of tobacco smoke, understanding underlying biological mechanisms, early screening of pediatric vision disorders, and preventing adverse impacts of these vision disorders.

项目摘要 儿童早期的视力障碍，如斜视、弱视和高度远视， 视觉、运动和认知功能的发展。有必要更好地了解他们的 本发明还涉及早期鉴定这些疾病的方法， 在许多儿童中仍然未被发现，直到他们年龄较大时，对治疗的反应更差。产妇 怀孕期间吸烟（MSP），特别是持续到妊娠晚期的持续吸烟， 一直与几种儿童视力障碍相关，包括远视、斜视和双侧 尼古丁被认为是造成这种影响的关键化学物质。MSP的广泛影响 表明宫内环境和胎儿发育障碍可能 在生命早期发生的视力障碍的发展中起着重要作用。然而，子宫内 由于报告不足，自我报告的MSP无法很好地记录烟草烟雾或尼古丁暴露， 暴露于被忽视的烟雾或尼古丁源（例如，环境烟草烟雾，尼古丁 替代疗法），以及母亲对烟草烟雾的吸收和代谢以及 胎儿对宫内紊乱的反应。生物有效剂量的客观可靠的测量方法 子宫内暴露于烟草烟雾或这种暴露的早期生物学效应是必要的。已经 在鉴定新生儿中差异甲基化的特定基因组位点方面取得了重大进展， 对MSP的反应，以及将出生时的DNA甲基化改变与儿童期联系起来的证据 疾病和结果，如低出生体重。这些使我们假设，表观遗传变化可以 改变胎儿视觉系统的发育，导致早期视力障碍的发展。 童年.为了验证这一假设，我们建议进行一项嵌套在多种族研究中的病例对照研究。 儿童眼病研究（MEPEDS），并检索新生儿干血斑（DBS）， 由加州州的遗传疾病筛查项目从MEPEDS儿童出生时收集。 利用这些生物样本，我们将：1）评估DBS中可替宁水平与烟草剂量计的关系 基于DNA甲基化标记，与自我报告的MSP相比，斜视，双侧减少 1508名学龄前儿童的视力和远视; 2）调查表观遗传易感性位点， 通过比较508例新生儿DBS和相同数量的随机对照的DNA甲基化， 对照这项拟议研究的结果将对评估人口和个人 子宫内暴露于不同来源的烟草烟雾的风险，了解潜在的生物学 机制，早期筛查儿童视力障碍，并防止这些视力的不良影响， 紊乱