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高通量测序时代的生物标志物开发中的胎儿重编程定量。

Quantifying Fetal Reprogramming for Biomarker Development in the Era of High-Throughput Sequencing.

机构信息

Division of Neonatology, Department of Pediatrics, Loma Linda University School of Medicine, Loma Linda, CA 92350, USA.

PXT Research & Data Analytics, LLC, Rancho Cucamonga, CA 91739, USA.

出版信息

Genes (Basel). 2021 Feb 25;12(3):329. doi: 10.3390/genes12030329.

Abstract

Gestational hypertensive disorders continue to threaten the well-being of pregnant women and their offspring. The only current definitive treatment for gestational hypertensive disorders is delivery of the fetus. The optimal timing of delivery remains controversial. Currently, the available clinical tools do not allow for assessment of fetal stress in its early stages. Placental insufficiency and fetal growth restriction secondary to gestational hypertensive disorders have been shown to have long-term impacts on offspring health even into their adulthood, becoming one of the major focuses of research in the field of developmental origins of health and disease. Fetal reprogramming was introduced to describe the long-lasting effects of the toxic intrauterine environment on the growing fetus. With the advent of high-throughput sequencing, there have been major advances in research attempting to quantify fetal reprogramming. Moreover, genes that are found to be differentially expressed as a result of fetal reprogramming show promise in the development of transcriptional biomarkers for clinical use in detecting fetal response to placental insufficiency. In this review, we will review key pathophysiology in the development of placental insufficiency, existing literature on high-throughput sequencing in the study of fetal reprogramming, and considerations regarding research design from our own experience.

摘要

妊娠高血压疾病仍然威胁着孕妇及其后代的健康。目前治疗妊娠高血压疾病的唯一明确方法是分娩胎儿。分娩的最佳时机仍存在争议。目前,现有的临床工具无法在早期评估胎儿的应激情况。妊娠高血压疾病引起的胎盘功能不全和胎儿生长受限已被证明对后代的健康有长期影响,甚至在成年后仍有影响,这成为健康与疾病发育起源领域研究的主要关注点之一。胎儿重编程被引入以描述有毒的宫内环境对生长中胎儿的持久影响。随着高通量测序的出现,在试图量化胎儿重编程的研究方面取得了重大进展。此外,由于胎儿重编程而差异表达的基因在开发转录生物标志物方面显示出了希望,这些生物标志物可用于临床检测胎儿对胎盘功能不全的反应。在这篇综述中,我们将回顾胎盘功能不全的关键病理生理学、高通量测序在胎儿重编程研究中的现有文献,以及我们自身经验对研究设计的考虑。

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