首页> 美国卫生研究院文献>Scoliosis and Spinal Disorders >Adolescent idiopathic scoliosis (AIS) environment exposome and epigenetics: a molecular perspective of postnatal normal spinal growth and the etiopathogenesis of AIS with consideration of a network approach and possible implications for medical therapy
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Adolescent idiopathic scoliosis (AIS) environment exposome and epigenetics: a molecular perspective of postnatal normal spinal growth and the etiopathogenesis of AIS with consideration of a network approach and possible implications for medical therapy

机译:青少年特发性脊柱侧凸(AIS)环境暴露和表观遗传学:考虑网​​络方法及其对药物治疗的影响从出生后正常脊柱生长和AIS的发病机理的分子观点出发

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摘要

Genetic factors are believed to play an important role in the etiology of adolescent idiopathic scoliosis (AIS). Discordant findings for monozygotic (MZ) twins with AIS show that environmental factors including different intrauterine environments are important in etiology, but what these environmental factors may be is unknown. Recent evidence for common chronic non-communicable diseases suggests epigenetic differences may underlie MZ twin discordance, and be the link between environmental factors and phenotypic differences. DNA methylation is one important epigenetic mechanism operating at the interface between genome and environment to regulate phenotypic plasticity with a complex regulation across the genome during the first decade of life. The word exposome refers to the totality of environmental exposures from conception onwards, comprising factors in external and internal environments. The word exposome is used here also in relation to physiologic and etiopathogenetic factors that affect normal spinal growth and may induce the deformity of AIS. In normal postnatal spinal growth we propose a new term and concept, physiologic growth-plate exposome for the normal processes particularly of the internal environments that may have epigenetic effects on growth plates of vertebrae. In AIS, we propose a new term and concept pathophysiologic scoliogenic exposome for the abnormal processes in molecular pathways particularly of the internal environment currently expressed as etiopathogenetic hypotheses; these are suggested to have deforming effects on the growth plates of vertebrae at cell, tissue, structure and/or organ levels that are considered to be epigenetic. New research is required for chromatin modifications including DNA methylation in AIS subjects and vertebral growth plates excised at surgery. In addition, consideration is needed for a possible network approach to etiopathogenesis by constructing AIS diseasomes. These approaches may lead through screening, genetic, epigenetic, biochemical, metabolic phenotypes and pharmacogenomic research to identify susceptible individuals at risk and modulate abnormal molecular pathways of AIS. The potential of epigenetic-based medical therapy for AIS cannot be assessed at present, and must await new research derived from the evaluation of epigenetic concepts of spinal growth in health and deformity. The tenets outlined here for AIS are applicable to other musculoskeletal growth disorders including infantile and juvenile idiopathic scoliosis.
机译:人们认为遗传因素在青少年特发性脊柱侧凸(AIS)的病因中起着重要作用。与AIS的单卵(MZ)双胞胎的不一致发现表明,包括不同宫内环境在内的环境因素在病因学中很重要,但是这些环境因素可能是未知的。有关常见的慢性非传染性疾病的最新证据表明,表观遗传学差异可能是MZ双胞胎不一致的基础,并且是环境因素与表型差异之间的联系。 DNA甲基化是一种重要的表观遗传机制,作用于基因组与环境之间的界面,以在生命的头十年中对整个基因组进行复杂的调节来调节表型可塑性。 “暴露”一词是指从受孕开始的所有环境暴露,包括外部和内部环境中的因素。在这里,“暴露小体”一词也与影响正常脊柱生长并可能导致AIS畸形的生理和病因相关。在正常的产后脊柱生长中,我们提出了一个新的术语和概念,即生理生长板暴露液,用于正常过程,尤其是可能对椎骨生长板产生表观遗传学影响的内部环境。在AIS中,我们提出了一个新的术语和概念病理生理性脊柱侧凸暴露,用于分子途径中的异常过程,特别是目前表示为病因假说的内部环境中的异常过程。这些被认为会对被认为是表观遗传的细胞,组织,结构和/或器官水平的椎骨生长板产生变形作用。染色质修饰需要新的研究,包括在AIS受试者和在手术中切除的椎骨生长板中的DNA甲基化。此外,还需要考虑通过构建AIS疾病来实现可能的网络方法来进行病原学研究。这些方法可能会通过筛选,遗传,表观遗传,生化,代谢表型和药物基因组学研究,以识别有风险的易感个体并调节AIS的异常分子途径。目前尚不能评估基于表观遗传学的AIS药物治疗的潜力,并且必须等待对健康和畸形脊柱生长的表观遗传学概念进行评估的新研究。此处概述的AIS原则适用于其他肌肉骨骼生长疾病,包括婴儿和青少年特发性脊柱侧弯。

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