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首页> 外文期刊>Journal of Molecular Endocrinology >Non-coding genome functions in diabetes
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Non-coding genome functions in diabetes

机译:糖尿病的非编码基因组功能

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摘要

Most of the genetic variation associated with diabetes, through genome-wide association studies, does not reside in protein-coding regions, making the identification of functional variants and their eventual translation to the clinic challenging. In recent years, high-throughput sequencing-based methods have enabled genome-scale high-resolution epigenomic profiling in a variety of human tissues, allowing the exploration of the human genome outside of the well-studied coding regions. These experiments unmasked tens of thousands of regulatory elements across several cell types, including diabetes-relevant tissues, providing new insights into their mechanisms of gene regulation. Regulatory landscapes are highly dynamic and cell-type specific and, being sensitive to DNA sequence variation, can vary with individual genomes. The scientific community is now in place to exploit the regulatory maps of tissues central to diabetes etiology, such as pancreatic progenitors and adult islets. This giant leap forward in the understanding of pancreatic gene regulation is revolutionizing our capacity to discriminate between functional and non-functional non-coding variants, opening opportunities to uncover regulatory links between sequence variation and diabetes susceptibility. In this review, we focus on the non-coding regulatory landscape of the pancreatic endocrine cells and provide an overview of the recent developments in this field.
机译:通过全基因组关联研究,与糖尿病相关的大多数遗传变异并不存在于蛋白质编码区域,这使得功能变异的鉴定及其最终向临床的翻译具有挑战性。近年来,基于高通量测序的方法已使各种人体组织中的基因组规模的高分辨率表观基因组分析成为可能,从而使人们可以在经过充分研究的编码区之外探索人类基因组。这些实验揭示了包括糖尿病相关组织在内的几种细胞类型中成千上万的调控元件,为他们的基因调控机制提供了新见解。调控环境是高度动态的,并且是细胞类型特异性的,并且对DNA序列变化敏感,可以随单个基因组而变化。现在,科学界已经可以利用糖尿病病因学的重要组织(例如胰腺祖细胞和成年胰岛)的调控图谱。在了解胰腺基因调控方面的这一巨大飞跃正在彻底改变我们区分功能性和非功能性非编码变异的能力,为揭示序列变异与糖尿病易感性之间的调控联系提供了机会。在这篇综述中,我们着眼于胰腺内分泌细胞的非编码调控态势,并概述了该领域的最新发展。

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