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心脏转录因子与非编码 RNA 之间的相互作用导致心房颤动易感性增加。

Interplay between cardiac transcription factors and non-coding RNAs in predisposing to atrial fibrillation.

机构信息

Institute of Health Sciences, University of A Coruña, Campus de Oza, Building El Fortin, E-15006, A Coruña, Spain.

出版信息

J Mol Med (Berl). 2018 Jul;96(7):601-610. doi: 10.1007/s00109-018-1647-4. Epub 2018 May 12.

Abstract

There is growing evidence that putative gene regulatory networks including cardio-enriched transcription factors, such as PITX2, TBX5, ZFHX3, and SHOX2, and their effector/target genes along with downstream non-coding RNAs can play a potentially important role in the process of adaptive and maladaptive atrial rhythm remodeling. In turn, expression of atrial fibrillation-associated transcription factors is under the control of upstream regulatory non-coding RNAs. This review broadly explores gene regulatory mechanisms associated with susceptibility to atrial fibrillation-with key examples from both animal models and patients-within the context of both cardiac transcription factors and non-coding RNAs. These two systems appear to have multiple levels of cross-regulation and act coordinately to achieve effective control of atrial rhythm effector gene expression. Perturbations of a dynamic expression balance between transcription factors and corresponding non-coding RNAs can provoke the development or promote the progression of atrial fibrillation. We also outline deficiencies in current models and discuss ongoing studies to clarify remaining mechanistic questions. An understanding of the function of transcription factors and non-coding RNAs in gene regulatory networks associated with atrial fibrillation risk will enable the development of innovative therapeutic strategies.

摘要

越来越多的证据表明,假定的基因调控网络,包括心脏丰富的转录因子,如 PITX2、TBX5、ZFHX3 和 SHOX2,及其效应物/靶基因以及下游非编码 RNA,可能在适应性和失调性心房节律重构过程中发挥重要作用。反过来,房颤相关转录因子的表达受上游调节性非编码 RNA 的控制。本综述广泛探讨了与房颤易感性相关的基因调控机制,重点介绍了心脏转录因子和非编码 RNA 两方面的动物模型和患者的关键实例。这两个系统似乎具有多层次的交叉调节作用,并协调一致地实现对心房节律效应基因表达的有效控制。转录因子和相应非编码 RNA 之间动态表达平衡的破坏会引发房颤的发生或促进其进展。我们还概述了当前模型的缺陷,并讨论了正在进行的研究,以阐明剩余的机制问题。理解转录因子和非编码 RNA 在与房颤风险相关的基因调控网络中的功能将为创新性治疗策略的发展提供依据。

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