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计算生物学时代的直接心脏重编程

Direct Cardiac Reprogramming in the Age of Computational Biology.

作者信息

Ambroise Rachelle, Takasugi Paige, Liu Jiandong, Qian Li

机构信息

Department of Bioinformatics and Computational Biology, University of North Carolina, Chapel Hill, NC 27599, USA.

McAllister Heart Institute, University of North Carolina, Chapel Hill, NC 27599, USA.

出版信息

J Cardiovasc Dev Dis. 2024 Sep 4;11(9):273. doi: 10.3390/jcdd11090273.

Abstract

Heart disease continues to be one of the most fatal conditions worldwide. This is in part due to the maladaptive remodeling process by which ischemic cardiac tissue is replaced with a fibrotic scar. Direct cardiac reprogramming presents a unique solution for restoring injured cardiac tissue through the direct conversion of fibroblasts into induced cardiomyocytes, bypassing the transition through a pluripotent state. Since its inception in 2010, direct cardiac reprogramming using the transcription factors Gata4, Mef2c, and Tbx5 has revolutionized the field of cardiac regenerative medicine. Just over a decade later, the field has rapidly evolved through the expansion of identified molecular and genetic factors that can be used to optimize reprogramming efficiency. The integration of computational tools into the study of direct cardiac reprogramming has been critical to this progress. Advancements in transcriptomics, epigenetics, proteomics, genome editing, and machine learning have not only enhanced our understanding of the underlying mechanisms driving this cell fate transition, but have also driven innovations that push direct cardiac reprogramming closer to clinical application. This review article explores how these computational advancements have impacted and continue to shape the field of direct cardiac reprogramming.

摘要

心脏病仍然是全球最致命的疾病之一。部分原因是适应性重塑过程,即缺血性心脏组织被纤维化瘢痕所取代。直接心脏重编程为恢复受损心脏组织提供了一种独特的解决方案,即通过将成纤维细胞直接转化为诱导性心肌细胞,绕过通过多能状态的转变。自2010年首次提出以来,使用转录因子Gata4、Mef2c和Tbx5进行的直接心脏重编程彻底改变了心脏再生医学领域。仅仅十多年后,该领域通过可用于优化重编程效率的已确定分子和遗传因素的扩展而迅速发展。将计算工具整合到直接心脏重编程研究中对这一进展至关重要。转录组学、表观遗传学、蛋白质组学、基因组编辑和机器学习的进步不仅加深了我们对驱动这种细胞命运转变的潜在机制的理解,还推动了创新,使直接心脏重编程更接近临床应用。这篇综述文章探讨了这些计算进展如何影响并将继续塑造直接心脏重编程领域。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1281/11432431/94d36d8470e3/jcdd-11-00273-g001.jpg

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