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Literature DB >> 33718351

Sall4 and Myocd Empower Direct Cardiac Reprogramming From Adult Cardiac Fibroblasts After Injury.

Hong Zhao^1,2, Yi Zhang³, Xiaochan Xu⁴, Qiushi Sun³, Chunyan Yang^1,2, Hao Wang^1,2,5, Junbo Yang^1,2, Yang Yang^1,2, Xiaochun Yang^1,2, Yi Liu³, Yang Zhao^1,2,5,6.

Abstract

Direct conversion of fibroblasts into induced cardiomyocytes (iCMs) holds promising potential to generate functional cardiomyocytes for drug development and clinical applications, especially for direct in situ heart regeneration by delivery of reprogramming genes into adult cardiac fibroblasts in injured hearts. For a decade, many cocktails of transcription factors have been developed to generate iCMs from fibroblasts of different tissues in vitro and some were applied in vivo. Here, we aimed to develop genetic cocktails that induce cardiac reprogramming directly in cultured cardiac fibroblasts isolated from adult mice with myocardial infarction (MICFs), which could be more relevant to heart diseases. We found that the widely used genetic cocktail, Gata4, Mef2c, and Tbx5 (GMT) were inefficient in reprogramming cardiomyocytes from MICFs. In a whole well of a 12-well plate, less than 10 mCherry+ cells (<0.1%) were observed after 2 weeks of GMT infection with Myh6-reporter transgenic MICFs. By screening 22 candidate transcription factors predicted through analyzing the gene regulatory network of cardiac development, we found that five factors, GMTMS (GMT plus Myocd and Sall4), induced more iCMs expressing the cardiac structural proteins cTnT and cTnI at a frequency of about 22.5 ± 2.7% of the transduced MICFs at day 21 post infection. What is more, GMTMS induced abundant beating cardiomyocytes at day 28 post infection. Specifically, Myocd contributed mainly to inducing the expression of cardiac proteins, while Sall4 accounted for the induction of functional properties, such as contractility. RNA-seq analysis of the iCMs at day 28 post infection revealed that they were reprogrammed to adopt a cardiomyocyte-like gene expression profile. Overall, we show here that Sall4 and Myocd play important roles in cardiac reprogramming from MICFs, providing a cocktail of genetic factors that have potential for further applications in in vivo cardiac reprogramming.

Entities: CellLine Chemical Disease Gene Species

Keywords: MICF; Myocd; Sall4; cardiac reprogramming; high efficiency; myofibroblast

Year: 2021 PMID： 33718351 PMCID： PMC7953844 DOI： 10.3389/fcell.2021.608367

Source DB: PubMed Journal: Front Cell Dev Biol ISSN： 2296-634X

48 in total

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Authors: Tilanthi M Jayawardena; Bakytbek Egemnazarov; Elizabeth A Finch; Lunan Zhang; J Alan Payne; Kumar Pandya; Zhiping Zhang; Paul Rosenberg; Maria Mirotsou; Victor J Dzau
Journal: Circ Res Date: 2012-04-26 Impact factor: 17.367

2. Activation of cardiac gene expression by myocardin, a transcriptional cofactor for serum response factor.

Authors: D Wang; P S Chang; Z Wang; L Sutherland; J A Richardson; E Small; P A Krieg; E N Olson
Journal: Cell Date: 2001-06-29 Impact factor: 41.582

3. Reprogramming of human fibroblasts toward a cardiac fate.

Authors: Young-Jae Nam; Kunhua Song; Xiang Luo; Edward Daniel; Kaleb Lambeth; Katherine West; Joseph A Hill; J Michael DiMaio; Linda A Baker; Rhonda Bassel-Duby; Eric N Olson
Journal: Proc Natl Acad Sci U S A Date: 2013-03-04 Impact factor: 11.205

4. Transcriptomic Profiling Maps Anatomically Patterned Subpopulations among Single Embryonic Cardiac Cells.

Authors: Guang Li; Adele Xu; Sopheak Sim; James R Priest; Xueying Tian; Tooba Khan; Thomas Quertermous; Bin Zhou; Philip S Tsao; Stephen R Quake; Sean M Wu
Journal: Dev Cell Date: 2016-11-10 Impact factor: 12.270

5. A robust and high-throughput Cre reporting and characterization system for the whole mouse brain.

Authors: Linda Madisen; Theresa A Zwingman; Susan M Sunkin; Seung Wook Oh; Hatim A Zariwala; Hong Gu; Lydia L Ng; Richard D Palmiter; Michael J Hawrylycz; Allan R Jones; Ed S Lein; Hongkui Zeng
Journal: Nat Neurosci Date: 2009-12-20 Impact factor: 24.884

Review 6. Myofibroblast-mediated mechanisms of pathological remodelling of the heart.

Authors: Karl T Weber; Yao Sun; Syamal K Bhattacharya; Robert A Ahokas; Ivan C Gerling
Journal: Nat Rev Cardiol Date: 2012-12-04 Impact factor: 32.419

7. Targeted Ablation of Periostin-Expressing Activated Fibroblasts Prevents Adverse Cardiac Remodeling in Mice.

Authors: Harmandeep Kaur; Mikito Takefuji; C Y Ngai; Jorge Carvalho; Julia Bayer; Astrid Wietelmann; Ansgar Poetsch; Soraya Hoelper; Simon J Conway; Helge Möllmann; Mario Looso; Christian Troidl; Stefan Offermanns; Nina Wettschureck
Journal: Circ Res Date: 2016-05-02 Impact factor: 17.367

8. High-efficiency reprogramming of fibroblasts into cardiomyocytes requires suppression of pro-fibrotic signalling.

Authors: Yuanbiao Zhao; Pilar Londono; Yingqiong Cao; Emily J Sharpe; Catherine Proenza; Rebecca O'Rourke; Kenneth L Jones; Mark Y Jeong; Lori A Walker; Peter M Buttrick; Timothy A McKinsey; Kunhua Song
Journal: Nat Commun Date: 2015-09-10 Impact factor: 14.919

Sall4 and Myocd Empower Direct Cardiac Reprogramming From Adult Cardiac Fibroblasts After Injury.

1. MicroRNA-mediated in vitro and in vivo direct reprogramming of cardiac fibroblasts to cardiomyocytes.

2. Activation of cardiac gene expression by myocardin, a transcriptional cofactor for serum response factor.

3. Reprogramming of human fibroblasts toward a cardiac fate.

4. Transcriptomic Profiling Maps Anatomically Patterned Subpopulations among Single Embryonic Cardiac Cells.

5. A robust and high-throughput Cre reporting and characterization system for the whole mouse brain.

Review 6. Myofibroblast-mediated mechanisms of pathological remodelling of the heart.

7. Targeted Ablation of Periostin-Expressing Activated Fibroblasts Prevents Adverse Cardiac Remodeling in Mice.

8. High-efficiency reprogramming of fibroblasts into cardiomyocytes requires suppression of pro-fibrotic signalling.

9. Direct reprogramming of human fibroblasts toward a cardiomyocyte-like state.

10. Genetic lineage tracing defines myofibroblast origin and function in the injured heart.

1. Fibroblast transition to an endothelial "trans" state improves cell reprogramming efficiency.

Review 2. Improving Cardiac Reprogramming for Heart Regeneration in Translational Medicine.