<i>pouC</i> Regulates Expression of <i>bmp4</i> During Atrioventricular Canal Formation in Zebrafish

Bhakta, Minoti; Padanad, Mahesh S.; Harris, Jonathan; Lubczyk, Christina; Amatruda, James F.; Munshi, Nikhil V.

doi:10.1002/dvdy.2

Cited by 3 publications

(2 citation statements)

References 89 publications

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“…The expression of heg1 in heart was twenty times higher than that in body tissues ( Figure 1 D). As tissue-specific markers, myosin heavy chain 6 ( myh6 ) is highly expressed in atrium [ 31 ], and fatty acid binding protein 2 ( fabp2/ifabp ) is known to be specifically expressed in intestinal epithelium [ 32 ]. As shown in Figure 1 E,F, the expression of myh6 in zebrafish cardiac tissue was more than 800 times higher than that in other tissues, while the expression level of ifabp in purified cardiac tissues was very low ( Figure 1 E,F).…”

Section: Resultsmentioning

confidence: 99%

Generation and Application of the Zebrafish heg1 Mutant as a Cardiovascular Disease Model

Wang

et al. 2020

Biomolecules

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Cardiovascular disease (CVD) is the leading cause of global mortality, which has caused a huge burden on the quality of human life. Therefore, experimental animal models of CVD have become essential tools for analyzing the pathogenesis, developing drug screening, and testing potential therapeutic strategies. In recent decades, zebrafish has entered the field of CVD as an important model organism. HEG1, a heart development protein with EGF like domains 1, plays important roles in the development of vertebrate cardiovascular system. Loss of HEG1 will affect the stabilization of vascular endothelial cell connection and eventually lead to dilated cardiomyopathy (DCM). Here, we generated a heg1-specific knockout zebrafish line using CRISPR/Cas9 technology. Zebrafish heg1 mutant demonstrated severe cardiovascular malformations, including atrial ventricular enlargement, heart rate slowing, venous thrombosis and slow blood flow, which were similar to human heart failure and thrombosis phenotype. In addition, the expression of zebrafish cardiac and vascular markers was abnormal in heg1 mutants. In order to apply zebrafish heg1 mutant in cardiovascular drug screening, four Traditional Chinese Medicine (TCM) herbs and three Chinese herbal monomers were used to treat heg1 mutant. The pericardial area, the distance between sinus venosus and bulbus arteriosus (SV-BA), heart rate, red blood cells (RBCs) accumulation in posterior cardinal vein (PCV), and blood circulation in the tail vein were measured to evaluate the therapeutic effects of those drugs on DCM and thrombosis. Here, a new zebrafish model of DCM and thrombosis was established, which was verified to be suitable for drug screening of cardiovascular diseases. It provided an alternative method for traditional in vitro screening, and produced potential clinical related drugs in a rapid and cost-effective way.

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Section: Resultsmentioning

confidence: 99%

Generation and Application of the Zebrafish heg1 Mutant as a Cardiovascular Disease Model

Wang

et al. 2020

Biomolecules

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“…The remaining eight TFs (ZNF524, CREB3L1, MYPOP, SOX8, POU6F1, HOXD3, ZFHX3 and HMG20B) had unknown regulatory roles in heart functions but there are some suggestive evidence to support their importance. For example, the orthologous gene of Pou6f1 is pouC in zebrafish whose knockdown impairs cardiac morphogenesis and affects cardiovascular function ( 61 ).…”

Section: Resultsmentioning

confidence: 99%

Taiji-reprogram: a framework to uncover cell-type specific regulators and predict cellular reprogramming cocktails

Wang

Liu

Chen

et al. 2021

NAR Genomics and Bioinformatics

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Cellular reprogramming is a promising technology to develop disease models and cell-based therapies. Identification of the key regulators defining the cell type specificity is pivotal to devising reprogramming cocktails for successful cell conversion but remains a great challenge. Here, we present a systems biology approach called Taiji-reprogram to efficiently uncover transcription factor (TF) combinations for conversion between 154 diverse cell types or tissues. This method integrates the transcriptomic and epigenomic data to construct cell-type specific genetic networks and assess the global importance of TFs in the network. Comparative analysis across cell types revealed TFs that are specifically important in a particular cell type and often tightly associated with cell-type specific functions. A systematic search of TFs with differential importance in the source and target cell types uncovered TF combinations for desired cell conversion. We have shown that Taiji-reprogram outperformed the existing methods to better recover the TFs in the experimentally validated reprogramming cocktails. This work not only provides a comprehensive catalog of TFs defining cell specialization but also suggests TF combinations for direct cell conversion.

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Atrioventricular Septal Defect (AVSD)

Dabbagh

Adachi²

2023

Congenital Heart Disease in Pediatric and Adult Patients

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pouC Regulates Expression of bmp4 During Atrioventricular Canal Formation in Zebrafish

Cited by 3 publications

References 89 publications

Generation and Application of the Zebrafish heg1 Mutant as a Cardiovascular Disease Model

Generation and Application of the Zebrafish heg1 Mutant as a Cardiovascular Disease Model

Taiji-reprogram: a framework to uncover cell-type specific regulators and predict cellular reprogramming cocktails

Atrioventricular Septal Defect (AVSD)

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