Efficient Direct Reprogramming of Mature Amniotic Cells into Endothelial Cells by ETS Factors and TGFβ Suppression

Ginsberg, Michael; James, Daylon; Ding, Bi-Sen; Nolan, Daniel J.; Geng, Fuqiang; Butler, Jason M.; Schachterle, William; Pulijaal, Venkat; Mathew, Susan; Chasen, Stephen T.; Xiang, Jenny; Rosenwaks, Zev; Shido, Koji; Elemento, Olivier; Rabbany, Sina Y.; Rafii, Shahin

doi:10.1016/j.cell.2012.09.032

Cited by 207 publications

(217 citation statements)

References 46 publications

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“…It is increasingly clear that obtaining ESC-derived cells with clinical quality by existing methods is a difficult task. Based on the same principle and methodology for iPSC reprogramming, a recent study demonstrated that forced expression of three transfection factors (Etv2, Fli1, and Erg1) that control vascular differentiation effectively converted hESCs to endothelial cells with significantly increased yield and maturity [23,45]. This study demonstrates that intervention at the transcriptional level can provide a strong internal driving force for cell-specific differentiation.…”

Section: Discussionmentioning

confidence: 99%

“…This study demonstrates that intervention at the transcriptional level can provide a strong internal driving force for cell-specific differentiation. However, the expression of the aforementioned transcription factors in that study was also mediated by viral vectors [23]. Using synthetic mRNA as an alternative gene expression approach could avoid the safety concerns associated with viral vectors.…”

Section: Discussionmentioning

confidence: 99%

“…It is conceivable that the inefficient differentiation of existing methods is, at least in part, due to insufficient transcription activation during in vitro differentiation. A recent study reported that hESCs can be effectively differentiated into endothelial cells by viral vectormediated expression of transcription factors that control vascular differentiation [23], demonstrating that intervention at the transcription level can provide a much stronger driving force for ESC differentiation into a specific cell fate.…”

Section: Introductionmentioning

confidence: 99%

“…To further determine the functionality and compatibility of synthetic mRNA with mESCs, we transfected D3 cells with the Etv2 mRNA (m 7 GpppA-Etv2-polyA), a member of the E-twenty-six (ETS) transcription factor family that directly transactivates several genes required for vascular development [23,45]. As shown in Fig.…”

mentioning

confidence: 99%

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Mouse Embryonic Stem Cells Have Underdeveloped Antiviral Mechanisms That Can Be Exploited for the Development of mRNA-Mediated Gene Expression Strategy

Wang

Teng

Spangler

et al. 2014

Stem Cells and Development

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We have recently reported that mouse embryonic stem cells (mESCs) are deficient in expressing type I interferons (IFN) when exposed to viral infection and double-stranded RNA. In this study, we extended our investigation and demonstrated that single-stranded RNA and protein-encoding mRNA can induce strong IFN expression and cytotoxicity in fibroblasts and epithelial cells, but none of the effects associated with these antiviral responses were observed in mESCs. Our results provided additional data to support the conclusion that mESCs are intrinsically deficient in antiviral responses. While our findings represent a novel feature of mESCs that in itself is important for understanding innate immunity development, we exploited this property to develop a novel mRNA-mediated gene expression cell model. Direct introduction of synthetic mRNA to express desired genes has been shown as an effective alternative to DNA/viral vector-based gene expression. However, a major biological challenge is that a synthetic mRNA is detected as a viral RNA analog by the host cell, resulting in a series of adverse effects associated with antiviral responses. We demonstrate that the lack of antiviral responses in mESCs effectively avoids this problem. mESCs can tolerate repeated transfection and effectively express proteins from their synthetic mRNA with expected biological functions, as demonstrated by the expression of green fluorescent protein and the transcription factor Etv2. Therefore, mRNA-based gene expression could be developed into a novel ESC differentiation strategy that avoids safety concerns associated with viral/DNA-based vectors in regenerative medicine.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

mentioning

confidence: 99%

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Mouse Embryonic Stem Cells Have Underdeveloped Antiviral Mechanisms That Can Be Exploited for the Development of mRNA-Mediated Gene Expression Strategy

Wang

Teng

Spangler

et al. 2014

Stem Cells and Development

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“…Since 2000, several transcription factors were discovered and were successfully used to reprogram target cells such as pancreatic islet cells (Zhou et al, 2008), neurons (Fishman et al, 2015;Vierbuchen et al, 2010), hepatocytes (Huang et al, 2011;Sekiya and Suzuki, 2011), endothelial cells (Ginsberg et al, 2012;Han et al, 2014), smooth muscle cells (Karamariti et al, 2013), and hepatocyte like cells (Simeonov and Uppal, 2014).…”

Section: Direct Reprogrammingmentioning

confidence: 99%

Direct reprogramming of somatic cells: an update

Pham

2015

Biomed Res Ther

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Abstract-Direct epigenetic reprogramming is a technique that converts a differentiated adult cell into another differentiated cell-such fibroblasts to cardiomyocytes-without passage through an undifferentiated pluripotent stage. This novel technology is opening doors in biological research and regenerative medicine. Some preliminary studies about direct reprogramming started in the 1980s when differentiated adult cells could be converted into other differentiated cells by overexpressing transcription-factor genes. These studies also showed that differentiated cells have plasticity. Direct reprogramming can be a powerful tool in biological research and regenerative medicine, especially the new frontier of personalized medicine. This review aims to summarize all direct reprogramming studies of somatic cells by master control genes as well as potential applications of these techniques in research and treatment of selected human diseases.

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M13 Bacteriophage and Adeno‐Associated Virus Hybrid for Novel Tissue Engineering Material with Gene Delivery Functions

Yoo

Jin

Choi

et al. 2015

Adv Healthcare Materials

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Efficient Direct Reprogramming of Mature Amniotic Cells into Endothelial Cells by ETS Factors and TGFβ Suppression

Cited by 207 publications

References 46 publications

Mouse Embryonic Stem Cells Have Underdeveloped Antiviral Mechanisms That Can Be Exploited for the Development of mRNA-Mediated Gene Expression Strategy

Mouse Embryonic Stem Cells Have Underdeveloped Antiviral Mechanisms That Can Be Exploited for the Development of mRNA-Mediated Gene Expression Strategy

Direct reprogramming of somatic cells: an update

M13 Bacteriophage and Adeno‐Associated Virus Hybrid for Novel Tissue Engineering Material with Gene Delivery Functions

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