Rapid Chromatin Switch in the Direct Reprogramming of Fibroblasts to Neurons

Wapinski, Orly L.; Lee, Qian Yi; Chen, Albert C.; Li, Rui; Corces, M. Ryan; Ang, Cheen Euong; Treutlein, Barbara; Xiang, Chaomei; Baubet, Valérie; Suchy, Fabian P.; Sankar, Venkat; Sim, Sopheak; Quake, Stephen R.; Dahmane, Nadia; Wernig, Marius; Chang, Howard Y.

doi:10.1016/j.celrep.2017.09.011

Cited by 119 publications

(124 citation statements)

References 59 publications

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“…Chromatin modifiers, such as the EZH2 and ASCL1 components, are also useful for DR to iNSCs or motor neurons [183, 201–203]. JMJD3 has been reported as an epigenetic enhancer of lineage conversion from bone marrow progenitors to liver cells [204].…”

Section: Potential Key Factors To Overcome the Obstacles To Cancer Cementioning

confidence: 99%

Potential application of cell reprogramming techniques for cancer research

Saito

Lin

Nakamura

et al. 2018

Cell. Mol. Life Sci.

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The ability to control the transition from an undifferentiated stem cell to a specific cell fate is one of the key techniques that are required for the application of interventional technologies to regenerative medicine and the treatment of tumors and metastases and of neurodegenerative diseases. Reprogramming technologies, which include somatic cell nuclear transfer, induced pluripotent stem cells, and the direct reprogramming of specific cell lineages, have the potential to alter cell plasticity in translational medicine for cancer treatment. The characterization of cancer stem cells (CSCs), the identification of oncogene and tumor suppressor genes for CSCs, and the epigenetic study of CSCs and their microenvironments are important topics. This review summarizes the application of cell reprogramming technologies to cancer modeling and treatment and discusses possible obstacles, such as genetic and epigenetic alterations in cancer cells, as well as the strategies that can be used to overcome these obstacles to cancer research.

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Section: Potential Key Factors To Overcome the Obstacles To Cancer Cementioning

confidence: 99%

Potential application of cell reprogramming techniques for cancer research

Saito

Lin

Nakamura

et al. 2018

Cell. Mol. Life Sci.

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“…Pioneer TFs induce the expression of endogenous secondary pro-neuronal TFs or of factors that repress the starting cell type-specific transcriptome, which further contributes to establishing neuronal identity [27]. Chromatin accessibility and transcriptome data have suggested that Zfp238, Sox8, and Dlx3 are among the most important endogenous secondary TF genes downstream of Ascl1 [32]. Some data indicate that Ngn2, when using an appropriate conversion medium, not only binds most of the Ascl1 binding sites in fibroblasts, but also possesses many additional binding sites [30,33].…”

Section: Enabling In Conversionmentioning

confidence: 99%

Next‐generation disease modeling with direct conversion: a new path to old neurons

2019

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Within just over a decade, human reprogramming-based disease modeling has developed from a rather outlandish idea into an essential part of disease research. While iPSCs are a valuable tool for modeling developmental and monogenetic disorders, their rejuvenated identity poses limitations for modeling age-associated diseases. Direct cell-type conversion of fibroblasts into induced neurons (iNs) circumvents rejuvenation and preserves hallmarks of cellular aging. iNs are thus advantageous for modeling diseases that possess strong age-related and epigenetic contributions and can complement iPSCbased strategies for disease modeling. In this review, we provide an overview of the state of the art of direct iN conversion and describe the key epigenetic, transcriptomic, and metabolic changes that occur in converting fibroblasts. Furthermore, we summarize new insights into this fascinating process, particularly focusing on the rapidly changing criteria used to define and characterize in vitro-born human neurons. Finally, we discuss the unique features that distinguish iNs from other reprogramming-based neuronal cell models and how iNs are relevant to disease modeling.

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“…One of the most commonly used TFs is the proneuronal gene achaete-scute homolog 1 (Ascl1). Many other TFs can also contribute to the reprogramming, such as brain-specific homeobox/POU domain protein 2 (Brn2) that does not access fibroblast chromatin actively on their own but it is recruited by Ascl1 [11,12]. Ascl1 alone can act as a pioneer factor occupying specific sites of the fibroblast genome [11].…”

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confidence: 99%

“…Ascl1 belongs to the family of the basic helix-loop-helix family, and it specifically binds DNA sequences containing an E-box motif [10]. Ascl1 alone can act as a pioneer factor occupying specific sites of the fibroblast genome [11]. Many other TFs can also contribute to the reprogramming, such as brain-specific homeobox/POU domain protein 2 (Brn2) that does not access fibroblast chromatin actively on their own but it is recruited by Ascl1 [11,12].…”

mentioning

confidence: 99%

“…Ascl1 alone can act as a pioneer factor occupying specific sites of the fibroblast genome [11]. Many other TFs can also contribute to the reprogramming, such as brain-specific homeobox/POU domain protein 2 (Brn2) that does not access fibroblast chromatin actively on their own but it is recruited by Ascl1 [11,12]. Also, microRNAs [13][14][15][16] and small molecules [17][18][19][20] have been shown to play a critical role in the conversion process.…”

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confidence: 99%

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Dual modulation of neuron‐specific microRNAs and the REST complex promotes functional maturation of human adult induced neurons

et al. 2019

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Direct neuronal reprogramming can be achieved using different approaches: by expressing neuronal transcription factors or microRNAs; and by knocking down neuronal repressive elements. However, there still exists a high variability in terms of the quality and maturity of the induced neurons obtained, depending on the reprogramming strategy employed. Here, we evaluate different long‐term culture conditions and study the effect of expressing the neuronal‐specific microRNAs, miR124 and miR9/9*, while reprogramming with forced expression of the transcription factors Ascl1, Brn2, and knockdown of the neuronal repressor REST. We show that the addition of microRNAs supports neuronal maturation in terms of gene and protein expression, as well as in terms of electrophysiological properties.

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Rapid Chromatin Switch in the Direct Reprogramming of Fibroblasts to Neurons

Cited by 119 publications

References 59 publications

Potential application of cell reprogramming techniques for cancer research

Potential application of cell reprogramming techniques for cancer research

Next‐generation disease modeling with direct conversion: a new path to old neurons

Dual modulation of neuron‐specific microRNAs and the REST complex promotes functional maturation of human adult induced neurons

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