Transplanted miR-219-overexpressing oligodendrocyte precursor cells promoted remyelination and improved functional recovery in a chronic demyelinated model

Fan, Huiying; Chen, Lixia; Qu, Xuebin; Ren, Chuanlu; Wu, Xiuxiang; Dong, Fuxing; Zhang, Baole; Yao, Ruiqin

doi:10.1038/srep41407

Cited by 55 publications

(53 citation statements)

References 74 publications

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“…The Journal of Clinical Investigation (102). MCT1 was suggested to be mediating the enhanced remyelination, but as the authors used a nonspecific MCT1 inhibitor in this study, the true importance of MCT1 in remyelination remains enigmatic.…”

Section: Involvement Of Oligodendrocyte Metabolic Support In Neurodegmentioning

confidence: 99%

Oligodendroglia: metabolic supporters of neurons

Philips¹,

Rothstein²

2017

Journal of Clinical Investigation

252

192

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Section: Involvement Of Oligodendrocyte Metabolic Support In Neurodegmentioning

confidence: 99%

Oligodendroglia: metabolic supporters of neurons

Philips¹,

Rothstein²

2017

Journal of Clinical Investigation

252

192

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“…(99) vs. All genes p = 1.7 × 10 -3 p = 5.0 × 10 -5 p = 8.5 × 10 -1 log2 (gliomas / cortices) CDF Among all miRNA families, the miR-219a-5p family had the highest number of targets in gliomas (300 out of 1,878 peaks contained 6mer, 7mer or 8mer seed matches to miR-219a-5p). miR-219-5p has been reported to regulate oligodendrocyte (OL) differentiation and myelination in mice via targeting important regulators of oligodendrocyte progenitor cell (OPC) maintenance (Dugas et al, 2010;Emery, 2010;Fan et al, 2017;Wang et al, 2017;Zhao et al, 2010). Interestingly, we observed a strong interaction between miR-219a-5p and Pdgfra (Figure 4f), a characteristic marker of OPCs and a key player in gliomagenesis.…”

Section: Identification Of Mirna Targets In Normal Adult Tissues and mentioning

confidence: 77%

High-resolution in vivo identification of miRNA targets by Halo-Enhanced Ago2 Pulldown

Pritykin

Concepcion

et al. 2019

Preprint

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The identification of miRNA targets by Ago2 crosslinking-immunoprecipitation (CLIP) methods has provided major insights into the biology of this important class of non-coding RNAs. However, these methods are technically challenging and not easily translated to an in vivo setting. To overcome these limitations and to facilitate the investigation of miRNA functions in mice, we have developed a method (HEAP: for Halo-Enhanced Ago2 Pulldown) to map miRNA-mRNA binding sites. This method is based on a novel genetically engineered mouse harboring a conditional, Cre-regulated, Halo-Ago2 allele expressed from the endogenous Ago2 locus. By using a resin conjugated to the HaloTag ligand, Ago2-miRNA-mRNA complexes can be efficiently purified from cells and tissues expressing the endogenous Halo-Ago2 allele. We demonstrate the reproducibility and sensitivity of this method in mouse embryonic stem cells, in developing embryos, in adult tissues and in autochthonous mouse models of human brain and lung cancers. The tools and the datasets we have generated will serve as a valuable resource to the scientific community and will facilitate the characterization of miRNA functions under physiological and pathological conditions.

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“…Mice lacking miR‐219 demonstrate impaired remyelination after lysolecithin‐induced injury, and overexpression of miR‐219 in oligodendrocyte lineage cells is sufficient to promote remyelination (Wang, Moyano, et al, ). Overexpression of miR‐219 in cuprizone‐treated mice also delays demyelination (Liu et al, ), and transplantation of OPCs overexpressing miR‐219 promotes remyelination (Fan et al, ). Furthermore, intrathecal administration of miR‐219 mimics promotes remyelination in both the lysolecithin and experimental autoimmune encephalomyelitis (EAE) mouse models (Wang, Moyano, et al, ).…”

Section: Mirnas As Intrinsic Cues Influencing Remyelinationmentioning

confidence: 99%

Inhibitory milieu at the multiple sclerosis lesion site and the challenges for remyelination

Galloway

Gowing

Setayeshgar

et al. 2019

Glia

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Regeneration of myelin, following injury, can occur within the central nervous system to reinstate proper axonal conductance and provide trophic support. Failure to do so renders the axons vulnerable, leading to eventual degeneration, and neuronal loss. Thus, it is essential to understand the mechanisms by which remyelination or failure to remyelinate occur, particularly in the context of demyelinating and neurodegenerative disorders. In multiple sclerosis, oligodendrocyte progenitor cells (OPCs) migrate to lesion sites to repair myelin. However, during disease progression, the ability of OPCs to participate in remyelination diminishes coincident with worsening of the symptoms. Remyelination is affected by a broad range of cues from intrinsic programming of OPCs and extrinsic local factors to the immune system and other systemic elements including diet and exercise. Here we review the literature on these diverse inhibitory factors and the challenges they pose to remyelination. Results spanning several disciplines from fundamental preclinical studies to knowledge gained in the clinic will be discussed.

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Transplanted miR-219-overexpressing oligodendrocyte precursor cells promoted remyelination and improved functional recovery in a chronic demyelinated model

Cited by 55 publications

References 74 publications

Oligodendroglia: metabolic supporters of neurons

Oligodendroglia: metabolic supporters of neurons

High-resolution in vivo identification of miRNA targets by Halo-Enhanced Ago2 Pulldown

Inhibitory milieu at the multiple sclerosis lesion site and the challenges for remyelination

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