Human Induced Pluripotent Stem Cell–Derived Motor Neuron Transplant for Neuromuscular Atrophy in a Mouse Model of Sciatic Nerve Injury

Pepper, Jon‐Paul; Wang, Tiffany V.; Hennes, Valerie; Sun, Soo Yeon; Ichida, Justin K.

doi:10.1001/jamafacial.2016.1544

Cited by 22 publications

(10 citation statements)

References 27 publications

(52 reference statements)

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“…In particular, the realization that Oct4, Sox2, Klf4 and Myc can reprogram easily obtained cell types to pluripotency has fueled new approaches to studying human disease. By reprogramming cells from individuals with genetic forms of disease into induced pluripotent stem cells (iPSCs) or somatic cell types, it has become possible to understand and develop interventions for cell type-specific pathologies that previously could have only been studied using postmortem tissues (Blanchard et al, 2015;Brennand et al, 2011;Ichida et al, 2009Ichida et al, , 2014Ichida and Kiskinis, 2015;Kiskinis et al, 2014;Kramer et al, 2018;Mertens et al, 2015;Pepper et al, 2017;Shi et al, 2018;Son et al, 2011;Takahashi et al, 2007a,b;Toma et al, 2015;Wainger et al, 2015;Wen et al, 2014;Wilkinson et al, 2018;Xu et al, 2015;Zhang et al, 2015;Zhao et al, 2015).…”

Section: Introductionmentioning

confidence: 99%

Comparative genomic analysis of embryonic, lineage-converted, and stem cell-derived motor neurons

et al. 2018

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Advances in stem cell science allow the production of different cell types in vitro either through the recapitulation of developmental processes, often termed 'directed differentiation', or the forced expression of lineage-specific transcription factors. Although cells produced by both approaches are increasingly used in translational applications, their quantitative similarity to their primary counterparts remains largely unresolved. To investigate the similarity between in vitro-derived and primary cell types, we harvested and purified mouse spinal motor neurons and compared them with motor neurons produced by transcription factor-mediated lineage conversion of fibroblasts or directed differentiation of pluripotent stem cells. To enable unbiased analysis of these motor neuron types and their cells of origin, we then subjected them to whole transcriptome and DNA methylome analysis by RNA sequencing (RNA-seq) and reduced representation bisulfite sequencing (RRBS). Despite major differences in methodology, lineage conversion and directed differentiation both produce cells that closely approximate the primary motor neuron state. However, we identify differences in Fas signaling, the Hox code and synaptic gene expression between lineage-converted and directed differentiation motor neurons that affect their utility in translational studies.

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Section: Introductionmentioning

confidence: 99%

Comparative genomic analysis of embryonic, lineage-converted, and stem cell-derived motor neurons

et al. 2018

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“…The control 03231 iPSC line was generated from a lymphoblastoid cell line derived from a healthy 56 year-old male (NINDS repository, ND03231) as previously described (34). For gene-editing, guide RNAs were cloned into pSpCas9(BB)-2A-Puro (PX459) V2.0 and the homologous recombination donor vector was constructed using the pFETCH_Donor plasmid (35,36).…”

Section: Cell Culture and Neural Differentiationmentioning

confidence: 99%

Endogenous Cell Type–Specific Disrupted in Schizophrenia 1 Interactomes Reveal Protein Networks Associated With Neurodevelopmental Disorders

Wilkinson

Evgrafov

Zheng

et al. 2019

Biological Psychiatry

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“…Both ESCs and iPSCs differentiated toward NS/PCs or glial cells have been transplanted directly into the spinal cord of rodent models of ALS. Human cells have been observed within transplanted animals up to 9 months post‐transplantation and have been shown to form neurites, axons, and even functional neuromuscular junctions . However, the terminal differentiation of these cells is variable.…”

Section: Human–animal Chimerismmentioning

confidence: 99%

“…Two separate groups observed that up to 1,600,000 human cells integrated into the spinal cord of mutant SOD1 transgenic rodents up to 9 months post‐transplant, with the majority of transplanted human cells differentiating toward astrocytes . Although some studies have shown grafted human neural stem cells to extend axons and innervate muscle, it is likely that the benefits seen are at least in part due to the neuroprotective mechanisms exerted by the engrafted human cells .…”

Section: Human–animal Chimerismmentioning

confidence: 99%

Concise Review: Human-Animal Neurological Chimeras: Humanized Animals or Human Cells in an Animal?

et al. 2019

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Blastocyst complementation is an emerging methodology in which human stem cells are transferred into genetically engineered preimplantation animal embryos eventually giving rise to fully developed human tissues and organs within the animal host for use in regenerative medicine. The ethical issues surrounding this method have caused the National Institutes of Health to issue a moratorium on funding for blastocyst complementation citing the potential for human cells to substantially contribute to the brain of the chimeric animal. To address this concern, we performed an in-depth review of the neural transplantation literature to determine how the integration of human cells into the nonhuman neural circuitry has altered the behavior of the host. Despite reports of widespread integration of human cell transplants, our review of 150 transplantation studies found no evidence suggestive of humanization of the animal host, and we thus conclude that, at present, concerns over humanization should not prevent research on blastocyst complementation to continue. We suggest proceeding in a controlled and transparent manner, however, and include recommendations for future research with careful consideration for how human cells may contribute to the animal host nervous system. STEM CELLS 2019;37:444-452 SIGNIFICANCE STATEMENTDue to a severe shortage of human organs and tissues, thousands of patients die each year due to an inability to procure organs for transplantation. Blastocyst complementation is a methodology that has the potential to generate large quantities of functioning human organs and tissues but is hindered by a National Institutes of Health moratorium on funding, citing concern over substantial human cell contribution to the brain of the animal. This review summarizes published, peer-reviewed studies on human-animal neural transplantation and suggests that this concern over neurological chimerism should not prevent research to continue in a controlled and transparent manner.

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Human Induced Pluripotent Stem Cell–Derived Motor Neuron Transplant for Neuromuscular Atrophy in a Mouse Model of Sciatic Nerve Injury

Cited by 22 publications

References 27 publications

Comparative genomic analysis of embryonic, lineage-converted, and stem cell-derived motor neurons

Comparative genomic analysis of embryonic, lineage-converted, and stem cell-derived motor neurons

Endogenous Cell Type–Specific Disrupted in Schizophrenia 1 Interactomes Reveal Protein Networks Associated With Neurodevelopmental Disorders

Concise Review: Human-Animal Neurological Chimeras: Humanized Animals or Human Cells in an Animal?

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