Your search keyword '"hESC"' showing total 341 results

1. Salbutamol attenuates arrhythmogenic effect of aminophylline in a hPSC-derived cardiac model.

Author

Kabanov, Daniil, Vrana Klimovic, Simon, Beckerová, Deborah, Molcan, Martin, Scurek, Martin, Brat, Kristian, Bebarova, Marketa, Rotrekl, Vladimir, Pribyl, Jan, and Pesl, Martin

Subjects

*BETA adrenoceptors, *NITRIC-oxide synthases, *PLURIPOTENT stem cells, *ATOMIC force microscopy, *OBSTRUCTIVE lung diseases

Abstract

The combination of aminophylline and salbutamol is frequently used in clinical practice in the treatment of obstructive lung diseases. While the side effects (including arrhythmias) of the individual bronchodilator drugs were well described previously, the side effects of combined treatment are almost unknown. We aimed to study the arrhythmogenic potential of combined aminophylline and salbutamol treatment in vitro. For this purpose, we used the established atomic force microscopy (AFM) model coupled with cardiac organoids derived from human pluripotent stem cells (hPSC-CMs). We focused on the chronotropic, inotropic, and arrhythmogenic effects of salbutamol alone and aminophylline and salbutamol combined treatment. We used a method based on heart rate/beat rate variability (HRV/BRV) analysis to detect arrhythmic events in the hPSC-CM based AFM recordings. Salbutamol and aminophylline had a synergistic chronotropic and inotropic effect compared to the effects of monotherapy. Our main finding was that salbutamol reduced the arrhythmogenic effect of aminophylline, most likely mediated by endothelial nitric oxide synthase activated by beta-2 adrenergic receptors. These findings were replicated and confirmed using hPSC-CM derived from two cell lines (CCTL4 and CCTL12). Data suggest that salbutamol as an add-on therapy may not only deliver a bronchodilator effect but also increase the cardiovascular safety of aminophylline, as salbutamol reduces its arrhythmogenic potential. [ABSTRACT FROM AUTHOR]

Published

2024

2. Salbutamol attenuates arrhythmogenic effect of aminophylline in a hPSC-derived cardiac model

Author

Daniil Kabanov, Simon Vrana Klimovic, Deborah Beckerová, Martin Molcan, Martin Scurek, Kristian Brat, Marketa Bebarova, Vladimir Rotrekl, Jan Pribyl, and Martin Pesl

Subjects

Salbutamol, Aminophylline, Atomic force microscopy, iPSC, HESC, Cardiomyocytes, Pulmonary drug screening, Medicine, Science

Abstract

Abstract The combination of aminophylline and salbutamol is frequently used in clinical practice in the treatment of obstructive lung diseases. While the side effects (including arrhythmias) of the individual bronchodilator drugs were well described previously, the side effects of combined treatment are almost unknown. We aimed to study the arrhythmogenic potential of combined aminophylline and salbutamol treatment in vitro. For this purpose, we used the established atomic force microscopy (AFM) model coupled with cardiac organoids derived from human pluripotent stem cells (hPSC-CMs). We focused on the chronotropic, inotropic, and arrhythmogenic effects of salbutamol alone and aminophylline and salbutamol combined treatment. We used a method based on heart rate/beat rate variability (HRV/BRV) analysis to detect arrhythmic events in the hPSC-CM based AFM recordings. Salbutamol and aminophylline had a synergistic chronotropic and inotropic effect compared to the effects of monotherapy. Our main finding was that salbutamol reduced the arrhythmogenic effect of aminophylline, most likely mediated by endothelial nitric oxide synthase activated by beta-2 adrenergic receptors. These findings were replicated and confirmed using hPSC-CM derived from two cell lines (CCTL4 and CCTL12). Data suggest that salbutamol as an add-on therapy may not only deliver a bronchodilator effect but also increase the cardiovascular safety of aminophylline, as salbutamol reduces its arrhythmogenic potential.

Published

2024

3. Human pallial MGE-type GABAergic interneuron cell therapy for chronic focal epilepsy.

Author

Bershteyn, Marina, Bröer, Sonja, Parekh, Mansi, Maury, Yves, Havlicek, Steven, Kriks, Sonja, Fuentealba, Luis, Lee, Seonok, Zhou, Robin, Subramanyam, Geetha, Sezan, Meliz, Sevilla, Eric, Blankenberger, Whitney, Spatazza, Julien, Zhou, Li, Nethercott, Hubert, Traver, David, Hampel, Philip, Kim, Hannah, Watson, Michael, Salter, Naomi, Nesterova, Anastasia, Au, Wai, Banik, Gautam, Bulfone, Alessandro, Priest, Catherine, Nicholas, Cory, Kriegstein, Arnold, Rubenstein, John, and Alvarez-Buylla, Arturo

Subjects

GABA, MGE, TLE, cell therapy, epilepsy, hESC, interneuron, seizure, transplant, Mice, Animals, Humans, Hippocampus, Epilepsy, Temporal Lobe, Seizures, Interneurons, Brain

Abstract

Mesial temporal lobe epilepsy (MTLE) is the most common focal epilepsy. One-third of patients have drug-refractory seizures and are left with suboptimal therapeutic options such as brain tissue-destructive surgery. Here, we report the development and characterization of a cell therapy alternative for drug-resistant MTLE, which is derived from a human embryonic stem cell line and comprises cryopreserved, post-mitotic, medial ganglionic eminence (MGE) pallial-type GABAergic interneurons. Single-dose intrahippocampal delivery of the interneurons in a mouse model of chronic MTLE resulted in consistent mesiotemporal seizure suppression, with most animals becoming seizure-free and surviving longer. The grafted interneurons dispersed locally, functionally integrated, persisted long term, and significantly reduced dentate granule cell dispersion, a pathological hallmark of MTLE. These disease-modifying effects were dose-dependent, with a broad therapeutic range. No adverse effects were observed. These findings support an ongoing phase 1/2 clinical trial (NCT05135091) for drug-resistant MTLE.

Published

2023

4. Proteomic and functional comparison between human induced and embryonic stem cells

Author

Alejandro J Brenes, Eva Griesser, Linda V Sinclair, Lindsay Davidson, Alan R Prescott, Francois Singh, Elizabeth KJ Hogg, Carmen Espejo-Serrano, Hao Jiang, Harunori Yoshikawa, Melpomeni Platani, Jason R Swedlow, Greg M Findlay, Doreen A Cantrell, and Angus I Lamond

Subjects

proteomics, iPSC, mass spectrometry, stem cell, hESC, protein content, Medicine, Science, Biology (General), QH301-705.5

Abstract

Human induced pluripotent stem cells (hiPSCs) have great potential to be used as alternatives to embryonic stem cells (hESCs) in regenerative medicine and disease modelling. In this study, we characterise the proteomes of multiple hiPSC and hESC lines derived from independent donors and find that while they express a near-identical set of proteins, they show consistent quantitative differences in the abundance of a subset of proteins. hiPSCs have increased total protein content, while maintaining a comparable cell cycle profile to hESCs, with increased abundance of cytoplasmic and mitochondrial proteins required to sustain high growth rates, including nutrient transporters and metabolic proteins. Prominent changes detected in proteins involved in mitochondrial metabolism correlated with enhanced mitochondrial potential, shown using high-resolution respirometry. hiPSCs also produced higher levels of secreted proteins, including growth factors and proteins involved in the inhibition of the immune system. The data indicate that reprogramming of fibroblasts to hiPSCs produces important differences in cytoplasmic and mitochondrial proteins compared to hESCs, with consequences affecting growth and metabolism. This study improves our understanding of the molecular differences between hiPSCs and hESCs, with implications for potential risks and benefits for their use in future disease modelling and therapeutic applications.

Published

2024

5. Single cell analysis provides insight into haematopoietic differentiation of human embryonic stem cells

Author

Nnadi, Nneka Concilia, Medvinsky, Alexander, and Kaji, Keisuke

Subjects

hESC, haematopoiesis, scRNA-seq, mitochondria activity

Abstract

One of the challenges in regenerative medicine remains generating functional haematopoietic stem cells (HSCs) of clinical quantity. Utilizing data from single cell RNA sequencing (scRNA-seq) of human embryonic stem cells (hESC) derived cells, I explored the differences that exist between in vitro and in vivo haematopoiesis, with the aim that understanding these differences could help improve future chances of generating HSCs in vitro. In the first part of this project, functional analysis into in vitro differentiation using an established haematopoietic differentiation protocol, confirmed that the protocol is myeloid and NK lineage biased compared to umbilical cord blood, with the population lineage dynamics changing over time. Using scRNA-seq, I investigated dynamic gene expression of cell populations emerging during hESC differentiation. I show that the haematogenic endothelium capable of generating the haematopoietic progenitors emerges as early as day 6 of differentiation. I also show that priming of the arterial endothelial cells to the haematogenic endothelium, and subsequent emergence of haematopoietic progenitors is associated with an increase in ribosomal and mitochondrial activity. Finally, a comparative analysis of the hESCs generated dataset with publicly available dataset of embryonic haematopoietic tissues revealed that hESC derived haematopoiesis, associated with increased mitochondrial gene activity, is likely mimicking events of the yolk sac haematopoiesis, rather than the haematopoiesis occurring in the AGM region. Based on the findings presented here, I hypothesize that increased mitochondrial activity, likely due to the normoxic culture conditions, may be contributing to the challenge in generating HSCs from hESCs in the dish.

Published

2022

6. Investigating the disruption of transcriptional homeostatic networks in driving motor neuron specific degeneration in Amyotrophic Lateral Sclerosis

Author

Moran, J., Bhinge, Akshay, Mill, Jon, and Dempster, Emma

Subjects

ALS, Amyotrophic lateral sclerosis, Nociceptor, Motor neuron, Stem cell, iPSC, induced pluripotent stem cell, human embryonic stem cell, hESC, Epigenetics, RNA sequencing, RNA seq, Neuronal culture, Calcium imaging, CRISPR

Abstract

Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disease caused by the progressive loss of upper and lower motor neurons, eventually culminating in patient paralysis and death via asphyxiation. At the time of diagnosis, approximately 50% of patient motor neurons are predicted to have degenerated, resulting in a prognosis of 3-5 years. While most incidences of ALS are sporadic (~90%) with no obvious genetic constituent, approximately 10% of cases are inherited in a dominant manner and are referred to as familial ALS. At the present time there is no cure for ALS and current pharmacological treatments, such as Riluzole, operate with limited efficacy. As such, gaining further insight into pathomechanisms driving ALS is paramount for the development of novel and effective therapeutics. The C9ORF72 hexanucleotide repeat expansion is attributed to 40-50% of familial and approximately 10% of sporadic ALS cases. Investigating pathomechanisms driving familial cases of C9-ALS could elucidate neurodegenerative mechanisms central to both familial and sporadic cases. The aim of this thesis was to investigate transcriptional perturbations in C9-ALS to elucidate de novo candidates rendering motor neurons particularly susceptible to pathology. Evidence from previous studies suggested that nociceptors of ALS patients remain functionally viable due to the presence of non-neuropathic pain in approximately 80% of patients. We subsequently developed a novel protocol to efficiently generate functional sensory neuron cultures predominantly consisting of spinal nociceptors (~75%). Utilizing our protocol, we compared the transcriptomes of C9-ALS nociceptors with C9-ALS motor neurons which elucidated dysregulation of synaptic genes in motor neurons, potentially suggesting increased susceptibility of motor neurons to excitotoxic mechanisms. Finally, we utilised CRISPR systems employing dCas9 fused to epigenetic effectors to selectively demethylate the C9ORF72 repeat expansion and proximally associated regions to investigate epigenetic contributions to pathology. We observed an increase in transcript variant 3 expression and retention of intron 1 was observed upon demethylation of the repeat expansion. While increased expression of C9ORF72 could exacerbate pathomechanisms driven by RNA foci and accumulation of DPR proteins, deficits in synaptic function could be attenuated by reducing C9ORF72 haploinsufficiency. In summary, the work presented in this thesis outlines novel approaches to investigating the mechanisms driving pathology in C9-ALS with the hope of elucidating de novo candidates for therapeutic targeting. Furthermore, the ability to generate functional nociceptors broadens the scope of pain research permitting in vitro experiments to understand the mechanics of pain in human cells.

Published

2022

7. Influence of glucose and oxygen on human embryos and embryonic stem cells

Author

Montufar Martinez, Maribel, Kimber, Susan, and Brison, Daniel

Subjects

Embryo development, OCR, Mitochondria, Gene expression, DNA methylation, HESC, Human embryo, Oxygen, Glucose, DOHAD, ART

Abstract

Despite the significant improvements in Assisted Reproductive Technologies (ART) there is an extensive area that remains unknown in regards to the effect of embryo culture on the long-term health of the offspring. The preimplantation embryo has specific requirements depending on the developmental stage; however, it remains unclear how the different compositions of commercial culture media can affect embryo development. The in vitro factors that most influence embryo health include cryopreservation methods, culture media components, and oxygen levels. Several studies have reported alterations in birth weight, and a higher risk of congenital anomalies when comparing between assisted and naturally conceived babies. Others have reported effects on epigenetic regulation, gene expression and imprinting, suggesting that embryo culture medium may have a potential impact on the further development of the newborn. Nevertheless, the most commonly reported alterations in offspring health outcomes include foetal growth, birth weight, childhood growth and long-term diseases such as metabolic, cardiovascular, and neurological. Due to the number of reports indicating the possible effect of the environment on embryo development, it is crucial to be aware of the mechanisms involved in order to prevent embryo alterations and long-term diseases. Therefore, the objective of this thesis was to determine whether specific components of embryo culture such as glucose and oxygen had any effect on the epigenetic patterns, at transcript levels, as well as on mitochondrial function. The analysis of transcripts was assessed to determine differential expression of genes related to pluripotency, mitochondrial function, apoptosis, oxidative stress, DNA methylation, glucose transporters, among others. The epigenome analysis (Bisulfite Sequencing) was carried out to determine differential DNA methylation levels on human blastocyst cultured in high or low glucose (0.9mM or 3.5mM). Finally, mitochondrial function was evaluated through the measurement of mitochondrial membrane potential (MitoProbe™ JC-1 assay) and through the analysis of mitochondrial respiration (Seahorse XF Cell Mito Stress Test) by directly measuring the oxygen consumption rate (OCR). In order to accomplish the objectives of this project and to obtain the most relevant clinical data, this research was conducted using preimplantation human embryos at blastocyst stage (day 6) and a model of human embryonic stem cells (HESCs). HESCs are pluripotent stem cells derived from the inner cell mass (ICM) of human blastocysts. The combination of the analysis on human embryos and HESCs allowed the validation of initial protocols, set up experimental conditions and the evaluation of different culture conditions. Firstly, I evaluated combined oxygen levels (5% and 20%) and glucose concentration (5mM and 17.5mM) on HESCs to determine their effect on transcript levels and mitochondrial function. Findings revealed altered transcript levels and mitochondrial function when cells were exposed to different concentrations of either oxygen or glucose, as well as to the combinations of both. However, the most significant effects were observed with changes in glucose concentration. Secondly, oxygen levels (5% and 20%), glucose concentration (0.9mM and 3.5mM) and the effect of cryoprotectants were evaluated on human blastocysts to determine their effect on transcript levels, mitochondrial function and DNA methylation. Findings revealed altered gene expression due to changes in oxygen but more significantly due to changes in glucose. Also, the analysis of DNA methylation showed significant differences as a result of glucose concentration. Furthermore, for the evaluation of mitochondrial function, the analysis of membrane potential was only carried out on blastocysts, treated/untreated with cryoprotectant. On the other hand, the measurement of OCR for mitochondrial respiration was only possible to determine the baseline on fresh blastocyst but not to make a comparison between culture conditions due to technical limitations. Overall, these findings suggest that altered culture conditions during early embryo development have the potential to affect several pathways that could be linked to the development of diseases. This project provides the first evidence about specific components of the embryo culture that could alter embryo development. Therefore, the conditions evaluated in this project are worth further investigation to elucidate the altered mechanisms and their direct association with the development of diseases.

Published

2021

8. Pancreatic progenitor epigenome maps prioritize type 2 diabetes risk genes with roles in development.

Author

Geusz, Ryan J, Wang, Allen, Chiou, Joshua, Lancman, Joseph J, Wetton, Nichole, Kefalopoulou, Samy, Wang, Jinzhao, Qiu, Yunjiang, Yan, Jian, Aylward, Anthony, Ren, Bing, Dong, P Duc Si, Gaulton, Kyle J, and Sander, Maike

Subjects

GWAS, Type 2 diabetes, Zebrafish, chromatin, developmental biology, genetics, genomics, hESC, human, pancreas, zebrafish, Cancer, Stem Cell Research, Regenerative Medicine, Rare Diseases, Digestive Diseases, Stem Cell Research - Embryonic - Human, Diabetes, Pancreatic Cancer, Genetics, Metabolic and endocrine, Biochemistry and Cell Biology

Abstract

Genetic variants associated with type 2 diabetes (T2D) risk affect gene regulation in metabolically relevant tissues, such as pancreatic islets. Here, we investigated contributions of regulatory programs active during pancreatic development to T2D risk. Generation of chromatin maps from developmental precursors throughout pancreatic differentiation of human embryonic stem cells (hESCs) identifies enrichment of T2D variants in pancreatic progenitor-specific stretch enhancers that are not active in islets. Genes associated with progenitor-specific stretch enhancers are predicted to regulate developmental processes, most notably tissue morphogenesis. Through gene editing in hESCs, we demonstrate that progenitor-specific enhancers harboring T2D-associated variants regulate cell polarity genes LAMA1 and CRB2. Knockdown of lama1 or crb2 in zebrafish embryos causes a defect in pancreas morphogenesis and impairs islet cell development. Together, our findings reveal that a subset of T2D risk variants specifically affects pancreatic developmental programs, suggesting that dysregulation of developmental processes can predispose to T2D.

Published

2021

9. The contribution of donated human embryos suitable for the production of embryonic stem cells to increase the quality of life: Selection and preparation of embryos in the Czech Republic.

Author

Ventruba, Tomáš, Ventruba, Pavel, Ješeta, Michal, Žáková, Jana, Lousová, Eva, Crha, Igor, Souralová, Tereza, Koutná, Irena, and Hampl, Aleš

Subjects

EMBRYONIC stem cells, HUMAN embryos, HUMAN embryonic stem cells, CURRENT good manufacturing practices, SOMATOTYPES

Abstract

Background. Human embryonic stem cells (hESCs) have the unique ability to differentiate into any cell type in the human body and to proliferate indefinitely. Cell therapies involving hESC have shown very promising results for the treatment of certain diseases and confirmed the safety of hESC-derived cells for humans. They are used in cell therapy, mainly in targeted therapy of diseases that are currently incurable. Objectives. The aim of this study was the derivation of clinical-grade hESCs usable in drug development, non-native medicine and cell therapy. Materials and methods. Embryos were thawed, cultivated to the blastocyst stage if necessary, and assisted hatching was subsequently performed. Embryoblasts were mechanically isolated using narrow needles. Each line was kept as a separate batch. The derived hESCs were cultured under hypoxic culture conditions (5% O2, 5% CO2, 37°C) in a NutriStem® hPSC XF Medium with a daily medium change. Results. From January 2018 to July 2020, 138 selected clients were asked for consent to donate embryos, of whom 52 did not respond, 19 terminated the storage of their embryos and 29 extended the storage. Only 38 clients (27.5%) agreed to donate embryos for the derivation of hESCs. At the same time, personal communication with clients took place and another 17 embryo donors were recruited. A total of 160 embryos from 55 donors aged 26-42 years were collected. The embryos were frozen at the blastocyst (33.1%) or morula (46.3%) stage. After the preparation of 64 embryos, embryoblasts were isolated and cultured. Finally, 7 hESC lines were obtained, 4 research-grade and 3 clinical-grade, the first in the Czech Republic. Conclusions. We established a current good manufacturing practice (cGMP)-defined xeno-free and feederfree system for the derivation, culture and banking of clinical-grade hESC lines that are suitable for preclinical and clinical trials. The quality control testing with criteria concerning sterility, safety and characterization according to cGMP ensured the clinical-grade quality of hESC lines. [ABSTRACT FROM AUTHOR]

Published

2023

10. GATA3 Mediates a Fast, Irreversible Commitment to BMP4-Driven Differentiation in Human Embryonic Stem Cells

Author

Gunne-Braden, Alexandra, Sullivan, Adrienne, Gharibi, Borzo, Sheriff, Rahuman SM, Maity, Alok, Wang, Yi-Fang, Edwards, Amelia, Jiang, Ming, Howell, Michael, Goldstone, Robert, Wollman, Roy, East, Philip, and Santos, Silvia DM

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Regenerative Medicine, Stem Cell Research, Stem Cell Research - Embryonic - Human, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Bone Morphogenetic Protein 4, Cell Differentiation, GATA3 Transcription Factor, Human Embryonic Stem Cells, Humans, Signal Transduction, BMP4, GATA3, bistability, commitment, differentiation, fate decisions, hESC, positive feedback, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences

Abstract

During early development, extrinsic triggers prompt pluripotent cells to begin the process of differentiation. When and how human embryonic stem cells (hESCs) irreversibly commit to differentiation is a fundamental yet unanswered question. By combining single-cell imaging, genomic approaches, and mathematical modeling, we find that hESCs commit to exiting pluripotency unexpectedly early. We show that bone morphogenetic protein 4 (BMP4), an important differentiation trigger, induces a subset of early genes to mirror the sustained, bistable dynamics of upstream signaling. Induction of one of these genes, GATA3, drives differentiation in the absence of BMP4. Conversely, GATA3 knockout delays differentiation and prevents fast commitment to differentiation. We show that positive feedback at the level of the GATA3-BMP4 axis induces fast, irreversible commitment to differentiation. We propose that early commitment may be a feature of BMP-driven fate choices and that interlinked feedback is the molecular basis for an irreversible transition from pluripotency to differentiation.

Published

2020

11. Characterization of the individual capacity for repair of genotoxic damage of a Bulgarian hESC line and two commonly used stabilized cell lines

Author

Rumena Petkova, Pavlina Chelenkova, Borislav Arabadjiev, Roumen Pankov, and Stoyan Chakarov

Subjects

DNA repair, individual repair capacity, hESC, genetic markers, T-cell leukaemia cell lines, Biotechnology, TP248.13-248.65

Abstract

AbstractThe number of stem cell lines worldwide grows steadily, including disease-specific lines and lines derived from specific tissues. The proportion of stem cell lines that were established in strictly xeno-free conditions is rapidly increasing, but it is still unclear whether these lines may be maintained in vitro for prolonged periods of time with satisfactory survival rates and minimal loss of their ‘stemness’ properties. The efficiency of repair of DNA damage has recently emerged as an important factor for maintenance of stem cells in culture with minimal genomic changes and preservation of the undifferentiated state. In this study we investigated the individual capacity for repair of DNA damage/maintenance of genomic integrity and additional markers in one human embryonic stem cell (hESC) line derived in Bulgaria from a discarded embryo and two of the human T-leukaemia cell lines commonly used for research purposes (T-1301 and Jurkat E6-1). Knowledge about the status of the studied cancer cell lines may be valuable for research purposes. Data about the individual repair capacity and the genetic risk for common late-onset diseases of newly established hESC lines as well as hESC lines currently in use may become a valuable tool in the assessment of the applicability of pluripotent human cell lines for research purposes, clinical trials and, potentially, clinical applications.

Published

2022

12. Patients’ views on using human embryonic stem cells to treat Parkinson’s disease: an interview study

Author

Jennifer Drevin, Dag Nyholm, Håkan Widner, Trinette Van Vliet, Jennifer Viberg Johansson, Elena Jiltsova, and Mats Hansson

Subjects

hESC, ATMP, Human embryonic stem cells, Advanced therapy medicinal product, Parkinson’s disease, Ethics, Medical philosophy. Medical ethics, R723-726

Abstract

Abstract Background Human embryonic stem cells (hESC) as a source for the development of advanced therapy medicinal products are considered for treatment of Parkinson’s disease (PD). Research has shown promising results and opened an avenue of great importance for patients who currently lack a disease modifying therapy. The use of hESC has given rise to moral concerns and been the focus of often heated debates on the moral status of human embryos. Approval for marketing is still pending. Objective To Investigate the perspectives and concerns of patients with PD, patients being the directly concerned stakeholders in the ethical discussion. Methods Qualitative semi-structured interviews related to this new therapy in seventeen patients from two Swedish cities. Results The participants expressed various interests related to the use of human embryos for development of medicinal therapies; however, overall, they were positive towards the use of hESC for treatment of PD. It was deemed important that the donating woman or couple made the choice to donate embryos voluntarily. Furthermore, there were concerns that the industry does not always prioritise the patient over profit; thus, transparency was seen as important.

Published

2022

13. Temporal and partial inhibition of GLI1 in neural stem cells (NSCs) results in the early maturation of NSC derived oligodendrocytes in vitro

Author

Namchaiw, Poommaree, Wen, Han, Mayrhofer, Florian, Chechneva, Olga, Biswas, Sangita, and Deng, Wenbin

Subjects

Biological Sciences, Genetics, Stem Cell Research - Induced Pluripotent Stem Cell, Human Genome, Stem Cell Research, Stem Cell Research - Induced Pluripotent Stem Cell - Human, Brain Disorders, Neurosciences, Regenerative Medicine, Multiple Sclerosis, Stem Cell Research - Nonembryonic - Non-Human, Stem Cell Research - Embryonic - Human, Neurodegenerative, Autoimmune Disease, Biotechnology, Stem Cell Research - Nonembryonic - Human, Underpinning research, 1.1 Normal biological development and functioning, Neurological, Animals, Axons, Cell Differentiation, Cells, Cultured, Female, Hedgehog Proteins, Humans, Induced Pluripotent Stem Cells, Male, Mice, Myelin Sheath, Neural Stem Cells, Neurons, Oligodendrocyte Transcription Factor 2, Oligodendroglia, Pyridines, Pyrimidines, Rats, Signal Transduction, Spinal Cord, Zinc Finger Protein GLI1, Oligodendrocyte, GANT61, Myelination, NSC, Sonic Hedgehog, SHH, OPC, RNA-Seq, Differentiation, GLI1, hiPSC, hESC, Small molecule, Technology, Medical and Health Sciences, Biological sciences

Abstract

BackgroundOligodendrocytes are a type of glial cells that synthesize the myelin sheath around the axons and are critical for the nerve conduction in the CNS. Oligodendrocyte death and defects are the leading causes of several myelin disorders such as multiple sclerosis, progressive multifocal leukoencephalopathy, periventricular leukomalacia, and several leukodystrophies. Temporal activation of the Sonic Hedgehog (SHH) pathway is critical for the generation of oligodendrocyte progenitors, and their differentiation and maturation in the brain and spinal cord during embryonic development in mammals.MethodsOur protocol utilized adherent cultures of human induced pluripotent stem cells (iPSC) and human embryonic stem cells (hESCs) with a green fluorescent protein (GFP) reporter knocked into one allele of the OLIG2 gene locus, dual SMAD inhibition, and transient partial inhibition of glioma-associated oncogene 1 (GLI1) by the small molecule GANT61 during the formation of the SOX2/PAX6-positive neural stem cells (NSCs). The SHH pathway was later restimulated by a Smoothened agonist purmorphamine to induce the generation of OLIG2 glial precursors. One hundred ninety-two individual oligodendrocyte precursor cells (OPCs) from GANT61 and control group were analyzed by single-cell RNA sequencing (RNA-Seq).ResultsWe demonstrate here that transient and partial inhibition of the SHH pathway transcription factor GLI1 in NSCs by a small molecule inhibitor GANT61 was found to generate OPCs that were more migratory and could differentiate earlier toward myelin-producing oligodendrocytes. Single-cell transcriptomic analysis (RNA-Seq) showed that GANT61-NSC-derived oligodendrocyte precursor cells (OPCs) had differential activation of some of the genes in the cytoskeleton rearrangement pathways that are involved in OPC motility and induction of maturation. At the protein level, this was also associated with higher levels of myelin-specific genes in the GANT61 group compared to controls. GANT61-NSC-derived OPCs were functional and could generate compact myelin in vitro and in vivo after transplantation in myelin-deficient shiverer mice.ConclusionsThis is a small molecule-based in vitro protocol that leads to the faster generation of functional oligodendrocytes. The development of protocols that lead to efficient and faster differentiation of oligodendrocytes from progenitors provides important advances toward the development of autologous neural stem cell-based therapies using human iPSCs.

Published

2019

14. BIN1 Induces the Formation of T-Tubules and Adult-Like Ca2+ Release Units in Developing Cardiomyocytes

Author

De La Mata, Ana, Tajada, Sendoa, O'Dwyer, Samantha, Matsumoto, Collin, Dixon, Rose E, Hariharan, Nirmala, Moreno, Claudia M, and Santana, Luis Fernando

Subjects

Medical Physiology, Biomedical and Clinical Sciences, Cardiovascular, Regenerative Medicine, Stem Cell Research - Embryonic - Human, Stem Cell Research, Heart Disease, Underpinning research, 1.1 Normal biological development and functioning, Adaptor Proteins, Signal Transducing, Calcium, Calcium Signaling, Cell Differentiation, Humans, Myocytes, Cardiac, Nuclear Proteins, Tumor Suppressor Proteins, hESC, Cardiac myocytes, BIN1, T-tubules, Ca(V)1.2, Calcium release units, CaV1.2, Biological Sciences, Technology, Medical and Health Sciences, Immunology, Biological sciences, Biomedical and clinical sciences

Abstract

Human embryonic stem cell-derived cardiomyocytes (hESC-CMs) are at the center of new cell-based therapies for cardiac disease, but may also serve as a useful in vitro model for cardiac cell development. An intriguing feature of hESC-CMs is that although they express contractile proteins and have sarcomeres, they do not develop transverse-tubules (T-tubules) with adult-like Ca2+ release units (CRUs). We tested the hypothesis that expression of the protein BIN1 in hESC-CMs promotes T-tubules formation, facilitates CaV 1.2 channel clustering along the tubules, and results in the development of stable CRUs. Using electrophysiology, [Ca2+ ]i imaging, and super resolution microscopy, we found that BIN1 expression induced T-tubule development in hESC-CMs, while increasing differentiation toward a more ventricular-like phenotype. Voltage-gated CaV 1.2 channels clustered along the surface sarcolemma and T-tubules of hESC-CM. The length and width of the T-tubules as well as the expression and size of CaV 1.2 clusters grew, as BIN1 expression increased and cells matured. BIN1 expression increased CaV 1.2 channel activity and the probability of coupled gating within channel clusters. Interestingly, BIN1 clusters also served as sites for sarcoplasmic reticulum (SR) anchoring and stabilization. Accordingly, BIN1-expressing cells had more CaV 1.2-ryanodine receptor junctions than control cells. This was associated with larger [Ca2+ ]i transients during excitation-contraction coupling. Our data support the view that BIN1 is a key regulator of T-tubule formation and CaV 1.2 channel delivery. By studying the role of BIN1 during the differentiation of hESC-CMs, we show that BIN1 is also important for CaV 1.2 channel clustering, junctional SR organization, and the establishment of excitation-contraction coupling. Stem Cells 2019;37:54-64.

Published

2019

15. Generation of CD34 + CD43 + Hematopoietic Progenitors to Induce Thymocytes from Human Pluripotent Stem Cells.

Author

Flippe, Léa, Gaignerie, Anne, Sérazin, Céline, Baron, Olivier, Saulquin, Xavier, Anegon, Ignacio, David, Laurent, and Guillonneau, Carole

Subjects

*HUMAN stem cells, *PLURIPOTENT stem cells, *THYMOCYTES, *HUMAN embryonic stem cells, *T cells, *BLOOD groups, *HEMATOPOIETIC stem cells

Abstract

Immunotherapy using primary T cells has revolutionized medical care in some pathologies in recent years, but limitations associated to challenging cell genome edition, insufficient cell number production, the use of only autologous cells, and the lack of product standardization have limited its clinical use. The alternative use of T cells generated in vitro from human pluripotent stem cells (hPSCs) offers great advantages by providing a self-renewing source of T cells that can be readily genetically modified and facilitate the use of standardized universal off-the-shelf allogeneic cell products and rapid clinical access. However, despite their potential, a better understanding of the feasibility and functionality of T cells differentiated from hPSCs is necessary before moving into clinical settings. In this study, we generated human-induced pluripotent stem cells from T cells (T-iPSCs), allowing for the preservation of already recombined TCR, with the same properties as human embryonic stem cells (hESCs). Based on these cells, we differentiated, with high efficiency, hematopoietic progenitor stem cells (HPSCs) capable of self-renewal and differentiation into any cell blood type, in addition to DN3a thymic progenitors from several T-iPSC lines. In order to better comprehend the differentiation, we analyzed the transcriptomic profiles of the different cell types and demonstrated that HPSCs differentiated from hiPSCs had very similar profiles to cord blood hematopoietic stem cells (HSCs). Furthermore, differentiated T-cell progenitors had a similar profile to thymocytes at the DN3a stage of thymic lymphopoiesis. Therefore, utilizing this approach, we were able to regenerate precursors of therapeutic human T cells in order to potentially treat a wide range of diseases. [ABSTRACT FROM AUTHOR]

Published

2022

16. Differentiating Human Pluripotent Stem Cells to Cardiomyocytes Using Purified Extracellular Matrix Proteins.

Author

Barnes, Ashlynn M., Holmstoen, Tessa B., Bonham, Andrew J., and Rowland, Teisha J.

Subjects

*PLURIPOTENT stem cells, *HUMAN stem cells, *HUMAN embryonic stem cells, *EXTRACELLULAR matrix, *PEPTIDES, *EXTRACELLULAR matrix proteins, *REGENERATIVE medicine

Abstract

Human embryonic stem cells (hESCs) and induced pluripotent stem cells (iPSCs) can be differentiated into cardiomyocytes (hESC-CMs and iPSC-CMs, respectively), which hold great promise for cardiac regenerative medicine and disease modeling efforts. However, the most widely employed differentiation protocols require undefined substrates that are derived from xenogeneic (animal) products, contaminating resultant hESC- and iPSC-CM cultures with xenogeneic proteins and limiting their clinical applicability. Additionally, typical hESC- and iPSC-CM protocols produce CMs that are significantly contaminated by non-CMs and that are immature, requiring lengthy maturation procedures. In this review, we will summarize recent studies that have investigated the ability of purified extracellular matrix (ECM) proteins to support hESC- and iPSC-CM differentiation, with a focus on commercially available ECM proteins and coatings to make such protocols widely available to researchers. The most promising of the substrates reviewed here include laminin-521 with laminin-221 together or Synthemax (a synthetic vitronectin-based peptide coating), which both resulted in highly pure CM cultures. Future efforts are needed to determine whether combinations of specific purified ECM proteins or derived peptides could further improve CM maturation and culture times, and significantly improve hESC- and iPSC-CM differentiation protocols. [ABSTRACT FROM AUTHOR]

Published

2022

17. Patients' views on using human embryonic stem cells to treat Parkinson's disease: an interview study.

Author

Drevin, Jennifer, Nyholm, Dag, Widner, Håkan, Van Vliet, Trinette, Viberg Johansson, Jennifer, Jiltsova, Elena, and Hansson, Mats

Subjects

HUMAN embryonic stem cells, PARKINSON'S disease, EMBRYONIC stem cells, HUMAN embryos

Abstract

Background: Human embryonic stem cells (hESC) as a source for the development of advanced therapy medicinal products are considered for treatment of Parkinson's disease (PD). Research has shown promising results and opened an avenue of great importance for patients who currently lack a disease modifying therapy. The use of hESC has given rise to moral concerns and been the focus of often heated debates on the moral status of human embryos. Approval for marketing is still pending.Objective: To Investigate the perspectives and concerns of patients with PD, patients being the directly concerned stakeholders in the ethical discussion.Methods: Qualitative semi-structured interviews related to this new therapy in seventeen patients from two Swedish cities.Results: The participants expressed various interests related to the use of human embryos for development of medicinal therapies; however, overall, they were positive towards the use of hESC for treatment of PD. It was deemed important that the donating woman or couple made the choice to donate embryos voluntarily. Furthermore, there were concerns that the industry does not always prioritise the patient over profit; thus, transparency was seen as important. [ABSTRACT FROM AUTHOR]

Published

2022

18. The Manufacture of Xeno- and Feeder-Free Clinical-Grade Human Embryonic Stem Cell Lines: First Step for Cell Therapy.

Author

Souralova, Tereza, Rehakova, Daniela, Jeseta, Michal, Tesarova, Lenka, Beranek, Jindrich, Ventruba, Pavel, Hampl, Ales, and Koutna, Irena

Subjects

*HUMAN embryonic stem cells, *CELLULAR therapy, *EMBRYONIC stem cells, *CURRENT good manufacturing practices, *CELL lines, *PLURIPOTENT stem cells

Abstract

Human embryonic stem cells (hESCs) are increasingly used in clinical trials as they can change the outcome of treatment for many human diseases. They are used as a starting material for further differentiation into specific cell types and to achieve the desirable result of the cell therapy; thus, the quality of hESCs has to be taken into account. Therefore, current good manufacturing practice (cGMP) has to be implemented in the transport of embryos, derivation of inner cell mass to xeno-free, feeder-free and defined hESC culture, and cell freezing. The in-depth characterization of hESC lines focused on safety, pluripotency, differentiation potential and genetic background has to complement this process. In this paper, we show the derivation of three clinical-grade hESC lines, MUCG01, MUCG02, and MUCG03, following these criteria. We developed and validated the system for the manufacture of xeno-free and feeder-free clinical-grade hESC lines that present high-quality starting material suitable for cell therapy according to cGMP. [ABSTRACT FROM AUTHOR]

Published

2022

19. The role of glial pathology in Huntington's disease

Author

Goldman, Steven A. and Goldman, Steven A.

Abstract

This review will focus on the contribution of glial pathology to HD, particularly so with regard to diseased glial progenitor cells and their derived astrocytes and oligodendrocytes. It will briefly discuss the body of data identifying the contribution of glial dysfunction to disease phenotype in rodent models of HD, and will then focus on recent studies of cell-intrinsic glial transcriptional dysregulation in HD. The review will emphasize recent studies of diseased human cells and humanized models of HD glial pathology, and on the contributions of that glial pathology to neuronal and synaptic dysfunction in HD., This review will focus on the contribution of glial pathology to HD, particularly so with regard to diseased glial progenitor cells and their derived astrocytes and oligodendrocytes. It will briefly discuss the body of data identifying the contribution of glial dysfunction to disease phenotype in rodent models of HD, and will then focus on recent studies of cell-intrinsic glial transcriptional dysregulation in HD. The review will emphasize recent studies of diseased human cells and humanized models of HD glial pathology, and on the contributions of that glial pathology to neuronal and synaptic dysfunction in HD.

Published

2024

20. Proteomic and functional comparison between human induced and embryonic stem cells.

Author

Brenes AJ, Griesser E, Sinclair LV, Davidson L, Prescott AR, Singh F, Hogg EKJ, Espejo-Serrano C, Jiang H, Yoshikawa H, Platani M, Swedlow JR, Findlay GM, Cantrell DA, and Lamond AI

Subjects

Humans, Embryonic Stem Cells metabolism, Embryonic Stem Cells cytology, Mitochondria metabolism, Cell Line, Human Embryonic Stem Cells metabolism, Induced Pluripotent Stem Cells metabolism, Induced Pluripotent Stem Cells cytology, Proteomics, Proteome metabolism

Abstract

Human induced pluripotent stem cells (hiPSCs) have great potential to be used as alternatives to embryonic stem cells (hESCs) in regenerative medicine and disease modelling. In this study, we characterise the proteomes of multiple hiPSC and hESC lines derived from independent donors and find that while they express a near-identical set of proteins, they show consistent quantitative differences in the abundance of a subset of proteins. hiPSCs have increased total protein content, while maintaining a comparable cell cycle profile to hESCs, with increased abundance of cytoplasmic and mitochondrial proteins required to sustain high growth rates, including nutrient transporters and metabolic proteins. Prominent changes detected in proteins involved in mitochondrial metabolism correlated with enhanced mitochondrial potential, shown using high-resolution respirometry. hiPSCs also produced higher levels of secreted proteins, including growth factors and proteins involved in the inhibition of the immune system. The data indicate that reprogramming of fibroblasts to hiPSCs produces important differences in cytoplasmic and mitochondrial proteins compared to hESCs, with consequences affecting growth and metabolism. This study improves our understanding of the molecular differences between hiPSCs and hESCs, with implications for potential risks and benefits for their use in future disease modelling and therapeutic applications., Competing Interests: AB, LS, LD, AP, FS, EH, CE, HJ, HY, GF, DC No competing interests declared, EG Now works for Boehringer Ingelheim Pharma GmbH & Co KG, MP Board member of Tartan Cell Technologies Ltd, JS Board member of Tartan Cell Technologies Ltd and Glencoe Software Ltd, AL Board member of Tartan Cell Technologies Ltd and Platinum Informatics Ltd, (© 2024, Brenes et al.)

Published

2024

21. Telomere fusions as a signal of term placental aging? A pilot study

Author

Fabiana B Kohlrausch, Fang Wang, Danxia Luo, Rebecca Mahn, and David L Keefe

Subjects

placenta, hesc, genomic instability, telomere, fusion, Reproduction, QH471-489, Gynecology and obstetrics, RG1-991

Abstract

The placenta plays an essential role at the beginning of life, nourishing and supporting the fetus, but its life span is limited. In late pregnancy, the placenta develops signs of aging, including inflammation and impaired function, which may complicate pregnancy. Placentas also show another sign of aging – cells with extra or missing chromosomes. Chromosomally abnormal cells could gather in the placenta if they get stranded there and/or if the cells do not separate normally. Chromosome separation goes wrong in aging cells when the DNA sequences, which protect the ends of the chromosomes, erode. When chromosomes lose their protective caps, they fuse which leads to abnormal numbers of chromosomes. In this pilot study, for the first time, we found fusions between the caps in a human placenta when it reaches full term. More studies are needed to decide whether this has an influence on how the placenta works and outcomes of pregnancy.

Published

2022

22. Stabilisation of hepatocyte phenotype using synthetic materials

Author

Lucendo Villarin, Baltasar, Hay, David, and Forbes, Stuart

Subjects

611, hESC, hepatocytes, PU134, synthetic substrate, phenotypic stability

Abstract

Primary human hepatocytes are a scare resource with limited lifespan and variable function which diminishes with time in culture. As a consequence, their use in tissue modelling and therapy is restricted. Human embryonic stem cells (hESC) could provide a stable source of human tissue due to their self-renewal properties and their ability to give rise to all the cell types of the human body. Therefore, hESC have the potential to provide an unlimited supply of hepatocytes. To date, the use of hESCs-derived somatic cells is limited due to the undefined, variable and xeno-containing microenvironment that influences the cell performance and life span, limiting scale-up and downstream application. Therefore, the development of highly defined cell based systems is required if the true potential of stem cell derived hepatocytes is to be realised. In order to replace the use of animal derived culture substrates to differentiate and maintain hESCs-derived hepatocytes, an interdisciplinary approach was employed to define synthetic materials, which maintain hepatocyte-like cell phenotype in culture. A simple polyurethane, PU134, was identified which improved hepatocyte performance and stability when compared to biological matrices. Moreover, the synthetic polymer was amenable to scale up and demonstrated batch-to-batch consistency. I subsequently used the synthetic polymer surface to probe the underlying biology, identifying key modulators of hepatocyte-like cell phenotype. This resulted in the identification of a novel genetic signature, MMP13, CTNND2 and THBS2, which was associated with stable hepatocyte performance. Importantly, those findings could be translated to two hESC lines derived at GMP. In conclusion, hepatocyte differentiation of pluripotent stem cells requires a defined microenvironment. The novel gene signature identified in this study represents an example of how to deliver stable hESCs-derived hepatocytes.

Published

2016

23. Evidence of Infection of Human Embryonic Stem Cells by SARS-CoV-2.

Author

Zeng, Weijie, Xing, Fan, Ji, Yanxi, Yang, Sidi, Xu, Tiefeng, Huang, Siyao, Li, Chunmei, Wu, Junyu, Cao, Liu, and Guo, Deyin

Subjects

HUMAN embryonic stem cells, SARS-CoV-2, EMBRYONIC stem cells

Abstract

The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) was initially described to target the respiratory system and now has been reported to infect a variety of cell types, including cardiomyocytes, neurons, hepatocytes, and gut enterocytes. However, it remains unclear whether the virus can directly infect human embryonic stem cells (hESCs) or early embryos. Herein, we sought to investigate this question in a cell-culture system of hESCs. Both the RNA and S protein of SARS-CoV-2 were detected in the infected hESCs and the formation of syncytium was observed. The increased level of subgenomic viral RNA and the presence of dsRNA indicate active replication of SARS-CoV-2 in hESCs. The increase of viral titers in the supernatants revealed virion release, further indicating the successful life cycle of SARS-CoV-2 in hESCs. Remarkably, immunofluorescence microscopy showed that only a small portion of hESCs were infected, which may reflect low expression of SARS-CoV-2 receptors. By setting |log2 (fold change)| > 0.5 as the threshold, a total of 1,566 genes were differentially expressed in SARS-CoV-2-infected hESCs, among which 17 interferon-stimulated genes (ISGs) were significantly upregulated. Altogether, our results provide novel evidence to support the ability of SARS-CoV-2 to infect and replicate in hESCs. [ABSTRACT FROM AUTHOR]

Published

2022

24. Variant-to-Gene-Mapping Analyses Reveal a Role for the Hypothalamus in Genetic Susceptibility to Inflammatory Bowel DiseaseSummary

Author

Chiara Lasconi, Matthew C. Pahl, Diana L. Cousminer, Claudia A. Doege, Alessandra Chesi, Kenyaita M. Hodge, Michelle E. Leonard, Sumei Lu, Matthew E. Johnson, Chun Su, Reza K. Hammond, James A. Pippin, Natalie A. Terry, Louis R. Ghanem, Rudolph L. Leibel, Andrew D. Wells, and Struan F.A. Grant

Subjects

HPA, Stress, Colonoids, hESC, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Background & Aims: Inflammatory bowel disease (IBD) is a polygenic disorder characterized principally by dysregulated inflammation impacting the gastrointestinal tract. However, there also is increasing evidence for a clinical association with stress and depression. Given the role of the hypothalamus in stress responses and in the pathogenesis of depression, useful insights could be gleaned from understanding its genetic role in IBD. Methods: We conducted genetic correlation analyses on publicly available genome-wide association study summary statistics for depression and IBD traits to identify genetic commonalities. We used partitioned linkage disequilibrium score regression, leveraging our ATAC sequencing and promoter-focused Capture C data, to measure enrichment of IBD single-nucleotide polymorphisms within promoter-interacting open chromatin regions of human embryonic stem cell-derived hypothalamic-like neurons (HNs). Using the same data sets, we performed variant-to-gene mapping to implicate putative IBD effector genes in HNs. To contrast these results, we similarly analyzed 3-dimensional genomic data generated in epithelium-derived colonoids from rectal biopsy specimens from donors without pathologic disease noted at the time of colonoscopy. Finally, we conducted enrichment pathway analyses on the implicated genes to identify putative IBD dysfunctional pathways. Results: We found significant genetic correlations (rg) of 0.122 with an adjusted P (Padj) = 1.4 × 10-4 for IBD: rg = 0.122; Padj = 2.5 × 10-3 for ulcerative colitis and genetic correlation (rg) = 0.094; Padj = 2.5 × 10-3 for Crohn’s disease, and significant approximately 4-fold (P = .005) and approximately 7-fold (P = .03) enrichment of IBD single-nucleotide polymorphisms in HNs and colonoids, respectively. We implicated 25 associated genes in HNs, among which CREM, CNTF, and RHOA encode key regulators of stress. Seven genes also additionally were implicated in the colonoids. We observed an overall enrichment for immune and hormonal signaling pathways, and a colonoid-specific enrichment for microbiota-relevant terms. Conclusions: Our results suggest that the hypothalamus warrants further study in the context of IBD pathogenesis.

Published

2021

25. Evidence of Infection of Human Embryonic Stem Cells by SARS-CoV-2

Author

Weijie Zeng, Fan Xing, Yanxi Ji, Sidi Yang, Tiefeng Xu, Siyao Huang, Chunmei Li, Junyu Wu, Liu Cao, and Deyin Guo

Subjects

SARS-CoV-2, infection, replication, mechanism, hESC, Microbiology, QR1-502

Abstract

The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) was initially described to target the respiratory system and now has been reported to infect a variety of cell types, including cardiomyocytes, neurons, hepatocytes, and gut enterocytes. However, it remains unclear whether the virus can directly infect human embryonic stem cells (hESCs) or early embryos. Herein, we sought to investigate this question in a cell-culture system of hESCs. Both the RNA and S protein of SARS-CoV-2 were detected in the infected hESCs and the formation of syncytium was observed. The increased level of subgenomic viral RNA and the presence of dsRNA indicate active replication of SARS-CoV-2 in hESCs. The increase of viral titers in the supernatants revealed virion release, further indicating the successful life cycle of SARS-CoV-2 in hESCs. Remarkably, immunofluorescence microscopy showed that only a small portion of hESCs were infected, which may reflect low expression of SARS-CoV-2 receptors. By setting |log2 (fold change)| > 0.5 as the threshold, a total of 1,566 genes were differentially expressed in SARS-CoV-2-infected hESCs, among which 17 interferon-stimulated genes (ISGs) were significantly upregulated. Altogether, our results provide novel evidence to support the ability of SARS-CoV-2 to infect and replicate in hESCs.

Published

2022

26. Aminophylline Induces Two Types of Arrhythmic Events in Human Pluripotent Stem Cell–Derived Cardiomyocytes.

Author

Klimovic, Simon, Scurek, Martin, Pesl, Martin, Beckerova, Deborah, Jelinkova, Sarka, Urban, Tomas, Kabanov, Daniil, Starek, Zdenek, Bebarova, Marketa, Pribyl, Jan, Rotrekl, Vladimir, and Brat, Kristian

Subjects

ATOMIC force microscopes, PLURIPOTENT stem cells, HEART cells, MYOCARDIUM, PHARMACODYNAMICS, ATOMIC force microscopy

Abstract

Cardiac side effects of some pulmonary drugs are observed in clinical practice. Aminophylline, a methylxanthine bronchodilator with documented proarrhythmic action, may serve as an example. Data on the action of aminophylline on cardiac cell electrophysiology and contractility are not available. Hence, this study was focused on the analysis of changes in the beat rate and contraction force of human pluripotent stem cell–derived cardiomyocytes (hPSC-CMs) and HL-1 cardiomyocytes in the presence of increasing concentrations of aminophylline (10 µM–10 mM in hPSC-CM and 8–512 µM in HL-1 cardiomyocytes). Basic biomedical parameters, namely, the beat rate (BR) and contraction force, were assessed in hPSC-CMs using an atomic force microscope (AFM). The beat rate changes under aminophylline were also examined on the HL-1 cardiac muscle cell line via a multielectrode array (MEA). Additionally, calcium imaging was used to evaluate the effect of aminophylline on intracellular Ca2+ dynamics in HL-1 cardiomyocytes. The BR was significantly increased after the application of aminophylline both in hPSC-CMs (with 10 mM aminophylline) and in HL-1 cardiomyocytes (with 256 and 512 µM aminophylline) in comparison with controls. A significant increase in the contraction force was also observed in hPSC-CMs with 10 µM aminophylline (a similar trend was visible at higher concentrations as well). We demonstrated that all aminophylline concentrations significantly increased the frequency of rhythm irregularities (extreme interbeat intervals) both in hPSC-CMs and HL-1 cells. The occurrence of the calcium sparks in HL-1 cardiomyocytes was significantly increased with the presence of 512 µM aminophylline. We conclude that the observed aberrant cardiomyocyte response to aminophylline suggests an arrhythmogenic potential of the drug. The acquired data represent a missing link between the arrhythmic events related to the aminophylline/theophylline treatment in clinical practice and describe cellular mechanisms of methylxanthine arrhythmogenesis. An AFM combined with hPSC-CMs may serve as a robust platform for direct drug effect screening. [ABSTRACT FROM AUTHOR]

Published

2022

27. Characterization of the individual capacity for repair of genotoxic damage of a Bulgarian hESC line and two commonly used stabilized cell lines.

Author

Petkova, Rumena, Chelenkova, Pavlina, Arabadjiev, Borislav, Pankov, Roumen, and Chakarov, Stoyan

Subjects

*CELL lines, *STEM cell culture, *HUMAN embryonic stem cells, *REPAIRING, *STEM cell factor, *MAINTENANCE, *HUMAN embryos, *DNA repair

Abstract

The number of stem cell lines worldwide grows steadily, including disease-specific lines and lines derived from specific tissues. The proportion of stem cell lines that were established in strictly xeno-free conditions is rapidly increasing, but it is still unclear whether these lines may be maintained in vitro for prolonged periods of time with satisfactory survival rates and minimal loss of their 'stemness' properties. The efficiency of repair of DNA damage has recently emerged as an important factor for maintenance of stem cells in culture with minimal genomic changes and preservation of the undifferentiated state. In this study we investigated the individual capacity for repair of DNA damage/maintenance of genomic integrity and additional markers in one human embryonic stem cell (hESC) line derived in Bulgaria from a discarded embryo and two of the human T-leukaemia cell lines commonly used for research purposes (T-1301 and Jurkat E6-1). Knowledge about the status of the studied cancer cell lines may be valuable for research purposes. Data about the individual repair capacity and the genetic risk for common late-onset diseases of newly established hESC lines as well as hESC lines currently in use may become a valuable tool in the assessment of the applicability of pluripotent human cell lines for research purposes, clinical trials and, potentially, clinical applications. [ABSTRACT FROM AUTHOR]

Published

2022

28. Aminophylline Induces Two Types of Arrhythmic Events in Human Pluripotent Stem Cell–Derived Cardiomyocytes

Author

Simon Klimovic, Martin Scurek, Martin Pesl, Deborah Beckerova, Sarka Jelinkova, Tomas Urban, Daniil Kabanov, Zdenek Starek, Marketa Bebarova, Jan Pribyl, Vladimir Rotrekl, and Kristian Brat

Subjects

aminophylline, IPSC, hESC, cardiomyocytes, drug cardiotoxicity, atomic force microscopy, Therapeutics. Pharmacology, RM1-950

Abstract

Cardiac side effects of some pulmonary drugs are observed in clinical practice. Aminophylline, a methylxanthine bronchodilator with documented proarrhythmic action, may serve as an example. Data on the action of aminophylline on cardiac cell electrophysiology and contractility are not available. Hence, this study was focused on the analysis of changes in the beat rate and contraction force of human pluripotent stem cell–derived cardiomyocytes (hPSC-CMs) and HL-1 cardiomyocytes in the presence of increasing concentrations of aminophylline (10 µM–10 mM in hPSC-CM and 8–512 µM in HL-1 cardiomyocytes). Basic biomedical parameters, namely, the beat rate (BR) and contraction force, were assessed in hPSC-CMs using an atomic force microscope (AFM). The beat rate changes under aminophylline were also examined on the HL-1 cardiac muscle cell line via a multielectrode array (MEA). Additionally, calcium imaging was used to evaluate the effect of aminophylline on intracellular Ca2+ dynamics in HL-1 cardiomyocytes. The BR was significantly increased after the application of aminophylline both in hPSC-CMs (with 10 mM aminophylline) and in HL-1 cardiomyocytes (with 256 and 512 µM aminophylline) in comparison with controls. A significant increase in the contraction force was also observed in hPSC-CMs with 10 µM aminophylline (a similar trend was visible at higher concentrations as well). We demonstrated that all aminophylline concentrations significantly increased the frequency of rhythm irregularities (extreme interbeat intervals) both in hPSC-CMs and HL-1 cells. The occurrence of the calcium sparks in HL-1 cardiomyocytes was significantly increased with the presence of 512 µM aminophylline. We conclude that the observed aberrant cardiomyocyte response to aminophylline suggests an arrhythmogenic potential of the drug. The acquired data represent a missing link between the arrhythmic events related to the aminophylline/theophylline treatment in clinical practice and describe cellular mechanisms of methylxanthine arrhythmogenesis. An AFM combined with hPSC-CMs may serve as a robust platform for direct drug effect screening.

Published

2022

29. Building Implantable Human Liver Tissue from Pluripotent Stem Cells

Author

David Hay

Subjects

hESC, iPSC, liver, hepatocyte, endothelial cell, tissue engineering, Plant ecology, QK900-989, Animal biochemistry, QP501-801, Biology (General), QH301-705.5

Abstract

Liver disease is an escalating global health issue. While liver transplantation is an effective mode of therapy, patient mortality has increased due to the shortage of donor organs. Therefore, developing renewable sources of human liver tissue is attractive. Pluripotent stem cell-derived liver tissue represents a potential alternative to cadaver derived hepatocytes and whole organ transplant. At present, two-dimensional differentiation procedures deliver tissue lacking certain functions and phenotypic instability. Efforts to overcome these limiting factors have led to the building of three-dimensional (3D) cellular aggregates. Although enabling for the field, their widespread application and adoption is limited due to the reliance on variable biological components. Our study focus on developing 3D liver tissue under defined conditions. We demonstrate that 3D derived tissue can be generated at scale and implanted underneath the skin of mice. Excitingly, implanted human tissue provides support to mice with metabolic liver disease. This includes immunocompetent recipients. In addition to their clinical application, in vitro generated 3D tissues have important roles to perform in developing safe and efficacious medicines to treat human diseases. We demonstrate that stem cell derived 3D liver tissue exhibits liver cell phenotype for over one year in culture, providing an attractive resource for long-term disease modelling and screening studies. In conclusion, stem cell derived liver tissue has great potential for in vitro and in vivo endeavours. Our most recent advances will be presented at the meeting.

Published

2023

30. Accept or Reject: The Role of Immune Tolerance in the Development of Stem Cell Therapies and Possible Future Approaches.

Author

Haworth, Richard and Sharpe, Michaela

Subjects

*STEM cell treatment, *EMBRYONIC stem cells, *IMMUNOLOGICAL tolerance, *PLURIPOTENT stem cells, *SOMATIC cells

Abstract

In 2011, Goldring and colleagues published a review article describing the potential safety issues of novel stem cell-derived treatments. Immunogenicity and immunotoxicity of the administered cell product were considered risks in the light of clinical experience of transplantation. The relative immunogenicity of mesenchymal stem cells, embryonic stem cells (ESCs), and induced pluripotent stem cells (iPSCs) was being addressed through in vitro and in vivo models. But the question arose as to whether the implanted cells needed to be identical to the recipient in every respect, including epigenetically, to evade immune recognition? If so, this set a high bar which may preclude use of many cells derived from iPSCs which have vestiges of a fetal phenotype and epigenetic memory of their cell of origin. However, for autologous iPSCs, the immunogenicity reduces once the surface antigen expression profile becomes close to that of the parent somatic cells. Therefore, a cell product containing incompletely differentiated cells could be more immunogenic. The properties of the administered cells, the immune privilege of the administration site, and the host immune status influence graft success or failure. In addition, the various approaches available to characterize potential immunogenicity of a cell therapy will be discussed. [ABSTRACT FROM AUTHOR]

Published

2021

31. Cellular models and therapies for age-related macular degeneration

Author

Forest, David L, Johnson, Lincoln V, and Clegg, Dennis O

Subjects

Stem Cell Research - Induced Pluripotent Stem Cell, Aging, Neurodegenerative, Regenerative Medicine, Neurosciences, Stem Cell Research, Transplantation, Macular Degeneration, Eye Disease and Disorders of Vision, Stem Cell Research - Induced Pluripotent Stem Cell - Human, Stem Cell Research - Embryonic - Human, 2.1 Biological and endogenous factors, Aetiology, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Eye, Animals, Humans, Models, Biological, Stem Cell Transplantation, AMD, RPE, Cell-culture models, hESC, iPSC, Stem-cell therapy, Biological Sciences, Medical and Health Sciences, Developmental Biology

Abstract

Age-related macular degeneration (AMD) is a complex neurodegenerative visual disorder that causes profound physical and psychosocial effects. Visual impairment in AMD is caused by the loss of retinal pigmented epithelium (RPE) cells and the light-sensitive photoreceptor cells that they support. There is currently no effective treatment for the most common form of this disease (dry AMD). A new approach to treating AMD involves the transplantation of RPE cells derived from either human embryonic or induced pluripotent stem cells. Multiple clinical trials are being initiated using a variety of cell therapies. Although many animal models are available for AMD research, most do not recapitulate all aspects of the disease, hampering progress. However, the use of cultured RPE cells in AMD research is well established and, indeed, some of the more recently described RPE-based models show promise for investigating the molecular mechanisms of AMD and for screening drug candidates. Here, we discuss innovative cell-culture models of AMD and emerging stem-cell-based therapies for the treatment of this vision-robbing disease.

Published

2015

32. Generation of CD34+CD43+ Hematopoietic Progenitors to Induce Thymocytes from Human Pluripotent Stem Cells

Author

Léa Flippe, Anne Gaignerie, Céline Sérazin, Olivier Baron, Xavier Saulquin, Ignacio Anegon, Laurent David, and Carole Guillonneau

Subjects

hiPSC, hESC, hematopoietic progenitor, T-cell progenitor, hematopoietic differentiation, Cytology, QH573-671

Abstract

Immunotherapy using primary T cells has revolutionized medical care in some pathologies in recent years, but limitations associated to challenging cell genome edition, insufficient cell number production, the use of only autologous cells, and the lack of product standardization have limited its clinical use. The alternative use of T cells generated in vitro from human pluripotent stem cells (hPSCs) offers great advantages by providing a self-renewing source of T cells that can be readily genetically modified and facilitate the use of standardized universal off-the-shelf allogeneic cell products and rapid clinical access. However, despite their potential, a better understanding of the feasibility and functionality of T cells differentiated from hPSCs is necessary before moving into clinical settings. In this study, we generated human-induced pluripotent stem cells from T cells (T-iPSCs), allowing for the preservation of already recombined TCR, with the same properties as human embryonic stem cells (hESCs). Based on these cells, we differentiated, with high efficiency, hematopoietic progenitor stem cells (HPSCs) capable of self-renewal and differentiation into any cell blood type, in addition to DN3a thymic progenitors from several T-iPSC lines. In order to better comprehend the differentiation, we analyzed the transcriptomic profiles of the different cell types and demonstrated that HPSCs differentiated from hiPSCs had very similar profiles to cord blood hematopoietic stem cells (HSCs). Furthermore, differentiated T-cell progenitors had a similar profile to thymocytes at the DN3a stage of thymic lymphopoiesis. Therefore, utilizing this approach, we were able to regenerate precursors of therapeutic human T cells in order to potentially treat a wide range of diseases.

Published

2022

33. Induction of early neural precursors and derivation of tripotent neural stem cells from human pluripotent stem cells under xeno‐free conditions

Author

Nguyen, Hal X, Nekanti, Usha, Haus, Daniel L, Funes, Gabrielle, Moreno, Denisse, Kamei, Noriko, Cummings, Brian J, and Anderson, Aileen J

Subjects

Regenerative Medicine, Stem Cell Research - Embryonic - Human, Neurosciences, Stem Cell Research - Induced Pluripotent Stem Cell, Stem Cell Research - Induced Pluripotent Stem Cell - Human, Stem Cell Research, Underpinning research, 1.1 Normal biological development and functioning, Generic health relevance, Cell Adhesion, Cell Differentiation, Cell Proliferation, Compomers, Embryonic Stem Cells, Epidermal Growth Factor, Fibroblast Growth Factor 2, Flow Cytometry, Gene Expression, Homeodomain Proteins, Humans, Induced Pluripotent Stem Cells, Intracellular Signaling Peptides and Proteins, Karyotype, Nanog Homeobox Protein, Nerve Tissue Proteins, Nuclear Proteins, Octamer Transcription Factor-3, Oligodendroglia, Proliferating Cell Nuclear Antigen, hESC, hiPSC, human neural stem cells, neuralization, oligoprogenitors, xeno-free, HESC, HiPSC, Human neural stem cells, Neuralization, Oligoprogenitors, Xeno-free, Zoology, Medical Physiology, Neurology & Neurosurgery

Abstract

Human embryonic stem cells (hESC) and induced pluripotent stem cells (hiPSC) can differentiate into many cell types and are important for regenerative medicine; however, further work is needed to reliably differentiate hESC and hiPSC into neural-restricted multipotent derivatives or specialized cell types under conditions that are free from animal products. Toward this goal, we tested the transition of hESC and hiPSC lines onto xeno-free (XF) / feeder-free conditions and evaluated XF substrate preference, pluripotency, and karyotype. Critically, XF transitioned H9 hESC, Shef4 hESC, and iPS6-9 retained pluripotency (Oct-4 and NANOG), proliferation (MKI67 and PCNA), and normal karyotype. Subsequently, XF transitioned hESC and hiPSC were induced with epidermal growth factor (EGF) and basic fibroblast growth factor (bFGF) to generate neuralized spheres containing primitive neural precursors, which could differentiate into astrocytes and neurons, but not oligoprogenitors. Further neuralization of spheres via LIF supplementation and attachment selection on CELLstart substrate generated adherent human neural stem cells (hNSC) with normal karyotype and high proliferation potential under XF conditions. Interestingly, adherent hNSC derived from H9, Shef4, and iPS6-9 differentiated into significant numbers of O4+ oligoprogenitors (∼20-30%) with robust proliferation; however, very few GalC+ cells were observed (∼2-4%), indicative of early oligodendrocytic lineage commitment. Overall, these data demonstrate the transition of multiple hESC and hiPSC lines onto XF substrate and media conditions, and a reproducible neuralization method that generated neural derivatives with multipotent cell fate potential and normal karyotype.

Published

2014

34. Mechanisms of action of hESC-secreted proteins that enhance human and mouse myogenesis

Author

Yousef, Hanadie, Conboy, Michael J, Mamiya, Hikaru, Zeiderman, Matthew, Schlesinger, Christina, Schaffer, David V, and Conboy, Irina M

Subjects

Transplantation, Stem Cell Research - Embryonic - Human, Stem Cell Research, Neurosciences, Regenerative Medicine, Stem Cell Research - Nonembryonic - Non-Human, Stem Cell Research - Nonembryonic - Human, 1.1 Normal biological development and functioning, Underpinning research, Musculoskeletal, Generic health relevance, Animals, Culture Media, Conditioned, Embryonic Stem Cells, Humans, Intracellular Signaling Peptides and Proteins, Membrane Proteins, Mice, Muscle Development, Receptor, Notch1, Signal Transduction, Transforming Growth Factor beta, hESC, muscle, myogenesis, Notch, MAPK, aging, rejuvenation, stem cell, Biochemistry and Cell Biology, Physiology, Oncology and Carcinogenesis, Developmental Biology

Abstract

Adult stem cells grow poorly in vitro compared to embryonic stem cells, and in vivo stem cell maintenance and proliferation by tissue niches progressively deteriorates with age. We previously reported that factors produced by human embryonic stem cells (hESCs) support a robust regenerative capacity for adult and old mouse muscle stem/progenitor cells. Here we extend these findings to human muscle progenitors and investigate underlying molecular mechanisms. Our results demonstrate that hESC-conditioned medium enhanced the proliferation of mouse and human muscle progenitors. Furthermore, hESC-produced factors activated MAPK and Notch signaling in human myogenic progenitors, and Delta/Notch-1 activation was dependent on MAPK/pERK. The Wnt, TGF-β and BMP/pSmad1,5,8 pathways were unresponsive to hESC-produced factors, but BMP signaling was dependent on intact MAPK/pERK. c-Myc, p57, and p18 were key effectors of the enhanced myogenesis promoted by the hECS factors. To define some of the active ingredients of the hESC-secretome which may have therapeutic potential, a comparative proteomic antibody array analysis was performed and identified several putative proteins, including FGF2, 6 and 19 which as ligands for MAPK signaling, were investigated in more detail. These studies emphasize that a "youthful" signaling of multiple signaling pathways is responsible for the pro-regenerative activity of the hESC factors.

Published

2014

35. Expandable Lung Epithelium Differentiated from Human Embryonic Stem Cells

Author

Kotasová, Hana, Capandová, Michaela, Pelková, Vendula, Dumková, Jana, Koledová, Zuzana, Remšík, Ján, Souček, Karel, Garlíková, Zuzana, Sedláková, Veronika, Rabata, Anas, Vaňhara, Petr, Moráň, Lukáš, Pečinka, Lukáš, Porokh, Volodymyr, Kučírek, Martin, Streit, Libor, Havel, Josef, and Hampl, Aleš

Published

2022

36. Hsa-miR-335 regulates cardiac mesoderm and progenitor cell differentiation

Author

Maryam Kay, Bahram Mohammad Soltani, Fahimeh Hosseini Aghdaei, Hassan Ansari, and Hossein Baharvand

Subjects

miRNA, Cardiomyocyte differentiation, hESC, WNT, TGFβ, Medicine (General), R5-920, Biochemistry, QD415-436

Abstract

Abstract Background WNT and TGFβ signaling pathways play critical regulatory roles in cardiomyocyte fate determination and differentiation. MiRNAs are also known to regulate different biological processes and signaling pathways. Here, we intended to find candidate miRNAs that are involved in cardiac differentiation through regulation of WNT and TGFβ signaling pathways. Methods Bioinformatics analysis suggested hsa-miR-335-3p and hsa-miR-335-5p as regulators of cardiac differentiation. Then, RT-qPCR, dual luciferase, TOP/FOP flash, and western blot analyses were done to confirm the hypothesis. Results Human embryonic stem cells (hESCs) were differentiated into beating cardiomyocytes, and these miRNAs showed significant expression during the differentiation process. Gain and loss of function of miR-335-3p and miR-335-5p resulted in BRACHYURY, GATA4, and NKX2-5 (cardiac differentiation markers) expression alteration during the course of hESC cardiac differentiation. The overexpression of miR-335-3p and miR-335-5p also led to upregulation of CNX43 and TNNT2 expression, respectively. Our results suggest that this might be mediated through enhancement of WNT and TGFβ signaling pathways. Conclusion Overall, we show that miR-335-3p/5p upregulates cardiac mesoderm (BRACHYURY) and cardiac progenitor cell (GATA4 and NKX2-5) markers, which are potentially mediated through activation of WNT and TGFβ signaling pathways. Our findings suggest miR-335-3p/5p to be considered as a regulator of the cardiac differentiation process.

Published

2019

37. Pancreatic progenitor epigenome maps prioritize type 2 diabetes risk genes with roles in development

Author

Ryan J Geusz, Allen Wang, Joshua Chiou, Joseph J Lancman, Nichole Wetton, Samy Kefalopoulou, Jinzhao Wang, Yunjiang Qiu, Jian Yan, Anthony Aylward, Bing Ren, P Duc Si Dong, Kyle J Gaulton, and Maike Sander

Subjects

Zebrafish, pancreas, hESC, chromatin, Type 2 diabetes, GWAS, Medicine, Science, Biology (General), QH301-705.5

Abstract

Genetic variants associated with type 2 diabetes (T2D) risk affect gene regulation in metabolically relevant tissues, such as pancreatic islets. Here, we investigated contributions of regulatory programs active during pancreatic development to T2D risk. Generation of chromatin maps from developmental precursors throughout pancreatic differentiation of human embryonic stem cells (hESCs) identifies enrichment of T2D variants in pancreatic progenitor-specific stretch enhancers that are not active in islets. Genes associated with progenitor-specific stretch enhancers are predicted to regulate developmental processes, most notably tissue morphogenesis. Through gene editing in hESCs, we demonstrate that progenitor-specific enhancers harboring T2D-associated variants regulate cell polarity genes LAMA1 and CRB2. Knockdown of lama1 or crb2 in zebrafish embryos causes a defect in pancreas morphogenesis and impairs islet cell development. Together, our findings reveal that a subset of T2D risk variants specifically affects pancreatic developmental programs, suggesting that dysregulation of developmental processes can predispose to T2D.

Published

2021

38. Hypoxia induces re‐entry of committed cells into pluripotency

Author

Mathieu, Julie, Zhang, Zhan, Nelson, Angelique, Lamba, Deepak A, Reh, Thomas A, Ware, Carol, and Ruohola‐Baker, Hannele

Subjects

Medical Biotechnology, Biological Sciences, Biomedical and Clinical Sciences, Regenerative Medicine, Stem Cell Research - Embryonic - Human, Stem Cell Research, Genetics, Transplantation, Underpinning research, 1.1 Normal biological development and functioning, Generic health relevance, Adult, Animals, Basic Helix-Loop-Helix Transcription Factors, Biomarkers, Cell Dedifferentiation, Cell Hypoxia, Cell Line, Cell Lineage, Embryonic Stem Cells, Green Fluorescent Proteins, Histone Deacetylases, Humans, Hypoxia-Inducible Factor 1, alpha Subunit, Mice, Models, Biological, Octamer Transcription Factor-3, Oxygen, Pluripotent Stem Cells, Human embryonic stem cell, Hypoxia, Stem cell fate, Plasticity, niche, dedifferentiation, hESC, Technology, Medical and Health Sciences, Immunology, Biological sciences, Biomedical and clinical sciences

Abstract

Adult stem cells reside in hypoxic niches, and embryonic stem cells (ESCs) are derived from a low oxygen environment. However, it is not clear whether hypoxia is critical for stem cell fate since for example human ESCs (hESCs) are able to self-renew in atmospheric oxygen concentrations as well. We now show that hypoxia can govern cell fate decisions since hypoxia alone can revert hESC- or iPSC-derived differentiated cells back to a stem cell-like state, as evidenced by re-activation of an Oct4-promoter reporter. Hypoxia-induced "de-differentiated" cells also mimic hESCs in their morphology, long-term self-renewal capacity, genome-wide mRNA and miRNA profiles, Oct4 promoter methylation state, cell surface markers TRA1-60 and SSEA4 expression, and capacity to form teratomas. These data demonstrate that hypoxia can influence cell fate decisions and could elucidate hypoxic niche function.

Published

2013

39. Naive Pluripotency in Human Primordial Germ Cell Development

Author

Hancock, Grace

Subjects

Developmental biology, Cellular biology, Molecular biology, embryo, hESC, PGCs, pluripotency, Primordial gem cells, Stem Cells

Abstract

Infertility is caused by a multitude of genetic and environmental factors, and many who seek treatment are unresponsive to in vitro fertilization. Treatments such as these are costly, as well as physically and emotionally demanding, so it is critical to better understand the individual underlying causes of infertility to improve patient care. Germ cells give rise to the next generation and are responsible for passing along genetic and epigenetic information, and abnormalities in germ cell development can result in infertility. In addition, mutations in certain genes related to germ cell formation can contribute to their improper development, resulting in germ cell tumor formation or other developmental disorders in their future offspring. In these studies, we investigated the earliest cell type in the human germline, known as human Primordial Germ Cells (hPGCs). We developed models and techniques to represent hPGC formation and identified genes of interest to investigate their potential role in healthy hPGC identify and development. Two genes, KLF4 and TFCP2L1, are upregulated in hPGCs and are known to have a role in naive pluripotency. Given this, and other shared characteristics between the hPGCs and naive pluripotency, we hypothesized that KLF4 and TFCP2L1 have a role in hPGC development. We first used CRISPR/Cas9 gene editing technology at the human embryonic stem cell (hESC) stage of our PGC-like cell (hPGCLC) aggregate model, to demonstrate the requirement of certain genes including EOMES in PGCLC induction. Then, we developed an extended culture system to study hPGCLCs in vitro. In extended culture, hPGCLCs begin the process of reprogramming to represent the later hPGC stage, where we can study characteristics such as cell cycle and survival. We knocked out KLF4 and TFCP2L1 separately in hESC lines, and discovered that neither gene is required for PGCLC induction, but each has an anticipated role in re-acquiring naive pluripotency in the hESC state. Despite these functional null mutations, neither gene is required for progression of hPGCLC development in vitro including in progression through S phase as measured by Edu, or for PGCLC colony survival. Given this, we conclude that the naive pluripotent states observed in the pre-implantation and hPGC stages are uniquely controlled, and that these transcription factors may serve alternate roles in hPGC development. Possible roles include protection against germ cell tumors, or facilitation of later and advanced stage hPGC development. Further work will address these possibilities, using animal and stem cell models of gonadal development to study later stage progression.

Published

2021

40. Development of a CRISPR activation-based approach for the treatment of SCN2A haploinsufficiency in Autism Spectrum Disorder

Author

Tamura, Serena

Subjects

Bioengineering, Genetics, Neurosciences, CRISPR, Electrophysiology, gene therapy, Haploinsufficiency, hESC, rAAV

Abstract

Haploinsufficiency, having only one functional gene copy, is associated with close to 100 autism spectrum disorder (ASD) risk genes. Here, using SCN2A haploinsufficiency, a major ASD risk condition, we show that CRISPR activation (CRISPRa) of the existing functional copy at adolescent stages provides a viable therapeutic approach. First, we demonstrate the potential for a therapeutic to rescue electrophysiological deficits in mice by utilizing heterozygous Scn2a conditional knockin mice. Next, using an AAV-based CRISPRa approach, we rescue these electrophysiological deficits in Scn2a heterozygous mice and human SCN2A heterozygous excitatory neurons. Our results provide a novel therapeutic approach for numerous ASD-associated genes and also suggest that rescue Scn2a function, even in relatively mature developmental stages, could ameliorate neurodevelopmental phenotypes.

Published

2021

41. Rapid and Reproducible Differentiation of Hematopoietic and T Cell Progenitors From Pluripotent Stem Cells

Author

Léa Flippe, Anne Gaignerie, Céline Sérazin, Olivier Baron, Xavier Saulquin, Maria Themeli, Carole Guillonneau, and Laurent David

Subjects

hiPSC, hESC, hematopoietic progenitor, T-cell progenitor, hematopoietic differentiation, Biology (General), QH301-705.5

Abstract

Cell therapy using T cells has revolutionized medical care in recent years but limitations are associated with the difficulty of genome editing of the cells, the production of a sufficient number of cells and standardization of the product. Human pluripotent stem cells (hPSCs) can self-renew and differentiate into T cells to provide a standardized homogenous product of defined origin in indefinite quantity, therefore they are of great potential to alleviate limitations of therapeutic T cell production. The differentiation of hPSCs takes place in two steps: first the induction of hematopoietic stem/progenitor cells (HSPCs), then the induction of lymphopoiesis by Notch signaling. However, the differentiation of T cells from hPSCs can be difficult and lack reproducibility. One parameter that needs to be better assessed is the potential of DLL1 vs. DLL4 ligands of the Notch pathway to induce T cells. In addition, culture of hPSCs is labor-intensive and not compatible with GMP production, especially when they are cultured on feeder cells. Thus, the definition of a robust GMP-compatible differentiation protocol from hPSCs cultured in feeder-free conditions would increase the accessibility to off-the-shelf hematopoietic and T cell progenitors derived from hPSCs. In this article, we describe an efficient, rapid and reproducible protocol for the generation of hematopoietic and T cell progenitors in two steps: (1) generation of HSPCs from embryoid bodies (EB) in serum free medium and GMP-compatible feeder-free systems, (2) directed differentiation of hPSC-derived HSPCs into T-cell progenitors in the presence of bone marrow stromal cells expressing Notch-ligands OP9-DLL1 vs. OP9-DLL4.

Published

2020

42. Embryonic anti-aging niche

Author

Conboy, Irina M, Yousef, Hanadie, and Conboy, Michael J

Subjects

Stem Cell Research - Embryonic - Non-Human, Transplantation, Stem Cell Research, Regenerative Medicine, Stem Cell Research - Nonembryonic - Non-Human, Aging, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Animals, Embryo, Mammalian, Humans, Mitogen-Activated Protein Kinases, Regeneration, Satellite Cells, Skeletal Muscle, Signal Transduction, Stem Cell Niche, Stem Cells, stem cell aging, regeneration, niche, senescent, cell cycle, Notch, TGF-beta, MAPK, muscle, hESC, Biochemistry and Cell Biology, Physiology, Oncology and Carcinogenesis, Developmental Biology

Abstract

Although functional organ stem cells persist in the old, tissue damage invariably overwhelms tissue repair, ultimately causing the demise of an organism. The poor performance of stem cells in an aged organ, such as skeletal muscle, is caused by the changes in regulatory pathways such as Notch, MAPK and TGF-β, where old differentiated tissue actually inhibits its own regeneration. This perspective analyzes the current literature on regulation of organ stem cells by their young versus old niches and suggests that determinants of healthy and prolonged life might be under a combinatorial control of cell cycle check point proteins and mitogens, which need to be tightly balanced in order to promote tissue regeneration without tumor formation. While responses of adult stem cells are regulated extrinsically and age-specifically, we put forward experimental evidence suggesting that embryonic cells have an intrinsic youthful barrier to aging and produce soluble pro-regenerative proteins that signal the MAPK pathway for rejuvenating myogenesis. Future identification of this activity will improve our understanding of embryonic versus adult regulation of tissue regeneration suggesting novel strategies for organ rejuvenation. Comprehensively, the current intersection of aging and stem cell science indicates that if the age-imposed decline in the regenerative capacity of stem cells was understood, the debilitating lack of organ maintenance in the old could be ameliorated and perhaps, even reversed.

Published

2011

43. Endothelial Progenitor Cells Produced From Human Pluripotent Stem Cells by a Synergistic Combination of Cytokines, Small Compounds, and Serum-Free Medium

Author

Simon Farkas, Pavel Simara, Daniela Rehakova, Lenka Veverkova, and Irena Koutna

Subjects

hiPSC, hESC, hPSC, mesoderm, endothelial progenitors, differentiation, Biology (General), QH301-705.5

Abstract

Human pluripotent stem cells (hPSCs) are a promising source of autologous endothelial progenitor cells (EPCs) that can be used for the treatment of vascular diseases. However, this kind of treatment requires a large amount of EPCs. Therefore, a highly efficient, robust, and easily reproducible differentiation protocol is necessary. We present a novel serum-free differentiation protocol that exploits the synergy of multiple powerful differentiation effectors. Our protocol follows the proper physiological pathway by differentiating EPCs from hPSCs in three phases that mimic in vivo embryonic vascular development. Specifically, hPSCs are differentiated into (i) primitive streak, which is subsequently turned into (ii) mesoderm, which finally differentiates into (iii) EPCs. This differentiation process yields up to 15 differentiated cells per seeded hPSC in 5 days. Endothelial progenitor cells constitute up to 97% of these derived cells. The experiments were performed on the human embryonic stem cell line H9 and six human induced pluripotent stem cell lines generated in our laboratory. Therefore, robustness was verified using many hPSC lines. Two previously established protocols were also adapted and compared to our synergistic three-phase protocol. Increased efficiency and decreased variability were observed for our differentiation protocol in comparison to the other tested protocols. Furthermore, EPCs derived from hPSCs by our protocol expressed the high-proliferative-potential EPC marker CD157 on their surface in addition to the standard EPC surface markers CD31, CD144, CD34, KDR, and CXCR4. Our protocol enables efficient fully defined production of autologous endothelial progenitors for research and clinical applications.

Published

2020

44. The limited application of stem cells in medicine: a review

Author

Jordan Poulos

Subjects

iPSC, hESC, Stem cell ethics, Stem cell regulation, Stem cell politics, STAP, Medicine (General), R5-920, Biochemistry, QD415-436

Abstract

Abstract The history of stem cell therapies is one of a limited number of clinical applications despite a vast therapeutic potential. Major breakthroughs in stem cell research have not yet enjoyed clinical success—all stem cell therapies bar hematopoietic stem cell transplantations remain experimental. With the increased risk of organ failure and neurodegenerative disease associated with our ability to push the boundaries of life expectancy comes an increased pressure to pioneer novel stem cell-based therapeutic approaches. We conclude that the failure of such therapies to achieve clinical translation stems from the polarising effect of the ethical debate around their use. The intractability of the ethical debate is double edged: legislators not only have placed tighter restrictions on certain stem cell therapies, but do so in favour of less controversial cells which will have worse outcomes for patients. It is by considering this relationship between the politics, ethics and science of stem cells that the reasons for the currently limited clinical significance of stem cell therapies be realised.

Published

2018

45. Deconstructing Stem Cell Tumorigenicity: A Roadmap to Safe Regenerative Medicine

Author

Knoepfler, Paul S

Subjects

Medical Biotechnology, Biomedical and Clinical Sciences, Regenerative Medicine, Stem Cell Research - Embryonic - Human, Stem Cell Research - Induced Pluripotent Stem Cell, Stem Cell Research - Induced Pluripotent Stem Cell - Human, Stem Cell Research, Stem Cell Research - Embryonic - Non-Human, 5.2 Cellular and gene therapies, Development of treatments and therapeutic interventions, Generic health relevance, Animals, Cell Transformation, Neoplastic, Embryonic Stem Cells, Epigenesis, Genetic, Humans, Pluripotent Stem Cells, Teratoma, Stem cells, IPSC, hESC, Tumors, Regenerative medicine, Safety, Biological Sciences, Technology, Medical and Health Sciences, Immunology, Biological sciences, Biomedical and clinical sciences

Abstract

Many of the earliest stem cell studies were conducted on cells isolated from tumors rather than from embryos. Of particular interest was research on embryonic carcinoma cells (EC), a type of stem cell derived from teratocarcinoma. The EC research laid the foundation for the later discovery of and subsequent work on embryonic stem cells (ESC). Both ESC isolated from the mouse (mESC) and then later from humans (hESC) shared not only pluripotency with their EC cousins, but also robust tumorigenicity as each readily form teratoma. Surprisingly, decades after the discovery of mESC, the question of what drives ESC to form tumors remains largely an open one. This gap in the field is particularly serious as stem cell tumorigenicity represents the key obstacle to the safe use of stem cell-based regenerative medicine therapies. Although some adult stem cell therapies appear to be safe, they have only a very narrow range of uses in human disease. Our understanding of the tumorigenicity of human induced pluripotent stem cells (IPSC), perhaps the most promising modality for future patient-specific regenerative medicine therapies, is rudimentary. However, IPSC are predicted to possess tumorigenic potential equal to or greater than that of ESC. Here, the links between pluripotency and tumorigenicity are explored. New methods for more accurately testing the tumorigenic potential of IPSC and of other stem cells applicable to regenerative medicine are proposed. Finally, the most promising emerging approaches for overcoming the challenges of stem cell tumorigenicity are highlighted.

Published

2009

46. Global gene expression profiling and senescence biomarker analysis of hESC exposed to H2O2 induced non-cytotoxic oxidative stress

Author

Maria Barandalla, Hui Shi, Hui Xiao, Silvia Colleoni, Cesare Galli, Pietro Lio, Matthew Trotter, and Giovanna Lazzari

Subjects

hESC, Oxidative stress, Microarray, Centrosome, NEDD1, Medicine (General), R5-920, Biochemistry, QD415-436

Abstract

Abstract Background Human embryonic stem cells (hESCs) potentially offer new routes to study, on the basis of the Developmental Origins of Health and Disease (DOHaD) concept, how the maternal environment during pregnancy influences the offspring’s health and can predispose to chronic disease in later life. Reactive oxygen species (ROS), antioxidant defences and cellular redox status play a key function in gene expression regulation and are involved in diabetes and metabolic syndromes as in ageing. Methods We have, therefore, designed an in vitro cell model of oxidative stress by exposing hESCs to hydrogen peroxide (H2O2) during 72 h, in order to resemble the period of preimplantation embryonic development. Results We have analysed the global gene expression profiles of hESCs (HUES3) exposed to non-cytotoxic H2O2 concentrations, using Illumina microarray HT-12 v4, and we found the differential expression of 569 upregulated and 485 downregulated genes. The most affected gene ontology categories were those related with RNA processing and splicing, oxidation reduction and sterol metabolic processes. We compared our findings with a published RNA-seq profiling dataset of human embryos developed in vitro, thereupon exposed to oxidative stress, and we observed that one of the common downregulated genes between this publication and our data, NEDD1, is involved in centrosome structure and function. Conclusions Therefore, we assessed the presence of supernumerary centrosomes and showed that the percentage of cells with more than two centrosomes increased acutely with H2O2 treatment in hESCs (HUES3 and 7) and in a control somatic cell line (Hs27), inducing a premature entry into senescence.

Published

2017

47. The role of methylation, DNA polymorphisms and microRNAs on HLA-G expression in human embryonic stem cells

Author

A. Verloes, C. Spits, M. Vercammen, M. Geens, J. LeMaoult, K. Sermon, W. Coucke, and H. Van de Velde

Subjects

HLA-G, hESC, Promoter methylation, 3′UTR, MicroRNA, Biology (General), QH301-705.5

Abstract

The human leukocyte antigen (HLA)-G gene seems to play a pivotal role in maternal tolerance to the fetus. Little is known about HLA-G expression and its molecular control during in vivo human embryogenesis. Human embryonic stem cells (hESC) provide an interesting in vitro model to study early human development. Different studies reported discrepant findings on whether HLA-G mRNA and protein are present or absent in hESC. Several lines of evidence indicate that promoter CpG methylation and 3′ untranslated region (3′UTR) polymorphisms may influence HLA-G expression.We investigated how HLA-G expression is linked to the patterns of promoter methylation and explored the role of the 3′UTR polymorphic sites and their binding microRNAs on the post-transcriptional regulation of HLA-G in eight hESC lines.We showed that, while the gross expression levels of HLA-G are controlled by promoter methylation, the genetic constitution of the HLA-G 3′UTR, more specifically the 14bp insertion in combination with the +3187A/A and +3142G/G SNP, plays a major role in HLA-G mRNA regulation in hESC.Our findings provide a solid first step towards future work using hESC as tools for the study of early human developmental processes in normal and pregnancy-related disorders such as preeclampsia.

Published

2017

48. PC1/3 Deficiency Impacts Pro-opiomelanocortin Processing in Human Embryonic Stem Cell-Derived Hypothalamic Neurons

Author

Liheng Wang, Lina Sui, Sunil K. Panigrahi, Kana Meece, Yurong Xin, Jinrang Kim, Jesper Gromada, Claudia A. Doege, Sharon L. Wardlaw, Dieter Egli, and Rudolph L. Leibel

Subjects

PC1/3 deficiency, hESC, hypothalamic neurons, POMC processing, obesity, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

We recently developed a technique for generating hypothalamic neurons from human pluripotent stem cells. Here, as proof of principle, we examine the use of these cells in modeling of a monogenic form of severe obesity: PCSK1 deficiency. The cognate enzyme, PC1/3, processes many prohormones in neuroendocrine and other tissues. We generated PCSK1 (PC1/3)-deficient human embryonic stem cell (hESC) lines using both short hairpin RNA and CRISPR-Cas9, and investigated pro-opiomelanocortin (POMC) processing using hESC-differentiated hypothalamic neurons. The increased levels of unprocessed POMC and the decreased ratios (relative to POMC) of processed POMC-derived peptides in both PCSK1 knockdown and knockout hESC-derived neurons phenocopied POMC processing reported in PC1/3-null mice and PC1/3-deficient patients. PC1/3 deficiency was associated with increased expression of melanocortin receptors and PRCP (prolylcarboxypeptidase, a catabolic enzyme for α-melanocyte stimulating hormone (αMSH)), and reduced adrenocorticotropic hormone secretion. We conclude that the obesity accompanying PCSK1 deficiency may not be primarily due to αMSH deficiency.

Published

2017

49. Effect of Valproic Acid on Promoting the Differentiation of Human Embryonic Stem Cells Into Cholangiocyte-Like Cells.

Author

Deng S, Zhao X, Kou Z, Zhu Y, Zhang X, and Chan HF

Subjects

Mice, Animals, Humans, Valproic Acid pharmacology, Mice, Inbred NOD, Mice, SCID, Epithelial Cells, Human Embryonic Stem Cells

Abstract

Cholangiocytes form a complex 3D network of bile ducts in the liver and contribute to liver function. The damage or destruction of cholangiocytes can lead to biliary diseases, and the shortage of cholangiocytes remains an obstacle for drug development targeting biliary diseases. Valproic acid (VPA) is a potent activator of Notch signaling pathway that is essential for cholangiocyte differentiation. Here, we report a VPA-based approach for cholangiocyte differentiation of human pluripotent stem cells. VPA activated Notch2 expression and upregulated HES-1, HEY-1, and Sox9 gene expression in hESC-derived hepatoblast. After 7 days treatment, VPA promoted successful differentiation of hepatoblast into cholangiocytes expressing cholangiocyte marker genes (AE2, AQP1, CFTR) and proteins (CK19 and CK7). In addition, the differentiated cholangiocytes formed bile duct-like structures after implantation into the spleen of NOD/SCID mice. Our results suggested that VPA can promote hESC differentiation to cholangiocyte-like cells. The induced cholangiocytes may serve as a potential cell source for both in vitro modeling and regenerative therapy of cholangiopathies. The findings can also support further development of small-molecule based differentiation protocols for cholangiocyte production., (© The Author(s) 2023. Published by Oxford University Press.)

Published

2024

50. Subcellular RNA distribution and its change during human embryonic stem cell differentiation.

Author

Zhou F, Tan P, Liu S, Chang L, Yang J, Sun M, Guo Y, Si Y, Wang D, Yu J, and Ma Y

Subjects

Humans, Embryonic Stem Cells metabolism, RNA metabolism, Cell Differentiation genetics, Chromatin genetics, Chromatin metabolism, Human Embryonic Stem Cells metabolism

Abstract

The spatial localization of RNA within cells is closely related to its function and also involved in cell fate determination. However, the atlas of RNA distribution within cells and dynamic changes during the developmental process are largely unknown. In this study, five subcellular components, including cytoplasmic extract, membrane extract, soluble nuclear extract, chromatin-bound nuclear extract, and cytoskeletal extract, were isolated and the rules of subcellular RNA distribution in human embryonic stem cells (hESCs) and its change during hESC differentiation are summarized for the first time. The overall distribution patterns of coding and non-coding RNAs are revealed. Interestingly, some developmental genes are found to be transcribed but confined to the chromatin in undifferentiated hESC. Unexpectedly, alternative splicing and polyadenylation endow spatial heterogeneity among different isoforms of the same gene. Finally, the dynamic pattern of RNA distribution during hESC differentiation is characterized, which provides new clues for a comprehensive understanding hESC pluripotency and differentiation., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024