Your search keyword '"Paul J. Gokhale"' showing total 41 results

1. Nucleosides Rescue Replication-Mediated Genome Instability of Human Pluripotent Stem Cells

Author

Oliver J. Bower, Zoe Hewitt, Peter W. Andrews, Sherif F. El-Khamisy, Paul J. Gokhale, Dylan Stavish, Jason A. Halliwell, Christopher J. Price, Thomas J. R. Frith, Owen Laing, and Ivana Barbaric

Subjects

DNA Replication, Pluripotent Stem Cells, 0301 basic medicine, Genome instability, replication, Somatic cell, DNA damage, Cellular differentiation, Mitosis, Biology, medicine.disease_cause, Origin of replication, Biochemistry, Genomic Instability, Cell Line, pluripotent, stress, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Report, Chromosome instability, medicine, Genetics, errors, Humans, human, Induced pluripotent stem cell, S phase, 030304 developmental biology, 0303 health sciences, Mutation, DNA replication, Nucleosides, DNA, Cell Biology, Culture Media, 3. Good health, Cell biology, 030104 developmental biology, mitotic, chemistry, Cytoprotection, Cancer cell, damage, 030217 neurology & neurosurgery, DNA Damage, Developmental Biology

Abstract

Summary Human pluripotent stem cells (PSCs) are subject to the appearance of recurrent genetic variants on prolonged culture. We have now found that, compared with isogenic differentiated cells, PSCs exhibit evidence of considerably more DNA damage during the S phase of the cell cycle, apparently as a consequence of DNA replication stress marked by slower progression of DNA replication, activation of latent origins of replication, and collapse of replication forks. As in many cancers, which, like PSCs, exhibit a shortened G1 phase and DNA replication stress, the resulting DNA damage may underlie the higher incidence of abnormal and abortive mitoses in PSCs, resulting in chromosomal non-dysjunction or cell death. However, we have found that the extent of DNA replication stress, DNA damage, and consequent aberrant mitoses can be substantially reduced by culturing PSCs in the presence of exogenous nucleosides, resulting in improved survival, clonogenicity, and population growth., Highlights • Human pluripotent stem cells are susceptible to replication stress • Nucleosides modulate replication stress and DNA damage in human PSCs • Nucleosides alleviate mitotic errors and improve the growth kinetics of human PSCs • These findings provide a means to reduce the incidence of recurrent genetic change, Halliwell et al. document the susceptibility of human PSCs to replication stress, which may lead to genetic instability. The results presented show that this phenotype can be moderated by culture in the presence of exogenous nucleosides. The findings provide an approach to reducing the incidence of recurrent genetic changes that may compromise the use of human PSCs in regenerative medicine.

Published

2020

2. Low rates of mutation in clinical grade human pluripotent stem cells under different culture conditions

Author

John Alexander, Ivana Barbaric, Zoe Hewitt, Sian Gregory, Wolf Reik, Peter W. Andrews, Richard Weightman, Harry Moore, Simon Andrews, Oliver Thompson, Serena Nik-Zainal, Andrew Wood, Felix Krueger, Kosuke Yusa, Paul J. Gokhale, Ferdinand von Meyenn, Marta Milo, von Meyenn, Ferdinand [0000-0001-9920-3075], Hewitt, Zoe [0000-0001-7519-7029], Alexander, John [0000-0003-3973-6501], Wood, Andrew [0000-0002-5973-2092], Weightman, Richard [0000-0002-2593-8631], Gregory, Sian [0000-0002-3014-2603], Krueger, Felix [0000-0002-5513-3324], Gokhale, Paul J. [0000-0001-7225-4403], Milo, Marta [0000-0002-6996-6431], Nik-Zainal, Serena [0000-0001-5054-1727], Yusa, Kosuke [0000-0002-3442-021X], Andrews, Peter W. [0000-0001-7215-4410], Apollo - University of Cambridge Repository, Gokhale, Paul J [0000-0001-7225-4403], and Andrews, Peter W [0000-0001-7215-4410]

Subjects

0301 basic medicine, Mutation rate, 49/47, DNA Mutational Analysis, 631/532/2064/2117, Cell Culture Techniques, General Physics and Astronomy, medicine.disease_cause, 38/70, Epigenesis, Genetic, 0302 clinical medicine, Mutation Rate, 38/23, Induced pluripotent stem cell, lcsh:Science, Mutation, Multidisciplinary, article, Chromatin, Cell biology, DNA methylation, DNA, Intergenic, Pluripotent Stem Cells, Embryonic stem cells, Science, 631/114/2403, Biology, General Biochemistry, Genetics and Molecular Biology, Cell Line, 631/208/726/649, 03 medical and health sciences, 13/100, medicine, Humans, Genetic variation, Epigenetics, Chromosomes, Human, X, Whole Genome Sequencing, Sequence Analysis, RNA, 631/208/176/1988, General Chemistry, DNA Methylation, Embryonic stem cell, Culture Media, Oxygen, Oxidative Stress, 030104 developmental biology, Cell culture, Gene ontology, lcsh:Q, 030217 neurology & neurosurgery

Abstract

The occurrence of repetitive genomic changes that provide a selective growth advantage in pluripotent stem cells is of concern for their clinical application. However, the effect of different culture conditions on the underlying mutation rate is unknown. Here we show that the mutation rate in two human embryonic stem cell lines derived and banked for clinical application is low and not substantially affected by culture with Rho Kinase inhibitor, commonly used in their routine maintenance. However, the mutation rate is reduced by >50% in cells cultured under 5% oxygen, when we also found alterations in imprint methylation and reversible DNA hypomethylation. Mutations are evenly distributed across the chromosomes, except for a slight increase on the X-chromosome, and an elevation in intergenic regions suggesting that chromatin structure may affect mutation rate. Overall the results suggest that pluripotent stem cells are not subject to unusually high rates of genetic or epigenetic alterations., Nature Communications, 11 (1), ISSN:2041-1723

Published

2020

3. Genetically variant human pluripotent stem cells selectively eliminate wild-type counterparts through YAP-mediated cell competition

Author

Ben A. Stevenson, Samantha Sargeant, Joanne Lacey, Ivana Barbaric, Tristan A. Rodriguez, Paul J. Gokhale, Christopher J. Price, Dylan Stavish, Medical Research Council (MRC), and Biotechnology and Biological Sciences Research Council (BBSRC)

Subjects

Pluripotent Stem Cells, EXPRESSION, Cytoplasm, Induced Pluripotent Stem Cells, Cell, Biology, Regenerative medicine, Article, ANTIGENS, culture-acquired variants, General Biochemistry, Genetics and Molecular Biology, CULTURE, medicine, Humans, human pluripotent stem cells, cell competition, Induced pluripotent stem cell, Molecular Biology, Cells, Cultured, 11 Medical and Health Sciences, Adaptor Proteins, Signal Transducing, Cell Proliferation, Science & Technology, Wild type, YAP-Signaling Proteins, Cell Differentiation, Cell Biology, 06 Biological Sciences, Phenotype, Cell biology, DIFFERENTIATION, DERIVATION, medicine.anatomical_structure, ANTIBODY, DRIVES, Apoptosis, GROWTH, 20Q11.21, YAP, Life Sciences & Biomedicine, Nuclear localization sequence, Transcription Factors, RAS, Developmental Biology

Abstract

Summary The appearance of genetic changes in human pluripotent stem cells (hPSCs) presents a concern for their use in research and regenerative medicine. Variant hPSCs that harbor recurrent culture-acquired aneuploidies display growth advantages over wild-type diploid cells, but the mechanisms that yield a drift from predominantly wild-type to variant cell populations remain poorly understood. Here, we show that the dominance of variant clones in mosaic cultures is enhanced through competitive interactions that result in the elimination of wild-type cells. This elimination occurs through corralling and mechanical compression by faster-growing variants, causing a redistribution of F-actin and sequestration of yes-associated protein (YAP) in the cytoplasm that induces apoptosis in wild-type cells. YAP overexpression or promotion of YAP nuclear localization in wild-type cells alleviates their “loser” phenotype. Our results demonstrate that hPSC fate is coupled to mechanical cues imposed by neighboring cells and reveal that hijacking this mechanism allows variants to achieve clonal dominance in cultures., Graphical abstract, Highlights • Genetically variant human pluripotent stem cells (hPSCs) eliminate wild-type cells • Mechanical cues mediate competitive interactions of wild-type and variant hPSCs • Mechanotransducer YAP is a key mediator of cell competition in hPSC cultures • Cell competition allows the fast overtake of cultures by variant hPSCs, Price et al. identify competitive interactions that enhance selective advantage of genetically variant human pluripotent stem cells (hPSCs). In the presence of faster-growing variant hPSCs, wild-type cells sequester yes-associated protein (YAP) in the cytoplasm and undergo apoptosis. Neighboring variant cells retain nuclear YAP, remaining proliferative. Modifying culture conditions reduces competitive advantage of variant hPSCs.

Published

2021

4. Genetically Variant Human Pluripotent Stem Cells Selectively Eliminate Wild-Type Counterparts Through YAP-Mediated Cell Competition

Author

Samantha Sargeant, Tristan A. Rodriguez, Joanne Lacey, Paul J. Gokhale, Ivana Barbaric, Christopher J. Price, and Dylan Stavish

Subjects

medicine.anatomical_structure, Cytoplasm, Apoptosis, Mechanism (biology), Cell, medicine, Wild type, Biology, Induced pluripotent stem cell, Regenerative medicine, Phenotype, Dominance (genetics), Cell biology

Abstract

The appearance of genetic changes in human pluripotent stem cells (hPSCs) presents a concern for their use in research and regenerative medicine. Variant hPSCs harbouring recurrent culture-acquired aneuploidies display growth advantages over wild-type diploid cells, but the mechanisms yielding a drift from predominantly wild-type to variant cell populations remain poorly understood. Here we show that the dominance of variant clones in mosaic cultures is enhanced through competitive interactions resulting in elimination of wild-type cells. This elimination occurs through corralling and mechanical compression by faster growing variants, causing a redistribution of F-actin and sequestration of YAP in the cytoplasm that induces apoptosis in wild-type cells. Importantly, YAP overexpression in wild-type cells is sufficient to alleviate their loser phenotype. Our results demonstrate that hPSC fate is coupled to mechanical cues imposed by neighbouring cells and reveal that hijacking this mechanism allows variants to achieve clonal dominance in cultures.

Published

2019

5. Multipotency of Adult Hippocampal NSCs In Vivo Is Restricted by Drosha/NFIB

Author

Chiara Rolando, Marta Milo, Verdon Taylor, Anna Engler, Robert Beattie, Sebastian Jessberger, Andrea Erni, Alice Grison, Paul J. Gokhale, and Thomas Wegleiter

Subjects

Ribonuclease III, 0301 basic medicine, Aging, Neurogenesis, Biology, Hippocampal formation, Hippocampus, Mice, 03 medical and health sciences, Neural Stem Cells, Genetics, Animals, RNA, Messenger, reproductive and urinary physiology, Drosha, Gliogenesis, Mice, Knockout, Base Sequence, Multipotent Stem Cells, Dentate gyrus, Cell Differentiation, Cell Biology, Neural stem cell, Adult Stem Cells, NFI Transcription Factors, Oligodendroglia, 030104 developmental biology, nervous system, NFIB, Gene Knockdown Techniques, Dentate Gyrus, Cancer research, biology.protein, Molecular Medicine, Neuroscience, Gene Deletion, Protein Binding, Dicer

Abstract

Adult neural stem cells (NSCs) are defined by their inherent capacity to self-renew and give rise to neurons, astrocytes, and oligodendrocytes. In vivo, however, hippocampal NSCs do not generate oligodendrocytes for reasons that have remained enigmatic. Here, we report that deletion of Drosha in adult dentate gyrus NSCs activates oligodendrogenesis and reduces neurogenesis at the expense of gliogenesis. We further find that Drosha directly targets NFIB to repress its expression independently of Dicer and microRNAs. Knockdown of NFIB in Drosha-deficient hippocampal NSCs restores neurogenesis, suggesting that the Drosha/NFIB mechanism robustly prevents oligodendrocyte fate acquisition in vivo. Taken together, our findings establish that adult hippocampal NSCs inherently possess multilineage potential but that Drosha functions as a molecular barrier preventing oligodendrogenesis.

Published

2016

6. Detecting Genetic Mosaicism in Cultures of Human Pluripotent Stem Cells

Author

Kerry Bean, Harry Moore, Peter W. Andrews, Miguel A. Juárez, Paul J. Gokhale, Mark Wheeler, Ivana Barbaric, Thomas F. Allison, Steve Williams, Adam J. Hirst, and Duncan Baker

Subjects

0301 basic medicine, Pluripotent Stem Cells, Resource, DNA Copy Number Variations, Karyotype, Cell Culture Techniques, Chromosomes, Human, Pair 20, Trisomy, Biology, Biochemistry, Regenerative medicine, Polymerase Chain Reaction, Cell Line, genetic changes, 03 medical and health sciences, 0302 clinical medicine, Genetics, Chromosomes, Human, Humans, Human pluripotent stem cells, Induced pluripotent stem cell, lcsh:QH301-705.5, Digital droplet pcr, Genetic mosaicism, In Situ Hybridization, Fluorescence, lcsh:R5-920, Mosaicism, Genetic Variation, Cell Biology, Genetic Status, sensitivity, 3. Good health, 030104 developmental biology, lcsh:Biology (General), detection methods, lcsh:Medicine (General), 030217 neurology & neurosurgery, Developmental Biology, Chromosomes, Human, Pair 17

Abstract

Summary Genetic changes in human pluripotent stem cells (hPSCs) gained during culture can confound experimental results and potentially jeopardize the outcome of clinical therapies. Particularly common changes in hPSCs are trisomies of chromosomes 1, 12, 17, and 20. Thus, hPSCs should be regularly screened for such aberrations. Although a number of methods are used to assess hPSC genotypes, there has been no systematic evaluation of the sensitivity of the commonly used techniques in detecting low-level mosaicism in hPSC cultures. We have performed mixing experiments to mimic the naturally occurring mosaicism and have assessed the sensitivity of chromosome banding, qPCR, fluorescence in situ hybridization, and digital droplet PCR in detecting variants. Our analysis highlights the limits of mosaicism detection by the commonly employed methods, a pivotal requirement for interpreting the genetic status of hPSCs and for setting standards for safe applications of hPSCs in regenerative medicine., Highlights • hPSCs conform to random sampling rules used for karyotyping • Excluding mosaicism at 500 metaphases • qPCR is a rapid assay for detection of commonly amplified regions in hPSCs • Cultures scored as normal by commonly used methods could harbor up to 10% variants, Barbaric and colleagues tested how many metaphases need to be scored to detect different levels of mosaicism in hPSC cultures. They also devised qPCR assays as a rapid means of detecting common chromosomal abnormalities. Testing of the sensitivity of qPCR, digital droplet PCR, and FISH revealed that these methods can miss as many as 10% abnormal cells in the population.

Published

2016

7. Statistical Texture-Based Mapping of Cell Differentiation Under Microfluidic Flow

Author

Paul J. Gokhale, Eduardo M. A. M. Mendes, Daniel Coca, Veronica Biga, Olívia M. Alves Coelho, James E. Mason, and Peter W. Andrews

Subjects

0301 basic medicine, Computer science, business.industry, Feature vector, Cellular differentiation, Microfluidics, Texture (geology), 03 medical and health sciences, 030104 developmental biology, Flow (mathematics), Long term monitoring, Principal component analysis, Computer vision, Artificial intelligence, Biological system, business, Energy (signal processing)

Abstract

Timelapse microscopy enables long term monitoring of biological processes, however a major bottleneck in assesing experimental outcome is the need for an automated analysis framework to extract statistics and evaluate results. In this study, we use Gabor energy texture descriptors to generate a high dimensional feature space which is analysed with principal component analysis to provide unsupervised characterisation of texture differences between pairs of images. We apply this technique to differentiation of human embryonic carcinoma cells in the presence of all-trans retinoic acid (RA) and show that differentiation outcome can be predicted directly from texture information. A microfluidic environment is used to deliver pulses of RA stimulation over five days in culture. Results provide insight into the dynamics of cell response to differentiation signals over time.

Published

2017

8. Karyotypically abnormal human ESCs are sensitive to HDAC inhibitors and show altered regulation of genes linked to cancers and neurological diseases

Author

Riitta Lahesmaa, Maheswarareddy Emani, Virpi Kivinen, Mark Jones, Peter W. Andrews, Duncan Baker, Paul J. Gokhale, Riikka Lund, Ivana Barbaric, and Matti Nykter

Subjects

Cyclin-Dependent Kinase Inhibitor p21, Down-Regulation, Histone Deacetylase 2, Histone Deacetylase 1, Biology, Genomic Instability, Cell Line, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Neoplasms, medicine, Humans, Epigenetics, RNA, Small Interfering, Embryonic Stem Cells, LDL-Receptor Related Proteins, Cell Proliferation, 030304 developmental biology, Chromosome Aberrations, Medicine(all), 0303 health sciences, Histone deacetylase 2, Retinoblastoma, Tumor Suppressor Proteins, ta1182, Cell Differentiation, General Medicine, Cell Biology, medicine.disease, Embryonic stem cell, Molecular biology, 3. Good health, Histone Deacetylase Inhibitors, Gene Expression Regulation, 030220 oncology & carcinogenesis, embryonic structures, Cancer research, Osteopontin, Histone deacetylase, Nervous System Diseases, Stem cell, Developmental Biology

Abstract

Genomic abnormalities may accumulate in human embryonic stem cells (hESCs) during in vitro maintenance. Characterization of the mechanisms enabling survival and expansion of abnormal hESCs is important due to consequences of genetic changes for the therapeutic utilization of stem cells. Furthermore, these cells provide an excellent model to study transformation in vitro. We report here that the histone deacetylase proteins, HDAC1 and HDAC2, are increased in karyotypically abnormal hESCs when compared to their normal counterparts. Importantly, similar to many cancer cell lines, we found that HDAC inhibitors repress proliferation of the karyotypically abnormal hESCs, whereas normal cells are more resistant to the treatment. The decreased proliferation correlates with downregulation of HDAC1 and HDAC2 proteins, induction of the proliferation inhibitor, cyclin-dependent kinase inhibitor 1A (CDKN1A), and altered regulation of tumor suppressor protein Retinoblastoma 1 (RB1). Through genome-wide transcriptome analysis we have identified genes with altered expression and responsiveness to HDAC inhibition in abnormal cells. Most of these genes are linked to severe developmental and neurological diseases and cancers. Our results highlight the importance of epigenetic mechanisms in the regulation of genomic stability of hESCs, and provide valuable candidates for targeted and selective growth inhibition of karyotypically abnormal cells.

Published

2013

9. Signalling of DNA damage and cytokines across cell barriers exposed to nanoparticles depends on barrier thickness

Author

R. Singh, M.-S. Suleiman, Duncan M. Baird, Gloria Lopez-Castejon, Saif Salih, C. P. Case, Michael Parry, Andrew D. Dick, Maeve A. Caldwell, John D. Aplin, C. Abbott, Karen Forbes, Laureline Roger, Hua Lin, R. Keehan, M. D. Lewis, N. Williams, Jack Ham, Melissa Westwood, B. Hardiman, I. Papageorgiou, Roger B. Newson, Andrew D. Randall, William Howard Evans, Helen Swalwell, M. Berry, Lizeth Lacharme-Lora, Eileen Ingham, Lucy A. Crompton, Jian Liu, Anna Katharina Simon, Aman Sood, Danny S. Roh, Peter W. Andrews, Paul J. Gokhale, Elke Winterhager, Ruth Grümmer, Mark A. Birch-Machin, Red Garland, Structure et Instabilité des Génomes (STRING), Muséum national d'Histoire naturelle (MNHN)-Université Pierre et Marie Curie - Paris 6 (UPMC)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS), and Muséum national d'Histoire naturelle (MNHN)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut de Chimie du CNRS (INC)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS)

Subjects

medicine.medical_treatment, [SDV]Life Sciences [q-bio], Cell, Lipid Bilayers, Medizin, Metal Nanoparticles, 02 engineering and technology, Connexins, Cornea, Mice, General Materials Science, ComputingMilieux_MISCELLANEOUS, 0303 health sciences, Chemistry, 021001 nanoscience & nanotechnology, Condensed Matter Physics, Atomic and Molecular Physics, and Optics, 3. Good health, Mitochondria, Trophoblasts, medicine.anatomical_structure, Cytokine, Nanomedicine, Cytokines, Signal transduction, 0210 nano-technology, Oligopeptides, Signal Transduction, Free Radicals, DNA damage, Biomedical Engineering, Bioengineering, Nanotechnology, [SDV.CAN]Life Sciences [q-bio]/Cancer, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Indirect DNA damage, 03 medical and health sciences, medicine, Animals, Humans, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Electrical and Electronic Engineering, 030304 developmental biology, Trophoblast, Mice, Inbred C57BL, [SDV.GEN.GH]Life Sciences [q-bio]/Genetics/Human genetics, Biophysics, Chromium Alloys, Ex vivo, DNA Damage

Abstract

The use of nanoparticles in medicine is ever increasing, and it is important to understand their targeted and non-targeted effects. We have previously shown that nanoparticles can cause DNA damage to cells cultured below a cellular barrier without crossing this barrier. Here, we show that this indirect DNA damage depends on the thickness of the cellular barrier, and it is mediated by signalling through gap junction proteins following the generation of mitochondrial free radicals. Indirect damage was seen across both trophoblast and corneal barriers. Signalling, including cytokine release, occurred only across bilayer and multilayer barriers, but not across monolayer barriers. Indirect toxicity was also observed in mice and using ex vivo explants of the human placenta. If the importance of barrier thickness in signalling is a general feature for all types of barriers, our results may offer a principle with which to limit the adverse effects of nanoparticle exposure and offer new therapeutic approaches.

Published

2016

10. High-Content Screening for Chemical Modulators of Embryonal Carcinoma Cell Differentiation and Survival

Author

Peter W. Andrews, Mark Jones, David J. Harley, Ivana Barbaric, and Paul J. Gokhale

Subjects

Embryonal Carcinoma Stem Cells, Cell Survival, Cellular differentiation, Biology, Biochemistry, Analytical Chemistry, Small Molecule Libraries, Embryonal carcinoma, Image Processing, Computer-Assisted, medicine, Humans, Benzopyrans, Protein Kinase Inhibitors, Cell potency, Embryonic Stem Cells, Acetophenones, Gene Expression Regulation, Developmental, Reproducibility of Results, Cell Differentiation, medicine.disease, Embryonic stem cell, High-Throughput Screening Assays, Cell biology, Phenotype, P19 cell, Stem cell fate, High-content screening, Molecular Medicine, Stem cell, Biotechnology

Abstract

Disentangling the complex interactions that govern stem cell fate choices of self-renewal, differentiation, or death presents a formidable challenge. Image-based phenotype-driven screening meets this challenge by providing means for rapid testing of many small molecules simultaneously. Pluripotent embryonal carcinoma (EC) cells offer a convenient substitute for embryonic stem (ES) cells in such screens because they are simpler to maintain and control. The authors developed an image-based screening assay to identify compounds that affect survival or differentiation of the human EC stem cell line NTERA2 by measuring the effect on cell number and the proportion of cells expressing a pluripotency-associated marker SSEA3. A pilot screen of 80 kinase inhibitors identified several compounds that improved cell survival or induced differentiation. The survival compounds Y-27632, HA-1077, and H-8 all strongly inhibit the kinases ROCK and PRK2, highlighting the important role of these kinases in EC cell survival. Two molecules, GF109203x and rottlerin, induced EC differentiation. The effects of rottlerin were also investigated in human ES cells. Rottlerin inhibited the self-renewal ability of ES cells, caused the cell cycle arrest, and repressed the expression of pluripotency-associated genes.

Published

2011

11. Mapping the stem cell state: eight novel human embryonic stem and embryonal carcinoma cell antibodies

Author

D. Harley, Peter W. Andrews, James Walsh, E. Pewsey, Paul J. Gokhale, Andrew Wright, N. Andrews, E. Rajpert-De Meyts, K. Bardsley, Harry Moore, Neil J. Harrison, Katie Avery, A. R. Nielsen, Mark Jones, and John E Nielsen

Subjects

Pathology, medicine.medical_specialty, medicine.drug_class, Urology, Endocrinology, Diabetes and Metabolism, Cellular differentiation, Biology, Monoclonal antibody, medicine.disease, Stem cell marker, Embryonic stem cell, Cell biology, Embryonal carcinoma, Reproductive Medicine, Cell culture, medicine, Stem cell, Adult stem cell

Abstract

Summary The antigenic profile of human embryonic stem (ES) and embryonal carcinoma (EC) cells has served as a key element of their characterization, with a common panel of surface and intracellular markers now widely used. Such markers have been used to identify cells within the ‘undifferentiated state’, yet it appears that this categorization may be an oversimplification, because a number of sub-states appear to exist within this state. To increase the resolution of the undifferentiated state, we have generated eight novel monoclonal antibodies, all capable of recognizing undifferentiated human ES and EC cells, and herein describe their characterization. The reactivity of these antibodies against a range of cell lines is reported, as well as their developmental regulation, basic biochemistry and reactivity in immunohistochemistry of testicular germ cell tumours. Our data reveal a range of reactivity for all antibodies against both ES and EC cells, suggesting that these markers will afford recognition of unique sub-states within the undifferentiated stem cell compartment.

Published

2011

12. Novel regulators of stem cell fates identified by a multivariate phenotype screen of small compounds on human embryonic stem cell colonies

Author

Mark Jones, Paul J. Gokhale, Duncan Baker, Adam Glen, Ivana Barbaric, and Peter W. Andrews

Subjects

Cell Survival, Cellular differentiation, Biology, Flow cytometry, Small Molecule Libraries, High-Throughput Screening Assays, medicine, Humans, Protein Kinase Inhibitors, Antihypertensive Agents, Embryonic Stem Cells, reproductive and urinary physiology, Cell Proliferation, Medicine(all), Genetics, medicine.diagnostic_test, Cell growth, Kinase, Pinacidil, Cell Differentiation, Cell Biology, General Medicine, Flow Cytometry, equipment and supplies, Embryonic stem cell, Phenotype, Cell biology, Antigens, Surface, embryonic structures, Proteoglycans, biological phenomena, cell phenomena, and immunity, Stem cell, Developmental Biology

Abstract

Understanding the complex mechanisms that govern the fate decisions of human embryonic stem cells (hESCs) is fundamental to their use in cell replacement therapies. The progress of dissecting these mechanisms will be facilitated by the availability of robust high-throughput screening assays on hESCs. In this study, we report an image-based high-content assay for detecting compounds that affect hESC survival or pluripotency. Our assay was designed to detect changes in the phenotype of hESC colonies by quantifying multiple parameters, including the number of cells in a colony, colony area and shape, intensity of nuclear staining, and the percentage of cells in the colony that express a marker of pluripotency (TRA-1-60), as well as the number of colonies per well. We used this assay to screen 1040 compounds from two commercial compound libraries, and identified 17 that promoted differentiation, as well as 5 that promoted survival of hESCs. Among the novel small compounds we identified with activity on hESC are several steroids that promote hESC differentiation and the antihypertensive drug, pinacidil, which affects hESC survival. The analysis of overlapping targets of pinacidil and the other survival compounds revealed that activity of PRK2, ROCK, MNK1, RSK1, and MSK1 kinases may contribute to the survival of hESCs.

Published

2010

13. High-content screening of small compounds on human embryonic stem cells

Author

Peter W. Andrews, Ivana Barbaric, and Paul J. Gokhale

Subjects

Cell type, Cell Survival, Cellular differentiation, Cell Differentiation, Computational biology, Biology, Stem cell marker, Models, Biological, Biochemistry, Embryonic stem cell, Regenerative medicine, High-Throughput Screening Assays, Small Molecule Libraries, High-content screening, Drug Discovery, Humans, Stem cell, Induced pluripotent stem cell, Algorithms, Embryonic Stem Cells

Abstract

Human ES (embryonic stem) cells and iPS (induced pluripotent stem) cells have been heralded as a source of differentiated cells that could be used in the treatment of degenerative diseases, such as Parkinson's disease or diabetes. Despite the great potential for their use in regenerative therapy, the challenge remains to understand the basic biology of these remarkable cells, in order to differentiate them into any functional cell type. Given the scale of the task, high-throughput screening of agents and culture conditions offers one way to accelerate these studies. The screening of small-compound libraries is particularly amenable to such high-throughput methods. Coupled with high-content screening technology that enables simultaneous assessment of multiple cellular features in an automated and quantitative way, this approach is proving powerful in identifying both small molecules as tools for manipulating stem cell fates and novel mechanisms of differentiation not previously associated with stem cell biology. Such screens performed on human ES cells also demonstrate the usefulness of human ES/iPS cells as cellular models for pharmacological testing of drug efficacy and toxicity, possibly a more imminent use of these cells than in regenerative medicine.

Published

2010

14. The Role of SMAD4 in Human Embryonic Stem Cell Self-Renewal and Stem Cell Fate

Author

Paul J. Gokhale, Stuart Avery, Gaetano Zafarana, and Peter W. Andrews

Subjects

KOSR, animal structures, Nodal Protein, Cellular differentiation, Down-Regulation, Nodal signaling, Biology, Transforming Growth Factor beta, TGF beta signaling pathway, Humans, Cell Lineage, Cells, Cultured, Embryonic Stem Cells, Smad4 Protein, Cell Differentiation, Cell Biology, Embryonic stem cell, Activins, Cell biology, embryonic structures, Molecular Medicine, RNA Interference, biological phenomena, cell phenomena, and immunity, Stem cell, NODAL, Cell Division, Signal Transduction, Developmental Biology, Adult stem cell

Abstract

Transforming growth factor (TGF)-β superfamily proteins play a key role in the regulation of human embryonic stem cells (hESCs). Those of the TGFβ/activin/nodal branch seem to support self-renewal and pluripotency, whereas those of the bone morphogenic protein (BMP) branch induce differentiation. In contrast to this generalization, we found that hESC remained undifferentiated after knockdown of SMAD4 with inducible short hairpin RNA interference, although the knockdown inhibited TGFβ signaling and rendered the cells nonresponsive to BMP-induced differentiation. Moreover, the rapid differentiation of hESC after pharmacological inhibition of TGFβ/activin/nodal receptor signaling was restricted after SMAD4 knockdown. These results suggest that TGFβ/activin/nodal signaling supports the undifferentiated phenotype of hESC by suppressing BMP activity. During long-term culture, SMAD4 knockdown cell populations became less stable and more permissive to neural induction, a situation that was rescued by re-establishment of SMAD4 expression. These results suggest that SMAD4 is not required for maintenance of the undifferentiated state of hESC, but rather to stabilize that state.

Published

2010

15. Comparison of defined culture systems for feeder cell free propagation of human embryonic stem cells

Author

Barbara B. Knowles, Lyn Healy, Outi Hovatta, Steve Oh, Victoria Fox, Nissim Benvenisty, Glyn Stacey, Paul J. Gokhale, Frida Holm, Peter W. Andrews, Veronika Akopian, Ronald D.G. McKay, Janet Rossant, Jennifer L. Brehm, Norio Nakatsuji, Takamichi Miyazaki, Angela Ford, Martin F. Pera, Tenneille Ludwig, Megan Christie, Stephen J. Beil, and Hirofumi Suemori

Subjects

Cell Survival, Cellular differentiation, Cell, Cell Culture Techniques, Cell Count, Biology, Article, Cell Line, Flow cytometry, Mice, Cell Adhesion, medicine, Animals, Humans, Embryonic Stem Cells, Cell Proliferation, medicine.diagnostic_test, Human embryonic stem cell, Cell growth, Cell Biology, General Medicine, Flow Cytometry, Embryonic stem cell, Cell biology, medicine.anatomical_structure, Cell culture, Defined cell culture media, Comparative study, Stem cell, Developmental biology, Developmental Biology

Abstract

There are many reports of defined culture systems for the propagation of human embryonic stem cells in the absence of feeder cell support, but no previous study has undertaken a multi-laboratory comparison of these diverse methodologies. In this study, five separate laboratories, each with experience in human embryonic stem cell culture, used a panel of ten embryonic stem cell lines (including WA09 as an index cell line common to all laboratories) to assess eight cell culture methods, with propagation in the presence of Knockout Serum Replacer, FGF-2, and mouse embryonic fibroblast feeder cell layers serving as a positive control. The cultures were assessed for up to ten passages for attachment, death, and differentiated morphology by phase contrast microscopy, for growth by serial cell counts, and for maintenance of stem cell surface marker expression by flow cytometry. Of the eight culture systems, only the control and those based on two commercial media, mTeSR1 and STEMPRO, supported maintenance of most cell lines for ten passages. Cultures grown in the remaining media failed before this point due to lack of attachment, cell death, or overt cell differentiation. Possible explanations for relative success of the commercial formulations in this study, and the lack of success with other formulations from academic groups compared to previously published results, include: the complex combination of growth factors present in the commercial preparations; improved development, manufacture, and quality control in the commercial products; differences in epigenetic adaptation to culture in vitro between different ES cell lines grown in different laboratories.

Published

2010

16. Modeling the evolution of culture-adapted human embryonic stem cells

Author

Paul J. Gokhale, Daniel Coca, Steve A. Billings, Duncan Baker, Peter W. Andrews, Victor Olariu, Visakan Kadirkamanathan, and Neil J. Harrison

Subjects

Medicine(all), Genetics, Mutation rate, Models, Genetic, Cellular differentiation, Population size, Mutant, Adaptation, Biological, Cell Differentiation, Small population size, Cell Biology, General Medicine, Biology, Biological Evolution, Embryonic stem cell, Cell Line, Cell biology, Cell culture, Humans, Adaptation, Monte Carlo Method, Embryonic Stem Cells, Cell Proliferation, Developmental Biology

Abstract

The long-term culture of human embryonic stem (ES) cells is inevitably subject to evolution, since any mutant that arises with a growth advantage will be selectively amplified. However, the evolutionary influences of population size, mutation rate, and selection pressure are frequently overlooked. We have constructed a Monte Carlo simulation model to predict how changes in these factors can influence the appearance and spread of mutant ES cells, and verified its applicability by comparison with in vitro data. This simulation provides an estimate for the expected rate of generation of culture-adapted ES cells under different assumptions for the key parameters. In particular, it highlights the effect of population size, suggesting that the maintenance of cells in small populations reduces the likelihood that abnormal cultures will develop.

Published

2010

17. Modified variational Bayes EM estimation of hidden Markov tree model of cell lineages

Author

Daniel Coca, Peter W. Andrews, Paul J. Gokhale, Visakan Kadirkamanathan, Victor Olariu, Stephen A. Billings, and Peter D. Tonge

Subjects

Pluripotent Stem Cells, Statistics and Probability, Arithmetic underflow, business.industry, Lineage (evolution), Bayesian probability, Bayes Theorem, Pattern recognition, Markov model, Biochemistry, Markov Chains, Computer Science Applications, Computational Mathematics, Bayes' theorem, Tree (data structure), Computational Theory and Mathematics, Expectation–maximization algorithm, Humans, Cell Lineage, Artificial intelligence, Hidden Markov model, business, Molecular Biology, Mathematics

Abstract

Motivation: Human pluripotent stem cell lines persist in culture as a heterogeneous population of SSEA3 positive and SSEA3 negative cells. Tracking individual stem cells in real time can elucidate the kinetics of cells switching between the SSEA3 positive and negative substates. However, identifying a cell's substate at all time points within a cell lineage tree is technically difficult. Results: A variational Bayesian Expectation Maximization (EM) with smoothed probabilities (VBEMS) algorithm for hidden Markov trees (HMT) is proposed for incomplete tree structured data. The full posterior of the HMT parameters is determined and the underflow problems associated with previous algorithms are eliminated. Example results for the prediction of the types of cells in synthetic and real stem cell lineage trees are presented. Availability:The Matlab code for the VBEMS algorithm is freely available at http://www.acse.dept.shef.ac.uk/repository/vbems_lineage_tree/VBEMS.ZIP Contact: visakan@sheffield.ac.uk Supplementary information: Supplementary data are available at Bioinformatics online.

Published

2009

18. OCT4 Spliced Variants Are Differentially Expressed in Human Pluripotent and Nonpluripotent Cells

Author

Paul J. Gokhale, Peter W. Andrews, Seyed Amir Mohsen Ziaee, Yaser Atlasi, and Seyed Javad Mowla

Subjects

Pluripotent Stem Cells, Stage-Specific Embryonic Antigens, Cell type, Cellular differentiation, Biology, Embryonal carcinoma, Cell Line, Tumor, medicine, Humans, Protein Isoforms, Antigens, Tumor-Associated, Carbohydrate, Embryonic Stem Cells, Regulation of gene expression, Stem Cells, Alternative splicing, Cell Differentiation, Exons, Cell Biology, medicine.disease, Embryonic stem cell, Molecular biology, Introns, Alternative Splicing, Gene Expression Regulation, Cell culture, Molecular Medicine, K562 Cells, Octamer Transcription Factor-3, HeLa Cells, Developmental Biology, K562 cells

Abstract

OCT4 is a master regulator of self-renewal in embryonic stem cells and can potentially encode two spliced variants, designated OCT4A and OCT4B. We have examined the expression pattern of these OCT4 isoforms in various human pluripotent and nonpluripotent cells. Our data revealed that whereas OCT4A expression is restricted to embryonic stem (ES) and embryonal carcinoma (EC) cells, OCT4B can be detected in various nonpluripotent cell types. Furthermore, we detected a novel OCT4 spliced variant, designated OCT4B1, that is expressed primarily in human ES and EC cells and is downregulated following their differentiation. We also found a significantly higher level of OCT4B1 expression in stage-specific embryonic antigen-3 (SSEA3)(+) compared with SSEA3(−) subpopulations of cultured ES cells. Taken together, our data demonstrated a distinctive expression pattern for OCT4 spliced variants in different cell types and highlight the necessity of defining the type of OCT4 when addressing the expression of this gene in different human cells. Disclosure of potential conflicts of interest is found at the end of this article.

Published

2008

19. Characterization of human embryonic stem cell lines by the International Stem Cell Initiative

Author

Nissim Benvenisty, Minal Patel, Glyn Stacey, Lesley Young, Sanna Vuoristo, Barak Blum, Robert Passier, Steve Oh, Rebecca S. Hamilton, Miodrag Stojkovic, Barbara B. Knowles, Benjamin Reubinoff, Kehkooi Kee, Barbara S. Mallon, Andras Nagy, Michal Amit, Janet Rossant, Paul J. Gokhale, Franck Lebrin, Henrike Siemen, Simon Bevan, Weidong Zhang, Milla Mikkola, Stephen L. Minger, Norio Nakatsuji, Peter W. Andrews, Eric S Sherrer, Paul Bello, Tikva Turetsky, Lorraine S. Berry, Behrouz Aflatoonian, Christine L. Mummery, Masha Mileikovsky, Yoav Mayshar, Angela Ford, Harry Moore, Mark Jones, Joseph Itskovitz-Eldor, Jackie Johnson, Lars Ährlund-Richter, Roland A. Fleck, Oluseun Adewumi, Jamie P. Jackson, Alex Hampl, Andre Bh Choo, Petr Dvorak, Timo Otonkoski, Daisy Manning, Henrik Semb, Marta P. Imreh, Justin Brooking, Marina Gertsenstein, Dorien Ward, Jin P. Szatkiewicz, Timo Tuuri, Thomas C Schulz, Marian S Piekarczyk, Kevin G. Chen, Karin Astrid Maria Gertow, Renee A. Reijo Pera, Thomas A Weaver, Gemma Beighton, Kye-Yoon Park, Majlinda Lako, Ronald D.G. McKay, Katarina Emanuelsson, Cia Olsson, Carmel M. O’Brien, Johan Hyllner, Hema Patel, Outi Hovatta, Allan J. Robins, Hirofumi Suemori, Peter J. Rugg-Gunn, Martin F. Pera, Marie Corbel, Gary A. Churchill, Ivan Damjanov, John S Draper, Benjamin L. King, Lyn Healy, Steineke van den Brink, Roger A. Pedersen, Anna E. Michalska, and Kristina Vintersten

Subjects

Homeobox protein NANOG, Genotype, Cellular differentiation, Biomedical Engineering, Bioengineering, Biology, Stem cell marker, Applied Microbiology and Biotechnology, Tetraspanin 29, 03 medical and health sciences, 0302 clinical medicine, Antigens, CD, Cluster Analysis, Humans, Cell Lineage, CD90, Cells, Cultured, Embryonic Stem Cells, 030304 developmental biology, 0303 health sciences, Membrane Glycoproteins, Gene Expression Profiling, Lineage markers, Cell Membrane, Gene Expression Regulation, Developmental, Cell Differentiation, Alkaline Phosphatase, Molecular biology, Embryonic stem cell, 3. Good health, 030220 oncology & carcinogenesis, embryonic structures, Molecular Medicine, Female, XIST, Glycolipids, Stem cell, Biotechnology

Abstract

The International Stem Cell Initiative characterized 59 human embryonic stem cell lines from 17 laboratories worldwide. Despite diverse genotypes and different techniques used for derivation and maintenance, all lines exhibited similar expression patterns for several markers of human embryonic stem cells. They expressed the glycolipid antigens SSEA3 and SSEA4, the keratan sulfate antigens TRA-1-60, TRA-1-81, GCTM2 and GCT343, and the protein antigens CD9, Thy1 (also known as CD90), tissue- nonspecific alkaline phosphatase and class 1 HLA, as well as the strongly developmentally regulated genes NANOG, POU5F1 (formerly known as OCT4), TDGF1, DNMT3B, GABRB3 and GDF3. Nevertheless, the lines were not identical: differences in expression of several lineage markers were evident, and several imprinted genes showed generally similar allele-specific expression patterns, but some gene-dependent variation was observed. Also, some female lines expressed readily detectable levels of XIST whereas others did not. No significant contamination of the lines with mycoplasma, bacteria or cytopathic viruses was detected.

Published

2007

20. Identification and Single-Cell Functional Characterization of an Endodermally Biased Pluripotent Substate in Human Embryonic Stem Cells

Author

Shan Sabri, Kathrin Plath, James O.S. Hackland, Paul J. Gokhale, Peter W. Andrews, Mark Jones, Andrew J.H. Smith, Ivana Barbaric, Daniel Coca, Veronica Biga, Konstantinos Anastassiadis, Thomas F. Allison, Justin Langerman, Jackie Sloane-Stanley, and Dylan Stavish

Subjects

0301 basic medicine, Cell, Human Embryonic Stem Cells, Regenerative Medicine, lineage priming, Biochemistry, Transcriptome, Genes, Reporter, GATA6 Transcription Factor, Cell Self Renewal, Induced pluripotent stem cell, GATA6, Endoderm, Cell Differentiation, Cell biology, medicine.anatomical_structure, embryonic structures, Development of treatments and therapeutic interventions, Stem cell, Single-Cell Analysis, Biotechnology, endocrine system, 1.1 Normal biological development and functioning, Clinical Sciences, Biology, Article, Immunophenotyping, 03 medical and health sciences, Underpinning research, differentiation bias, Genetics, medicine, Humans, Stem Cell Research - Embryonic - Human, Reporter, Cloning, 5.2 Cellular and gene therapies, Gene Expression Profiling, Cell Biology, Stem Cell Research, Embryonic stem cell, 030104 developmental biology, Genes, human embryonic stem cell heterogeneity, Generic health relevance, Biochemistry and Cell Biology, Biomarkers, Developmental Biology

Abstract

Summary Human embryonic stem cells (hESCs) display substantial heterogeneity in gene expression, implying the existence of discrete substates within the stem cell compartment. To determine whether these substates impact fate decisions of hESCs we used a GFP reporter line to investigate the properties of fractions of putative undifferentiated cells defined by their differential expression of the endoderm transcription factor, GATA6, together with the hESC surface marker, SSEA3. By single-cell cloning, we confirmed that substates characterized by expression of GATA6 and SSEA3 include pluripotent stem cells capable of long-term self-renewal. When clonal stem cell colonies were formed from GATA6-positive and GATA6-negative cells, more of those derived from GATA6-positive cells contained spontaneously differentiated endoderm cells than similar colonies derived from the GATA6-negative cells. We characterized these discrete cellular states using single-cell transcriptomic analysis, identifying a potential role for SOX17 in the establishment of the endoderm-biased stem cell state., Graphical Abstract, Highlights • Subsets of hESCs can co-express pluripotency-associated and lineage-specific genes • hESCs co-expressing GATA6 are capable of long-term self-renewal • Single GATA6-expressing hESCs regenerate GATA6-negative cells • GATA6-expressing hESCs are biased in their propensity for differentiation, Human embryonic stem cells have the capacity to turn into any cell type within the adult. Peter Andrews and colleagues have shown that subtle differences between individual cells can functionally bias the resulting cell type that is produced. Generating and purifying these biased cells may therefore improve the derivation of medically relevant cell types.

Published

2015

21. Evidence for bystander signalling between human trophoblast cells and human embryonic stem cells

Author

Barry Sampson, Simon Grant, Nicholas D. Allen, C. Patrick Case, Anna J. Jones, Sharan Athwal, Thomas F. Allison, Paul J. Gokhale, and Peter W. Andrews

Subjects

Embryonic stem cells, Cell signaling, DNA damage, Cellular differentiation, Human Embryonic Stem Cells, Apoptosis, Cell Communication, Stem cells, Biology, Article, Pluripotent stem cells, Metals, Heavy, medicine, Bystander effect, Humans, Induced pluripotent stem cell, QH426, reproductive and urinary physiology, Multidisciplinary, Tumor Necrosis Factor-alpha, Gap Junctions, Trophoblast, Cell Differentiation, Cell Cycle Checkpoints, Fibroblasts, Embryonic stem cell, Trophoblasts, Cell biology, medicine.anatomical_structure, Connexin 43, Cytokines, Stem cell, DNA Damage, Signal Transduction

Abstract

Maternal exposure during pregnancy to toxins can occasionally lead to miscarriage and malformation. It is currently thought that toxins pass through the placental barrier, albeit bi-layered in the first trimester and damage the fetus directly, albeit at low concentration. Here we examined the responses of human embryonic stem (hES) cells in tissue culture to two metals at low concentration. We compared direct exposures with indirect exposures across a bi-layered model of the placenta cell barrier. Direct exposure caused increased DNA damage without apoptosis or a loss of cell number but with some evidence of altered differentiation. Indirect exposure caused increased DNA damage and apoptosis but without loss of pluripotency. This was not caused by metal ions passing through the barrier. Instead the hES cells responded to signalling molecules (including TNF-α) secreted by the barrier cells. This mechanism was dependent on connexin 43 mediated intercellular ‘bystander signalling’ both within and between the trophoblast barrier and the hES colonies. These results highlight key differences between direct and indirect exposure of hES cells across a trophoblast barrier to metal toxins. It offers a theoretical possibility that an indirectly mediated toxicity of hES cells might have biological relevance to fetal development.

Published

2015

22. Points to consider in the development of seed stocks of pluripotent stem cells for clinical applications: International Stem Cell Banking Initiative (ISCBI)

Author

S. Talib, Oliver Brüstle, L. Leopoldo, Mahendra Rao, Derek J. Hei, Miho Furue, Fanyi Zeng, Hirofumi Suemori, R. Ruttachuk, C. Hunt, N. Benvinisty, Benjamin Reubinoff, S. M. Hwang, Martin F. Pera, P.A. De Sousa, Shelly E. Tannenbaum, Outi Hovatta, Peter W. Andrews, Glyn Stacey, Meri T. Firpo, E. Han, M. C. Kibbey, Y. Nakamura, Marc Peschanski, Geoffrey P. Lomax, Douglas Sipp, L. Healy, Christine L. Mummery, Norio Nakatsuji, B. Miranda, V. Jekerle, Patricia Pranke, M. Choi, Karen Dyer Montgomery, Paul J. Gokhale, K. Bruce, Kristiina Rajala, Timo Otonkoski, Andras Nagy, Jeanne F. Loring, Qi Zhou, Sun Kyung Oh, Jeremy M. Crook, Petr Dvorak, Steve Oh, Ivana Knezevic, Christian Freund, S. K. Koo, Heather M. Rooke, B. Z. Yuan, L. Ricco, Marisa Jaconi, H. Y. Ha, David Baker, Tsuneo Takahashi, Y. Laabi, Y. M. Choi, Pentao Liu, P. Kamthorn, Tenneille Ludwig, Maneesha S. Inamdar, Simone Haupt, B. B. Knowles, K. Takada, Rosario Isasi, and Jaconi Dévaud, Marisa

Subjects

Pluripotent Stem Cells, Embryology, Carcinogenicity Tests, International Cooperation, education, Biomedical Engineering, ethics [Biological Specimen Banks], Biology, ddc:616.07, Risk Assessment, Genomic Instability, Genomic Stability, Cell Line, methods [Tissue Preservation], Humans, Carcinogenicity Test, ddc:610, Induced pluripotent stem cell, Stock (geology), Biological Specimen Banks, business.industry, Embryonic stem cell, Tissue Donors, 3. Good health, Biotechnology, Practice Guidelines as Topic, Engineering ethics, Stem cell line, Tissue Preservation, Stem cell, Safety, business

Abstract

In 2009 the International Stem Cell Banking Initiative (ISCBI) contributors and the Ethics Working Party of the International Stem Cell Forum published a consensus on principles of best practice for the procurement, cell banking, testing and distribution of human embryonic stem cell (hESC) lines for research purposes [1] , which was broadly also applicable to human induced pluripotent stem cell (hiPSC) lines. Here, we revisit this guidance to consider what the requirements would be for delivery of the early seed stocks of stem cell lines intended for clinical applications. The term 'seed stock' is used here to describe those cryopreserved stocks of cells established early in the passage history of a pluripotent stem cell line in the lab that derived the line or a stem cell bank, hereafter called the 'repository'. The seed stocks should provide cells with suitable documentation and provenance that would enable them to be taken forward for development in human therapeutic applications. WHO recommendations for the evaluation of animal cell cultures as substrates for the manufacture of biologicals and for the characterization of cell banks were updated in 2010 and provide a number of definitions and guiding principles that may apply to stem cells. The term 'cell bank' is used to describe a stock of vials or other containers of cells with consistent composition aliquoted from a single pool of cells of the same culture history (for other specific definitions see PAS 84 [2] and WHO [3] ).Three important assumptions have been made in the preparation of this document. First, that seed stocks of hPSCs are used as starting materials to make cell banks for use in clinical trials. The cell banks made within a clinical trial would need to be established according to Good Manufacturing Practice (GMP) in a facility with a relevant product manufacturing license. These banks would need additional risk assessment focused on the new banking process/reagents and the specific intended clinical application. Second, it has been assumed that undifferentiated pluripotent stem cells would not be inoculated into patients. Third, where feeder cells are used to culture hPSC lines, their cellular nature and intimate contact with the therapeutic cells means that they should be subject to similar risk assessment and banking procedures as applied to the hPSC cells.It is important to note that responsibility for establishing and updating national regulations for medicinal products relies on National Regulatory Authorities. Therefore, national requirements for cell therapy may vary considerably. Accordingly, it is not intended that this international consensus provides comprehensive guidance that will ensure compliance with requirements in any given jurisdiction. Rather, it is designed to aid the development of clinical grade materials by providing points to consider in the preparation of seed stocks of stem cell lines for use in cell therapy. It may arise that there are circumstances where it is not reasonably possible to meet specific procedures presented in this document. Where this is the case any alternative procedures should be justified and mitigate against any adverse consequences. Finally, this document could also serve as a useful reference to assist in the evaluation of potential sources of candidate cell lines for the development of cell-based medicines, and provide the links necessary to identify some of the key differences in regulatory requirements between countries.

Published

2015

23. Specific Knockdown of Oct4 and β2‐microglobulin Expression by RNA Interference in Human Embryonic Stem Cells and Embryonic Carcinoma Cells

Author

A James R. Walsh, Ahmad Reza Bahrami, Paul J. Gokhale, Ian N Morton, Peter W. Andrews, Maryam Moghaddam Matin, Harry Moore, and Jonathan S. Draper

Subjects

Pluripotent Stem Cells, KOSR, Embryonal Carcinoma Stem Cells, Cellular differentiation, Down-Regulation, Embryonic Development, Biology, Chorionic Gonadotropin, Cell Line, RNA interference, Ectoderm, Humans, reproductive and urinary physiology, Cell Proliferation, Gene knockdown, Neuropeptides, Gene Expression Regulation, Developmental, Nuclear Proteins, Cell Differentiation, Cell Biology, Embryonic stem cell, Molecular biology, DNA-Binding Proteins, P19 cell, Antigens, Surface, embryonic structures, Neoplastic Stem Cells, Molecular Medicine, RNA Interference, biological phenomena, cell phenomena, and immunity, Stem cell, beta 2-Microglobulin, Octamer Transcription Factor-3, Transcription Factors, Developmental Biology, Adult stem cell

Abstract

We have used RNA interference (RNAi) to downregulate beta2-microglobulin and Oct4 in human embryonal carcinoma (hEC) cells and embryonic stem (hES) cells, demonstrating that RNAi is an effective tool for regulating specific gene activity in these human stem cells. The knockdown of Oct4 but not beta2-microglobulin expression in both EC and ES cells resulted in their differentiation, as indicated by a marked change in morphology, growth rate, and surface antigen phenotype, with respect to SSEA1, SSEA3, and TRA-1-60 expression. Expression of hCG and Gcm1 was also induced following knockdown of Oct4 expression, in both 2102Ep hEC cells and in H7 and H14 hES cells, consistent with the conclusion that, as in the mouse, Oct4 is required to maintain the undifferentiated stem cell state, and that differentiation to trophectoderm occurs in its absence. NTERA2 hEC cells also differentiated, but not to trophectoderm, suggesting their equivalence to a later stage of embryogenesis than other hEC and hES cells.

Published

2004

24. A recipe for pluripotency: the correct sp(l)ices make all the difference. Focus on 'Induced overexpression of OCT4A in human embryonic stem cells increases cloning efficiency'

Author

Paul J. Gokhale

Subjects

Cloning, Octamer Transcription Factor-3, Physiology, Embryo, Cell Biology, Anatomy, Biology, Embryonic stem cell, Cell biology, Clone Cells, Normal cell, Human embryogenesis, Animals, Humans, Protein Isoforms, Induced pluripotent stem cell, Embryonic Stem Cells

Abstract

human pluripotent stem cells (PSCs), either directly isolated from embryos or induced by exogenous factors, have not only opened up the possibility of deriving genetically normal cell types in large numbers, but they also offer a window into normally inaccessible human embryogenesis. The

Published

2014

25. Characterization of human pluripotent stem cells

Author

Peter W. Andrews and Paul J. Gokhale

Subjects

Pluripotent Stem Cells, Ethical issues, General Neuroscience, Biology, Embryonic stem cell, Regenerative medicine, Cell biology, Mice, Human embryogenesis, Animals, Humans, Lack of knowledge, Stem cell, Induced pluripotent stem cell, Embryonic Stem Cells

Abstract

Human pluripotent stem cells (PSCs), whether embryonic stem cells or induced PSCs, offer enormous opportunities for regenerative medicine and other biomedical applications once we have developed the ability to harness their capacity for extensive differentiation. Central to this is our ability to identify and characterize such PSCs, but this is fraught with potential difficulties that arise from a tension between functional definitions of pluripotency and the more convenient use of 'markers', a problem exacerbated by ethical issues, our lack of knowledge of early human embryonic development, and differences from the mouse paradigm.

Published

2013

26. ESTOOLS Data@Hand: human stem cell gene expression resource

Author

Reija Autio, Matti Nykter, Olli Yli-Harja, Elisa Närvä, Laura Järvenpää, Kirsti Laurila, Kirsi J. Granberg, Heidi Pukkila, Janne Seppälä, Lauri Hahne, Lingjia Kong, Paul J. Gokhale, Kaisa-Leena Aho, Riitta Lahesmaa, Peter W. Andrews, Jarno Mäkelä, Riikka Lund, Kalle Leinonen, and Christophe Roos

Subjects

Pluripotent Stem Cells, Resource (biology), Microarray analysis techniques, Stem Cells, ta1182, Gene Expression, Cell Biology, Computational biology, Biology, Bioinformatics, ta3111, Biochemistry, High-Throughput Screening Assays, User-Computer Interface, Databases, Genetic, Gene expression, Humans, Stem cell, Induced pluripotent stem cell, Molecular Biology, Biotechnology

Published

2013

27. Deficient DNA damage response and cell cycle checkpoints lead to accumulation of point mutations in human embryonic stem cells

Author

Peter W. Andrews, Thierry Nouspikel, Mark Meuth, Mark Jones, Nevila Hyka-Nouspikel, Joelle A. Desmarais, and Paul J. Gokhale

Subjects

Cell cycle checkpoint, DNA Repair, DNA repair, DNA damage, Apoptosis, Cell Growth Processes, Biology, chemistry.chemical_compound, Humans, Point Mutation, Cells, Cultured, Embryonic Stem Cells, Point mutation, Mutagenesis, Cell Biology, Cell Cycle Checkpoints, Molecular biology, Embryonic stem cell, Cell biology, chemistry, Molecular Medicine, biological phenomena, cell phenomena, and immunity, DNA, Developmental Biology, Nucleotide excision repair, DNA Damage

Abstract

Human embryonic stem cells (hESCs) tend to lose genomic integrity during long periods of culture in vitro and to acquire a cancer-like phenotype. In this study, we aim at understanding the contribution of point mutations to the adaptation process and at providing a mechanistic explanation for their accumulation. We observed that, due to the absence of p21/Waf1/Cip1, cultured hESCs lack proper cell cycle checkpoints and are vulnerable to the kind of DNA damage usually repaired by the highly versatile nucleotide excision repair (NER) pathway. In response to UV-induced DNA damage, the majority of hESCs succumb to apoptosis; however, a subpopulation continues to proliferate, carrying damaged DNA and accumulating point mutations with a typical UV-induced signature. The UV-resistant cells retain their proliferative capacity and potential for pluripotent differentiation and are markedly less apoptotic to subsequent UV exposure. These findings demonstrate that, due to deficient DNA damage response, the modest NER activity in hESCs is insufficient to prevent increased mutagenesis. This provides for the appearance of genetically aberrant hESCs, paving the way for further major genetic changes.

Published

2012

28. The development of pluripotent stem cells

Author

Peter W. Andrews and Paul J. Gokhale

Subjects

Pluripotent Stem Cells, Cellular differentiation, Teratoma, Embryo, Cell Differentiation, Biology, medicine.disease, Embryonic stem cell, Cell biology, Mice, Genetics, medicine, Neoplastic Stem Cells, Animals, Humans, Stem cell, Induced pluripotent stem cell, Reprogramming, Embryonic Stem Cells, Developmental Biology, Adult stem cell

Abstract

Stem cell biology has many roots, and the current interest in the possible medical and pharmaceutical applications of pluripotent stem cells has far removed origins in the biology of a rare but peculiar type of tumor, the teratomas. The identification of their stem cells and their relationship to the early embryo paved the way, first in the mouse and later in humans, to the development of embryonic stem (ES) and induced pluripotent stem (iPS) cells, and to approaches for controlling their differentiations. More recently, the recognition of genetic change and culture adaptation of these cells after prolonged culture has returned us to those cancer roots.

Published

2012

29. Human embryonic stem cells: 10 years on

Author

Peter W. Andrews and Paul J. Gokhale

Subjects

Pluripotent Stem Cells, Somatic cell, Cellular differentiation, Phase contrast microscopy, Cell Differentiation, Cell Biology, Anatomy, Biology, Embryonic stem cell, Pathology and Forensic Medicine, law.invention, Mice, law, Animals, Humans, Microscopy, Phase-Contrast, Stem cell, Induced pluripotent stem cell, Molecular Biology, Neuroscience, Biomarkers, Embryonic Stem Cells

Abstract

Substantial advances in the biology of human embryonic stem (ES) cells, and the technology for working with them, have been made over the past 10 years. Regulatory frameworks for their study are well developed, although some countries remain particularly restrictive. Markers and criteria for characterising human ES cells are also generally agreed, and protocols for promoting their differentiation are being established, providing the groundwork for the development of applications over the next 10 years. The recent appearance of technology to convert somatic cells to 'induced Pluripotent Stem Cells' closely resembling ES cells will certainly speed up these developments.

Published

2009

30. New insights into the control of stem cell pluripotency

Author

Peter W. Andrews and Paul J. Gokhale

Subjects

Homeobox protein NANOG, Pluripotent Stem Cells, Cellular differentiation, Rex1, Biology, Mice, Genetics, Animals, Humans, Gene Regulatory Networks, Induced pluripotent stem cell, Cell potency, reproductive and urinary physiology, Embryonic Stem Cells, Feedback, Physiological, Homeodomain Proteins, SOXB1 Transcription Factors, Nanog Homeobox Protein, Gene Expression Regulation, Developmental, Cell Differentiation, Cell Biology, Embryonic stem cell, Cell biology, embryonic structures, Molecular Medicine, biological phenomena, cell phenomena, and immunity, Stem cell, Octamer Transcription Factor-3

Abstract

Nanog is a transcription factor that is expressed by mouse and human embryonic stem (ES) cells and by primordial germ cells. New research published recently in Nature (Chambers et al., 2007) points to an unexpected role for Nanog in the maintenance of pluripotency in mouse ES cells.

Published

2008

31. How Do Cells Change Their Phenotype

Author

Peter W. Andrews and Paul J. Gokhale

Subjects

Biology, Phenotype, Cell biology

Published

2008

32. List of Contributors

Author

Jon D. Ahlstrom, Taby Ahsan, Julie Allickson, Alejandro J. Almarza, James M. Anderson, Peter Andrews, Hadi Aslan, Anthony Atala, Stephen F. Badylak, Ashok Batra, M. Douglas Baumann, Ravi V. Bellamkonda, Nicole M. Bergman, Z. Beyhan, Mickie Bhatia, Sangeeta N. Bhatia, Peter M. Black, Helen Blau, Scott D. Boden, Eric M. Brey, Ali H. Brivanlou, Chris R. Brown, Scott P. Bruder, S.M. Chambers, Christopher S. Chen, LiHow Chen, Mike Chen, Sulin Chen, N. Cheng, George J. Christ, Seyung Chung, J.B. Cibelli, Massimo Cimini, Paolo De Coppi, Mahesh C. Dodla, Juan Dominguez-Bendala, AM Doyle, Charles N. Durfor, Yann Echelard, Rita B. Effros, Jennifer Elisseeff, Ewa C.S. Ellis, Juliet A. Emamaullee, Carol A. Erickson, Roger De Filippo, Donald Fink, William H. Fissell, Gary E. Friedlaender, Mark E. Furth, Yossi Gafni, Keneth Gage, Andres Garcia, William Gavin, Daniel Gazit, Zulma Gazit, Christopher S. Gemmiti, Jörg C. Gerlach, Paul J. Gokhale, M.A. Goodell, May Griffith, Louis M. Guenin, Stefano Giuliani, Robert E. Guldberg, M.C. Hacker, Benjamin S. Harrison, Bernd Hartmann, Stephen H. Hilbert, Alexander Hillel, Jason Hipp, Col. J.B. Holcomb, Jeffrey O. Hollinger, Chantal E. Holy, Mariah Hout, Jiang Hu, George T.-J. Huang, Johnny Huard, Elliot E. Hui, H. David Humes, Marcos Intaglietta, Junfeng Ji, Yueha Jiang, Christa Johnen, Josephine Johnston, Akira Joraku, David L. Kaplan, David S. Kaplan, Gilson Khang, Rehan N. Khanzada, Soon Hee Kim, Moon Suk Kim, Nadav Kimelman, Irina Klimanskaya, Jonathan A. Kluge, Yash Kolambkar, Chester J. Koh, Makoto Komura, Douglas Kondziolka, Deniz Konya, Wilfried A. Kues, Francois Ng kee Kwong, Deepak Lamba, Hai Bang Lee, Hyukjin Lee, Gary G. Leisk, Kam W. Leong, Ariel J. Levine, Ren Ke Li, Wan-Ju Li, Grace J. Lim, Yan Lin, William J. Lindblad, Wendy F. Liu, Xiaohua Liu, Andrea Lucas-Hahn, Aernout Luttun, Samuel Lynch, Peter X. Ma, Ellen Maher, Manuela Martins-Green, Randall E. McClelland, Richard McFarland, Larry V. McIntire, Harry Meade, David L. Melican, A.G. Mikos, Fernando Ulloa Montoya, Robert M. Nerem, Heiner Niemann, Aparna Nori, Patrea L. Pabst, Kook In Park, Tae Gwan Park, David P. Patterson, Karen Pauwelyn, Gadi Pelled, Laura Perin, M. Petreaca, Antonello Pileggi, Jason H. Pomerantz, Blaise Porter, Milica Radisic, Buddy D. Ratner, A. Hari Reddi, Thomas A. Reh, Lola M. Reid, Camillo Ricordi, Jeff Ross, Alan J. Russell, Filipe N.C. Santos, John P. Schmitz, Gunter Schuch, Sargis Sedrakyan, Michael V. Sefton, Marta Serafini, Paulesh Shah, A.M. James Shapiro, Heather Sheardown, Molly S. Shoichet, M. Minhaj Siddiqui, Richard L. Sidman, Ronald Silverman, Daniel Skuk, Evan Snyder, Shay Soker, Myron Spector, David L. Stocum, Stephen C. Strom, Doris A. Taylor, Yang D. Teng, James Thomson, Robert T. Tranquillo, Jacques P. Tremblay, Amy Tsai, Rocky S. Tuan, Ross S. Tubo, Mark Van Dyke, Deborah Vavoie, Catherine Verfaillie, F. Jerry Volenec, Sara Wargo, Joseph W. Warnwath, Lawrence Wechsler, Shen Wei, Richard D. Weisel, Jennifer L. West, Chrysanthi Williams, J. Koudy Williams, Celia Witten, Steven E. Wolf, Savio L.-Y. Woo, Jordan H. Wosnick, Christine Wrenzycki, Munira Xaymardan, Hsin-Lei Yao, Saami K. Yazdani, Pamela C. Yelick, James J. Yoo, Junying Yu, Katrin Zeilinger, Lepeng Zeng, Andrey G. Zenovich, Bonan Zhong, Carol A. Ziomek, and Laurie Zoloth

Published

2008

33. Cell-cell signaling through NOTCH regulates human embryonic stem cell proliferation

Author

Peter W. Andrews, Maryam Moghaddam Matin, Paul J. Gokhale, Victoria Fox, Mark Jones, and James Walsh

Subjects

Pluripotent Stem Cells, Cell Survival, Cellular differentiation, Notch signaling pathway, Apoptosis, Cell Communication, Biology, Mice, Carcinoma, Embryonal, Animals, Humans, Enzyme Inhibitors, Cells, Cultured, Embryonic Stem Cells, Cell Proliferation, Receptors, Notch, Antibodies, Monoclonal, Cell Differentiation, Cell Biology, Embryonic stem cell, Cell biology, Protein Structure, Tertiary, Protein Transport, P19 cell, Notch proteins, Hes3 signaling axis, Antigens, Surface, Molecular Medicine, Stem cell, Cell-cell signaling, Protein Processing, Post-Translational, Developmental Biology, Signal Transduction

Abstract

Unlike pluripotent mouse embryonic stem (ES) cells, human ES cells and their malignant equivalents, embryonal carcinoma (EC) cells, require close cell-cell contact for efficient growth. Signaling through the NOTCH receptor, initiated by interaction with ligands of the DELTA/JAGGED family expressed on neighboring cells, plays a role in regulating the self-renewal of several stem cell systems. Members of the NOTCH and DELTA/JAGGED families are expressed by human EC and ES cells, and we have therefore investigated the possible role of NOTCH in the maintenance of these cells. Cleavage of both NOTCH1 and NOTCH2 to yield the intracellular domain responsible for the canonical signaling pathway of NOTCH was detected in several human EC and ES cell lines, suggesting that NOTCH signaling is active. Furthermore, the proliferation of human EC cells, as well as the expression of several downstream NOTCH target genes, was markedly reduced after small interfering RNA knockdown of NOTCH1, NOTCH2, and the canonical effector CBF-1 or after blocking NOTCH signaling with the γ-secretase inhibitor L-685,458. The inhibitor also caused a reduction in the growth of human ES cells, although without evidence of differentiation. The results indicate that cell-cell signaling through the NOTCH system provides a critical cue for the proliferation of human EC and ES cell in vitro. Disclosure of potential conflicts of interest is found at the end of this article.

Published

2007

34. Culture Adaptation Alters Transcriptional Hierarchies among Single Human Embryonic Stem Cells Reflecting Altered Patterns of Differentiation

Author

Paul J. Gokhale, SriVidya Dadi, Tariq Enver, Peter W. Andrews, Neil J. Harrison, Mark Jones, David N. Keys, Jon K. Sherlock, Shamit Soneji, and Janice K. Au-Young

Subjects

Homeobox protein NANOG, Stage-Specific Embryonic Antigens, Science, Cellular differentiation, Human Embryonic Stem Cells, Population, Biology, Real-Time Polymerase Chain Reaction, Transcriptome, Cluster Analysis, Humans, Antigens, Tumor-Associated, Carbohydrate, education, Cells, Cultured, Homeodomain Proteins, education.field_of_study, Multidisciplinary, Nanog Homeobox Protein, Cell Differentiation, Molecular biology, Embryonic stem cell, Cell biology, Medicine, Stem cell, Octamer Transcription Factor-3, Research Article

Abstract

We have used single cell transcriptome analysis to re-examine the substates of early passage, karyotypically Normal, and late passage, karyotypically Abnormal (‘Culture Adapted’) human embryonic stem cells characterized by differential expression of the cell surface marker antigen, SSEA3. The results confirmed that culture adaptation is associated with alterations to the dynamics of the SSEA3(+) and SSEA3(-) substates of these cells, with SSEA3(-) Adapted cells remaining within the stem cell compartment whereas the SSEA3(-) Normal cells appear to have differentiated. However, the single cell data reveal that these substates are characterized by further heterogeneity that changes on culture adaptation. Notably the Adapted population includes cells with a transcriptome substate suggestive of a shift to a more naïve-like phenotype in contrast to the cells of the Normal population. Further, a subset of the Normal SSEA3(+) cells expresses genes typical of endoderm differentiation, despite also expressing the undifferentiated stem cell genes, POU5F1 (OCT4) and NANOG, whereas such apparently lineage-primed cells are absent from the Adapted population. These results suggest that the selective growth advantage gained by genetically variant, culture adapted human embryonic stem cells may derive in part from a changed substate structure that influences their propensity for differentiation.

Published

2015

35. A prospective on stem cell research

Author

Peter W. Andrews and Paul J. Gokhale

Subjects

Somatic cell, Endocrinology, Diabetes and Metabolism, Adaptation, Biological, Biology, medicine.disease_cause, Endocrinology, Physiology (medical), Neoplasms, medicine, Animals, Humans, Progenitor cell, Cell potency, Cells, Cultured, Embryonic Stem Cells, Cell Proliferation, Cell growth, Multipotent Stem Cells, Research, Stem Cells, Obstetrics and Gynecology, Embryonic stem cell, Adult Stem Cells, Reproductive Medicine, Immunology, Disease Progression, Stem cell, Adaptation, Carcinogenesis, Neuroscience, Biomarkers

Abstract

Stem cell research has stimulated considerable recent interest, but the concepts are old. Nevertheless, our understanding of the basic biology of different stem cell systems is poor. Many questions remain to be answered: How can we recognize stem cells? Are the underlying control mechanisms common to different types of stem cell, the so-called stemness concept, or is the control of self-renewal and commitment distinct in different stem cell types? What is the significance of differences in stem cells from different species? Do stem cells from somatic tissues really show plasticity with an ability to generate cells from distinct lineages, or are the observed examples consequences of experimental artifact, or rare events of no physiological significance? Do genetic mutations in the genes controlling stem cell self-renewal and differentiation lie at the heart of carcinogenesis? Answers to these and related questions now offer exciting future possibilities for both basic biology and medicine.

Published

2006

36. Dysfunction of the mitotic:meiotic switch as a potential cause of neoplastic conversion of primordial germ cells

Author

Peter W. Andrews, D. J. Eastwood, E. Rajpert De-Meyts, Harry Moore, J. R. Walsh, D. J. B. Adamah, Paul J. Gokhale, and John R. Goepel

Subjects

Male, Urology, Endocrinology, Diabetes and Metabolism, Notch signaling pathway, Mitosis, Cell Cycle Proteins, Biology, Cell Line, Embryonal carcinoma, Meiosis, Proto-Oncogene Proteins, medicine, Humans, Receptor, Notch2, Receptor, Notch4, Genetics, Gonadal ridge, Receptors, Notch, Stem Cells, Nuclear Proteins, Neoplasms, Germ Cell and Embryonal, medicine.disease, Cell biology, Seminoma, DNA-Binding Proteins, Synaptonemal complex, medicine.anatomical_structure, Reproductive Medicine, Germ line development, Germ cell, Signal Transduction

Abstract

Germ cell tumours (GCT) are thought to arise as the result of a defect in early development, probably shortly after arrival of the migrating primordial germ cells (PGC) in the genital ridge when, if in a male genital ridge, the germ cells arrest in mitosis, but in a female genital ridge they enter meiosis. We suggest that dysfunction of the mitotic:meiotic switch, with cells aberrantly co-expressing functions pertinent to both states, might provide the genetic instability that could initiate tumour development. If this hypothesis is correct, GCT could arise because of disruption in the function of any one of a number of different genes involved in controlling mitosis and meiosis, rather than being dependent upon a single prominent susceptibility gene. The Notch signalling system is one candidate system for controlling the switch and we have identified expression of Notch2 and Notch4 in seminomas and carcinoma in situ. Thus those two members of the Notch family are candidates for proto-oncogenes that could play a role in GCT development. We have also identified a human homologue of the synaptonemal complex protein, SCP3, and have found its apparently aberrant expression in some established EC cell lines. One possibility is that abnormal regulation of such proteins involved in the synaptonemal complex could also lead to genetic instability in PGC and so also initiate tumour development.

Published

2006

37. Embryonic stem (ES) cells and embryonal carcinoma (EC) cells: opposite sides of the same coin

Author

Peter W. Andrews, Jonathan S. Draper, Ivan Damjanov, Maryam Moghaddam Matin, Ahmad Reza Bahrami, and Paul J. Gokhale

Subjects

KOSR, Transplantation, Heterologous, Mice, SCID, Biology, Biochemistry, Embryonal carcinoma, Mice, Carcinoma, Embryonal, medicine, Inner cell mass, Animals, Humans, Cells, Cultured, Stem Cells, Cell Differentiation, medicine.disease, Embryo, Mammalian, Embryonic stem cell, Cell biology, P19 cell, Teratocarcinoma, Immunology, RNA Interference, Stem cell, Octamer Transcription Factor-3, Adult stem cell

Abstract

Embryonal carcinoma (EC) cells are the stem cells of teratocarcinomas, and the malignant counterparts of embryonic stem (ES) cells derived from the inner cell mass of blastocyst-stage embryos, whether human or mouse. On prolonged culture in vitro , human ES cells acquire karyotypic changes that are also seen in human EC cells. They also ‘adapt’, proliferating faster and becoming easier to maintain with time in culture. Furthermore, when cells from such an ‘adapted’ culture were inoculated into a SCID (severe combined immunodeficient) mouse, we obtained a teratocarcinoma containing histologically recognizable stem cells, which grew out when the tumour was explanted into culture and exhibited properties of the starting ES cells. In these features, the ‘adapted’ ES cells resembled malignant EC cells. The results suggest that ES cells may develop in culture in ways that mimic changes occurring in EC cells during tumour progression.

Published

2005

38. Cellular differentiation hierarchies in normal and culture-adapted human embryonic stem cells

Author

Thomas Thykjaer, Peter W. Andrews, Shamit Soneji, Jonathan S. Draper, Edna Maltby, Paul J. Gokhale, Chirag Joshi, Torben F. Ørntoft, John M. Brown, Maryam Moghaddam Matin, Raed Abu Dawud, Tariq Enver, Kath Smith, Mark Edmondson Jones, and Francisco J. Iborra

Subjects

Stage-Specific Embryonic Antigens, Cellular differentiation, Biology, medicine.disease_cause, Glycosphingolipids, Cell Line, Epigenesis, Genetic, X Chromosome Inactivation, Gene expression, Genetics, medicine, Chromosomes, Human, Humans, Antigens, Tumor-Associated, Carbohydrate, Epigenetics, Induced pluripotent stem cell, Molecular Biology, Genetics (clinical), DNA Primers, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Stem Cells, Gene Expression Regulation, Developmental, Cell Differentiation, General Medicine, Embryo, Mammalian, Flow Cytometry, Embryonic stem cell, Phenotype, Adaptation, Physiological, Cell biology, Microscopy, Fluorescence, RNA Interference, Stem cell, Carcinogenesis

Abstract

Human embryonic stem cell (HESC) lines vary in their characteristics and behaviour not only because they are derived from genetically outbred populations, but also because they may undergo progressive adaptation upon long-term culture in vitro. Such adaptation may reflect selection of variants with altered propensity for survival and retention of an undifferentiated phenotype. Elucidating the mechanisms involved will be important for understanding normal self-renewal and commitment to differentiation and for validating the safety of HESC-based therapy. We have investigated this process of adaptation at the cellular and molecular levels through a comparison of early passage (normal) and late passage (adapted) sublines of a single HESC line, H7. To account for spontaneous differentiation that occurs in HESC cultures, we sorted cells for SSEA3, which marks undifferentiated HESC. We show that the gene expression programmes of the adapted cells partially reflected their aberrant karyotype, but also resulted from a failure in X-inactivation, emphasizing the importance in adaptation of karyotypically silent epigenetic changes. On the basis of growth potential, ability to re-initiate ES cultures and global transcription profiles, we propose a cellular differentiation hierarchy for maintenance cultures of HESC: normal SSEA3+ cells represent pluripotent stem cells. Normal SSEA3- cells have exited this compartment, but retain multilineage differentiation potential. However, adapted SSEA3+ and SSEA3- cells co-segregate within the stem cell territory, implying that adaptation reflects an alteration in the balance between self-renewal and differentiation. As this balance is also an essential feature of cancer, the mechanisms of culture adaptation may mirror those of oncogenesis and tumour progression.

Published

2005

39. Culture and characterization of human embryonic stem cells

Author

Paul J. Gokhale, Ludmila Ruban, Peter W. Andrews, Harry Moore, and Jonathan S. Draper

Subjects

KOSR, Matrigel, business.industry, Cellular differentiation, Stem Cells, Cell Culture Techniques, Cell Differentiation, Cell Biology, Hematology, Biology, Embryo, Mammalian, Regenerative medicine, Embryonic stem cell, In vitro, Cell biology, Biotechnology, Cell Line, Cell culture, Antigens, Surface, Humans, Stem cell, business, Developmental Biology

Abstract

Human embryonic stem (ES) cells offer substantial opportunities for providing well-defined differentiated cells for drug discovery, toxicology, and regenerative medicine, but the development of efficient techniques for their large-scale culture under defined conditions, and for controlling and directing their differentiation, presents a substantial challenge. Markers for defining the undifferentiated cells are well established, based upon previous studies of embryonal carcinoma (EC) cells, their malignant counterparts from teratocarcinomas. These provide valuable tools for monitoring human ES cultures and their state of differentiation. However, current culture techniques are suboptimal and involve the use of poorly defined culture media and the use of feeder cells. Over time, the cells may also acquire karyotypic changes, reflecting genetic selection and adaptation to in vitro culture conditions. Nevertheless, progress is being made. Originally, human ES cells were derived and maintained in medium containing fetal calf serum. They are now widely cultured in a proprietary serum-free formulation (serum replacement from Invitrogen Corp., Carlsbad, CA), and recently we have derived a new human ES line in this medium without fetal calf serum. Human fibroblasts can also be used to replace mouse embryo fibroblasts as feeder cells. We have now found it possible to culture a subline of human ES cells on Matrigel, or purified collagen type IV, laminin, and fibronectin, without feeders or feeder-conditioned medium. These cells nevertheless retain the features of undifferentiated human ES cells, including a capacity for differentiation. Although these cells also carried karyotypic changes, further research focused upon understanding the mechanisms that control self-renewal, apoptosis, and commitment to differentiation will facilitate the development of defined culture conditions that minimize genetic change and optimize the maintenance of the undifferentiated stem cells.

Published

2004

40. A Notch-related Gene Located on the Long Arm of Human Chromosome 12

Author

Peter W. Andrews, James Walsh, David Adamah, and Paul J. Gokhale

Subjects

endocrine system, Intratubular germ cell neoplasia, Seminoma, Biology, medicine.disease, biology.organism_classification, medicine.anatomical_structure, Notch Family, medicine, Cancer research, Gene family, Gene, Chromosome 12, Germ cell, Caenorhabditis elegans

Abstract

Family and cytogenetic studies of testicular germ cell tumours (TGCT) suggest a strong genetic component in the aetiology of these tumours. We have focused upon genes that may play a key regulatory role in the development of germ cells. Following studies in the nematode worm, Caenorhabditis elegans [1], we have investigated the Notch gene family. Initial results indicate that members of the Notch family are expressed by primordial germ cells, and by seminoma and intratubular germ cell neoplasia, consistent with a possible role in tumour development (unpublished results).

Published

2002

41. Recurrent gain of chromosomes 17q and 12 in cultured human embryonic stem cells

Author

Harry Moore, Kath Smith, Jonathan S. Draper, Peter W. Andrews, James A. Thomson, Thomas P. Zwaka, Paul J. Gokhale, Lorraine F. Meisner, Edna Maltby, and Julie A. Johnson

Subjects

Cellular differentiation, Biomedical Engineering, Aneuploidy, Bioengineering, Karyotype, Biology, medicine.disease, Applied Microbiology and Biotechnology, Embryonic stem cell, Molecular biology, Cell biology, Chromosome 17 (human), Transplantation, medicine, Molecular Medicine, biological phenomena, cell phenomena, and immunity, Stem cell, reproductive and urinary physiology, Chromosome 12, Biotechnology

Abstract

We have observed karyotypic changes involving the gain of chromosome 17q in three independent human embryonic stem (hES) cell lines on five independent occasions. A gain of chromosome 12 was seen occasionally. This implies that increased dosage of chromosome 17q and 12 gene(s) provides a selective advantage for the propagation of undifferentiated hES cells. These observations are instructive for the future application of hES cells in transplantation therapies in which the use of aneuploid cells could be detrimental.

Published

2003