Your search keyword '"Cellular Reprogramming"' showing total 11,090 results

101. HMGA1 stimulates cancer stem-like features and sensitivity to monensin in gastric cancer.

Author

Pádua, Diana, Figueira, Paula, Pombinho, António, Monteiro, Inês, Pereira, Carlos Filipe, Almeida, Raquel, and Mesquita, Patrícia

Subjects

*CANCER stem cells, *STOMACH cancer, *DISEASE relapse, *DRUG resistance, *MONENSIN

Abstract

Gastric cancer represents a serious health problem worldwide, with insufficient molecular biomarkers and therapeutic options. Consequently, several efforts have been directed towards finding specific disease markers in order to develop new therapies capable of defeating gastric cancer. Attention has been pointed to cancer stem cells (CSCs) as they are primarily responsible for tumor initiation and recurrence, making them essential therapeutic targets. Using the SORE6-GFP reporter system, based on the expression of SOX2 and/or OCT4 to drive GFP expression, we isolated gastric cancer stem-like cells (SORE6+ cells) enriched in several molecules, including SOX2, C-MYC, KLF4, HIF-1α, NOTCH1 and HMGA1. Here, we explored the previously undisclosed link of HMGA1 with gastric CSCs. Our results indicated that HMGA1 can activate a transcriptional program that includes SOX2, C-MYC, and KLF4 and endows cells with CSC features. We further showed that chemical induction of gastric CSCs using ciclopirox (CPX) can be mediated by HMGA1. Finally, we showed that HMGA1 GFP+ cells were sensitive to monensin confirming the selective activity of this drug over CSCs. Thus, HMGA1 is a key player in the cellular reprogramming of gastric non-CSCs to cancer stem-like cells. [ABSTRACT FROM AUTHOR]

Published

2024

102. Exogenous OCT4 and SOX2 Contribution to In Vitro Reprogramming in Cattle

Author

Lucas Simões Machado, Camila Martins Borges, Marina Amaro de Lima, Juliano Rodrigues Sangalli, Jacinthe Therrien, Laís Vicari de Figueiredo Pessôa, Paulo Fantinato Neto, Felipe Perecin, Lawrence Charles Smith, Flavio Vieira Meirelles, and Fabiana Fernandes Bressan

Subjects

bovine, epigenetics, pluripotency, cellular reprogramming, OCT4, SOX2, Biology (General), QH301-705.5

Abstract

Mechanisms of cell reprogramming by pluripotency-related transcription factors or nuclear transfer seem to be mediated by similar pathways, and the study of the contribution of OCT4 and SOX2 in both processes may help elucidate the mechanisms responsible for pluripotency. Bovine fibroblasts expressing exogenous OCT4 or SOX2, or both, were analyzed regarding the expression of pluripotency factors and imprinted genes H19 and IGF2R, and used for in vitro reprogramming. The expression of the H19 gene was increased in the control sorted group, and putative iPSC-like cells were obtained when cells were not submitted to cell sorting. When sorted cells expressing OCT4, SOX2, or none (control) were used as donor cells for somatic cell nuclear transfer, fusion rates were 60.0% vs. 64.95% and 70.53% vs. 67.24% for SOX2 vs. control and OCT4 vs. control groups, respectively; cleavage rates were 66.66% vs. 81.68% and 86.47% vs. 85.18%, respectively; blastocyst rates were 33.05% vs. 44.15% and 52.06% vs. 44.78%, respectively. These results show that the production of embryos by NT resulted in similar rates of in vitro developmental competence compared to control cells regardless of different profiles of pluripotency-related gene expression presented by donor cells; however, induced reprogramming was compromised after cell sorting.

Published

2023

103. Pluripotent Stem Cell Derived Neurons as In Vitro Models for Studying Autosomal Recessive Parkinson’s Disease (ARPD): PLA2G6 and Other Gene Loci

Author

Gopurappilly, Renjitha, Crusio, Wim E., Series Editor, Dong, Haidong, Series Editor, Radeke, Heinfried H., Series Editor, Rezaei, Nima, Series Editor, Steinlein, Ortrud, Series Editor, Xiao, Junjie, Series Editor, and Turksen, Kursad, editor

Published

2021

104. Regeneration and Reprogramming

Author

Paro, Renato, Grossniklaus, Ueli, Santoro, Raffaella, Wutz, Anton, Paro, Renato, Grossniklaus, Ueli, Santoro, Raffaella, and Wutz, Anton

Published

2021

105. Induced pluripotent stem cells from domesticated ruminants and their potential for enhancing livestock production

Author

Prasanna Weeratunga, Rebecca M. Harman, and Gerlinde R. Van de Walle

Subjects

ruminants, cellular reprogramming, characterization, induced pluripotency, stem cells, Veterinary medicine, SF600-1100

Abstract

Ruminant livestock, including cattle, sheep, goat, and buffalo, are essential for global food security and serve valuable roles in sustainable agricultural systems. With the limited availability of embryonic stem cells (ESCs) from these species, ruminant induced pluripotent stem cells (iPSCs) and iPSC-like cells provide a valuable research tool for agricultural, veterinary, biomedical, and pharmaceutical applications, as well as for the prospect of translation to human medicine. iPSCs are generated by reprogramming of adult or fetal cells to an ESC-like state by ectopic expression of defined transcription factors. Despite the slow pace the field has evolved in livestock species compared to mice and humans, significant progress has been made over the past 15 years in using different cell sources and reprogramming protocols to generate iPSCs/iPSC-like cells from ruminants. This mini review summarizes the current literature related to the derivation of iPSCs/iPSC-like cells from domesticated ruminants with a focus on reprogramming protocols, characterization, associated limitations, and potential applications in ruminant basic science research and production.

Published

2023

106. Editorial: Pluripotent stem cell engineered 3D structures for disease modeling and tissue repairing

Author

Liang Qiang, Michael A. Lane, Claudia A. Doege, Orly Reiner, and Itzhak Fischer

Subjects

3D structure, organoid, hiPSC, cellular reprogramming, disease modeling, cell therapy, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Published

2023

107. Restoring vision and rebuilding the retina by Müller glial cell reprogramming

Author

Devansh Agarwal, Hope Do, Kevin W. Mazo, Manan Chopra, and Karl J. Wahlin

Subjects

Müller glia, Retinal regeneration, Cellular reprogramming, Biology (General), QH301-705.5

Abstract

Müller glia are non-neuronal support cells that play a vital role in the homeostasis of the eye. Their radial-oriented processes span the width of the retina and respond to injury through a cellular response that can be detrimental or protective depending on the context. In some species, protective responses include the expression of stem cell-like genes which help to fuel new neuron formation and even restoration of vision. In many lower vertebrates including fish and amphibians, this response is well documented, however, in mammals it is severely limited. The remarkable plasticity of cellular reprogramming in lower vertebrates has inspired studies in mammals for repairing the retina and restoring sight, and recent studies suggest that mammals are also capable of regeneration, albeit to a lesser degree. Endogenous regeneration, whereby new retinal neurons are created from existing support cells, offers an exciting alternative approach to existing tissue transplant, gene therapy, and neural prosthetic approaches being explored in parallel. This review will highlight the role of Müller glia during retinal injury and repair. In the end, prospects for advancing retinal regeneration research will be considered.

Published

2023

108. Gene-agnostic therapeutic approaches for inherited retinal degenerations

Author

Molly C. John, Joel Quinn, Monica L. Hu, Jasmina Cehajic-Kapetanovic, and Kanmin Xue

Subjects

retina - medical therapies, inherited retinal degeneration, gene-independent, cellular reprogramming, stem cells, optogenetics, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Inherited retinal diseases (IRDs) are associated with mutations in over 250 genes and represent a major cause of irreversible blindness worldwide. While gene augmentation or gene editing therapies could address the underlying genetic mutations in a small subset of patients, their utility remains limited by the great genetic heterogeneity of IRDs and the costs of developing individualised therapies. Gene-agnostic therapeutic approaches target common pathogenic pathways that drive retinal degeneration or provide functional rescue of vision independent of the genetic cause, thus offering potential clinical benefits to all IRD patients. Here, we review the key gene-agnostic approaches, including retinal cell reprogramming and replacement, neurotrophic support, immune modulation and optogenetics. The relative benefits and limitations of these strategies and the timing of clinical interventions are discussed.

Published

2023

109. Direct Generation of Human Cortical Organoids from Primary Cells

Author

Schukking, Monique, Miranda, Helen C, Trujillo, Cleber A, Negraes, Priscilla D, and Muotri, Alysson R

Subjects

Clinical Research, Stem Cell Research - Nonembryonic - Human, Brain Disorders, Stem Cell Research - Embryonic - Human, Stem Cell Research - Induced Pluripotent Stem Cell, Neurosciences, Stem Cell Research - Induced Pluripotent Stem Cell - Human, Stem Cell Research, Underpinning research, 1.1 Normal biological development and functioning, Neurological, Animals, Brain, Cell Culture Techniques, Cell Differentiation, Cellular Reprogramming, Humans, Induced Pluripotent Stem Cells, Organoids, induced pluripotent stem cell, organoids, high-throughput, neural development, Biological Sciences, Technology, Medical and Health Sciences, Developmental Biology, Immunology

Abstract

The study of variations in human neurodevelopment and cognition is limited by the availability of experimental models. While animal models only partially recapitulate the human brain development, genetics, and heterogeneity, human-induced pluripotent stem cells can provide an attractive experimental alternative. However, cellular reprogramming and further differentiation techniques are costly and time-consuming and therefore, studies using this approach are often limited to a small number of samples. In this study, we describe a rapid and cost-effective method to reprogram somatic cells and the direct generation of cortical organoids in a 96-well format. Our data are a proof-of-principle that a large cohort of samples can be generated for experimental assessment of the human neural development.

Published

2018

110. Mapping Cellular Reprogramming via Pooled Overexpression Screens with Paired Fitness and Single-Cell RNA-Sequencing Readout.

Author

Parekh, Udit, Wu, Yan, Zhao, Dongxin, Worlikar, Atharv, Shah, Neha, Zhang, Kun, and Mali, Prashant

Subjects

Cell Line, Humans, Transcription Factors, Gene Expression Profiling, Sequence Analysis, RNA, Male, Gene Regulatory Networks, Epithelial-Mesenchymal Transition, Single-Cell Analysis, Cellular Reprogramming, ORF overexpression, cellular reprogramming, pluripotent stem cells, single-cell screens, Sequence Analysis, RNA, Human Genome, Stem Cell Research, Regenerative Medicine, Biotechnology, Genetics, Generic Health Relevance, Biochemistry and Cell Biology

Abstract

Understanding the effects of genetic perturbations on the cellular state has been challenging using traditional pooled screens, which typically rely on the delivery of a single perturbation per cell and unidimensional phenotypic readouts. Here, we use barcoded open reading frame overexpression libraries coupled with single-cell RNA sequencing to assay cell state and fitness, a technique we call SEUSS (scalable functional screening by sequencing). Using SEUSS, we perturbed hPSCs with a library of developmentally critical transcription factors (TFs) and assayed the impact of TF overexpression on fitness and transcriptomic states. We further leveraged the versatility of the ORF library approach to assay mutant genes and whole gene families. From the transcriptomic responses, we built genetic co-regulatory networks to identify altered gene modules and found that KLF4 and SNAI2 drive opposing effects along the epithelial-mesenchymal transition axis. From the fitness responses, we identified ETV2 as a driver of reprogramming toward an endothelial-like state.

Published

2018

111. Vitamin D Receptor Is Required for Proliferation, Migration, and Differentiation of Epidermal Stem Cells and Progeny during Cutaneous Wound Repair

Author

Oda, Yuko, Hu, Lizhi, Nguyen, Thai, Fong, Chak, Zhang, Jing, Guo, Pan, and Bikle, Daniel D

Subjects

Regenerative Medicine, Nutrition, Stem Cell Research - Nonembryonic - Non-Human, Stem Cell Research, Underpinning research, 1.1 Normal biological development and functioning, Skin, Animals, Cell Differentiation, Cell Movement, Cell Proliferation, Cell Self Renewal, Cell Transdifferentiation, Cellular Reprogramming, Epidermal Cells, Mice, Mice, Knockout, Receptors, Calcitriol, Regeneration, Sebaceous Glands, Signal Transduction, Stem Cells, Wound Healing, beta Catenin, Clinical Sciences, Oncology and Carcinogenesis, Dermatology & Venereal Diseases

Abstract

Epidermal stem cells residing in the skin play an essential role in epidermal regeneration. When skin is injured, the stem cells are first activated to proliferate, and subsequently the progeny migrate and differentiate to regenerate the epidermis. Here, we demonstrate that the vitamin D receptor (VDR) is essential for these processes to occur. The requirement for VDR on epidermal stem cell function was revealed in conditional VDR knockout mice, in which VDR was deleted from stem cells and progeny, and mice were maintained on a low calcium diet. First, self-renewal and niche formation of epidermal stem cells were impaired. Wound-induced activation of epidermal stem cells was blunted associated with a reduction of β-catenin signaling. Second, wound induced migration of stem cells and progeny was impaired as shown by lineage tracing and delayed migration of VDR silenced cells. Epidermal differentiation of progeny was impaired at the wounding site associated with reduced E-cadherin expression. Deletion of VDR also changed stem cell fate blunting hair development, increasing sebaceous glands, and altering expression and location of epidermal markers. These results suggest that VDR is required for self-renewal, migration, and differentiation of epidermal stem cells and progeny during cutaneous wound healing.

Published

2018

112. Reprogramming normal human epithelial tissues to a common, lethal neuroendocrine cancer lineage

Author

Park, Jung Wook, Lee, John K, Sheu, Katherine M, Wang, Liang, Balanis, Nikolas G, Nguyen, Kim, Smith, Bryan A, Cheng, Chen, Tsai, Brandon L, Cheng, Donghui, Huang, Jiaoti, Kurdistani, Siavash K, Graeber, Thomas G, and Witte, Owen N

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Lung, Aging, Prostate Cancer, Lung Cancer, Cancer, Human Genome, Orphan Drug, Genetics, Urologic Diseases, Rare Diseases, 2.1 Biological and endogenous factors, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Aetiology, Carcinogenesis, Carcinoma, Neuroendocrine, Cell Line, Tumor, Cell Lineage, Cellular Reprogramming, Cellular Reprogramming Techniques, Drug Delivery Systems, Epithelial Cells, Epithelium, Humans, Lung Neoplasms, Male, Prostate, Prostatic Neoplasms, Retinoblastoma Protein, Small Cell Lung Carcinoma, Tumor Suppressor Protein p53, General Science & Technology

Abstract

The use of potent therapies inhibiting critical oncogenic pathways active in epithelial cancers has led to multiple resistance mechanisms, including the development of highly aggressive, small cell neuroendocrine carcinoma (SCNC). SCNC patients have a dismal prognosis due in part to a limited understanding of the molecular mechanisms driving this malignancy and the lack of effective treatments. Here, we demonstrate that a common set of defined oncogenic drivers reproducibly reprograms normal human prostate and lung epithelial cells to small cell prostate cancer (SCPC) and small cell lung cancer (SCLC), respectively. We identify shared active transcription factor binding regions in the reprogrammed prostate and lung SCNCs by integrative analyses of epigenetic and transcriptional landscapes. These results suggest that neuroendocrine cancers arising from distinct epithelial tissues may share common vulnerabilities that could be exploited for the development of drugs targeting SCNCs.

Published

2018

113. Reprogramming human T cell function and specificity with non-viral genome targeting.

Author

Roth, Theodore L, Puig-Saus, Cristina, Yu, Ruby, Shifrut, Eric, Carnevale, Julia, Li, P Jonathan, Hiatt, Joseph, Saco, Justin, Krystofinski, Paige, Li, Han, Tobin, Victoria, Nguyen, David N, Lee, Michael R, Putnam, Amy L, Ferris, Andrea L, Chen, Jeff W, Schickel, Jean-Nicolas, Pellerin, Laurence, Carmody, David, Alkorta-Aranburu, Gorka, Del Gaudio, Daniela, Matsumoto, Hiroyuki, Morell, Montse, Mao, Ying, Cho, Min, Quadros, Rolen M, Gurumurthy, Channabasavaiah B, Smith, Baz, Haugwitz, Michael, Hughes, Stephen H, Weissman, Jonathan S, Schumann, Kathrin, Esensten, Jonathan H, May, Andrew P, Ashworth, Alan, Kupfer, Gary M, Greeley, Siri Atma W, Bacchetta, Rosa, Meffre, Eric, Roncarolo, Maria Grazia, Romberg, Neil, Herold, Kevan C, Ribas, Antoni, Leonetti, Manuel D, and Marson, Alexander

Subjects

T-Lymphocytes, Cells, Cultured, Animals, Humans, Mice, Receptors, Antigen, T-Cell, Protein Engineering, Neoplasm Transplantation, Autoimmunity, Genome, Human, Male, Interleukin-2 Receptor alpha Subunit, CRISPR-Cas Systems, Cellular Reprogramming, Gene Editing, Human Genome, Biotechnology, Genetics, Gene Therapy, 5.2 Cellular and gene therapies, 5.1 Pharmaceuticals, Inflammatory and immune system, Cancer, General Science & Technology

Abstract

Decades of work have aimed to genetically reprogram T cells for therapeutic purposes1,2 using recombinant viral vectors, which do not target transgenes to specific genomic sites3,4. The need for viral vectors has slowed down research and clinical use as their manufacturing and testing is lengthy and expensive. Genome editing brought the promise of specific and efficient insertion of large transgenes into target cells using homology-directed repair5,6. Here we developed a CRISPR-Cas9 genome-targeting system that does not require viral vectors, allowing rapid and efficient insertion of large DNA sequences (greater than one kilobase) at specific sites in the genomes of primary human T cells, while preserving cell viability and function. This permits individual or multiplexed modification of endogenous genes. First, we applied this strategy to correct a pathogenic IL2RA mutation in cells from patients with monogenic autoimmune disease, and demonstrate improved signalling function. Second, we replaced the endogenous T cell receptor (TCR) locus with a new TCR that redirected T cells to a cancer antigen. The resulting TCR-engineered T cells specifically recognized tumour antigens and mounted productive anti-tumour cell responses in vitro and in vivo. Together, these studies provide preclinical evidence that non-viral genome targeting can enable rapid and flexible experimental manipulation and therapeutic engineering of primary human immune cells.

Published

2018

114. Insights into the Mutational Burden of Human Induced Pluripotent Stem Cells from an Integrative Multi-Omics Approach

Author

D’Antonio, Matteo, Benaglio, Paola, Jakubosky, David, Greenwald, William W, Matsui, Hiroko, Donovan, Margaret KR, Li, He, Smith, Erin N, D’Antonio-Chronowska, Agnieszka, and Frazer, Kelly A

Subjects

Stem Cell Research, Genetics, Stem Cell Research - Induced Pluripotent Stem Cell, Biotechnology, Stem Cell Research - Induced Pluripotent Stem Cell - Human, Stem Cell Research - Induced Pluripotent Stem Cell - Non-Human, Human Genome, Regenerative Medicine, Aetiology, 2.1 Biological and endogenous factors, Generic health relevance, Good Health and Well Being, Cell Differentiation, Cells, Cultured, Cellular Reprogramming, Humans, Induced Pluripotent Stem Cells, Mutation, Mutation Rate, RNA-seq, UV damage, epigenome, iPSCs, somatic mutations, stem cells, sublonal mutations, whole genome sequencing, Biochemistry and Cell Biology, Medical Physiology

Abstract

To understand the mutational burden of human induced pluripotent stem cells (iPSCs), we sequenced genomes of 18 fibroblast-derived iPSC lines and identified different classes of somatic mutations based on structure, origin, and frequency. Copy-number alterations affected 295 kb in each sample and strongly impacted gene expression. UV-damage mutations were present in ∼45% of the iPSCs and accounted for most of the observed heterogeneity in mutation rates across lines. Subclonal mutations (not present in all iPSCs within a line) composed 10% of point mutations and, compared with clonal variants, showed an enrichment in active promoters and increased association with altered gene expression. Our study shows that, by combining WGS, transcriptome, and epigenome data, we can understand the mutational burden of each iPSC line on an individual basis and suggests that this information could be used to prioritize iPSC lines for models of specific human diseases and/or transplantation therapy.

Published

2018

115. mTORC1 Promotes Metabolic Reprogramming by the Suppression of GSK3-Dependent Foxk1 Phosphorylation

Author

He, Long, Gomes, Ana P, Wang, Xin, Yoon, Sang Oh, Lee, Gina, Nagiec, Michal J, Cho, Sungyun, Chavez, Andre, Islam, Tasnia, Yu, Yonghao, Asara, John M, Kim, Bo Yeon, and Blenis, John

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Genetics, 2.1 Biological and endogenous factors, Underpinning research, 1.1 Normal biological development and functioning, Aetiology, Generic health relevance, 14-3-3 Proteins, Active Transport, Cell Nucleus, Animals, Binding Sites, Cell Proliferation, Cellular Reprogramming, Down-Regulation, Energy Metabolism, Forkhead Transcription Factors, Glycogen Synthase Kinase 3, HEK293 Cells, Humans, Hypoxia-Inducible Factor 1, alpha Subunit, Mechanistic Target of Rapamycin Complex 1, Mice, Phosphorylation, Protein Binding, Signal Transduction, Foxk1, Foxk2, GSK3, Hif1α, mTOR, metabolism, phosphorylation, transcription, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

The mammalian Target of Rapamycin Complex 1 (mTORC1)-signaling system plays a critical role in the maintenance of cellular homeostasis by sensing and integrating multiple extracellular and intracellular cues. Therefore, uncovering the effectors of mTORC1 signaling is pivotal to understanding its pathophysiological effects. Here we report that the transcription factor forkhead/winged helix family k1 (Foxk1) is a mediator of mTORC1-regulated gene expression. Surprisingly, Foxk1 phosphorylation is increased upon mTORC1 suppression, which elicits a 14-3-3 interaction, a reduction of DNA binding, and nuclear exclusion. Mechanistically, this occurs by mTORC1-dependent suppression of nuclear signaling by the Foxk1 kinase, Gsk3. This pathway then regulates the expression of multiple genes associated with glycolysis and downstream anabolic pathways directly modulated by Foxk1 and/or by Foxk1-regulated expression of Hif-1α. Thus, Foxk1 mediates mTORC1-driven metabolic rewiring, and it is likely to be critical for metabolic diseases where improper mTORC1 signaling plays an important role.

Published

2018

116. Cancer-cell-secreted exosomal miR-105 promotes tumour growth through the MYC-dependent metabolic reprogramming of stromal cells

Author

Yan, Wei, Wu, Xiwei, Zhou, Weiying, Fong, Miranda Y, Cao, Minghui, Liu, Juan, Liu, Xiaojing, Chen, Chih-Hong, Fadare, Oluwole, Pizzo, Donald P, Wu, Jiawen, Liu, Liang, Liu, Xuxiang, Chin, Andrew R, Ren, Xiubao, Chen, Yuan, Locasale, Jason W, and Wang, Shizhen Emily

Subjects

Biochemistry and Cell Biology, Biological Sciences, Breast Cancer, Cancer, Nutrition, Genetics, Biotechnology, 2.1 Biological and endogenous factors, Aetiology, Animals, Breast Neoplasms, Cancer-Associated Fibroblasts, Cell Line, Tumor, Cell Proliferation, Cellular Reprogramming, Energy Metabolism, Exosomes, Female, Gene Expression Regulation, Neoplastic, Humans, Mice, Mice, Inbred NOD, Mice, SCID, MicroRNAs, NIH 3T3 Cells, Paracrine Communication, Proto-Oncogene Proteins c-myc, Signal Transduction, Stromal Cells, Time Factors, Tumor Burden, Tumor Cells, Cultured, Tumor Microenvironment, Medical and Health Sciences, Developmental Biology, Biochemistry and cell biology

Abstract

Cancer and other cells residing in the same niche engage various modes of interactions to synchronize and buffer the negative effects of environmental changes. Extracellular microRNAs (miRNAs) have recently been implicated in the intercellular crosstalk. Here we show a mechanistic model involving breast-cancer-secreted, extracellular-vesicle-encapsulated miR-105, which is induced by the oncoprotein MYC in cancer cells and, in turn, activates MYC signalling in cancer-associated fibroblasts (CAFs) to induce a metabolic program. This results in the capacity of CAFs to display different metabolic features in response to changes in the metabolic environment. When nutrients are sufficient, miR-105-reprogrammed CAFs enhance glucose and glutamine metabolism to fuel adjacent cancer cells. When nutrient levels are low and metabolic by-products accumulate, these CAFs detoxify metabolic wastes, including lactic acid and ammonium, by converting them into energy-rich metabolites. Thus, the miR-105-mediated metabolic reprogramming of stromal cells contributes to sustained tumour growth by conditioning the shared metabolic environment.

Published

2018

117. X Chromosome Dosage Influences DNA Methylation Dynamics during Reprogramming to Mouse iPSCs

Author

Pasque, Vincent, Karnik, Rahul, Chronis, Constantinos, Petrella, Paula, Langerman, Justin, Bonora, Giancarlo, Song, Juan, Vanheer, Lotte, Dimashkie, Anupama Sadhu, Meissner, Alexander, and Plath, Kathrin

Subjects

Biological Sciences, Genetics, Stem Cell Research - Induced Pluripotent Stem Cell, Stem Cell Research - Induced Pluripotent Stem Cell - Non-Human, Human Genome, Stem Cell Research, Stem Cell Research - Embryonic - Non-Human, Regenerative Medicine, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Animals, Binding Sites, Cellular Reprogramming, Chromosomes, Mammalian, CpG Islands, DNA Methylation, Embryonic Stem Cells, Enhancer Elements, Genetic, Female, Genome, Genomic Imprinting, Induced Pluripotent Stem Cells, Male, Mice, Transcription Factors, X Chromosome, DNA methylation, ESC, X chromosome inactivation, embryonic stem cells, epigenetics, iPSC, induced pluripotency, pluripotency, reprogramming, Biochemistry and Cell Biology, Clinical Sciences, Biochemistry and cell biology

Abstract

A dramatic difference in global DNA methylation between male and female cells characterizes mouse embryonic stem cells (ESCs), unlike somatic cells. We analyzed DNA methylation changes during reprogramming of male and female somatic cells and in resulting induced pluripotent stem cells (iPSCs). At an intermediate reprogramming stage, somatic and pluripotency enhancers are targeted for partial methylation and demethylation. Demethylation within pluripotency enhancers often occurs at ESC binding sites of pluripotency transcription factors. Late in reprogramming, global hypomethylation is induced in a female-specific manner. Genome-wide hypomethylation in female cells affects many genomic landmarks, including enhancers and imprint control regions, and accompanies the reactivation of the inactive X chromosome. The loss of one of the two X chromosomes in propagating female iPSCs is associated with genome-wide methylation gain. Collectively, our findings highlight the dynamic regulation of DNA methylation at enhancers during reprogramming and reveal that X chromosome dosage dictates global DNA methylation levels in iPSCs.

Published

2018

118. CXCL12γ Promotes Development of Metastatic Castration Resistant Prostate Cancer by Induction of Cancer Stem Cell and Neuroendocrine Phenotypes

Author

Jung, Younghun, Cackowski, Frank C, Yumoto, Kenji, Decker, Ann M, Wang, Jingcheng, Kim, Jin Koo, Lee, Eunsohl, Wang, Yugang, Chung, Jae-Seung, Gursky, Amy M, Krebsbach, Paul H, Pienta, Kenneth J, Morgan, Todd M, and Taichman, Russell S

Subjects

Stem Cell Research, Prostate Cancer, Stem Cell Research - Nonembryonic - Human, Cancer, Aging, Stem Cell Research - Nonembryonic - Non-Human, Urologic Diseases, Animals, Bone Neoplasms, Cell Line, Tumor, Cell Proliferation, Cellular Reprogramming, Chemokine CXCL12, Female, Heterografts, Humans, Male, Mice, SCID, NF-kappa B, Neoplastic Stem Cells, Neuroendocrine Cells, Phenotype, Prostatic Neoplasms, Castration-Resistant, Protein Kinase C-alpha, Receptors, CXCR4, Signal Transduction, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

There is evidence that cancer stem-like cells (CSC) and neuroendocrine behavior play critical roles in the pathogenesis and clinical course of metastatic castration-resistant prostate cancer (m-CRPC). However, there is limited mechanistic understanding of how CSC and neuroendocrine phenotypes impact the development of m-CRPC. In this study, we explored the role of the intracellular chemokine CXCL12γ in CSC induction and neuroendocrine differentiation and its impact on m-CRPC. CXCL12γ expression was detected in small-cell carcinoma of metastatic tissues and circulating tumor cells from m-CRPC patients and in prostate cancer cells displaying an neuroendocrine phenotype. Mechanistic investigations demonstrated that overexpression of CXCL12γ induced CSC and neuroendocrine phenotypes in prostate cancer cells through CXCR4-mediated PKCα/NFκB signaling, which promoted prostate tumor outgrowth, metastasis, and chemoresistance in vivo Together, our results establish a significant function for CXCL12γ in m-CRPC development and suggest it as a candidate therapeutic target to control aggressive disease.Significance: Expression of CXCL12γ induces the expression of a cancer stem cell and neuroendocrine phenotypes, resulting in the development of aggressive m-CRPC. Cancer Res; 78(8); 2026-39. ©2018 AACR.

Published

2018

119. A Gene Regulatory Network for Cellular Reprogramming in Plant Regeneration

Author

Ikeuchi, Momoko, Shibata, Michitaro, Rymen, Bart, Iwase, Akira, Bågman, Anne-Maarit, Watt, Lewis, Coleman, Duncan, Favero, David S, Takahashi, Tatsuya, Ahnert, Sebastian E, Brady, Siobhan M, and Sugimoto, Keiko

Subjects

Genetics, Biotechnology, Regenerative Medicine, 2.1 Biological and endogenous factors, Aetiology, Arabidopsis Proteins, Cellular Reprogramming, Cytokinins, Gene Regulatory Networks, Genes, Plant, Indoleacetic Acids, Plant Cells, Plants, Promoter Regions, Genetic, Regeneration, Transcription Factors, Auxin, Callus formation, Cellular reprogramming, Cytokinin, Wound stress, Biochemistry and Cell Biology, Plant Biology, Plant Biology & Botany

Abstract

Wounding triggers organ regeneration in many plant species, and application of plant hormones, such as auxin and cytokinin, enhances their regenerative capacities in tissue culture. Recent studies have identified several key players mediating wound- and/or plant hormone-induced cellular reprogramming, but the global architecture of gene regulatory relationships underlying plant cellular reprogramming is still far from clear. In this study, we uncovered a gene regulatory network (GRN) associated with plant cellular reprogramming by using an enhanced yeast one-hybrid (eY1H) screen systematically to identify regulatory relationships between 252 transcription factors (TFs) and 48 promoters. Our network analyses suggest that wound- and/or hormone-invoked signals exhibit extensive cross-talk and regulate many common reprogramming-associated genes via multilayered regulatory cascades. Our data suggest that PLETHORA 3 (PLT3), ENHANCER OF SHOOT REGENERATION 1 (ESR1) and HEAT SHOCK FACTOR B 1 (HSFB1) act as critical nodes that have many overlapping targets and potentially connect upstream stimuli to downstream developmental decisions. Interestingly, a set of wound-inducible APETALA 2/ETHYLENE RESPONSE FACTORs (AP2/ERFs) appear to regulate these key genes, which, in turn, form feed-forward cascades that control downstream targets associated with callus formation and organ regeneration. In addition, we found another regulatory pathway, mediated by LATERAL ORGAN BOUNDARY/ASYMMETRIC LEAVES 2 (LOB/AS2) TFs, which probably plays a distinct but partially overlapping role alongside the AP2/ERFs in the putative gene regulatory cascades. Taken together, our findings provide the first global picture of the GRN governing plant cell reprogramming, which will serve as a valuable resource for future studies.

Published

2018

120. MYC Releases Early Reprogrammed Human Cells from Proliferation Pause via Retinoblastoma Protein Inhibition

Author

Rand, Tim A, Sutou, Kenta, Tanabe, Koji, Jeong, Daeun, Nomura, Masaki, Kitaoka, Fumiyo, Tomoda, Emi, Narita, Megumi, Nakamura, Michiko, Nakamura, Masahiro, Watanabe, Akira, Rulifson, Eric, Yamanaka, Shinya, and Takahashi, Kazutoshi

Subjects

Biochemistry and Cell Biology, Biological Sciences, Rare Diseases, 1.1 Normal biological development and functioning, Underpinning research, Antigens, Surface, Cell Line, Cell Proliferation, Cellular Reprogramming, Cyclin-Dependent Kinase Inhibitor p16, Humans, Induced Pluripotent Stem Cells, Kruppel-Like Factor 4, Phosphorylation, Proteoglycans, Proto-Oncogene Proteins c-myc, RNA Interference, RNA, Small Interfering, Retinoblastoma Protein, Transcription Factors, Tripartite Motif Proteins, Ubiquitin-Protein Ligases, LIN41, MYC, immortalization, induced pluripotent stem cell, pluripotency, post-transcriptional regulation, proliferation, reprogramming, senescence, Medical Physiology, Biological sciences

Abstract

Here, we report that MYC rescues early human cells undergoing reprogramming from a proliferation pause induced by OCT3/4, SOX2, and KLF4 (OSK). We identified ESRG as a marker of early reprogramming cells that is expressed as early as day 3 after OSK induction. On day 4, ESRG positive (+) cells converted to a TRA-1-60 (+) intermediate state. These early ESRG (+) or TRA-1-60 (+) cells showed a proliferation pause due to increased p16INK4A and p21 and decreased endogenous MYC caused by OSK. Exogenous MYC did not enhance the appearance of initial reprogramming cells but instead reactivated their proliferation and improved reprogramming efficiency. MYC increased expression of LIN41, which potently suppressed p21 post-transcriptionally. MYC suppressed p16 INK4A. These changes inactivated retinoblastoma protein (RB) and reactivated proliferation. The RB-regulated proliferation pause does not occur in immortalized fibroblasts, leading to high reprogramming efficiency even without exogenous MYC.

Published

2018

121. Human cytomegalovirus reprogrammes haematopoietic progenitor cells into immunosuppressive monocytes to achieve latency

Author

Zhu, Dihan, Pan, Chaoyun, Sheng, Jingxue, Liang, Hongwei, Bian, Zhen, Liu, Yuan, Trang, Phong, Wu, Jianguo, Liu, Fenyong, Zhang, Chen-Yu, and Zen, Ke

Subjects

Microbiology, Biological Sciences, Infectious Diseases, Stem Cell Research, Stem Cell Research - Nonembryonic - Human, Genetics, Aetiology, 2.2 Factors relating to the physical environment, Infection, Cell Differentiation, Cellular Reprogramming, Cytomegalovirus, Hematopoietic Stem Cells, Host-Pathogen Interactions, Humans, Immune Tolerance, Interleukin-10, Monocytes, Nitric Oxide, Nitric Oxide Synthase Type II, STAT3 Transcription Factor, V-Set Domain-Containing T-Cell Activation Inhibitor 1, Virus Latency, Medical Microbiology

Abstract

The precise cell type hosting latent human cytomegalovirus (HCMV) remains elusive. Here, we report that HCMV reprogrammes human haematopoietic progenitor cells (HPCs) into a unique monocyte subset to achieve latency. Unlike conventional monocytes, this monocyte subset possesses higher levels of B7-H4, IL-10 and inducible nitric oxide synthase (iNOS), a longer lifespan and strong immunosuppressive capacity. Cell sorting of peripheral blood from latently infected human donors confirms that only this monocyte subset, representing less than 0.1% of peripheral mononuclear cells, is HCMV genome-positive but immediate-early-negative. Mechanistic studies demonstrate that HCMV promotes the differentiation of HPCs into this monocyte subset by activating cellular signal transducer and activator of transcription 3 (STAT3). In turn, this monocyte subset generates a high level of nitric oxide (NO) to silence HCMV immediate-early transcription and promote viral latency. By contrast, the US28-knockout HCMV mutant, which is incapable of activating STAT3, fails to reprogramme the HPCs and achieve latency. Our findings reveal that via activating the STAT3-iNOS-NO axis, HCMV differentiates human HPCs into a longevous, immunosuppressive monocyte subset for viral latency.

Published

2018

122. Metabolic reprogramming by PCK1 promotes TCA cataplerosis, oxidative stress and apoptosis in liver cancer cells and suppresses hepatocellular carcinoma

Author

Liu, Meng-Xi, Jin, Lei, Sun, Si-Jia, Liu, Peng, Feng, Xu, Cheng, Zhou-Li, Liu, Wei-Ren, Guan, Kun-Liang, Shi, Ying-Hong, Yuan, Hai-Xin, and Xiong, Yue

Subjects

Cancer, Liver Disease, Digestive Diseases, Rare Diseases, Liver Cancer, Aetiology, 2.1 Biological and endogenous factors, Animals, Apoptosis, Carcinoma, Hepatocellular, Cells, Cultured, Cellular Reprogramming, Citric Acid Cycle, Genes, Tumor Suppressor, Gluconeogenesis, HEK293 Cells, Hep G2 Cells, Humans, Intracellular Signaling Peptides and Proteins, Liver Neoplasms, MCF-7 Cells, Male, Mice, Mice, Inbred ICR, Mice, Nude, Oxidative Stress, Phosphoenolpyruvate Carboxykinase (GTP), Clinical Sciences, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

Phosphoenolpyruvate carboxykinase (PEPCK or PCK) catalyzes the first rate-limiting step in hepatic gluconeogenesis pathway to maintain blood glucose levels. Mammalian cells express two PCK genes, encoding for a cytoplasmic (PCPEK-C or PCK1) and a mitochondrial (PEPCK-M or PCK2) isoforms, respectively. Increased expressions of both PCK genes are found in cancer of several organs, including colon, lung, and skin, and linked to increased anabolic metabolism and cell proliferation. Here, we report that the expressions of both PCK1 and PCK2 genes are downregulated in primary hepatocellular carcinoma (HCC) and low PCK expression was associated with poor prognosis in patients with HCC. Forced expression of either PCK1 or PCK2 in liver cancer cell lines results in severe apoptosis under the condition of glucose deprivation and suppressed liver tumorigenesis in mice. Mechanistically, we show that the pro-apoptotic effect of PCK1 requires its catalytic activity. We demonstrate that forced PCK1 expression in glucose-starved liver cancer cells induced TCA cataplerosis, leading to energy crisis and oxidative stress. Replenishing TCA intermediate α-ketoglutarate or inhibition of reactive oxygen species production blocked the cell death caused by PCK expression. Taken together, our data reveal that PCK1 is detrimental to malignant hepatocytes and suggest activating PCK1 expression as a potential treatment strategy for patients with HCC.

Published

2018

123. Next-generation pacemakers: from small devices to biological pacemakers.

Author

Cingolani, Eugenio, Goldhaber, Joshua I, and Marbán, Eduardo

Subjects

Heart Conduction System, Animals, Humans, Treatment Outcome, Cardiac Pacing, Artificial, Cell Transplantation, Equipment Design, Gene Transfer Techniques, Pacemaker, Artificial, Biological Clocks, Action Potentials, Heart Rate, Miniaturization, Arrhythmias, Cardiac, Genetic Therapy, Cellular Reprogramming, Cellular Reprogramming Techniques, Cardiovascular System & Hematology, Cardiorespiratory Medicine and Haematology

Abstract

Electrogenesis in the heart begins in the sinoatrial node and proceeds down the conduction system to originate the heartbeat. Conduction system disorders lead to slow heart rates that are insufficient to support the circulation, necessitating implantation of electronic pacemakers. The typical electronic pacemaker consists of a subcutaneous generator and battery module attached to one or more endocardial leads. New leadless pacemakers can be implanted directly into the right ventricular apex, providing single-chamber pacing without a subcutaneous generator. Modern pacemakers are generally reliable, and their programmability provides options for different pacing modes tailored to specific clinical needs. Advances in device technology will probably include alternative energy sources and dual-chamber leadless pacing in the not-too-distant future. Although effective, current electronic devices have limitations related to lead or generator malfunction, lack of autonomic responsiveness, undesirable interactions with strong magnetic fields, and device-related infections. Biological pacemakers, generated by somatic gene transfer, cell fusion, or cell transplantation, provide an alternative to electronic devices. Somatic reprogramming strategies, which involve transfer of genes encoding transcription factors to transform working myocardium into a surrogate sinoatrial node, are furthest along in the translational pipeline. Even as electronic pacemakers become smaller and less invasive, biological pacemakers might expand the therapeutic armamentarium for conduction system disorders.

Published

2018

124. The sea lamprey germline genome provides insights into programmed genome rearrangement and vertebrate evolution

Author

Smith, Jeramiah J, Timoshevskaya, Nataliya, Ye, Chengxi, Holt, Carson, Keinath, Melissa C, Parker, Hugo J, Cook, Malcolm E, Hess, Jon E, Narum, Shawn R, Lamanna, Francesco, Kaessmann, Henrik, Timoshevskiy, Vladimir A, Waterbury, Courtney KM, Saraceno, Cody, Wiedemann, Leanne M, Robb, Sofia MC, Baker, Carl, Eichler, Evan E, Hockman, Dorit, Sauka-Spengler, Tatjana, Yandell, Mark, Krumlauf, Robb, Elgar, Greg, and Amemiya, Chris T

Subjects

Biological Sciences, Bioinformatics and Computational Biology, Genetics, Stem Cell Research - Nonembryonic - Non-Human, Human Genome, Prevention, Stem Cell Research, Underpinning research, 1.1 Normal biological development and functioning, Generic health relevance, Animals, Cellular Reprogramming, Chromatin Assembly and Disassembly, Evolution, Molecular, Genome, Germ Cells, Mutagenesis, Petromyzon, Vertebrates, Medical and Health Sciences, Developmental Biology, Agricultural biotechnology, Bioinformatics and computational biology

Abstract

The sea lamprey (Petromyzon marinus) serves as a comparative model for reconstructing vertebrate evolution. To enable more informed analyses, we developed a new assembly of the lamprey germline genome that integrates several complementary data sets. Analysis of this highly contiguous (chromosome-scale) assembly shows that both chromosomal and whole-genome duplications have played significant roles in the evolution of ancestral vertebrate and lamprey genomes, including chromosomes that carry the six lamprey HOX clusters. The assembly also contains several hundred genes that are reproducibly eliminated from somatic cells during early development in lamprey. Comparative analyses show that gnathostome (mouse) homologs of these genes are frequently marked by polycomb repressive complexes (PRCs) in embryonic stem cells, suggesting overlaps in the regulatory logic of somatic DNA elimination and bivalent states that are regulated by early embryonic PRCs. This new assembly will enhance diverse studies that are informed by lampreys' unique biology and evolutionary/comparative perspective.

Published

2018

125. Nudt21 Controls Cell Fate by Connecting Alternative Polyadenylation to Chromatin Signaling

Author

Brumbaugh, Justin, Di Stefano, Bruno, Wang, Xiuye, Borkent, Marti, Forouzmand, Elmira, Clowers, Katie J, Ji, Fei, Schwarz, Benjamin A, Kalocsay, Marian, Elledge, Stephen J, Chen, Yue, Sadreyev, Ruslan I, Gygi, Steven P, Hu, Guang, Shi, Yongsheng, and Hochedlinger, Konrad

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Stem Cell Research, Stem Cell Research - Embryonic - Non-Human, Regenerative Medicine, Stem Cell Research - Nonembryonic - Non-Human, Genetics, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Animals, Cells, Cultured, Cellular Reprogramming, Chromatin, Chromatin Assembly and Disassembly, Cleavage And Polyadenylation Specificity Factor, Embryonic Stem Cells, HEK293 Cells, Humans, Mice, Polyadenylation, Signal Transduction, Alternative polyadenylation, chromatin, embryonic stem cells, epigenetic regulation, induced pluripotent stem cells, induced trophoblast stem cells, microRNA, pluripotency, reprogramming, transdifferentiation, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences

Abstract

Cell fate transitions involve rapid gene expression changes and global chromatin remodeling, yet the underlying regulatory pathways remain incompletely understood. Here, we identified the RNA-processing factor Nudt21 as a novel regulator of cell fate change using transcription-factor-induced reprogramming as a screening assay. Suppression of Nudt21 enhanced the generation of induced pluripotent stem cells, facilitated transdifferentiation into trophoblast stem cells, and impaired differentiation of myeloid precursors and embryonic stem cells, suggesting a broader role for Nudt21 in cell fate change. We show that Nudt21 directs differential polyadenylation of over 1,500 transcripts in cells acquiring pluripotency, although only a fraction changed protein levels. Remarkably, these proteins were strongly enriched for chromatin regulators, and their suppression neutralized the effect of Nudt21 during reprogramming. Collectively, our data uncover Nudt21 as a novel post-transcriptional regulator of cell fate and establish a direct, previously unappreciated link between alternative polyadenylation and chromatin signaling.

Published

2018

126. Validation and Detection of Exon Skipping Boosters in DMD Patient Cell Models and mdx Mouse

Author

Barthelemy, Florian, Wang, Dereck, Nelson, Stanley F, and Miceli, M Carrie

Subjects

Muscular Dystrophy, Rare Diseases, Brain Disorders, Duchenne/ Becker Muscular Dystrophy, Prevention, Pediatric, Intellectual and Developmental Disabilities (IDD), Genetics, Aetiology, 2.1 Biological and endogenous factors, Animals, Cellular Reprogramming, Disease Models, Animal, Dystrophin, Exons, Fibroblasts, Genetic Therapy, Humans, Immunohistochemistry, Mice, Mice, Inbred mdx, Muscle Cells, Muscle Fibers, Skeletal, Muscular Dystrophy, Duchenne, Mutation, MyoD Protein, RNA Splicing, Reverse Transcriptase Polymerase Chain Reaction, Exon skipping, Dantrolene, Muscular dystrophies, Therapies, Other Chemical Sciences, Biochemistry and Cell Biology, Developmental Biology

Abstract

Duchenne muscular dystrophy (DMD) is caused by mutations in the DMD gene. Most deletions, duplications, or indels lead to shift of mRNA reading frame, which prevent the production of dystrophin protein. DMD is the leading fatal genetic disorder in childhood. One therapeutic strategy aims to skip one or more exons to restore reading frame to enable the production of internally truncated proteins with partial functionality. However, to date the efficiency of this strategy is suboptimal. Here we present methods for assessing exon skipping using AON alone or in combination with skip booster in the context of human DMD patient fibroblast derived myotubes and in the mdx mouse model of DMD.

Published

2018

127. Metabolic Reprogramming in Leaf Lettuce Grown Under Different Light Quality and Intensity Conditions Using Narrow-Band LEDs

Author

Kitazaki, Kazuyoshi, Fukushima, Atsushi, Nakabayashi, Ryo, Okazaki, Yozo, Kobayashi, Makoto, Mori, Tetsuya, Nishizawa, Tomoko, Reyes-Chin-Wo, Sebastian, Michelmore, Richard W, Saito, Kazuki, Shoji, Kazuhiro, and Kusano, Miyako

Subjects

Medical Biochemistry and Metabolomics, Plant Biology, Biological Sciences, Biomedical and Clinical Sciences, Affordable and Clean Energy, Cellular Reprogramming, Gene Expression Regulation, Plant, High-Throughput Nucleotide Sequencing, Lettuce, Light, Lighting, Metabolic Networks and Pathways, Metabolome, Photosynthesis, Plant Leaves, Transcriptome

Abstract

Light-emitting diodes (LEDs) are an artificial light source used in closed-type plant factories and provide a promising solution for a year-round supply of green leafy vegetables, such as lettuce (Lactuca sativa L.). Obtaining high-quality seedlings using controlled irradiation from LEDs is critical, as the seedling health affects the growth and yield of leaf lettuce after transplantation. Because key molecular pathways underlying plant responses to a specific light quality and intensity remain poorly characterised, we used a multi-omics-based approach to evaluate the metabolic and transcriptional reprogramming of leaf lettuce seedlings grown under narrow-band LED lighting. Four types of monochromatic LEDs (one blue, two green and one red) and white fluorescent light (control) were used at low and high intensities (100 and 300 μmol·m-2·s-1, respectively). Multi-platform mass spectrometry-based metabolomics and RNA-Seq were used to determine changes in the metabolome and transcriptome of lettuce plants in response to different light qualities and intensities. Metabolic pathway analysis revealed distinct regulatory mechanisms involved in flavonoid and phenylpropanoid biosynthetic pathways under blue and green wavelengths. Taken together, these data suggest that the energy transmitted by green light is effective in creating a balance between biomass production and the production of secondary metabolites involved in plant defence.

Published

2018

128. Reprogramming stem cells in regenerative medicine

Author

Jiayi Mao, Qimanguli Saiding, Shutong Qian, Zhimo Liu, Binfan Zhao, Qiuyu Zhao, Bolun Lu, Xiyuan Mao, Liucheng Zhang, Yuguang Zhang, Xiaoming Sun, and Wenguo Cui

Subjects

cell therapies, cellular reprogramming, human disease model, induced pluripotent stem cells, tissue regeneration, Medical technology, R855-855.5

Abstract

Abstract Induced pluripotent stem cells (iPSCs) that are generated from adult somatic cells are induced to express genes that make them pluripotent through reprogramming techniques. With their unlimited proliferative capacity and multifaceted differentiation potential and circumventing the ethical problems encountered in the application of embryonic stem cells (ESC), iPSCs have a broad application in the fields of cell therapy, drug screening, and disease models and may open up new possibilities for regenerative medicine to treat diseases in the future. In this review, we begin with different reprogramming cell technologies to obtain iPSCs, including biotechnological, chemical, and physical modulation techniques, and present their respective strengths, and limitations, as well as the recent progress of research. Secondly, we review recent research advances in iPSC reprogramming‐based regenerative therapies. iPSCs are now widely used to study various clinical diseases of hair follicle defects, myocardial infarction, neurological disorders, liver diseases, and spinal cord injuries. This review focuses on the translational clinical research around iPSCs as well as their potential for growth in the medical field. Finally, we summarize the overall review and look at the potential future of iPSCs in the field of cell therapy as well as tissue regeneration engineering and possible problems. We believe that the advancing iPSC research will help drive long‐awaited breakthroughs in cellular therapy.

Published

2022

129. Indirect Mechanisms of Transcription Factor‐Mediated Gene Regulation during Cell Fate Changes

Author

Michael R. Larcombe, Sheng Hsu, Jose M. Polo, and Anja S. Knaupp

Subjects

cellular reprogramming, decoy DNA, iPSCs, pluripotency, sponge effect, transcription factor, Genetics, QH426-470

Abstract

Abstract Transcription factors (TFs) are the master regulators of cellular identity, capable of driving cell fate transitions including differentiations, reprogramming, and transdifferentiations. Pioneer TFs recognize partial motifs exposed on nucleosomal DNA, allowing for TF‐mediated activation of repressed chromatin. Moreover, there is evidence suggesting that certain TFs can repress actively expressed genes either directly through interactions with accessible regulatory elements or indirectly through mechanisms that impact the expression, activity, or localization of other regulatory factors. Recent evidence suggests that during reprogramming, the reprogramming TFs initiate opening of chromatin regions rich in somatic TF motifs that are inaccessible in the initial and final cellular states. It is postulated that analogous to a sponge, these transiently accessible regions “soak up” somatic TFs, hence lowering the initial barriers to cell fate changes. This indirect TF‐mediated gene regulation event, which is aptly named the “sponge effect,” may play an essential role in the silencing of the somatic transcriptional network during different cellular conversions.

Published

2022

130. Molecular and cellular paradigms of multidrug resistance in cancer

Author

Foram U. Vaidya, Abu SufiyanChhipa, Vinita Mishra, Vishal Kumar Gupta, Shiv Govind Rawat, Ajay Kumar, and Chandramani Pathak

Subjects

Multi drug resistance and cancer, Tumor microenvironment, Cellular reprogramming, Cancer metabolism, Programmed cell death, Inflammation, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background The acquisition of resistance to chemotherapy is a major hurdle in the successful application of cancer therapy. Several anticancer approaches, including chemotherapies, radiotherapy, surgery and targeted therapies are being employed for the treatment of cancer. However, cancer cells reprogram themselves in multiple ways to evade the effect of these therapies, and over a period of time, the drug becomes inactive due to the development of multi‐drug resistance (MDR). MDR is a complex phenomenon where malignant cells become insensitive to anticancer drugs and attain the ability to survive even after several exposures of anticancer drugs. In this review, we have discussed the molecular and cellular paradigms of multidrug resistance in cancer. Recent Findings An Extensive research in cancer biology revealed that drug resistance in cancer is the result of perpetuated intracellular and extracellular mechanisms such as drug efflux, drug inactivation, drug target alteration, oncogenic mutations, altered DNA damage repair mechanism, inhibition of programmed cell death signaling, metabolic reprogramming, epithelial mesenchymal transition (EMT), inherent cell heterogeneity, epigenetic changes, redox imbalance, or any combination of these mechanisms. An inevitable cross‐link between inflammation and drug resistance has been discussed. This review provided insight molecular mechanism to understand the vulnerabilities of cancer cells to develop drug resistance. Conclusion MDR is an outcome of interplays between multiple intricate pathways responsible for the inactivation of drug and development of resistance. MDR is a major obstacle in regimens of successful application of anti‐cancer therapy. An improved understanding of the molecular mechanism of multi drug resistance and cellular reprogramming can provide a promising opportunity to combat drug resistance in cancer and intensify anti‐cancer therapy for the upcoming future.

Published

2022

131. Chronic cAMP activation induces adipocyte browning through discordant biphasic remodeling of transcriptome and chromatin accessibility

Author

Jisun So, Solaema Taleb, Jamie Wann, Olivia Strobel, Kyungchan Kim, and Hyun Cheol Roh

Subjects

Beige adipocyte, Transcriptome, Epigenome, NFIL3, Cellular reprogramming, Obesity, Internal medicine, RC31-1245

Abstract

Objective: Adipose tissue thermogenesis has been suggested as a new therapeutic target to promote energy metabolism for obesity and metabolic disease. Cold-inducible thermogenic adipocytes, called beige adipocytes, have attracted significant attention for their potent anti-obesity activity in adult humans. In this study, we identified the mechanisms underlying beige adipocyte recruitment, so-called adipocyte browning, by different stimuli. Methods: We generated a new adipocyte cell line with enhanced browning potentials and determined its transcriptomic and epigenomic responses following cAMP (forskolin, FSK) versus PPARγ activation (rosiglitazone). We performed time-course RNA-seq and compared the treatments and in vivo adipocyte browning. We also developed an improved protocol for Assay for Transposase Accessible Chromatin-sequencing (ATAC-seq) and defined changes in chromatin accessibility in a time course. The RNA-seq and ATAC-seq data were integrated to determine the kinetics of their coordinated regulation and to identify a transcription factor that drives these processes. We conducted functional studies using pharmacological and genetic approaches with specific inhibitors and shRNA-mediated knockdown, respectively. Results: FSK, not rosiglitazone, resulted in a biphasic transcriptomic response, resembling the kinetics of in vivo cold-induced browning. FSK promoted tissue remodeling first and subsequently shifted energy metabolism, concluding with a transcriptomic profile similar to that induced by rosiglitazone. The thermogenic effects of FSK were abolished by PPARγ antagonists, indicating PPARγ as a converging point. ATAC-seq uncovered that FSK leads to a significant chromatin remodeling that precedes or persists beyond transcriptomic changes, whereas rosiglitazone induces minimal changes. Motif analysis identified nuclear factor, interleukin 3 regulated (NFIL3) as a transcriptional regulator connecting the biphasic response of FSK-induced browning, as indicated by disrupted thermogenesis with NFIL3 knockdown. Conclusions: Our findings elucidated unique dynamics of the transcriptomic and epigenomic remodeling in adipocyte browning, providing new mechanistic insights into adipose thermogenesis and molecular targets for obesity treatment.

Published

2022

132. TBX20 Improves Contractility and Mitochondrial Function During Direct Human Cardiac Reprogramming.

Author

Tang, Yawen, Aryal, Sajesan, Geng, Xiaoxiao, Zhou, Xinyue, Fast, Vladimir G., Zhang, Jianyi, Lu, Rui, and Zhou, Yang

Subjects

*CARDIAC contraction, *GENE enhancers, *MITOCHONDRIA, *HEART cells, *HEART development

Abstract

Background: Direct cardiac reprogramming of fibroblasts into cardiomyocytes has emerged as a promising strategy to remuscularize injured myocardium. However, it is insufficient to generate functional induced cardiomyocytes from human fibroblasts using conventional reprogramming cocktails, and the underlying molecular mechanisms are not well studied.Methods: To discover potential missing factors for human direct reprogramming, we performed transcriptomic comparison between human induced cardiomyocytes and functional cardiomyocytes.Results: We identified TBX20 (T-box transcription factor 20) as the top cardiac gene that is unable to be activated by the MGT133 reprogramming cocktail (MEF2C, GATA4, TBX5, and miR-133). TBX20 is required for normal heart development and cardiac function in adult cardiomyocytes, yet its role in cardiac reprogramming remains undefined. We show that the addition of TBX20 to the MGT133 cocktail (MGT+TBX20) promotes cardiac reprogramming and activates genes associated with cardiac contractility, maturation, and ventricular heart. Human induced cardiomyocytes produced with MGT+TBX20 demonstrated more frequent beating, calcium oscillation, and higher energy metabolism as evidenced by increased mitochondria numbers and mitochondrial respiration. Mechanistically, comprehensive transcriptomic, chromatin occupancy, and epigenomic studies revealed that TBX20 colocalizes with MGT reprogramming factors at cardiac gene enhancers associated with heart contraction, promotes chromatin binding and co-occupancy of MGT factors at these loci, and synergizes with MGT for more robust activation of target gene transcription.Conclusions: TBX20 consolidates MGT cardiac reprogramming factors to activate cardiac enhancers to promote cardiac cell fate conversion. Human induced cardiomyocytes generated with TBX20 showed enhanced cardiac function in contractility and mitochondrial respiration. [ABSTRACT FROM AUTHOR]

Published

2022

133. Fluorescent tagged episomals for stoichiometric induced pluripotent stem cell reprogramming

Author

Schmitt, Christopher E, Morales, Blanca M, Schmitz, Ellen MH, Hawkins, John S, Lizama, Carlos O, Zape, Joan P, Hsiao, Edward C, and Zovein, Ann C

Subjects

Stem Cell Research - Embryonic - Non-Human, Stem Cell Research, Biotechnology, Regenerative Medicine, Genetics, Generic health relevance, Analysis of Variance, Cell Differentiation, Cell Line, Cellular Reprogramming, Cellular Reprogramming Techniques, Gene Expression, Genetic Vectors, Green Fluorescent Proteins, Humans, Induced Pluripotent Stem Cells, Plasmids, Statistics, Nonparametric, Induced pluripotent stem cells, Reprogramming, Pluripotent stem cells, Episomals, Yamanaka factors, OKSM, Biological Sciences, Technology, Medical and Health Sciences

Abstract

BackgroundNon-integrating episomal vectors have become an important tool for induced pluripotent stem cell reprogramming. The episomal vectors carrying the "Yamanaka reprogramming factors" (Oct4, Klf, Sox2, and L-Myc + Lin28) are critical tools for non-integrating reprogramming of cells to a pluripotent state. However, the reprogramming process remains highly stochastic, and is hampered by an inability to easily identify clones that carry the episomal vectors.MethodsWe modified the original set of vectors to express spectrally separable fluorescent proteins to allow for enrichment of transfected cells. The vectors were then tested against the standard original vectors for reprogramming efficiency and for the ability to enrich for stoichiometric ratios of factors.ResultsThe reengineered vectors allow for cell sorting based on reprogramming factor expression. We show that these vectors can assist in tracking episomal expression in individual cells and can select the reprogramming factor dosage.ConclusionsTogether, these modified vectors are a useful tool for understanding the reprogramming process and improving induced pluripotent stem cell isolation efficiency.

Published

2017

134. Direct Reprogramming of Mouse Subchondral Bone Osteoblasts into Chondrocyte-like Cells.

Author

Li, Meihan, Zhang, Lingzhi, Li, Jing, and Zhu, Qing

Subjects

CARTILAGE cell transplantation, CARTILAGE regeneration, OSTEOBLASTS, CARTILAGE cells, GENE expression profiling, ARTICULAR cartilage

Abstract

Treatment of full-thickness articular cartilage defects with exposure of subchondral bone often seen in osteoarthritic conditions has long been a great challenge, especially with a focus on the feasibility of in situ cartilage regeneration through minimally invasive procedures. Osteoblasts that situate in the subchondral bone plate may be considered a potentially vital endogenous source of cells for cartilage resurfacing through direct reprogramming into chondrocytes. Microarray-based gene expression profiles were generated to compare tissue-specific transcripts between subchondral bone and cartilage of mice and to assess age-dependent differences of chondrocytes as well. On osteoblast cell lines established from mouse proximal tibial subchondral bone, sequential screening by co-transduction of transcription factor (TF) genes that distinguish chondrocytes from osteoblasts reveals a shortlist of potential reprogramming factors exhibiting combined effects in inducing chondrogenesis of subchondral bone osteoblasts. A further combinatorial approach unexpectedly identified two 3-TF combinations containing Sox9 and Sox5 that exhibit differences in reprogramming propensity with the third TF c-Myc or Plagl1, which appeared to direct the converted chondrocytes toward either a superficial or a deeper zone phenotype. Thus, our approach demonstrates the possibility of converting osteoblasts into two major chondrocyte subpopulations with two combinations of three genes (Sox9, Sox5, and c-Myc or Plagl1). The findings may have important implications for developing novel in situ regeneration strategies for the reconstruction of full-thickness cartilage defects. [ABSTRACT FROM AUTHOR]

Published

2022

135. Comparative Biology of Vertebrate Retinal Regeneration: Restoration of Vision through Cellular Reprogramming

Author

Thomas A. Reh and Levi Todd

Subjects

Mammals, Retina, genetic structures, Regeneration (biology), Mammalian retina, Vertebrate, Comparative biology, Biology, Cellular Reprogramming, eye diseases, General Biochemistry, Genetics and Molecular Biology, Nerve Regeneration, medicine.anatomical_structure, biology.animal, Vertebrates, medicine, Animals, sense organs, Neuroscience, Reprogramming, Vertebrate retina, Retinal regeneration

Abstract

The regenerative capacity of the vertebrate retina varies substantially across species. Whereas fish and amphibians can regenerate functional retina, mammals do not. In this perspective piece, we outline the various strategies nonmammalian vertebrates use to achieve functional regeneration of vision. We review key differences underlying the regenerative potential across species including the cellular source of postnatal progenitors, the diversity of cell fates regenerated, and the level of functional vision that can be achieved. Finally, we provide an outlook on the field of engineering the mammalian retina to replace neurons lost to injury or disease.

Published

2024

136. Epigenetic Reprogramming in Early Animal Development

Author

Zhenhai Du, Wei Xie, and Ke Zhang

Subjects

Epigenomics, Zygote, Totipotent, Embryonic Development, Gene Expression Regulation, Developmental, Embryo, Epigenome, Biology, Cellular Reprogramming, General Biochemistry, Genetics and Molecular Biology, Chromatin, Cell biology, Epigenesis, Genetic, medicine.anatomical_structure, medicine, Gamete, Animals, Reprogramming, Gametogenesis

Abstract

Dramatic nuclear reorganization occurs during early development to convert terminally differentiated gametes to a totipotent zygote, which then gives rise to an embryo. Aberrant epigenome resetting severely impairs embryo development and even leads to lethality. How the epigenomes are inherited, reprogrammed, and reestablished in this critical developmental period has gradually been unveiled through the rapid development of technologies including ultrasensitive chromatin analysis methods. In this review, we summarize the latest findings on epigenetic reprogramming in gametogenesis and embryogenesis, and how it contributes to gamete maturation and parental-to-zygotic transition. Finally, we highlight the key questions that remain to be answered to fully understand chromatin regulation and nuclear reprogramming in early development.

Published

2024

137. Magnetic and electric response of gold nanoparticles for low frequency applications in biological cells

Author

Harke, Saba and Harke, Saba

Abstract

In the context of biomedicine, electromagnetic fields are utilized in a variety of applications, such as cellular reprogramming. At frequencies below the microwave spectrum, electric and magnetic fields can often be considered as decoupled. Controlled reprogramming is an example in which biological cells (and gold nanoparticles) are exposed to an external magnetic field. In contrast, tumor treating fields (TTFields) subject tumor cells to an external electric field. The controlled reprogramming of cells is an important part of regenerative medicine and a promising treatment strategy for degenerative diseases like Parkinson’s. In biological in vitro experiments with cell cultures and in some in vivo studies, it has been shown that exposure of cells in combination with gold nanoparticles (AuNPs) to magnetic fields can lead to a significant improvement in cell conversion rates. However, the initial interaction between magnetic fields and cells involving physical laws is still not fully understood. TTFields have been approved for clinical use in Germany for the treatment of glioblastoma since 2015, resulting in a relatively new treatment method for these highly malignant tumors. The effects of TTFields on tumor cells have been extensively studied in association with physical laws, but are not yet fully resolved. In this thesis, I contribute to the understanding of the initial effect of electric and magnetic fields on cells and cells with gold nanoparticles. In particular, electromagnetic parameters are examined that are typical for TTFields and cellular reprogramming. I evaluate and apply analytical and numerical methods to calculate electromagnetic field distributions. These calculations serve as the basis for the assessment of possible mechanisms of action. Furthermore, an electric lumped element model for a cell is developed which compared to other models, analytical calculations and numerical electromagnetic simulations, implifies the approximation of the relative e

Published

2024

138. rTM reprograms macrophages via the HIF-1α/METTL3/PFKM axis to protect mice against sepsis.

Author

Yao C, Zhu H, Ji B, Guo H, Liu Z, Yang N, Zhang Q, Hai K, Gao C, Zhao J, Li X, Li R, Chen X, Meng F, Pan X, Fu C, Cheng W, Dong F, Yang J, Pan Y, and Ikezoe T

Subjects

Animals, Mice, Humans, Male, Mice, Inbred C57BL, Methyltransferases metabolism, Methyltransferases genetics, Mice, Knockout, Glycolysis, Cellular Reprogramming, Cytokines metabolism, Female, Sepsis metabolism, Hypoxia-Inducible Factor 1, alpha Subunit metabolism, Hypoxia-Inducible Factor 1, alpha Subunit genetics, Macrophages metabolism

Abstract

The metabolic reprogramming of macrophages is a potential therapeutic strategy for sepsis treatment, but the mechanism underlying this reprogramming remains unclear. Since glycolysis can drive macrophage phenotype switching, the rate-limiting enzymes in glycolysis may be key to treating sepsis. Here, we found that, compared with other isoenzymes, the expression of 6-phosphofructokinase, muscle type (PFKM) was the most upregulated in monocytes from septic patients. Recombinant thrombomodulin (rTM) treatment downregulated the protein expression of PFKM in macrophages. Both rTM treatment and Pfkm knockout protected mice from sepsis and reduced the production of the proinflammatory cytokines IL-1β, IL-6, TNF-α, and IL-27, whereas PFKM overexpression increased the production of these cytokines. Mechanistically, rTM treatment inhibited glycolysis in macrophages by decreasing PFKM expression in a hypoxia-inducible factor-1α (HIF-1α)-dependent manner. HIF-1α overexpression increased methyltransferase-like 3 (METTL3) expression, elevated the m 6 A level on Pfkm, and upregulated the protein expression of PFKM. METTL3 silence attenuated HIF-1α-mediated PFKM expression. These findings provide insight into the underlying mechanism of macrophage reprogramming for the treatment of sepsis., Competing Interests: Declarations Conflict of interest The authors have no relevant financial or nonfinancial interests to disclose. Ethics approval and consent to participate The study was approved by the Ethics Committee of Xuzhou Medical University (ethical approval number: XYFY2022-KL442-01). All animal studies and all experimental protocols were approved by the Institutional Animal Care and Use Committee of Xuzhou Medical University. Consent for publication All the authors approved the submission of the manuscript to this journal., (© 2024. The Author(s).)

Published

2024

139. Integrins α5β1 and αvβ3 Differentially Participate in the Recruitment and Reprogramming of Tumor-associated Macrophages in the In Vitro and In Vivo Models of Breast Tumor.

Author

Dalpati N, Rai SK, Dash SP, Kumar P, Singh D, and Sarangi PP

Subjects

Animals, Mice, Female, Cell Line, Tumor, Humans, Mice, Inbred BALB C, Disease Models, Animal, Cellular Reprogramming, Monocytes immunology, Monocytes metabolism, Signal Transduction immunology, Integrin alpha5beta1 metabolism, Breast Neoplasms immunology, Breast Neoplasms pathology, Breast Neoplasms metabolism, Tumor-Associated Macrophages immunology, Tumor-Associated Macrophages metabolism, Integrin alphaVbeta3 metabolism

Abstract

Tumor-associated macrophages (TAMs) drive the protumorigenic responses and facilitate tumor progression via matrix remodeling, angiogenesis, and immunosuppression by interacting with extracellular matrix proteins via integrins. However, the expression dynamics of integrin and its correlation with TAM functional programming in the tumors remain unexplored. In this study, we examined surface integrins' role in TAM recruitment and phenotypic programming in a 4T1-induced murine breast tumor model. Our findings show that integrin α5β1 is upregulated in CD11b+Ly6Chi monocytes in the bone marrow and blood by day 10 after tumor induction. Subsequent analysis revealed elevated integrin α5β1 expression on tumor-infiltrating monocytes (Ly6ChiMHC class II [MHCII]low) and M1 TAMs (F4/80+Ly6ClowMHCIIhi), whereas integrin αvβ3 was predominantly expressed on M2 TAMs (F4/80+Ly6ClowMHCIIlow), correlating with higher CD206 and MERTK expression. Gene profiling of cells sorted from murine tumors showed that CD11b+Ly6G-F4/80+α5+ TAMs had elevated inflammatory genes (IL-6, TNF-α, and STAT1/2), whereas CD11b+Ly6G-F4/80+αv+ TAMs exhibited a protumorigenic phenotype (IL-10, Arg1, TGF-β, and STAT3/6). In vitro studies demonstrated that blocking integrin α5 and αv during macrophage differentiation from human peripheral blood monocytes reduced cell spreading and expression of CD206 and CD163 in the presence of specific matrix proteins, fibronectin, and vitronectin. Furthermore, RNA sequencing data analysis (GEO dataset: GSE195857) from bone marrow-derived monocytes and TAMs in 4T1 mammary tumors revealed differential integrin α5 and αv expression and their association with FAK and SRC kinase. In line with this, FAK inhibition during TAM polarization reduced SRC, STAT1, and STAT6 phosphorylation. In conclusion, these findings underscore the crucial role of integrins in TAM recruitment, polarization, and reprogramming in tumors., (Copyright © 2024 by The American Association of Immunologists, Inc.)

Published

2024

140. Neural crest precursors from the skin are the primary source of directly reprogrammed neurons.

Author

Belair-Hickey JJ, Fahmy A, Zhang W, Sajid RS, Coles BLK, Salter MW, and van der Kooy D

Subjects

Animals, Mice, Fibroblasts cytology, Fibroblasts metabolism, Cells, Cultured, Neural Crest cytology, Neurons cytology, Neurons metabolism, Cellular Reprogramming, Skin cytology, Cell Lineage, Neural Stem Cells cytology, Neural Stem Cells metabolism, Cell Differentiation

Abstract

Direct reprogramming involves the conversion of differentiated cell types without returning to an earlier developmental state. Here, we explore how heterogeneity in developmental lineage and maturity of the starting cell population contributes to direct reprogramming using the conversion of murine fibroblasts into neurons. Our hypothesis is that a single lineage of cells contributes to most reprogramming and that a rare elite precursor with intrinsic bias is the source of reprogrammed neurons. We find that nearly all reprogrammed neurons are derived from the neural crest (NC) lineage. Moreover, when rare proliferating NC precursors are selectively ablated, there is a large reduction in the number of reprogrammed neurons. Previous interpretations of this paradigm are that it demonstrates a cell fate conversion across embryonic germ layers (mesoderm to ectoderm). Our interpretation is that this is actually directed differentiation of a neural lineage stem cell in the skin that has intrinsic bias to produce neuronal progeny., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

141. Reprogramming tumor-associated macrophages using exosomes from M1 macrophages.

Author

Mahmoudi M, Taghavi-Farahabadi M, Hashemi SM, Mousavizadeh K, Rezaei N, and Mojtabavi N

Subjects

Animals, Mice, RAW 264.7 Cells, Cellular Reprogramming, Cytokines metabolism, Macrophages metabolism, Macrophages immunology, Macrophage Activation, Tumor Microenvironment immunology, Exosomes metabolism, Tumor-Associated Macrophages immunology, Tumor-Associated Macrophages metabolism, Tumor-Associated Macrophages pathology, Phagocytosis

Abstract

Macrophages, abundant in tumors, are classified as M1 or M2 types with M2 dominating the tumor microenvironment. Shifting macrophages from M2 to M1 using exosomes is a promising intervention. The properties of exosomes depend on their source cells. M1-exosomes are expected to polarize macrophages towards M1 phenotype. We compared M1-exosomes and M0-exosomes' effects on M2 macrophage polarization. The RAW264.7 cells were cultured and one group of them was exposed to LPS. The serum-free medium was collected and exosomes were extracted. Exosomes were analyzed by scanning and transmission electron microscopy, dynamic light scattering and Western blot. Subsequently, M1 or M0 exosomes were applied to M2 macrophages induced by IL4. The macrophages polarization, including M1 and M2 genes and surface markers expression, cytokines secretion, and phagocytosis ability were evaluated. It was demonstrated that M1-exosomes induced macrophage polarization toward the M1 phenotype, characterized by an upregulation of M1-specific markers and a downregulation of M2 markers. Furthermore, the secretion of TNF-α was increased, while the secretion of IL-10 was decreased. The phagocytosis ability of M1-exosome-treated macrophages was also augmented. This research suggested that M1-exosomes might be promising candidates for modulating immune response in situations marked by an overabundance of M2 polarization, like in cancer., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

142. Various Strategies of Tendon Stem/Progenitor Cell Reprogramming for Tendon Regeneration.

Author

Ahn SY

Subjects

Humans, Animals, Rotator Cuff Injuries metabolism, Rotator Cuff Injuries therapy, Cellular Reprogramming, Regenerative Medicine methods, Rotator Cuff, Regeneration, Tendons cytology, Tendons metabolism, Tendons physiology, Stem Cells metabolism, Stem Cells cytology

Abstract

Rotator cuff tears (RCT) are the most common cause of shoulder pain among adults. "Rotator cuff" refers to the four muscles that cover the shoulder joint: supraspinatus, infraspinatus, subscapularis, and teres minor. These muscles help maintain the rotational movement and stability of the shoulder joint. RCT is a condition in which one or more of these four muscles become ruptured or damaged, causing pain in the arms and shoulders. RCT results from degenerative changes caused by chronic inflammation of the tendons and consequent tendon tissue defects. This phenomenon occurs because of the exhaustion of endogenous tendon stem cells. Tendon regeneration requires rejuvenation of these endogenous tendon stem/progenitor cells (TSPCs) prior to their growth phase. TSPCs exhibit clonogenicity, multipotency, and self-renewal properties; they express classical stem cell markers and genes associated with the tendon lineage. However, specific markers for TSPC are yet to be identified. In this review, we introduce novel TSPC markers and discuss various strategies for TSPC reprogramming. With further research, TSPC reprogramming technology could be adapted to treat age-related degenerative diseases, providing a new strategy for regenerative medicine.

Published

2024

143. Central role of hypoxia-inducible factor-1α in metabolic reprogramming of cancer cells: A review.

Author

Zhu B, Cheng L, Huang B, Liu R, and Ren B

Subjects

Humans, Antineoplastic Agents pharmacology, Antineoplastic Agents therapeutic use, Cellular Reprogramming, Metabolic Reprogramming, Hypoxia-Inducible Factor 1, alpha Subunit metabolism, Neoplasms metabolism, Neoplasms drug therapy, Drug Resistance, Neoplasm

Abstract

Metabolic reprogramming is one of the characteristics of tumor cell metabolism. In tumor cells, there are multiple metabolic enzymes and membrane proteins to regulate metabolic reprogramming, and hypoxia inducible factor-1α (HIF-1α) can be regulated in transcription, translation, posttranslational modification and other aspects through multiple pathways, and HIF-1α affects multiple metabolic enzymes and membrane proteins during metabolic reprogramming, thus playing a central role in the metabolic reprogramming process, and thus has some implications for tumor therapy and understanding chemotherapy drug resistance. HIF-1α affects a number of metabolic enzymes and membrane proteins in the metabolic reprogramming process, thus playing a central role in the metabolic reprogramming process, which has certain significance for the treatment of tumors and the understanding of chemotherapeutic drug resistance. In this paper, we review the central role of HIF-1α in metabolic reprogramming, chemotherapeutic agents targeting HIF-1α, and chemotherapeutic drug resistance., Competing Interests: The authors have no funding and conflicts of interest to disclose., (Copyright © 2024 the Author(s). Published by Wolters Kluwer Health, Inc.)

Published

2024

144. Ependymal cell lineage reprogramming as a potential therapeutic intervention for hydrocephalus.

Author

Kaplani K, Lalioti ME, Vassalou S, Lokka G, Parlapani E, Kritikos G, Lygerou Z, and Taraviras S

Subjects

Animals, Mice, Disease Models, Animal, Astrocytes metabolism, Cell Lineage, Hydrocephalus therapy, Hydrocephalus pathology, Hydrocephalus genetics, Hydrocephalus metabolism, Ependyma metabolism, Ependyma cytology, Cellular Reprogramming

Abstract

Hydrocephalus is a common neurological condition, characterized by the excessive accumulation of cerebrospinal fluid in the cerebral ventricles. Primary treatments for hydrocephalus mainly involve neurosurgical cerebrospinal fluid diversion, which hold high morbidity and failure rates, highlighting the necessity for the discovery of novel therapeutic approaches. Although the pathophysiology of hydrocephalus is highly multifactorial, impaired function of the brain ependymal cells plays a fundamental role in hydrocephalus. Here we show that GemC1 and McIdas, key regulators of multiciliated ependymal cell fate determination, induce direct cellular reprogramming towards ependyma. Our study reveals that ectopic expression of GemC1 and McIdas reprograms cortical astrocytes and programs mouse embryonic stem cells into ependyma. McIdas is sufficient to establish functional activity in the reprogrammed astrocytes. Furthermore, we show that McIdas' expression promotes ependymal cell regeneration in two different postnatal hydrocephalus mouse models: an intracranial hemorrhage and a genetic form of hydrocephalus and ameliorates the cytoarchitecture of the neurogenic niche. Our study provides evidence on the restoration of ependyma in animal models mimicking hydrocephalus that could be exploited towards future therapeutic interventions., Competing Interests: Disclosure and competing interests statement Zoi Lygerou is an EMBO Council member. This has no bearing on the editorial consideration of this article for publication. The remaining authors declare no competing interests., (© 2024. The Author(s).)

Published

2024

145. Small Molecule-Mediated Stage-Specific Reprogramming of MSCs to Hepatocyte-Like Cells and Hepatic Tissue for Liver Injury Treatment.

Author

Gupta S, Sharma A, Rajakannu M, Bisevac J, Rela M, and Verma RS

Subjects

Animals, Rats, Humans, Cellular Reprogramming, Male, Mesenchymal Stem Cell Transplantation, Cells, Cultured, Hepatocytes metabolism, Hepatocytes cytology, Mesenchymal Stem Cells cytology, Mesenchymal Stem Cells metabolism, Cell Differentiation, Liver cytology, Liver metabolism

Abstract

Background: Derivation of hepatocytes from stem cells has been established through various protocols involving growth factor (GF) and small molecule (SM) agents, among others. However, mesenchymal stem cell-based derivation of hepatocytes still remains expensive due to the use of a cocktail of growth factors, and a long duration of differentiation is needed, thus limiting its potential clinical application., Methods: In this study, we developed a chemically defined differentiation strategy that is exclusively based on SM and takes 14 days, while the GF-based protocol requires 23-28 days., Results: We optimized a stage-specific differentiation protocol for the differentiation of rat bone marrow-derived mesenchymal stem cells (MSCs) into functional hepatocyte-like cells (dHeps) that involved four stages, i.e., definitive endoderm (DE), hepatic competence (HC), hepatic specification (HS) and hepatic differentiation and growth. We further generated hepatic tissue using human decellularized liver extracellular matrix and compared it with hepatic tissue derived from the growth factor-based protocol at the transcriptional level. dHep, upon transplantation in a rat model of acute liver injury (ALI), was capable of ameliorating liver injury in rats and improving liver function and tissue damage compared to those in the ALI model., Conclusions: In summary, this is the first study in which hepatocytes and hepatic tissue were derived from MSCs utilizing a stage-specific strategy by exclusively using SM as a differentiation factor., Competing Interests: Declarations Ethics Approval and Consent to Participate The patient(s) or their guardian(s)/legally authorized representative(s) provided written informed consent for participation in the study and/or the use of samples. Information regarding ethical approval as follows. Animal study: Title—“Development of vascularized liver tissue using Mesenchymal Stem Cells (MSCs) and HUVECs in decellularized liver biomatrix”, Approval no—IEC/2018/01/RSV-6/10 approved date – 15.07.2018. Human sample: Title – “Reengineering vascularized liver tissue using decellularized liver matrix”. Approval no – 03092018, Approval date – 04.09.2018. No clinical data from healthy or surviving liver ailment related patients were used in the study. Consent for Publication The study does not include person data in any form. Cadaveric liver organ was used in the present study and the ethical information approved by the institute has been included under the section “Animal and Human Ethics Approval” in the materials and method section. The patient(s) or their guardian(s)/legally authorized representative(s) provided written informed consent for participation in the study and/or the use of samples. Conflic of Interest The authors declare no conflicts of interest., (© 2024. The Author(s).)

Published

2024

146. Bioprocessing considerations for generation of iPSCs intended for clinical application: perspectives from the ISCT Emerging Regenerative Medicine Technology working group.

Author

Song HW, Solomon JN, Masri F Ph.D, Mack A, Durand N, Cameau E, Dianat N, Hunter A, Oh S, Schoen B, Marsh M, Bravery C, Sumen C, Clarke D, Bharti K, Allickson JG, and Lakshmipathy U

Subjects

Humans, Cell- and Tissue-Based Therapy methods, Cell Differentiation, Cell Culture Techniques methods, Cellular Reprogramming, Cryopreservation methods, Induced Pluripotent Stem Cells cytology, Regenerative Medicine methods

Abstract

Approval of induced pluripotent stem cells (iPSCs) for the manufacture of cell therapies to support clinical trials is now becoming realized after 20 years of research and development. In 2022 the International Society for Cell and Gene Therapy (ISCT) established a Working Group on Emerging Regenerative Medicine Technologies, an area in which iPSCs-derived technologies are expected to play a key role. In this article, the Working Group surveys the steps that an end user should consider when generating iPSCs that are stable, well-characterised, pluripotent, and suitable for making differentiated cell types for allogeneic or autologous cell therapies. The objective is to provide the reader with a holistic view of how to achieve high-quality iPSCs from selection of the starting material through to cell banking. Key considerations include: (i) intellectual property licenses; (ii) selection of the raw materials and cell sources for creating iPSC intermediates and master cell banks; (iii) regulatory considerations for reprogramming methods; (iv) options for expansion in 2D vs. 3D cultures; and (v) available technologies and equipment for harvesting, washing, concentration, filling, cryopreservation, and storage. Some key process limitations are highlighted to help drive further improvement and innovation, and includes recommendations to close and automate current open and manual processes., (Copyright © 2024. Published by Elsevier Inc.)

Published

2024

147. Reprogramming astroglia into neurons with hallmarks of fast-spiking parvalbumin-positive interneurons by phospho-site-deficient Ascl1.

Author

Marichal N, Péron S, Beltrán Arranz A, Galante C, Franco Scarante F, Wiffen R, Schuurmans C, Karow M, Gascón S, and Berninger B

Subjects

Animals, Mice, Neurons metabolism, Neurons cytology, Action Potentials, Phosphorylation, Cell Differentiation, Basic Helix-Loop-Helix Transcription Factors metabolism, Basic Helix-Loop-Helix Transcription Factors genetics, Astrocytes metabolism, Astrocytes cytology, Cellular Reprogramming, Interneurons metabolism, Parvalbumins metabolism

Abstract

Cellular reprogramming of mammalian glia to an induced neuronal fate holds the potential for restoring diseased brain circuits. While the proneural factor achaete-scute complex-like 1 ( Ascl1 ) is widely used for neuronal reprogramming, in the early postnatal mouse cortex, Ascl1 fails to induce the glia-to-neuron conversion, instead promoting the proliferation of oligodendrocyte progenitor cells (OPC). Since Ascl1 activity is posttranslationally regulated, here, we investigated the consequences of mutating six serine phospho-acceptor sites to alanine (Ascl1SA6) on lineage reprogramming in vivo. Ascl1SA6 exhibited increased neurogenic activity in the glia of the early postnatal mouse cortex, an effect enhanced by coexpression of B cell lymphoma 2 ( Bcl2 ). Genetic fate-mapping revealed that most induced neurons originated from astrocytes, while only a few derived from OPCs. Many Ascl1SA6/Bcl2-induced neurons expressed parvalbumin and were capable of high-frequency action potential firing. Our study demonstrates the authentic conversion of astroglia into neurons featuring subclass hallmarks of cortical interneurons, advancing our scope of engineering neuronal fates in the brain.

Published

2024

148. Isocitrate dehydrogenases 2-mediated dysfunctional metabolic reprogramming promotes intestinal cancer progression via regulating HIF-1A signaling pathway.

Author

Liu S, Zhou Y, Chen Y, Qiao Y, Bai L, Zhang S, Men D, Zhang H, Pan F, Gao Y, Wang J, and Wang Y

Subjects

Humans, Animals, Cell Line, Tumor, Mice, Colorectal Neoplasms metabolism, Colorectal Neoplasms pathology, Ketoglutaric Acids metabolism, Citric Acid Cycle, Glycolysis, Mice, Nude, Disease Progression, Adenosine Triphosphate metabolism, Cell Proliferation, Cellular Reprogramming, Mitochondria metabolism, Intestinal Neoplasms pathology, Intestinal Neoplasms metabolism, Metabolic Reprogramming, Isocitrate Dehydrogenase metabolism, Isocitrate Dehydrogenase genetics, Hypoxia-Inducible Factor 1, alpha Subunit metabolism, Hypoxia-Inducible Factor 1, alpha Subunit genetics, Signal Transduction

Abstract

Changes in isocitrate dehydrogenases (IDH) lead to the production of the cancer-causing metabolite 2-hydroxyglutarate, making them a cause of cancer. However, the specific role of IDH in the progression of colon cancer is still not well understood. Our current study provides evidence that IDH2 is significantly increased in colorectal cancer (CRC) cells and actively promotes cell growth in vitro and the development of tumors in vivo. Inhibiting the activity of IDH2, either through genetic silencing or pharmacological inhibition, results in a significant increase in α-ketoglutarate (α-KG), indicating a decrease in the reductive citric acid cycle. The excessive accumulation of α-KG caused by the inactivation of IDH2 obstructs the generation of ATP in mitochondria and promotes the downregulation of HIF-1A, eventually inhibiting glycolysis. This dual metabolic impact results in a reduction in ATP levels and the suppression of tumor growth. Our study reveals a metabolic trait of colorectal cancer cells, which involves the active utilization of glutamine through reductive citric acid cycle metabolism. The data suggests that IDH2 plays a crucial role in this metabolic process and has the potential to be a valuable target for the advancement of treatments for colorectal cancer., (Copyright © 2024. Published by Elsevier B.V.)

Published

2024

149. Mitochondrial morphology and energy metabolism in reprogrammed porcine expanded potential stem cells.

Author

Lee YJ, Song JH, Lee JW, Hong TK, Uhm SJ, Hong K, and Do JT

Abstract

Objective: Expanded potential stem cells (EPSCs) are stem cells that can differentiate into embryonic and extraembryonic lineages, including extraembryonic endoderm and trophoblast lineages. Therefore, EPSCs have great potential in advancing regenerative medicine, elucidating disease mechanisms, and exploring early embryonic development. However, the generation and characterization of EPSCs in pigs have not been thoroughly explored. In this study, we successfully generated porcine EPSCs (pEPSCs)., Methods: We reprogrammed porcine fetal fibroblasts (PFFs) using an integration-free method with Sendai virus vectors., Results: The resulting pEPSCs expressed key pluripotency markers and demonstrated the ability to differentiate between embryonic and extraembryonic lineages. Notably, reprogramming into pEPSCs was associated with a transformation of mitochondrial morphology from the elongated form observed in PFFs to a globular shape, reflecting potential alterations in energy metabolism. We observed significant remodeling of mitochondrial morphology and a subsequent shift towards glycolytic energy dependence during the reprogramming of PFFs into pEPSCs., Conclusion: Our findings provide valuable insights into the characteristics of EPSCs in pigs and highlight their potential applications in regenerative medicine, disease modeling, and emerging fields such as cell-based meat production.

Published

2024

150. Glucose impacts onto the reciprocal reprogramming between mammary adipocytes and cancer cells.

Author

Ambrosio MR, Adriaens M, Derks K, Migliaccio T, Costa V, Liguoro D, Cataldi S, D'Esposito V, Maneli G, Bassolino R, Di Paola S, Pirozzi M, Schonauer F, D'Andrea F, Beguinot F, Arts I, and Formisano P

Subjects

Humans, Female, Mesenchymal Stem Cells metabolism, Cellular Reprogramming, Cell Differentiation, Transcriptome, Tumor Microenvironment, Cell Line, Tumor, Adipocytes metabolism, Glucose metabolism, Breast Neoplasms metabolism, Breast Neoplasms pathology, Coculture Techniques

Abstract

An established hallmark of cancer cells is metabolic reprogramming, largely consisting in the exacerbated glucose uptake. Adipocytes in the tumor microenvironment contribute toward breast cancer (BC) progression and are highly responsive to metabolic fluctuations. Metabolic conditions characterizing obesity and/or diabetes associate with increased BC incidence and mortality. To explore BC-adipocytes interaction and define the impact of glucose in such dialogue, Mammary Adipose-derived Mesenchymal Stem Cells (MAd-MSCs) were differentiated into adipocytes and co-cultured with ER + BC cells while exposed to glucose concentration resembling hyperglycemia or normoglycemia in humans (25mM or 5.5mM). The transcriptome of both cell types in co-culture as in mono-culture was profiled by RNA-Seq to define the impact of adipocytes on BC cells and viceversa (i), the action of glucose on BC cells, adipocytes (ii) and their crosstalk (iii). Noteworthy, we provided evidence that co-culture with adipocytes in a glucose-rich environment determined a re-program of BC cell transcriptome driving lipid accumulation, a hallmark of BC aggressiveness, promoting stem-like properties and reducing Tamoxifen responsiveness. Moreover, our data point out to a transcriptional effect through which BC cells induce adipocytes de-lipidation, paralleled by pluripotency gain, as source of lipids when glucose lowering occurs. Thus, modulating plasticity of peri-tumoral adipocytes may represent a key point for halting BC progression in metabolically unbalanced patients., (© 2024. The Author(s).)

Published

2024