Your search keyword '"NEUROG3"' showing total 97 results

1. Single-cell transcriptome and accessible chromatin dynamics during endocrine pancreas development

Author

Duvall, Eliza, Benitez, Cecil M, Tellez, Krissie, Enge, Martin, Pauerstein, Philip T, Li, Lingyu, Baek, Songjoon, Quake, Stephen R, Smith, Jason P, Sheffield, Nathan C, Kim, Seung K, and Arda, H Efsun

Subjects

Biochemistry and Cell Biology, Genetics, Biological Sciences, Stem Cell Research - Nonembryonic - Non-Human, Cancer, Orphan Drug, Pancreatic Cancer, Rare Diseases, Human Genome, Digestive Diseases, Diabetes, Biotechnology, Stem Cell Research, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Metabolic and endocrine, Animals, Basic Helix-Loop-Helix Transcription Factors, Cell Differentiation, Cell Lineage, Chromatin, Gene Expression Regulation, Developmental, Islets of Langerhans, Mice, Nerve Tissue Proteins, Single-Cell Analysis, Transcriptome, ATAC-seq, Neurog3, pancreas, scRNA-seq

Abstract

Delineating gene regulatory networks that orchestrate cell-type specification is a continuing challenge for developmental biologists. Single-cell analyses offer opportunities to address these challenges and accelerate discovery of rare cell lineage relationships and mechanisms underlying hierarchical lineage decisions. Here, we describe the molecular analysis of mouse pancreatic endocrine cell differentiation using single-cell transcriptomics, chromatin accessibility assays coupled to genetic labeling, and cytometry-based cell purification. We uncover transcription factor networks that delineate β-, α-, and δ-cell lineages. Through genomic footprint analysis, we identify transcription factor-regulatory DNA interactions governing pancreatic cell development at unprecedented resolution. Our analysis suggests that the transcription factor Neurog3 may act as a pioneer transcription factor to specify the pancreatic endocrine lineage. These findings could improve protocols to generate replacement endocrine cells from renewable sources, like stem cells, for diabetes therapy.

Published

2022

2. Single-cell transcriptome analysis of NEUROG3+ cells during pancreatic endocrine differentiation with small molecules

Author

Jin Li, Junru Chen, Xiaoyu Luo, Guangxiu Lu, and Ge Lin

Subjects

Pancreatic endocrine cells, hESCs, DAPT + 4FS, NEUROG3, Medicine (General), R5-920, Biochemistry, QD415-436

Abstract

Abstract The efficiency of inducing human embryonic stem cells into NEUROG3+ pancreatic endocrine cells is a bottleneck in stem cell therapy for diabetes. To understand the cell properties and fate decisions during differentiation, we analyzed the modified induction method using single-cell transcriptome and found that DAPT combined with four factors (4FS): nicotinamide, dexamethasone, forskolin and Alk5 inhibitor II (DAPT + 4FS) increased the expression of NEUROG3 to approximately 34.3%. The increased NEUROG3+ cells were mainly concentrated in Insulin + Glucagon + (INS + GCG+) and SLAC18A1 + Chromogranin A+(SLAC18A1 + CHGA +) populations, indicating that the increased NEUROG3+ cells promoted the differentiation of pancreatic endocrine cells and enterochromaffin-like cells. Single-cell transcriptome analysis provided valuable clues for further screening of pancreatic endocrine cells and differentiation of pancreatic islet cells. The gene set enrichment analysis (GSEA) suggest that we can try to promote the expression of INS + GCG+ population by up-regulating G protein-coupled receptor (GPCR) and mitogen-activated protein kinase signals and down-regulating Wnt, NIK/NF-KappaB and cytokine-mediated signal pathways. We can also try to regulate GPCR signaling through PLCE1, so as to increase the proportion of NEUROG3+ cells in INS+GCG+ populations. To exclude non-pancreatic endocrine cells, ALCAMhigh CD9low could be used as a marker for endocrine populations, and ALCAMhigh CD9lowCDH1low could remove the SLC18A1 + CHGA+ population.

Published

2023

3. Single-cell transcriptome analysis of NEUROG3+ cells during pancreatic endocrine differentiation with small molecules.

Author

Li, Jin, Chen, Junru, Luo, Xiaoyu, Lu, Guangxiu, and Lin, Ge

Subjects

*SMALL molecules, *NICOTINAMIDE, *HUMAN embryonic stem cells, *MITOGEN-activated protein kinases, *CELL analysis, *G protein coupled receptors, *GLUCAGON-like peptide-1 receptor, *MITOGENS

Abstract

The efficiency of inducing human embryonic stem cells into NEUROG3+ pancreatic endocrine cells is a bottleneck in stem cell therapy for diabetes. To understand the cell properties and fate decisions during differentiation, we analyzed the modified induction method using single-cell transcriptome and found that DAPT combined with four factors (4FS): nicotinamide, dexamethasone, forskolin and Alk5 inhibitor II (DAPT + 4FS) increased the expression of NEUROG3 to approximately 34.3%. The increased NEUROG3+ cells were mainly concentrated in Insulin + Glucagon + (INS + GCG+) and SLAC18A1 + Chromogranin A+(SLAC18A1 + CHGA +) populations, indicating that the increased NEUROG3+ cells promoted the differentiation of pancreatic endocrine cells and enterochromaffin-like cells. Single-cell transcriptome analysis provided valuable clues for further screening of pancreatic endocrine cells and differentiation of pancreatic islet cells. The gene set enrichment analysis (GSEA) suggest that we can try to promote the expression of INS + GCG+ population by up-regulating G protein-coupled receptor (GPCR) and mitogen-activated protein kinase signals and down-regulating Wnt, NIK/NF-KappaB and cytokine-mediated signal pathways. We can also try to regulate GPCR signaling through PLCE1, so as to increase the proportion of NEUROG3+ cells in INS+GCG+ populations. To exclude non-pancreatic endocrine cells, ALCAMhigh CD9low could be used as a marker for endocrine populations, and ALCAMhigh CD9lowCDH1low could remove the SLC18A1 + CHGA+ population. [ABSTRACT FROM AUTHOR]

Published

2023

4. Extensive NEUROG3 occupancy in the human pancreatic endocrine gene regulatory network

Author

Valérie Schreiber, Reuben Mercier, Sara Jiménez, Tao Ye, Emmanuel García-Sánchez, Annabelle Klein, Aline Meunier, Sabitri Ghimire, Catherine Birck, Bernard Jost, Kristian Honnens de Lichtenberg, Christian Honoré, Palle Serup, and Gérard Gradwohl

Subjects

NEUROG3, iPSC, Islet progenitors, CUT&RUN, T2DM, SNPs, Internal medicine, RC31-1245

Abstract

Objective: Mice lacking the bHLH transcription factor (TF) Neurog3 do not form pancreatic islet cells, including insulin-secreting beta cells, the absence of which leads to diabetes. In humans, homozygous mutations of NEUROG3 manifest with neonatal or childhood diabetes. Despite this critical role in islet cell development, the precise function of and downstream genetic programs regulated directly by NEUROG3 remain elusive. Therefore, we mapped genome-wide NEUROG3 occupancy in human induced pluripotent stem cell (hiPSC)–derived endocrine progenitors and determined NEUROG3 dependency of associated genes to uncover direct targets. Methods: We generated a novel hiPSC line (NEUROG3-HA-P2A-Venus) where NEUROG3 is HA-tagged and fused to a self-cleaving fluorescent VENUS reporter. We used the CUT&RUN technique to map NEUROG3 occupancy and epigenetic marks in pancreatic endocrine progenitors (PEP) that were differentiated from this hiPSC line. We integrated NEUROG3 occupancy data with chromatin status and gene expression in PEPs as well as their NEUROG3-dependence. In addition, we investigated whether NEUROG3 binds type 2 diabetes mellitus (T2DM)–associated variants at the PEP stage. Results: CUT&RUN revealed a total of 863 NEUROG3 binding sites assigned to 1263 unique genes. NEUROG3 occupancy was found at promoters as well as at distant cis-regulatory elements that frequently overlapped within PEP active enhancers. De novo motif analyses defined a NEUROG3 consensus binding motif and suggested potential co-regulation of NEUROG3 target genes by FOXA or RFX transcription factors. We found that 22% of the genes downregulated in NEUROG3−/− PEPs, and 10% of genes enriched in NEUROG3-Venus positive endocrine cells were bound by NEUROG3 and thus likely to be directly regulated. NEUROG3 binds to 138 transcription factor genes, some with important roles in islet cell development or function, such as NEUROD1, PAX4, NKX2-2, SOX4, MLXIPL, LMX1B, RFX3, and NEUROG3 itself, and many others with unknown islet function. Unexpectedly, we uncovered that NEUROG3 targets genes critical for insulin secretion in beta cells (e.g., GCK, ABCC8/KCNJ11, CACNA1A, CHGA, SCG2, SLC30A8, and PCSK1). Thus, analysis of NEUROG3 occupancy suggests that the transient expression of NEUROG3 not only promotes islet destiny in uncommitted pancreatic progenitors, but could also initiate endocrine programs essential for beta cell function. Lastly, we identified eight T2DM risk SNPs within NEUROG3-bound regions. Conclusion: Mapping NEUROG3 genome occupancy in PEPs uncovered unexpectedly broad, direct control of the endocrine genes, raising novel hypotheses on how this master regulator controls islet and beta cell differentiation.

Published

2021

5. Gene Signatures of NEUROGENIN3+ Endocrine Progenitor Cells in the Human Pancreas

Author

Hyo Jeong Yong, Gengqiang Xie, Chengyang Liu, Wei Wang, Ali Naji, Jerome Irianto, and Yue J. Wang

Subjects

NEUROG3, endocrine progenitor, epsilon cells, human pancreas, single-cell RNA-seq, data integration, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

NEUROGENIN3+ (NEUROG3+) cells are considered to be pancreatic endocrine progenitors. Our current knowledge on the molecular program of NEUROG3+ cells in humans is largely extrapolated from studies in mice. We hypothesized that single-cell RNA-seq enables in-depth exploration of the rare NEUROG3+ cells directly in humans. We aligned four large single-cell RNA-seq datasets from postnatal human pancreas. Our integrated analysis revealed 10 NEUROG3+ epithelial cells from a total of 11,174 pancreatic cells. Noticeably, human NEUROG3+ cells clustered with mature pancreatic cells and epsilon cells displayed the highest frequency of NEUROG3 positivity. We confirmed the co-expression of NEUROG3 with endocrine markers and the high percentage of NEUROG3+ cells among epsilon cells at the protein level based on immunostaining on pancreatic tissue sections. We further identified unique genetic signatures of the NEUROG3+ cells. Regulatory network inference revealed novel transcription factors including Prospero homeobox protein 1 (PROX1) may act jointly with NEUROG3. As NEUROG3 plays a central role in endocrine differentiation, knowledge gained from our study will accelerate the development of beta cell regeneration therapies to treat diabetes.

Published

2021

6. Immunohistochemical characterization of pancreatic duodenal homeobox protein-1, neurogenin-3 and insulin protein expressions in islet-mesenchymal cell in vitro interactions from injured adult pancreatic tissues: a morphochronological evaluation

Author

Juziel Manda and Venant Tchokonte-Nana

Subjects

Co-culture, Duct ligated pancreas, Insulin, Islet, MSC, NeuroG3, Pdx1, Transplantation, Medicine

Abstract

Objective(s): The use of a co-culture of islets with mesenchymal stromal cells (MSCs) is a promising therapy in islet transplantation to revert hyperglycaemia, but the resulting insulin-producing cells (IPCs) express low levels of pancreas endocrine developmental genes. This study aims to investigate the morphochronology of a co-culture of islets with MSCs from injured adult pancreata, and characterize pancreatic duodenal homeobox protein-1 (Pdx1), neurogenin-3 (Ngn3) and insulin protein expressions to establish the fate of their interaction. Materials and Methods: Islets and MSCs were isolated from sham operated control (SOC) and duct-ligated (PPDL) pancreata. Islets from SOC or PPDL tissues were cultured with or without MSCs in RPMI1640, supplemented by 1% Penicillin-Streptomycin, and maintained at 37 °C±1 °C at 95% relative humidity and 95% /5% air/CO2. Pdx1, Ngn3 and insulin expressions were determined by immunohistochemistry and islet morphochronological changes were assessed. Results: Pdx1 was expressed in all islet-cell cultures with or without MSCs. Pdx1+ islet cells were significantly increased in the presence of MSCs compared to the islet culture without MSCs. Similarly, Ngn3 was highly expressed in all cultures with MSCs from both SOC and PPDL tissues and the expression was prolonged in cultures using PPDL tissues before it was down-regulated, thereby, extending the period of Ngn3+ cell expansion and differentiation into mature functional islets. Conclusion: In vitro, MSCs maintain a pool of Ngn3+ that contributes to insulin production from mature beta cells but the activation of insulin production from non-beta cells may not be induced by direct signals from MSCs.

Published

2018

7. Transcription factors that shape the mammalian pancreas.

Author

Jennings, Rachel E., Scharfmann, Raphael, and Staels, Willem

Abstract

Improving our understanding of mammalian pancreas development is crucial for the development of more effective cellular therapies for diabetes. Most of what we know about mammalian pancreas development stems from mouse genetics. We have learnt that a unique set of transcription factors controls endocrine and exocrine cell differentiation. Transgenic mouse models have been instrumental in studying the function of these transcription factors. Mouse and human pancreas development are very similar in many respects, but the devil is in the detail. To unravel human pancreas development in greater detail, in vitro cellular models (including directed differentiation of stem cells, human beta cell lines and human pancreatic organoids) are used; however, in vivo validation of these results is still needed. The current best 'model' for studying human pancreas development are individuals with monogenic forms of diabetes. In this review, we discuss mammalian pancreas development, highlight some discrepancies between mouse and human, and discuss selected transcription factors that, when mutated, cause permanent neonatal diabetes. [ABSTRACT FROM AUTHOR]

Published

2020

8. Ascl1 is required to specify a subset of ventromedial hypothalamic neurons.

Author

Aslanpour, Shaghayegh, Rosin, Jessica M., Balakrishnan, Anjali, Klenin, Natalia, Blot, Florence, Gradwohl, Gerard, Schuurmans, Carol, and Kurrasch, Deborah M.

Subjects

*NEURONS, *HYPOTHALAMUS, *DEVELOPMENTAL programs

Abstract

Despite clear physiological roles, the ventromedial hypothalamus (VMH) developmental programs are poorly understood. Here, we asked whether the proneural gene achaete-scute homolog 1 (Ascl1) contributes to VMH development. Ascl1 transcripts were detected in embryonic day (E) 10.5 to postnatal day 0 VMH neural progenitors. The elimination of Ascl1 reduced the number of VMH neurons at E12.5 and E15.5, particularly within the VMH-central (VMHC) and -dorsomedial (VMHDM) subdomains, and resulted in a VMH cell fate change from glutamatergic to GABAergic. We observed a loss of Neurog3 expression in Ascl1-/- hypothalamic progenitors and an upregulation of Neurog3 when Ascl1 was overexpressed. We also demonstrated a glutamatergic to GABAergic fate switch in Neurog3- null mutant mice, suggesting that Ascl1 might act via Neurog3 to drive VMH cell fate decisions. We also showed a concomitant increase in expression of the central GABAergic fate determinant Dlx1/2 in the Ascl1-null hypothalamus. However, Ascl1 was not sufficient to induce an ectopic VMH fate when overexpressed outside the normal window of competency. Combined, Ascl1 is required but not sufficient to specify the neurotransmitter identity of VMH neurons, acting in a transcriptional cascade with Neurog3. [ABSTRACT FROM AUTHOR]

Published

2020

9. Single-Cell Gene Expression Analysis of a Human ESC Model of Pancreatic Endocrine Development Reveals Different Paths to β-Cell Differentiation

Author

Maja Borup Kjær Petersen, Ajuna Azad, Camilla Ingvorsen, Katja Hess, Mattias Hansson, Anne Grapin-Botton, and Christian Honoré

Subjects

endocrine, pancreas, progenitor, differentiation, hormone, lineage, NEUROG3, pluripotent stem cells, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

The production of insulin-producing β cells from human embryonic stem cells (hESCs) in vitro represents a promising strategy for a cell-based therapy for type 1 diabetes mellitus. To explore the cellular heterogeneity and temporal progression of endocrine progenitors and their progeny, we performed single-cell qPCR on more than 500 cells across several stages of in vitro differentiation of hESCs and compared them with human islets. We reveal distinct subpopulations along the endocrine differentiation path and an early lineage bifurcation toward either polyhormonal cells or β-like cells. We uncover several similarities and differences with mouse development and reveal that cells can take multiple paths to the same differentiation state, a principle that could be relevant to other systems. Notably, activation of the key β-cell transcription factor NKX6.1 can be initiated before or after endocrine commitment. The single-cell temporal resolution we provide can be used to improve the production of functional β cells.

Published

2017

10. Rfx6 promotes the differentiation of peptide-secreting enteroendocrine cells while repressing genetic programs controlling serotonin production.

Author

Piccand, Julie, Vagne, Constance, Blot, Florence, Meunier, Aline, Beucher, Anthony, Strasser, Perrine, Lund, Mari L., Ghimire, Sabitri, Nivlet, Laure, Lapp, Céline, Petersen, Natalia, Engelstoft, Maja S., Thibault-Carpentier, Christelle, Keime, Céline, Correa, Sara Jimenez, Schreiber, Valérie, Molina, Nacho, Schwartz, Thue W., De Arcangelis, Adèle, and Gradwohl, Gérard

Abstract

Enteroendocrine cells (EECs) of the gastro-intestinal tract sense gut luminal factors and release peptide hormones or serotonin (5-HT) to coordinate energy uptake and storage. Our goal is to decipher the gene regulatory networks controlling EECs specification from enteroendocrine progenitors. In this context, we studied the role of the transcription factor Rfx6 which had been identified as the cause of Mitchell–Riley syndrome, characterized by neonatal diabetes and congenital malabsorptive diarrhea. We previously reported that Rfx6 was essential for pancreatic beta cell development and function; however, the role of Rfx6 in EECs differentiation remained to be elucidated. We examined the molecular, cellular, and metabolic consequences of constitutive and conditional deletion of Rfx6 in the embryonic and adult mouse intestine. We performed single cell and bulk RNA-Seq to characterize EECs diversity and identify Rfx6-regulated genes. Rfx6 is expressed in the gut endoderm; later, it is turned on in, and restricted to, enteroendocrine progenitors and persists in hormone-positive EECs. In the embryonic intestine, the constitutive lack of Rfx6 leads to gastric heterotopia, suggesting a role in the maintenance of intestinal identity. In the absence of intestinal Rfx6, EECs differentiation is severely impaired both in the embryo and adult. However, the number of serotonin-producing enterochromaffin cells and mucosal 5-HT content are increased. Concomitantly, Neurog3-positive enteroendocrine progenitors accumulate. Combined analysis of single-cell and bulk RNA-Seq data revealed that enteroendocrine progenitors differentiate in two main cell trajectories, the enterochromaffin (EC) cells and the Peptidergic Enteroendocrine (PE) cells, the differentiation programs of which are differentially regulated by Rfx6. Rfx6 operates upstream of Arx , Pax6 and Isl1 to trigger the differentiation of peptidergic EECs such as GIP-, GLP-1-, or CCK-secreting cells. On the contrary, Rfx6 represses Lmx1a and Tph1 , two genes essential for serotonin biosynthesis. Finally, we identified transcriptional changes uncovering adaptive responses to the prolonged lack of enteroendocrine hormones and leading to malabsorption and lower food efficiency ratio in Rfx6-deficient mouse intestine. These studies identify Rfx6 as an essential transcriptional regulator of EECs specification and shed light on the molecular mechanisms of intestinal failures in human RFX6-deficiencies such as Mitchell–Riley syndrome. • The lack of Rfx6 impairs the differentiation of peptide-producing enteroendocrine cells. • The number of 5-HT-expressing-cells is increased in Rfx6-deficient intestine. • Intestinal inactivation of Rfx6 leads to lipid malabsorption and decreased food efficiency. [ABSTRACT FROM AUTHOR]

Published

2019

11. A transcriptomic roadmap to alpha- and beta cell differentiation in the embryonic pancreas.

Author

van Gurp, Léon, Muraro, Mauro J., Dielen, Tim, Seneby, Lina, Dharmadhikari, Gitanjali, Gradwohl, Gerard, van Oudenaarden, Alexander, and de Koning, Eelco J. P.

Subjects

*PANCREATIC beta cells, *CELL differentiation, *PANCREAS, *EMBRYOLOGY, *GENETIC regulation, *DEVELOPMENTAL programs

Abstract

During pancreatic development, endocrine cells appear from the pancreatic epithelium when Neurog3 positive cells delaminate and differentiate into alpha, beta, gamma and delta cells. The mechanisms involved in this process are still incompletely understood. We characterized the temporal, lineage-specific developmental programs during pancreatic development by sequencing the transcriptome of thousands of individual pancreatic cells from embryonic day E12.5 to E18.5 in mice, and identified all known cell types that are present in the embryonic pancreas, but focused specifically on alpha and beta cell differentiation by enrichment of a MIP-GFP reporter. We characterized transcriptomic heterogeneity in the tip domain based on proliferation, and characterized two endocrine precursor clusters marked by expression of Neurog3 and Fev. Pseudotime analysis revealed specific branches for developing alpha- and beta cells, which allowed identification of specific gene regulation patterns. These include some known and many previously unreported genes that appear to define pancreatic cell fate transitions. This resource allows dynamic profiling of embryonic pancreas development at single cell resolution and reveals novel gene signatures during pancreatic differentiation into alpha and beta cells. [ABSTRACT FROM AUTHOR]

Published

2019

12. Kateter Enfeksiyonlarına Alternatif Çözüm: Kilit Tedavisi.

Author

Kardaş, Ayşenur, Dalgıç, Nazan, Güller, Dilek, İlgar, Sibel Değim, Bayraktar, Banu, and Tabakçı, Ömer Naci

Subjects

*SHORT bowel syndrome, *AMPHOTERICIN B, *MALABSORPTION syndromes, *PARENTERAL therapy, *CONGENITAL disorders, *CATHETER-related infections

Abstract

One of the main complications of long-term use of permanent catheters is infection of the catheter. Guidelines issued by the Infectious Diaseases Society of America (IDSA) recommend the additon of antibiotic lock therapy to parenteral antibiotic therapy for tunneled or implantable catheter-associated infections caused by coagulase-negative Staphylococcus, S aureus, and gram-negative rods when removal of the catheter is not an option. However, IDSA guidelines strongly recommend removal of the catheter if possible in patients with catheter-associated infections secondary to Candida. However, Candida-associated catheter infections are common in certain high-risk patient groups including those with short bowel syndrome and congenital diarrheal disorders. Such situationsmay necessitate frequent ghange of catheters along with a host of other complications, resulting in huge loss of revenue to hospitals as well as inconvenience to patients. Here, we present a case in which C. glabrata-associated catheter infection was successfully treated by applying liposomal amphotericin B lock along with systemic antifungal treatment. The patient was a young girl aged 2 years and 9 months having Neurogenin-3 (NEUROG3) gene defect associated with congenital intestinal malabsorption syndrome. [ABSTRACT FROM AUTHOR]

Published

2020

13. Immunohistochemical characterization of pancreatic duodenal homeobox protein-1, neurogenin-3, and insulin protein expressions in islet-mesenchymal cell in vitro: a morphochronological evaluation.

Author

Manda, Juziel K. and Tchokonte-Nana, Venant

Subjects

*HOMEOBOX proteins, *IMMUNOHISTOCHEMISTRY, *PROTEIN expression, *MESENCHYMAL stem cells, *ISLANDS of Langerhans

Abstract

Objective(s): The use of a co-culture of islets with mesenchymal stromal cells (MSCs) is a promising therapy in islet transplantation to revert hyperglycaemia, but the resulting insulin-producing cells (IPCs) express low levels of pancreas endocrine developmental genes. This study aims to investigate the morphochronology of a co-culture of islets with MSCs from injured adult pancreata, and characterize pancreatic duodenal homeobox protein-1 (Pdx1), neurogenin-3 (Ngn3) and insulin protein expressions to establish the fate of their interaction. Materials and Methods: Islets and MSCs were isolated from sham operated control (SOC) and ductligated (PPDL) pancreata. Islets from SOC or PPDL tissues were cultured with or without MSCs in RPMI1640, supplemented by 1% Penicillin-Streptomycin, and maintained at 37 °C±1 °C at 95% relative humidity and 95%/5% air/CO2. Pdx1, Ngn3 and insulin expressions were determined by immunohistochemistry and islet morphochronological changes were assessed. Results: Pdx1 was expressed in all islet-cell cultures with or without MSCs. Pdx1+ islet cells were significantly increased in the presence of MSCs compared to the islet culture without MSCs. Similarly, Ngn3 was highly expressed in all cultures with MSCs from both SOC and PPDL tissues and the expression was prolonged in cultures using PPDL tissues before it was down-regulated, thereby, extending the period of Ngn3+ cell expansion and differentiation into mature functional islets. Conclusion: In vitro, MSCs maintain a pool of Ngn3+ that contributes to insulin production from mature beta cells but the activation of insulin production from non-beta cells may not be induced by direct signals from MSCs. [ABSTRACT FROM AUTHOR]

Published

2018

14. A novel NEUROG3 mutation in neonatal diabetes associated with a neuro‐intestinal syndrome.

Author

Hancili, Suna, Bonnefond, Amélie, Philippe, Julien, Vaillant, Emmanuel, De Graeve, Franck, Sand, Olivier, Busiah, Kanetee, Robert, Jean‐Jacques, Polak, Michel, Froguel, Philippe, Güven, Ayla, and Vaxillaire, Martine

Subjects

*GENETICS of diabetes, *INTESTINAL diseases, *GENES, *GENETIC mutation, *TRANSCRIPTION factors, *SEQUENCE analysis, *CHILDREN, *GENETICS

Abstract

Neonatal diabetes mellitus (NDM) is a rare form of non‐autoimmune diabetes usually diagnosed in the first 6 months of life. Various genetic defects have been shown to cause NDM with diverse clinical presentations and variable severity. Among transcriptional factor genes associated with isolated or syndromic NDM, a few cases of homozygous mutations in the NEUROG3 gene have been reported, all mutated patients presenting with congenital malabsorptive diarrhea with or without diabetes at a variable age of onset from early life to childhood. Through a targeted next‐generation sequencing assay for monogenic diabetes genes, we aimed to search for pathogenic deleterious mutation in a Turkish patient with NDM, severe malabsorptive diarrhea, neurointestinal dysplasia and other atypical features. In this patient, we identified a novel homozygous nonsense mutation (p.Q4*) in NEUROG3. The same biallelic mutation was found in another affected family member. Of note, the study proband presents with abnormalities of the intrahepatic biliary tract, thyroid gland and central nervous system, which has never been reported before in NEUROG3 mutation carriers. Our findings extend the usually described clinical features associated with NEUROG3 deficiency in humans, and question the extent to which a complete lack of NEUROG3 expression may affect pancreas endocrine function in humans. [ABSTRACT FROM AUTHOR]

Published

2018

15. Pancreas agenesis mutations disrupt a lead enhancer controlling a developmental enhancer cluster

Author

Irene Miguel-Escalada, Miguel Ángel Maestro, Diego Balboa, Anamaria Elek, Aina Bernal, Edgar Bernardo, Vanessa Grau, Javier García-Hurtado, Arnau Sebé-Pedrós, Jorge Ferrer, Wellcome Trust, Imperial College Healthcare NHS Trust- BRC Funding, and Medical Research Council (MRC)

Subjects

non-coding mutations, Regulatory Sequences, Nucleic Acid, General Biochemistry, Genetics and Molecular Biology, Mice, NEUROG3, Animals, Humans, stem cell differentiation, Molecular Biology, Pancreas, 11 Medical and Health Sciences, Infant, Newborn, Gene Expression Regulation, Developmental, Cell Differentiation, Cell Biology, 06 Biological Sciences, endocrine differentiation, Enhancer Elements, Genetic, PTF1A, diabetes mellitus, Mutation, enhancers, Mendelian disease, pancreas development, Transcription Factors, Developmental Biology

Abstract

Sequence variants in cis-acting enhancers are important for polygenic disease, but their role in Mendelian disease is poorly understood. Redundancy between enhancers that regulate the same gene is thought to mitigate the pathogenic impact of enhancer mutations. Recent findings, however, have shown that loss-of-function mutations in a single enhancer near PTF1A cause pancreas agenesis and neonatal diabetes. Using mouse and human genetic models, we show that this enhancer activates an entire PTF1A enhancer cluster in early pancreatic multipotent progenitors. This leading role, therefore, precludes functional redundancy. We further demonstrate that transient expression of PTF1A in multipotent progenitors sets in motion an epigenetic cascade that is required for duct and endocrine differentiation. These findings shed insights into the genome regulatory mechanisms that drive pancreas differentiation. Furthermore, they reveal an enhancer that acts as a regulatory master key and is thus vulnerable to pathogenic loss-of-function mutations. This research was supported by Ministerio de Ciencia e Innovación (BFU2014-54284-R, RTI2018-095666-B-I00), Medical Research Council (MR/L02036X/1), a Wellcome Trust Senior Investigator Award (WT101033), European Research Council Advanced Grant (789055), and CIBERDEM-Instituto de Salud Carlos III. Research in A.S.-P. group was supported by the European Research Council (ERC) under the European Union’s Horizon 2020 Research and Innovation Programme Grant Agreement (851647).

Published

2022

16. Single-cell transcriptome and accessible chromatin dynamics during endocrine pancreas development

Author

Eliza Duvall, Cecil M. Benitez, Krissie Tellez, Martin Enge, Philip T. Pauerstein, Lingyu Li, Songjoon Baek, Stephen R. Quake, Jason P. Smith, Nathan C. Sheffield, Seung K. Kim, and H. Efsun Arda

Subjects

1.1 Normal biological development and functioning, Neurog3, Nerve Tissue Proteins, Pancreatic Cancer, Islets of Langerhans, Mice, Rare Diseases, Underpinning research, scRNA-seq, Genetics, Basic Helix-Loop-Helix Transcription Factors, Animals, Developmental, Cell Lineage, pancreas, Metabolic and endocrine, Cancer, Multidisciplinary, Diabetes, Human Genome, Gene Expression Regulation, Developmental, Cell Differentiation, ATAC-seq, Stem Cell Research, Chromatin, Orphan Drug, Gene Expression Regulation, Stem Cell Research - Nonembryonic - Non-Human, Generic health relevance, Single-Cell Analysis, Digestive Diseases, Transcriptome, Biotechnology

Abstract

Delineating gene regulatory networks that orchestrate cell-type specification is an ongoing challenge for developmental biology studies. Single-cell analyses offer opportunities to address these challenges and accelerate discovery of rare cell lineage relationships and mechanisms underlying hierarchical lineage decisions. Here, we describe the molecular analysis of pancreatic endocrine cell differentiation using single-cell gene expression, chromatin accessibility assays coupled to genetic labeling and cell sorting. We uncover transcription factor networks that delineate β-, α- and δ-cell lineages. Through genomic footprint analysis we identify transcription factor-regulatory DNA interactions governing pancreatic cell development at unprecedented resolution. Our analysis suggests that the transcription factor Neurog3 may act as a pioneer transcription factor to specify the pancreatic endocrine lineage. These findings could improve protocols to generate replacement endocrine cells from renewable sources, like stem cells, for diabetes therapy.

Published

2022

17. Modeling coexistence of oscillation and Delta/Notch-mediated lateral inhibition in pancreas development and neurogenesis.

Author

Tiedemann, Hendrik B., Schneltzer, Elida, Beckers, Johannes, Przemeck, Gerhard K.H., and Hrabě de Angelis, Martin

Subjects

*PANCREAS development, *DEVELOPMENTAL neurobiology, *GENE regulatory networks, *NOTCH signaling pathway, *OSCILLATIONS

Abstract

During pancreas development, Neurog3 positive endocrine progenitors are specified by Delta/Notch (D/N) mediated lateral inhibition in the growing ducts. During neurogenesis, genes that determine the transition from the proneural state to neuronal or glial lineages are oscillating before their expression is sustained. Although the basic gene regulatory network is very similar, cycling gene expression in pancreatic development was not investigated yet, and previous simulations of lateral inhibition in pancreas development excluded by design the possibility of oscillations. To explore this possibility, we developed a dynamic model of a growing duct that results in an oscillatory phase before the determination of endocrine progenitors by lateral inhibition. The basic network (D/N + Hes1 + Neurog3) shows scattered, stable Neurog3 expression after displaying transient expression. Furthermore, we included the Hes1 negative feedback as previously discussed in neurogenesis and show the consequences for Neurog3 expression in pancreatic duct development. Interestingly, a weakened HES1 action on the Hes1 promoter allows the coexistence of stable patterning and oscillations. In conclusion, cycling gene expression and lateral inhibition are not mutually exclusive. In this way, we argue for a unified mode of D/N mediated lateral inhibition in neurogenic and pancreatic progenitor specification. [ABSTRACT FROM AUTHOR]

Published

2017

18. An Activating STAT3 Mutation Causes Neonatal Diabetes through Premature Induction of Pancreatic Differentiation.

Author

Saarimäki-Vire, Jonna, Balboa, Diego, Russell, Mark A., Saarikettu, Juha, Kinnunen, Matias, Keskitalo, Salla, Malhi, Amrinder, Valensisi, Cristina, Andrus, Colin, Eurola, Solja, Grym, Heli, Ustinov, Jarkko, Wartiovaara, Kirmo, Hawkins, R. David, Silvennoinen, Olli, Varjosalo, Markku, Morgan, Noel G., and Otonkoski, Timo

Abstract

Summary Activating germline mutations in STAT3 were recently identified as a cause of neonatal diabetes mellitus associated with beta-cell autoimmunity. We have investigated the effect of an activating mutation, STAT3 K392R , on pancreatic development using induced pluripotent stem cells (iPSCs) derived from a patient with neonatal diabetes and pancreatic hypoplasia. Early pancreatic endoderm differentiated similarly from STAT3 K392R and healthy-control cells, but in later stages, NEUROG3 expression was upregulated prematurely in STAT3 K392R cells together with insulin (INS) and glucagon (GCG). RNA sequencing (RNA-seq) showed robust NEUROG3 downstream targets upregulation. STAT3 mutation correction with CRISPR/Cas9 reversed completely the disease phenotype. STAT3 K392R -activating properties were not explained fully by altered DNA-binding affinity or increased phosphorylation. Instead, reporter assays demonstrated NEUROG3 promoter activation by STAT3 in pancreatic cells. Furthermore, proteomic and immunocytochemical analyses revealed increased nuclear translocation of STAT3 K392R . Collectively, our results demonstrate that the STAT3 K392R mutation causes premature endocrine differentiation through direct induction of NEUROG3 expression. [ABSTRACT FROM AUTHOR]

Published

2017

19. Évaluation de la morbi-mortalité des enfants et adolescents porteurs d'une entéropathie d'origine génétique nécessitant une nutrition parentérale au long cours en France

Author

Gostinicchi, Marion, Brunet, Valentine, Aix-Marseille Université - École de médecine (AMU SMPM MED), Aix-Marseille Université - Faculté des sciences médicales et paramédicales (AMU SMPM), Aix Marseille Université (AMU)-Aix Marseille Université (AMU), and Alexandre Fabre

Subjects

RFX6, EPCAM, [SDV]Life Sciences [q-bio], PCSK1, Atrésie intestinale multiple, SPINT2, TTC37, Syndrome oto-ostéo-hépato-entérique, Syndrome tricho-hépato-entérique, TTC7A, UNC45A, MYO5B, Atrophie micro- villositaire, STXBP2, SKIV2L, Entéro-endocriniennes, NEUROG3, Diarrhées, Entéropathie congénitale, Dysplasies épithéliales, Nutrition parentérale, Transplantation intestinale, STX3, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology

Abstract

Introduction : le groupe des entéropathies congénitales est un ensemble hétérogène de pathologies rares liées à une anomalie des entérocytes. Parmi les pathologies liées à une anomalie du trafic et de la polarité épithéliale, on compte plusieurs sous-groupes de pathologies. Peu de données épidémiologiques et d'évolution sont disponibles dans la littérature. Dans une première étude rétrospective regroupant revue de la littérature, case-reports et séries publiées, Caralli et al. ont étudié les données de 323 patients entre 2003 et 2012, les effectifs étaient échelonnés de 4 patients porteurs d’une mutation de STX3 à 105 patients porteurs d’une mutation de EPCAM. Cette étude a mis en évidence une mortalité de 20,3%, à un âge médian de 13,5 mois. Le décès survenait dans 40% des cas au décours d’une infection. Le recours à la nutrition parentérale était nécessaire dans 95,4% des cas, un sevrage était possible dans 29.4 % des cas à un âge médian de 23 mois. En dépit d’un nombre total de sujets conséquent pour des pathologies rares, cette étude comportait de nombreuses limites en partie liées au nombre important de données manquantes (absence de suivi régulier, prises en charge différentes selon les pays.). Une nouvelle étude est donc nécessaire pour compléter et vérifier ces résultats. Cette étude propose d’évaluer la morbi-mortalité des patients nés après 2005 pris en charge pour une entéropathie congénitale dans chacun de ces centres. Matériel et Méthodes : cette étude rétrospective et multicentrique recense les patients pris en charge dans les centres de maladies rares digestives, et centres de nutrition parentérale. Pour chaque centre, les patients nés après le 1er janvier 2005 et présentant une entéropathie congénitale due à une mutation d’un des gènes suivants ont été inclus et répartis en 2 groupes selon la classification de THIAGARAJAH et al. : les pathologies du transport et de la polarité épithéliale : mutations des gènes EPCAM, SPINT2, MYO5B, STX3, STXBP2, TTC37, SKIV2L, TTC7A, UNC45A et les pathologies entéro-endocriniennes : mutations des gènes PCSK1, NEUROG3, ARX, RFX6. Résultats : 79 patients ont été inclus. 70 patients (88,6%) présentaient une maladie du transport et de la polarité épithéliale et 9 patients (11,4%) présentaient une pathologie entéro-endocrinienne. Il y avait 47 patients (59,5%) qui présentaient au moins une anomalie anténatale. Il y avait 77 patients (97,5%) qui ont eu recours à une nutrition parentérale au long cours. Le nombre moyen d’infection était de 0,64 infections (±0,41) par an, soit 1,75 infections (±1,22) pour 1000 jours. Le nombre moyen d’infections après mise en place du Taurolock® était de 0,55 infections (±1,04) par an contre 0,93 infections (±1,34) par an avant la mise en place (p=0,001). 6 patients (7,6%) ont bénéficié d’une transplantation intestinale. 5 décès (6,3%) sont survenus au cours du suivi. Conclusion : cette étude présente les données d’évolution de morbi-mortalité de 79 patients atteints de 11 pathologies différentes. Nous notons une amélioration de la survie par rapport aux données rapportées dans la littérature. Cependant, la croissance de ces enfants n’est pas suffisante en dépit de la nutrition parentérale, et peut amener à remettre en question certains éléments de la prise en charge au long cours.

Published

2021

20. Matters arising: Insufficient evidence that pancreatic β cells are derived from adult ductal Neurog3-expressing progenitors.

Author

Magenheim J, Maestro MA, Sharon N, Herrera PL, Murtaugh LC, Kopp J, Sander M, Gu G, Melton DA, Ferrer J, and Dor Y

Subjects

Evidence Gaps, Cell Differentiation, Pancreas physiology, Pancreatic Ducts, Insulin, Somatostatin, Insulin-Secreting Cells

Abstract

Understanding the origin of pancreatic β cells has profound implications for regenerative therapies in diabetes. For over a century, it was widely held that adult pancreatic duct cells act as endocrine progenitors, but lineage-tracing experiments challenged this dogma. Gribben et al. recently used two existing lineage-tracing models and single-cell RNA sequencing to conclude that adult pancreatic ducts contain endocrine progenitors that differentiate to insulin-expressing β cells at a physiologically important rate. We now offer an alternative interpretation of these experiments. Our data indicate that the two Cre lines that were used directly label adult islet somatostatin-producing ∂ cells, which precludes their use to assess whether β cells originate from duct cells. Furthermore, many labeled ∂ cells, which have an elongated neuron-like shape, were likely misclassified as β cells because insulin-somatostatin coimmunolocalizations were not used. We conclude that most evidence so far indicates that endocrine and exocrine lineage borders are rarely crossed in the adult pancreas., Competing Interests: Declaration of interests D.A.M. serves on the advisory board for Cell Stem Cell., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2023

21. Uncovering the mechanisms of beta-cell neogenesis and maturation toward development of a regenerative therapy for diabetes.

Author

Miyatsuka, Takeshi

Abstract

Knowledge of the pathways involved in islet cell differentiation has been exploited to develop new methods for generating beta cells from non-beta cells, such as embryonic stem cells and pancreatic acinar cells, which should lead to the development of future cell therapies for the cure of diabetes. However, these methods do not enable insulin-producing cells to complete their final maturation to fully functional beta cells that are capable of producing high levels of insulin and of responding to normal physiological signals. This obstacle arises from our lack of a complete understanding of how the pancreas is formed and how beta cells differentiate from their precursors during development. Here I review the recent progress in our understanding of the molecular mechanisms controlling beta-cell neogenesis and maturation. [ABSTRACT FROM AUTHOR]

Published

2015

22. Extensive NEUROG3 occupancy in the human pancreatic endocrine gene regulatory network

Author

Schreiber, Valérie, Mercier, Reuben, Jiménez, Sara, Ye, Tao, García-Sánchez, Emmanuel, Klein, Annabelle, Meunier, Aline, Ghimire, Sabitri, Birck, Catherine, Jost, Bernard, de Lichtenberg, Kristian Honnens, Honoré, Christian, Serup, Palle, Gradwohl, Gérard, Schreiber, Valérie, Mercier, Reuben, Jiménez, Sara, Ye, Tao, García-Sánchez, Emmanuel, Klein, Annabelle, Meunier, Aline, Ghimire, Sabitri, Birck, Catherine, Jost, Bernard, de Lichtenberg, Kristian Honnens, Honoré, Christian, Serup, Palle, and Gradwohl, Gérard

Abstract

Objective: Mice lacking the bHLH transcription factor (TF) Neurog3 do not form pancreatic islet cells, including insulin-secreting beta cells, the absence of which leads to diabetes. In humans, homozygous mutations of NEUROG3 manifest with neonatal or childhood diabetes. Despite this critical role in islet cell development, the precise function of and downstream genetic programs regulated directly by NEUROG3 remain elusive. Therefore, we mapped genome-wide NEUROG3 occupancy in human induced pluripotent stem cell (hiPSC)–derived endocrine progenitors and determined NEUROG3 dependency of associated genes to uncover direct targets. Methods: We generated a novel hiPSC line (NEUROG3-HA-P2A-Venus) where NEUROG3 is HA-tagged and fused to a self-cleaving fluorescent VENUS reporter. We used the CUT&RUN technique to map NEUROG3 occupancy and epigenetic marks in pancreatic endocrine progenitors (PEP) that were differentiated from this hiPSC line. We integrated NEUROG3 occupancy data with chromatin status and gene expression in PEPs as well as their NEUROG3-dependence. In addition, we investigated whether NEUROG3 binds type 2 diabetes mellitus (T2DM)–associated variants at the PEP stage. Results: CUT&RUN revealed a total of 863 NEUROG3 binding sites assigned to 1263 unique genes. NEUROG3 occupancy was found at promoters as well as at distant cis-regulatory elements that frequently overlapped within PEP active enhancers. De novo motif analyses defined a NEUROG3 consensus binding motif and suggested potential co-regulation of NEUROG3 target genes by FOXA or RFX transcription factors. We found that 22% of the genes downregulated in NEUROG3−/− PEPs, and 10% of genes enriched in NEUROG3-Venus positive endocrine cells were bound by NEUROG3 and thus likely to be directly regulated. NEUROG3 binds to 138 transcription factor genes, some with important roles in islet cell development or function, such as NEUROD1, PAX4, NKX2-2, SOX4, MLXIPL, LMX1B, RFX3, and NEUROG3

Published

2021

23. Gene Signatures of NEUROGENIN3+ Endocrine Progenitor Cells in the Human Pancreas

Author

Chengyang Liu, Wei Wang, Jerome Irianto, Hyo Jeong Yong, Ali Naji, Yue J. Wang, and Gengqiang Xie

Subjects

endocrine system, epsilon cells, Endocrinology, Diabetes and Metabolism, Nerve Tissue Proteins, Biology, Diseases of the endocrine glands. Clinical endocrinology, Endocrinology, NEUROG3, medicine, Basic Helix-Loop-Helix Transcription Factors, Endocrine system, Humans, Gene Regulatory Networks, Progenitor cell, Transcription factor, data integration, Pancreas, Original Research, single-cell RNA-seq, Regeneration (biology), Stem Cells, Gene Expression Regulation, Developmental, Cell Differentiation, endocrine progenitor, RC648-665, Cell biology, medicine.anatomical_structure, human pancreas, Homeobox, Beta cell, Endocrine Cells, Immunostaining

Abstract

NEUROGENIN3+ (NEUROG3+) cells are considered to be pancreatic endocrine progenitors. Our current knowledge on the molecular program of NEUROG3+ cells in humans is largely extrapolated from studies in mice. We hypothesized that single-cell RNA-seq enables in-depth exploration of the rare NEUROG3+ cells directly in humans. We aligned four large single-cell RNA-seq datasets from postnatal human pancreas. Our integrated analysis revealed 10 NEUROG3+ epithelial cells from a total of 11,174 pancreatic cells. Noticeably, human NEUROG3+ cells clustered with mature pancreatic cells and epsilon cells displayed the highest frequency of NEUROG3 positivity. We confirmed the co-expression of NEUROG3 with endocrine markers and the high percentage of NEUROG3+ cells among epsilon cells at the protein level based on immunostaining on pancreatic tissue sections. We further identified unique genetic signatures of the NEUROG3+ cells. Regulatory network inference revealed novel transcription factors including Prospero homeobox protein 1 (PROX1) may act jointly with NEUROG3. As NEUROG3 plays a central role in endocrine differentiation, knowledge gained from our study will accelerate the development of beta cell regeneration therapies to treat diabetes.

Published

2021

24. Pancreas agenesis mutations disrupt a lead enhancer controlling a developmental enhancer cluster.

Author

Miguel-Escalada, Irene, Maestro, Miguel Ángel, Balboa, Diego, Elek, Anamaria, Bernal, Aina, Bernardo, Edgar, Grau, Vanessa, García-Hurtado, Javier, Sebé-Pedrós, Arnau, and Ferrer, Jorge

Subjects

*PANCREAS, *GENETIC models, *CIS-regulatory elements (Genetics), *EPIGENETICS, *GENETIC mutation

Abstract

Sequence variants in cis -acting enhancers are important for polygenic disease, but their role in Mendelian disease is poorly understood. Redundancy between enhancers that regulate the same gene is thought to mitigate the pathogenic impact of enhancer mutations. Recent findings, however, have shown that loss-of-function mutations in a single enhancer near PTF1A cause pancreas agenesis and neonatal diabetes. Using mouse and human genetic models, we show that this enhancer activates an entire PTF1A enhancer cluster in early pancreatic multipotent progenitors. This leading role, therefore, precludes functional redundancy. We further demonstrate that transient expression of PTF1A in multipotent progenitors sets in motion an epigenetic cascade that is required for duct and endocrine differentiation. These findings shed insights into the genome regulatory mechanisms that drive pancreas differentiation. Furthermore, they reveal an enhancer that acts as a regulatory master key and is thus vulnerable to pathogenic loss-of-function mutations. [Display omitted] • The pancreas agenesis enhancer (EnhP) activates PTF1A in early pancreatic progenitors • EnhP also activates other progenitor PTF1A enhancers • This master key function explains why EnhP is vulnerable to loss-of-function mutations • Transient PTF1A expression in progenitors controls pancreas growth and endocrinogenesis Miguel-Escalada et al. show that pancreas agenesis mutations disrupt a lead enhancer that activates other PTF1A enhancers in early progenitors of the embryonic pancreas. This enables transient PTF1A expression in progenitors, which controls pancreas growth and creates epigenetic competence for subsequent endocrine differentiation. [ABSTRACT FROM AUTHOR]

Published

2022

25. New ideas connecting the cell cycle and pancreatic endocrine-lineage specification.

Author

Bechard, Matthew E. and Wright, Christopher V. E.

Published

2017

26. Sequential introduction and dosage balance of defined transcription factors affect reprogramming efficiency from pancreatic duct cells into insulin-producing cells.

Author

Miyashita, Kazuyuki, Miyatsuka, Takeshi, Matsuoka, Taka-Aki, Sasaki, Shugo, Takebe, Satomi, Yasuda, Tetsuyuki, Watada, Hirotaka, Kaneto, Hideaki, and Shimomura, Iichiro

Subjects

*TRANSCRIPTION factors, *INSULIN, *PANCREATIC duct, *CELL lines, *GENE expression, *CYTOLOGY

Abstract

Highlights: [•] A cell line to evaluate the reprogramming efficiency to β-like cells was generated. [•] Expression of Pdx1 prior to Neurog3 and Mafa increased reprogramming efficiency. [•] A polycistronic vector expressing Pdx1, Neurog3 and Mafa increased reprogramming. [•] Excessive Mafa expression together with Pdx1 and Neurog3 suppressed reprogramming. [ABSTRACT FROM AUTHOR]

Published

2014

27. Transcription factors that shape the mammalian pancreas

Author

Willem Staels, Rachel E. Jennings, Raphael Scharfmann, Pediatrics, Pathology/molecular and cellular medicine, and Beta Cell Neogenesis

Subjects

Pluripotent Stem Cells, 0301 basic medicine, Genetically modified mouse, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Review, In Vitro Techniques, Biology, Cell Line, Regulatory factor X6, Mice, 03 medical and health sciences, 0302 clinical medicine, Directed differentiation, NEUROG3, Insulin-Secreting Cells, Diabetes Mellitus, Internal Medicine, medicine, Animals, Humans, Pediatrics, Perinatology, and Child Health, Pancreas and duodenal homeobox 1, Pancreas, development, Transcription factor, mouse, neurogenin 3, RFX6, Neonatal diabetes, Gene Expression Regulation, Developmental, Cell biology, Organoids, pdx1, 030104 developmental biology, medicine.anatomical_structure, PDX1, islets of Langerhans, Beta cell, Stem cell, Human, Transcription Factors

Abstract

Improving our understanding of mammalian pancreas development is crucial for the development of more effective cellular therapies for diabetes. Most of what we know about mammalian pancreas development stems from mouse genetics. We have learnt that a unique set of transcription factors controls endocrine and exocrine cell differentiation. Transgenic mouse models have been instrumental in studying the function of these transcription factors. Mouse and human pancreas development are very similar in many respects, but the devil is in the detail. To unravel human pancreas development in greater detail, in vitro cellular models (including directed differentiation of stem cells, human beta cell lines and human pancreatic organoids) are used; however, in vivo validation of these results is still needed. The current best ‘model’ for studying human pancreas development are individuals with monogenic forms of diabetes. In this review, we discuss mammalian pancreas development, highlight some discrepancies between mouse and human, and discuss selected transcription factors that, when mutated, cause permanent neonatal diabetes. Graphical abstract Electronic supplementary material The online version of this article (10.1007/s00125-020-05161-0) contains a slide of the figure for download, which is available to authorised users.

Published

2020

28. Ascl1 is required to specify a subset of ventromedial hypothalamic neurons

Author

Deborah M. Kurrasch, Shaghayegh Aslanpour, Florence Blot, Carol Schuurmans, Anjali Balakrishnan, Gerard Gradwohl, Jessica M. Rosin, Natalia Klenin, University of Calgary, Department of Biochemistry [University of Toronto], University of Toronto, Institut de Génétique et de Biologie Moléculaire et Cellulaire (IGBMC), Université de Strasbourg (UNISTRA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Institut National de la Santé et de la Recherche Médicale (INSERM), and Gradwohl, Gérard

Subjects

endocrine system, Neurog3, Cell fate determination, Biology, 03 medical and health sciences, chemistry.chemical_compound, Glutamatergic, 0302 clinical medicine, Downregulation and upregulation, [SDV.BDD] Life Sciences [q-bio]/Development Biology, Ascl1, Progenitor cell, Neurotransmitter, Molecular Biology, Cell fate decision, [SDV.BDD]Life Sciences [q-bio]/Development Biology, 030304 developmental biology, 0303 health sciences, Ventromedial hypothalamus, Cell biology, ASCL1, chemistry, Hypothalamus, Differentiation, GABAergic, 030217 neurology & neurosurgery, Developmental Biology

Abstract

International audience; Despite clear physiological roles, the ventromedial hypothalamus (VMH) developmental programs are poorly understood. Here, we asked whether the proneural gene, Achaete-scute homolog1 (Ascl1), contributes to VMH development. Ascl1 transcripts were detected in E10.5-P0 VMH neural progenitors. The elimination of Ascl1 reduced the number of VMH neurons at E12.5 and E15.5, particularly within the VMH-central (VMHC) and -dorsomedial (VMHDM) subdomains and resulted in a VMH cell fate change from glutamatergic to GABAergic. We observed a loss of Neurog3 expression in Ascl1−/− hypothalamic progenitors and an upregulation of Neurog3 when Ascl1 was overexpressed. We also demonstrated a glutamatergic to GABAergic fate switch in Neurog3-null mutant mice, suggesting that Ascl1 might act via Neurog3 to drive VMH cell fate decisions. We also showed a concomitant increase in the central GABAergic fate determinant Dlx1/2 expression in the Ascl1-null hypothalamus. However, Ascl1 was not sufficient to induce an ectopic VMH fate when overexpressed outside of the normal window of competency. Combined, Ascl1 is required but not sufficient to specify the neurotransmitter identity of VMH neurons, acting in a transcriptional cascade with Neurog3.

Published

2020

29. Ascl1b and Neurod1, instead of Neurog3, control pancreatic endocrine cell fate in zebrafish.

Author

Flasse, Lydie C., Pirson, Justine L., Stern, David G., Von Berg, Virginie, Manfroid, Isabelle, Peers, Bernard, and Voz, Marianne L.

Subjects

*PANCREAS, *ENDOCRINE glands, *CELL differentiation, *PANCREATIC secretions, *ZEBRA danio, *HYPOGLYCEMIC agents, *STEM cells

Abstract

Background: NEUROG3 is a key regulator of pancreatic endocrine cell differentiation in mouse, essential for the generation of all mature hormone producing cells. It is repressed by Notch signaling that prevents pancreatic cell differentiation by maintaining precursors in an undifferentiated state. Results: We show that, in zebrafish, neurog3 is not expressed in the pancreas and null neurog3 mutant embryos do not display any apparent endocrine defects. The control of endocrine cell fate is instead fulfilled by two basic helixloop- helix factors, Ascl1b and Neurod1, that are both repressed by Notch signaling. ascl1b is transiently expressed in the mid-trunk endoderm just after gastrulation and is required for the generation of the first pancreatic endocrine precursor cells. Neurod1 is expressed afterwards in the pancreatic anlagen and pursues the endocrine cell differentiation program initiated by Ascl1b. Their complementary role in endocrine differentiation of the dorsal bud is demonstrated by the loss of all hormone-secreting cells following their simultaneous inactivation. This defect is due to a blockage of the initiation of endocrine cell differentiation. Conclusions: This study demonstrates that NEUROG3 is not the unique pancreatic endocrine cell fate determinant in vertebrates. A general survey of endocrine cell fate determinants in the whole digestive system among vertebrates indicates that they all belong to the ARP/ASCL family but not necessarily to the Neurog3 subfamily. The identity of the ARP/ASCL factor involved depends not only on the organ but also on the species. One could, therefore, consider differentiating stem cells into insulin-producing cells without the involvement of NEUROG3 but via another ARP/ASCL factor. [ABSTRACT FROM AUTHOR]

Published

2013

30. Competence of failed endocrine progenitors to give rise to acinar but not ductal cells is restricted to early pancreas development

Author

Beucher, Anthony, Martín, Mercè, Spenle, Caroline, Poulet, Martine, Collin, Caitlin, and Gradwohl, Gérard

Subjects

*ENDOCRINE system, *PANCREAS development, *PANCREATIC acinar cells, *GENE expression, *CELL differentiation, *GENETIC carriers

Abstract

Abstract: During mouse pancreas development, the transient expression of Neurogenin3 (Neurog3) in uncommitted pancreas progenitors is required to determine endocrine destiny. However it has been reported that Neurog3-expressing cells can eventually adopt acinar or ductal fates and that Neurog3 levels were important to secure the islet destiny. It is not known whether the competence of Neurog3-induced cells to give rise to non-endocrine lineages is an intrinsic property of these progenitors or depends on pancreas developmental stage. Using temporal genetic labeling approaches we examined the dynamic of endocrine progenitor differentiation and explored the plasticity of Neurog3-induced cells throughout development. We found that Neurog3+ progenitors develop into hormone-expressing cells in a fast process taking less then 10h. Furthermore, fate-mapping studies in heterozygote (Neurog3CreERT/+) and Neurog3-deficient (Neurog3CreERT/CreERT) embryos revealed that Neurog3-induced cells have different potential over time. At the early bud stage, failed endocrine progenitors can adopt acinar or ductal fate, whereas later in the branching pancreas they do not contribute to the acinar lineage but Neurog3-deficient cells eventually differentiate into duct cells. Thus these results provide evidence that the plasticity of Neurog3-induced cells becomes restricted during development. Furthermore these data suggest that during the secondary transition, endocrine progenitor cells arise from bipotent precursors already committed to the duct/endocrine lineages and not from domain of cells having distinct potentialities. [Copyright &y& Elsevier]

Published

2012

31. Neonatal Diabetes: An Expanding List of Genes Allows for Improved Diagnosis and Treatment.

Author

Greeley, Siri, Naylor, Rochelle, Philipson, Louis, and Bell, Graeme

Abstract

There has been major progress in recent years uncovering the genetic causes of diabetes presenting in the first year of life. Twenty genes have been identified to date. The most common causes accounting for the majority of cases are mutations in the genes encoding the two subunits of the ATP-sensitive potassium channel (K), KCNJ11 and ABCC8, and the insulin gene ( INS), as well as abnormalities in chromosome 6q24. Patients with activating mutations in KCNJ11 and ABCC8 can be treated with oral sulfonylureas in lieu of insulin injections. This compelling example of personalized genetic medicine leading to improved glucose regulation and quality of life may-with continued research-be repeated for other forms of neonatal diabetes in the future. [ABSTRACT FROM AUTHOR]

Published

2011

32. The Krüppel-like zinc finger protein GLIS3 transactivates neurogenin 3 for proper fetal pancreatic islet differentiation in mice.

Author

Yang, Y., Chang, B., Yechoor, V., Chen, W., Li, L., Tsai, M.-J., and Chan, L.

Abstract

Aims/hypothesis: Mutations in GLIS3, which encodes a Krüppel-like zinc finger transcription factor, were found to underlie sporadic neonatal diabetes. Inactivation of Glis3 by gene targeting in mice was previously shown to lead to neonatal diabetes, but the underlying mechanism remains largely unknown. We aimed to elucidate the mechanism of action of GLIS family zinc finger 3 (GLIS3) in Glis3 mice and to further decipher its action in in-vitro systems. Methods: We created Glis3 mice and monitored the morphological and biochemical phenotype of their pancreatic islets at different stages of embryonic development. We combined these observations with experiments on Glis3 expressed in cultured cells, as well as in in vitro systems in the presence of other reconstituted components. Results: In vivo and in vitro analyses placed Glis3 upstream of Neurog3, the endocrine pancreas lineage-defining transcription factor. We found that GLIS3 binds to specific GLIS3-response elements in the Neurog3 promoter, activating Neurog3 gene transcription both directly, and synergistically with hepatic nuclear factor 6 and forkhead box A2. Conclusions/interpretation: These results indicate that GLIS3 controls fetal islet differentiation via direct transactivation of Neurog3, a perturbation that causes neonatal diabetes in mice. [ABSTRACT FROM AUTHOR]

Published

2011

33. Neurog3 gene dosage regulates allocation of endocrine and exocrine cell fates in the developing mouse pancreas

Author

Wang, Sui, Yan, Jingbo, Anderson, Daniel A., Xu, Yanwen, Kanal, Maneesh C., Cao, Zheng, Wright, Christopher V.E., and Gu, Guoqiang

Subjects

*LABORATORY mice, *PANCREATIC physiology, *HELIX-loop-helix motifs, *CELL differentiation, *ENDOCRINE glands, *EXOCRINE glands, *EMBRYOLOGY, *GENE expression

Abstract

Abstract: The basic helix–loop–helix transcription factor Neurog3 (Neurogenin3 or Ngn3) actively drives endodermal progenitor cells towards endocrine islet cell differentiation during embryogenesis. Here, we manipulate Neurog3 expression levels in endocrine progenitor cells without altering its expression pattern using heterozygosity and a hypomorph. Lowered Neurog3 gene dosage in the developing pancreatic epithelium reduces the overall production of endocrine islet cells without significantly affecting the proportions of various islet cell types that do form. A reduced Neurog3 production level in the endocrine-directed pancreatic progenitor population activates the expression of Neurog3 in an increased number of epithelial progenitors. Yet a significant number of these Neurog3+ cells detected in heterozygous and hypomorphic pancreata, possibly those that express low levels of Neurog3, move on to adopt pancreatic ductal or acinar fates. These data directly demonstrate that achieving high levels of Neurog3 expression is a critical step for endocrine commitment from multipotent pancreatic progenitors. These findings also suggest that a high level of Neurog3 expression could mediate lateral inhibition or other unknown feedback mechanisms to regulate the number of cells that initiate Neurog3 transcription and protein production. The control of Neurog3+ cell number and the Neurog3 threshold-dependent endocrine differentiation mechanism combine to select a specific proportion of pancreatic progenitor cells to adopt the islet cell fate. [Copyright &y& Elsevier]

Published

2010

34. Modeling coexistence of oscillation and Delta/Notch-mediated lateral inhibition in pancreas development and neurogenesis

Author

Elida Schneltzer, Johannes Beckers, Hendrik B. Tiedemann, Gerhard K. H. Przemeck, and Martin Hrabě de Angelis

Subjects

0301 basic medicine, Statistics and Probability, endocrine system, medicine.medical_specialty, Neurogenesis, Gene regulatory network, Endocrine System, Nerve Tissue Proteins, Biology, Models, Biological, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, Lateral inhibition, Oscillometry, Internal medicine, Gene expression, Basic Helix-Loop-Helix Transcription Factors, medicine, Animals, Cell Lineage, HES1, Pancreas, Body Patterning, Progenitor, Feedback, Physiological, Pancreatic duct, Receptors, Notch, General Immunology and Microbiology, Applied Mathematics, Gene Expression Regulation, Developmental, General Medicine, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Modeling and Simulation, Transcription Factor HES-1, General Agricultural and Biological Sciences, Neurog3, Pancreatogenesis, Cycling Gene Expression, Endocrine Progenitor, Simulation

Abstract

During pancreas development, Neurog3 positive endocrine progenitors are specified by Delta/Notch (D/N) mediated lateral inhibition in the growing ducts. During neurogenesis, genes that determine the transition from the proneural state to neuronal or glial lineages are oscillating before their expression is sustained. Although the basic gene regulatory network is very similar, cycling gene expression in pancreatic development was not investigated yet, and previous simulations of lateral inhibition in pancreas development excluded by design the possibility of oscillations. To explore this possibility, we developed a dynamic model of a growing duct that results in an oscillatory phase before the determination of endocrine progenitors by lateral inhibition. The basic network (D/N + Hes1 + Neurog3) shows scattered, stable Neurog3 expression after displaying transient expression. Furthermore, we included the Hes1 negative feedback as previously discussed in neurogenesis and show the consequences for Neurog3 expression in pancreatic duct development. Interestingly, a weakened HES1 action on the Hes1 promoter allows the coexistence of stable patterning and oscillations. In conclusion, cycling gene expression and lateral inhibition are not mutually exclusive. In this way, we argue for a unified mode of D/N mediated lateral inhibition in neurogenic and pancreatic progenitor specification.

Published

2017

35. Polymorphisms in the neurogenin 3 gene (NEUROG) and their relation to altered insulin secretion and diabetes in the Danish Caucasian population.

Author

Jensen, J. N., Hansen, L., Ekstrøm, C. T., Pociot, F., Nerup, J., Hansen, T., and Pedersen, O.

Subjects

TRANSCRIPTION factors, PROTEINS, TYPE 2 diabetes, DIABETES, CARBOHYDRATE intolerance, ENDOCRINE diseases, NUTRITION disorders

Abstract

Aim/hypothesis. Neurogenin 3 (NEUROG3) is a member of the subfamily of basic-helix-loop-helix (bHLH) transcription factors involved in differentiation of the endocrine pancreas and therefore a possible candidate gene for maturity-onset diabetes of the young (MODY) and Type II (non-insulin-dependent) diabetes mellitus.¶Methods. Using Polymerase-chain-reaction single-stranded-conformation polymorphism, we examined the coding region including the 5'-untranslated and 3'- untranslated regions of the NEUROG3 in a group of 133 diabetic patients comprising 19 MODY patients, 19 patients with dominant Type I diabetes, and 31 early-onset and 64 late-onset Type II diabetic patients.¶Results. We found two missense mutations, Gly167Arg and Ser199Phe, as well as two non-coding variants in the 5' UTR, a c → t nucleotide variant at position –10 upstream of the start codon in one MODY patient and a 2 base pair (CA) deletion polymorphism at position –44/-45. Allele frequencies measured in 377 diabetic patients and in 217 glucose-tolerant control subjects were: Gly167Arg, 0.04 (95 % CI: 0.02–0.06) and 0.04 (0.02–0.06); Ser199Phe, 0.31 (0.26–0.36) and 0.30 (0.24–0.36); –44–45delCA, 0.33 (0.31–0.35) and 0.35 (0.32–0.38), respectively. Both Ser199Phe and the –44–45delCA were in linkage disequilibrium (χ2 > 60) but the Ser199Phe and the –44–45delCA polymorphism were not associated with consistent changes in fasting- or glucose-induced insulin secretion in 249 glucose-tolerant offspring (first-degree relatives) of Type II diabetic parents or in 217 unrelated middle-aged glucose tolerant subjects.¶Conclusion/interpretation. Genetic variability in NEUROG3 is not associated with dominant Type I diabetes, MODY, Type II diabetes or changes in insulin secretion in the Danish Caucasians examined subjects. [Diabetologia (2001) 44: 123–126] [ABSTRACT FROM AUTHOR]

Published

2001

36. A transcriptomic roadmap to alpha- and beta cell differentiation in the embryonic pancreas

Author

Mauro J. Muraro, Lina Seneby, Gerard Gradwohl, Tim Dielen, Eelco J.P. de Koning, Léon van Gurp, Gitanjali Dharmadhikari, Alexander van Oudenaarden, Hubrecht Institute for Developmental Biology and Stem Cell Research, University Medical Center [Utrecht], Hubrecht Institute [Utrecht] (KNAW), Single Cell Discoveries [Utrecht], Institut de Génétique et de Biologie Moléculaire et Cellulaire (IGBMC), Université de Strasbourg (UNISTRA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Oncode Institute [Utrecht], Leiden University Medical Center (LUMC), and Gradwohl, Gérard

Subjects

Cell type, Organogenesis, [SDV]Life Sciences [q-bio], Cellular differentiation, Green Fluorescent Proteins, Nerve Tissue Proteins, Neurog3, Enteroendocrine cell, Cell Separation, Cell fate determination, Biology, Transcriptome, Mice, Single cell transcriptome sequencing, 03 medical and health sciences, 0302 clinical medicine, Insulin-Secreting Cells, [SDV.BDD] Life Sciences [q-bio]/Development Biology, Endocrine progenitors, Basic Helix-Loop-Helix Transcription Factors, medicine, Animals, Pancreas development, Cell Lineage, Pancreas, [SDV.BDD]Life Sciences [q-bio]/Development Biology, Molecular Biology, Gene Library, 030304 developmental biology, Regulation of gene expression, 0303 health sciences, Stem Cells, MESH: Alpha cells, Beta cells, Gene Expression Regulation, Developmental, Cell Differentiation, Flow Cytometry, Embryonic stem cell, Alpha cells, Cell biology, [SDV] Life Sciences [q-bio], medicine.anatomical_structure, Glucagon-Secreting Cells, 030217 neurology & neurosurgery, Transcription Factors, Developmental Biology

Abstract

During pancreatic development, endocrine cells appear from the pancreatic epithelium when Neurog3 positive cells delaminate and differentiate into alpha, beta, gamma and delta cells. The mechanisms involved in this process are still incompletely understood. We characterized the temporal, lineage-specific developmental programs during pancreatic development by sequencing the transcriptome of thousands of individual pancreatic cells from embryonic day E12.5 to E18.5 in mice, and identified all known cell types that are present in the embryonic pancreas, but focused specifically on alpha and beta cell differentiation by enrichment of a MIP-GFP reporter. We characterized transcriptomic heterogeneity in the tip domain based on proliferation, and characterized two endocrine precursor clusters marked by expression of Neurog3 and Fev. Pseudotime analysis revealed specific branches for developing alpha- and beta cells, which allowed identification of specific gene regulation patterns. These include some known and many previously unreported genes that appear to define pancreatic cell fate transitions. This resource allows dynamic profiling of embryonic pancreas development at single cell resolution and reveals novel gene signatures during pancreatic differentiation into alpha and beta cells.

Published

2019

37. Rfx6 promotes the differentiation of peptide-secreting enteroendocrine cells while repressing genetic programs controlling serotonin production

Author

Thue W. Schwartz, Julie Piccand, Adèle De Arcangelis, Nacho Molina, Mari L. Lund, Anthony Beucher, Sabitri Ghimire, Florence Blot, Valérie Schreiber, Sara Jimenez Correa, Christelle Thibault-Carpentier, Maja S. Engelstoft, Aline Meunier, Céline Lapp, Constance Vagne, Gérard Gradwohl, Perrine Strasser, Céline Keime, Laure Nivlet, Natalia Petersen, Institut de Génétique et de Biologie Moléculaire et Cellulaire (IGBMC), and Université de Strasbourg (UNISTRA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)

Subjects

0301 basic medicine, Male, [SDV]Life Sciences [q-bio], Enteroendocrine cell, Neurog3, Lmx1a, Mice, 0302 clinical medicine, Transcriptional regulation, Intestinal Mucosa, [SDV.BDD]Life Sciences [q-bio]/Development Biology, ComputingMilieux_MISCELLANEOUS, Mice, Knockout, Enteroendocrine cells, 0303 health sciences, Mitchell- Riley syndrome, Cell Differentiation, Cell biology, Intestine, Enterochromaffin cells, Enterochromaffin cell, Female, Original Article, Serotonin Production, Single-Cell Analysis, Mitchell–Riley syndrome, Diarrhea, lcsh:Internal medicine, Serotonin, Malabsorption, LIM-Homeodomain Proteins, 030209 endocrinology & metabolism, Regulatory Factor X Transcription Factors, Cell fate determination, Biology, 03 medical and health sciences, Animals, Cell Lineage, lcsh:RC31-1245, Molecular Biology, Transcription factor, 030304 developmental biology, Homeodomain Proteins, Rfx6, Cell Biology, MitchelleRiley syndrome, Embryonic stem cell, Mice, Inbred C57BL, 030104 developmental biology, Gene Expression Regulation, Cell fate, PAX6, Energy Metabolism, RFX6, 030217 neurology & neurosurgery, Transcription Factors

Abstract

Objective Enteroendocrine cells (EECs) of the gastro-intestinal tract sense gut luminal factors and release peptide hormones or serotonin (5-HT) to coordinate energy uptake and storage. Our goal is to decipher the gene regulatory networks controlling EECs specification from enteroendocrine progenitors. In this context, we studied the role of the transcription factor Rfx6 which had been identified as the cause of Mitchell–Riley syndrome, characterized by neonatal diabetes and congenital malabsorptive diarrhea. We previously reported that Rfx6 was essential for pancreatic beta cell development and function; however, the role of Rfx6 in EECs differentiation remained to be elucidated. Methods We examined the molecular, cellular, and metabolic consequences of constitutive and conditional deletion of Rfx6 in the embryonic and adult mouse intestine. We performed single cell and bulk RNA-Seq to characterize EECs diversity and identify Rfx6-regulated genes. Results Rfx6 is expressed in the gut endoderm; later, it is turned on in, and restricted to, enteroendocrine progenitors and persists in hormone-positive EECs. In the embryonic intestine, the constitutive lack of Rfx6 leads to gastric heterotopia, suggesting a role in the maintenance of intestinal identity. In the absence of intestinal Rfx6, EECs differentiation is severely impaired both in the embryo and adult. However, the number of serotonin-producing enterochromaffin cells and mucosal 5-HT content are increased. Concomitantly, Neurog3-positive enteroendocrine progenitors accumulate. Combined analysis of single-cell and bulk RNA-Seq data revealed that enteroendocrine progenitors differentiate in two main cell trajectories, the enterochromaffin (EC) cells and the Peptidergic Enteroendocrine (PE) cells, the differentiation programs of which are differentially regulated by Rfx6. Rfx6 operates upstream of Arx, Pax6 and Isl1 to trigger the differentiation of peptidergic EECs such as GIP-, GLP-1-, or CCK-secreting cells. On the contrary, Rfx6 represses Lmx1a and Tph1, two genes essential for serotonin biosynthesis. Finally, we identified transcriptional changes uncovering adaptive responses to the prolonged lack of enteroendocrine hormones and leading to malabsorption and lower food efficiency ratio in Rfx6-deficient mouse intestine. Conclusion These studies identify Rfx6 as an essential transcriptional regulator of EECs specification and shed light on the molecular mechanisms of intestinal failures in human RFX6-deficiencies such as Mitchell–Riley syndrome., Highlights • The lack of Rfx6 impairs the differentiation of peptide-producing enteroendocrine cells. • The number of 5-HT-expressing-cells is increased in Rfx6-deficient intestine. • Intestinal inactivation of Rfx6 leads to lipid malabsorption and decreased food efficiency.

Published

2019

38. Congenital enteropathies involving defects in enterocyte structure or differentiation.

Author

Goulet O, Pigneur B, and Charbit-Henrion F

Subjects

Diarrhea etiology, Diarrhea therapy, Humans, Infant, Newborn, Intestines pathology, Parenteral Nutrition, Enterocytes pathology, Intestinal Diseases diagnosis, Intestinal Diseases genetics, Intestinal Diseases therapy

Abstract

Congenital enteropathies (CE) are a group of rare inherited diseases with a typical onset early in life. They involve defects in enterocyte structure or differentiation. They can cause a severe condition of intestinal failure (IF). The diagnostic approach is based first on clinical presentation (consanguinity, prenatal expression, polyhydramnios, early neonatal onset, aspect of stools, persistence at bowel rest, associated extra-digestive manifestations….) and histo-pathological analyses. These rare intestinal diseases cause protracted diarrhea that might resolve, for a few, with a dietetic approach. However, protracted or permanent IF may require long term parenteral nutrition and, in limited cases, intestinal transplantation. With the progresses in both clinical nutrition and genetics, many of these CE are nowadays associated with recognized gene mutations. It improved our knowledge and the understanding in the patho-physiology of these diseases, thus, leading potentially to therapeutic perspectives. These review cover most of the early onset CE and excludes the immune related diarrhea., (Copyright © 2021. Published by Elsevier Ltd.)

Published

2022

39. Effect of NEUROG3 polymorphism rs144643855 on regional spontaneous brain activity in major depressive disorder.

Author

Hou, Zhuoliang, Liu, Xiaoyun, Jiang, Wenhao, Hou, Zhenghua, Yin, Yingying, Xie, Chunming, Zhang, Haisan, Zhang, Hongxing, Zhang, Zhijun, and Yuan, Yonggui

Subjects

*MENTAL depression, *FUNCTIONAL magnetic resonance imaging, *SINGLE nucleotide polymorphisms, *FRONTAL lobe, *ANHEDONIA

Abstract

• The first study visualized the influence of rs144643855 in the brains of MDD patients. • Frontal lobes were shown to be affected by the interaction between rs144643855 and MDD. • Anhedonia levels are linked to spontaneous brain activity of the IFG-L in MDD patients. • Altered ALFF of the frontal lobe might be the intermediate phenotype of anhedonia in MDD. Our previous study identified a significant association between a single nucleotide polymorphism (SNP) located in the neurogenin3 (NEUROG3) gene and post-stroke depression (PSD) in Chinese populations. The present work explores whether polymorphism rs144643855 affects regional brain activity and clinical phenotypes in major depressive disorder (MDD). A total of 182 participants were included: 116 MDD patients and 66 normal controls. All participants underwent resting-state functional magnetic resonance imaging (rs-fMRI) scanning at baseline. Spontaneous brain activity was assessed using amplitude of low-frequency fluctuation (ALFF). The Hamilton Depression Scale-24 (HAMD-24) and Snaith-Hamilton Pleasure Scale (SHAPS) were used to assess participants at baseline. Two-way analysis of covariance (ANCOVA) was used to explore the interaction between diagnostic groups and NEUROG3 rs144643855 on regional brain activity. We performed correlation analysis to further test the association between these interactive brain regions and clinical manifestations of MDD. Genotype and disease significantly interacted in the left inferior frontal gyrus (IFG-L), right superior frontal gyrus (SFG-R), and left paracentral lobule (PCL-L) (P < 0.05). ALFF values of the IFG-L were found to be significantly associated with anhedonia in MDD patients. These findings suggest a potential relationship between rs144643855 variations and altered frontal brain activity in MDD. NEUROG3 may play an important role in the neuropathophysiology of MDD. [ABSTRACT FROM AUTHOR]

Published

2021

40. Targeted Derivation of Organotypic Glucose- and GLP-1-Responsive β Cells Prior to Transplantation into Diabetic Recipients

Author

Zhiguang Zhou, Yogish C. Kudva, Andre Terzic, Qian Liu, Kuntol Rakshit, Yaxi Zhu, Dennis A. Wigle, Claire A. Schreiber, Aleksey V. Matveyenko, Yasuhiro Ikeda, and Jason M. Tonne

Subjects

0301 basic medicine, Maf Transcription Factors, Large, Mice, SCID, Biochemistry, Transduction (genetics), Mice, 0302 clinical medicine, Glucagon-Like Peptide 1, Transduction, Genetic, NEUROG3, Insulin-Secreting Cells, Insulin Secretion, Basic Helix-Loop-Helix Transcription Factors, lcsh:QH301-705.5, transcription factor, lcsh:R5-920, PDX1, iPSC, C-Peptide, Cell Differentiation, MAFA, 3. Good health, Cell biology, Homeobox Protein Nkx-2.2, β-cell regeneration, lcsh:Medicine (General), Reprogramming, endocrine system, Induced Pluripotent Stem Cells, Incretin, Nerve Tissue Proteins, Biology, Article, Diabetes Mellitus, Experimental, 03 medical and health sciences, Downregulation and upregulation, Diabetes mellitus, Genetics, medicine, Animals, Humans, Transcription factor, Homeodomain Proteins, reprogramming, Cell Biology, Glucose Tolerance Test, Zebrafish Proteins, medicine.disease, Transplantation, 030104 developmental biology, Glucose, lcsh:Biology (General), Gene Expression Regulation, Trans-Activators, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Summary Generation of functional β cells from pluripotent sources would accelerate diagnostic and therapeutic applications for diabetes research and therapy. However, it has been challenging to generate competent β cells with dynamic insulin-secretory capacity to glucose and incretin stimulations. We introduced transcription factors, critical for β-cell development and function, in differentiating human induced pluripotent stem cells (PSCs) and assessed the impact on the functionality of derived β-cell (psBC) progeny. A perifusion system revealed stepwise transduction of the PDX1, NEUROG3, and MAFA triad (PNM) enabled in vitro generation of psBCs with glucose and GLP-1 responsiveness within 3 weeks. PNM transduction upregulated genes associated with glucose sensing, insulin secretion, and β-cell maturation. In recipient diabetic mice, PNM-transduced psBCs showed glucose-responsive insulin secretion as early as 1 week post transplantation. Thus, enhanced pre-emptive β-cell specification of PSCs by PNM drives generation of glucose- and incretin-responsive psBCs in vitro, offering a competent tissue-primed biotherapy., Highlights • PNM transduction facilitates generation of glucose- and GLP1-responsive β cells • Stepwise PNM improves glucose sensing, insulin secretion, and β-cell maturation • PNM-transduced psBCs showed glucose-responsive insulin secretion in diabetic mice, In this article, Ikeda Yasuhiro and colleagues show that stepwise transduction of the triad of transcription factors PDX1, NEUROG3, and MAFA (PNM) enabled in vitro generation of glucose- and GLP-1-responsive β cells from iPSCs within 3 weeks. PNM transduction improves glucose sensing, insulin secretion, and β-cell maturation of generated cells. PNM-transduced β cells showed glucose-responsive insulin secretion as early as 1 week post transplantation in diabetic mice.

Published

2018

41. Extensive NEUROG3 occupancy in the human pancreatic endocrine gene regulatory network.

Author

Schreiber V, Mercier R, Jiménez S, Ye T, García-Sánchez E, Klein A, Meunier A, Ghimire S, Birck C, Jost B, de Lichtenberg KH, Honoré C, Serup P, and Gradwohl G

Subjects

Cells, Cultured, Humans, Basic Helix-Loop-Helix Transcription Factors genetics, Basic Helix-Loop-Helix Transcription Factors metabolism, Endocrine System metabolism, Gene Regulatory Networks genetics, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Pancreas metabolism

Abstract

Objective: Mice lacking the bHLH transcription factor (TF) Neurog3 do not form pancreatic islet cells, including insulin-secreting beta cells, the absence of which leads to diabetes. In humans, homozygous mutations of NEUROG3 manifest with neonatal or childhood diabetes. Despite this critical role in islet cell development, the precise function of and downstream genetic programs regulated directly by NEUROG3 remain elusive. Therefore, we mapped genome-wide NEUROG3 occupancy in human induced pluripotent stem cell (hiPSC)-derived endocrine progenitors and determined NEUROG3 dependency of associated genes to uncover direct targets., Methods: We generated a novel hiPSC line (NEUROG3-HA-P2A-Venus) where NEUROG3 is HA-tagged and fused to a self-cleaving fluorescent VENUS reporter. We used the CUT&RUN technique to map NEUROG3 occupancy and epigenetic marks in pancreatic endocrine progenitors (PEP) that were differentiated from this hiPSC line. We integrated NEUROG3 occupancy data with chromatin status and gene expression in PEPs as well as their NEUROG3-dependence. In addition, we investigated whether NEUROG3 binds type 2 diabetes mellitus (T2DM)-associated variants at the PEP stage., Results: CUT&RUN revealed a total of 863 NEUROG3 binding sites assigned to 1263 unique genes. NEUROG3 occupancy was found at promoters as well as at distant cis-regulatory elements that frequently overlapped within PEP active enhancers. De novo motif analyses defined a NEUROG3 consensus binding motif and suggested potential co-regulation of NEUROG3 target genes by FOXA or RFX transcription factors. We found that 22% of the genes downregulated in NEUROG3 -/- PEPs, and 10% of genes enriched in NEUROG3-Venus positive endocrine cells were bound by NEUROG3 and thus likely to be directly regulated. NEUROG3 binds to 138 transcription factor genes, some with important roles in islet cell development or function, such as NEUROD1, PAX4, NKX2-2, SOX4, MLXIPL, LMX1B, RFX3, and NEUROG3 itself, and many others with unknown islet function. Unexpectedly, we uncovered that NEUROG3 targets genes critical for insulin secretion in beta cells (e.g., GCK, ABCC8/KCNJ11, CACNA1A, CHGA, SCG2, SLC30A8, and PCSK1). Thus, analysis of NEUROG3 occupancy suggests that the transient expression of NEUROG3 not only promotes islet destiny in uncommitted pancreatic progenitors, but could also initiate endocrine programs essential for beta cell function. Lastly, we identified eight T2DM risk SNPs within NEUROG3-bound regions., Conclusion: Mapping NEUROG3 genome occupancy in PEPs uncovered unexpectedly broad, direct control of the endocrine genes, raising novel hypotheses on how this master regulator controls islet and beta cell differentiation., (Copyright © 2021 The Authors. Published by Elsevier GmbH.. All rights reserved.)

Published

2021

42. Gene Signatures of NEUROGENIN3+ Endocrine Progenitor Cells in the Human Pancreas.

Author

Yong HJ, Xie G, Liu C, Wang W, Naji A, Irianto J, and Wang YJ

Subjects

Basic Helix-Loop-Helix Transcription Factors metabolism, Cell Differentiation physiology, Gene Expression Regulation, Developmental, Gene Regulatory Networks, Humans, Nerve Tissue Proteins metabolism, Basic Helix-Loop-Helix Transcription Factors genetics, Endocrine Cells metabolism, Nerve Tissue Proteins genetics, Pancreas metabolism, Stem Cells metabolism

Abstract

NEUROGENIN3+ (NEUROG3+) cells are considered to be pancreatic endocrine progenitors. Our current knowledge on the molecular program of NEUROG3+ cells in humans is largely extrapolated from studies in mice. We hypothesized that single-cell RNA-seq enables in-depth exploration of the rare NEUROG3+ cells directly in humans. We aligned four large single-cell RNA-seq datasets from postnatal human pancreas. Our integrated analysis revealed 10 NEUROG3+ epithelial cells from a total of 11,174 pancreatic cells. Noticeably, human NEUROG3+ cells clustered with mature pancreatic cells and epsilon cells displayed the highest frequency of NEUROG3 positivity. We confirmed the co-expression of NEUROG3 with endocrine markers and the high percentage of NEUROG3+ cells among epsilon cells at the protein level based on immunostaining on pancreatic tissue sections. We further identified unique genetic signatures of the NEUROG3+ cells. Regulatory network inference revealed novel transcription factors including Prospero homeobox protein 1 (PROX1) may act jointly with NEUROG3. As NEUROG3 plays a central role in endocrine differentiation, knowledge gained from our study will accelerate the development of beta cell regeneration therapies to treat diabetes., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Yong, Xie, Liu, Wang, Naji, Irianto and Wang.)

Published

2021

43. Single-Cell Gene Expression Analysis of a Human ESC Model of Pancreatic Endocrine Development Reveals Different Paths to β-Cell Differentiation

Author

Petersen, Maja Borup Kjær, Azad, Ajuna, Ingvorsen, Camilla, Hess, Katja, Hansson, Mattias, Grapin-Botton, Anne, Honoré, Christian, Petersen, Maja Borup Kjær, Azad, Ajuna, Ingvorsen, Camilla, Hess, Katja, Hansson, Mattias, Grapin-Botton, Anne, and Honoré, Christian

Abstract

The production of insulin-producing β cells from human embryonic stem cells (hESCs) in vitro represents a promising strategy for a cell-based therapy for type 1 diabetes mellitus. To explore the cellular heterogeneity and temporal progression of endocrine progenitors and their progeny, we performed single-cell qPCR on more than 500 cells across several stages of in vitro differentiation of hESCs and compared them with human islets. We reveal distinct subpopulations along the endocrine differentiation path and an early lineage bifurcation toward either polyhormonal cells or β-like cells. We uncover several similarities and differences with mouse development and reveal that cells can take multiple paths to the same differentiation state, a principle that could be relevant to other systems. Notably, activation of the key β-cell transcription factor NKX6.1 can be initiated before or after endocrine commitment. The single-cell temporal resolution we provide can be used to improve the production of functional β cells. In this article, Honoré, Grapin-Botton, and colleagues use single-cell expression profiling to show a differentiation sequence from hESCs to pancreatic endocrine cells and early divergence of paths to different endocrine subtypes. Two paths lead to β-cell differentiation where NKX6.1 can be initiated before or after endocrine commitment.

Published

2017

44. Single-Cell Gene Expression Analysis of a Human ESC Model of Pancreatic Endocrine Development Reveals Different Paths to β-Cell Differentiation

Author

Katja Hess, Maja Borup Kjær Petersen, Mattias Hansson, Camilla Ingvorsen, Ajuna Azad, Anne Grapin-Botton, and Christian Honoré

Subjects

0301 basic medicine, Organogenesis, Cellular differentiation, Biochemistry, Transcriptome, 0302 clinical medicine, Single-cell analysis, Genes, Reporter, NEUROG3, Insulin-Secreting Cells, Basic Helix-Loop-Helix Transcription Factors, pancreas, 10. No inequality, Induced pluripotent stem cell, lcsh:QH301-705.5, Genetics, lcsh:R5-920, Gene Expression Regulation, Developmental, Cell Differentiation, differentiation, Cell biology, Phenotype, medicine.anatomical_structure, Single-Cell Analysis, pluripotent stem cells, lcsh:Medicine (General), Pancreas, endocrine, hormone, Nerve Tissue Proteins, Biology, Models, Biological, Article, Immunophenotyping, 03 medical and health sciences, medicine, Humans, Cell Lineage, Progenitor cell, Embryonic Stem Cells, Homeodomain Proteins, Gene Expression Profiling, Computational Biology, progenitor, Cell Biology, Embryonic stem cell, Gene expression profiling, 030104 developmental biology, lcsh:Biology (General), Biomarkers, 030217 neurology & neurosurgery, Developmental Biology, lineage

Abstract

Summary The production of insulin-producing β cells from human embryonic stem cells (hESCs) in vitro represents a promising strategy for a cell-based therapy for type 1 diabetes mellitus. To explore the cellular heterogeneity and temporal progression of endocrine progenitors and their progeny, we performed single-cell qPCR on more than 500 cells across several stages of in vitro differentiation of hESCs and compared them with human islets. We reveal distinct subpopulations along the endocrine differentiation path and an early lineage bifurcation toward either polyhormonal cells or β-like cells. We uncover several similarities and differences with mouse development and reveal that cells can take multiple paths to the same differentiation state, a principle that could be relevant to other systems. Notably, activation of the key β-cell transcription factor NKX6.1 can be initiated before or after endocrine commitment. The single-cell temporal resolution we provide can be used to improve the production of functional β cells., Graphical Abstract, Highlights • Single-cell qPCR identifies subpopulations on hESC to endocrine differentiation paths • All hESC-derived endocrine cells transcribe multiple hormones in vitro • A subpopulation of hESC-derived INS+ cells transcriptionally resembles adult β cells • NKX6.1 onset before or after endocrine commitment leads to β-cell differentiation, In this article, Honoré, Grapin-Botton, and colleagues use single-cell expression profiling to show a differentiation sequence from hESCs to pancreatic endocrine cells and early divergence of paths to different endocrine subtypes. Two paths lead to β-cell differentiation where NKX6.1 can be initiated before or after endocrine commitment.

Published

2017

45. Neurog3 gene dosage regulates allocation of endocrine and exocrine cell fates in the developing mouse pancreas

Author

Christopher V.E. Wright, Daniel A. Anderson, Maneesh C. Kanal, Jingbo Yan, Zheng Cao, Sui Wang, Guoqiang Gu, and Yanwen Xu

Subjects

Islet, endocrine system, medicine.medical_specialty, Cell type, Notch, Cellular differentiation, Endocrine progenitor, Population, Gene Dosage, Neurog3, Mice, Transgenic, Nerve Tissue Proteins, Haploinsufficiency, Cell fate determination, Biology, Article, Ngn3, Mice, 03 medical and health sciences, Dosage, Exocrine Glands, 0302 clinical medicine, Endocrine Glands, Internal medicine, Basic Helix-Loop-Helix Transcription Factors, medicine, Animals, Lateral inhibition, Cell Lineage, Progenitor cell, education, Pancreas, Molecular Biology, 030304 developmental biology, Progenitor, 0303 health sciences, geography, education.field_of_study, geography.geographical_feature_category, Reverse Transcriptase Polymerase Chain Reaction, Diabetes, Cell Biology, Cell biology, Endocrinology, medicine.anatomical_structure, 030217 neurology & neurosurgery, Developmental Biology

Abstract

The basic helix–loop–helix transcription factor Neurog3 (Neurogenin3 or Ngn3) actively drives endodermal progenitor cells towards endocrine islet cell differentiation during embryogenesis. Here, we manipulate Neurog3 expression levels in endocrine progenitor cells without altering its expression pattern using heterozygosity and a hypomorph. Lowered Neurog3 gene dosage in the developing pancreatic epithelium reduces the overall production of endocrine islet cells without significantly affecting the proportions of various islet cell types that do form. A reduced Neurog3 production level in the endocrine-directed pancreatic progenitor population activates the expression of Neurog3 in an increased number of epithelial progenitors. Yet a significant number of these Neurog3+ cells detected in heterozygous and hypomorphic pancreata, possibly those that express low levels of Neurog3, move on to adopt pancreatic ductal or acinar fates. These data directly demonstrate that achieving high levels of Neurog3 expression is a critical step for endocrine commitment from multipotent pancreatic progenitors. These findings also suggest that a high level of Neurog3 expression could mediate lateral inhibition or other unknown feedback mechanisms to regulate the number of cells that initiate Neurog3 transcription and protein production. The control of Neurog3+ cell number and the Neurog3 threshold-dependent endocrine differentiation mechanism combine to select a specific proportion of pancreatic progenitor cells to adopt the islet cell fate.

Published

2010

46. Identification of Enteroendocrine Regulators by Real-Time Single-Cell Differentiation Mapping.

Author

Gehart, Helmuth, van Es, Johan H., Hamer, Karien, Beumer, Joep, Kretzschmar, Kai, Dekkers, Johanna F., Rios, Anne, and Clevers, Hans

Subjects

*ENTEROENDOCRINE cells, *CELL differentiation, *CELLULAR mappings (Mathematics), *PHENOTYPES, *ORGANOIDS

Abstract

Summary Homeostatic regulation of the intestinal enteroendocrine lineage hierarchy is a poorly understood process. We resolved transcriptional changes during enteroendocrine differentiation in real time at single-cell level using a novel knockin allele of Neurog3 , the master regulator gene briefly expressed at the onset of enteroendocrine specification. A bi-fluorescent reporter, Neurog3Chrono, measures time from the onset of enteroendocrine differentiation and enables precise positioning of single-cell transcriptomes along an absolute time axis. This approach yielded a definitive description of the enteroendocrine hierarchy and its sub-lineages, uncovered differential kinetics between sub-lineages, and revealed time-dependent hormonal plasticity in enterochromaffin and L cells. The time-resolved map of transcriptional changes predicted multiple novel molecular regulators. Nine of these were validated by conditional knockout in mice or CRISPR modification in intestinal organoids. Six novel candidate regulators (Sox4, Rfx6, Tox3, Myt1, Runx1t1, and Zcchc12) yielded specific enteroendocrine phenotypes. Our time-resolved single-cell transcriptional map presents a rich resource to unravel enteroendocrine differentiation. Graphical Abstract Highlights • Neurog3Chrono arranges enteroendocrine single-cell transcriptomes on real-time axis • Enteroendocrine cells show hormonal plasticity in the course of their maturation • A time-resolved map characterizes fate specification of all enteroendocrine lineages • Individual knockout of 6 identified regulators gives robust enteroendocrine phenotypes The hierarchical lineage of intestinal enteroendocrine cells is defined at a spatiotemporal single-cell manner and validated using organoid and in vivo models. [ABSTRACT FROM AUTHOR]

Published

2019

47. Targeted Derivation of Organotypic Glucose- and GLP-1-Responsive β Cells Prior to Transplantation into Diabetic Recipients.

Author

Zhu Y, Tonne JM, Liu Q, Schreiber CA, Zhou Z, Rakshit K, Matveyenko AV, Terzic A, Wigle D, Kudva YC, and Ikeda Y

Subjects

Animals, Basic Helix-Loop-Helix Transcription Factors genetics, Basic Helix-Loop-Helix Transcription Factors metabolism, C-Peptide metabolism, Cell Differentiation, Diabetes Mellitus, Experimental chemically induced, Gene Expression Regulation, Glucose Tolerance Test, Homeobox Protein Nkx-2.2, Homeodomain Proteins genetics, Homeodomain Proteins metabolism, Humans, Induced Pluripotent Stem Cells cytology, Induced Pluripotent Stem Cells metabolism, Insulin-Secreting Cells cytology, Insulin-Secreting Cells metabolism, Maf Transcription Factors, Large genetics, Maf Transcription Factors, Large metabolism, Mice, Mice, SCID, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Trans-Activators genetics, Trans-Activators metabolism, Transduction, Genetic, Zebrafish Proteins genetics, Zebrafish Proteins metabolism, Diabetes Mellitus, Experimental therapy, Glucagon-Like Peptide 1 pharmacology, Glucose pharmacology, Induced Pluripotent Stem Cells transplantation, Insulin Secretion drug effects

Abstract

Generation of functional β cells from pluripotent sources would accelerate diagnostic and therapeutic applications for diabetes research and therapy. However, it has been challenging to generate competent β cells with dynamic insulin-secretory capacity to glucose and incretin stimulations. We introduced transcription factors, critical for β-cell development and function, in differentiating human induced pluripotent stem cells (PSCs) and assessed the impact on the functionality of derived β-cell (psBC) progeny. A perifusion system revealed stepwise transduction of the PDX1, NEUROG3, and MAFA triad (PNM) enabled in vitro generation of psBCs with glucose and GLP-1 responsiveness within 3 weeks. PNM transduction upregulated genes associated with glucose sensing, insulin secretion, and β-cell maturation. In recipient diabetic mice, PNM-transduced psBCs showed glucose-responsive insulin secretion as early as 1 week post transplantation. Thus, enhanced pre-emptive β-cell specification of PSCs by PNM drives generation of glucose- and incretin-responsive psBCs in vitro, offering a competent tissue-primed biotherapy., (Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2019

48. Comprehensive single cell mRNA profiling reveals a detailed roadmap for pancreatic endocrinogenesis.

Author

Bastidas-Ponce A, Tritschler S, Dony L, Scheibner K, Tarquis-Medina M, Salinno C, Schirge S, Burtscher I, Böttcher A, Theis FJ, Lickert H, and Bakhti M

Subjects

Animals, Cell Differentiation genetics, Cell Lineage, Endocrine Cells cytology, Gene Expression Profiling, Gene Expression Regulation, Developmental, Genes, Reporter, Insulin-Secreting Cells cytology, Mice, Regeneration, Signal Transduction, Stem Cells cytology, Wnt Proteins metabolism, Basic Helix-Loop-Helix Transcription Factors genetics, Nerve Tissue Proteins genetics, Pancreas embryology, Sequence Analysis, RNA methods, Single-Cell Analysis methods

Abstract

Deciphering mechanisms of endocrine cell induction, specification and lineage allocation in vivo will provide valuable insights into how the islets of Langerhans are generated. Currently, it is ill defined how endocrine progenitors segregate into different endocrine subtypes during development. Here, we generated a novel neurogenin 3 (Ngn3)-Venus fusion (NVF) reporter mouse line, that closely mirrors the transient endogenous Ngn3 protein expression. To define an in vivo roadmap of endocrinogenesis, we performed single cell RNA sequencing of 36,351 pancreatic epithelial and NVF + cells during secondary transition. This allowed Ngn3 low endocrine progenitors, Ngn3 high endocrine precursors, Fev + endocrine lineage and hormone + endocrine subtypes to be distinguished and time-resolved, and molecular programs during the step-wise lineage restriction steps to be delineated. Strikingly, we identified 58 novel signature genes that show the same transient expression dynamics as Ngn3 in the 7260 profiled Ngn3 -expressing cells. The differential expression of these genes in endocrine precursors associated with their cell-fate allocation towards distinct endocrine cell types. Thus, the generation of an accurately regulated NVF reporter allowed us to temporally resolve endocrine lineage development to provide a fine-grained single cell molecular profile of endocrinogenesis in vivo ., Competing Interests: Competing interestsThe authors declare no competing or financial interests., (© 2019. Published by The Company of Biologists Ltd.)

Published

2019

49. Single-Cell Transcriptome Profiling of Mouse and hESC-Derived Pancreatic Progenitors.

Author

Krentz NAJ, Lee MYY, Xu EE, Sproul SLJ, Maslova A, Sasaki S, and Lynn FC

Subjects

Animals, Cell Differentiation, Cell Lineage, Embryo, Mammalian cytology, Humans, Mice, RNA metabolism, Time Factors, Human Embryonic Stem Cells metabolism, Mouse Embryonic Stem Cells metabolism, Pancreas cytology, Single-Cell Analysis, Transcriptome genetics

Abstract

Human embryonic stem cells (hESCs) are a potential unlimited source of insulin-producing β cells for diabetes treatment. A greater understanding of how β cells form during embryonic development will improve current hESC differentiation protocols. All pancreatic endocrine cells, including β cells, are derived from Neurog3-expressing endocrine progenitors. This study characterizes the single-cell transcriptomes of 6,905 mouse embryonic day (E) 15.5 and 6,626 E18.5 pancreatic cells isolated from Neurog3-Cre; Rosa26 mT/mG embryos, allowing for enrichment of endocrine progenitors (yellow; tdTomato + EGFP) and endocrine cells (green; EGFP). Using a NEUROG3-2A-eGFP CyT49 hESC reporter line (N5-5), 4,462 hESC-derived GFP+ cells were sequenced. Differential expression analysis revealed enrichment of markers that are consistent with progenitor, endocrine, or previously undescribed cell-state populations. This study characterizes the single-cell transcriptomes of mouse and hESC-derived endocrine progenitors and serves as a resource (https://lynnlab.shinyapps.io/embryonic&#95;pancreas) for improving the formation of functional β-like cells from hESCs., (Copyright © 2018 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2018

50. Pancreatic Endocrine Tumourigenesis : Genes of potential importance

Author

Johansson, Térèse A.

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, endocrine system, Notch1, Pdx1, Rpl10, endocrine system diseases, Dkk1, Dlk1, Cell- och molekylärbiologi, Neurod1, Neurog3, Tumourigenesis, menin, Hes1, Men1, Pancreatic endocrine tumour, Multiple endocrine neoplasia type 1, Tph1, Notch signalling, Pou3f4, Ascl1, Cell and Molecular Biology

Abstract

Understanding signalling pathways that control pancreatic endocrine tumour (PET) development and proliferation may reveal novel targets for therapeutic intervention. The pathogenesis for sporadic and hereditary PETs, apart from mutations of the MEN1 and VHL tumour suppressor genes, is still elusive. The protein product of the MEN1 gene, menin, regulates many genes. The aim of this thesis was to identify genes involved in pancreatic endocrine tumourigenesis, with special reference to Notch signalling. Messenger RNA and protein expression of NOTCH1, HES1, HEY1, ASCL1, NEUROG3, NEUROD1, DLK1, POU3F4, PDX1, RPL10, DKK1 and TPH1 were studied in human PETs, sporadic and MEN 1, as well as in tumours from heterozygous Men1 mice. For comparison, normal and MEN1 non-tumourous human and mouse pancreatic specimens were used. Nuclear expression of HES1 was consistently absent in PETs. In mouse tumours this coincided with loss of menin expression, and there was a correlation between Men1 expression and several Notch signalling factors. A new phenotype consisting of numerous menin-expressing endocrine cell clusters, smaller than islets, was found in Men1 mice. Expression of NEUROG3 and NEUROD1 was predominantly localised to the cytoplasm in PETs and islets from MEN 1 patients and Men1 mice, whereas expression was solely nuclear in wt mice. Differences in expression levels of Pou3f4, Rpl10 and Dlk1 between islets of Men1 and wt mice were observed. In addition, combined RNA interference and microarray expression analysis in the pancreatic endocrine cell line BON1 identified 158 target genes of ASCL1. For two of these, DKK1 (a negative regulator of the WNT/β-catenin signalling pathway) and TPH1, immunohistochemistry was performed on PETs. In concordance with the microarray finding, DKK1 expression showed an inverse relation to ASCL1 expression. Altered subcellular localisation of HES1, NEUROD1 and NEUROG3 and down-regulation of DKK1 may contribute to tumourigenesis.

Published

2008