Your search keyword '"Bradley W Doble"' showing total 81 results

1. IRE1 signaling increases PERK expression during chronic ER stress

Author

Gideon Ong, Rosemund Ragetli, Katarzyna Mnich, Bradley W. Doble, Wafa Kammouni, and Susan E. Logue

Subjects

Cytology, QH573-671

Abstract

Abstract The Unfolded Protein Response (UPR) is an essential cellular process activated by the accumulation of unfolded proteins within the Endoplasmic Reticulum (ER), a condition referred to as ER stress. Three ER anchored receptors, IRE1, PERK and ATF6 act as ER stress sensors monitoring the health of the ER. Upon detection of ER stress, IRE1, PERK and ATF6 initiate downstream signaling pathways collectively referred to as the UPR. The overarching aim of the UPR is to restore ER homeostasis by reducing ER stress, however if that is not possible, the UPR transitions from a pro-survival to a pro-death response. While our understanding of the key signaling pathways central to the UPR is well defined, the same is not true of the subtle signaling events that help fine tune the UPR, supporting its ability to adapt to varying amplitudes or durations of ER stress. In this study, we demonstrate cross talk between the IRE1 and PERK branches of the UPR, wherein IRE1 via XBP1s signaling helps to sustain PERK expression during prolonged ER stress. Our findings suggest cross talk between UPR branches aids adaptiveness thereby helping to support the plasticity of UPR signaling responses.

Published

2024

2. Gene expression profiling in mouse embryonic stem cells reveals glycogen synthase kinase-3-dependent targets of phosphatidylinositol 3-kinase and Wnt/β-catenin signaling pathways

Author

Colleen M Bartman, Jennifer eEgelston, Sravya eKattula, Leigh C Zeidner, Anthony eD'Ippolito, Bradley W Doble, and Christopher J Phiel

Subjects

Embryonic Stem Cells, Gene Expression, Phosphatidylinositol 3-Kinase, Signal Transduction, Microarray, Wnt, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Glycogen synthase kinase-3 (Gsk-3) activity is an important regulator of numerous signal transduction pathways. Gsk-3 activity is the sum of two largely redundant proteins, Gsk-3α and Gsk-3β, and in general, Gsk-3 is a negative regulator of cellular signaling. Genetic deletion of both Gsk-3α and Gsk-3β in mouse embryonic stem cells (ESCs) has previously been shown to lead to the constitutive activation of the Wnt/β-catenin signaling pathway. However, in addition to Wnt signaling, all Gsk-3-regulated pathways, such as insulin signaling, are also affected simultaneously in Gsk-3α-/-; Gsk-3β-/- ESCs. In an effort to better understand how specific signaling pathways contribute to the global pattern of gene expression in Gsk-3α-/-; Gsk-3β-/- ESCs, we compared the gene expression profiles in Gsk-3α-/-; Gsk-3β-/- ESCs to mouse ESCs in which either Wnt/β-catenin signaling or phosphatidylinositol 3-kinase (PI3K)-dependent insulin signaling are constitutively active. Our results show that Wnt signaling has a greater effect on up-regulated genes in the Gsk-3α-/-; Gsk-3β-/- ESCs, whereas PI3K-dependent insulin signaling is more responsible for the down-regulation of genes in the same cells. These data show the importance of Gsk-3 activity on gene expression in mouse ESCs, and that these effects are due to the combined effects of multiple signaling pathways.

Published

2014

3. Ectopic γ-catenin expression partially mimics the effects of stabilized β-catenin on embryonic stem cell differentiation.

Author

Sujeivan Mahendram, Kevin F Kelly, Sabrina Paez-Parent, Sharmeen Mahmood, Enio Polena, Austin J Cooney, and Bradley W Doble

Subjects

Medicine, Science

Abstract

β-catenin, an adherens junction component and key Wnt pathway effector, regulates numerous developmental processes and supports embryonic stem cell (ESC) pluripotency in specific contexts. The β-catenin homologue γ-catenin (also known as Plakoglobin) is a constituent of desmosomes and adherens junctions and may participate in Wnt signaling in certain situations. Here, we use β-catenin((+/+)) and β-catenin((-/-)) mouse embryonic stem cells (mESCs) to investigate the role of γ-catenin in Wnt signaling and mESC differentiation. Although γ-catenin protein is markedly stabilized upon inhibition or ablation of GSK-3 in wild-type (WT) mESCs, efficient silencing of its expression in these cells does not affect β-catenin/TCF target gene activation after Wnt pathway stimulation. Nonetheless, knocking down γ-catenin expression in WT mESCs appears to promote their exit from pluripotency in short-term differentiation assays. In β-catenin((-/-)) mESCs, GSK-3 inhibition does not detectably alter cytosolic γ-catenin levels and does not activate TCF target genes. Intriguingly, β-catenin/TCF target genes are induced in β-catenin((-/-)) mESCs overexpressing stabilized γ-catenin and the ability of these genes to be activated upon GSK-3 inhibition is partially restored when wild-type γ-catenin is overexpressed in these cells. This suggests that a critical threshold level of total catenin expression must be attained before there is sufficient signaling-competent γ-catenin available to respond to GSK-3 inhibition and to regulate target genes as a consequence. WT mESCs stably overexpressing γ-catenin exhibit robust Wnt pathway activation and display a block in tri-lineage differentiation that largely mimics that observed upon overexpression of β-catenin. However, β-catenin overexpression appears to be more effective than γ-catenin overexpression in sustaining the retention of markers of naïve pluripotency in cells that have been subjected to differentiation-inducing conditions. Collectively, our study reveals a function for γ-catenin in the regulation of mESC differentiation and has implications for human cancers in which γ-catenin is mutated and/or aberrantly expressed.

Published

2013

4. Genetic deficiency of glycogen synthase kinase-3beta corrects diabetes in mouse models of insulin resistance.

Author

Katsuya Tanabe, Zhonghao Liu, Satish Patel, Bradley W Doble, Lin Li, Corentin Cras-Méneur, Sara C Martinez, Cris M Welling, Morris F White, Ernesto Bernal-Mizrachi, James R Woodgett, and M Alan Permutt

Subjects

Biology (General), QH301-705.5

Abstract

Despite treatment with agents that enhance beta-cell function and insulin action, reduction in beta-cell mass is relentless in patients with insulin resistance and type 2 diabetes mellitus. Insulin resistance is characterized by impaired signaling through the insulin/insulin receptor/insulin receptor substrate/PI-3K/Akt pathway, leading to elevation of negatively regulated substrates such as glycogen synthase kinase-3beta (Gsk-3beta). When elevated, this enzyme has antiproliferative and proapoptotic properties. In these studies, we designed experiments to determine the contribution of Gsk-3beta to regulation of beta-cell mass in two mouse models of insulin resistance. Mice lacking one allele of the insulin receptor (Ir+/-) exhibit insulin resistance and a doubling of beta-cell mass. Crossing these mice with those having haploinsufficiency for Gsk-3beta (Gsk-3beta+/-) reduced insulin resistance by augmenting whole-body glucose disposal, and significantly reduced beta-cell mass. In the second model, mice missing two alleles of the insulin receptor substrate 2 (Irs2-/-), like the Ir+/- mice, are insulin resistant, but develop profound beta-cell loss, resulting in early diabetes. We found that islets from these mice had a 4-fold elevation of Gsk-3beta activity associated with a marked reduction of beta-cell proliferation and increased apoptosis. Irs2-/- mice crossed with Gsk-3beta+/- mice preserved beta-cell mass by reversing the negative effects on proliferation and apoptosis, preventing onset of diabetes. Previous studies had shown that islets of Irs2-/- mice had increased cyclin-dependent kinase inhibitor p27(kip1) that was limiting for beta-cell replication, and reduced Pdx1 levels associated with increased cell death. Preservation of beta-cell mass in Gsk-3beta+/- Irs2-/- mice was accompanied by suppressed p27(kip1) levels and increased Pdx1 levels. To separate peripheral versus beta-cell-specific effects of reduction of Gsk3beta activity on preservation of beta-cell mass, mice homozygous for a floxed Gsk-3beta allele (Gsk-3(F/F)) were then crossed with rat insulin promoter-Cre (RIP-Cre) mice to produce beta-cell-specific knockout of Gsk-3beta (betaGsk-3beta-/-). Like Gsk-3beta+/- mice, betaGsk-3beta-/- mice also prevented the diabetes of the Irs2-/- mice. The results of these studies now define a new, negatively regulated substrate of the insulin signaling pathway specifically within beta-cells that when elevated, can impair replication and increase apoptosis, resulting in loss of beta-cells and diabetes. These results thus form the rationale for developing agents to inhibit this enzyme in obese insulin-resistant individuals to preserve beta-cells and prevent diabetes onset.

Published

2008

5. Supplementary Tables 1-6 from Pyrvinium Targets CD133 in Human Glioblastoma Brain Tumor–Initiating Cells

Author

Sheila K. Singh, John A. Hassell, Mickie Bhatia, Bradley W. Doble, Naresh K. Murty, Kesava Reddy, John P. Provias, Boleslaw Lach, Thusyanth Vijayakumar, Neha Garg, David Bakhshinyan, Mohini Singh, Sara M. Nolte, Minomi Subapanditha, Nicole McFarlane, Maleeha A. Qazi, Sujeivan Mahendram, Branavan Manoranjan, Parvez Vora, Robin Hallett, and Chitra Venugopal

Abstract

Supplementary Tables 1-6. Supplementary Table 1: Clinico-pathological demographics of CD133high and CD133low GBM; Supplementary Table 2: Positive and negative correlation probe sets present in CD133-signature; Supplementary Table 3: Drug targets acquired from CD133 gene signature connectivity map; Supplementary Table 4: qRT-PCR Primers; Supplementary Table 5: Genes used to complete network analysis; Supplementary Table 6: Molecular Subtypes of GBM samples used

Published

2023

6. Supplementary Figures 1-6 from Pyrvinium Targets CD133 in Human Glioblastoma Brain Tumor–Initiating Cells

Author

Sheila K. Singh, John A. Hassell, Mickie Bhatia, Bradley W. Doble, Naresh K. Murty, Kesava Reddy, John P. Provias, Boleslaw Lach, Thusyanth Vijayakumar, Neha Garg, David Bakhshinyan, Mohini Singh, Sara M. Nolte, Minomi Subapanditha, Nicole McFarlane, Maleeha A. Qazi, Sujeivan Mahendram, Branavan Manoranjan, Parvez Vora, Robin Hallett, and Chitra Venugopal

Abstract

Supplementary Figures 1-6. Supplementary Figure 1: CD133 correlates patient outcome with GIC selfrenewal and proliferative capacities in human GBM; Supplementary Figure 2: Gene Set Enrichment Analysis (GSEA) results for embryonic stem cell gene sets in CD133high- and CD133low-signature REMBRANDT samples; Supplementary Figure 3: CD133+ GICs are resistant to most compounds selected from CD133 connectivity mapping; Supplementary Figure 4: Pyrvinium specifically targets CD133+ GICs; Supplementary Figure 5: Overexpression of CD133; Supplementary Figure 6: Gene Set Enrichment Analysis (GSEA) results of Pyrvinium or DMSO control treated GICs

Published

2023

7. Data from Pyrvinium Targets CD133 in Human Glioblastoma Brain Tumor–Initiating Cells

Author

Sheila K. Singh, John A. Hassell, Mickie Bhatia, Bradley W. Doble, Naresh K. Murty, Kesava Reddy, John P. Provias, Boleslaw Lach, Thusyanth Vijayakumar, Neha Garg, David Bakhshinyan, Mohini Singh, Sara M. Nolte, Minomi Subapanditha, Nicole McFarlane, Maleeha A. Qazi, Sujeivan Mahendram, Branavan Manoranjan, Parvez Vora, Robin Hallett, and Chitra Venugopal

Abstract

Purpose: Clonal evolution of cancer may be regulated by determinants of stemness, specifically self-renewal, and current therapies have not considered how genetic perturbations or properties of stemness affect such functional processes. Glioblastoma-initiating cells (GICs), identified by expression of the cell surface marker CD133, are shown to be chemoradioresistant. In the current study, we sought to elucidate the functional role of CD133 in self-renewal and identify compounds that can specifically target this CD133+ treatment-refractory population.Experimental Design: Using gain/loss-of-function studies for CD133 we assessed the in vitro self-renewal and in vivo tumor formation capabilities of patient-derived glioblastoma cells. We generated a CD133 signature combined with an in silico screen to find compounds that target GICs. Self-renewal and proliferation assays on CD133-sorted samples were performed to identify the preferential action of hit compounds. In vivo efficacy of the lead compound pyrvinium was assessed in intracranial GIC xenografts and survival studies. Lastly, microarray analysis was performed on pyrvinium-treated GICs to discover core signaling events involved.Results: We discovered pyrvinium, a small-molecule inhibitor of GIC self-renewal in vitro and in vivo, in part through inhibition of Wnt/β-catenin signaling and other essential stem cell regulatory pathways. We provide a therapeutically tractable strategy to target self-renewing, chemoradioresistant, and functionally important CD133+ stem cells that drive glioblastoma relapse and mortality.Conclusions: Our study provides an integrated approach for the eradication of clonal populations responsible for cancer progression, and may apply to other aggressive and heterogeneous cancers. Clin Cancer Res; 21(23); 5324–37. ©2015 AACR.

Published

2023

8. Arhgef2 regulates mitotic spindle orientation in hematopoietic stem cells and is essential for productive hematopoiesis

Author

Victor Gordon, Laura P.M.H. de Rooij, Cailin E. Joyce, Robert Rottapel, Nicholas Wong, Steven Moreira, Bradley W. Doble, Ana Vujovic, María-José Sandí, Carl D. Novina, Derek C.H. Chan, Kristin J Hope, Jose La Rose, and Joshua Xu

Subjects

RHOA, biology, Hematopoiesis and Stem Cells, Apoptosis, Bone Marrow Cells, Spindle Apparatus, Hematology, Cell cycle, Hematopoietic Stem Cells, Hematopoiesis, Cell biology, Haematopoiesis, medicine.anatomical_structure, medicine, biology.protein, Humans, Bone marrow, Stem cell, Progenitor cell, Rho Guanine Nucleotide Exchange Factors, Progenitor, Homing (hematopoietic)

Abstract

How hematopoietic stem cells (HSCs) coordinate their divisional axis and whether this orientation is important for stem cell–driven hematopoiesis is poorly understood. Single-cell RNA sequencing data from patients with Shwachman-Diamond syndrome (SDS), an inherited bone marrow failure syndrome, show that ARHGEF2, a RhoA-specific guanine nucleotide exchange factor and determinant of mitotic spindle orientation, is specifically downregulated in SDS hematopoietic stem and progenitor cells (HSPCs). We demonstrate that transplanted Arhgef2−/− fetal liver and bone marrow cells yield impaired hematopoietic recovery and a production deficit from long-term HSCs, phenotypes that are not the result of differences in numbers of transplanted HSCs, their cell cycle status, level of apoptosis, progenitor output, or homing ability. Notably, these defects are functionally restored in vivo by overexpression of ARHGEF2 or its downstream activated RHOA GTPase. By using live imaging of dividing HSPCs, we show an increased frequency of misoriented divisions in the absence of Arhgef2. ARHGEF2 knockdown in human HSCs also impairs their ability to regenerate hematopoiesis, culminating in significantly smaller xenografts. Together, these data demonstrate a conserved role for Arhgef2 in orienting HSPC division and suggest that HSCs may divide in certain orientations to establish hematopoiesis, the loss of which could contribute to HSC dysfunction in bone marrow failure.

Published

2021

9. Multimerin 1 supports platelet function in vivo and binds to specific GPAGPOGPX motifs in fibrillar collagens that enhance platelet adhesion

Author

Heyu Ni, Bradley W. Doble, Samir W. Hamaia, Peter L. Gross, Subia Tasneem, Catherine P.M. Hayward, Dominique Bihan, D'Andra Parker, Arkadiusz Bonna, Richard W. Farndale, Alexander Leatherdale, David Lillicrap, and Yiming Wang

Subjects

Blood Platelets, Impaired platelet adhesion, Fibrillar Collagens, Multimerin 1, 030204 cardiovascular system & hematology, von Willebrand factor, Fibrinogen, 03 medical and health sciences, Mice, 0302 clinical medicine, Von Willebrand factor, Platelet adhesiveness, medicine, Animals, Platelet, multimerin, platelet adhesiveness, biology, Chemistry, Hematology, Adhesion, Original Articles, Blood Proteins, PLATELETS, Cell biology, biology.protein, Original Article, Ex vivo, medicine.drug

Abstract

Background Multimerin 1 (human: MMRN1, mouse: Mmrn1) is a homopolymeric, adhesive, platelet and endothelial protein that binds to von Willebrand factor and enhances platelet adhesion to fibrillar collagen ex vivo. Objectives To examine the impact of Mmrn1 deficiency on platelet adhesive function, and the molecular motifs in fibrillar collagen that bind MMRN1 to enhance platelet adhesion. Methods Mmrn1‐deficient mice were generated and assessed for altered platelet adhesive function. Collagen Toolkit peptides, and other triple‐helical collagen peptides, were used to identify multimerin 1 binding motifs and their contribution to platelet adhesion. Results MMRN1 bound to conserved GPAGPOGPX sequences in collagens I, II, and III (including GPAGPOGPI, GPAGPOGPV, and GPAGPOGPQ) that enhanced activated human platelet adhesion to collagen synergistically with other triple‐helical collagen peptides (P

Published

2020

10. Neuron-specific protein network mapping of autism risk genes identifies shared biological mechanisms and disease-relevant pathologies

Author

Nadeem Murtaza, Annie A. Cheng, Chad O. Brown, Durga Praveen Meka, Shuai Hong, Jarryll A. Uy, Joelle El-Hajjar, Neta Pipko, Brianna K. Unda, Birgit Schwanke, Sansi Xing, Bhooma Thiruvahindrapuram, Worrawat Engchuan, Brett Trost, Eric Deneault, Froylan Calderon de Anda, Bradley W. Doble, James Ellis, Evdokia Anagnostou, Gary D. Bader, Stephen W. Scherer, Yu Lu, and Karun K. Singh

Subjects

Neurons, Autism Spectrum Disorder, Humans, Proteins, Protein Interaction Maps, Autistic Disorder, Wnt Signaling Pathway, General Biochemistry, Genetics and Molecular Biology

Abstract

There are hundreds of risk genes associated with autism spectrum disorder (ASD), but signaling networks at the protein level remain unexplored. We use neuron-specific proximity-labeling proteomics (BioID2) to identify protein-protein interaction (PPI) networks for 41 ASD risk genes. Neuron-specific PPI networks, including synaptic transmission proteins, are disrupted by de novo missense variants. The PPI network map reveals convergent pathways, including mitochondrial/metabolic processes, Wnt signaling, and MAPK signaling. CRISPR knockout displays an association between mitochondrial activity and ASD risk genes. The PPI network shows an enrichment of 112 additional ASD risk genes and differentially expressed genes from postmortem ASD patients. Clustering of risk genes based on PPI networks identifies gene groups corresponding to clinical behavior score severity. Our data report that cell type-specific PPI networks can identify individual and convergent ASD signaling networks, provide a method to assess patient variants, and highlight biological insight into disease mechanisms and sub-cohorts of ASD.

Published

2022

11. Wnt activation as a therapeutic strategy in medulloblastoma

Author

Minomi Subapanditha, Chitra Venugopal, Neil Winegarden, Ashley A. Adile, Robin M. Hallett, Blake Yarascavitch, John Provias, David Bakhshinyan, Blessing Bassey-Archibong, Neil Savage, Bradley W. Doble, Laura M. Richards, Dillon McKenna, Trevor J. Pugh, Olufemi Ajani, Owen Whitley, Nazanin Tatari, Michelle Kameda-Smith, Adam Fleming, Anna Dvorkin-Gheva, Branavan Manoranjan, Sheila K. Singh, and Gary D. Bader

Subjects

0301 basic medicine, Cancer therapy, Carcinogenesis, Cell, General Physics and Astronomy, 02 engineering and technology, medicine.disease_cause, Mice, lcsh:Science, Wnt Signaling Pathway, beta Catenin, Regulation of gene expression, Multidisciplinary, Cancer stem cells, Stem Cells, Wnt signaling pathway, 021001 nanoscience & nanotechnology, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Heterografts, Stem cell, 0210 nano-technology, Science, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Paediatric cancer, 03 medical and health sciences, Cancer stem cell, Cell Line, Tumor, medicine, Animals, Humans, Cerebellar Neoplasms, neoplasms, Cell Proliferation, Medulloblastoma, Cell growth, Gene Expression Profiling, General Chemistry, medicine.disease, nervous system diseases, Wnt Proteins, CNS cancer, Disease Models, Animal, stomatognathic diseases, 030104 developmental biology, Cancer research, lcsh:Q

Abstract

Medulloblastoma (MB) is defined by four molecular subgroups (Wnt, Shh, Group 3, Group 4) with Wnt MB having the most favorable prognosis. Since prior reports have illustrated the antitumorigenic role of Wnt activation in Shh MB, we aimed to assess the effects of activated canonical Wnt signaling in Group 3 and 4 MBs. By using primary patient-derived MB brain tumor-initiating cell (BTIC) lines, we characterize differences in the tumor-initiating capacity of Wnt, Group 3, and Group 4 MB. With single cell RNA-seq technology, we demonstrate the presence of rare Wnt-active cells in non-Wnt MBs, which functionally retain the impaired tumorigenic potential of Wnt MB. In treating MB xenografts with a Wnt agonist, we provide a rational therapeutic option in which the protective effects of Wnt-driven MBs may be augmented in Group 3 and 4 MB and thereby support emerging data for a context-dependent tumor suppressive role for Wnt/β-catenin signaling., The Wnt molecular subgroup of medulloblastoma is associated with better prognosis than the other molecular subgroups. Here, the authors show that activating Wnt signaling impairs tumor development and improves survival in Group 3 and Group 4 medulloblastoma preclinical models.

Published

2020

12. A CD133-AKT-Wnt signaling axis drives glioblastoma brain tumor-initiating cells

Author

Branavan Manoranjan, Nazanin Tatari, Jason Moffat, Sheila K. Singh, Chitra Venugopal, Chirayu Chokshi, John Provias, Neil Savage, Bradley W. Doble, Minomi Subapanditha, and Naresh Murty

Subjects

0301 basic medicine, Cancer Research, Carcinogenesis, medicine.medical_treatment, Brain tumor, Biology, 03 medical and health sciences, 0302 clinical medicine, Cell surface receptor, Cell Line, Tumor, Genetics, medicine, Humans, AC133 Antigen, Wnt Signaling Pathway, Molecular Biology, Protein kinase B, PI3K/AKT/mTOR pathway, Wnt signaling pathway, Cancer, Immunotherapy, medicine.disease, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer research, Signal transduction, Glioblastoma, Proto-Oncogene Proteins c-akt

Abstract

Mechanistic insight into signaling pathways downstream of surface receptors has been revolutionized with integrated cancer genomics. This has fostered current treatment modalities, namely immunotherapy, to capitalize on targeting key oncogenic signaling nodes downstream of a limited number of surface markers. Unfortunately, rudimentary mechanistic understanding of most other cell surface proteins has reduced the clinical utility of these markers. CD133 has reproducibly been shown to correlate with disease progression, recurrence, and poor overall survivorship in the malignant adult brain tumor, glioblastoma (GBM). Using several patient-derived CD133high and CD133low GBMs we describe intrinsic differences in determinants of stemness, which we owe to a CD133-AKT-Wnt signaling axis in which CD133 functions as a putative cell surface receptor for AKT-dependent Wnt activation. These findings may have implications for personalized oncology trials targeting PI3K/AKT or Wnt as both pathways may be activated independent of their canonical drivers, leading to treatment resistance and disease relapse.

Published

2019

13. TCF/LEF regulation of the topologically associated domain ADI promotes mESCs to exit the pluripotent ground state

Author

Nikolaos Doumpas, Smarth Narula, Simon Söderholm, Bradley W. Doble, Konrad Basler, Claudio Cantù, Steven Moreira, University of Zurich, Cantù, Claudio, and Basler, Konrad

Subjects

Pyridines, medicine.medical_treatment, Transcription Factor 7-Like 1 Protein, Medical Biotechnology (with a focus on Cell Biology (including Stem Cell Biology), Molecular Biology, Microbiology, Biochemistry or Biopharmacy), Mice, mESC, DNA (Cytosine-5-)-Methyltransferases, Hepatocyte Nuclear Factor 1-alpha, Biology (General), Cell Self Renewal, RNA, Small Interfering, beta Catenin, Gene Editing, LEF Transcription Factors, Effector, Chemistry, Wnt signaling pathway, Mouse Embryonic Stem Cells, 10124 Institute of Molecular Life Sciences, Cell biology, Cytokine, embryonic structures, Benzamides, RNA Interference, Transcription Factor 7-Like 2 Protein, animal structures, QH301-705.5, Lymphoid Enhancer-Binding Factor 1, Down-Regulation, Genetics and Molecular Biology, macromolecular substances, General Biochemistry, Genetics and Molecular Biology, TCF/LEF, Inducible T-Cell Co-Stimulator Ligand, Downregulation and upregulation, 1300 General Biochemistry, Genetics and Molecular Biology, medicine, Animals, Medicinsk bioteknologi (med inriktning mot cellbiologi (inklusive stamcellsbiologi), molekylärbiologi, mikrobiologi, biokemi eller biofarmaci), Gene, Diphenylamine, β-catenin, pluripotency, Wnt signaling, Embryonic stem cell, Culture Media, Pyrimidines, General Biochemistry, 570 Life sciences, biology, Leukemia inhibitory factor, Octamer Transcription Factor-3, Transcription Factors

Abstract

Mouse embryonic stem cells (mESCs) can bemaintained in vitro in defined N2B27 medium supplemented with two chemical inhibitors for GSK3 and MEK (2i) and the cytokine leukemia inhibitory factor (LIF), which act synergistically to promote self-renewal and pluripotency. Here, we find that genetic deletion of the four genes encoding the TCF/LEF transcription factors confersm ESCs with the ability to self-renew in N2B27 medium alone. TCF/LEF quadruple knockout (qKO) mESCs display dysregulation of several genes, including Aire, Dnmt3l, and IcosL, located adjacent to each other within a topologically associated domain (TAD). Aire, Dnmt3l, and IcosL appear to be regulated by TCF/LEF in a beta-catenin independent manner. Moreover, downregulation of Aire and Dnmt3l in wild-type mESCs mimics the loss of TCF/LEF and increases mESC survival in the absence of 2iL. Hence, this study identifies TCF/LEF effectors that mediate exit from the pluripotent state. Funding Agencies|Swiss National Science FoundationSwiss National Science Foundation (SNSF)European Commission; Canton of Zurich; Knut and Alice Wallenberg FoundationKnut & Alice Wallenberg Foundation; CancerfondenSwedish Cancer Society [CAN 2018/542]; Canadian Institutes of Health ResearchCanadian Institutes of Health Research (CIHR) [MOP133610]; Swedish Research CouncilSwedish Research CouncilEuropean Commission [2018-05973]

Published

2021

14. β-Catenin safeguards the ground state of mouse pluripotency by strengthening the robustness of the transcriptional apparatus

Author

Xiuling Fu, Jacob H. Hanna, Gang Ma, Jiajian Zhou, Liang Chen, Yunpan Li, Yan Qin, Axel Schambach, Vladislav Krupalnik, Hao Sun, Tian-Tian Zhou, Longqi Liu, Miguel A. Esteban, Fei Gao, Shuhan Chen, Hao Liu, Hui Zhang, Andrew P. Hutchins, Lulu Wang, Bradley W. Doble, Mazid Md. Abdul, Huating Wang, Xichen Bao, Yan Xu, Mengling Jiang, Shahzina Kanwal, Yiwei Lai, Christine Hartmann, Na Li, Xiangpeng Guo, Pengcheng Guo, Jie Yuan, Minghui He, Baoming Qin, David P. Ibañez, Umberto Di Vicino, Xueting Xu, Zhijun Yu, Wenjuan Li, Zhiwei Luo, Giacomo Volpe, Yuan Lv, Ao Jiang, Jianguo Zhou, Muqddas Tariq, Carl Ward, Guoliang Xu, Yayan Feng, Yinghua Huang, Guangming Wu, Dongye Wang, Isaac A. Babarinde, Karthik Arumugam, Runsheng Chen, Meng Zhang, and Maria Pia Cosma

Subjects

0303 health sciences, Multidisciplinary, biology, Chemistry, Kinase, SciAdv r-articles, RNA polymerase II, Cell Biology, Embryonic stem cell, Cell Cycle Gene, 3. Good health, Cell biology, 03 medical and health sciences, 0302 clinical medicine, GSK-3, Transcription (biology), 030220 oncology & carcinogenesis, biology.protein, Protein kinase A, Leukemia inhibitory factor, Molecular Biology, Research Articles, 030304 developmental biology, Research Article

Abstract

β-Catenin recruits BRD4 and other coregulators to protect pluripotency gene transcription against network perturbation., Mouse embryonic stem cells cultured with MEK (mitogen-activated protein kinase kinase) and GSK3 (glycogen synthase kinase 3) inhibitors (2i) more closely resemble the inner cell mass of preimplantation blastocysts than those cultured with SL [serum/leukemia inhibitory factor (LIF)]. The transcriptional mechanisms governing this pluripotent ground state are unresolved. Release of promoter-proximal paused RNA polymerase II (Pol2) is a multistep process necessary for pluripotency and cell cycle gene transcription in SL. We show that β-catenin, stabilized by GSK3 inhibition in medium with 2i, supplies transcriptional coregulators at pluripotency loci. This selectively strengthens pluripotency loci and renders them addicted to transcription initiation for productive gene body elongation in detriment to Pol2 pause release. By contrast, cell cycle genes are not bound by β-catenin, and proliferation/self-renewal remains tightly controlled by Pol2 pause release under 2i conditions. Our findings explain how pluripotency is reinforced in the ground state and also provide a general model for transcriptional resilience/adaptation upon network perturbation in other contexts.

Published

2020

15. A Single TCF Transcription Factor, Regardless of Its Activation Capacity, Is Sufficient for Effective Trilineage Differentiation of ESCs

Author

Alexandre Blais, Solen Abdulla, Geoffrey A. Wood, Victor Gordon, Bradley W. Doble, Anna Dvorkin-Gheva, Enio Polena, Sujeivan Mahendram, Jiayi Cao, and Steven Moreira

Subjects

Male, 0301 basic medicine, Lineage (genetic), Transcription Factor 7-Like 1 Protein, ESC, Embryoid body, Biology, General Biochemistry, Genetics and Molecular Biology, TCF/LEF, Transcriptome, TCF7, Mice, 03 medical and health sciences, Transactivation, Wnt, Gene expression, Animals, LEF1, TCFL2, Hepatocyte Nuclear Factor 1-alpha, Wnt Signaling Pathway, Transcription factor, lcsh:QH301-705.5, beta Catenin, Wnt signaling pathway, Gene Expression Regulation, Developmental, Cell Differentiation, differentiation, β-catenin, pluripotency, Immunohistochemistry, Molecular biology, TCF7L1, 030104 developmental biology, lcsh:Biology (General), Cell culture, embryonic structures, TCF Transcription Factors, Transcription Factors

Abstract

Summary Co-expression and cross-regulation of the four TCF/LEFs render their redundant and unique functions ambiguous. Here, we describe quadruple-knockout (QKO) mouse ESCs lacking all full-length TCF/LEFs and cell lines rescued with TCF7 or TCF7L1. QKO cells self-renew, despite gene expression patterns that differ significantly from WT, and display delayed, neurectoderm-biased, embryoid body (EB) differentiation. QKO EBs have no contracting cardiomyocytes and differentiate poorly into mesendoderm but readily generate neuronal cells. QKO cells and TCF7L1-rescued cells cannot efficiently activate TCF reporters, whereas TCF7-rescued cells exhibit significant reporter responsiveness. Surprisingly, despite dramatically different transactivation capacities, re-expression of TCF7L1 or TCF7 in QKO cells restores their tri-lineage differentiation ability, with similar lineage marker expression patterns and beating cardiomyocyte frequencies observed in EBs. Both factors also similarly affect the transcriptome of QKO cells. Our data reveal that a single TCF, regardless of its activation capacity, is sufficient for effective trilineage differentiation of ESCs.

Published

2017

16. Lfc/Arhgef2 regulates mitotic spindle orientation in hematopoietic stem and progenitor cells and is essential for productive hematopoiesis

Author

Bradley W. Doble, María-José Sandí, Kristin J Hope, Victor Gordon, Nicholas Wong, Robert Rottapel, Cailin E. Joyce, Jose La Rose, Joshua Xu, Carl D. Novina, Ana Vujovic, Laura P.M.H. de Rooij, and Derek C.H. Chan

Subjects

0303 health sciences, Bone marrow failure, Cell cycle, Biology, medicine.disease, Cell biology, 03 medical and health sciences, Haematopoiesis, 0302 clinical medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, medicine, Bone marrow, Stem cell, Progenitor cell, 030304 developmental biology, Progenitor, Homing (hematopoietic)

Abstract

How hematopoietic stem cells (HSCs) coordinate their divisional axis relative to supportive niche cells and whether or not their divisional orientation is important for stem cell-driven hematopoiesis is poorly understood. Single cell RNA sequencing data from patients with the inherited bone marrow failure Shwachman-Diamond syndrome (SDS) show that ARHGEF2, a RhoA-specific guanine nucleotide exchange factor (GEF) and determinant of mitotic spindle orientation, is one of a restricted group of genes specifically downregulated in SDS HSCs and multipotent progenitors. Here, we describe Lfc/Arhgef2 as an important regulator of hematopoiesis in vivo. Transplanted Lfc/Arhgef2-/- bone marrow shows impaired hematopoietic recovery and a production deficit of long-term HSCs. These phenotypes cannot be explained by differences in numbers of transplanted HSCs, their cell cycle status, level of apoptosis, progenitor output or homing ability. Using live imaging of dividing hematopoietic stem and progenitor cells (HSPCs), we show an increased frequency of misoriented divisions in the absence of Lfc/Arhgef2. Functional ARHGEF2 knockdown in human HSCs also impairs their ability to regenerate hematopoiesis, culminating in significantly smaller hematopoietic xenografts. Together, these data provide evidence demonstrating a conserved role for Lfc/Arhgef2 in orienting HSPC division and suggest that HSCs divide in certain orientations to establish hematopoiesis, the loss of which leads to their exhaustion in a mechanism that may underlie certain bone marrow failure syndromes.

Published

2019

17. Regulation of thymocyte β-selection, development and positive selection by glycogen synthase kinase-3

Author

Bradley W. Doble, Michael J. Parsons, Satish Patel, James R. Woodgett, and Pamela S. Ohashi

Subjects

0303 health sciences, biology, Chemistry, Kinase, T cell, T-cell receptor, macromolecular substances, Cell biology, 03 medical and health sciences, Thymocyte, 0302 clinical medicine, medicine.anatomical_structure, GSK-3, medicine, biology.protein, Glycogen synthase, Beta (finance), CD8, 030304 developmental biology, 030215 immunology

Abstract

Glycogen synthase kinase-3 (GSK-3) is a ubiquitously expressed serine/threonine kinase, that exists as two isoforms in mammals, GSK-3α and GSK-3β, that are key downstream mediators of the phosphatidylinositol 3’ kinase, Wnt, Notch and other pathways. Here, we report that simultaneous inactivation of both GSK-3α and GSK-3β during early thymocyte ontogeny has profound effects on both β-selection and positive selection, key checkpoints essential to producing functionally mature αβ T cells. Conditional GSK-3α/β knockout animals (LckCre+ GSK-3αβfl/fl) possessed pre-double positive (pre-DP) thymocytes (CD4−CD8−CD117−CD25−) with compromised TCRβ chain expression along with elevated levels of β-catenin and reduced Notch activity. β-selection was impaired allowing pre-DP thymocytes to differentiate to DP thymocytes (CD4+CD8+) while bypassing strict requirements for productive TCRβ chain rearrangements and functional expression. Also impaired was the requisite pre-TCR and Notch-mediated expansion that normally precedes differentiation to the DP stage. Consequently, LckCre+ GSK-3αβfl/fl mice initially generated fewer DP thymocytes that expressed significantly reduced levels of mature TCR. The aberrant DP thymocytes expressed high levels of the pro-survival Bcl-2 family member Mcl-1, failed positive selection and accumulated as CD4hiCD8lo positive selection intermediates resulting in loss of both mature CD4 and CD8 lineages. LckCre+ GSK-3αβfl/fl mice succumbed to oligoclonal peripheral lymphomas with high penetrance. These data reveal essential roles for GSK-3 in several checkpoints of early T cell development.

Published

2019

18. GSK3 Deficiencies in Hematopoietic Stem Cells Initiate Pre-neoplastic State that Is Predictive of Clinical Outcomes of Human Acute Leukemia

Author

Bradley W. Doble, Mickie Bhatia, Borhane Guezguez, Borko Tanasijevic, Riccardo Masetti, Susann Rahmig, Mohammed Almakadi, Aline Fiebig-Comyn, Zoya Shapovalova, Silvia Bresolin, Yannick D. Benoit, Fanny L. Casado, Guezguez, Borhane, Almakadi, Mohammed, Benoit, Yannick D., Shapovalova, Zoya, Rahmig, Susann, Fiebig-Comyn, Aline, Casado, Fanny L., Tanasijevic, Borko, Bresolin, Silvia, Masetti, Riccardo, Doble, Bradley W., and Bhatia, Mickie

Subjects

Myeloid, 0301 basic medicine, Cancer Research, Mice, Transgenic, macromolecular substances, Acute, Biology, Animals, Disease Models, Animal, Glycogen Synthase Kinase 3, Glycogen Synthase Kinase 3 beta, Hematopoietic Stem Cells, Humans, Leukemia, Myeloid, Acute, Proto-Oncogene Proteins c-akt, Signal Transduction, Transgenic, Mice, 03 medical and health sciences, hemic and lymphatic diseases, medicine, Acute leukemia, Leukemia, Animal, Myelodysplastic syndromes, Wnt signaling pathway, Myeloid leukemia, hemic and immune systems, Hematopoietic Stem Cell, Cell Biology, medicine.disease, 3. Good health, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Oncology, Disease Models, Cancer research, Stem cell, Human

Abstract

Initial pathway alternations required for pathogenesis of human acute myeloid leukemia (AML) are poorly understood. Here we reveal that removal of glycogen synthase kinase-3α (GSK-3α) and GSK-3β dependency leads to aggressive AML. Although GSK-3α deletion alone has no effect, GSK-3β deletion in hematopoietic stem cells (HSCs) resulted in a pre-neoplastic state consistent with human myelodysplastic syndromes (MDSs). Transcriptome and functional studies reveal that each GSK-3β and GSK-3α uniquely contributes to AML by affecting Wnt/Akt/mTOR signaling and metabolism, respectively. The molecular signature of HSCs deleted for GSK-3β provided a prognostic tool for disease progression and survival of MDS patients. Our study reveals that GSK-3α- and GSK-3β-regulated pathways can be responsible for stepwise transition to MDS and subsequent AML, thereby providing potential therapeutic targets of disease evolution. Guezguez et al. show that progressive removal of glycogen synthase kinase-3 (GSK-3) signaling by Gsk3b allelic deletion results in an MDS state that, when combined with Gsk3a deletion, leads to AML. A molecular signature derived from Gsk3b-null cells has prognostic potential for MDS patients.

Published

2016

19. TCF7L1 and TCF7 differentially regulate specific mouse ES cell genes in response to GSK-3 inhibition

Author

Eloi Mercier, Alexandre Blais, Seo C, Sujeivan Mahendram, Bradley W. Doble, Enio Polena, and Steven Moreira

Subjects

0303 health sciences, biology, Chemistry, Cell, Wnt signaling pathway, Repressor, Epitope, 3. Good health, Chromatin, Cell biology, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, GSK-3, medicine, biology.protein, Antibody, Gene, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

The genome-wide chromatin occupancy of the TCF/LEF factors and its modulation by Wnt pathway activation remain poorly defined. Here, we describe mouse ES cell (mESC) lines expressing a single copy knock-in of the 3xFLAG epitope at the N-terminus of TCF7L1 and TCF7, the two most-highly expressed TCF/LEF factors in mESCs. TCF7L1 protein levels, detected by immunoblotting with a FLAG antibody, were much higher than TCF7 in mESCs maintained in standard serum- and LIF-supplemented medium, even in the presence of the GSK-3 inhibitor, CHIR99021 (CHIR). We used FLAG antibody-mediated ChIP-seq to determine TCF7 and TCF7L1 chromatin occupancy in mESCs cultured in standard medium with or without CHIR for 14 hours. TCF7 and TCF7L1 displayed very few overlapping ChIP peaks across the genome, with TCF7L1 binding significantly more genes than TCF7 in both culture conditions. Despite a reduction in total TCF7L1 protein after CHIR treatment, the TCF7L1 ChIP peak profiles were not uniformly attenuated. Our data demonstrate that TCF7L1 chromatin occupancy upon short-term CHIR treatment is modulated in a target-specific manner. Our findings also suggest that Wnt target genes in mESCs are not regulated by TCF/LEF switching, and TCF7L1, although often called a constitutive repressor, may serve as a transcriptional activator of certain target genes in CHIR-treated mESCs.HighlightsChIP and cytometry data suggest that TCF7L1 does not directly regulate mESC Nanog expression.TCF7L1 remains associated with β-catenin in the presence of CHIR99021.TCF7 and TCF7L1 display different chromatin occupancies in mESCs.TCF7L1 binding at specific genomic sites is variably altered by CHIR99021.

Published

2018

20. Endogenous BioID elucidates TCF7L1 interactome modulation upon GSK-3 inhibition in mouse ESCs

Author

Steven Moreira, Brett Larsen, David Ng, Sansi Xing, Enio Polena, Yu Lu, Fung, Brian Raught, Bradley W. Doble, Ruilin Wu, Anne-Claude Gingras, Wong Cj, Gordon, and Seo C

Subjects

chemistry.chemical_classification, DNA ligase, 0303 health sciences, Transgene, 030302 biochemistry & molecular biology, Wnt signaling pathway, Endogeny, Biology, Interactome, Cell biology, chemistry.chemical_compound, 03 medical and health sciences, 0302 clinical medicine, Biotin, chemistry, GSK-3, Biotinylation, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Modulation of Wnt target gene expression via the TCF/LEFs remains poorly understood. We employ proximity-based biotin labeling (BioID) to examine GSK-3 inhibitor effects on the TCF7L1 interactome in mouse ESCs. We generated ESC lines with biotin ligase BirA* fused to TCF7L1 by knocking it into the endogenousTCF7L1locus or by inserting a doxinducible BirA*-TCF7L1 transgene into theRosa26locus. Induction yielded BirA*-TCF7L1 levels 3-fold higher than in the endogenous system, but substantial overlap in biotinylated proteins with high peptide counts were detected by each method. Known TCF7L1 interactors TLE3/4 and β-catenin, and numerous proteins not previously associated with TCF7L1, were identified in both systems. Despite reduced BirA*-TCF7L1 levels, the number of hits identified with both BioID approaches increased after GSK-3 inhibition. We elucidate the network of TCF7L1 proximal proteins regulated by GSK-3 inhibition, validate the utility of endogenous BioID, and provide mechanistic insights into TCF7L1 target gene regulation.HighlightsBirA*-TCF7L1 at single-copy physiological levels generates robust BioID dataCHIR99021 reduces TCF7L1 levels but increases detectable TCF7L1-proximal proteinsThe TCF7L1 interactome of largely epigenetic/transcription factors fluctuates with GSK-3 inhibitionJMJD1C, SALL4 and BRG1/SMARCA4 are validated as TCF7L-interacting proteins

Published

2018

21. Fine-Tuning of the RIG-I-Like Receptor/Interferon Regulatory Factor 3-Dependent Antiviral Innate Immune Response by the Glycogen Synthase Kinase 3/β-Catenin Pathway

Author

Priscilla Doyon, Alexandre Marineau, Marc J. Servant, Jean-François Clément, James R. Woodgett, Kashif Aziz Khan, Bradley W. Doble, and Florence Dô

Subjects

macromolecular substances, Biology, RIG-I-like receptor, Respirovirus Infections, Sendai virus, Vesicular stomatitis Indiana virus, DEAD-box RNA Helicases, Glycogen Synthase Kinase 3, Mice, Immune system, Cell Line, Tumor, Rhabdoviridae Infections, medicine, Animals, Humans, Phosphorylation, RNA, Small Interfering, Receptors, Immunologic, Molecular Biology, beta Catenin, Mice, Knockout, Glycogen Synthase Kinase 3 beta, Innate immune system, Pattern recognition receptor, Articles, Cell Biology, Molecular biology, Immunity, Innate, HEK293 Cells, Viperin, Interferon Type I, DEAD Box Protein 58, Interferon Regulatory Factor-3, RNA Interference, IRF3, Interferon type I, HeLa Cells, medicine.drug, Interferon regulatory factors

Abstract

Induction of an antiviral innate immune response relies on pattern recognition receptors, including retinoic acid-inducible gene 1-like receptors (RLR), to detect invading pathogens, resulting in the activation of multiple latent transcription factors, including interferon regulatory factor 3 (IRF3). Upon sensing of viral RNA and DNA, IRF3 is phosphorylated and recruits coactivators to induce type I interferons (IFNs) and selected sets of IRF3-regulated IFN-stimulated genes (ISGs) such as those for ISG54 (Ifit2), ISG56 (Ifit1), and viperin (Rsad2). Here, we used wild-type, glycogen synthase kinase 3α knockout (GSK-3α(-/-)), GSK-3β(-/-), and GSK-3α/β double-knockout (DKO) embryonic stem (ES) cells, as well as GSK-3β(-/-) mouse embryonic fibroblast cells in which GSK-3α was knocked down to demonstrate that both isoforms of GSK-3, GSK-3α and GSK-3β, are required for this antiviral immune response. Moreover, the use of two selective small-molecule GSK-3 inhibitors (CHIR99021 and BIO-acetoxime) or ES cells reconstituted with the catalytically inactive versions of GSK-3 isoforms showed that GSK-3 activity is required for optimal induction of antiviral innate immunity. Mechanistically, GSK-3 isoform activation following Sendai virus infection results in phosphorylation of β-catenin at S33/S37/T41, promoting IRF3 DNA binding and activation of IRF3-regulated ISGs. This study identifies the role of a GSK-3/β-catenin axis in antiviral innate immunity.

Published

2015

22. CSIG-22. A CD133-Akt-Wnt SIGNALING AXIS PROVIDES FUNCTIONAL INSIGHT INTO THE ROLE OF CD133 IN GLIOBLASTOMA BRAIN TUMOR-INITIATING CELLS

Author

Sujeivan Mahendram, Minomi Subapanditha, Sheila K. Singh, Branavan Manoranjan, Jason Moffat, Chitra Venugopal, Neil Savage, Bradley W. Doble, Maleeha Qazi, and Parvez Vora

Subjects

Cancer Research, business.industry, Wnt signaling pathway, Brain tumor, Biology, medicine.disease, Abstracts, Text mining, Oncology, Cancer research, medicine, Neurology (clinical), business, Protein kinase B, Glioblastoma

Abstract

Current transcriptional profiles of adult glioblastoma (GBM) recognize the activation of distinct signaling programs. Single-cell sequencing efforts have provided greater resolution of core developmental pathways implicated in disease progression and relapse. Of note, the Wnt pathway is activated in a subset of patients, despite the lack of recurrent activating mutations in human GBM. Given the description of CD133 as a marker of tumor-initiating cells in a number of human cancers associated with activated Wnt signaling, we investigated the role of CD133 in human GBM as a novel Wnt regulator. CD133high GBM lines were found to have greater Wnt levels when compared to CD133low lines. To establish a signaling axis between CD133 and Wnt we investigated the CD133-dependent activation of Akt and the subsequent downstream inhibition of GSK leading to beta-catenin activation. Ectopic expression of CD133 resulted in increased pAKT, pGSK (Ser 9), and beta-catenin. To further describe the context-dependent role for Akt activation of Wnt through GSK inhibition, CD133high lines were treated with the Akt inhibitor, MK-2006, which decreased pAKT, pGSK (Ser 9), and beta-catenin. In order to validate the tumorigenic potential of Wnt-activated cells, a Wnt reporter was used to isolate cells with endogenous Wnt signaling. Wnt-active cells maintained an increased self-renewal and tumor-initiating capacity when compared to Wnt-inactive cells. Xenografts generated from Wnt active cells had a reduced survival advantage as these contained an enhanced expression of stemness genes when compared to Wnt-inactive xenografts. To develop a rationale clinical therapeutic, we used RWO3, a novel humanized antibody directed at CD133. In vivo treatment with RW03 showed a significant reduction in activated Wnt signaling, highlighting the role of CD133 in modulating the Wnt pathway. Our work establishes a CD133-Akt-Wnt signaling axis in GBM through the functional characterization of CD133 and subsequent context-specific Akt-dependent regulation of the canonical Wnt pathway.

Published

2017

23. TRTH-29. CONTEXT-SPECIFIC TUMOR SUPPRESSIVE FUNCTION OF THE CANONICAL WNT PATHWAY IN PEDIATRIC MEDULLOBLASTOMA HIGHLIGHTS A THERAPEUTIC STRATEGY FOR TREATMENT-REFRACTORY SUBGROUPS

Author

Minomi Subapanditha, Branavan Manoranjan, Chitra Venugopal, Bradley W. Doble, David Bakhshinyan, Michelle Kameda-Smith, and Sheila K. Singh

Subjects

Medulloblastoma, Cancer Research, business.industry, Treatment refractory, Wnt signaling pathway, Pharmacology, medicine.disease, Abstracts, Text mining, Oncology, Context specific, Cancer research, Medicine, Neurology (clinical), Signal transduction, business, Function (biology), Therapeutic strategy

Abstract

Current molecular subgroups of childhood medulloblastoma (MB) recognize distinct disease entities of which activated Wnt signaling is associated with a distinct subgroup and the best overall outcome. In contrast, non-Wnt MBs are characterized by metastatic disease, increased rate of recurrence, and poor overall survivorship. Given the excellent clinical outcome in Wnt-driven MB, we aimed to convert treatment-resistant MB subgroups 3 and 4 into an ostensibly benign tumor. Activated Wnt signaling by way of Wnt agonists decreased in vitro self-renewal of primary MB cells. Comparative RNA-sequencing of control and transgenic lines containing a stabilized beta-catenin mutant demonstrated a reduction in self-renewal genes following beta-catenin overexpression, including Sox2 and Bmi1. In order to validate the therapy-sensitive nature of Wnt-activated cells, we developed stable human Group 3 and 4 patient-derived lines containing a 7XTOPFlash reporter to determine the presence of endogenous Wnt signaling. Rare subclonal Wnt-active cells demonstrated a reduced self-renewal and tumor-initiating capacity through in vivo limiting dilution assays when compared to bulk Wnt-inactive cells from Group 3 and 4 MBs. The therapeutic relevance of these findings were demonstrated with an in vivo survival advantage in mice with orthotopic injections of cells containing stabilized beta-catenin overexpression or endogenous Wnt-active cells. Resulting xenograft tumors were smaller in size, maintained a lower rate of proliferation, and reduction in MB self-renewal genes. To develop a rationale clinical therapeutic, we used a novel substrate-competitive peptide inhibitor for GSK. Treatment with our peptide inhibitor showed a significant reduction in tumor burden and metastatic disease with a corresponding increase in survival of patient-derived Group 3 and 4 tumors that were otherwise treatment-resistant. Our work establishes activated Wnt signaling as a novel treatment paradigm in childhood MB, identifies a rationale therapeutic approach for recurrent MB, and provides evidence for the context-specific tumor suppressive function of the canonical Wnt pathway.

Published

2017

24. The responses of neural stem cells to the level of GSK-3 depend on the tissue of origin

Author

James R. Woodgett, Derek van der Kooy, Tamara Holowacz, Bradley W. Doble, Brenda L. K. Coles, Tania O. Alexson, and Kevin F. Kelly

Subjects

QH301-705.5, Science, Hippocampal formation, Biology, Bioinformatics, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, GSK-3, Precursor cell, Genetic model, Progenitor cell, Biology (General), reproductive and urinary physiology, 030304 developmental biology, Neural stem cells, 0303 health sciences, Wnt signaling pathway, Embryonic stem cell, Wnt signaling, ES cells, Neural stem cell, Cell biology, nervous system, Neurosphere assay, General Agricultural and Biological Sciences, 030217 neurology & neurosurgery, Research Article

Abstract

Summary Neural stem cells (NSCs) can be obtained from a variety of sources, but not all NSCs exhibit the same characteristics. We have examined how the level of glycogen synthase kinase-3 activity regulates NSCs obtained from different sources: the mouse embryonic striatum, embryonic hippocampus, and mouse ES cells. Growth of striatal NSCs is enhanced by mild inhibition of GSK-3 but not by strong inhibition that is accompanied by Wnt/TCF transcriptional activation. In contrast, the growth of hippocampal NSCs is enhanced by both mild inhibition of GSK-3 as well as stronger inhibition. Active Wnt/TCF signaling, which occurs normally in the embryonic hippocampus, is required for growth of neural stem and progenitor cells. In the embryonic striatal germinal zone, however, TCF signaling is normally absent and its activation inhibits growth of NSCs from this region. Using a genetic model for progressive loss of GSK-3, we find that primitive ES cell-derived NSCs resemble striatal NSCs. That is, partial loss of GSK-3 alleles leads to an increase in NSCs while complete ablation of GSK-3, and activation of TCF-signaling, leads to their decline. Furthermore, expression of dominant negative TCF-4 in the GSK-3-null background was effective in blocking expression of Wnt-response genes and was also able to rescue neuronal gene expression. These results reveal that GSK-3 regulates NSCs by divergent pathways depending on the tissue of origin. The responses of these neural precursor cells may be contingent on baseline Wnt/TCF signaling occurring in a particular tissue.

Published

2013

25. Phosphatidylinositol 3-Kinase (PI3K) Signaling via Glycogen Synthase Kinase-3 (Gsk-3) Regulates DNA Methylation of Imprinted Loci

Author

Sigrid Eckardt, Leigh C. Zeidner, Joanna Groden, Bruce J. Aronow, Peter White, K. John McLaughlin, Anthony P. Popkie, Ashley M. Albrecht, David E. Newsom, Christopher J. Phiel, Anthony D'Ippolito, and Bradley W. Doble

Subjects

RNA, Untranslated, Mice, Transgenic, macromolecular substances, Models, Biological, Biochemistry, DNA methyltransferase, Gene Expression Regulation, Enzymologic, Receptor, IGF Type 2, Genomic Imprinting, Glycogen Synthase Kinase 3, Mice, Phosphatidylinositol 3-Kinases, Insulin-Like Growth Factor II, GSK-3, Animals, Epigenetics, Glycogen synthase, Molecular Biology, Embryonic Stem Cells, Oligonucleotide Array Sequence Analysis, biology, Kinase, Cell Biology, DNA Methylation, Molecular biology, DNA methylation, biology.protein, RNA, Long Noncoding, Genomic imprinting, Signal Transduction, DNA hypomethylation

Abstract

Glycogen synthase kinase-3 (Gsk-3) isoforms, Gsk-3α and Gsk-3β, are constitutively active, largely inhibitory kinases involved in signal transduction. Underscoring their biological significance, altered Gsk-3 activity has been implicated in diabetes, Alzheimer disease, schizophrenia, and bipolar disorder. Here, we demonstrate that deletion of both Gsk-3α and Gsk-3β in mouse embryonic stem cells results in reduced expression of the de novo DNA methyltransferase Dnmt3a2, causing misexpression of the imprinted genes Igf2, H19, and Igf2r and hypomethylation of their corresponding imprinted control regions. Treatment of wild-type embryonic stem cells and neural stem cells with the Gsk-3 inhibitor, lithium, phenocopies the DNA hypomethylation at these imprinted loci. We show that inhibition of Gsk-3 by phosphatidylinositol 3-kinase (PI3K)-mediated activation of Akt also results in reduced DNA methylation at these imprinted loci. Finally, we find that N-Myc is a potent Gsk-3-dependent regulator of Dnmt3a2 expression. In summary, we have identified a signal transduction pathway that is capable of altering the DNA methylation of imprinted loci.

Published

2010

26. Abstract 148: Canonical Wnt activation as a therapeutic strategy in pediatric medulloblastoma

Author

Neil Savage, Bradley W. Doble, Olufemi Ajani, Sheila K. Singh, David Bakhshinyan, Adam Fleming, Anna Dvorkin-Gheva, Chitra Venugopal, Michelle Kameda-Smith, Blake Yarascavitch, Branavan Manoranjan, Ashley A. Adile, Minomi Subapanditha, and Steven Moreira

Subjects

Medulloblastoma, Cancer Research, Oncology, business.industry, medicine, Cancer research, Wnt signaling pathway, medicine.disease, business, Therapeutic strategy

Abstract

Brain tumors represent the leading cause of childhood cancer mortality, of which medulloblastoma (MB) is the most frequent malignant pediatric brain tumor. Current molecular subgroups of MB recognize distinct disease entities of which activated Wnt signaling (monosomy 6, exon 3 mutations in CTNNB1, and Wnt gene signature) is associated with a distinct subgroup and the best overall outcome. In contrast, only non-Wnt MBs are characterized by metastatic disease, increased rate of recurrence, and poor overall survivorship. Given the excellent clinical outcome in patients with Wnt-driven MB, we aimed to convert treatment-resistant MB subgroups into an ostensibly benign tumor through selective activation of the canonical Wnt pathway. Initial characterization of patient-derived Wnt and non-Wnt MB lines demonstrated a significant reduction in in vitro self-renewal and proliferative capacity of Wnt MBs. This was further validated by RNA-seq, which identified a marked reduction in the expression of stem cell self-renewal genes Bmi1 and Sox2 in Wnt MBs compared to non-Wnt MBs. Further, Wnt MB-derived xenografts maintained a significant increase in overall survival compared to non-Wnt MB xengrafts, further highlighting the protective nature of activated Wnt signaling in MB. Activated Wnt signaling by way of small molecule Wnt agonists in treatment-refractory MBs resulted in decreased in vitro self-renewal and expression of self-renewal genes, Bmi1 and Sox2. In order to validate the therapy-sensitive nature of Wnt-activated cells, we developed stable patient-derived lines containing a 7XTOPFlash reporter for endogenous Wnt signaling. Rare subclonal Wnt-active cells demonstrated a reduced self-renewal and tumor-initiating capacity through in vivo limiting dilution assays when compared to bulk Wnt-inactive cells. The therapeutic relevance of these findings were demonstrated with an in vivo survival advantage in those mice with orthotopic injections of cells with endogenous Wnt activity when compared to xenografts generated from Wnt-inactive cells. To develop a rationale clinical therapeutic, we used a novel substrate-competitive peptide inhibitor for GSK. Treatment with our peptide inhibitor showed a significant reduction in tumor burden with a corresponding increase in survival of patient-derived tumors that were otherwise treatment-resistant. The clinical utility of our findings is further supported by our analysis of integrated genomics data from 763 primary MBs, in which a validated Wnt gene signature was found to predict improved survivorship among children with poor-outcome and metastatic MBs. Our work establishes activated Wnt signaling as a novel treatment paradigm in childhood MB, identifies a rationale therapeutic approach for recurrent MB, and provides evidence for the context-specific tumor suppressive function of the canonical Wnt pathway. Citation Format: Sheila Kumari Singh, Branavan Manoranjan, Anna Dvorkin-Gheva, Chitra Venugopal, Steven Moreira, Michelle Kameda-Smith, Minomi Subapanditha, Ashley Adile, David Bakhshinyan, Neil Savage, Blake Yarascavitch, Olufemi Ajani, Adam Fleming, Bradley Doble. Canonical Wnt activation as a therapeutic strategy in pediatric medulloblastoma [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 148.

Published

2018

27. Tissue-Specific Role of Glycogen Synthase Kinase 3β in Glucose Homeostasis and Insulin Action

Author

Bradley W. Doble, Daniel J. Drucker, Satish Patel, Katrina MacAulay, Elaine M. Sinclair, and James R. Woodgett

Subjects

medicine.medical_specialty, macromolecular substances, AKT3, Cell Line, MAP2K7, Glycogen Synthase Kinase 3, Mice, chemistry.chemical_compound, GSK-3, Internal medicine, medicine, Animals, Homeostasis, Insulin, Muscle, Skeletal, Phosphorylase kinase, Glycogen synthase, Molecular Biology, GSK3B, Alleles, Mice, Knockout, Glycogen Synthase Kinase 3 beta, Glycogen, biology, Biological Transport, Articles, Cell Biology, Mice, Inbred C57BL, Insulin receptor, Glucose, Endocrinology, Liver, chemistry, Organ Specificity, Gene Targeting, biology.protein, Gene Deletion, Signal Transduction

Abstract

Dysregulation of the protein kinase glycogen synthase kinase 3 (GSK-3) has been implicated in the development of type 2 diabetes mellitus. GSK-3 protein expression and kinase activity are elevated in diabetes, while selective GSK-3 inhibitors have shown promise as modulators of glucose metabolism and insulin sensitivity. There are two GSK-3 isoforms in mammals, GSK-3 and GSK-3. Mice engineered to lack GSK-3 die in late embryogenesis from liver apoptosis, whereas mice engineered to lack GSK-3 are viable and exhibit improved insulin sensitivity and hepatic glucose homeostasis. To assess the potential role of GSK-3 in insulin function, a conditional gene-targeting approach whereby mice in which expression of GSK-3 was specifically ablated within insulin-sensitive tissues were generated was undertaken. Liver-specific GSK-3 knockout mice are viable and glucose and insulin tolerant and display “normal” metabolic characteristics and insulin signaling. Mice lacking expression of GSK-3 in skeletal muscle are also viable but, in contrast to the liver-deleted animals, display improved glucose tolerance that is coupled with enhanced insulin-stimulated glycogen synthase regulation and glycogen deposition. These data indicate that there are not only distinct roles for GSK-3 and GSK-3 within the adult but also tissue-specific phenotypes associated with each of these isoforms. Glycogen synthase kinase 3 (GSK-3) is a highly conserved, ubiquitously expressed serine/threonine protein kinase that exists as two isoforms, GSK-3 (51 kDa) and GSK-3 (47 kDa), which are encoded by separate genes that produce highly ho

Published

2008

28. Phosphorylation by p38 MAPK as an Alternative Pathway for GSK3β Inactivation

Author

James L. Clements, Bin Deng, C. David Wood, Alexander Aronshtam, Bradley W. Doble, Guadalupe Sabio, Tina M. Thornton, Mercedes Rincon, Gustavo Pedraza-Alva, Dwight E. Matthews, and Roger J. Davis

Subjects

endocrine system diseases, Thymus Gland, macromolecular substances, Mitogen-activated protein kinase kinase, p38 Mitogen-Activated Protein Kinases, Article, Phosphorylation cascade, MAP2K7, Glycogen Synthase Kinase 3, Mice, Serine, Animals, Humans, ASK1, Phosphorylation, Protein Kinase Inhibitors, beta Catenin, Glycogen Synthase Kinase 3 beta, Multidisciplinary, MAP kinase kinase kinase, biology, Chemistry, Akt/PKB signaling pathway, Cyclin-dependent kinase 2, Brain, enzymes and coenzymes (carbohydrates), Biochemistry, biology.protein, Cyclin-dependent kinase 9, biological phenomena, cell phenomena, and immunity, Proto-Oncogene Proteins c-akt, hormones, hormone substitutes, and hormone antagonists

Abstract

Glycogen synthase kinase 3beta (GSK3beta) is involved in metabolism, neurodegeneration, and cancer. Inhibition of GSK3beta activity is the primary mechanism that regulates this widely expressed active kinase. Although the protein kinase Akt inhibits GSK3beta by phosphorylation at the N terminus, preventing Akt-mediated phosphorylation does not affect the cell-survival pathway activated through the GSK3beta substrate beta-catenin. Here, we show that p38 mitogen-activated protein kinase (MAPK) also inactivates GSK3beta by direct phosphorylation at its C terminus, and this inactivation can lead to an accumulation of beta-catenin. p38 MAPK-mediated phosphorylation of GSK3beta occurs primarily in the brain and thymocytes. Activation of beta-catenin-mediated signaling through GSK3beta inhibition provides a potential mechanism for p38 MAPK-mediated survival in specific tissues.

Published

2008

29. Role of Glycogen Synthase Kinase-3 in Cell Fate and Epithelial-Mesenchymal Transitions

Author

Bradley W. Doble and James R. Woodgett

Subjects

Histology, Cadherin, Mesenchymal stem cell, Wnt signaling pathway, food and beverages, Epithelial Cells, Biology, Cadherins, Models, Biological, Epithelium, Cell biology, Mesoderm, Wnt Proteins, Glycogen Synthase Kinase 3, Basal (phylogenetics), GSK-3, Neoplasms, Snail Family Transcription Factors, Animals, Humans, Epithelial–mesenchymal transition, Anatomy, Transcription Factors, Epithelial polarity

Abstract

Epithelial cells usually exist as sheets of immotile, tightly packed, well-coupled, polarized cells with distinct apical, basal and lateral surfaces. Remarkably, these cells can dramatically alter their morphology to become motile, fibroblast-like mesenchymal cells in a process of epithelial-mesenchymal transition (EMT). This process and the reverse, mesenchymal-epithelial transition, occur repeatedly during normal embryonic development. A phenomenon similar to physiological EMT occurs during the pathophysiological progression of some cancers. Tumours of epithelial origin, as they transform to malignancy, appear to exploit the innate plasticity of epithelial cells, with EMT conferring increased invasiveness and metastatic potential. Key to the maintenance of epithelial cell identity is the expression of E-cadherin, a protein that is required for tight intercellular adhesion along the lateral surfaces of adjacent epithelial cells. Loss of functional E-cadherin is a critical event in EMT. An important regulator of E-cadherin expression is the protein Snail, a zinc-finger transcriptional repressor. Snail contains several consensus sites for the kinase, glycogen synthase kinase-3 (GSK-3), and accumulating evidence indicates that it is a GSK-3 substrate. Phosphorylation of Snail by GSK-3 facilitates its proteasomal degradation. Conversely, inhibition of GSK-3 leads to Snail accumulation, E-cadherin downregulation, and development of EMT in cultured epithelial cells. Several signalling pathways implicated in the progression of EMT, including the Wnt and phosphoinositide 3-kinase pathways, use GSK-3 to mediate their responses. In these pathways, GSK-3’s regulation of other transcriptional effectors like β-catenin works in concert with changes in Snail to orchestrate the EMT process. This review focuses on the emerging role of GSK-3 as a modulator of cell fate and EMT in the contexts of development, in vitro cell culture and cancer.

Published

2007

30. STEM-23PYRVINIUM TARGETS CD133 IN HUMAN GLIOBLASTOMA BRAIN TUMOR-INITIATING CELLS

Author

Mickie Bhatia, Sara M. Nolte, Nicole McFarlane, Bradley W. Doble, Sheila K. Singh, Minomi Subapanditha, Sujeivan Mahendram, Parvez Vora, Robin M. Hallett, Maleeha Qazi, Lach Boleslaw, Chitra Venugopal, Mohini Singh, David Bakhshinyan, Provias John, John A. Hassell, Kesava Reddy, Branavan Manoranjan, Neha Garg, and Naresh Murty

Subjects

Cancer Research, Text mining, Oncology, business.industry, Brain tumor, medicine, Cancer research, Neurology (clinical), Tumor initiation, medicine.disease, business, Abstracts from the 20th Annual Scientific Meeting of the Society for Neuro-Oncology, Glioblastoma

Published

2015

31. Glycogen synthase kinase-3 (Gsk-3) plays a fundamental role in maintaining DNA methylation at imprinted loci in mouse embryonic stem cells

Author

Anthony D'Ippolito, Bradley W. Doble, Leigh C. Zeidner, George Marnellos, Kelsie J. Faulds, Gavin Meredith, Logan Hostetter, Thomas H. Arnold, Yulei Wang, Christopher M Adams, Miroslav Dudas, Christopher J. Phiel, and Anthony P. Popkie

Subjects

macromolecular substances, Biology, 03 medical and health sciences, chemistry.chemical_compound, Genomic Imprinting, Glycogen Synthase Kinase 3, Mice, 0302 clinical medicine, Animals, Epigenetics, Molecular Biology, RNA-Directed DNA Methylation, Embryonic Stem Cells, 030304 developmental biology, Genetics, Mice, Knockout, 0303 health sciences, Glycogen Synthase Kinase 3 beta, High-Throughput Nucleotide Sequencing, Cell Biology, Epigenome, Articles, DNA Methylation, Signaling, Differentially methylated regions, chemistry, Genetic Loci, DNA methylation, Illumina Methylation Assay, Genomic imprinting, 030217 neurology & neurosurgery, DNA, Signal Transduction

Abstract

A genome-wide analysis is given of DNA methylation in mouse embryonic stem cells in which both Gsk-3α and Gsk-3β have been genetically deleted. DNA methylation patterns are compared to those of wild-type cells. More than 75% of known imprinted loci have reduced DNA methylation in the Gsk-3–knockout cells., Glycogen synthase kinase-3 (Gsk-3) is a key regulator of multiple signal transduction pathways. Recently we described a novel role for Gsk-3 in the regulation of DNA methylation at imprinted loci in mouse embryonic stem cells (ESCs), suggesting that epigenetic changes regulated by Gsk-3 are likely an unrecognized facet of Gsk-3 signaling. Here we extend our initial observation to the entire mouse genome by enriching for methylated DNA with the MethylMiner kit and performing next-generation sequencing (MBD-Seq) in wild-type and Gsk-3α−/−;Gsk-3β−/− ESCs. Consistent with our previous data, we found that 77% of known imprinted loci have reduced DNA methylation in Gsk-3-deficient ESCs. More specifically, we unambiguously identified changes in DNA methylation within regions that have been confirmed to function as imprinting control regions. In many cases, the reduced DNA methylation at imprinted loci in Gsk-3α−/−;Gsk-3β−/− ESCs was accompanied by changes in gene expression as well. Furthermore, many of the Gsk-3–dependent, differentially methylated regions (DMRs) are identical to the DMRs recently identified in uniparental ESCs. Our data demonstrate the importance of Gsk-3 activity in the maintenance of DNA methylation at a majority of the imprinted loci in ESCs and emphasize the importance of Gsk-3–mediated signal transduction in the epigenome.

Published

2015

32. Glycogen Synthase Kinase-3 - An Overview of An Over-Achieving Protein Kinase

Author

Satish Patel, Lisa Kockeritz, Bradley W. Doble, and James R. Woodgett

Subjects

Pharmacology, Programmed cell death, Kinase, Clinical Biochemistry, macromolecular substances, Metabolism, Biology, Substrate Specificity, Cell biology, Glycogen Synthase Kinase 3, Biochemistry, GSK-3, Drug Discovery, biology.protein, Animals, Humans, Molecular Medicine, Phosphorylation, Signal transduction, Protein kinase A, Glycogen synthase, Protein Kinase Inhibitors, Signal Transduction

Abstract

Glycogen synthase kinase-3 (GSK-3) has attracted much scrutiny due to its plethora of cellular functions, novel mechanisms of regulation and its potential as a therapeutic target for several common diseases. In mammals, GSK-3 is encoded by two genes, termed GSK-3alpha and GSK-3beta, that yield related but distinct protein-serine kinases. GSK-3 is unusual in that its protein kinase activity tends to be high in resting cells and cellular stimuli, such as hormones and growth factors, result in its catalytic inactivation. Further, many of the substrate proteins of GSK-3 are functionally inhibited by phosphorylation. Thus, signals that inhibit GSK-3 often cause activation of its diverse array of target proteins. Regulation of GSK-3 is important for normal development, regulation of metabolism, neuronal growth and differentiation and modulation of cell death. Dysregulation of GSK-3 activity has been implicated in human pathologies such as neurodegenerative diseases and type-2 diabetes. In this introductory chapter we provide a primer on the modes of GSK-3 regulation and a description of the various signaling pathways and cellular processes in which GSK-3 is an active participant.

Published

2006

33. Pyrvinium Targets CD133 in Human Glioblastoma Brain Tumor-Initiating Cells

Author

Boleslaw Lach, Sara M. Nolte, Chitra Venugopal, Naresh Murty, Bradley W. Doble, Minomi Subapanditha, Sheila K. Singh, John A. Hassell, Branavan Manoranjan, Robin M. Hallett, Thusyanth Vijayakumar, David Bakhshinyan, Maleeha Qazi, Neha Garg, Nicole McFarlane, Mohini Singh, Kesava Reddy, Parvez Vora, John Provias, Mickie Bhatia, and Sujeivan Mahendram

Subjects

Cancer Research, In silico, Population, Gene Expression, Antineoplastic Agents, Biology, Bioinformatics, Somatic evolution in cancer, Pyrvinium, chemistry.chemical_compound, Pyrvinium Compounds, In vivo, Antigens, CD, Spheroids, Cellular, Tumor Cells, Cultured, Animals, Humans, Gene Regulatory Networks, AC133 Antigen, Cell Self Renewal, education, Cell Proliferation, Glycoproteins, education.field_of_study, Microarray analysis techniques, Brain Neoplasms, Gene Expression Profiling, Wnt signaling pathway, Prognosis, Xenograft Model Antitumor Assays, Gene Expression Regulation, Neoplastic, Disease Models, Animal, Oncology, chemistry, Gene Knockdown Techniques, Cancer research, Neoplastic Stem Cells, Stem cell, Glioblastoma, Peptides, Signal Transduction

Abstract

Purpose: Clonal evolution of cancer may be regulated by determinants of stemness, specifically self-renewal, and current therapies have not considered how genetic perturbations or properties of stemness affect such functional processes. Glioblastoma-initiating cells (GICs), identified by expression of the cell surface marker CD133, are shown to be chemoradioresistant. In the current study, we sought to elucidate the functional role of CD133 in self-renewal and identify compounds that can specifically target this CD133+ treatment-refractory population. Experimental Design: Using gain/loss-of-function studies for CD133 we assessed the in vitro self-renewal and in vivo tumor formation capabilities of patient-derived glioblastoma cells. We generated a CD133 signature combined with an in silico screen to find compounds that target GICs. Self-renewal and proliferation assays on CD133-sorted samples were performed to identify the preferential action of hit compounds. In vivo efficacy of the lead compound pyrvinium was assessed in intracranial GIC xenografts and survival studies. Lastly, microarray analysis was performed on pyrvinium-treated GICs to discover core signaling events involved. Results: We discovered pyrvinium, a small-molecule inhibitor of GIC self-renewal in vitro and in vivo, in part through inhibition of Wnt/β-catenin signaling and other essential stem cell regulatory pathways. We provide a therapeutically tractable strategy to target self-renewing, chemoradioresistant, and functionally important CD133+ stem cells that drive glioblastoma relapse and mortality. Conclusions: Our study provides an integrated approach for the eradication of clonal populations responsible for cancer progression, and may apply to other aggressive and heterogeneous cancers. Clin Cancer Res; 21(23); 5324–37. ©2015 AACR.

Published

2014

34. GSK-3: tricks of the trade for a multi-tasking kinase

Author

James R. Woodgett and Bradley W. Doble

Subjects

macromolecular substances, Article, MAP2K7, Glycogen Synthase Kinase 3, Alzheimer Disease, Cyclin-dependent kinase, GSK-3, Proto-Oncogene Proteins, Diabetes Mellitus, Animals, Humans, Hedgehog Proteins, ASK1, Phosphorylation, Protein kinase A, MAPK14, Serine/threonine-specific protein kinase, Cyclin-dependent kinase 1, biology, Cell Biology, Zebrafish Proteins, Cell biology, Wnt Proteins, Eukaryotic Cells, Biochemistry, Trans-Activators, biology.protein, Signal Transduction

Abstract

Glycogen synthase kinase 3 (GSK-3) is a multifunctional serine/threonine kinase found in all eukaryotes. The enzyme is a key regulator of numerous signalling pathways, including cellular responses to Wnt, receptor tyrosine kinases and G-protein-coupled receptors and is involved in a wide range of cellular processes, ranging from glycogen metabolism to cell cycle regulation and proliferation. GSK-3 is unusual in that it is normally active in cells and is primarily regulated through inhibition of its activity. Another peculiarity compared with other protein kinases is its preference for primed substrates,that is, substrates previously phosphorylated by another kinase. Several recent advances have improved our understanding of GSK-3 regulation in multiple pathways. These include the solution of the crystal structure of GSK-3, which has provided insight into GSK-3's penchant for primed substrates and the regulation of GSK-3 by serine phosphorylation, and findings related to the involvement of GSK-3 in the Wnt/β-catenin and Hedgehog pathways. Finally, since increased GSK-3 activity may be linked to pathology in diseases such as Alzheimer's disease and non-insulin-dependent diabetes mellitus,several new GSK-3 inhibitors, such as the aloisines, the paullones and the maleimides, have been developed. Although they are just starting to be characterized in cell culture experiments, these new inhibitors hold promise as therapeutic agents.

Published

2003

35. PKC-Dependent Phosphorylation May Regulate the Ability of Connexin43 to Inhibit DNA Synthesis

Author

Robert R. Fandrich, S. Banerji, Peter A. Cattini, Bradley W. Doble, Yan Jin, Elissavet Kardami, and Xitong Dang

Subjects

DNA Replication, medicine.medical_treatment, Clinical Biochemistry, Mitosis, Stimulation, Protein Kinase C-epsilon, macromolecular substances, Biology, Phosphorylation cascade, Serine, medicine, Animals, Humans, Myocytes, Cardiac, Cloning, Molecular, Phosphorylation, Protein kinase A, Cells, Cultured, Protein Kinase C, Protein kinase C, DNA synthesis, Growth factor, Cell Biology, General Medicine, Rats, Cell biology, Enzyme Activation, Biochemistry, Connexin 43, Mutation, cardiovascular system, Fibroblast Growth Factor 2, sense organs, biological phenomena, cell phenomena, and immunity, HeLa Cells

Abstract

Phosphorylation affects several biological functions of connexin43 (Cx43), although its role on Cx43-mediated inhibition of DNA synthesis is not known. Previous studies showed increased Cx43 phosphorylation on serine in response to growth factor stimulation of cardiomyocytes, mediated by protein kinase C-epsilon (PKCepsilon). Here we report that activation of PKCepsilon is also necessary for stimulation of cardiomyocyte DNA synthesis and mitosis. We have investigated the participation of specific serine residues that are putative PKC targets in producing phosphorylated Cx43 species and also in regulating DNA synthesis in cardiomyocytes. Interference with the PKC signaling system and/or the phosphorylation of specific amino-acids of Cx43 may allow regulation of the mitogenic response.

Published

2003

36. Abstract 5831: Activated Wnt signaling for the treatment of recurrent medulloblastoma

Author

Sheila K. Singh, Chitra Venugopal, Minomi Subapanditha, Bradley W. Doble, Jason Moffat, Zvezdan Pavlovic, David Bakhshinyan, Michelle Kameda-Smith, Sujeivan Mahendram, and Branavan Manoranjan

Subjects

Medulloblastoma, Cancer Research, business.industry, Wnt signaling pathway, Cancer, LRP5, Gene signature, medicine.disease, Oncology, SOX2, BMI1, medicine, Cancer research, Stem cell, business

Abstract

Brain tumors represent the leading cause of childhood cancer mortality, of which medulloblastoma (MB) is the most frequent malignant pediatric brain tumor. Current molecular subgroups of MB recognize distinct disease entities of which activated Wnt signaling (monosomy 6, exon 3 mutations in CTNNB1, and Wnt gene signature) is associated with a distinct subgroup and the best overall outcome. In contrast, only non-Wnt MBs are characterized by metastatic disease, increased rate of recurrence, and poor overall survivorship. Given the excellent clinical outcome in patients with Wnt-driven MB, we aimed to convert treatment-resistant MB subgroups into an ostensibly benign tumor through selective targeting by small molecules and transgenic patient-derived lines containing a stabilized beta-catenin mutant. Activated Wnt signaling by way of Wnt agonists in treatment-refractory MBs resulted in decreased in vitro self-renewal and promoted differentiation. Comparative gene expression profiling of control and transgenic lines containing a stabilized beta-catenin mutant demonstrated a reduction in stem cell self-renewal genes following beta-catenin overexpression, including Sox2 and Bmi1. In order to validate the therapy-sensitive nature of Wnt-activated cells, we developed stable patient-derived lines containing a 7XTOPFlash reporter for endogenous Wnt signaling. Rare subclonal Wnt-active cells demonstrated a reduced self-renewal and tumor-initiating capacity through in vivo limiting dilution assays when compared to bulk Wnt-inactive cells. The therapeutic relevance of these findings were demonstrated with an in vivo survival advantage in mice with orthotopic injections of cells containing a stabilized beta-catenin mutant representative of constitutively active Wnt signaling or endogenous Wnt-active cells. Xenografts generated from Wnt-activated tumors were smaller in size, maintained a lower rate of proliferation, and reduction in MB self-renewal genes. To further illustrate the clinical utility of activated Wnt signaling, we modified the Children’s Oncology Group therapy protocol for childhood MB so that xenografts may receive chemo/radiotherapy. Tumors generated from Wnt-active xenografts were much more radiosensitive and displayed a significant reduction in spinal metastasis when compared to mice receiving standard therapy without Wnt activation. To develop a rationale clinical therapeutic, we developed unique agonist antibodies that target the Wnt co-receptor LRP5. Treatment with LRP5 antibodies showed a significant reduction in tumor burden and increase in survival of patient-derived tumors that were otherwise treatment-resistant. Our work establishes for the first time activated Wnt signaling as a novel treatment paradigm in childhood MB, identifies a rationale therapeutic approach for recurrent MB, and provides evidence for the context-specific tumor suppressive function of the canonical Wnt pathway. Note: This abstract was not presented at the meeting. Citation Format: Branavan Manoranjan, Chitra Venugopal, Zvezdan Pavlovic, David Bakhshinyan, Michelle Kameda-Smith, Minomi Subapanditha, Sujeivan Mahendram, Jason Moffat, Bradley W. Doble, Sheila Singh. Activated Wnt signaling for the treatment of recurrent medulloblastoma [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr 5831. doi:10.1158/1538-7445.AM2017-5831

Published

2017

37. Gene Expression Profiling in Mouse Embryonic Stem Cells Reveals Glycogen Synthase Kinase-3-Dependent Targets of Phosphatidylinositol 3-Kinase and Wnt/β-Catenin Signaling Pathways

Author

Bradley W. Doble, Jennifer N. Egelston, Colleen Marie Bartman, Anthony D'Ippolito, Sravya Kattula, Leigh C. Zeidner, and Christopher J. Phiel

Subjects

Cell signaling, phosphatidylinositol 3-kinase, Endocrinology, Diabetes and Metabolism, macromolecular substances, lcsh:Diseases of the endocrine glands. Clinical endocrinology, 03 medical and health sciences, Wnt, 0302 clinical medicine, Endocrinology, GSK-3, Glycogen synthase, PI3K/AKT/mTOR pathway, 030304 developmental biology, Original Research, glycogen synthase kinase-3, 0303 health sciences, lcsh:RC648-665, biology, Wnt signaling pathway, embryonic stem cells, Molecular biology, Cell biology, Gene expression profiling, Insulin receptor, quantitative PCR, biology.protein, gene expression, Signal transduction, microarray, 030217 neurology & neurosurgery, signal transduction

Abstract

Glycogen synthase kinase-3 (Gsk-3) activity is an important regulator of numerous signal transduction pathways. Gsk-3 activity is the sum of two largely redundant proteins, Gsk-3α and Gsk-3β, and in general, Gsk-3 is a negative regulator of cellular signaling. Genetic deletion of both Gsk-3α and Gsk-3β in mouse embryonic stem cells (ESCs) has previously been shown to lead to the constitutive activation of the Wnt/β-catenin signaling pathway. However, in addition to Wnt signaling, all Gsk-3-regulated pathways, such as insulin signaling, are also affected simultaneously in Gsk-3α(-) (/) (-); Gsk-3β(-) (/) (-)ESCs. In an effort to better understand how specific signaling pathways contribute to the global pattern of gene expression in Gsk-3α(-) (/) (-); Gsk-3β(-) (/) (-)ESCs, we compared the gene expression profiles in Gsk-3α(-) (/) (-); Gsk-3β(-) (/) (-) ESCs to mouse ESCs in which either Wnt/β-catenin signaling or phosphatidylinositol 3-kinase (PI3K)-dependent insulin signaling are constitutively active. Our results show that Wnt signaling has a greater effect on up-regulated genes in the Gsk-3α(-) (/) (-); Gsk-3β(-) (/) (-)ESCs, whereas PI3K-dependent insulin signaling is more responsible for the down-regulation of genes in the same cells. These data show the importance of Gsk-3 activity on gene expression in mouse ESCs, and that these effects are due to the combined effects of multiple signaling pathways.

Published

2014

38. CUG-initiated FGF-2 induces chromatin compaction in cultured cardiac myocytes and in vitro

Author

Bradley W. Doble, James R. Davie, Jian-Min Sun, Peter A. Cattini, Guangping Sun, Elissavet Kardami, Robert R. Fandrich, Lorrie A. Kirshenbaum, and Robert Z. Florkiewicz

Subjects

biology, Physiology, Clinical Biochemistry, Cell Biology, Molecular biology, In vitro, Chromatin, Cell biology, Histone, medicine.anatomical_structure, Prophase, Histone H1, biology.protein, medicine, Nuclear lamina, Fibroblast, Mitosis

Abstract

Fibroblast growth factor-2 (FGF-2) is a mitogen found in CUG-initiated 21-25 kDa ("hi") or AUG-initiated 16-18 kDa ("lo") forms. Previously we demonstrated that "hi"-but not "lo"-FGF-2 caused a distinct nuclear phenotype characterized by apparently condensed chromatin present as separate clumps in the nucleus of cardiac myocytes. In this manuscript we investigated whether these effects were related to apoptosis or mitosis and whether they reflected a direct effect of "hi" FGF-2 on chromatin. Myocytes overexpressing "hi" FGF-2 and presenting the clumped chromatin phenotype: (i) were not labeled above background with antibodies to phosphorylated histones H1 and H3 used as indicators of mitotic chromatin condensation; (ii) did not stain positive for TUNEL; (iii) their nuclear lamina, visualized by anti-laminB immunofluorescence, appeared intact; (iv) neither caspase inhibitors, nor Bcl-2 or "lo" FGF-2 overexpression prevented the manifestation of the compacted nuclear phenotype. Purified recombinant "hi" FGF-2 was more potent than "lo" FGF-2 in promoting the condensation/aggregation of chick erythrocyte chromatin partially reconstituted with histone H1 in vitro. We conclude that the DNA phenotype induced by "hi" FGF-2 in cardiac myocytes likely reflects a direct effect on chromatin structure that does not require the engagement of mitosis or apoptosis. By affecting chromatin compaction "hi" FGF-2 may contribute to the regulation of gene expression.

Published

2001

39. The ε Subtype of Protein Kinase C Is Required for Cardiomyocyte Connexin-43 Phosphorylation

Author

Elissavet Kardami, Peipei Ping, and Bradley W. Doble

Subjects

Physiology, Immunoprecipitation, Protein Kinase C-epsilon, Connexin, Biology, chemistry.chemical_compound, Alkaloids, Animals, Humans, Tissue Distribution, Enzyme Inhibitors, Phosphorylation, Protein kinase A, Cells, Cultured, Protein Kinase C, Protein kinase C, Benzophenanthridines, Kinase, Myocardium, Gap Junctions, Molecular biology, Recombinant Proteins, Phenanthridines, Rats, Cell biology, Isoenzymes, Chelerythrine, chemistry, Connexin 43, cardiovascular system, Tetradecanoylphorbol Acetate, Fibroblast Growth Factor 2, sense organs, Mitogen-Activated Protein Kinases, biological phenomena, cell phenomena, and immunity, Cardiology and Cardiovascular Medicine

Abstract

Abstract —Gap junctions (GJs), composed of connexins, are intercellular channels ensuring electric and metabolic coupling between cardiomyocytes. We have shown previously that an endogenous mitogenic and cardioprotective protein, fibroblast growth factor-2 (FGF-2), decreases cardiomyocyte GJ permeability by stimulating phosphorylation of connexin-43 (Cx43). Identifying the kinase(s) phosphorylating cardiac Cx43 may thus provide a way of modulating cardiac intercellular communication. Because FGF-2 activates receptors linked to protein kinase C (PKC) and mitogen-activated protein kinase, we first investigated participation of these enzymatic systems in Cx43 phosphorylation. The inhibitor PD98059 blocked activation of mitogen-activated protein kinase, but it did not prevent the FGF-2 effects on GJs. In contrast, the PKC inhibitor chelerythrine blocked the effects of FGF-2 on Cx43 phosphorylation and permeability. Because the ε-isoform of PKC localizes to plasma membrane sites, we examined whether it is directly involved in the FGF-2–induced Cx43 phosphorylation. In nonstimulated myocytes, PKCε displayed a discontinuous pattern of localization at intercellular contact sites and partial colocalization with Cx43. Treatment with FGF-2 or phorbol 12-myristate 13-acetate induced a more continuous pattern of PKCε distribution, whereas the anti-Cx43 staining appeared to overlap extensively with that of PKCε. In immunoprecipitation experiments using specific anti-Cx43 antibodies, PKCε but not PKCα coprecipitated with Cx43. FGF-2 increased levels of coprecipitated PKCε, suggesting increased association between PKCε and Cx43 on stimulation. Transient gene transfer and overexpression of cDNAs coding for truncated or mutated dominant-negative forms of PKCε decreased cardiomyocyte Cx43 phosphorylation significantly. We conclude that PKC mediates the FGF-2–induced effects on cardiac GJs and that PKCε likely interacts with and phosphorylates cardiac Cx43 at sites of intercellular contact.

Published

2000

40. Exploring Pluripotency with Chemical Genetics

Author

Bradley W. Doble and James R. Woodgett

Subjects

Genetics, Pluripotent Stem Cells, Chemical biology, Regulator, Computational biology, Cell Biology, Biology, Article, Glycogen Synthase Kinase 3, GSK-3, biology.protein, Animals, Humans, Molecular Medicine, Enzyme Inhibitors, Glycogen synthase, Chemical genetics, beta Catenin, Signal Transduction

Abstract

In a recent issue of Chemistry & Biology, Bone et al. (2009) employed a chemical biology approach to probe the role of glycogen synthase kinase-3 (GSK-3), a key regulator of pluripotentiality, providing new insights and tools for modulating this process.

Published

2009

41. Cardiomyocyte Gap Junctions: A Target of Growth-Promoting Signaling

Author

Bradley W. Doble and Elissavet Kardami

Subjects

Gap junction, Connexin, Biology, Cell biology, medicine.anatomical_structure, cardiovascular system, medicine, Phosphorylation, Membrane channel, sense organs, Signal transduction, Cardiology and Cardiovascular Medicine, Fibroblast, Intracellular, Transforming growth factor

Abstract

Gap junctions (GJ), composed of connexins, are membrane channels that connect and enable communication between neighboring cells and which, in addition to being essential for the coordinated electrical and contractile activity of the heart, may regulate intercellular transmission of signals affecting proliferative growth. Alterations in GJ permeability that have been associated with the regulation of growth can occur acutely through phosphorylation of connexins: fibroblast growth factor-2 (FGF-2) causes decreased coupling and increased phosphorylation of a major cardiomyocyte connexin, connexin43 (Cx43), while stimulating proliferation of cardiomyocytes. On the other hand, transforming growth factor-β (TGFβ) prevents the effects of FGF-2 on Cx43 phosphorylation, as well as canceling the FGF-2-induced proliferation. Parallel to its link with growth regulation, Cx43 phosphorylation emerges as a functionally important end point for delineating cardiac signal transduction pathways elicited by diverse physiologic or pathologic stimuli.

Published

1998

42. Selective Monoclonal Antibody Recognition and Cellular Localization of an Unphosphorylated Form of Connexin43

Author

Elliot L. Hertzberg, James I. Nagy, Elissavet Kardami, W.E.I. Li, C. Roy, J.S. Gilchrist, and Bradley W. Doble

Subjects

medicine.drug_class, Blotting, Western, Muscle Fibers, Skeletal, Fluorescent Antibody Technique, Biology, Monoclonal antibody, Epitope, Rats, Sprague-Dawley, Dogs, Antibody Specificity, medicine, Animals, Phosphorylation, Microscopy, Immunoelectron, Cells, Cultured, Cellular localization, Myocardium, Gap junction, Antibodies, Monoclonal, Gap Junctions, Muscle, Smooth, Cell Biology, Molecular biology, Rats, Trachea, Polyclonal antibodies, Connexin 43, cardiovascular system, biology.protein, Rabbits, sense organs, Antibody, Immunostaining

Abstract

A sequence-specific monoclonal antibody directed against the gap junction protein connexin43 (Cx43) is shown here to be specific for the unphosphorylated form of this protein. In tissues and cultured cells containing different phosphorylated and unphosphorylated forms of Cx43, the antibody detected only the latter as shown by Western blotting of native and alkaline phosphatase-treated samples. Immunohistochemically, this monoclonal antibody did not recognize gap junctions in the vast majority of cultured cardiac myocytes, where nearly all detectable Cx43 is phosphorylated. In contrast, it was able to detect some intracellular Cx43 in tracheal smooth muscle cells and an epithelial cell line (Cl-9 cells), producing patterns of labeling consistent with those seen using a polyclonal antibody that recognizes both phosphorylated and unphosphorylated forms of Cx43. Immunostaining of gap junctions in the cultured cells indicates that both phosphorylated and unphosphorylated Cx43 are present in some assembled gap junctions, suggesting that assembled junctions do not contain exclusively the phosphorylated form of the protein. Annular gap junctions, believed to form as part of the pathway for internalization and degradation of gap junctions, were only occasionally and sparsely labeled by the monoclonal antibody, indicating that complete protein dephosphorylation is not required for uptake and degradation of gap junctions. Furthermore, the ability of this antibody to recognize only unphosphorylated Cx43, and not any of the phosphorylated forms present in the tissues and cell types examined, suggests that a unique phosphorylation site, perhaps present in the epitope recognized by this antibody, must be phosphorylated prior to phosphorylation of Cx43 at other sites.

Published

1997

43. Ectopic γ-catenin expression partially mimics the effects of stabilized β-catenin on embryonic stem cell differentiation

Author

Austin J. Cooney, Kevin F. Kelly, Bradley W. Doble, Sabrina Paez-Parent, Sujeivan Mahendram, Enio Polena, and Sharmeen Mahmood

Subjects

Anatomy and Physiology, Mouse, Cellular differentiation, Gene Expression, lcsh:Medicine, TCF/LEF family, Cell Fate Determination, Glycogen Synthase Kinase 3, Mice, 0302 clinical medicine, Molecular Cell Biology, Signaling in Cellular Processes, lcsh:Science, Wnt Signaling Pathway, beta Catenin, Mice, Knockout, Neurons, Regulation of gene expression, 0303 health sciences, Multidisciplinary, Protein Stability, Stem Cells, Mechanisms of Signal Transduction, Wnt signaling pathway, Cell Differentiation, Animal Models, Beta-Catenin Signaling, Nuclear Signaling, Cell biology, Protein Transport, Gene Knockdown Techniques, 030220 oncology & carcinogenesis, TCF Transcription Factors, Research Article, Signal Transduction, Cell Physiology, Beta-catenin, Adhesion Molecules, Cell Potency, Plakoglobin, Biology, Signaling Pathways, Cell Line, Adherens junction, Catenin Signal Transduction, 03 medical and health sciences, Model Organisms, Animals, Humans, Embryonic Stem Cells, 030304 developmental biology, lcsh:R, Molecular Development, Molecular biology, Signaling, Gene Expression Regulation, Catenin, biology.protein, lcsh:Q, Transcriptional Signaling, gamma Catenin, Developmental Biology

Abstract

β-catenin, an adherens junction component and key Wnt pathway effector, regulates numerous developmental processes and supports embryonic stem cell (ESC) pluripotency in specific contexts. The β-catenin homologue γ-catenin (also known as Plakoglobin) is a constituent of desmosomes and adherens junctions and may participate in Wnt signaling in certain situations. Here, we use β-catenin((+/+)) and β-catenin((-/-)) mouse embryonic stem cells (mESCs) to investigate the role of γ-catenin in Wnt signaling and mESC differentiation. Although γ-catenin protein is markedly stabilized upon inhibition or ablation of GSK-3 in wild-type (WT) mESCs, efficient silencing of its expression in these cells does not affect β-catenin/TCF target gene activation after Wnt pathway stimulation. Nonetheless, knocking down γ-catenin expression in WT mESCs appears to promote their exit from pluripotency in short-term differentiation assays. In β-catenin((-/-)) mESCs, GSK-3 inhibition does not detectably alter cytosolic γ-catenin levels and does not activate TCF target genes. Intriguingly, β-catenin/TCF target genes are induced in β-catenin((-/-)) mESCs overexpressing stabilized γ-catenin and the ability of these genes to be activated upon GSK-3 inhibition is partially restored when wild-type γ-catenin is overexpressed in these cells. This suggests that a critical threshold level of total catenin expression must be attained before there is sufficient signaling-competent γ-catenin available to respond to GSK-3 inhibition and to regulate target genes as a consequence. WT mESCs stably overexpressing γ-catenin exhibit robust Wnt pathway activation and display a block in tri-lineage differentiation that largely mimics that observed upon overexpression of β-catenin. However, β-catenin overexpression appears to be more effective than γ-catenin overexpression in sustaining the retention of markers of naïve pluripotency in cells that have been subjected to differentiation-inducing conditions. Collectively, our study reveals a function for γ-catenin in the regulation of mESC differentiation and has implications for human cancers in which γ-catenin is mutated and/or aberrantly expressed.

Published

2013

44. MB-22ACTIVATED Wnt SIGNALING FOR THE THERAPEUTIC TARGETING OF TREATMENT-REFRACTORY MEDULLOBLASTOMA STEM CELLS

Author

Sujeivan Mahendram, Michelle Kameda-Smith, Bradley W. Doble, Sheila K. Singh, Chitra Venugopal, Branavan Manoranjan, and David Bakhshinyan

Subjects

Medulloblastoma, Cancer Research, business.industry, Treatment refractory, Wnt signaling pathway, Therapeutic targeting, medicine.disease, Abstracts, Text mining, Oncology, medicine, Cancer research, Neurology (clinical), Signal transduction, Stem cell, business

Published

2016

45. Medulloblastoma stem cells: modeling tumor heterogeneity

Author

Katrin Scheinemann, Branavan Manoranjan, Chitra Venugopal, Sheila K. Singh, Nicole McFarlane, Sandra E. Dunn, and Bradley W. Doble

Subjects

Medulloblastoma, Cancer Research, Pathology, medicine.medical_specialty, Models, Genetic, Childhood cancer, Biology, medicine.disease, Tumor heterogeneity, Molecular heterogeneity, Gene Expression Regulation, Neoplastic, Genetic Heterogeneity, Oncology, Cancer stem cell, medicine, Neoplastic Stem Cells, Humans, Signal transduction, Stem cell, Cerebellar Neoplasms, Child, Childhood brain tumor, Cell Proliferation, Signal Transduction

Abstract

Brain tumors represent the leading cause of childhood cancer mortality, with medulloblastoma (MB) being the most frequent malignant tumor. In this review we discuss the morphological and molecular heterogeneity of this malignant childhood brain tumor and how this key feature has implicated the presence of a MB stem cell. We focus on evidence from cerebellar development, histopathological and molecular subtypes of MB, the recent identification of brain tumor-initiating cells (BTICs, also referred to as MB stem cells), and the current limitations in studying the interplay between MB stem cells and tumor heterogeneity.

Published

2012

46. Medulloblastoma stem cells: where development and cancer cross pathways

Author

Branavan Manoranjan, Chitra Venugopal, Nicole McFarlane, Sandra E. Dunn, Sheila K. Singh, Bradley W. Doble, and Katrin Scheinemann

Subjects

Context (language use), Biology, medicine.disease_cause, Models, Biological, Pediatrics, Cancer stem cell, Cerebellum, medicine, Humans, Hedgehog Proteins, Epigenetics, Sonic hedgehog, Cerebellar Neoplasms, Child, Medulloblastoma, Wnt signaling pathway, medicine.disease, Wnt Proteins, Cell Transformation, Neoplastic, Pediatrics, Perinatology and Child Health, Immunology, Cancer research, biology.protein, Neoplastic Stem Cells, Stem cell, Carcinogenesis, Signal Transduction

Abstract

Brain tumors are the leading cause of childhood cancer mortality, with medulloblastoma (MB) representing the most frequent malignant tumor. The recent molecular classification of MB has reconceptualized the heterogeneity that exists within pathological subtypes by giving context to the role of key developmental signaling pathways in MB pathogenesis. The identification of cancer stem cell (CSC) populations, termed brain tumor-initiating cells (BTICs), in MB has provided novel cellular targets for the study of these aberrantly activated signaling pathways, namely, Sonic hedgehog (Shh) and Wingless (Wnt), along with the identification of novel BTIC self-renewal pathways. In this review, we discuss recent evidence for the presence of a MB stem cell that drives tumorigenesis in this malignant childhood tumor. We focus on evidence from cerebellar development, the recent identification of BTICs, the presence of activated developmental signaling pathways in MB, the role of epigenetic stem cell regulatory mechanisms, and how these developmental and epigenetic pathways may be targeted for novel therapeutic options.

Published

2012

47. Over-expression of CUG- or AUG-initiated Forms of Basic Fibroblast Growth Factor in Cardiac Myocytes Results in Similar Effects on Mitosis and Protein Synthesis but Distinct Nuclear Morphologies

Author

Elissavet Kardami, Peter A. Cattini, Bradley W. Doble, and Kishore B.S. Pasumarthi

Subjects

DNA Replication, DNA, Complementary, Recombinant Fusion Proteins, Molecular Sequence Data, Basic fibroblast growth factor, Mitosis, Muscle Proteins, Chick Embryo, Biology, Transfection, chemistry.chemical_compound, Species Specificity, Myosin, Genes, Synthetic, Protein biosynthesis, Animals, Myocyte, Amino Acid Sequence, Codon, Peptide Chain Initiation, Translational, Molecular Biology, Cells, Cultured, Cell Nucleus, Messenger RNA, Sequence Homology, Amino Acid, DNA synthesis, Myocardium, Cardiac myocyte, Molecular biology, Rats, Molecular Weight, Gene Expression Regulation, Microscopy, Fluorescence, chemistry, cardiovascular system, Fibroblast Growth Factor 2, Rabbits, Cardiology and Cardiovascular Medicine, Thymidine, Sequence Alignment

Abstract

Initiation of translation from alternate codons in the same mRNA results in multiple forms of basic fibroblast growth factor (bFGF). High molecular weight species of bFGF make use of leucine translation initiation sites located upstream of the methionine residue used to produce the 18 kiloDalton (kDa) form. Although the addition of exogenous 18 kDa bFGF is known to stimulate DNA synthesis and proliferation of several cell types including embryonic chicken cardiac myocytes, little is known about the role of high molecular weight forms of bFGF. We modified the rat bFGF cDNA to yield high (22/21.5 kDa) or low (18 kDa) molecular weight species of bFGF. Expression of 22/21.5 kDa or 18 kDa bFGF in transfected embryonic chicken ventricular myocyte cultures was confirmed by protein blotting. Expression of both high and low molecular weight species of bFGF was associated with (i) a three-fold increase in overall thymidine incorporation as well as cardiomyocyte labelling index (fraction of cardiomyocyte nuclei incorporating tritiated thymidine); (ii) a two- to three-fold increase in cell number; (iii) an eight-fold increase in protein synthesis; and (iv) a three-fold decrease in myosin accumulation. Subcellular localization of bFGF in the transfected myocyte cultures was also assessed by immunofluorescence microscopy. Over-expression of cDNAs yielding high molecular weight bFGF resulted in predominantly nuclear bFGF staining. By contrast, both cytoplasmic and nuclear staining were observed following over-expression of 18 kDa bFGF. Over-expression of 22/21.5 kDa bFGF was associated with the formation of multiple DNA-containing "clumps" resembling condensed chromatin in cardiac myocyte nuclei. These DNA "clumps" were not observed in cardiac myocyte cultures over-expressing 18 kDa bFGF. These data indicate that over-expression of high as well as low molecular weight forms of bFGF can stimulate cardiac myocyte proliferative potential and decrease myosin accumulation. However, these forms possess distinct subcellular localizations and can have different biological functions in the nucleus.

Published

1994

48. Molecular Mechanisms Underlying Pluripotency and Lineage Commitment – The Role of GSK-3

Author

Bradley W. Doble, Kevin F. Kelly, and James R. Woodgett

Subjects

0303 health sciences, Lineage commitment, Kinase, Mechanism (biology), Wnt signaling pathway, macromolecular substances, Biology, Embryonic stem cell, Cell biology, Serine, 03 medical and health sciences, 0302 clinical medicine, GSK-3, Induced pluripotent stem cell, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

The highly related serine/threonine kinases GSK3┙ and GSK3┚ are transducers of Wnt/┚catenin, PI-3K, Notch and Hedgehog signalling pathways, placing them at the hub of key developmental and metabolic processes. There is accumulating evidence suggesting that GSK-3 inhibitors aid in the acquisition or sustenance of pluripotency in embryonic stem cells of mouse, rat and human origin. However, the mechanism through which GSK-3 inhibitors impart their effects is unclear due to the myriad cellular processes in which GSK-3 plays a role. Here, we review the studies that have examined the consequences of GSK-3 inhibition in pluripotent stem cells with a focus on key signalling pathways, which have been implicated in GSK-3 inhibitor-mediated effects.

Published

2011

49. GSK-3α directly regulates β-adrenergic signaling and the response of the heart to hemodynamic stress in mice

Author

Bradley W. Doble, Hind Lal, Risto Kerkelä, Morgan DeCaul, Jianliang Song, Yingxin Li, Erhe Gao, Katrina MacAulay, Thomas Force, Xiying Shang, Jibin Zhou, John L. Farber, Xiongwen Chen, Walter J. Koch, and James R. Woodgett

Subjects

medicine.medical_specialty, Cardiomegaly, Biology, Protein Serine-Threonine Kinases, Muscle hypertrophy, Glycogen Synthase Kinase 3, Mice, Norepinephrine, Adrenergic Agents, GSK-3, Internal medicine, medicine, Myocyte, Animals, Protein Isoforms, Myocytes, Cardiac, Glycogen synthase, GSK3B, Mice, Knockout, Glycogen Synthase Kinase 3 beta, Kinase, Hemodynamics, Gene targeting, Heart, General Medicine, Hypertrophy, Endocrinology, biology.protein, Signal transduction, Research Article, Signal Transduction

Abstract

The glycogen synthase kinase-3 (GSK-3) family of serine/threonine kinases consists of 2 highly related isoforms, alpha and beta. Although GSK-3beta has an important role in cardiac development, much remains unknown about the function of either GSK-3 isoform in the postnatal heart. Herein, we present what we believe to be the first studies defining the role of GSK-3alpha in the mouse heart using gene targeting. Gsk3a(-/-) mice over 2 months of age developed progressive cardiomyocyte and cardiac hypertrophy and contractile dysfunction. Following thoracic aortic constriction in young mice, we observed enhanced hypertrophy that rapidly transitioned to ventricular dilatation and contractile dysfunction. Surprisingly, markedly impaired beta-adrenergic responsiveness was found at both the organ and cellular level. This phenotype was reproduced by acute treatment of WT cardiomyocytes with a small molecule GSK-3 inhibitor, confirming that the response was not due to a chronic adaptation to LV dysfunction. Thus, GSK-3alpha appears to be the central regulator of a striking range of essential processes, including acute and direct positive regulation of beta-adrenergic responsiveness. In the absence of GSK-3alpha, the heart cannot respond effectively to hemodynamic stress and rapidly fails. Our findings identify what we believe to be a new paradigm of regulation of beta-adrenergic signaling and raise concerns given the rapid expansion of drug development targeting GSK-3.

Published

2010

50. Abnormalities in brain structure and behavior in GSK-3alpha mutant mice

Author

Oksana Kaidanovich-Beilin, Mustafa Khan, James R. Woodgett, Paul J. Fletcher, R. Mark Henkelman, John C. Roder, Tatiana V. Lipina, Matthijs C. van Eede, Tsuyoshi Miyakawa, Kenichi Okamoto, John W. Chambers, Satoko Hattori, Christine L. Laliberté, Keizo Takao, Katrina MacAulay, and Bradley W. Doble

Subjects

Memory, Long-Term, Emotions, Mutant, macromolecular substances, Biology, lcsh:RC346-429, Serine, Glycogen Synthase Kinase 3, Mice, Mice, Neurologic Mutants, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Neurochemical, GSK-3, Animals, Threonine, Social Behavior, Glycogen synthase, Protein kinase A, Gene, Molecular Biology, lcsh:Neurology. Diseases of the nervous system, 030304 developmental biology, Mice, Knockout, Neurotransmitter Agents, 0303 health sciences, Behavior, Animal, Depression, Research, Brain, Magnetic Resonance Imaging, Cell biology, Aggression, Mice, Inbred C57BL, biology.protein, Female, Neuroscience, 030217 neurology & neurosurgery

Abstract

Background Glycogen synthase kinase-3 (GSK-3) is a widely expressed and highly conserved serine/threonine protein kinase encoded by two genes that generate two related proteins: GSK-3α and GSK-3β. Mice lacking a functional GSK-3α gene were engineered in our laboratory; they are viable and display insulin sensitivity. In this study, we have characterized brain functions of GSK-3α KO mice by using a well-established battery of behavioral tests together with neurochemical and neuroanatomical analysis. Results Similar to the previously described behaviours of GSK-3β+/-mice, GSK-3α mutants display decreased exploratory activity, decreased immobility time and reduced aggressive behavior. However, genetic inactivation of the GSK-3α gene was associated with: decreased locomotion and impaired motor coordination, increased grooming activity, loss of social motivation and novelty; enhanced sensorimotor gating and impaired associated memory and coordination. GSK-3α KO mice exhibited a deficit in fear conditioning, however memory formation as assessed by a passive avoidance test was normal, suggesting that the animals are sensitized for active avoidance of a highly aversive stimulus in the fear-conditioning paradigm. Changes in cerebellar structure and function were observed in mutant mice along with a significant decrease of the number and size of Purkinje cells. Conclusion Taken together, these data support a role for the GSK-3α gene in CNS functioning and possible involvement in the development of psychiatric disorders.

Published

2009