Your search keyword '"Fabian V. Filipp"' showing total 69 results

1. Quiescence and aging of melanocyte stem cells and a novel association with programmed death-ligand 1

Author

Joseph W. Palmer, Kyrene M. Villavicencio, Misgana Idris, Ian J. Baranyk, Nunaya Polycarp, Alex D. Dawson, Dominique Weddle, William J. Pavan, Fabian V. Filipp, and Melissa L. Harris

Subjects

Stem cells research, Functional aspects of cell biology, Science

Abstract

Summary: Cellular quiescence is a reversible and tightly regulated stem cell function essential for healthy aging. However, the elements that control quiescence during aging remain poorly defined. Using melanocyte stem cells (McSCs), we find that stem cell quiescence is neither passive nor static. For example, gene expression profiling of the transition from proliferating melanoblasts to quiescent melanocyte stem cells reveals tissue-specific regulation of the immune checkpoint protein PD-L1. In vitro, quiescence assays demonstrate that PD-L1 expression is a physiological attribute of quiescence in this cell lineage and reinforces this cell state. In vivo, a subset of quiescent McSCs is marked by PD-L1. While the overall number of McSCs decreases with age, PD-L1+ McSCs appear resistant to depletion. This phenomenon coincides with an aged McSC pool that exhibits a deeper transcriptomic quiescence. We predict that quiescent PD-L1+ stem cells retained with age may serve as cellular targets for reactivation.

Published

2024

2. Bromodomain and extra-terminal domain (BET) proteins regulate melanocyte differentiation

Author

Archit Trivedi, Aanchal Mehrotra, Caitlin E. Baum, Brandon Lewis, Tupa Basuroy, Thomas Blomquist, Robert Trumbly, Fabian V. Filipp, Vijayasaradhi Setaluri, and Ivana L. de la Serna

Subjects

Bromodomain and extra-terminal domain, BET, JQ1, BRD4, MITF, ChIP-Seq, Genetics, QH426-470

Abstract

Abstract Background Pharmacologic inhibition of bromodomain and extra-terminal (BET) proteins is currently being explored as a new therapeutic approach in cancer. Some studies have also implicated BET proteins as regulators of cell identity and differentiation through their interactions with lineage-specific factors. However, the role of BET proteins has not yet been investigated in melanocyte differentiation. Melanocyte inducing transcription factor (MITF) is the master regulator of melanocyte differentiation, essential for pigmentation and melanocyte survival. In this study, we tested the hypothesis that BET proteins regulate melanocyte differentiation through interactions with MITF. Results Here we show that chemical inhibition of BET proteins prevents differentiation of unpigmented melanoblasts into pigmented melanocytes and results in de-pigmentation of differentiated melanocytes. BET inhibition also slowed cell growth, without causing cell death, increasing the number of cells in G1. Transcriptional profiling revealed that BET inhibition resulted in decreased expression of pigment-specific genes, including many MITF targets. The expression of pigment-specific genes was also down-regulated in melanoma cells, but to a lesser extent. We found that RNAi depletion of the BET family members, bromodomain-containing protein 4 (BRD4) and bromodomain-containing protein 2 (BRD2) inhibited expression of two melanin synthesis enzymes, TYR and TYRP1. Both BRD4 and BRD2 were detected on melanocyte promoters surrounding MITF-binding sites, were associated with open chromatin structure, and promoted MITF binding to these sites. Furthermore, BRD4 and BRD2 physically interacted with MITF. Conclusion These findings indicate a requirement for BET proteins in the regulation of pigmentation and melanocyte differentiation. We identified changes in pigmentation specific gene expression that occur upon BET inhibition in melanoblasts, melanocytes, and melanoma cells.

Published

2020

3. Evaluation of integrin αvβ6 cystine knot PET tracers to detect cancer and idiopathic pulmonary fibrosis

Author

Richard H. Kimura, Ling Wang, Bin Shen, Li Huo, Willemieke Tummers, Fabian V. Filipp, Haiwei Henry Guo, Thomas Haywood, Lotfi Abou-Elkacem, Lucia Baratto, Frezghi Habte, Rammohan Devulapally, Timothy H. Witney, Yan Cheng, Suhas Tikole, Subhendu Chakraborti, Jay Nix, Christopher A. Bonagura, Negin Hatami, Joshua J. Mooney, Tushar Desai, Scott Turner, Richard S. Gaster, Andrea Otte, Brendan C. Visser, George A. Poultsides, Jeffrey Norton, Walter Park, Mark Stolowitz, Kenneth Lau, Eric Yang, Arutselvan Natarajan, Ohad Ilovich, Shyam Srinivas, Ananth Srinivasan, Ramasamy Paulmurugan, Juergen Willmann, Frederick T. Chin, Zhen Cheng, Andrei Iagaru, Fang Li, and Sanjiv S. Gambhir

Subjects

Science

Abstract

Knottin is a cystine knot peptide. Here, the authors develop a knottin-based tracer for positron emission tomography and demonstrate its ability to detect cancer and idiopathic pulmonary fibrosis through selective binding to integrin αvβ6.

Published

2019

4. The triennial International Pigment Cell Conference (IPCC)

Author

Neil F. Box, Lionel Larue, Prashiela Manga, Lluis Montoliu, Richard A. Spritz, and Fabian V. Filipp

Subjects

Melanocyte, Melanin, Melanoma, Melasma, Albinism, Vitiligo, Medicine

Abstract

Abstract The International Federation of Pigment Cell Societies (IFPCS) held its XXIII triennial International Pigment Cell Conference (IPCC) in Denver, Colorado in August 2017. The goal of the summit was to provide a venue promoting a vibrant interchange among leading basic and clinical researchers working on leading-edge aspects of melanocyte biology and disease. The philosophy of the meeting, entitled Breakthroughs in Pigment Cell and Melanoma Research, was to deliver a comprehensive program in an inclusive environment fostering scientific exchange and building new academic bridges. This document provides an outlook on the history, accomplishments, and sustainability of the pigment cell and melanoma research community. Shared progress in the understanding of cellular homeostasis of pigment cells but also clinical successes and hurdles in the treatment of melanoma and dermatological disorders continue to drive future research activities. A sustainable direction of the societies creates an international forum identifying key areas of imminent needs in laboratory research and clinical care and ensures the future of this vibrant, diverse and unique research community at the same time. Important advances showcase wealth and breadth of the field in melanocyte and melanoma research and include emerging frontiers in melanoma immunotherapy, medical and surgical oncology, dermatology, vitiligo, albinism, genomics and systems biology, precision bench-to-bedside approaches, epidemiology, pigment biophysics and chemistry, and evolution. This report recapitulates highlights of the federate meeting agenda designed to advance clinical and basic research frontiers from melanoma and dermatological sciences followed by a historical perspective of the associated societies and conferences.

Published

2018

5. Metabolic shift in density-dependent stem cell differentiation

Author

Simar J. Singh, William Turner, Drew E. Glaser, Kara E. McCloskey, and Fabian V. Filipp

Subjects

Stem cells, Differentiation, Vascular fate, Cell seeding density, Systems biology, Metabolism, Medicine, Cytology, QH573-671

Abstract

Abstract Background Vascular progenitor cells (VPCs) derived from embryonic stem cells (ESCs) are a valuable source for cell- and tissue-based therapeutic strategies. During the optimization of endothelial cell (EC) inductions from mouse ESCs using our staged and chemically-defined induction methods, we found that cell seeding density but not VEGF treatment between 10 ng/mL and 40 ng/mL was a significant variable directing ESCs into FLK1+ VPCs during stage 1 induction. Here, we examine potential contributions from cell-to-cell signaling or cellular metabolism in the production of VPCs from ESCs seeded at different cell densities. Methods Using 1D 1H-NMR spectroscopy, transcriptomic arrays, and flow cytometry, we observed that the density-dependent differentiation of ESCs into FLK1+ VPCs positively correlated with a shift in metabolism and cellular growth. Results Specifically, cell differentiation correlated with an earlier plateauing of exhaustive glycolysis, decreased lactate production, lower metabolite consumption, decreased cellular proliferation and an increase in cell size. In contrast, cells seeded at a lower density of 1,000 cells/cm2 exhibited increased rates of glycolysis, lactate secretion, metabolite utilization, and proliferation over the same induction period. Gene expression analysis indicated that high cell seeding density correlated with up-regulation of several genes including cell adhesion molecules of the notch family (NOTCH1 and NOTCH4) and cadherin family (CDH5) related to vascular development. Conclusions These results confirm that a distinct metabolic phenotype correlates with cell differentiation of VPCs.

Published

2017

6. Somatic Copy Number Amplification and Hyperactivating Somatic Mutations of EZH2 Correlate With DNA Methylation and Drive Epigenetic Silencing of Genes Involved in Tumor Suppression and Immune Responses in Melanoma

Author

Jessamy Tiffen, Stephen Wilson, Stuart J. Gallagher, Peter Hersey, and Fabian V. Filipp

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The epigenetic modifier EZH2 is in the center of a repressive complex controlling differentiation of normal cells. In cancer EZH2 has been implicated in silencing tumor suppressor genes. Its role in melanoma as well as target genes affected by EZH2 are poorly understood. In view of this we have used an integrated systems biology approach to analyze 471 cases of skin cutaneous melanoma (SKCM) in The Cancer Genome Atlas (TCGA) for mutations and amplifications of EZH2. Identified changes in target genes were validated by interrogation of microarray data from melanoma cells treated with the EZH2 inhibitor GSK126. We found that EZH2 activation by mutations, gene amplification and increased transcription occurred in about 20% of the cohort. These alterations were associated with significant hypermethylation of DNA and significant downregulation of 11% of transcripts in patient RNASeq data. GSK126 treatment of melanoma lines containing EZH2 activation reversed such transcriptional repression in 98 candidate target genes. Gene enrichment analysis revealed genes associated with tumor suppression, cell differentiation, cell cycle inhibition and repression of metastases as well as antigen processing and presentation pathways. The identified changes in EZH2 were associated with an adverse prognosis in the TCGA dataset. These results suggest that inhibiting of EZH2 is a promising therapeutic avenue for a substantial fraction of melanoma patients.

Published

2016

7. Unusual binding of ursodeoxycholic acid to ileal bile acid binding protein: role in activation of FXRα

Author

Changming Fang, Fabian V. Filipp, and Jeffrey W. Smith

Subjects

farnesoid X receptor α, colorectal cancer, bile salts, Biochemistry, QD415-436

Abstract

Ursodeoxycholic acid (UDCA, ursodiol) is used to prevent damage to the liver in patients with primary biliary cirrhosis. The drug also prevents the progression of colorectal cancer and the recurrence of high-grade colonic dysplasia. However, the molecular mechanism by which UDCA elicits its beneficial effects is not entirely understood. The aim of this study was to determine whether ileal bile acid binding protein (IBABP) has a role in mediating the effects of UDCA. We find that UDCA binds to a single site on IBABP and increases the affinity for major human bile acids at a second binding site. As UDCA occupies one of the bile acid binding sites on IBABP, it reduces the cooperative binding that is often observed for the major human bile acids. Furthermore, IBABP is necessary for the full activation of farnesoid X receptor α (FXRα) by bile acids, including UDCA. These observations suggest that IBABP may have a role in mediating some of the intestinal effects of UDCA.

Published

2012

8. Epigenetic and pharmacological control of pigmentation via Bromodomain Protein 9 (BRD9)

Author

Tupa Basuroy, Megan Dreier, Caitlin Baum, Thomas Blomquist, Robert Trumbly, Fabian V. Filipp, and Ivana L. de la Serna

Subjects

Oncology, Brd9, Swi/snf, Bromodomain, Chromatin Remodeling, Epigenetic, Melanocyte Differentiation, Melanoma, Pigmentation, Dermatology, General Biochemistry, Genetics and Molecular Biology

Abstract

Lineage-specific differentiation programs are activated by epigenetic changes in chromatin structure. Melanin-producing melanocytes maintain a gene expression program ensuring appropriate enzymatic conversion of metabolites into the pigment, melanin, and transfer to surrounding cells. During neuroectodermal development, SMARCA4 (BRG1), the catalytic subunit of SWItch/Sucrose Non-Fermentable (SWI/SNF) chromatin remodeling complexes, is essential for lineage specification. SMARCA4 is also required for development of multipotent neural crest precursors into melanoblasts, which differentiate into pigment-producing melanocytes. In addition to the catalytic domain, SMARCA4 and several SWI/SNF subunits contain bromodomains which are amenable to pharmacological inhibition. We investigated the effects of pharmacological inhibitors of SWI/SNF bromodomains on melanocyte differentiation. Strikingly, treatment of murine melanoblasts and human neonatal epidermal melanocytes with selected bromodomain inhibitors abrogated melanin synthesis and visible pigmentation. Using functional genomics, iBRD9, a small molecule selective for the bromodomain of BRD9 was found to repress pigmentation-specific gene expression. Depletion of BRD9 confirmed a requirement for expression of pigmentation genes in the differentiation program from melanoblasts into pigmented melanocytes and in melanoma cells. Chromatin immunoprecipitation assays showed that iBRD9 disrupts the occupancy of BRD9 and the catalytic subunit SMARCA4 at melanocyte-specific loci. These data indicate that BRD9 promotes melanocyte pigmentation whereas pharmacological inhibition of BRD9 is repressive.

Published

2023

9. Bromodomain and extra-terminal domain (BET) proteins regulate melanocyte differentiation

Author

Vijayasaradhi Setaluri, Caitlin E. Baum, Ivana L. de la Serna, Brandon Lewis, Thomas M. Blomquist, Tupa Basuroy, Robert J. Trumbly, Archit R. Trivedi, Aanchal Mehrotra, and Fabian V. Filipp

Subjects

Epigenomics, Bromodomain And Extra-terminal Domain, Bet, Jq1, Brd4, Mitf, Chip-seq, Systems Biology, Melanocyte Differentiation, Melanoma, Pigmentation, Transcriptional Networks, Cell Cycle Proteins, ChIP-Seq, 0302 clinical medicine, Melanocyte differentiation, Gene expression, TYRP1, Promoter Regions, Genetic, Cells, Cultured, Transcriptional networks, 0303 health sciences, Membrane Glycoproteins, Monophenol Monooxygenase, Cell Differentiation, hemic and immune systems, Microphthalmia-associated transcription factor, 3. Good health, Cell biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Melanocytes, BRD4, Systems biology, Oxidoreductases, Protein Binding, lcsh:QH426-470, JQ1, chemical and pharmacologic phenomena, Biology, Melanocyte, 03 medical and health sciences, Genetics, medicine, Humans, Molecular Biology, Transcription factor, 030304 developmental biology, Melanins, Microphthalmia-Associated Transcription Factor, MITF, Bromodomain and extra-terminal domain, Research, BET, Bromodomain, lcsh:Genetics, HEK293 Cells, Transcription Factors

Abstract

BackgroundPharmacologic inhibition of bromodomain and extra-terminal (BET) proteins is currently being explored as a new therapeutic approach in cancer. Some studies have also implicated BET proteins as regulators of cell identity and differentiation through their interactions with lineage-specific factors. However, the role of BET proteins has not yet been investigated in melanocyte differentiation. Melanocyte inducing transcription factor (MITF) is the master regulator of melanocyte differentiation, essential for pigmentation and melanocyte survival. In this study, we tested the hypothesis that BET proteins regulate melanocyte differentiation through interactions with MITF.ResultsHere we show that chemical inhibition of BET proteins prevents differentiation of unpigmented melanoblasts into pigmented melanocytes and results in de-pigmentation of differentiated melanocytes. BET inhibition also slowed cell growth, without causing cell death, increasing the number of cells in G1. Transcriptional profiling revealed that BET inhibition resulted in decreased expression of pigment-specific genes, including many MITF targets. The expression of pigment-specific genes was also down-regulated in melanoma cells, but to a lesser extent. We found that RNAi depletion of the BET family members, bromodomain-containing protein 4 (BRD4) and bromodomain-containing protein 2 (BRD2) inhibited expression of two melanin synthesis enzymes, TYR and TYRP1. Both BRD4 and BRD2 were detected on melanocyte promoters surrounding MITF-binding sites, were associated with open chromatin structure, and promoted MITF binding to these sites. Furthermore, BRD4 and BRD2 physically interacted with MITF.ConclusionThese findings indicate a requirement for BET proteins in the regulation of pigmentation and melanocyte differentiation. We identified changes in pigmentation specific gene expression that occur upon BET inhibition in melanoblasts, melanocytes, and melanoma cells.

Published

2020

10. Opportunities for Artificial Intelligence in Advancing Precision Medicine

Author

Fabian V. Filipp

Subjects

FOS: Computer and information sciences, 0301 basic medicine, Computer Science - Machine Learning, Computer Science - Artificial Intelligence, Computer science, Molecular Networks (q-bio.MN), Systems biology, Big data, Article, Machine Learning (cs.LG), Spatial transcriptomics, 03 medical and health sciences, 0302 clinical medicine, DL, Machine learning, Digital pathology, Quantitative Biology - Genomics, Quantitative Biology - Molecular Networks, Cluster analysis, Biomedicine, Ai, Dl, Dnn, Deep Learning, Digital Health, Digital Pathology, Ml, Machine Learning, Multi-omics, Precision Medicine, Single-cell Transcriptomics, Spatial Transcriptomics, Systems Biology, Genomics (q-bio.GN), business.industry, Deep learning, Precision medicine, Biomolecules (q-bio.BM), General Medicine, ML, Digital health, 3. Good health, Artificial Intelligence (cs.AI), ComputingMethodologies_PATTERNRECOGNITION, 030104 developmental biology, Quantitative Biology - Biomolecules, AI, FOS: Biological sciences, 030220 oncology & carcinogenesis, Artificial intelligence, business, Single-cell transcriptomics, DNN

Abstract

Purpose of Review We critically evaluate the future potential of machine learning (ML), deep learning (DL), and artificial intelligence (AI) in precision medicine. The goal of this work is to show progress in ML in digital health, to exemplify future needs and trends, and to identify any essential prerequisites of AI and ML for precision health. Recent Findings High-throughput technologies are delivering growing volumes of biomedical data, such as large-scale genome-wide sequencing assays; libraries of medical images; or drug perturbation screens of healthy, developing, and diseased tissue. Multi-omics data in biomedicine is deep and complex, offering an opportunity for data-driven insights and automated disease classification. Learning from these data will open our understanding and definition of healthy baselines and disease signatures. State-of-the-art applications of deep neural networks include digital image recognition, single-cell clustering, and virtual drug screens, demonstrating breadths and power of ML in biomedicine. Summary Significantly, AI and systems biology have embraced big data challenges and may enable novel biotechnology-derived therapies to facilitate the implementation of precision medicine approaches.

Published

2019

11. Down-regulation of FZD3 receptor suppresses growth and metastasis of human melanoma independently of canonical WNT signaling

Author

Alexander D. Boiko, Shawn Sharkas, Fabian V. Filipp, Kaitlyn N Clark, Tara Zahed, Chen Li, and Vincent Nguyen

Subjects

MAPK/ERK pathway, Frizzled, Medical Sciences, Down-Regulation, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, Cyclin-dependent kinase, melanoma, medicine, Humans, Neoplasm Invasiveness, Neoplasm Metastasis, frizzled, Wnt Signaling Pathway, Cell Proliferation, 030304 developmental biology, 0303 health sciences, Multidisciplinary, biology, Oncogene, Gene Expression Profiling, Melanoma, Wnt signaling pathway, Neural crest, systems biology, Biological Sciences, medicine.disease, MAPK, Frizzled Receptors, ddc, 3. Good health, Mapk, Systems Biology, Gene Expression, PNAS Plus, 030220 oncology & carcinogenesis, gene expression, Cancer research, biology.protein, Carcinogenesis

Abstract

Significance In malignant melanoma, one of the most aggressive cancers, the components of the WNT pathway are frequently deregulated and have been shown to drive self-renewal and metastatic progression of melanoma cells. Identifying tumorigenic properties of key members of the WNT signaling network in the pathogenesis of melanoma represents a pivotal task in the field and underlies successful design of targeted therapeutic approaches. In the present study, we characterized Frizzled 3 receptor (FZD3) as a critical factor underlying tumorigenic properties of aggressive human melanoma. Using in vivo and in vitro tumorigenic assays, combined with functional transcriptomics analysis of FZD3 knockdown in human patient-derived cells, we determined key signaling nodes regulated by FZD3 activity during malignant transformation., Frizzled 3 receptor (FZD3) plays an important role in the homeostasis of the neural crest and its derivatives, which give rise to pigment-synthesizing cells, melanocytes. While the role for FZD3 in specification of the melanocytic lineage from neural crest is well established, its significance in the formation of melanoma, its associated malignancy, is less understood. In this study we identified FZD3 as a critical regulator of human melanoma tumorigenesis. Down-regulation of FZD3 abrogated growth, colony-forming potential, and invasive capacity of patient-derived melanoma cells. Xenotransplantation of tumor cells with down-regulated FZD3 levels originating from melanomas carrying the BRAF(V600) mutation uniformly suppressed their capacity for tumor and metastasis formation. FZD3 knockdown leads to the down-regulation of the core cell cycle protein components (cyclins D1, E2, B1, and CDKs 1, 2, and 4) in melanomas with a hyperactive BRAF oncogene, indicating a dominant role of this receptor during melanoma pathogenesis. Enriched pathway analysis revealed that FZD3 inhibits transcriptional networks controlled by CREB5, FOXD1, and ATF3, which suppress the activity of MAPK-mediated signaling. Thus, FZD3 establishes a positive-feedback mechanism that activates MAPK signal transduction network, critical to melanoma carcinogenesis. Importantly, high levels of FZD3 mRNA were found to be correlated with melanoma advancement to metastatic stages and limited patient survival. Changes in gene-expression patterns mediated by FZD3 activity occur in the absence of nuclear β-catenin function, thus representing an important therapeutic target for the melanoma patients whose disease progresses independent of canonical WNT signaling.

Published

2019

12. Lipogenesis and innate immunity in hepatocellular carcinoma cells reprogrammed by an isoenzyme switch of hexokinases

Author

Marc-Thorsten Hütt, Keedrian I. Olmstead, Pierre-Olivier Vidalain, Rautureau Gjp, Rodrigue Rossignol, Fabian V. Filipp, Piotr Nyczka, Olivier Diaz, Lotteau, Baptiste Panthu, Laure Perrin-Cocon, Anne Aublin-Gex, Clémence Jacquemin, Patrice Andre, Nivea Dias Amoedo, Centre International de Recherche en Infectiologie - UMR (CIRI), École normale supérieure - Lyon (ENS Lyon)-Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Helmholtz Zentrum München Institute of Computational Biology Neuherberg, Germany, Cardiovasculaire, métabolisme, diabétologie et nutrition (CarMeN), Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Institut National des Sciences Appliquées de Lyon (INSA Lyon), Université de Lyon-Institut National des Sciences Appliquées (INSA)-Institut National des Sciences Appliquées (INSA)-Hospices Civils de Lyon (HCL)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE), Centre de RMN à très hauts champs de Lyon (CRMN), École normale supérieure - Lyon (ENS Lyon)-Centre National de la Recherche Scientifique (CNRS)-Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon, Jacobs University [Bremen], Cellomet [CHU Pellegrin, Bordeaux], CHU de Bordeaux Pellegrin [Bordeaux], Laboratoire Maladies Rares: Génétique et Métabolisme (Bordeaux) (U1211 INSERM/MRGM), Université de Bordeaux (UB)-Groupe hospitalier Pellegrin-Institut National de la Santé et de la Recherche Médicale (INSERM), Institut National de la Santé et de la Recherche Médicale (INSERM)-École normale supérieure - Lyon (ENS Lyon)-Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Centre National de la Recherche Scientifique (CNRS), Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE)-Université Claude Bernard Lyon 1 (UCBL), and Université de Lyon-Institut National des Sciences Appliquées (INSA)-Institut National des Sciences Appliquées (INSA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Hospices Civils de Lyon (HCL)

Subjects

0303 health sciences, Innate immune system, Glycogen, Glucokinase, [SDV]Life Sciences [q-bio], [SDV.CAN]Life Sciences [q-bio]/Cancer, [SDV.BC.BC]Life Sciences [q-bio]/Cellular Biology/Subcellular Processes [q-bio.SC], Biology, [SDV.IMM.II]Life Sciences [q-bio]/Immunology/Innate immunity, Isozyme, digestive system diseases, 3. Good health, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, Cell culture, 030220 oncology & carcinogenesis, Lipogenesis, Cancer research, Glycolysis, Secretion, 030304 developmental biology

Abstract

Hexokinases catalyze the first step of glycolysis by phosphorylating glucose. In the liver, normal hepatocytes express the low-affinity hexokinase 4, also known as glucokinase (GCK), which is adapting hepatocyte function to glycaemia. Conversely, hepatocellular carcinoma (HCC) cells express the high-affinity hexokinase 2 (HK2) to sustain tumor proliferation even at low glucose concentrations. A switch from GCK to HK2 isoenzymes is occurring during the transition from primary hepatocytes to HCC. HK2 induction is a recurrent event in the carcinogenic process and relates to the highly glycolytic phenotype of HCC but the consequence of GCK loss is unknown. To explore functional consequences of the GCK-to-HK2 isoenzyme switch, HK2 was knocked-out in the HCC cell line Huh7 and replaced by GCK, to generate the Huh7-GCK+/HK2- cell line. We then compared the transcriptomic, metabolomic and immunological profiles of both cell lines. The analysis of transcriptomic data from human HCC tumors shows that GCK and HK2 expression levels are inversely correlated and associated with patient survival. The replacement of HK2 by GCK rewired central carbon metabolism and restored some essential metabolic functions of normal hepatocytes such as lipogenesis, VLDL secretion and glycogen storage. It also reactivated innate immune responses and sensitivity to NK lysis. Our results suggest that the GCK-to-HK2 isoenzyme switch is playing a key role in dedifferentiation and immune escape of HCC cells.

Published

2020

13. Chemoprevention agents for melanoma: A path forward into phase 3 clinical trials

Author

Darrel L. Ellis, Maria L. Wei, Jennifer G. Powers, Svetomir N. Markovic, Jerry D. Brewer, Fabian V. Filipp, John A. Thompson, Mark R. Albertini, Joanne M. Jeter, Suephy C. Chen, John M. Kirkwood, Susan M. Swetter, Jennifer L. Hay, Aaron R. Mangold, Debjani Sahni, Emily Y. Chu, Clara Curiel-Lewandrowski, Jack L. Arbiser, Mohammed Kashani-Sabet, Tawnya L. Bowles, Kelly C. Nelson, Douglas Grossman, Pamela B. Cassidy, Jeffrey E. Gershenwald, Michael E. Ming, Zalfa A. Abdel-Malek, David E. Fisher, Pauline Funchain, Robert P. Dellavalle, June K. Robinson, Ashfaq A. Marghoob, Kari Kendra, Vernon K. Sondak, Sherry L. Pagoto, John T. Vetto, Martin A. Weinstock, Kim Margolin, Sancy A. Leachman, Neil F. Box, Jonathan S. Zager, Larisa J. Geskin, and Aleksandar Sekulic

Subjects

Cancer Research, medicine.medical_specialty, business.industry, Melanoma, Cancer, Phases of clinical research, Evidence-based medicine, Disease, medicine.disease, Clinical trial, 03 medical and health sciences, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, Epidemiology, Medicine, 030212 general & internal medicine, business, Intensive care medicine, Repurposing

Abstract

Recent progress in the treatment of advanced melanoma has led to unprecedented improvements in overall survival and, as these new melanoma treatments have been developed and deployed in the clinic, much has been learned about the natural history of the disease. Now is the time to apply that knowledge toward the design and clinical evaluation of new chemoprevention agents. Melanoma chemoprevention has the potential to reduce dramatically both the morbidity and the high costs associated with treating patients who have metastatic disease. In this work, scientific and clinical melanoma experts from the national Melanoma Prevention Working Group, composed of National Cancer Trials Network investigators, discuss research aimed at discovering and developing (or repurposing) drugs and natural products for the prevention of melanoma and propose an updated pipeline for translating the most promising agents into the clinic. The mechanism of action, preclinical data, epidemiological evidence, and results from available clinical trials are discussed for each class of compounds. Selected keratinocyte carcinoma chemoprevention studies also are considered, and a rationale for their inclusion is presented. These data are summarized in a table that lists the type and level of evidence available for each class of agents. Also included in the discussion is an assessment of additional research necessary and the likelihood that a given compound may be a suitable candidate for a phase 3 clinical trial within the next 5 years.

Published

2018

14. A network of epigenomic and transcriptional cooperation encompassing an epigenomic master regulator in cancer

Author

Fabian V. Filipp and Stephen Wilson

Subjects

0301 basic medicine, biology, Applied Mathematics, Gene regulatory network, Promoter, Computational biology, General Biochemistry, Genetics and Molecular Biology, Article, Computer Science Applications, Chromatin, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Histone, lcsh:Biology (General), 030220 oncology & carcinogenesis, Modeling and Simulation, Drug Discovery, biology.protein, Demethylase, Epigenetics, Transcription factor, lcsh:QH301-705.5, Epigenomics

Abstract

Coordinated experiments focused on transcriptional responses and chromatin states are well-equipped to capture different epigenomic and transcriptomic levels governing the circuitry of a regulatory network. We propose a workflow for the genome-wide identification of epigenomic and transcriptional cooperation to elucidate transcriptional networks in cancer. Gene promoter annotation in combination with network analysis and sequence-resolution of enriched transcriptional motifs in epigenomic data reveals transcription factor families that act synergistically with epigenomic master regulators. By investigating complementary omics levels, a close teamwork of the transcriptional and epigenomic machinery was discovered. The discovered network is tightly connected and surrounds the histone lysine demethylase KDM3A, basic helix-loop-helix factors MYC, HIF1A, and SREBF1, as well as differentiation factors AP1, MYOD1, SP1, MEIS1, ZEB1, and ELK1. In such a cooperative network, one component opens the chromatin, another one recognizes gene-specific DNA motifs, others scaffold between histones, cofactors, and the transcriptional complex. In cancer, due to the ability to team up with transcription factors, epigenetic factors concert mitogenic and metabolic gene networks, claiming the role of a cancer master regulators or epioncogenes. Significantly, specific histone modification patterns are commonly associated with open or closed chromatin states, and are linked to distinct biological outcomes by transcriptional activation or repression. Disruption of patterns of histone modifications is associated with the loss of proliferative control and cancer. There is tremendous therapeutic potential in understanding and targeting histone modification pathways. Thus, investigating cooperation of chromatin remodelers and the transcriptional machinery is not only important for elucidating fundamental mechanisms of chromatin regulation, but also necessary for the design of targeted therapeutics., Systems Biology helps explain how cancer controls specific effector networks—findings with important implications for the future of cancer therapy The cancer systems biology team of Professor Fabian V. Filipp at the University of California Merced introduces a universal workflow for elucidation of regulatory cooperation networks. The authors show that by integrating different genomic features of complementary epigenomic and transcriptomic data a highly specific and hyperconnected network can be identified. On the one hand epigenomic target regions define accessible chromatin, on the other hand motifs of differentially expressed transcripts determine the target genes controlled by the cooperative forces. In cancer, epigenetic master regulators govern the epigenome and accomplish target specificity of their phenotypic program by cooperation with members of the transcriptional machinery. The research establishes how genome-wide data in combination with systems biology analyses ascertains master regulators and new drug targets of therapy resistance in cancer.

Published

2018

15. Crosstalk between epigenetics and metabolism—Yin and Yang of histone demethylases and methyltransferases in cancer

Author

Fabian V. Filipp

Subjects

0301 basic medicine, Methyltransferase, cancer metabolism, Biochemistry, Epigenesis, Genetic, epigenetics, epigenetic drug, precision medicine, KDM, oncogene, Neoplasms, Histone methylation, 2.1 Biological and endogenous factors, Aetiology, Letter to the Editor, Cancer, Epigenomics, Histone Demethylases, tumor suppressors, histone methyltransferase, EZH2, High-Throughput Nucleotide Sequencing, General Medicine, KMT, Cell biology, JMJD, Histone, Histone methyltransferase, Histone Methyltransferases, Biotechnology, driver, cancer systems biology, Biology, 03 medical and health sciences, Rare Diseases, Genetic, histone demethylase, melanoma, Genetics, Humans, Epigenetics, Molecular Biology, master regulator, Human Genome, Histone-Lysine N-Methyltransferase, oncometabolite, 030104 developmental biology, epigenomics, jumonji, biology.protein, Digestive Diseases, Epigenesis, Developmental Biology

Abstract

Histone methylation is an epigenetic modification of chromatin undergoing dynamic changes and balancing tissue-specific demands of proliferation and differentiation. In cancer, aberrant histone methylation can facilitate oncogenic and tumor suppression programs by modulating gene expression. Histone remodelers such as lysine methyltransferases and lysine demethylases are seemingly opposite or contrary forces but may be part of an interconnected network complementing each other. We identify several layers of molecular communication where epigenetic master regulators engage in crosstalk between tumor metabolism and histone remodeling. Epigenetic master regulators have the ability to cooperate with members of the transcriptional machinery, DNA methyltransferases, as well as other histone modifiers. High-throughput sequencing and omics data in combination with cancer systems biology analysis have the power to prioritize regulatory events epigenome-wide.

Published

2017

16. CD271 is a molecular switch with divergent roles in melanoma and melanocyte development

Author

Alexander D. Boiko, Chen Li, and Fabian V. Filipp

Subjects

0301 basic medicine, DNA Repair, Cell Survival, lcsh:Medicine, Nerve Tissue Proteins, Receptors, Nerve Growth Factor, Biology, Cell fate determination, Real-Time Polymerase Chain Reaction, Article, Malignant transformation, 03 medical and health sciences, 0302 clinical medicine, Humans, Gene Regulatory Networks, Neoplastic transformation, lcsh:Science, E2F, Melanoma, Regulation of gene expression, Multidisciplinary, Cell growth, lcsh:R, Regulatory networks, ddc, Neoplasm Proteins, Cell biology, Gene Expression Regulation, Neoplastic, AP-1 transcription factor, Cell Transformation, Neoplastic, 030104 developmental biology, Disease Progression, Melanocytes, lcsh:Q, Signal transduction, Transcriptome, 030217 neurology & neurosurgery, Signal Transduction

Abstract

Dysregulation of signaling networks controlling self-renewal and migration of developmental cell lineages is closely linked to the proliferative and invasive properties of tumors. Identification of such signaling pathways and their critical regulators is vital for successful design of effective targeted therapies against neoplastic tissue growth. The neurotrophin receptor (CD271/NGFR/p75NTR) is a key regulator of the melanocytic cell lineage through its ability to mediate cell growth, survival, and differentiation. Using clinical melanoma samples, normal melanocytes and global gene expression profiling we have investigated the role of CD271 in rewiring signal transduction networks of melanoma cells during neoplastic transformation. Our analysis demonstrates that depending on the cell fate of tumor initiation vs normal development, elevated levels of CD271 can serve as a switch between proliferation/survival and differentiation/cell death. Two divergent arms of neurotrophin signaling hold the balance between positive regulators of tumor growth controlled by E2F, MYC, SREBP1 and AKT3 pathways on the one hand, and differentiation, senescence, and apoptosis controlled by TRAF6/IRAK-dependent activation of AP1 and TP53 mediated processes on the other hand. A molecular network map revealed in this study uncovers CD271 as a context-specific molecular switch between normal development and malignant transformation.

Published

2019

17. Erratum: Jeter JM, Bowles TL, Curiel‐Lewandrowski C, et al. Chemoprevention agents for melanoma: A path forward into phase 3 clinical trials. Cancer . 2019:125:18‐44

Author

Martin A. Weinstock, Tawnya L. Bowles, Debjani Sahni, Kari Kendra, Kim Margolin, Jack L. Arbiser, Joanne M. Jeter, Jeffrey E. Gershenwald, Maria L. Wei, Clara Curiel-Lewandrowski, Svetomir N. Markovic, Douglas Grossman, Fabian V. Filipp, John T. Vetto, John A. Thompson, Pamela B. Cassidy, Darrel L. Ellis, June K. Robinson, David E. Fisher, Jerry D. Brewer, Jennifer G. Powers, Aaron R. Mangold, Michael E. Ming, Susan M. Swetter, Pauline Funchain, Jonathan S. Zager, Mark R. Albertini, Mohammed Kashani-Sabet, Zalfa A. Abdel-Malek, Suephy C. Chen, Jennifer L. Hay, Vernon K. Sondak, Larisa J. Geskin, Emily Y. Chu, Sherry L. Pagoto, Meyskens Frank L Jr, Robert P. Dellavalle, Sancy A. Leachman, Kelly C. Nelson, John M. Kirkwood, Ashfaq A. Marghoob, Aleksandar Sekulic, and Neil F. Box

Subjects

Cancer Research, Grossman, Oncology, biology, business.industry, Larisa, Medicine, biology.organism_classification, business, Humanities

Abstract

Author(s): Jeter, Joanne M; Bowles, Tawnya L; Curiel-Lewandrowski, Clara; Swetter, Susan M; Filipp, Fabian V; Abdel-Malek, Zalfa A; Geskin, Larisa J; Brewer, Jerry D; Arbiser, Jack L; Gershenwald, Jeffrey E; Chu, Emily Y; Kirkwood, John M; Box, Neil F; Funchain, Pauline; Fisher, David E; Kendra, Kari L; Marghoob, Ashfaq A; Chen, Suephy C; Ming, Michael E; Albertini, Mark R; Vetto, John T; Margolin, Kim A; Pagoto, Sherry L; Hay, Jennifer L; Grossman, Douglas; Ellis, Darrel L; Kashani-Sabet, Mohammed; Mangold, Aaron R; Markovic, Svetomir N; Jr, Meyskens Frank L; Nelson, Kelly C; Powers, Jennifer G; Robinson, June K; Sahni, Debjani; Sekulic, Aleksandar; Sondak, Vernon K; Wei, Maria L; Zager, Jonathan S; Dellavalle, Robert P; Thompson, John A; Weinstock, Martin A; Leachman, Sancy A; Cassidy, Pamela B

Published

2019

18. Targeting glutamate metabolism in melanoma

Author

Simar J. Singh, Fabian V. Filipp, Raj Shah, and Suzie Chen

Subjects

Molecular Networks (q-bio.MN), Quantitative Biology - Quantitative Methods, chemistry.chemical_compound, Biosynthesis, In vivo, 0502 economics and business, medicine, Quantitative Biology - Genomics, Quantitative Biology - Molecular Networks, 050207 economics, Autocrine signalling, Tissues and Organs (q-bio.TO), Quantitative Methods (q-bio.QM), Genomics (q-bio.GN), 050208 finance, Glutamate secretion, Melanoma, 05 social sciences, Glutamate receptor, Quantitative Biology - Tissues and Organs, medicine.disease, 3. Good health, Metabotropic receptor, chemistry, FOS: Biological sciences, Cancer research, Signal transduction

Abstract

The glutamate metabotropic receptor 1 (GRM1) drives oncogenesis when aberrantly activated in melanoma and several other cancers. Metabolomics reveals that patient-derived xenografts with GRM1-positive melanoma tumors exhibit elevated plasma glutamate levels associated with metastatic melanoma in vivo. Stable isotope tracing and GCMS analysis determined that cells expressing GRM1 fuel a substantial fraction of glutamate from glycolytic carbon. Stimulation of GRM1 by glutamate leads to activation of mitogenic signaling pathways, which in turn increases the production of glutamate, fueling autocrine feedback. Implementing a rational drug-targeting strategy, we critically evaluate metabolic bottlenecks in vitro and in vivo. Combined inhibition of glutamate secretion and biosynthesis is an effective rational drug targeting strategy suppressing tumor growth and restricting tumor bioavailability of glutamate., Comment: 6 figures

Published

2019

19. Evaluation of integrin αvβ6 cystine knot PET tracers to detect cancer and idiopathic pulmonary fibrosis

Author

Joshua J. Mooney, Subhendu Chakraborti, Bin Shen, Brendan C. Visser, Ohad Ilovich, Fabian V. Filipp, Timothy H. Witney, Christopher A. Bonagura, Ramasamy Paulmurugan, Juergen K. Willmann, Jeffrey A. Norton, Fang Li, Ling Wang, Zhen Cheng, S. Srinivas, Lotfi Abou-Elkacem, Thomas Haywood, Scott Turner, Arutselvan Natarajan, Walter G. Park, Eric J Yang, H. Henry Guo, Frederick T. Chin, Andrei Iagaru, Negin Hatami, Willemieke S. Tummers, Richard S. Gaster, Richard H. Kimura, George A. Poultsides, Frezghi Habte, Mark L. Stolowitz, Kenneth Lau, Yan Cheng, Rammohan Devulapally, Andrea Otte, Ananth Srinivasan, Jay C. Nix, Sanjiv S. Gambhir, Lucia Baratto, Suhas Tikole, Tushar J. Desai, and Li Huo

Subjects

0301 basic medicine, Integrins, General Physics and Astronomy, Crystallography, X-Ray, Idiopathic pulmonary fibrosis, 0302 clinical medicine, Neoplasms, Medicine, lcsh:Science, Lung, Cancer, screening and diagnosis, Multidisciplinary, Crystallography, medicine.diagnostic_test, biology, Cystine knot, Magnetic Resonance Imaging, Healthy Volunteers, 3. Good health, ddc, Detection, medicine.anatomical_structure, Positron emission tomography, 030220 oncology & carcinogenesis, Respiratory, Biomedical Imaging, 4.2 Evaluation of markers and technologies, Biodistribution, Science, Integrin, Bioengineering, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Rare Diseases, Antigens, Neoplasm, Clinical Research, Humans, Antigens, X-ray crystallography, business.industry, Diagnostic markers, General Chemistry, medicine.disease, Idiopathic Pulmonary Fibrosis, 4.1 Discovery and preclinical testing of markers and technologies, 030104 developmental biology, Positron-Emission Tomography, Cancer research, biology.protein, X-Ray, Neoplasm, Cancer imaging, lcsh:Q, Protein design, Molecular imaging, business, Solution-state NMR

Abstract

Advances in precision molecular imaging promise to transform our ability to detect, diagnose and treat disease. Here, we describe the engineering and validation of a new cystine knot peptide (knottin) that selectively recognizes human integrin αvβ6 with single-digit nanomolar affinity. We solve its 3D structure by NMR and x-ray crystallography and validate leads with 3 different radiolabels in pre-clinical models of cancer. We evaluate the lead tracer’s safety, biodistribution and pharmacokinetics in healthy human volunteers, and show its ability to detect multiple cancers (pancreatic, cervical and lung) in patients at two study locations. Additionally, we demonstrate that the knottin PET tracers can also detect fibrotic lung disease in idiopathic pulmonary fibrosis patients. Our results indicate that these cystine knot PET tracers may have potential utility in multiple disease states that are associated with upregulation of integrin αvβ6., Knottin is a cystine knot peptide. Here, the authors develop a knottin-based tracer for positron emission tomography and demonstrate its ability to detect cancer and idiopathic pulmonary fibrosis through selective binding to integrin αvβ6.

Published

2019

20. Concurrent targeting of glutaminolysis and metabotropic glutamate receptor 1 (GRM1) reduces glutamate bioavailability in GRM1(+) melanoma

Author

Kevinn Eddy, Suzie Chen, Simar J. Singh, Fabian V. Filipp, and Raj Shah

Subjects

0301 basic medicine, Cancer Research, Benzeneacetamides, Biological Availability, Glutamic Acid, Apoptosis, Receptors, Metabotropic Glutamate, Article, Mice, 03 medical and health sciences, Glutamatergic, 0302 clinical medicine, Glutaminase, Thiadiazoles, Tumor Cells, Cultured, medicine, Animals, Humans, Neoplastic transformation, Autocrine signalling, Melanoma, Cell Proliferation, Mice, Hairless, Riluzole, Glutaminolysis, Chemistry, Glutamate receptor, Xenograft Model Antitumor Assays, Neuroprotective Agents, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, Metabotropic glutamate receptor 1, Drug Therapy, Combination, Female, Signal Transduction, medicine.drug

Abstract

Aberrant glutamatergic signaling has been implicated in altered metabolic activity in many cancer types, including malignant melanoma. Previously, we have illustrated the role of metabotropic glutamate receptor 1 (GRM1) in neoplastic transformation of melanocytes in vitro and spontaneous metastatic melanoma in vivo. In this study, we showed that autocrine stimulation constitutively activates the GRM1 receptor and its downstream mitogenic signaling. GRM1-activated (GRM1+) melanomas exhibited significantly increased expression of glutaminase (GLS), which catalyzes the first step in the conversion of glutamine to glutamate. In cultured GRM1+ melanoma cell lines, CB-839, a potent, selective, and orally bioavailable inhibitor of GLS, suppressed cell proliferation, while riluzole, an inhibitor of glutamate release, promoted apoptotic cell death in vitro and in vivo. Combined treatment with CB-839 and riluzole treatment proved to be superior to single-agent treatment, restricting glutamate bioavailability and leading to effective suppression of tumor cell proliferation in vitro and tumor progression in vivo. Hyperactivation of GRM1 in malignant melanoma is an oncogenic driver, which acts independently of canonical melanoma proto-oncogenes, BRAF or NRAS. Overall, these results indicate that expression of GRM1 promotes a metabolic phenotype that supports increased glutamate production and autocrine glutamatergic signaling, which can be pharmacologically targeted by decreasing glutamate bioavailability and the GLS-dependent glutamine to glutamate conversion.Significance:These findings demonstrate that targeting glutaminolytic glutamate bioavailability is an effective therapeutic strategy for GRM1-activated tumors.

Published

2019

21. BCL-2 and BCL-Xl Use Different Molecular Mechanisms to Regulate Carbohydrate Metabolism

Author

Catalina Olea, Laurent M. Dejean, Krish Krishnan, Fabian V. Filipp, and Itzel Lopez

Subjects

Biochemistry, biology, Chemistry, Biophysics, biology.protein, Bcl-xL, Carbohydrate metabolism

Published

2021

22. EZH2 as a mediator of treatment resistance in melanoma

Author

Stuart J. Gallagher, Barbara Fazekas de St Groth, Peter Hersey, Jessamy Tiffen, Hsin-Yi Tseng, and Fabian V. Filipp

Subjects

0301 basic medicine, medicine.medical_treatment, macromolecular substances, Dermatology, Biology, Bioinformatics, Article, General Biochemistry, Genetics and Molecular Biology, Epigenesis, Genetic, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, Mediator, Immune system, medicine, Humans, Enhancer of Zeste Homolog 2 Protein, Melanoma, EZH2, Cancer, Immunosuppression, Immunotherapy, medicine.disease, 030104 developmental biology, Oncology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research

Abstract

Direct treatments of cancer such as chemotherapy, radiotherapy and targeted therapy have been shown to depend on recruitment of the immune system for their effectiveness. Recent studies have shown that development of resistance to direct therapies such as BRAF inhibitors in melanoma is associated with suppression of immune responses. We point to emerging data that implicates activation of the polycomb repressive complex 2 (PRC2) and its catalytic component - enhancer of zeste homolog 2 (EZH2) - in progression of melanoma and suppression of immune responses. EZH2 appears to have an important role in differentiation of CD4 T cells and particularly in the function of T regulatory cells, which suppress immune responses to melanoma. We review mechanisms of EZH2 activation at genomic level and from activation of the MAP Kinase, E2F or NF-kB2 pathways. These studies are consistent with activation of EZH2 as a common mechanism for induction of immune suppression in patients failing direct therapies and suggest EZH2 inhibitors may have a role in combination with immunotherapy and targeted therapies to prevent development of immunosuppression.

Published

2016

23. Somatic Copy Number Amplification and Hyperactivating Somatic Mutations of EZH2 Correlate With DNA Methylation and Drive Epigenetic Silencing of Genes Involved in Tumor Suppression and Immune Responses in Melanoma

Author

Stuart J. Gallagher, Fabian V. Filipp, Jessamy Tiffen, Stephen Wilson, and Peter Hersey

Subjects

0301 basic medicine, Cancer Research, Indoles, DNA Copy Number Variations, Pyridones, Cellular differentiation, macromolecular substances, Biology, Polymorphism, Single Nucleotide, lcsh:RC254-282, Article, Epigenesis, Genetic, 03 medical and health sciences, medicine, Humans, Gene silencing, Enhancer of Zeste Homolog 2 Protein, Genes, Tumor Suppressor, Melanoma, Regulation of gene expression, Microarray analysis techniques, EZH2, DNA Methylation, Microarray Analysis, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Molecular biology, Immunity, Innate, 3. Good health, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Mutation, DNA methylation, Cutaneous melanoma, Cancer research

Abstract

The epigenetic modifier EZH2 is in the center of a repressive complex controlling differentiation of normal cells. In cancer EZH2 has been implicated in silencing tumor suppressor genes. Its role in melanoma as well as target genes affected by EZH2 are poorly understood. In view of this we have used an integrated systems biology approach to analyze 471 cases of skin cutaneous melanoma (SKCM) in The Cancer Genome Atlas (TCGA) for mutations and amplifications of EZH2. Identified changes in target genes were validated by interrogation of microarray data from melanoma cells treated with the EZH2 inhibitor GSK126. We found that EZH2 activation by mutations, gene amplification and increased transcription occurred in about 20% of the cohort. These alterations were associated with significant hypermethylation of DNA and significant downregulation of 11% of transcripts in patient RNASeq data. GSK126 treatment of melanoma lines containing EZH2 activation reversed such transcriptional repression in 98 candidate target genes. Gene enrichment analysis revealed genes associated with tumor suppression, cell differentiation, cell cycle inhibition and repression of metastases as well as antigen processing and presentation pathways. The identified changes in EZH2 were associated with an adverse prognosis in the TCGA dataset. These results suggest that inhibiting of EZH2 is a promising therapeutic avenue for a substantial fraction of melanoma patients.

Published

2016

24. Bcl-2 Overexpression Stimulates Cell Proliferation and Lactic Fermentation without Affecting Whole Cell Respiration

Author

Bushra Mahmood, Nawras Saaman, Krish Krishnan, Fabian V. Filipp, Lucineh Kasnakjian, and Laurent M. Dejean

Subjects

Chemistry, Cell growth, Respiration, Biophysics, Whole cell, Lactic acid fermentation, Cell biology

Published

2020

25. Frontiers in Pigment Cell and Melanoma Research

Author

Keiran S.M. Smalley, Tamara Terzian, Feng Liu-Smith, Sancy A. Leachman, John A. D'Orazio, Kazumasa Wakamatsu, Boon Kee Goh, Mayumi Fujita, Caroline Le Poole, Meenhard Herlyn, Jeffrey S. Weber, Richard A. Sturm, Suzie Chen, Prashiela Manga, Douglas E. Brash, Neil F. Box, Richard A. Spritz, Stanca A. Birlea, Yiqun G. Shellman, Fabian V. Filipp, Pamela B. Cassidy, Arup K. Indra, David A. Norris, Lluis Montoliu, Susan M. Swetter, Marcus Bosenberg, and Lionel Larue

Subjects

0301 basic medicine, vitiligo, melanocyte, q-bio.TO, Biomedical Research, Drug Resistance, albinism, Vitiligo, Medical and Health Sciences, 0302 clinical medicine, Basic research, pigmentation, Tissues and Organs (q-bio.TO), Melanoma, oncology_oncogenics, cancer prevention, Pigmentation, Biological Sciences, melanin, dermatology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Melanocytes, immunotherapy, skin, medicine.medical_specialty, Systems biology, Dermatology, Melanocyte, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, International Pigment Cell Conference, melanoma, medicine, Animals, Humans, melasma, Animal, business.industry, Dermatology & Venereal Diseases, Quantitative Biology - Tissues and Organs, medicine.disease, Precision medicine, UV, Disease Models, Animal, 030104 developmental biology, Drug Resistance, Neoplasm, FOS: Biological sciences, Disease Models, Neoplasm, business

Abstract

© 2018 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd In this perspective, we identify emerging frontiers in clinical and basic research of melanocyte biology and its associated biomedical disciplines. We describe challenges and opportunities in clinical and basic research of normal and diseased melanocytes that impact current approaches to research in melanoma and the dermatological sciences. We focus on four themes: (1) clinical melanoma research, (2) basic melanoma research, (3) clinical dermatology, and (4) basic pigment cell research, with the goal of outlining current highlights, challenges, and frontiers associated with pigmentation and melanocyte biology. Significantly, this document encapsulates important advances in melanocyte and melanoma research including emerging frontiers in melanoma immunotherapy, medical and surgical oncology, dermatology, vitiligo, albinism, genomics and systems biology, epidemiology, pigment biophysics and chemistry, and evolution.

Published

2018

26. The triennial International Pigment Cell Conference (IPCC)

Author

Fabian V. Filipp, Neil F. Box, Prashiela Manga, Richard A. Spritz, Lluis Montoliu, and Lionel Larue

Subjects

0301 basic medicine, Albinism, education, Vitiligo, Color, Cellular homeostasis, lcsh:Medicine, IFPCS, Dermatology, General Biochemistry, Genetics and Molecular Biology, Cancer prevention, BRAF, 03 medical and health sciences, Melanocyte, Basic research, Melanin, Dermatological disorders, Melasma, ICB, Tissues and Organs (q-bio.TO), Melanoma, Skin, geography, Summit, geography.geographical_feature_category, Pigmentation, IPCC, Precision medicine, lcsh:R, Translational medicine, Pigment cells, Conference, Quantitative Biology - Tissues and Organs, CPD, General Medicine, Other Quantitative Biology (q-bio.OT), MAPK, Quantitative Biology - Other Quantitative Biology, UV, 030104 developmental biology, Oncology, Pigment, FOS: Biological sciences, Sustainability, Commentary, Engineering ethics, Immunotherapy

Abstract

The International Federation of Pigment Cell Societies (IFPCS) held its XXIII triennial International Pigment Cell Conference (IPCC) in Denver, Colorado in August 2017. The goal of the summit was to provide a venue promoting a vibrant interchange among leading basic and clinical researchers working on leading-edge aspects of melanocyte biology and disease. The philosophy of the meeting, entitled Breakthroughs in Pigment Cell and Melanoma Research, was to deliver a comprehensive program in an inclusive environment fostering scientific exchange and building new academic bridges. This document provides an outlook on the history, accomplishments, and sustainability of the pigment cell and melanoma research community. Shared progress in the understanding of cellular homeostasis of pigment cells but also clinical successes and hurdles in the treatment of melanoma and dermatological disorders continue to drive future research activities. A sustainable direction of the societies creates an international forum identifying key areas of imminent needs in laboratory research and clinical care and ensures the future of this vibrant, diverse and unique research community at the same time. Important advances showcase wealth and breadth of the field in melanocyte and melanoma research and include emerging frontiers in melanoma immunotherapy, medical and surgical oncology, dermatology, vitiligo, albinism, genomics and systems biology, precision bench-to-bedside approaches, epidemiology, pigment biophysics and chemistry, and evolution. This report recapitulates highlights of the federate meeting agenda designed to advance clinical and basic research frontiers from melanoma and dermatological sciences followed by a historical perspective of the associated societies and conferences.

Published

2018

27. Increased glutaminolytic flux and activation of mitochondrial metabolism by BCL2 hyperactivity in lymphoma

Author

Laurent Dejean, Simar J. Singh, Helma Zecena, Fabian V. Filipp, and Kirandeep Kaur

Subjects

Citric acid cycle, HIF1A, Pyruvate dehydrogenase kinase, Glutaminolysis, Chemistry, Glutaminase, immune system diseases, hemic and lymphatic diseases, Glycolysis, Pyruvate dehydrogenase complex, Flux (metabolism), Carbon utilization, Cell biology

Abstract

B-cell lymphoma 2 (BCL2) is an important apoptosis regulator during developmental and pathological states, and its overexpression is a key feature of several malignancies. Genomic data from The Cancer Genome Atlas (TCGA) reveals significant somatic copy number amplification, overexpression, and/or elevated protein activity of BCL2 in 50 % of diffuse large B-cell lymphoma (DLBC) patients. While its canonical role in mitochondria-directed apoptosis is well established, the effect of BCL2 on transcriptional and metabolic networks remains elusive. Using an established lymphocytic pro-B-cell line overexpressing BCL2, we identified dysregulated transcriptional and metabolic networks by transcriptomic profiling arrays. Elevated BCL2 levels affect transcription factor complexes and mitogenic programs of NF-κB/REL, HIF1A/ARNT, AP1, E2F, and STAT factors. Using stable isotope-assisted metabolic flux measurements we quantify that elevated BCL2 expression increases carbon utilization boosting cellular proliferation. Tumorigenic overexpression of BCL2 significantly increases glycolytic flux, glutaminolysis, and anaplerotic flux into the TCA cycle. At the same time, the mitochondrial acetyl-CoA pool is separated from the glycolytic one by inactivating the pyruvate dehydrogenase complex via transcriptional regulation of pyruvate dehydrogenase kinase (PDK3). As compensatory fuel, mitochondrial TCA cycle metabolism is supported by asparagine synthase (ASNS) and oxidative glutaminolysis creating targets for small molecule inhibition of glutaminase. Lymphoma cells overexpressing BCL2 contained more mitochondrial mass and were more sensitive to L-glutamine deprivation and glutaminase inhibition. Cells overexpressing a mutant BCL2 G145E, which is incapable of binding BH domain members, failed to increase proliferation, glycolysis, or glutaminolysis. Taken together, the oncogene BCL2 has the ability to ramp up a metabolic phenotype supporting proliferation independent of its anti-apoptotic role. The cellular model of BCL2 activation supports NF-KB-positive subtypes of DLBC and identifies metabolic bottlenecks with dependency on anaplerotic flux as an actionable BCL2 effector network in cancer.

Published

2017

28. Metabolic shift in density-dependent stem cell differentiation

Author

Drew E. Glaser, Kara E. McCloskey, Simar J. Singh, Fabian V. Filipp, and William S. Turner

Subjects

0301 basic medicine, Cellular differentiation, Endothelial cells, lcsh:Medicine, Cell Count, Cell contact, Stem cells, Regenerative Medicine, Biochemistry, Mice, Vascular fate, Flow cytometry, lcsh:Cytology, Cell adhesion molecule, Cancer stem cells, Cell Differentiation, Cell biology, Endothelial stem cell, Differentiation, Fluorescence-activated cell sorting, Stem Cell Research - Nonembryonic - Non-Human, Stem cell, Systems biology, Signal Transduction, Embryonic stem cells, Biochemistry & Molecular Biology, Microenvironment, 1.1 Normal biological development and functioning, Biology, Cell communication, Cell Line, 03 medical and health sciences, Cancer stem cell, Underpinning research, Genetics, Animals, Metabolomics, Cell seeding density, lcsh:QH573-671, Progenitor cell, Molecular Biology, Cell growth, Research, lcsh:R, Cell adhesion, Cell Biology, Stem Cell Research, Molecular biology, Embryonic stem cell, NMR, 030104 developmental biology, Metabolism, Vascular progenitor cells, Biochemistry and Cell Biology

Abstract

Background Vascular progenitor cells (VPCs) derived from embryonic stem cells (ESCs) are a valuable source for cell- and tissue-based therapeutic strategies. During the optimization of endothelial cell (EC) inductions from mouse ESCs using our staged and chemically-defined induction methods, we found that cell seeding density but not VEGF treatment between 10 ng/mL and 40 ng/mL was a significant variable directing ESCs into FLK1+ VPCs during stage 1 induction. Here, we examine potential contributions from cell-to-cell signaling or cellular metabolism in the production of VPCs from ESCs seeded at different cell densities. Methods Using 1D 1H-NMR spectroscopy, transcriptomic arrays, and flow cytometry, we observed that the density-dependent differentiation of ESCs into FLK1+ VPCs positively correlated with a shift in metabolism and cellular growth. Results Specifically, cell differentiation correlated with an earlier plateauing of exhaustive glycolysis, decreased lactate production, lower metabolite consumption, decreased cellular proliferation and an increase in cell size. In contrast, cells seeded at a lower density of 1,000 cells/cm2 exhibited increased rates of glycolysis, lactate secretion, metabolite utilization, and proliferation over the same induction period. Gene expression analysis indicated that high cell seeding density correlated with up-regulation of several genes including cell adhesion molecules of the notch family (NOTCH1 and NOTCH4) and cadherin family (CDH5) related to vascular development. Conclusions These results confirm that a distinct metabolic phenotype correlates with cell differentiation of VPCs.

Published

2017

29. Metabolic profiling of triple-negative breast cancer cells reveals metabolic vulnerabilities

Author

Elizabeth A. Tovar, Carrie R. Graveel, Joshua P. Castle, Fabian V. Filipp, Andre N. Leon, Jeffrey P. MacKeigan, Nathan J. Lanning, Amandeep Sanghera, and Simar J. Singh

Subjects

0301 basic medicine, medicine.drug_class, Receptor tyrosine kinase, Tyrosine kinase inhibitor, Tyrosine-kinase inhibitor, 03 medical and health sciences, 0302 clinical medicine, Rate-limiting enzymes, Triple-negative breast cancer, Metabolic flux analysis, Breast Cancer, Genetics, medicine, 2.1 Biological and endogenous factors, Epidermal growth factor receptor, Aetiology, Cancer, EGFR inhibitors, Metabolic inhibitor, biology, Research, 3. Good health, Psychiatry and Mental health, Metabolism, 030104 developmental biology, 5.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Erlotinib, Development of treatments and therapeutic interventions, Tyrosine kinase, medicine.drug

Abstract

Background Among breast cancers, the triple-negative breast cancer (TNBC) subtype has the worst prognosis with no approved targeted therapies and only standard chemotherapy as the backbone of systemic therapy. Unique metabolic changes in cancer progression provide innovative therapeutic opportunities. The receptor tyrosine kinases (RTKs) epidermal growth factor receptor (EGFR), and MET receptor are highly expressed in TNBC, making both promising therapeutic targets. RTK signaling profoundly alters cellular metabolism by increasing glucose consumption and subsequently diverting glucose carbon sources into metabolic pathways necessary to support the tumorigenesis. Therefore, detailed metabolic profiles of TNBC subtypes and their response to tyrosine kinase inhibitors may identify therapeutic sensitivities. Methods We quantified the metabolic profiles of TNBC cell lines representing multiple TNBC subtypes using gas chromatography mass spectrometry. In addition, we subjected MDA-MB-231, MDA-MB-468, Hs578T, and HCC70 cell lines to metabolic flux analysis of basal and maximal glycolytic and mitochondrial oxidative rates. Metabolic pool size and flux measurements were performed in the presence and absence of the MET inhibitor, INC280/capmatinib, and the EGFR inhibitor, erlotinib. Further, the sensitivities of these cells to modulators of core metabolic pathways were determined. In addition, we annotated a rate-limiting metabolic enzymes library and performed a siRNA screen in combination with MET or EGFR inhibitors to validate synergistic effects. Results TNBC cell line models displayed significant metabolic heterogeneity with respect to basal and maximal metabolic rates and responses to RTK and metabolic pathway inhibitors. Comprehensive systems biology analysis of metabolic perturbations, combined siRNA and tyrosine kinase inhibitor screens identified a core set of TCA cycle and fatty acid pathways whose perturbation sensitizes TNBC cells to small molecule targeting of receptor tyrosine kinases. Conclusions Similar to the genomic heterogeneity observed in TNBC, our results reveal metabolic heterogeneity among TNBC subtypes and demonstrate that understanding metabolic profiles and drug responses may prove valuable in targeting TNBC subtypes and identifying therapeutic susceptibilities in TNBC patients. Perturbation of metabolic pathways sensitizes TNBC to inhibition of receptor tyrosine kinases. Such metabolic vulnerabilities offer promise for effective therapeutic targeting for TNBC patients. Electronic supplementary material The online version of this article (doi:10.1186/s40170-017-0168-x) contains supplementary material, which is available to authorized users.

Published

2017

30. Insulin induces a shift in lipid and primary carbon metabolites in a model of fasting-induced insulin resistance

Author

Fabian V. Filipp, Dmitry Grapov, Johannes Francois Fahrmann, Jose A. Viscarra, Michael R. La Frano, Rudy M. Ortiz, Oliver Fiehn, John W. Newman, Keedrian I. Olmstead, and Daniel E. Crocker

Subjects

0301 basic medicine, medicine.medical_specialty, Substrate metabolism, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Clinical Biochemistry, Clinical Sciences, 030209 endocrinology & metabolism, Biology, Biochemistry, Article, Analytical Chemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Insulin resistance, Internal medicine, medicine, Lipolysis, Metabolomics, Obesity, Fatty acids, Metabolic and endocrine, Nutrition, Triglyceride, Insulin, Diabetes, Lipid metabolism, Metabolism, medicine.disease, Protein catabolism, 030104 developmental biology, Endocrinology, chemistry, Lipidomics, Ketone bodies, Biochemistry and Cell Biology, Endocannabinoids

Abstract

© 2017, Springer Science+Business Media New York. Introduction: Prolonged fasting in northern elephant seals (NES) is characterized by a reliance on lipid metabolism, conservation of protein, and reduced plasma insulin. During early fasting, glucose infusion previously reduced plasma free fatty acids (FFA); however, during late-fasting, it induced an atypical elevation in FFA despite comparable increases in insulin during both periods suggestive of a dynamic shift in tissue responsiveness to glucose-stimulated insulin secretion. Objective: To better assess the contribution of insulin to this fasting-associated shift in substrate metabolism. Methods: We compared the responses of plasma metabolites (amino acids (AA), FFA, endocannabinoids (EC), and primary carbon metabolites (PCM)) to an insulin infusion (65 mU/kg) in early- and late-fasted NES pups (n = 5/group). Plasma samples were collected prior to infusion (T0) and at 10, 30, 60, and 120 min post-infusion, and underwent untargeted and targeted metabolomics analyses utilizing a variety of GC-MS and LC-MS technologies. Results: In early fasting, the majority (72%) of metabolite trajectories return to baseline levels within 2 h, but not in late fasting indicative of an increase in tissue sensitivity to insulin. In late-fasting, increases in FFA and ketone pools, coupled with decreases in AA and PCM, indicate a shift toward lipolysis, beta-oxidation, ketone metabolism, and decreased protein catabolism. Conversely, insulin increased PCM AUC in late fasting suggesting that gluconeogenic pathways are activated. Insulin also decreased FFA AUC between early and late fasting suggesting that insulin suppresses triglyceride hydrolysis. Conclusion: Naturally adapted tolerance to prolonged fasting in these mammals is likely accomplished by suppressing insulin levels and activity, providing novel insight on the evolution of insulin during a condition of temporary, reversible insulin resistance.

Published

2017

31. Reversing the rewiring of cancer

Author

Fabian V, Filipp

Subjects

Article

Published

2017

32. The histone demethylase KDM3A regulates the transcriptional program of the androgen receptor in prostate cancer cells

Author

Natasha Sahgal, Stephen Wilson, Fabian V. Filipp, Jianfei Qi, and Lingling Fan

Subjects

Male, 0301 basic medicine, Aging, Jumonji Domain-Containing Histone Demethylases, Transcription, Genetic, Androgen, Epigenesis, Genetic, Histones, ChIP-Seq, Histone demethylation, oncogene, Receptors, 2.1 Biological and endogenous factors, Gene Regulatory Networks, Aetiology, Cancer, Epigenomics, Tumor, Prostate Cancer, High-Throughput Nucleotide Sequencing, Genomics, prostate cancer, Lysine demethylase 3A, 3. Good health, Cell biology, Gene Expression Regulation, Neoplastic, Histone, Oncology, Receptors, Androgen, Gene Knockdown Techniques, Transcription, Protein Binding, Signal Transduction, Research Paper, Urologic Diseases, Chromatin Immunoprecipitation, Oncology and Carcinogenesis, cancer systems biology, Biology, Methylation, Cell Line, Androgen receptor binding, 03 medical and health sciences, Genetic, Cell Line, Tumor, Genetics, Humans, Epigenetics, Neoplastic, Gene Expression Profiling, Human Genome, Computational Biology, Prostatic Neoplasms, Molecular Sequence Annotation, Molecular biology, Enzyme Activation, Androgen receptor, 030104 developmental biology, Gene Expression Regulation, epigenomics, biology.protein, Demethylase, Epigenesis

Abstract

The lysine demethylase 3A (KDM3A, JMJD1A or JHDM2A) controls transcriptional networks in a variety of biological processes such as spermatogenesis, metabolism, stem cell activity, and tumor progression. We matched transcriptomic and ChIP-Seq profiles to decipher a genome-wide regulatory network of epigenetic control by KDM3A in prostate cancer cells. ChIP-Seq experiments monitoring histone 3 lysine 9 (H3K9) methylation marks show global histone demethylation effects of KDM3A. Combined assessment of histone demethylation events and gene expression changes presented major transcriptional activation suggesting that distinct oncogenic regulators may synergize with the epigenetic patterns by KDM3A. Pathway enrichment analysis of cells with KDM3A knockdown prioritized androgen signaling indicating that KDM3A plays a key role in regulating androgen receptor activity. Matched ChIP-Seq and knockdown experiments of KDM3A in combination with ChIP-Seq of the androgen receptor resulted in a gain of H3K9 methylation marks around androgen receptor binding sites of selected transcriptional targets in androgen signaling including positive regulation of KRT19, NKX3-1, KLK3, NDRG1, MAF, CREB3L4, MYC, INPP4B, PTK2B, MAPK1, MAP2K1, IGF1, E2F1, HSP90AA1, HIF1A, and ACSL3. The cancer systems biology analysis of KDM3A-dependent genes identifies an epigenetic and transcriptional network in androgen response, hypoxia, glycolysis, and lipid metabolism. Genome-wide ChIP-Seq data highlights specific gene targets and the ability of epigenetic master regulators to control oncogenic pathways and cancer progression.

Published

2017

33. Precision medicine driven by cancer systems biology

Author

Fabian V. Filipp

Subjects

0301 basic medicine, Epigenomics, Cancer Research, Subtype, Driver, medicine.disease_cause, Neoplasms, Precisionmedicine, 2.1 Biological and endogenous factors, Molecular Targeted Therapy, Precision Medicine, Melanoma, Cancer, CTLA4, Cancer systems biology, Systems Biology, Cancer metabolism, PRC2, MEK, PD1, SWI/SNF, Oncology, 5.1 Pharmaceuticals, Immunotherapy, Biotechnology, Systems biology, Oncology and Carcinogenesis, Biology, Article, BRAF, CSD, 03 medical and health sciences, Big data, ARID2, PDL1, medicine, Genetics, Humans, EZH2, Oncology & Carcinogenesis, Combination therapy, Protein kinase A, business.industry, Human Genome, Precision medicine, ARID1A, Personalized medicine, 030104 developmental biology, Targeted drug delivery, Oncometabolite, SCNA, Cancer research, business, Carcinogenesis, Neoantigen

Abstract

Molecular insights from genome and systems biology are influencing how cancer is diagnosed and treated. We critically evaluate big data challenges in precision medicine. The melanoma research community has identified distinct subtypes involving chronic sun-induced damage and the mitogen-activated protein kinase driver pathway. In addition, despite low mutation burden, non-genomic mitogen-activated protein kinase melanoma drivers are found in membrane receptors, metabolism, or epigenetic signaling with the ability to bypass central mitogen-activated protein kinase molecules and activating a similar program of mitogenic effectors. Mutation hotspots, structural modeling, UV signature, and genomic as well as non-genomic mechanisms of disease initiation and progression are taken into consideration to identify resistance mutations and novel drug targets. A comprehensive precision medicine profile of a malignant melanoma patient illustrates future rational drug targeting strategies. Network analysis emphasizes an important role of epigenetic and metabolic master regulators in oncogenesis. Co-occurrence of driver mutations in signaling, metabolic, and epigenetic factors highlights how cumulative alterations of our genomes and epigenomes progressively lead to uncontrolled cell proliferation. Precision insights have the ability to identify independent molecular pathways suitable for drug targeting. Synergistic treatment combinations of orthogonal modalities including immunotherapy, mitogen-activated protein kinase inhibitors, epigenetic inhibitors, and metabolic inhibitors have the potential to overcome immune evasion, side effects, and drug resistance.

Published

2017

34. Diet reprogrammes glucocorticoid rhythms

Author

Kenneth A. Dyar, Johann Hawe, Grant D. Barish, Ashfaq Ali Mir, Matthias Heinig, Céline Jouffe, Kinga Balazs, Konstantinos Makris, Fabian V. Filipp, Nina Henriette Uhlenhaut, Michael Wierer, and Fabiana Quagliarini

Subjects

Blood Glucose, Male, Time Factors, Transcription, Genetic, Endocrinology, Diabetes and Metabolism, Regulator, Ligands, 0302 clinical medicine, Glucocorticoid receptor, Endocrinology, Gene expression, STAT5 Transcription Factor, STAT5, Mice, Knockout, 0303 health sciences, Secretory Pathway, biology, Fasting, Postprandial Period, Chromatin, Circadian Rhythm, Postprandial, Liver, Glucocorticoid, Signal Transduction, medicine.drug, medicine.medical_specialty, Diet, High-Fat, Article, 03 medical and health sciences, Receptors, Glucocorticoid, Rhythm, Circadian Clocks, Internal medicine, medicine, High fat, Humans, Animals, PPAR alpha, Obesity, Circadian rhythm, Molecular Biology, Gene, Glucocorticoids, Triglycerides, 030304 developmental biology, business.industry, Gluconeogenesis, Cell Biology, Dietary Fats, Diet, Mice, Inbred C57BL, Disease Models, Animal, Gene Expression Regulation, biology.protein, Energy Metabolism, business, 030217 neurology & neurosurgery

Abstract

Summary The glucocorticoid receptor (GR) is a potent metabolic regulator and a major drug target. While GR is known to play integral roles in circadian biology, its rhythmic genomic actions have never been characterized. Here we mapped GR’s chromatin occupancy in mouse livers throughout the day and night cycle. We show how GR partitions metabolic processes by time-dependent target gene regulation and controls circulating glucose and triglycerides differentially during feeding and fasting. Highlighting the dominant role GR plays in synchronizing circadian amplitudes, we find that the majority of oscillating genes are bound by and depend on GR. This rhythmic pattern is altered by high-fat diet in a ligand-independent manner. We find that the remodeling of oscillatory gene expression and postprandial GR binding results from a concomitant increase of STAT5 co-occupancy in obese mice. Altogether, our findings highlight GR’s fundamental role in the rhythmic orchestration of hepatic metabolism.

Published

2019

35. Abstract 1839: Concurrent inhibition of glutaminase (GLS) and metabotropic receptor 1 (GRM1) reduced glutamate bioavailability and led to a decrease in GRM1-expressing melanoma cell proliferation in vitro and tumor progression in vivo

Author

Kevinn Eddy, Simar J. Singh, Suzie Chen, Fabian V. Filipp, and Raj Shah

Subjects

Cancer Research, Glutaminase, Chemistry, Melanoma, Glutamate receptor, medicine.disease, Riluzole, Metabotropic receptor, Oncology, Cancer research, medicine, Metabotropic glutamate receptor 1, Neoplastic transformation, Autocrine signalling, medicine.drug

Abstract

Aberrant glutamatergic signaling has been implicated in multiple metabolic processes and several types of cancer. Our laboratory has previously illustrated the role of metabotropic glutamate receptor 1 (GRM1), a G-protein coupled receptor, in neoplastic transformation of melanocytes in vitro and spontaneous development of metastatic melanoma in vivo. Here, we demonstrate significant overexpression of glutaminase (GLS) in GRM1 expressing melanoma cells, resulting in excess production of GRM1’s natural ligand, glutamate, and the establishment of autocrine loops. GLS catalyzes the first step in glutamine metabolism–the conversion of glutamine to glutamate before entering the TCA cycle. Comparison of glutamate levels in circulating blood plasma between melanoma prone GRM1-transgenic and wild type mice showed elevated glutamate levels in melanoma prone GRM1-transgenic mice, suggesting that aberrant GRM1 expression also promotes an increase in circulating glutamate, to ensure constitutive activation of the GRM1 receptor and its downstream signaling effecters in vivo. We also discovered that manipulation of GRM1 expression by genetic means led to robust parallel changes in metabolite expression levels and intracellular glutamate concentrations by mass spectrometry analysis, as well as the endogenous levels of GLS in melanoma cells, suggesting a strong association between GRM1 and GLS. Inclusion of CB-839, a potent, selective, and orally bioavailable inhibitor of GLS, resulted in significant inhibition of GRM1+ melanoma cell proliferation compared to GRM1- ones. The sensitivity of GRM1+ melanoma cells to modulation of GLS points to the dependency of these cells to glutamate amounts via GLS activity. We also demonstrated that treatment with Riluzole, an inhibitor of glutamatergic signaling by decreasing the available ligand, glutamate, led to significantly reduced melanoma cell proliferation in vitro and tumor progression in vivo. We found that simultaneous targeting of glutamate production (CB-839) and release (Riluzole) in GRM1+ melanoma cells led to additive suppression of cell proliferation in vitro. Most importantly, disruption of GRM1 signaling through combined actions of CB-839 and Riluzole significantly suppressed tumor growth in two independent xenograft mouse models of melanoma, with no obvious symptoms of toxicity detected in these mice. Taken together, these results describe a novel pathway for GRM1-mediated tumorigenesis through rewiring of cellular metabolic networks. We are continuing to investigate the mechanisms and regulation of GLS in our experimental system, with the goal of developing a rational strategy for the treatment of GRM1-expressing cancers. Citation Format: Raj Shah, Simar Singh, Kevinn Eddy, Fabian Filipp, Suzie Chen. Concurrent inhibition of glutaminase (GLS) and metabotropic receptor 1 (GRM1) reduced glutamate bioavailability and led to a decrease in GRM1-expressing melanoma cell proliferation in vitro and tumor progression in vivo [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 1839.

Published

2019

36. Refinement of the androgen response element based on ChIP-Seq in androgen-insensitive and androgen-responsive prostate cancer cell lines

Author

Fabian V. Filipp, Jianfei Qi, and Stephen Wilson

Subjects

0301 basic medicine, Male, Chromatin Immunoprecipitation, Biology, Response Elements, DNA-binding protein, Article, 03 medical and health sciences, Cell Line, Tumor, Humans, Nucleotide Motifs, Enhancer, Promoter Regions, Genetic, Transcription factor, Genetics, Multidisciplinary, Binding Sites, Prostatic Neoplasms, Promoter, Cell biology, Androgen receptor, DNA-Binding Proteins, 030104 developmental biology, Receptors, Androgen, Androgens, Neoplasm Recurrence, Local, Androgen Response Element, Sequence motif, Chromatin immunoprecipitation, Protein Binding

Abstract

Sequence motifs are short, recurring patterns in DNA that can mediate sequence-specific binding for proteins such as transcription factors or DNA modifying enzymes. The androgen response element (ARE) is a palindromic, dihexameric motif present in promoters or enhancers of genes targeted by the androgen receptor (AR). Using chromatin immunoprecipitation sequencing (ChIP-Seq) we refined AR-binding and AREs at a genome-scale in androgen-insensitive and androgen-responsive prostate cancer cell lines. Model-based searches identified more than 120,000 ChIP-Seq motifs allowing for expansion and refinement of the ARE. We classified AREs according to their degeneracy and their transcriptional involvement. Additionally, we quantified ARE utilization in response to somatic copy number amplifications, AR splice-variants, and steroid treatment. Although imperfect AREs make up 99.9% of the motifs, the degree of degeneracy correlates negatively with validated transcriptional outcome. Weaker AREs, particularly ARE half sites, benefit from neighboring motifs or cooperating transcription factors in regulating gene expression. Taken together, ARE full sites generate a reliable transcriptional outcome in AR positive cells, despite their low genome-wide abundance. In contrast, the transcriptional influence of ARE half sites can be modulated by cooperating factors.

Published

2016

37. Glutamine-fueled mitochondrial metabolism is decoupled from glycolysis in melanoma

Author

Andrei L. Osterman, Jeffrey W. Smith, Boris I. Ratnikov, David A. Scott, Fabian V. Filipp, and Jessica De Ingeniis

Subjects

Alanine, chemistry.chemical_classification, Arginine, Dermatology, Metabolism, Mitochondrion, Biology, General Biochemistry, Genetics and Molecular Biology, Amino acid, Glutamine, Citric acid cycle, Oncology, Biochemistry, chemistry, Glycolysis

Abstract

In this perspective, we revise the historic notion that cancer is a disease of mitochondria. We summarize recent findings on the function and rewiring of central carbon metabolism in melanoma. Metabolic profiling studies using stable isotope tracers show that glycolysis is decoupled from the tricarboxylic acid (TCA) cycle. This decoupling is not 'dysfunction' but rather an alternate wiring required by tumor cells to remain metabolically versatile. In large part, this requirement is met by glutamine feeding the TCA cycle as an alternative source of carbon. Glutamine is also used in non-conventional ways, like traveling in reverse through the TCA flux to feed fatty acid biosynthesis. Biosynthetic networks linked with non-essential amino acids alanine, serine, arginine, and proline are also significantly impacted by the use of glutamine as an alternate carbon source.

Published

2012

38. Unusual binding of ursodeoxycholic acid to ileal bile acid binding protein: role in activation of FXRα

Author

Jeffrey W. Smith, Fabian V. Filipp, and Changming Fang

Subjects

Isopropyl Thiogalactoside, medicine.medical_specialty, Protein Conformation, Receptors, Cytoplasmic and Nuclear, colorectal cancer, QD415-436, Plasma protein binding, Bile acid binding, Biology, Chenodeoxycholic Acid, Transfection, Biochemistry, chemistry.chemical_compound, Endocrinology, Primary biliary cirrhosis, Internal medicine, Chenodeoxycholic acid, Escherichia coli, medicine, Humans, bile salts, Binding site, Promoter Regions, Genetic, Research Articles, Binding Sites, Ursodeoxycholic Acid, Hydroxysteroid Dehydrogenases, Cooperative binding, farnesoid X receptor α, Cell Biology, medicine.disease, Recombinant Proteins, Ursodeoxycholic acid, chemistry, RNA Interference, Farnesoid X receptor, Caco-2 Cells, Plasmids, Protein Binding, medicine.drug

Abstract

Ursodeoxycholic acid (UDCA, ursodiol) is used to prevent damage to the liver in patients with primary biliary cirrhosis. The drug also prevents the progression of colorectal cancer and the recurrence of high-grade colonic dysplasia. However, the molecular mechanism by which UDCA elicits its beneficial effects is not entirely understood. The aim of this study was to determine whether ileal bile acid binding protein (IBABP) has a role in mediating the effects of UDCA. We find that UDCA binds to a single site on IBABP and increases the affinity for major human bile acids at a second binding site. As UDCA occupies one of the bile acid binding sites on IBABP, it reduces the cooperative binding that is often observed for the major human bile acids. Furthermore, IBABP is necessary for the full activation of farnesoid X receptor α (FXRα) by bile acids, including UDCA. These observations suggest that IBABP may have a role in mediating some of the intestinal effects of UDCA.

Published

2012

39. Reverse TCA cycle flux through isocitrate dehydrogenases 1 and 2 is required for lipogenesis in hypoxic melanoma cells

Author

David A. Scott, Jeffrey W. Smith, Andrei L. Osterman, Fabian V. Filipp, and Ze'ev Ronai

Subjects

Reverse Krebs cycle, Acetyl-CoA, Dermatology, Metabolism, Biology, General Biochemistry, Genetics and Molecular Biology, Glutamine, Citric acid cycle, chemistry.chemical_compound, Isocitrate dehydrogenase, Oncology, chemistry, Biochemistry, Glycolysis, Flux (metabolism)

Abstract

The tricarboxylic acid (TCA) cycle is the central hub of oxidative metabolism, running in the classic forward direction to provide carbon for biosynthesis and reducing agents for generation of ATP. Our metabolic tracer studies in melanoma cells showed that in hypoxic conditions the TCA cycle is largely disconnected from glycolysis. By studying the TCA branch point metabolites, acetyl CoA and citrate, as well as the metabolic endpoint glutamine and fatty acids, we developed a comprehensive picture of the rewiring of the TCA cycle that occurs in hypoxia. Hypoxic tumor cells maintain proliferation by running the TCA cycle in reverse. The source of carbon for acetyl CoA, citrate, and fatty acids switches from glucose in normoxia to glutamine in hypoxia. This hypoxic flux from glutamine into fatty acids is mediated by reductive carboxylation. This reductive carboxylation is catalyzed by two isocitrate dehydrogenases, IDH1 and IDH2. Their combined action is necessary and sufficient to effect the reverse TCA flux and maintain cellular viability.

Published

2012

40. An epigenetic master regulator teams up to become an epioncogene

Author

Jianfei Qi and Fabian V. Filipp

Subjects

0301 basic medicine, precision medicine, master regulator, Master regulator, cancer systems biology, Computational biology, Biology, Precision medicine, 03 medical and health sciences, Editorial, 030104 developmental biology, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, Cancer systems biology, epigenomics, transcription factor network, Epigenetics, Epigenomics

Published

2017

41. Comparative Metabolic Flux Profiling of Melanoma Cell Lines

Author

Ze'ev Ronai, Fabian V. Filipp, Andrei L. Osterman, Jeffrey W. Smith, David A. Scott, Christine A. Knutzen, Gary G. Chiang, and Adam D. Richardson

Subjects

Melanoma, Pasteur effect, Cell Biology, Metabolism, Biology, medicine.disease, Biochemistry, Warburg effect, Flux balance analysis, Glutamine, Citric acid cycle, medicine, Glycolysis, Molecular Biology

Abstract

Metabolic rewiring is an established hallmark of cancer, but the details of this rewiring at a systems level are not well characterized. Here we acquire this insight in a melanoma cell line panel by tracking metabolic flux using isotopically labeled nutrients. Metabolic profiling and flux balance analysis were used to compare normal melanocytes to melanoma cell lines in both normoxic and hypoxic conditions. All melanoma cells exhibited the Warburg phenomenon; they used more glucose and produced more lactate than melanocytes. Other changes were observed in melanoma cells that are not described by the Warburg phenomenon. Hypoxic conditions increased fermentation of glucose to lactate in both melanocytes and melanoma cells (the Pasteur effect). However, metabolism was not strictly glycolytic, as the tricarboxylic acid (TCA) cycle was functional in all melanoma lines, even under hypoxia. Furthermore, glutamine was also a key nutrient providing a substantial anaplerotic contribution to the TCA cycle. In the WM35 melanoma line glutamine was metabolized in the “reverse” (reductive) direction in the TCA cycle, particularly under hypoxia. This reverse flux allowed the melanoma cells to synthesize fatty acids from glutamine while glucose was primarily converted to lactate. Altogether, this study, which is the first comprehensive comparative analysis of metabolism in melanoma cells, provides a foundation for targeting metabolism for therapeutic benefit in melanoma.

Published

2011

42. Abstract 5493: Targeted inhibition of glutaminase in GRM1-expressing melanoma cells inhibits cell proliferation by reducing glutamate bioavailability

Author

Suzie Chen, Fabian V. Filipp, Raj Shah, Mengying Zhu, and Andrew J. Boreland

Subjects

Cancer Research, Cell growth, Chemistry, Glutaminase, Glutamate receptor, Riluzole, Glutamatergic, Oncology, Cancer research, medicine, Metabotropic glutamate receptor 1, Neoplastic transformation, Autocrine signalling, medicine.drug

Abstract

Aberrant glutamatergic signaling has been implicated in many cancer types. Our laboratory has previously illustrated the role of metabotropic glutamate receptor 1 (GRM1) in neoplastic transformation of melanocytes in vitro and spontaneous metastatic melanoma in vivo. Glutamate, the natural ligand of GRM1 is also the predominant excitatory neurotransmitter in the central nervous system. We have demonstrated significant upregulation of glutaminase (GLS) expression in GRM1 expressing melanoma cells, resulting in excess glutamate production and the establishment of autocrine loops in vitro. GLS catalyzes the first step in glutamine metabolism–the conversion of glutamine to glutamate. Comparison of glutamate levels in circulating blood plasma between melanoma prone and wild type mice showed elevated glutamate levels in melanoma prone GRM1-transgenic mice, suggesting that aberrant GRM1 expression also promotes an increase in circulating glutamate, to ensure constitutive activation of the GRM1 receptor and its downstream signaling affecters in vivo. Inclusion of CB-839, a potent, selective, and orally bioavailable inhibitor of GLS, resulted in significant inhibition of GRM1+ melanoma cell proliferation compared to GRM1- ones. We also demonstrated that treatment with Riluzole, an inhibitor of glutamatergic signaling by decreasing the available ligand, glutamate, led to significantly reduced melanoma cell proliferation in vitro and tumor progression in vivo. We found that simultaneous targeting of glutamate production (CB-839) and release (Riluzole) in GRM1+ melanoma cells led to synergistic suppression of cell proliferation in vitro. Furthermore, we found that CB-839 altered the function not the expression of GLS in melanoma cells. Additionally, we also discovered that manipulation of GRM1 expression by genetic means led to robust parallel changes in gene expression levels and intracellular glutamate concentrations by mass spectrometry analysis, as well as the endogenous levels of GLS in melanoma cells, suggesting association between GRM1 and GLS. The sensitivity of GRM1+ melanoma cells to modulation of GLS point to the dependency of these cells to glutamate amounts via GLS activity. We are continuing to investigate the mechanisms and regulation of GLS in our experimental system, with the goal of developing a rational approach for the treatment of GRM1 expressing tumors. Citation Format: Raj Shah, Mengying Zhu, Andrew Boreland, Fabian Filipp, Suzie Chen. Targeted inhibition of glutaminase in GRM1-expressing melanoma cells inhibits cell proliferation by reducing glutamate bioavailability [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 5493.

Published

2018

43. Labeling strategies for 13C-detected aligned-sample solid-state NMR of proteins

Author

Stanley J. Opella, Neeraj Sinha, Lena Jairam, Joel Bradley, and Fabian V. Filipp

Subjects

Carbon Isotopes, Nuclear and High Energy Physics, Magnetic Resonance Spectroscopy, Chemistry, Biophysics, Analytical chemistry, Nuclear magnetic resonance spectroscopy, Condensed Matter Physics, Biochemistry, Article, Phase Transition, Homonuclear molecule, Isotopic labeling, Bacterial protein, Bacterial Proteins, Solid-state nuclear magnetic resonance, Isotopes of carbon, Isotope Labeling, Peptide bond, Powders

Abstract

(13)C-detected solid-state NMR experiments have substantially higher sensitivity than the corresponding (15)N-detected experiments on stationary, aligned samples of isotopically labeled proteins. Several methods for tailoring the isotopic labeling are described that result in spatially isolated (13)C sites so that dipole-dipole couplings among the (13)C are minimized, thus eliminating the need for homonuclear (13)C-(13)C decoupling in either indirect or direct dimensions of one- or multi-dimensional NMR experiments that employ (13)C detection. The optimal percentage for random fractional (13)C labeling is between 25% and 35%. Specifically labeled glycerol and glucose can be used at the carbon sources to tailor the isotopic labeling, and the choice depends on the resonances of interest for a particular study. For investigations of the protein backbone, growth of the bacteria on [2-(13)C]-glucose-containing media was found to be most effective.

Published

2009

44. Probing lipid- and drug-binding domains with fluorescent dyes

Author

Matthias Wilmanns, Michael Sattler, Shannon L. Black, Michelle Bhairo, Ashwani Verma, Oliver Wichmann, Will A. Stanley, Carsten Schultz, and Fabian V. Filipp

Subjects

Models, Molecular, Alkylation, Clinical Biochemistry, Pharmaceutical Science, Calorimetry, Biochemistry, Article, chemistry.chemical_compound, Phenothiazine, Drug Discovery, Animals, Humans, Bovine serum albumin, Binding site, Molecular Biology, Fluorescent Dyes, Chromatography, Molecular Structure, biology, Organic Chemistry, Titrimetry, Nile red, Serum Albumin, Bovine, Isothermal titration calorimetry, Lipids, Fluorescence, Pharmaceutical Preparations, chemistry, biology.protein, Biophysics, Butyric Acid, Molecular Medicine, Cattle, Titration, Carrier Proteins, Plant lipid transfer proteins

Abstract

A series of 2- and 3-OH Nile red dyes was prepared in order to generate water-soluble probes that could be used to probe lipid binding to proteins. Various substitutions in positions 2-/3-, 6-, and 7-shifted wavelengths while maintaining the environmental sensitivity of Nile red. In order to increase the solubility of the dyes in aqueous solutions, we attached butyric acid groups to the 2- or 3-OH position. In addition, phenothiazine dyes, which exhibited particularly long excitation properties, were synthesized and tested for the first time. All dyes showed Stoke’s shifts of 70–100 nm and changes in excitation and emission of over 100 nm, depending on the hydrophobicity of the environment. Binding studies with bovine serum albumin and the non-specific lipid transfer protein SCP2 revealed emission changes of more than 30 nm upon binding to the protein and a five-fold increase in emission intensity. Titration of the dye-loaded proteins with various lipids or drugs replaced the dye and thereby reversed the shift in wavelength intensity. This allowed us to estimate the lipid binding affinity of the investigated proteins. For SCP2, isothermal calorimetry (ITC) data verified the titration experiments. NMR titration experiments of SCP2 with Nile red 2-O-butyric acid (1a) revealed that the dye is bound within the lipid binding pocket and competes with lipid ligands for this binding site. These results give valuable insight into lipid and drug transport by proteins outside and inside cells.

Published

2008

45. Conformational Plasticity of the Lipid Transfer Protein SCP2

Author

Fabian V. Filipp and Michael Sattler

Subjects

Models, Molecular, Fatty acid metabolism, Protein Conformation, Chemistry, Chemical shift, Relaxation (NMR), Electron Spin Resonance Spectroscopy, Nanosecond, Ligands, Biochemistry, Article, Microsecond, chemistry.chemical_compound, Crystallography, Sterol carrier protein, Biophysics, Spin Labels, Carrier Proteins, Plant lipid transfer proteins, Protein Binding, SCP2

Abstract

The nonspecific lipid transfer protein sterol carrier protein 2 (SCP2) is involved in organellar fatty acid metabolism. A hydrophobic cavity in the structure of SCP2 accommodates a wide variety of apolar ligands such as cholesterol derivatives or fatty acyl-coenzyme A (CoA) conjugates. The properties of this nonspecific lipid binding pocket are explored using NMR chemical shift perturbations, paramagnetic relaxation enhancement, amide hydrogen exchange, and 15N relaxation measurements. A common binding cavity shared by different physiological ligands is identified. NMR relaxation measurements reveal that residues in the three C-terminal alpha-helices within the lipid binding region exhibit mobility at fast (picosecond to nanosecond) and slow (microsecond to millisecond) time scales. Ligand binding is associated with a considerable loss of peptide backbone mobility. The observed conformational dynamics in SCP2 may play a role for the access of hydrophobic ligands to an occluded binding pocket. The C-terminal peroxisomal targeting signal of SCP2 is specifically recognized by the Pex5p receptor protein, which conducts cargo proteins toward the peroxisomal organelle. Neither the C-terminal targeting signal nor the N-terminal precursor sequence interferes with lipid binding by SCP2. The alpha-helices involved in lipid binding also mediate a secondary interaction interface with the Pex5p receptor. Silencing of conformational dynamics of the peptide backbone in these helices upon either lipid or Pex5p binding might communicate the loading state of the cargo protein to the targeting receptor.

Published

2007

46. Tailoring13C labeling for triple-resonance solid-state NMR experiments on aligned samples of proteins

Author

Fabian V. Filipp, Stanley J. Opella, Neeraj Sinha, Joel Bradley, Sang Ho Park, and Lena Jairam

Subjects

Viral Structural Proteins, Carbon Isotopes, Magnetic Resonance Spectroscopy, Magic angle, Chemistry, Viral Core Proteins, Analytical chemistry, Membrane Proteins, General Chemistry, Nuclear magnetic resonance spectroscopy, Micelle, Article, Homonuclear molecule, NMR spectra database, Isotopic labeling, Solid-state nuclear magnetic resonance, Bacteriophages, General Materials Science, Magnetic dipole–dipole interaction

Abstract

In order to develop triple-resonance solid-state NMR spectroscopy of membrane proteins, we have implemented several different 13C labeling schemes with the purpose of overcoming the interfering effects of 13C13C dipole–dipole couplings in stationary samples. The membrane-bound form of the major coat protein of the filamentous bacteriophage Pf1 was used as an example of a well-characterized helical membrane protein. Aligned protein samples randomly enriched to 35% 13C in all sites and metabolically labeled from bacterial growth on media containing [2-13C]-glycerol or [1,3-13C]-glycerol enables direct 13C detection in solid-state NMR experiments without the need for homonuclear 13C13C dipole–dipole decoupling. The 13C-detected NMR spectra of Pf1 coat protein show a substantial increase in sensitivity compared to the equivalent 15N-detected spectra. The isotopic labeling pattern was analyzed for [2-13C]-glycerol and [1,3-13C]-glycerol as metabolic precursors by solution-state NMR of micelle samples. Polarization inversion spin exchange at the magic angle (PISEMA) and other solid-state NMR experiments work well on 35% random fractionally and metabolically tailored 13C-labeled samples, in contrast to their failure with conventional 100% uniformly 13C-labeled samples. Copyright © 2007 John Wiley & Sons, Ltd.

Published

2007

47. Hypermutation of DPYD Deregulates Pyrimidine Metabolism and Promotes Malignant Progression

Author

Fabian V. Filipp, Lauren Edwards, and Rohit Gupta

Subjects

0301 basic medicine, Models, Molecular, Cancer Research, Mutation rate, Skin Neoplasms, Somatic cell, Somatic hypermutation, Biology, Article, 03 medical and health sciences, medicine, Dihydropyrimidine dehydrogenase, Humans, Molecular Biology, Gene, Melanoma, Dihydrouracil Dehydrogenase (NADP), Genetics, Binding Sites, Systems Biology, medicine.disease, 030104 developmental biology, Pyrimidines, Oncology, Pyrimidine metabolism, Mutation, Cancer research, Disease Progression, DPYD

Abstract

New strategies are needed to diagnose and target human melanoma. To this end, genomic analyses was performed to assess somatic mutations and gene expression signatures using a large cohort of human skin cutaneous melanoma (SKCM) patients from The Cancer Genome Atlas (TCGA) project to identify critical differences between primary and metastatic tumors. Interestingly, pyrimidine metabolism is one of the major pathways to be significantly enriched and deregulated at the transcriptional level in melanoma progression. In addition, dihydropyrimidine dehydrogenase ( DPYD ) and other important pyrimidine-related genes: DPYS , AK9 , CAD , CANT1 , ENTPD1 , NME6 , NT5C1A , POLE , POLQ , POLR3B , PRIM2 , REV3L , and UPP2 are significantly enriched in somatic mutations relative to the background mutation rate. Structural analysis of the DPYD protein dimer reveals a potential hotspot of recurring somatic mutations in the ligand-binding sites as well as the interfaces of protein domains that mediated electron transfer. Somatic mutations of DPYD are associated with upregulation of pyrimidine degradation, nucleotide synthesis, and nucleic acid processing while salvage and nucleotide conversion is downregulated in TCGA SKCM. Implications: At a systems biology level, somatic mutations of DPYD cause a switch in pyrimidine metabolism and promote gene expression of pyrimidine enzymes toward malignant progression. Mol Cancer Res; 14(2); 196–206. ©2015 AACR . This article is featured in Highlights of This Issue, [p. 125][1] [1]: /lookup/volpage/14/125?iss=2

Published

2015

48. Pharmacogenomic and clinical data link non-pharmacokinetic metabolic dysregulation to drug side effect pathogenesis

Author

Daniel C. Zielinski, Fabian V. Filipp, Kasper Lynge Jensen, Aarash Bordbar, Monica L. Mo, Bernhard O. Palsson, Markus J. Herrgård, and Jeffrey W. Smith

Subjects

Drug, Side effect, Databases, Factual, Drug-Related Side Effects and Adverse Reactions, Bioinformatics, media_common.quotation_subject, General Physics and Astronomy, Metabolic network, Drug action, Biology, Pharmacology, General Biochemistry, Genetics and Molecular Biology, Article, Databases, Medical research, SDG 3 - Good Health and Well-being, Genetics, Humans, 2.1 Biological and endogenous factors, Aetiology, Factual, Metabolic and endocrine, media_common, Nutrition, 2. Zero hunger, Multidisciplinary, Mechanism (biology), General Chemistry, 3. Good health, Biological sciences, Cell metabolism, Good Health and Well Being, Pharmacogenetics, 5.1 Pharmaceuticals, Pharmacogenomics, Patient Safety, Development of treatments and therapeutic interventions

Abstract

Drug side effects cause a significant clinical and economic burden. However, mechanisms of drug action underlying side effect pathogenesis remain largely unknown. Here, we integrate pharmacogenomic and clinical data with a human metabolic network and find that non-pharmacokinetic metabolic pathways dysregulated by drugs are linked to the development of side effects. We show such dysregulated metabolic pathways contain genes with sequence variants affecting side effect incidence, play established roles in pathophysiology, have significantly altered activity in corresponding diseases, are susceptible to metabolic inhibitors and are effective targets for therapeutic nutrient supplementation. Our results indicate that metabolic dysregulation represents a common mechanism underlying side effect pathogenesis that is distinct from the role of metabolism in drug clearance. We suggest that elucidating the relationships between the cellular response to drugs, genetic variation of patients and cell metabolism may help managing side effects by personalizing drug prescriptions and nutritional intervention strategies., Adverse drug reactions are an important clinical problem. Here the authors combine information about drug-induced gene expression changes and genetic variability of patients with a genome-scale metabolic model to identify drug-induced changes in cellular metabolism that may be linked to drug side effects.

Published

2015

49. Recognition of a Functional Peroxisome Type 1 Target by the Dynamic Import Receptor Pex5p

Author

Petri Kursula, Ralf Erdmann, Will A. Stanley, Wolfgang Schliebs, Michael Sattler, Nicole Schüller, Matthias Wilmanns, and Fabian V. Filipp

Subjects

Models, Molecular, Protein Folding, Peroxisome-Targeting Signal 1 Receptor, Protein Conformation, Molecular Sequence Data, Receptors, Cytoplasmic and Nuclear, Chromosomal translocation, Biology, Crystallography, X-Ray, Article, Peroxisomes, Humans, Amino Acid Sequence, Receptor, Molecular Biology, Peroxisomal targeting signal, Binding Sites, Cell Biology, Peroxisome, Protein Structure, Tertiary, Cell biology, Transport protein, Protein Transport, Tetratricopeptide, Sterol carrier protein, Biochemistry, Function (biology)

Abstract

Peroxisomes require the translocation of folded and functional target proteins of various sizes across the peroxisomal membrane. We have investigated the structure and function of the principal import receptor Pex5p, which recognizes targets bearing a C-terminal peroxisomal targeting signal type 1. Crystal structures of the receptor in the presence and absence of a peroxisomal target, sterol carrier protein 2, reveal major structural changes from an open, snail-like conformation into a closed, circular conformation. These changes are caused by a long loop C terminal to the 7-fold tetratricopeptide repeat segments. Mutations in residues of this loop lead to defects in peroxisomal import in human fibroblasts. The structure of the receptor/cargo complex demonstrates that the primary receptor-binding site of the cargo is structurally and topologically autonomous, enabling the cargo to retain its native structure and function.

Published

2006

50. Determinants of conformational dimerization of Mad2 and its inhibition by p31comet

Author

Andrea Musacchio, Stefano Confalonieri, Gunter Stier, Giulia Rancati, Luigi Nezi, Fabian V. Filipp, Simonetta Piatti, Michael Sattler, Marina Mapelli, Lucia Massimiliano, and Robert S. Hagan

Subjects

Models, Molecular, Mad2, Mad1, Cdc20 Proteins, Protein Conformation, Molecular Sequence Data, Cell Cycle Proteins, Saccharomyces cerevisiae, Spindle Apparatus, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Mad2 Proteins, Humans, Amino Acid Sequence, Prometaphase, Kinetochores, Nuclear Magnetic Resonance, Biomolecular, Molecular Biology, Adaptor Proteins, Signal Transducing, Binding Sites, Sequence Homology, Amino Acid, General Immunology and Microbiology, Kinetochore, General Neuroscience, Calcium-Binding Proteins, Nuclear Proteins, Mitotic checkpoint complex, Spindle apparatus, Repressor Proteins, Spindle checkpoint, Biochemistry, Mutation, Biophysics, Carrier Proteins, Dimerization, Biologie

Abstract

The spindle assembly checkpoint (SAC) monitors chromosome attachment to spindle microtubules. SAC proteins operate at kinetochores, scaffolds mediating chromosome-microtubule attachment. The ubiquitous SAC constituents Mad1 and Mad2 are recruited to kinetochores in prometaphase. Mad2 sequesters Cdc20 to prevent its ability to mediate anaphase onset. Its function is counteracted by p31comet (formerly CMT2). Upon binding Cdc20, Mad2 changes its conformation from O-Mad2 (Open) to C-Mad2 (Closed). A Mad1-bound C-Mad2 template, to which O-Mad2 binds prior to being converted into Cdc20-bound C-Mad2, assists this process. A molecular understanding of this prion-like property of Mad2 is missing. We characterized the molecular determinants of the O-Mad2:C-Mad2 conformational dimer and derived a rationalization of the binding interface in terms of symmetric and asymmetric components. Mutation of individual interface residues abrogates the SAC in Saccharomyces cerevisiae. NMR chemical shift perturbations indicate that O-Mad2 undergoes a major conformational rearrangement upon binding C-Mad2, suggesting that dimerization facilitates the structural conversion of O-Mad2 required to bind Cdc20. We also show that the negative effects of p31comet on the SAC are based on its competition with O-Mad2 for C-Mad2 binding.

Published

2006