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1. Full Text Deleting Full Length Titin Versus the Titin M-Band Region Leads to Differential Mechanosignaling and Cardiac Phenotypes
by Radke, Michael H and Polack, Christopher and Methawasin, Mei and Fink, Claudia and Granzier, Henk L and Gotthardt, Michael
Circulation, ISSN 0009-7322, 04/2019, Volume 139, Issue 15, pp. 1813 - 1827
BACKGROUND:Titin is a giant elastic protein that spans the half-sarcomere from Z-disk to M-band. It acts as a molecular spring and mechanosensor and has been... 
models, animal | muscles | myocardial contraction | hypertrophy | cardiomyopathies | heart diseases | Proteins | Cardiomyopathy | Physiological aspects | Cellular signal transduction | Research | Cardiovascular research | Muscle proteins | Structure | Health aspects | Heart diseases | Risk factors | Heart muscle
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2. Full Text M Line-Deficient Titin Causes Cardiac Lethality through Impaired Maturation of the Sarcomere
by Stefanie Weinert and Nora Bergmann and Xiuju Luo and Bettina Erdmann and Michael Gotthardt
The Journal of Cell Biology, ISSN 0021-9525, 5/2006, Volume 173, Issue 4, pp. 559 - 570
Titin, the largest protein known to date, has been linked to sarcomere assembly and function through its elastic adaptor and signaling domains. Titin's M-line... 
Protein isoforms | Cell motility | Phenotypes | RNA probes | Antibodies | Myocardium | Region of integration | Embryos | Sarcomeres | Myofibrils | IMMUNOELECTRON MICROSCOPY | ACTIVATED SKELETAL-MUSCLE | MOLECULAR-STRUCTURE | MUSCULAR-DYSTROPHY | MYOSIN BINDING | M-BAND | THICK FILAMENTS | Z-DISK | KINASE DOMAIN | ALPHA-ACTININ | CELL BIOLOGY | Protein Kinases - metabolism | Phosphorylation | Protein Kinases - genetics | Connectin | Heart Defects, Congenital - embryology | Heart - embryology | Gene Expression Regulation, Developmental - genetics | Protein Kinases - chemistry | Male | Heart Defects, Congenital - genetics | Myocardium - metabolism | Muscle Proteins - metabolism | Female | Microscopy, Electron, Transmission | Sarcomeres - metabolism | Protein Structure, Tertiary - genetics | Mutation - genetics | Mice, Knockout | Muscle Proteins - genetics | Sarcomeres - ultrastructure | Animals | Genes, Lethal - genetics | Myocytes, Cardiac - metabolism | Mice | Muscle Proteins - chemistry | Myocytes, Cardiac - ultrastructure | Protein Binding - physiology | Binding proteins | Maturation (Psychology) | Health aspects | Abnormalities
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3. Full Text Dense genotyping of immune-related disease regions identifies nine new risk loci for primary sclerosing cholangitis
by Liu, Jimmy Z and Hov, Johannes Roksund and Folseraas, Trine and Ellinghaus, Eva and Rushbrook, Simon M and Doncheva, Nadezhda T and Aneassen, Ole A and Weersma, Rinse K and Weismüller, Tobias J and Eksteen, Bertus and Invernizzi, Pietro and Hirschfield, Gideon M and Gotthardt, Daniel Nils and Pares, Albert and Ellinghaus, David and Shah, Tejas and Juran, Brian D and Milkiewicz, Piotr and Rust, Christian and Schramm, Christoph and Müller, Tobias and Srivastava, Brijesh and Dalekos, Georgios and Nöthen, Markus M and Herms, Stefan and Winkelmann, Juliane and Mitrovic, Mitja and Braun, Felix and Ponsioen, Cyriel Y and Croucher, Peter J. P and Sterneck, Martina and Teufel, Aneas and Mason, Anew L and Saarela, Janna and Leppa, Virpi and Dorfman, Ruslan and Alvaro, Domenico and Floreani, Annarosa and Onengut-Gumuscu, Suna and Rich, Stephen S and Thompson, Wesley K and Schork, Anew J and Næss, Sigrid and Thomsen, Ingo and Mayr, Gabriele and König, Inke R and Hveem, Kristian and Cleynen, Isabelle and Gutierrez-Achury, Javier and Ricaño-Ponce, Isis and van Heel, David and Björnsson, Einar and Sandford, Richard N and Durie, Peter R and Melum, Espen and Vatn, Morten H and Silverberg, Mark S and Duerr, Richard H and Padyukov, Leonid and Brand, Stephan and Sans, Miquel and Annese, Vito and Achkar, Jean-Paul and Boberg, Kirsten Muri and Marschall, Hanns-Ulrich and Chazouillères, Olivier and Bowlus, Christopher L and Wijmenga, Cisca and Schrumpf, Erik and Vermeire, Severine and Albrecht, Mario and Rioux, John D and Alexander, Graeme and Bergquist, Annika and Cho, Judy and Schreiber, Stefan and Manns, Michael P and Färkkilä, Martti and Dale, Anders M and Chapman, Roger W and Lazaridis, Konstantinos N and Franke, Ane and Anderson, Carl A and Karlsen, Tom H and Int PSCSC Study Grp and UK-PSCSC Consortium and Int IBD Genetics Consortium and International PSC Study Group and International IBD Genetics Consortium and The UK-PSCSC Consortium and The International IBD Genetics Consortium and The International PSC Study Group and Sahlgrenska akademin and Institute of Medicine, Department of Internal Medicine and Clinical Nutrition and Göteborgs universitet and Gothenburg University and Institutionen för medicin, avdelningen för invärtesmedicin och klinisk nutrition and Sahlgrenska Academy
Nature genetics, ISSN 1061-4036, 2013, Volume 45, Issue 6, pp. 670 - 675
Primary sclerosing cholangitis (PSC) is a severe liver disease of unknown etiology leading to fibrotic destruction of the bile ducts and ultimately to the need... 
FALSE DISCOVERY RATE | MIXED-MODEL | GENETIC RISK | ULCERATIVE-COLITIS | GENETICS & HEREDITY | SUSCEPTIBILITY LOCI | NATURAL-HISTORY | HLA | HISTONE DEACETYLASE | GENOME-WIDE ASSOCIATION | BOWEL-DISEASE | Genome-Wide Association Study | Oligonucleotide Array Sequence Analysis | Gene Frequency | Humans | Risk Factors | Cholangitis, Sclerosing - genetics | Genetic Pleiotropy | Genotyping Techniques | Case-Control Studies | Linkage Disequilibrium | Genetic Loci - immunology | Cholangitis, Sclerosing - immunology | Polymorphism, Single Nucleotide | Usage | Histocompatibility antigens | Liver | Cholangitis | HLA histocompatibility antigens | Genotype | Genetic aspects | Transplantation | Research | Health aspects | Risk factors | Proteins | Inflammatory bowel disease | Pathogenesis | Genes | Quality control | Genetics | T cell receptors | Genomes | Diabetes | Kinases | Autoimmune diseases | Methods | immunogenetics | liver | disease genetics | genetic association study | Sclerosing | Genetic Loci | Single Nucleotide | Medicinsk genetik | Medical Genetics | genetics | immunology | Polymorphism
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4. Full Text Genome-wide association study of primary sclerosing cholangitis identifies new risk loci and quantifies the genetic relationship with inflammatory bowel disease
by Ji, Sun-Gou and Juran, Brian D and Mucha, Soeren and Folseraas, Trine and Jostins, Luke and Melum, Espen and Kumasaka, Natsuhiko and Atkinson, Elizabeth J and Schlicht, Erik M and Liu, Jimmy Z and Shah, Tejas and Gutierrez-Achury, Javier and Boberg, Kirsten M and Bergquist, Annika and Vermeire, Severine and Eksteen, Bertus and Durie, Peter R and Farkkila, Martti and Mueller, Tobias and Schramm, Christoph and Sterneck, Martina and Weismueller, Tobias J and Gotthardt, Daniel Nils and Ellinghaus, David and Braun, Felix and Teufel, Aneas and Laudes, Mattias and Lieb, Wolfgang and Jacobs, Gunnar and Beuers, Ulrich and Weersma, Rinse K and Wijmenga, Cisca and Marschall, Hanns-Ulrich and Milkiewicz, Piotr and Pares, Albert and Kontula, Kimmo and Chazouilleres, Olivier and Invernizzi, Pietro and Goode, Elizabeth and Spiess, Kelly and Moore, Carmel and Sambrook, Jennifer and Ouwehand, Willem H and Roberts, David J and Danesh, John and Floreani, Annarosa and Gulamhusein, Aliya F and Eaton, John E and Schreiber, Stefan and Coltescu, Catalina and Int PSC Study Grp and UK-PSC Consortium and Int IBD Genetics Consortium and International PSC Study Group and International IBD Genetics Consortium and The International IBD Genetics Consortium and The International PSC Study Group and The UK-PSC Consortium and Sahlgrenska akademin and Institute of Medicine, Department of Molecular and Clinical Medicine and Institutionen för medicin, avdelningen för molekylär och klinisk medicin and Göteborgs universitet and Gothenburg University and Sahlgrenska Academy
Nature Genetics, ISSN 1061-4036, 02/2017, Volume 49, Issue 2, pp. 269 - 273
Primary sclerosing cholangitis (PSC) is a rare progressive disorder leading to bile duct destruction; similar to 75% of patients have comorbid inflammatory... 
METAANALYSIS | TRANSCRIPTOME | VARIANTS | ULCERATIVE-COLITIS | REGIONS | SUSCEPTIBILITY LOCI | PSORIATIC-ARTHRITIS | REVEALS | GENETICS & HEREDITY | Humans | RNA, Messenger - genetics | Risk Factors | Adaptor Proteins, Signal Transducing - genetics | Alleles | Cholangitis, Sclerosing - genetics | Colitis, Ulcerative - genetics | Inflammatory Bowel Diseases - genetics | Polymorphism, Single Nucleotide - genetics | Genome-Wide Association Study - methods | Quantitative trait loci | Inflammatory bowel diseases | Cholangitis | Development and progression | Genetic aspects | Identification and classification | Health aspects | Risk factors | Inflammatory bowel disease | Consortia | Medical research | Celiac disease | Biomedical research | Transplants & implants | Genes | Quality control | Genetics | Genomes | Grants | Inflammation | Gastroenterologia | Inflamació | Malalties inflamatòries intestinals | Gastroenterology | Gastroenterology and Hepatology | Gastroenterologi
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5. Full Text Altered contractility of skeletal muscle in mice deficient in titin's M-Band region
by Ottenheijm, C.A.C and Hidalgo, C and Rost, K and Gotthardt, M and Granzier, H
Journal of Molecular Biology, ISSN 0022-2836, 2009, Volume 393, Issue 1, pp. 10 - 26
We investigated the contractile phenotype of skeletal muscle deficient in exons MEx1 and MEx2 (KO) of the titin M-band by using the cre-lox recombination... 
titin | M-band | sensitivity | skeletal muscle | BINDING-PROTEIN-C | BIOCHEMISTRY & MOLECULAR BIOLOGY | Ca2+ sensitivity | CARDIAC-MUSCLE | MOLECULAR-WEIGHT PROTEINS | KINASE DOMAIN | MOUSE MYOCARDIUM | PASSIVE TENSION | TIBIAL MUSCULAR-DYSTROPHY | M-LINE | STRIATED-MUSCLE | RING FINGER PROTEINS | Sequence Deletion | Connectin | Calcium - metabolism | Exons | Carrier Proteins - biosynthesis | Muscle Proteins - deficiency | Muscle, Skeletal - physiology | Animals | Muscle Contraction | Models, Biological | Recombination, Genetic | Mice | Protein Kinases - deficiency | Cell research | Analysis | Myosin | Physiological aspects | Protein C | Muscle proteins | Binding proteins | Protein binding
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6. Full Text Conditional Expression of Mutant M-line Titins Results in Cardiomyopathy with Altered Sarcomere Structure
by Michael Gotthardt and Robert E. Hammer and Norbert Hübner and Jan Monti and Christian C. Witt and Mark McNabb and James A. Richardson and Henk Granzier and Siegfried Labeit and Joachim Herz
Journal of Biological Chemistry, ISSN 0021-9258, 02/2003, Volume 278, Issue 8, pp. 6059 - 6065
Titin is a giant protein responsible for muscle elasticity and provides a scaffold for several sarcomeric proteins, including the novel titin-binding protein... 
LIGHT-CHAIN KINASE | IMMUNOELECTRON MICROSCOPY | ELASTICITY | FAMILIAL DILATED CARDIOMYOPATHY | GENE | BIOCHEMISTRY & MOLECULAR BIOLOGY | CRE RECOMBINASE | MUSCLE | ANKYRIN-REPEAT PROTEIN | C-ELEGANS | DROSOPHILA | Protein Kinases - metabolism | Protein Kinases - genetics | Connectin | Elasticity | Myosin Heavy Chains - genetics | Protein Kinases - chemistry | Muscle Proteins - deficiency | Actins - genetics | Sarcomeres - pathology | Cardiomyopathies - genetics | Recombination, Genetic | Chromosomes, Artificial, Bacterial | Cloning, Molecular | Muscle Proteins - metabolism | Protein Kinases - deficiency | Binding Sites | Promoter Regions, Genetic | Major Histocompatibility Complex | Gene Expression Regulation | Cardiomyopathies - pathology | Muscle, Skeletal - physiology | Organ Specificity | Mice, Knockout | Muscle Proteins - genetics | Sarcomeres - ultrastructure | Animals | Stem Cells - physiology | Mice | Muscle Proteins - chemistry
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7. Full Text Genetic association analysis identifies variants associated with disease progression in primary sclerosing cholangitis
by Alberts, Rudi and de Vries, Elisabeth M G and Goode, Elizabeth C and Jiang, Xiaojun and Sampaziotis, Fotis and Rombouts, Krista and Böttcher, Katrin and Folseraas, Trine and Weismüller, Tobias J and Mason, Andrew L and Wang, Weiwei and Alexander, Graeme and Alvaro, Domenico and Bergquist, Annika and Björkström, Niklas K and Beuers, Ulrich and Björnsson, Einar and Boberg, Kirsten Muri and Bowlus, Christopher L and Bragazzi, Maria C and Carbone, Marco and Chazouillères, Olivier and Cheung, Angela and Dalekos, Georgios and Eaton, John and Eksteen, Bertus and Ellinghaus, David and Färkkilä, Martti and Festen, Eleonora A M and Floreani, Annarosa and Franceschet, Irene and Gotthardt, Daniel Nils and Hirschfield, Gideon M and Hoek, Bart van and Holm, Kristian and Hohenester, Simon and Hov, Johannes Roksund and Imhann, Floris and Invernizzi, Pietro and Juran, Brian D and Lenzen, Henrike and Lieb, Wolfgang and Liu, Jimmy Z and Marschall, Hanns-Ulrich and Marzioni, Marco and Melum, Espen and Milkiewicz, Piotr and Müller, Tobias and Pares, Albert and Rupp, Christian and Rust, Christian and Sandford, Richard N and Schramm, Christoph and Schreiber, Stefan and Schrumpf, Erik and Silverberg, Mark S and Srivastava, Brijesh and Sterneck, Martina and Teufel, Andreas and Vallier, Ludovic and Verheij, Joanne and Vila, Arnau Vich and Vries, Boudewijn de and Zachou, Kalliopi and Chapman, Roger W and Manns, Michael P and Pinzani, Massimo and Rushbrook, Simon M and Lazaridis, Konstantinos N and Franke, Andre and Anderson, Carl A and Karlsen, Tom H and Ponsioen, Cyriel Y and Weersma, Rinse K and PSC Study Grp and UK PSC Consortium and International PSC Study Group, The UK PSC Consortium and Sahlgrenska akademin and Institute of Medicine, Department of Molecular and Clinical Medicine and Institutionen för medicin, avdelningen för molekylär och klinisk medicin and Göteborgs universitet and Gothenburg University and Sahlgrenska Academy
Gut, ISSN 0017-5749, 08/2018, Volume 67, Issue 8, pp. 1517 - 1524
ObjectivePrimary sclerosing cholangitis (PSC) is a genetically complex, inflammatory bile duct disease of largely unknown aetiology often leading to liver... 
Primary sclerosing cholangitis | liver transplantation | genetics | RISK LOCI | ACTIVATION | MALIGNANCY | HEPATIC STELLATE CELLS | CIRRHOSIS | ULCERATIVE-COLITIS | LIVER FIBROSIS | GASTROENTEROLOGY & HEPATOLOGY | MULTIPLE | EPIDEMIOLOGY | GENOME-WIDE ASSOCIATION | Animal models | Transplants & implants | Disease | Syngeneic grafts | Association analysis | Effector cells | Genomes | Single-nucleotide polymorphism | Allografts | Etiology | Gastroenterology | Genetic analysis | Gallbladder | Antigens | Stellate cells | Liver diseases | Cholangitis | Regression analysis | Gene expression | Bile duct | Inflammatory bowel disease | Genetic variance | Hepatocytes | Quality control | Liver cirrhosis | Bile | Liver transplantation | Gastroenterology and Hepatology | Gastroenterologi
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8. Full Text Coxsackie and Adenovirus Receptor Is a Modifier of Cardiac Conduction and Arrhythmia Vulnerability in the Setting of Myocardial Ischemia
by Marsman, Roos F.J., MSc and Bezzina, Connie R., PhD and Freiberg, Fabian, MSc and Verkerk, Arie O., PhD and Adriaens, Michiel E., PhD and Podliesna, Svitlana, MSc and Chen, Chen, PhD and Purfürst, Bettina, PhD and Spallek, Bastian, DVM and Koopmann, Tamara T., PhD and Baczko, Istvan, MD, PhD and dos Remedios, Cristobal G., PhD and George, Alfred L., MD and Bishopric, Nanette H., MD and Lodder, Elisabeth M., PhD and de Bakker, Jacques M.T., PhD and Fischer, Robert, MD and Coronel, Ruben, MD, PhD and Wilde, Arthur A.M., MD, PhD and Gotthardt, Michael, MD and Remme, Carol Ann, MD, PhD
Journal of the American College of Cardiology, ISSN 0735-1097, 2014, Volume 63, Issue 6, pp. 549 - 559
Objectives The aim of this study was to investigate the modulatory effect of the coxsackie and adenovirus receptor (CAR) on ventricular conduction and... 
Cardiovascular | Internal Medicine | ventricular fibrillation | single nucleotide polymorphism genetics | arrhythmia | ion channels | ischemia | ANKYRIN-G | CARDIAC & CARDIOVASCULAR SYSTEMS | VENTRICULAR-FIBRILLATION | DEATH | INTERCALATED DISC | TIGHT JUNCTION | HEART | INFARCTION | CAR | JUNCTION PROTEIN | EXPRESSION | Myocardial Ischemia - metabolism | Humans | Ventricular Function | Male | NAV1.5 Voltage-Gated Sodium Channel - metabolism | Arrhythmias, Cardiac - etiology | Carbenoxolone | Animals | Heart Conduction System - physiopathology | Myocardial Ischemia - complications | Myocardium - metabolism | HEK293 Cells | Myocardial Ischemia - physiopathology | Female | Mice | Coxsackie and Adenovirus Receptor-Like Membrane Protein - physiology | Sects | Medical colleges | Ischemia | Adenoviruses | Physiological aspects | Electron microscopy | Heart diseases | Cells | Cardiac arrhythmia | Heart attacks | Cardiomyopathy | Cardiovascular disease | Gene expression | Cell adhesion & migration | Studies | Proteins | Genotype & phenotype | Rodents | Cell cycle
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9. Full Text Patient Age, Sex, and Inflammatory Bowel Disease Phenotype Associate With Course of Primary Sclerosing Cholangitis
by Weismüller, Tobias J and Trivedi, Palak J and Bergquist, Annika and Imam, Mohamad and Lenzen, Henrike and Ponsioen, Cyriel Y and Holm, Kristian and Gotthardt, Daniel and Färkkilä, Martti A and Marschall, Hanns-Ulrich and Thorburn, Douglas and Weersma, Rinse K and Fevery, Johan and Mueller, Tobias and Chaouillères, Olivier and Schulze, Kornelius and Lazaridis, Konstantinos N and Almer, Sven and Pereira, Stephen P and Levy, Cynthia and Mason, Andrew and Naess, Sigrid and Bowlus, Christopher L and Floreani, Annarosa and Halilbasic, Emina and Yimam, Kidist K and Milkiewicz, Piotr and Beuers, Ulrich and Huynh, Dep K and Pares, Albert and Manser, Christine N and Dalekos, George N and Eksteen, Bertus and Invernizzi, Pietro and Berg, Christoph P and Kirchner, Gabi I and Sarrazin, Christoph and Zimmer, Vincent and Fabris, Luca and Braun, Felix and Marzioni, Marco and Juran, Brian D and Said, Karouk and Rupp, Christian and Jokelainen, Kalle and Benito de Valle, Maria and Saffioti, Francesca and Cheung, Angela and Trauner, Michael and Schramm, Christoph and Chapman, Roger W and Karlsen, Tom H and Schrumpf, Erik and Strassburg, Christian P and Manns, Michael P and Lindor, Keith D and Hirschfield, Gideon M and Hansen, Bettina E and Boberg, Kirsten M and Int PSC Study Grp and International PSC Study Group and Region Östergötland and Avdelningen för inflammationsmedicin and Linköpings universitet and Institutionen för klinisk och experimentell medicin and Magtarmmedicinska kliniken and Hjärt- och Medicincentrum and Hälsouniversitetet
Gastroenterology, ISSN 0016-5085, 2017, Volume 152, Issue 8, pp. 1975 - 1984.e8
Background & Aims Primary sclerosing cholangitis (PSC) is an orphan hepatobiliary disorder associated with inflammatory bowel disease (IBD). We aimed to... 
Gastroenterology and Hepatology | Risk Stratification | Immune-Mediated Liver Disease | Autoimmune Liver Disease | Cholestasis | DOSE URSODEOXYCHOLIC ACID | RISK-FACTORS | LIVER-TRANSPLANTATION | ALKALINE-PHOSPHATASE | ULCERATIVE-COLITIS | NATURAL-HISTORY | CLINICAL PRESENTATION | PRIMARY BILIARY-CIRRHOSIS | PROGNOSTIC VARIABLES | GASTROENTEROLOGY & HEPATOLOGY | GENOME-WIDE ASSOCIATION | Crohn Disease - epidemiology | Multivariate Analysis | Liver Transplantation | Age Distribution | Prognosis | Humans | Middle Aged | Crohn Disease - surgery | Crohn Disease - mortality | Male | Colitis, Ulcerative - epidemiology | Incidence | Young Adult | Time Factors | Crohn Disease - diagnosis | Adult | Colitis, Ulcerative - surgery | Female | Retrospective Studies | Cholangitis, Sclerosing - surgery | Risk Assessment | Risk Factors | Kaplan-Meier Estimate | Proportional Hazards Models | Europe - epidemiology | Chi-Square Distribution | Australia - epidemiology | Disease Progression | Phenotype | Cholangitis, Sclerosing - epidemiology | Colitis, Ulcerative - diagnosis | Colitis, Ulcerative - mortality | Sex Distribution | Cholangitis, Sclerosing - diagnosis | North America - epidemiology | Cholangitis, Sclerosing - mortality | Gastrointestinal diseases | Genetic aspects | Analysis | Colitis ulcerosa | Inflammation | Inflamació | Ulcerative colitis | Clinical Medicine | Medical and Health Sciences | Medicin och hälsovetenskap | Gastroenterologi | Risk Stratification; Immune-Mediated Liver Disease; Autoimmune Liver Disease; Cholestasis | Klinisk medicin
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10. Full Text Muscle atrophy in Titin M-line deficient mice
by Peng, J and Raddatz, K and Labeit, S and Granzier, H and Gotthardt, M
Journal of Muscle Research and Cell Motility, ISSN 0142-4319, 12/2005, Volume 26, Issue 6, pp. 381 - 388
We investigated the response to deletion of the titin M-line region in striated muscle, using a titin knockout model and a range of techniques that include... 
Life Sciences | Animal Anatomy / Morphology / Histology | Biomedicine general | Proteomics | Cell Biology | RAT SKELETAL-MUSCLE | LIGHT-CHAIN KINASE | EXPRESSION PATTERNS | SARCOMERIC M-BAND | PASSIVE STIFFNESS | MOLECULAR-STRUCTURE | FIBER-TYPE | MUSCULAR-DYSTROPHY | DILATED CARDIOMYOPATHY | ONLY PROTEIN FHL2 | CELL BIOLOGY | Protein Kinases - genetics | Connectin | Gene Expression - genetics | Muscle Fibers, Fast-Twitch - metabolism | Electrophoresis, Gel, Two-Dimensional | Muscle Proteins - deficiency | Muscle, Skeletal - metabolism | Muscle Fibers, Slow-Twitch - metabolism | Muscle Fibers, Skeletal - metabolism | Sarcomeres - pathology | In Situ Hybridization | Protein Isoforms - metabolism | Protein Kinases - deficiency | Muscular Atrophy - metabolism | Sarcomeres - metabolism | Heat-Shock Proteins - metabolism | Muscular Atrophy - pathology | Muscle, Skeletal - ultrastructure | Exons - genetics | Muscular Atrophy - genetics | Mice, Inbred Strains | Microscopy, Electron | Mice, Knockout | Muscle Proteins - genetics | Sarcomeres - ultrastructure | Animals | Muscle Fibers, Slow-Twitch - pathology | Muscle Fibers, Fast-Twitch - pathology | Muscle Fibers, Skeletal - pathology | Mice | Muscle, Skeletal - pathology | Proteasome Endopeptidase Complex - metabolism | Protein Isoforms - genetics | Proteins | Muscular system | Kinases | Binding sites
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