Your search keyword '"Antigens, CD/genetics"' showing total 25 results

1. Genotype-first approach to identify associations between CDH1 germline variants and cancer phenotypes: a multicentre study by the European Reference Network on Genetic Tumour Risk Syndromes

Author

José Garcia-Pelaez, Rita Barbosa-Matos, Silvana Lobo, Alexandre Dias, Luzia Garrido, Sérgio Castedo, Sónia Sousa, Hugo Pinheiro, Liliana Sousa, Rita Monteiro, Joaquin J Maqueda, Susana Fernandes, Fátima Carneiro, Nádia Pinto, Carolina Lemos, Carla Pinto, Manuel R Teixeira, Stefan Aretz, Svetlana Bajalica-Lagercrantz, Judith Balmaña, Ana Blatnik, Patrick R Benusiglio, Maud Blanluet, Vincent Bours, Hilde Brems, Joan Brunet, Daniele Calistri, Gabriel Capellá, Sergio Carrera, Chrystelle Colas, Karin Dahan, Robin de Putter, Camille Desseignés, Elena Domínguez-Garrido, Conceição Egas, D Gareth Evans, Damien Feret, Eleanor Fewings, Rebecca C Fitzgerald, Florence Coulet, María Garcia-Barcina, Maurizio Genuardi, Lisa Golmard, Karl Hackmann, Helen Hanson, Elke Holinski-Feder, Robert Hüneburg, Mateja Krajc, Kristina Lagerstedt-Robinson, Conxi Lázaro, Marjolijn J L Ligtenberg, Cristina Martínez-Bouzas, Sonia Merino, Geneviève Michils, Srdjan Novaković, Ana Patiño-García, Guglielmina Nadia Ranzani, Evelin Schröck, Inês Silva, Catarina Silveira, José L Soto, Isabel Spier, Verena Steinke-Lange, Gianluca Tedaldi, María-Isabel Tejada, Emma R Woodward, Marc Tischkowitz, Nicoline Hoogerbrugge, Carla Oliveira, Institut Català de la Salut, [Garcia-Pelaez J] Instituto de Investigação e Inovação em Saúde (i3S), University of Porto, Porto, Portugal. Faculty of Medicine, University of Porto, Porto, Portugal. Instituto de Patologia e Imunologia Molecular da Universidade do Porto, Porto, Portugal. Porto Comprehensive Cancer Center Raquel Seruca, Porto, Portugal. [Barbosa-Matos R, Lobo S] Instituto de Investigação e Inovação em Saúde (i3S), University of Porto, Porto, Portugal. Institute of Biomedical Sciences Abel Salazar, University of Porto, Porto, Portugal. Instituto de Patologia e Imunologia Molecular da Universidade do Porto, Porto, Portugal. Porto Comprehensive Cancer Center Raquel Seruca, Porto, Portugal. [Dias A] Instituto de Investigação e Inovação em Saúde (i3S), University of Porto, Porto, Portugal. Instituto de Patologia e Imunologia Molecular da Universidade do Porto, Porto, Portugal. Porto Comprehensive Cancer Center Raquel Seruca, Porto, Portugal. [Garrido L] Centro Hospitalar Universitário São João, Porto, Portugal. [Castedo S] Instituto de Investigação e Inovação em Saúde (i3S), University of Porto, Porto, Portugal. Faculty of Medicine, University of Porto, Porto, Portugal. Instituto de Patologia e Imunologia Molecular da Universidade do Porto, Porto, Portugal. Centro Hospitalar Universitário São João, Porto, Portugal. Porto Comprehensive Cancer Center Raquel Seruca, Porto, Portugal. European Reference Network on Genetic Tumour Risk Syndromes (ERN GENTURIS), Porto, Portugal. [Balmaña J] Vall d'Hebron Hospital Universitari, Barcelona, Spain. Universitat Autònoma de Barcelona, Bellaterra, Spain. ERN GENTURIS, Barcelona, Spain, and Vall d'Hebron Barcelona Hospital Campus

Subjects

neoplasias::neoplasias por localización::neoplasias del sistema digestivo::neoplasias gastrointestinales::neoplasias gástricas [ENFERMEDADES], Genotype, Neoplasms::Neoplasms by Site::Breast Neoplasms [DISEASES], enfermedades de la piel y tejido conjuntivo::enfermedades de la piel::enfermedades de la mama [ENFERMEDADES], Genetic Phenomena::Genotype::Genetic Predisposition to Disease [PHENOMENA AND PROCESSES], Mutation, Missense, Breast Neoplasms, All institutes and research themes of the Radboud University Medical Center, Germ Cells/pathology, Antigens, CD, Stomach Neoplasms, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Humans, Genetic Predisposition to Disease, Genotip, Càncer, Germ-Line Mutation, fenómenos genéticos::genotipo::predisposición genética a la enfermedad [FENÓMENOS Y PROCESOS], Cancer, Retrospective Studies, Breast Neoplasms/epidemiology, Cadherins/genetics, Antigens, CD/genetics, Stomach Neoplasms/epidemiology, Cadherins, Pedigree, Fenotip, Carcinoma, Lobular, Germ Cells, Phenotype, Oncology, Aparell digestiu - Càncer - Aspectes genètics, Mama - Càncer - Aspectes genètics, Neoplasms::Neoplasms by Site::Digestive System Neoplasms::Gastrointestinal Neoplasms::Stomach Neoplasms [DISEASES], Female

Abstract

Genotype; Cancer phenotypes; Genetic tumour Genotip; Fenotips del càncer; Tumor genètic Genotipo; Fenotipos del cáncer; Tumor genético Background Truncating pathogenic or likely pathogenic variants of CDH1 cause hereditary diffuse gastric cancer (HDGC), a tumour risk syndrome that predisposes carrier individuals to diffuse gastric and lobular breast cancer. Rare CDH1 missense variants are often classified as variants of unknown significance. We conducted a genotype–phenotype analysis in families carrying rare CDH1 variants, comparing cancer spectrum in carriers of pathogenic or likely pathogenic variants (PV/LPV; analysed jointly) or missense variants of unknown significance, assessing the frequency of families with lobular breast cancer among PV/LPV carrier families, and testing the performance of lobular breast cancer-expanded criteria for CDH1 testing. Methods This genotype-first study used retrospective diagnostic and clinical data from 854 carriers of 398 rare CDH1 variants and 1021 relatives, irrespective of HDGC clinical criteria, from 29 institutions in ten member-countries of the European Reference Network on Tumour Risk Syndromes (ERN GENTURIS). Data were collected from Oct 1, 2018, to Sept 20, 2022. Variants were classified by molecular type and clinical actionability with the American College of Medical Genetics and Association for Molecular Pathology CDH1 guidelines (version 2). Families were categorised by whether they fulfilled the 2015 and 2020 HDGC clinical criteria. Genotype–phenotype associations were analysed by Student's t test, Kruskal-Wallis, χ2, and multivariable logistic regression models. Performance of HDGC clinical criteria sets were assessed with an equivalence test and Youden index, and the areas under the receiver operating characteristic curves were compared by Z test. Findings From 1971 phenotypes (contributed by 854 probands and 1021 relatives aged 1–93 years), 460 had gastric and breast cancer histology available. CDH1 truncating PV/LPVs occurred in 176 (21%) of 854 families and missense variants of unknown significance in 169 (20%) families. Multivariable logistic regression comparing phenotypes occurring in families carrying PV/LPVs or missense variants of unknown significance showed that lobular breast cancer had the greatest positive association with the presence of PV/LPVs (odds ratio 12·39 [95% CI 2·66–57·74], p=0·0014), followed by diffuse gastric cancer (8·00 [2·18–29·39], p=0·0017) and gastric cancer (7·81 [2·03–29·96], p=0·0027). 136 (77%) of 176 families carrying PV/LPVs fulfilled the 2015 HDGC criteria. Of the remaining 40 (23%) families, who did not fulfil the 2015 criteria, 11 fulfilled the 2020 HDGC criteria, and 18 had lobular breast cancer only or lobular breast cancer and gastric cancer, but did not meet the 2020 criteria. No specific CDH1 variant was found to predispose individuals specifically to lobular breast cancer, although 12 (7%) of 176 PV/LPV carrier families had lobular breast cancer only. Addition of three new lobular breast cancer-centred criteria improved testing sensitivity while retaining high specificity. The probability of finding CDH1 PV/LPVs in patients fulfilling the lobular breast cancer-expanded criteria, compared with the 2020 criteria, increased significantly (AUC 0·92 vs 0·88; Z score 3·54; p=0·0004). Interpretation CDH1 PV/LPVs were positively associated with HDGC-related phenotypes (lobular breast cancer, diffuse gastric cancer, and gastric cancer), and no evidence for a positive association with these phenotypes was found for CDH1 missense variants of unknown significance. CDH1 PV/LPVs occurred often in families with lobular breast cancer who did not fulfil the 2020 HDGC criteria, supporting the expansion of lobular breast cancer-centred criteria. Funding European Reference Network on Genetic Tumour Risk Syndromes, European Regional Development Fund, Fundação para a Ciência e a Tecnologia (Portugal), Cancer Research UK, and European Union's Horizon 2020 research and innovation programme. European Reference Network on Genetic Tumour Risk Syndromes, European Regional Development Fund, Fundação para a Ciência e a Tecnologia (Portugal), Cancer Research UK, and European Union's Horizon 2020 research and innovation programme.

Published

2023

2. The Orphan Immune Receptor LILRB3 Modulates Fc Receptor-Mediated Functions of Neutrophils

Author

Zhao, Yuxi, van Woudenbergh, Esther, Zhu, Jing, Heck, Albert J R, van Kessel, Kok P M, de Haas, Carla J C, Aerts, Piet C, van Strijp, Jos A G, McCarthy, Alex J, Zhao, Yuxi, van Woudenbergh, Esther, Zhu, Jing, Heck, Albert J R, van Kessel, Kok P M, de Haas, Carla J C, Aerts, Piet C, van Strijp, Jos A G, and McCarthy, Alex J

Abstract

Neutrophils are critical to the generation of effective immune responses and for killing invading microbes. Paired immune receptors provide important mechanisms to modulate neutrophil activation thresholds and effector functions. Expression of the leukocyte Ig-like receptor (LILR)A6 (ILT8/CD85b) and LILRB3 (ILT5/CD85a) paired-receptor system on human neutrophils has remained unclear because of the lack of specific molecular tools. Additionally, there is little known of their possible functions in neutrophil biology. The objective of this study was to characterize expression of LILRA6/LILRB3 receptors during human neutrophil differentiation and activation, and to assess their roles in modulating Fc receptor-mediated effector functions. LILRB3, but not LILRA6, was detected in human neutrophil lysates following immunoprecipitation by mass spectrometry. We demonstrate high LILRB3 expression on the surface of resting neutrophils and release from the surface following neutrophil activation. Surface expression was recapitulated in a human PLB-985 cell model of neutrophil-like differentiation. Continuous ligation of LILRB3 inhibited key IgA-mediated effector functions, including production of reactive oxygen species, phagocytic uptake, and microbial killing. This suggests that LILRB3 provides an important checkpoint to control human neutrophil activation and their antimicrobial effector functions during resting and early-activation stages of the neutrophil life cycle.

Published

2020

3. The absence of the CD163 receptor has distinct temporal influences on intracerebral hemorrhage outcomes

Author

Jenna L Leclerc, Andrew S Lampert, Søren K. Moestrup, Terrie Vasilopoulos, Pia Svendsen, Claudia Loyola Amador, Brandon Schlakman, and Sylvain Doré

Subjects

Male, Receptors, Cell Surface/genetics, 0301 basic medicine, Pathology, Hematoma/genetics, Hemoglobins, Mice, iron, 0302 clinical medicine, Neovascularization, Pathologic/genetics, oxidative stress, Gliosis, Receptor, Mice, Knockout, Hematoma, Neovascularization, Pathologic, Microglia, Brain, Antigens, CD/genetics, heme oxygenase, stroke, medicine.anatomical_structure, Neurology, Cerebral Hemorrhage/genetics, Blood-Brain Barrier, medicine.symptom, Cardiology and Cardiovascular Medicine, Gliosis/etiology, medicine.medical_specialty, Iron, Antigens, Differentiation, Myelomonocytic, Receptors, Cell Surface, Brain damage, Blood–brain barrier, 03 medical and health sciences, Antigens, CD, medicine, Animals, Brain/pathology, Scavenger receptor, Cerebral Hemorrhage, Intracerebral hemorrhage, business.industry, Hemoglobins/metabolism, Antigens, Differentiation, Myelomonocytic/genetics, Recovery of Function, medicine.disease, Mice, Inbred C57BL, 030104 developmental biology, Neurology (clinical), business, Iron/metabolism, CD163, Neuroscience, Psychomotor Performance, 030217 neurology & neurosurgery

Abstract

Hemoglobin (Hb) toxicity precipitates secondary brain damage following intracerebral hemorrhage (ICH). CD163 is an anti-inflammatory Hb scavenger receptor and CD163-positive macrophages/microglia locally accumulate post-bleed, yet no studies have investigated the role of CD163 after ICH. ICH was induced in wildtype and CD163−/− mice and various anatomical and functional outcomes were assessed. At 3 d, CD163−/− mice have 43.4 ± 5.0% (p = 0.0002) and 34.8 ± 3.4% (p = 0.0003) less hematoma volume and tissue injury, respectively. Whereas, at 10 d, CD163−/− mice have 49.2 ± 15.0% larger lesions (p = 0.0385). An inflection point was identified, where CD163−/− mice perform better on neurobehavioral testing and have less mortality before 4 d, but increased mortality and worse function after 4 d (p = 0.0389). At 3 d, CD163−/− mice have less Hb, iron, and blood–brain barrier dysfunction, increased astrogliosis and neovascularization, and no change in heme oxygenase 1 (HO1) expression. At 10 d, CD163−/− mice have increased iron and VEGF immunoreactivity, but no significant change in HO1 or astrogliosis. These novel findings reveal that CD163 deficiency has distinct temporal influences following ICH, with early beneficial properties but delayed injurious effects. While it is unclear why CD163 deficiency is initially beneficial, the late injurious effects are consistent with the key anti-inflammatory role of CD163 in the recovery phase of tissue damage.

Published

2017

4. Dysregulation of macrophage development and phenotype in diabetic human macrophages can be rescued by Hoxa3 protein transduction

Author

Kimberly A. Mace, Edward A. McKenzie, Andrew J.M. Boulton, Tanja Torbica, Frank L. Bowling, Hadeel Al Sadoun, and Salma Alrdahe

Subjects

Male, Cellular differentiation, Up-Regulation/drug effects, Pathology and Laboratory Medicine, Biochemistry, Monocytes, Endocrinology, 0302 clinical medicine, Tumor Necrosis Factors/analysis, Animal Cells, Immune Response, Cells, Cultured, Innate Immune System, Antigens, CD/genetics, Up-Regulation, 3. Good health, RUNX1, Cytokines, Medicine, Tumor necrosis factor alpha, Cellular Types, Endocrine Disorders, Immune Cells, Science, Immunology, 03 medical and health sciences, Signs and Symptoms, Antigens, CD, Manchester Institute of Biotechnology, DNA-binding proteins, Diabetes Mellitus, Genetics, Humans, Blood Cells, Macrophages, Core Binding Factor Alpha 2 Subunit/genetics, Antigens, Differentiation, Myelomonocytic/genetics, Biology and Life Sciences, Proteins, Molecular Development, Regulatory Proteins, 030104 developmental biology, Diabetes Mellitus, Type 2, chemistry, Culture Media, Conditioned, Case-Control Studies, Leukocytes, Mononuclear, Transcription Factors, Developmental Biology, 0301 basic medicine, Myeloid, Physiology, Gene Expression, Cell Maturation, White Blood Cells, chemistry.chemical_compound, Immune Physiology, Medicine and Health Sciences, Leukocytes, Mononuclear/cytology, Multidisciplinary, Cell Differentiation, Middle Aged, Recombinant Proteins, Interleukin-6/analysis, medicine.anatomical_structure, Phenotype, Core Binding Factor Alpha 2 Subunit, Tumor Necrosis Factors, Female, medicine.symptom, Research Article, Cell Survival/drug effects, Adult, Culture Media, Conditioned/chemistry, Cell Survival, Antigens, Differentiation, Myelomonocytic, Bone Marrow Cells, Inflammation, Biology, Downregulation and upregulation, Diagnostic Medicine, medicine, Gene Regulation, Recombinant Proteins/biosynthesis, Homeodomain Proteins, Interleukin-6, Macrophages/cytology, Cell Biology, ResearchInstitutes_Networks_Beacons/manchester_institute_of_biotechnology, Diabetes Mellitus, Type 2/metabolism, Metabolic Disorders, Immune System, Cancer research, Bone marrow, Homeodomain Proteins/genetics, 030215 immunology

Abstract

Controlled inflammatory responses of myeloid cells recruited to wounds are essential for effective repair. In diabetes, the inflammatory response is prolonged and augmented over time, with increased myeloid cells present in the wound that fail to switch from a pro-inflammatory phenotype to a pro-healing phenotype. These defects lead to delayed angiogenesis and tissue repair and regeneration, and contribute to chronic wound formation. In mouse models of diabetes, this aberrant phenotype is partially mediated by stable intrinsic changes to the developing myeloid cells in the bone marrow, affecting their maturation and polarization potential. Previous studies have shown that freshly isolated peripheral blood mononuclear cells from diabetic patients are more inflammatory than non-diabetic counterparts. However, the phenotype of macrophages from human diabetic patients has not been well characterized. Here we show that diabetic-derived human macrophages cultured for 6 days in vitro maintain a pro-inflammatory priming and hyperpolarize to a pro-inflammatory phenotype when stimulated with LPS and INF-ɣ or TNF. In addition, diabetic-derived macrophages show maturation defects associated with reduced expression of the RUNX1 transcription factor that promotes myeloid cell development. Targeting intrinsic defects in myeloid cells by protein transduction of the Hoxa3 transcription factor can rescue some inflammation and maturation defects in human macrophages from diabetic patients via upregulation of Runx1. In addition, Hoxa3 can modulate the levels of p65/NF-κB and histone acetyltransferase and deacetylase activity, as well as inhibit acetylation of the TNF promoter. Altogether, these results show a link between myeloid cell maturation and inflammatory responses, and that diabetes induces intrinsic changes to human myeloid cells that are maintained over time, as well as potentially therapeutic Hoxa3-mediated mechanisms of controlling the inflammatory response in diabetes.

Published

2019

5. Oncofoetal insulin receptor isoform A marks the tumour endothelium; an underestimated pathway during tumour angiogenesis and angiostatic treatment

Author

Laurie A. Mans, Elisabeth J. M. Huijbers, Judy R. van Beijnum, Paula C Gasull, Arjan W. Griffioen, Patrycja Nowak-Sliwinska, Axel Bex, Medical oncology laboratory, and CCA - Cancer biology and immunology

Subjects

Male, Cancer Research, Angiogenesis, medicine.medical_treatment, Chick Embryo, Neovascularization, Pathologic/genetics/pathology, Chorioallantoic Membrane, Chorioallantoic Membrane/metabolism/pathology, Neovascularization, Mice, 0302 clinical medicine, Tumor Cells, Cultured, Medicine, Insulin, Protein Isoforms, RNA, Small Interfering, Receptor, RNA, Small Interfering/genetics, ddc:615, biology, Neovascularization, Pathologic, Antigens, CD/genetics, Kidney Neoplasms, 3. Good health, Chorioallantoic membrane, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Gene Knockdown Techniques, Female, medicine.symptom, hormones, hormone substitutes, and hormone antagonists, endocrine system, Endothelium, Article, 03 medical and health sciences, Cell Proliferation/genetics, Targeted therapies, In vivo, Antigens, CD, Protein Isoforms/genetics, Human Umbilical Vein Endothelial Cells, Receptor, Insulin/genetics, Animals, Humans, Cell Proliferation, Insulin/genetics/metabolism, business.industry, Genome, Human, Endothelium/metabolism/pathology, nutritional and metabolic diseases, Receptor, Insulin, Insulin receptor, Disease Models, Animal, biology.protein, Cancer research, Genome, Human/genetics, business, Kidney Neoplasms/genetics/pathology, Tumour angiogenesis

Abstract

BACKGROUND: In a genomic screen for determinants of the tumour vasculature, we identified insulin receptor (INSR) to mark the tumour endothelium. As a functional role for insulin/INSR in cancer has been suggested and markers of the tumour endothelium may be attractive therapeutic targets, we investigated the role of INSR in angiogenesis.METHODS: In a genomic screen for determinants of the tumour vasculature we identified insulin receptor to mark the tumour endothelium.RESULTS: The current report demonstrates the following: (i) the heavy overexpression of INSR on angiogenic vasculature in human tumours and the correlation to short survival, (ii) that INSR expression in the tumour vasculature is mainly representing the short oncofoetal and non-metabolic isoform INSR-A, (iii) the angiogenic activity of insulin on endothelial cells (EC) in vitro and in vivo, (iv) suppression of proliferation and sprouting of EC in vitro after antibody targeting or siRNA knockdown, and (v) inhibition of in vivo angiogenesis in the chicken chorioallantoic membrane (CAM) by anti-INSR antibodies. We additionally show, using preclinical mouse as well as patient data, that treatment with the inhibitor sunitinib significantly reduces the expression of INSR-A.CONCLUSIONS: The current study underscores the oncogenic impact of INSR and suggests that targeting the INSR-A isoform should be considered in therapeutic settings.

Published

2019

6. Variants in members of the cadherin-catenin complex, CDH1 and CTNND1, cause blepharocheilodontic syndrome

Author

Kievit, Anneke, Tessadori, Federico, Douben, Hannie, Jordens, Ingrid, Maurice, Madelon, Hoogeboom, Jeannette, Hennekam, Raoul, Nampoothiri, Sheela, Kayserili, Hülya, Castori, Marco, Whiteford, Margo, Motter, Connie, Melver, Catherine, Cunningham, Michael, Hing, Anne, Kokitsu-Nakata, Nancy M, Vendramini-Pittoli, Siulan, Richieri-Costa, Antonio, Baas, Annette F, Breugem, Corstiaan C, Duran, Karen, Massink, Maarten, Derksen, Patrick W B, van IJcken, Wilfred F J, van Unen, Leontine, Santos-Simarro, Fernando, Lapunzina, Pablo, Gil-da Silva Lopes, Vera L, Lustosa-Mendes, Elaine, Krall, Max, Slavotinek, Anne, Martinez-Glez, Victor, Bakkers, Jeroen, van Gassen, Koen L I, de Klein, Annelies, van den Boogaard, Marie-José H, van Haaften, Gijs, Kievit, Anneke, Tessadori, Federico, Douben, Hannie, Jordens, Ingrid, Maurice, Madelon, Hoogeboom, Jeannette, Hennekam, Raoul, Nampoothiri, Sheela, Kayserili, Hülya, Castori, Marco, Whiteford, Margo, Motter, Connie, Melver, Catherine, Cunningham, Michael, Hing, Anne, Kokitsu-Nakata, Nancy M, Vendramini-Pittoli, Siulan, Richieri-Costa, Antonio, Baas, Annette F, Breugem, Corstiaan C, Duran, Karen, Massink, Maarten, Derksen, Patrick W B, van IJcken, Wilfred F J, van Unen, Leontine, Santos-Simarro, Fernando, Lapunzina, Pablo, Gil-da Silva Lopes, Vera L, Lustosa-Mendes, Elaine, Krall, Max, Slavotinek, Anne, Martinez-Glez, Victor, Bakkers, Jeroen, van Gassen, Koen L I, de Klein, Annelies, van den Boogaard, Marie-José H, and van Haaften, Gijs

Abstract

Blepharocheilodontic syndrome (BCDS) consists of lagophthalmia, ectropion of the lower eyelids, distichiasis, euryblepharon, cleft lip/palate and dental anomalies and has autosomal dominant inheritance with variable expression. We identified heterozygous variants in two genes of the cadherin-catenin complex, CDH1, encoding E-cadherin, and CTNND1, encoding p120 catenin delta1 in 15 of 17 BCDS index patients, as was recently described in a different publication. CDH1 plays an essential role in epithelial cell adherence; CTNND1 binds to CDH1 and controls the stability of the complex. Functional experiments in zebrafish and human cells showed that the CDH1 variants impair the cell adhesion function of the cadherin-catenin complex in a dominant-negative manner. Variants in CDH1 have been linked to familial hereditary diffuse gastric cancer and invasive lobular breast cancer; however, no cases of gastric or breast cancer have been reported in our BCDS cases. Functional experiments reported here indicated the BCDS variants comprise a distinct class of CDH1 variants. Altogether, we identified the genetic cause of BCDS enabling DNA diagnostics and counseling, in addition we describe a novel class of dominant negative CDH1 variants.

Published

2018

7. Variants in members of the cadherin–catenin complex, CDH1 and CTNND1, cause blepharocheilodontic syndrome

Author

Victor Martinez-Glez, Vera Lúcia Gil da Silva Lopes, Federico Tessadori, Sheela Nampoothiri, Connie S. Motter, Marie-José H. van den Boogaard, Patrick W. B. Derksen, Catherine Ward Melver, Madelon M. Maurice, Corstiaan C. Breugem, Hülya Kayserili, Max Krall, Leontine van Unen, Fernando Santos-Simarro, Annelies de Klein, Jeroen Bakkers, Pablo Lapunzina, Elaine Lustosa-Mendes, Anneke Kievit, Margo L. Whiteford, Anne Slavotinek, Hannie Douben, Michael L. Cunningham, Nancy Mizue Kokitsu-Nakata, Wilfred F. J. van IJcken, Koen L.I. van Gassen, Gijs van Haaften, Anne V. Hing, Annette F. Baas, Antonio Richieri-Costa, Maarten P.G. Massink, Raoul C.M. Hennekam, Karen Duran, Siulan Vendramini-Pittoli, Jeannette Hoogeboom, Marco Castori, Ingrid Jordens, Clinical Genetics, APH - Quality of Care, Paediatric Genetics, ARD - Amsterdam Reproduction and Development, and Hubrecht Institute for Developmental Biology and Stem Cell Research

Subjects

0301 basic medicine, Male, Delta Catenin, Ectropion, 030105 genetics & heredity, medicine.disease_cause, CDH1, Ectropion/genetics, Child, Genetics (clinical), Zebrafish, Mutation, CTNND1, Cleft Lip/genetics, Antigens, CD/genetics, Catenins, Cadherins, Cleft Palate, CD/genetics, Child, Preschool, MCF-7 Cells, Female, Catenin complex, Hereditary diffuse gastric cancer, Protein Binding, Adult, ANORMALIDADES CRANIOFACIAIS, Adolescent, Cleft Lip, Catenins/genetics, Biology, Article, 03 medical and health sciences, Antigens, CD, Cleft Palate/genetics, Tooth Abnormalities/genetics, Genetics, medicine, Cell Adhesion, Animals, Humans, Antigens, Preschool, Gene, Cadherin, Tooth Abnormalities, Cadherins/genetics, medicine.disease, Blepharocheilodontic syndrome, 030104 developmental biology, Cancer research, biology.protein

Abstract

Blepharocheilodontic syndrome (BCDS) consists of lagophthalmia, ectropion of the lower eyelids, distichiasis, euryblepharon, cleft lip/palate and dental anomalies and has autosomal dominant inheritance with variable expression. We identified heterozygous variants in two genes of the cadherin-catenin complex, CDH1, encoding E-cadherin, and CTNND1, encoding p120 catenin delta1 in 15 of 17 BCDS index patients, as was recently described in a different publication. CDH1 plays an essential role in epithelial cell adherence; CTNND1 binds to CDH1 and controls the stability of the complex. Functional experiments in zebrafish and human cells showed that the CDH1 variants impair the cell adhesion function of the cadherin-catenin complex in a dominant-negative manner. Variants in CDH1 have been linked to familial hereditary diffuse gastric cancer and invasive lobular breast cancer; however, no cases of gastric or breast cancer have been reported in our BCDS cases. Functional experiments reported here indicated the BCDS variants comprise a distinct class of CDH1 variants. Altogether, we identified the genetic cause of BCDS enabling DNA diagnostics and counseling, in addition we describe a novel class of dominant negative CDH1 variants.

Published

2018

8. Interaction of CDCP1 with HER2 Enhances HER2-Driven Tumorigenesis and Promotes Trastuzumab Resistance in Breast Cancer

Author

Manuela Sarti, Andrea Alimonti, Ilaria Guccini, Andrea Rinaldi, Erica Montani, Carlo V. Catapano, Ramón García-Escudero, Filippo Montemurro, Tiziano Bernasocchi, Sandra Pinton, Francesco Bertoni, and Abdullah Alajati

Subjects

Genetics and Molecular Biology (all), Carcinogenesis, Receptor, ErbB-2, Drug Resistance, medicine.disease_cause, Biochemistry, Animals, Antigens, CD, Antineoplastic Agents, Breast Neoplasms, Cell Adhesion Molecules, Female, Humans, MCF-7 Cells, Mice, Neoplasm Proteins, Protein Binding, Trastuzumab, src-Family Kinases, Drug Resistance, Neoplasm, Biochemistry, Genetics and Molecular Biology (all), ErbB-2, 0302 clinical medicine, Neoplasm, skin and connective tissue diseases, lcsh:QH301-705.5, 0303 health sciences, Antigens, CD/genetics, Antigens, CD/metabolism, Antineoplastic Agents/pharmacology, Breast Neoplasms/genetics, Breast Neoplasms/metabolism, Carcinogenesis/genetics, Carcinogenesis/metabolism, Cell Adhesion Molecules/genetics, Cell Adhesion Molecules/metabolism, Neoplasm Proteins/genetics, Neoplasm Proteins/metabolism, Receptor, ErbB-2/genetics, Receptor, ErbB-2/metabolism, Trastuzumab/pharmacology, src-Family Kinases/metabolism, Cell migration, CD, 3. Good health, 030220 oncology & carcinogenesis, CDCP1, Tyrosine kinase, Receptor, Proto-oncogene tyrosine-protein kinase Src, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Breast cancer, Antigens, Neoplasm, medicine, Antigens, neoplasms, 030304 developmental biology, business.industry, medicine.disease, Biomarker, lcsh:Biology (General), Immunology, Cancer research, business

Abstract

SummaryUnderstanding the molecular pathways that contribute to the aggressive behavior of HER2-positive breast cancers may aid in the development of novel therapeutic interventions. Here, we show that CDCP1 and HER2 are frequently co-overexpressed in metastatic breast tumors and associated with poor patient prognosis. HER2 and CDCP1 co-overexpression leads to increased transformation ability, cell migration, and tumor formation in vivo, and enhanced HER2 activation and downstream signaling in different breast cancer cell lines. Mechanistically, we demonstrate that CDCP1 binds to HER2 through its intracellular domain, thereby increasing HER2 interaction with the non-receptor tyrosine kinase c-SRC (SRC), leading to trastuzumab resistance. Taken together, our findings establish that CDCP1 is a modulator of HER2 signaling and a biomarker for the stratification of breast cancer patients with poor prognosis. Our results also provide a rationale for therapeutic targeting of CDCP1 in HER2-positive breast cancer patients.

Published

2015

9. Immune cell and transcriptomic analysis of the human decidua in term and preterm parturition

Author

Rinaldi, S F, Makieva, S, Saunders, P T, Rossi, A G, and Norman, J E

Subjects

Cytokines/genetics, Gene Expression Profiling, Infant, Newborn, Antigens, CD/genetics, Transcriptome/immunology, Decidua/cytology, Flow Cytometry, Microarray Analysis, Obstetric Labor, Premature/genetics, Labor, Obstetric/genetics, Term Birth/immunology, Cell Lineage/genetics, Pregnancy, Humans, Female, Lymphocyte Count, Lymphocytes/classification

Abstract

STUDY QUESTION: Is labour, both at term and preterm, associated with alterations in decidual lymphocyte densities and widespread changes to the decidual transcriptome?SUMMARY ANSWER: The onset of parturition, both at term and preterm, is associated with widespread gene expression changes in the decidua, many of which are related to inflammatory signalling, but is not associated with changes in the number of any of the decidual lymphocyte populations examined.WHAT IS KNOWN ALREADY: Given its location, directly at the maternal-foetal interface, the decidua is likely to play a pivotal role in the onset of parturition, however, the molecular events occurring in the decidua in association with the onset of labour, both at term and preterm, remain relatively poorly defined. Using flow cytometry and microarray analysis, the present study aimed to investigate changes to the immune cell milieu of the decidua in association with the onset of parturition and define the decidual gene signature associated with term and preterm labour (PTL).STUDY DESIGN, SIZE, DURATION: This study used decidual samples collected from 36 women across four clinical groups: term (38-42 weeks of gestation) not in labour, TNL; term in labour, TL; preterm (PARTICIPANTS/MATERIALS, SETTING, METHODS: Decidual lymphocytes were isolated from fresh decidual tissue collected from women in each of our four patient groups and stained with a panel of antibodies (CD45, CD3, CD19, CD56, CD4, CD8 and TCRVα24-Jα18) to investigate lymphocyte populations present in the decidua (TNL, n = 8; TL, n = 7; PTNL, n = 5; PTL, n = 5). RNA was extracted from decidual tissue and subjected to Illumina HT-12v4.0 BeadChip expression microarrays (TNL, n = 11; TL, n = 8; PTNL, n = 7; PTL, n = 10). Quantitative real-time PCR (qRT-PCR) was used to validate the microarray results.MAIN RESULTS AND THE ROLE OF CHANCE: The relative proportions of decidual lymphocytes (T cells, NK cells, B cells and invariant natural killer (iNKT) cells) were unaffected by either gestation or labour status. However, we found elevated expression of the non-classical MHC-protein, CD1D, in PTL decidua samples (P < 0.05), suggesting the potential for increased activation of decidual invariant NKT (iNKT) cells in PTL. Both term and PTL were associated with widespread gene expression changes, particularly related to inflammatory signalling. Up-regulation of candidate genes in TL (IL-6, PTGS2, ATF3, IER3 and TNFAIP3) and PTL (CXCL8, MARCO, LILRA3 and PLAU) were confirmed by qRT-PCR analysis.LARGE SCALE DATA: Microarray data are available at www.ebi.ac.uk/arrayexpress under accession number E-MTAB-5353.LIMITATIONS REASONS FOR CAUTION: Whilst no changes in lymphocyte number were observed across our patient samples, we did not investigate the activation state of any of the immune cell sub-populations examined, therefore, it is possible that the function of these cells may be altered in association with labour onset. Additionally, the results of our transcriptomic analyses are descriptive and at this stage, we cannot prove direct causal link with the up-regulation of any of the genes examined and the onset of either term or PTL.WIDER IMPLICATIONS OF THE FINDINGS: Our findings demonstrate that the onset of parturition is associated with widespread changes to the decidual transcriptome, and there are distinct gene expression changes associated with term and PTL. We confirmed that an inflammatory signature is present within the decidua, and we also report the up-regulation of several genes involved in regulating the inflammatory response. The identification of genes involved in regulating the inflammatory response may provide novel molecular targets for the development of new, more effective therapies for the prevention of preterm birth (PTB). Such targets are urgently required.STUDY FUNDING AND COMPETING INTEREST(S): This work was supported by Medical Research Council (grant number MR/L002657/1) and Tommy's, the baby charity. Jane Norman has had research grants from the charity Tommy's and from the National Institute for Health Research on PTB during the lifetime of this project. Jane Norman also sits on a data monitoring committee for GSK for a study on PTB prevention and her institution receives financial recompense for this. The other authors do not have any conflicts of interest to declare.

Published

2017

10. Tumor cells in multiple myeloma patients inhibit myeloma-reactive T cells through carcinoembryonic antigen-related cell adhesion molecule-6

Author

Christina Pfirschke, Tobias Meißner, Brigitte Gueckel, Simone Jünger, Philipp Beckhove, Kai Neben, Mathias Witzens-Harig, Hartmut Goldschmidt, Bernard Klein, Bettina Brackertz, Helga Bernhard, Thierry Rème, Ludmila Umansky, Dirk Hose, Anja Seckinger, Anthony D. Ho, Michael Hundemer, Heinke Conrad, Nisit Khandelwal, Jean-François Rossi, Hematology, and Basic (bio-) Medical Sciences

Subjects

Cytotoxicity, Immunologic, medicine.drug_class, T cell, Plasma Cells, Immunology, GPI-Linked Proteins/genetics, CD8-Positive T-Lymphocytes, GPI-Linked Proteins, CD8-Positive T-Lymphocytes/immunology, Monoclonal antibody, Biochemistry, Interleukin 21, Multiple Myeloma/immunology, Antigen, Antigens, CD, hemic and lymphatic diseases, Tumor Cells, Cultured, medicine, Humans, Cytotoxic T cell, MCF-7 cells, RNA, Small Interfering, Antigen-presenting cell, Multiple myeloma, RNA, Small Interfering/genetics, Signal Transduction/immunology, Chemistry, Antigens, CD/genetics, U937 Cells, Cell Biology, Hematology, T-Lymphocytes, Cytotoxic/immunology, medicine.disease, Coculture Techniques, medicine.anatomical_structure, Plasma Cells/immunology, Cytotoxicity, Immunologic/genetics, oncology, Immunotherapy/methods, Cancer research, Interleukin 12, Immunotherapy, Multiple Myeloma, Cell Adhesion Molecules/genetics, Cell Adhesion Molecules, Signal Transduction, T-Lymphocytes, Cytotoxic

Abstract

Although functionally competent cytotoxic, T cells are frequently observed in malignant diseases, they possess little ability to react against tumor cells. This phenomenon is particularly apparent in multiple myeloma. We here demonstrate that cytotoxic T cells reacted against myeloma antigens when presented by autologous dendritic cells, but not by myeloma cells. We further show by gene expression profiling and flow cytometry that, similar to many other malignant tumors, freshly isolated myeloma cells expressed several carcinoembryonic antigen-related cell adhesion molecules (CEACAMs) at varying proportions. Binding and crosslinking of CEACAM-6 by cytotoxic T cells inhibited their activation and resulted in T-cell unresponsiveness. Blocking of CEACAM-6 on the surface of myeloma cells by specific monoclonal antibodies or CEACAM-6 gene knock down by short interfering RNA restored T-cell reactivity against malignant plasma cells. These findings suggest that CEACAM-6 plays an important role in the regulation of CD8+ T-cell responses against multiple myeloma; therefore, therapeutic targeting of CEACAM-6 may be a promising strategy to improve myeloma immunotherapy.

Published

2013

11. Common Variants at Abca7, Ms4A6A/Ms4A4E, Epha1, Cd33 and Cd2Ap Are Associated with Alzheimer'S Disease

Author

Neill R. Graff-Radford, Caroline S. Widdowson, John Hardy, Simon Lovestone, Stefan Schreiber, Ana Frank-García, Amy Gerrish, Kevin Mayo, Alexandra Stretton, Michael John Owen, Minerva M. Carrasquillo, Seth Love, Jade Chapman, Vincent Chouraki, Monique M.B. Breteler, Francesco Panza, Emma R L C Vardy, Ronald C. Petersen, Harald Hampel, S. Nicolhaus, Lenore J. Launer, Michelle K. Lupton, Eckart Rüther, A. David Smith, David C. Rubinsztein, Rebecca Sims, Gill Livingston, Diana Zelenika, Simon Mead, Martin N. Rossor, Hilkka Soininen, Christine Van Broeckhoven, Kristel Sleegers, Thorlakur Jonsson, M. Arfan Ikram, Helen Beaumont, Michael Conlon O'Donovan, Federico Licastro, Sudha Seshadri, Alexander Richards, Nick C. Fox, Markus M. Nöthen, Claudine Berr, T. Feulner, Benedetta Nacmias, Carlos Cruchaga, Peter Passmore, Oscar L. Lopez, Julie Williams, Matthias Riemenschneider, Florence Pasquier, John Gallacher, Didier Hannequin, Sigrid Botne Sando, Jens Wiltfang, Charlene Thomas, Gabriele Siciliano, Maria Barcikowska, Mikko Hiltunen, Carol Brayne, Dobril Ivanov, Anita L. DeStefano, Bernadette McGuinness, Norman Klopp, Gordon K. Wilcock, Aoibhinn Lynch, Wolfgang Maier, Peter Holmans, H.-Erich Wichmann, Giorgio Annoni, Beatrice Arosio, Alison Goate, Sigurbjorn Bjornsson, Karl-Heinz Jöckel, Dan Rujescu, Hugh Gurling, Nigel M. Hooper, Clive Holmes, Andrew McQuillin, Patricia Friedrich, John Powell, Rhian Gwilliam, R. Heun, Jacques Epelbaum, Isabella Heuser, Magda Tsolaki, Dennis W. Dickson, Alberto Pilotto, Stephen Todd, Dominique Campion, Michael Krawczak, Jan O. Aasly, Olivier Hanon, Patrick G. Kehoe, Johannes Kornhuber, Marc Delepine, Peter Paul De Deyn, Britta Schürmann, Brian A. Lawlor, Christophe Tzourio, Richard Abraham, Petra Nowotny, Jean-François Dartigues, Heike Kölsch, Michelangelo Mancuso, Marian L. Hamshere, Zbigniew K. Wszolek, Paola Piccardi, Paolo Bosco, Jean-Charles Lambert, Denise Harold, Frank Jessen, Palmi V. Jonsson, Paola Bossù, Paul Hollingworth, Jon Snaedal, Michael Gill, Onofre Combarros, David M. A. Mann, John C. Morris, Annette L. Fitzpatrick, Christopher Shaw, Alexis Brice, Philippe Amouyel, Elio Scarpini, Lesley Jones, Sebastiaan Engelborghs, Daniela Galimberti, Vincenzo Solfrizzi, V. Shane Pankratz, John Collinge, María J. Bullido, Kristelle Brown, Nicholas Bass, Andrew B. Singleton, Jaspreet Singh Pahwa, Kari Stefansson, Lutz Frölich, Steven G. Younkin, Ignacio Mateo, Annick Alpérovitch, Benjamin Genier-Boley, Ina Giegling, Caterina Riehle, Kimberley Dowzell, Mark Lathrop, Hreinn Stefansson, Sandro Sorbi, Rita Guerreiro, Thomas W. Mühleisen, Karolien Bettens, Michael Hüll, Martin Dichgans, Petroula Proitsi, Panagiotis Deloukas, Valentina Moskvina, Cornelia M. van Duijn, Donald Warden, Victoria Alvarez, Eliecer Coto, Kevin Morgan, Susanne Moebus, Ammar Al-Chalabi, Elisa Porcellini, Stefan Wagenpfeil, Hendrik van den Bussche, John S. K. Kauwe, Stacy Steinberg, David Craig, Nicola Jones, Manuel Mayhaus, Davide Seripa, Neurology, NCA - Neurodegeneration, HOLLINGWORTH P, HAROLD D, SIMS R, GERRISH A, LAMBERT JC, CARRASQUILLO MM, ABRAHAM R, HAMSHERE ML, PAHWA JS, MOSKVINA V, DOWZELL K, JONES N, STRETTON A, THOMAS C, RICHARDS A, IVANOV D, WIDDOWSON C, CHAPMAN J, LOVESTONE S, POWELL J, PROITSI P, LUPTON MK, BRAYNE C, RUBINSZTEIN DC, GILL M, LAWLOR B, LYNCH A, BROWN KS, PASSMORE PA, CRAIG D, MCGUINNESS B, TODD S, HOLMES C, MANN D, SMITH AD, BEAUMONT H, WARDEN D, WILCOCK G, LOVE S, KEHOE PG, HOOPER NM, VARDY ER, HARDY J, MEAD S, FOX NC, ROSSOR M, COLLINGE J, MAIER W, JESSEN F, RÜTHER E, SCHÜRMANN B, HEUN R, KÖLSCH H, VAN DEN BUSSCHE H, HEUSER I, KORNHUBER J, WILTFANG J, DICHGANS M, FRÖLICH L, HAMPEL H, GALLACHER J, HÜLL M, RUJESCU D, GIEGLING I, GOATE AM, KAUWE JS, CRUCHAGA C, NOWOTNY P, MORRIS JC, MAYO K, SLEEGERS K, BETTENS K, ENGELBORGHS S, DE DEYN PP, VAN BROECKHOVEN C, LIVINGSTON G, BASS NJ, GURLING H, MCQUILLIN A, GWILLIAM R, DELOUKAS P, AL-CHALABI A, SHAW CE, TSOLAKI M, SINGLETON AB, GUERREIRO R, MÜHLEISEN TW, NÖTHEN MM, MOEBUS S, JÖCKEL KH, KLOPP N, WICHMANN HE, PANKRATZ VS, SANDO SB, AASLY JO, BARCIKOWSKA M, WSZOLEK ZK, DICKSON DW, GRAFF-RADFORD NR, PETERSEN RC, ALZHEIMER'S DISEASE NEUROIMAGING INITIATIVE, VAN DUIJN CM, BRETELER MM, IKRAM MA, DESTEFANO AL, FITZPATRICK AL, LOPEZ O, LAUNER LJ, SESHADRI S, CHARGE CONSORTIUM, BERR C, CAMPION D, EPELBAUM J, DARTIGUES JF, TZOURIO C, ALPÉROVITCH A, LATHROP M, EADI1 CONSORTIUM, FEULNER TM, FRIEDRICH P, RIEHLE C, KRAWCZAK M, SCHREIBER S, MAYHAUS M, NICOLHAUS S, WAGENPFEIL S, STEINBERG S, STEFANSSON H, STEFANSSON K, SNAEDAL J, BJÖRNSSON S, JONSSON PV, CHOURAKI V, GENIER-BOLEY B, HILTUNEN M, SOININEN H, COMBARROS O, ZELENIKA D, DELEPINE M, BULLIDO MJ, PASQUIER F, MATEO I, FRANK-GARCIA A, PORCELLINI E, HANON O, COTO E, ALVAREZ V, BOSCO P, SICILIANO G, MANCUSO M, PANZA F, SOLFRIZZI V, NACMIAS B, SORBI S, BOSSÙ P, PICCARDI P, AROSIO B, ANNONI G, SERIPA D, PILOTTO A, SCARPINI E, GALIMBERTI D, BRICE A, HANNEQUIN D, LICASTRO F, JONES L, HOLMANS PA, JONSSON T, RIEMENSCHNEIDER M, MORGAN K, YOUNKIN SG, OWEN MJ, O'DONOVAN M, AMOUYEL P, WILLIAMS J, Epidemiology, Radiology & Nuclear Medicine, Clinical sciences, Pathologic Biochemistry and Physiology, Hollingworth, P, Harold, D, Sims, R, Gerrish, A, Lambert, J, Carrasquillo, M, Abraham, R, Hamshere, M, Pahwa, J, Moskvina, V, Dowzell, K, Jones, N, Stretton, A, Thomas, C, Richards, A, Ivanov, D, Widdowson, C, Chapman, J, Lovestone, S, Powell, J, Proitsi, P, Lupton, M, Brayne, C, Rubinsztein, D, Gill, M, Lawlor, B, Lynch, A, Brown, K, Passmore, P, Craig, D, Mcguinness, B, Todd, S, Holmes, C, Mann, D, Smith, A, Beaumont, H, Warden, D, Wilcock, G, Love, S, Kehoe, P, Hooper, N, Vardy, E, Hardy, J, Mead, S, Fox, N, Rossor, M, Collinge, J, Maier, W, Jessen, F, Rüther, E, Schürmann, B, Heun, R, Kölsch, H, van den Bussche, H, Heuser, I, Kornhuber, J, Wiltfang, J, Dichgans, M, Frölich, L, Hampel, H, Gallacher, J, Hüll, M, Rujescu, D, Giegling, I, Goate, A, Kauwe, J, Cruchaga, C, Nowotny, P, Morris, J, Mayo, K, Sleegers, K, Bettens, K, Engelborghs, S, De Deyn, P, Van Broeckhoven, C, Livingston, G, Bass, N, Gurling, H, Mcquillin, A, Gwilliam, R, Deloukas, P, Al Chalabi, A, Shaw, C, Tsolaki, M, Singleton, A, Guerreiro, R, Mühleisen, T, Nöthen, M, Moebus, S, Jöckel, K, Klopp, N, Wichmann, H, Pankratz, V, Sando, S, Aasly, J, Barcikowska, M, Wszolek, Z, Dickson, D, Graff Radford, N, Petersen, R, van Duijn, C, Breteler, M, Ikram, M, Destefano, A, Fitzpatrick, A, Lopez, O, Launer, L, Seshadri, S, Berr, C, Campion, D, Epelbaum, J, Dartigues, J, Tzourio, C, Alpérovitch, A, Lathrop, M, Feulner, T, Friedrich, P, Riehle, C, Krawczak, M, Schreiber, S, Mayhaus, M, Nicolhaus, S, Wagenpfeil, S, Steinberg, S, Stefansson, H, Stefansson, K, Snædal, J, Björnsson, S, Jonsson, P, Chouraki, V, Genier Boley, B, Hiltunen, M, Soininen, H, Combarros, O, Zelenika, D, Delepine, M, Bullido, M, Pasquier, F, Mateo, I, Frank Garcia, A, Porcellini, E, Hanon, O, Coto, E, Alvarez, V, Bosco, P, Siciliano, G, Mancuso, M, Panza, F, Solfrizzi, V, Nacmias, B, Sorbi, S, Bossù, P, Piccardi, P, Arosio, B, Annoni, G, Seripa, D, Pilotto, A, Scarpini, E, Galimberti, D, Brice, A, Hannequin, D, Licastro, F, Jones, L, Holmans, P, Jonsson, T, Riemenschneider, M, Morgan, K, Younkin, S, Owen, M, O'Donovan, M, Amouyel, P, and Williams, J

Subjects

Male, ABCA7 protein, human, ATP-Binding Cassette Transporters/genetics, Sialic Acid Binding Ig-like Lectin 3, CD33, SORL1, Medizin, genetics [Alzheimer Disease], Adaptor Proteins, Signal Transducing/genetics, Disease, PICALM, ABCA7, Disease susceptibility, 0302 clinical medicine, genetics [Adaptor Proteins, Signal Transducing], Databases, Genetic, GWAS, GENE-EXPRESSION, Medicine(all), Aged, 80 and over, Genetics, 0303 health sciences, Alzheimer's disease, genetic predisposition, Receptor, EphA1, ALZHEIMER’S DISEASE, Antigens, CD/genetics, genetics [Receptor, EphA1], genetics [Membrane Proteins], Multigene Family, Female, genetics [Antigens, Differentiation, Myelomonocytic], APOE, Antigens, Differentiation, Myelomonocytic, Single-nucleotide polymorphism, Case-control studies, Cytoskeletal Proteins/genetics, Biology, Polymorphism, Single Nucleotide, Article, 03 medical and health sciences, CD33 protein, human, Alzheimer Disease, Antigens, CD, ddc:570, Humans, Genetic Predisposition to Disease, Membrane Proteins/genetics, CLUSTERIN, Aged, genetics [Cytoskeletal Proteins], Adaptor Proteins, Signal Transducing, 030304 developmental biology, Alzheimer Disease/genetics, Antigens, Differentiation, Myelomonocytic/genetics, Genetic Variation, Membrane Proteins, CD2-associated protein, genetics [Antigens, CD], Cytoskeletal Proteins, MS4A4E protein, human, Case-Control Studies, Susceptibility locus, biology.protein, ATP-Binding Cassette Transporters, Human medicine, genetics [ATP-Binding Cassette Transporters], aged, 80 and over, Receptor, EphA1/genetics, 030217 neurology & neurosurgery, Genome-Wide Association Study

Abstract

We sought to identify new susceptibility loci for Alzheimer's disease through a staged association study (GERAD+) and by testing suggestive loci reported by the Alzheimer's Disease Genetic Consortium (ADGC) in a companion paper. We undertook a combined analysis of four genome-wide association datasets (stage 1) and identified ten newly associated variants with P ĝ‰Currency sign 1 × 10 -5. We tested these variants for association in an independent sample (stage 2). Three SNPs at two loci replicated and showed evidence for association in a further sample (stage 3). Meta-analyses of all data provided compelling evidence that ABCA7 (rs3764650, meta P = 4.5 × 10 -17; including ADGC data, meta P = 5.0 × 10 -21) and the MS4A gene cluster (rs610932, meta P = 1.8 × 10 -14; including ADGC data, meta P = 1.2 × 10 -16) are new Alzheimer's disease susceptibility loci. We also found independent evidence for association for three loci reported by the ADGC, which, when combined, showed genome-wide significance: CD2AP (GERAD+, P = 8.0 × 10 -4; including ADGC data, meta P = 8.6 × 10 -9), CD33 (GERAD+, P = 2.2 × 10 -4; including ADGC data, meta P = 1.6 × 10 -9) and EPHA1 (GERAD+, P = 3.4 × 10 -4; including ADGC data, meta P = 6.0 × 10 -10). © 2011 Nature America, Inc. All rights reserved.

Published

2011

12. Genome-wide association study and meta-analysis find that over 40 loci affect risk of type 1 diabetes

Author

Andrew Paterson, Neeraj Kumar, Luis Castaño, Jinny Willis, Valdis Pirags, David Altshuler, Farren Briggs, Neil Walker, Ondrej Cinek, Helen Schuilenburg, Francisco Javier Ampudia Blasco, Claire Vandiedonck, Mark A. Hall, Ana M Wägner, Xiaoying Li, Flemming Pociot, Didac Mauricio, Vaidotas Urbanavicius, Jennifer Couper, Adam Kretowski, Deborah Smyth, Professor David Dunger, Federico Vázquez, Ian Nicholson, Ellen Schofield, John Todd, Angela Simpson, Ingrid Kockum, Mikael Knip, Tadej Battelino, Thomas Brodnicki, Patrick Concannon, Jesús Argente, Johnny Ludvigsson, Peter Colman, Gurvinder Kaur, Vincent Plagnol, Oliver Burren, Rohana Abdul Ghani, Marta Hernández, William McLaren, Alessandro Doria, Raquel Corripio, Stephen Rich, Daniel Metzger, Jesper Johannesen, Steven Willi, Cécile JULIER, Vallo Tillmann, Bart Van der Auwera, Pathology/molecular and cellular medicine, and Diabetes Pathology & Therapy

Subjects

Male, Candidate gene, Interferon-Induced Helicase, IFIH1, Endocrinology, Diabetes and Metabolism, Genome-wide association study, Protein Tyrosine Phosphatase, Non-Receptor Type 22/genetics, DEAD-box RNA Helicases, 0302 clinical medicine, Chromosomes, Human, Pair 17/genetics, HLA Antigens, Genotype, CTLA-4 Antigen, Chromosomes, Human, Pair 2/genetics, Genetics, 0303 health sciences, Antigens, CD/genetics, Chromosome Mapping, HLA Antigens/genetics, Polymorphism, Single Nucleotide/genetics, 3. Good health, Chromosomes, Human, Pair 1/genetics, DEAD-box RNA Helicases/genetics, Chromosomes, Human, Pair 1, Chromosomes, Human, Pair 2, Meta-analysis, Female, Algorithms, 030209 endocrinology & metabolism, Locus (genetics), CLEC16A, DNA/genetics, Biology, Polymorphism, Single Nucleotide, Risk Assessment, Article, PTPN22, 03 medical and health sciences, Meta-Analysis as Topic, Antigens, CD, medicine, Humans, Family, 030304 developmental biology, Type 1 diabetes, Siblings, Protein Tyrosine Phosphatase, Non-Receptor Type 22, DNA, medicine.disease, Diabetes Mellitus, Type 1, Diabetes Mellitus, Type 1/epidemiology, Chromosome Mapping/methods, Chromosomes, Human, Pair 17, Genome-Wide Association Study

Abstract

Type 1 diabetes (T1D) is a common autoimmune disorder that arises from the action of multiple genetic and environmental risk factors. We report the findings of a new genome-wide association study of T1D, combined in a meta-analysis with two previously published studies. The total sample set included 7,514 cases and 9,045 reference samples. Forty-one distinct genomic locations provided evidence for association to T1D in the meta-analysis (P < 10-6). After excluding previously reported associations, 27 regions were further tested in an independent set of 4,267 cases, 4,463 controls and 2,319 affected sib-pair (ASP) families. Of these, 18 regions were replicated (P < 0.01; overall P < 5 × 10-8) and four additional regions provided nominal evidence of replication (P < 0.05). The many new candidate genes suggested by these results include IL10, IL19, IL20, GLIS3, CD69 and IL27.

Published

2009

13. Metabolism and insulin signaling in common metabolic disorders and inherited insulin resistance

Author

Kurt Højlund

Subjects

Hypoglycemia/genetics, Insulin/metabolism, Insulin Resistance/genetics, Obesity/genetics, Antigens, CD, Glycogen Synthase/metabolism, Receptor, Insulin/genetics, Glucose/metabolism, Humans, Insulin, Obesity, Muscle, Skeletal, Muscle, Skeletal/metabolism, Glucose Transporter Type 4, Polycystic Ovary Syndrome/genetics, Antigens, CD/genetics, Lipid Metabolism, Hypoglycemia, Receptor, Insulin, Adiponectin/metabolism, Glucose, Glycogen Synthase, Diabetes Mellitus, Type 2, Diabetes Mellitus, Type 2/genetics, Female, Adiponectin, Insulin Resistance, Glucose Transporter Type 4/metabolism, Polycystic Ovary Syndrome, Signal Transduction

Abstract

Type 2 diabetes, obesity and polycystic ovary syndrome (PCOS) are common metabolic disorders which are observed with increasing prevalences, and which are caused by a complex interplay between genetic and environmental factors, including increased calorie intake and physical inactivity. These metabolic disorders are all characterized by reduced plasma adiponectin and insulin resistance in peripheral tissues. Quantitatively skeletal muscle is the major site of insulin resistance. Both low plasma adiponectin and insulin resistance contribute to an increased risk of type 2 diabetes and cardiovascular disease. In several studies, we have investigated insulin action on glucose and lipid metabolism, and at the molecular level, insulin signaling to glucose transport and glycogen synthesis in skeletal muscle from healthy individuals and in obesity, PCOS and type 2 diabetes. Moreover, we have described a novel syndrome characterized by postprandial hyperinsulinemic hypoglycemia and insulin resistance. This syndrome is caused by a mutation in the tyrosine kinase domain of the insulin receptor gene (INSR). We have studied individuals with this mutation as a model of inherited insulin resistance. Type 2 diabetes, obesity and PCOS are characterized by pronounced defects in the insulin-stimulated glucose uptake, in particular glycogen synthesis and to a lesser extent glucose oxidation, and the ability of insulin to suppress lipid oxidation. In inherited insulin resistance, however, only insulin action on glucose uptake and glycogen synthesis is impaired. This suggests that the defects in glucose and lipid oxidation in the common metabolic disorders are secondary to other factors. In young women with PCOS, the degree of insulin resistance was similar to that seen in middle-aged patients with type 2 diabetes. This supports the hypothesis of an unique pathogenesis of insulin resistance in PCOS. Insulin in physiological concentrations stimulates glucose uptake in human skeletal muscle in vivo by activation of the insulin signaling cascade to glucose transport through the enzymes IRS1, PI3K, Akt2, AS160/TBC1D4 and RAC1, and to glycogen synthesis through Akt2, inhibition of GSK3 and activation of glycogen synthase (GS) via dephosphorylation of serine residues in both the NH2-terminal (site 2+2a) and the COOH-terminal end (site 3a+3b). In type 2 diabetes, obesity and PCOS, there is, although with some variation from study to study, defects in insulin signaling through IRS1, PI3K, Akt2 and AS160/TBC1D4, which can explain reduced insulin action on glucose transport. In type 2 diabetes an altered intracellular distribution of SNAP23 and impaired activation of RAC1 also seem to play a role for reduced insulin action on glucose transport. In all common metabolic disorders, we observed an impaired insulin activation of GS, which seems to be caused by attenuated dephosphorylation of GS at site 2+2a, whereas as the inhibition of GSK3 and the dephosphorylation of GS at its target sites, site 3a+3a, appeared to be completely normal. In individuals with inherited insulin resistance, we observed largely the same defects in insulin action on IRS1, PI3K, Akt2 and GS, as well as a normal inhibition of GSK3 and dephosphorylation of GS at site 3a+3b. In these individuals, however, a markedly reduced insulin clearance seems to partially rescue insulin signaling to glucose transport and GS. Adiponectin is thought to improve insulin sensitivity primarily by increasing lipid oxidation through activation of the enzyme AMPK, and possibly via cross-talking of adiponectin with insulin signaling, and hence glucose transport and glycogen synthesis. We demonstrated a strong correlation between plasma adiponectin and insulin action on glucose disposal and glycogen synthesis in obesity, type 2 diabetes and PCOS. In individuals with inherited insulin resistance, plasma adiponectin was normal, but the correlation of adiponectin with insulin-stimulated glucose uptake and glycogen synthesis was at least equally strong. Moreover, we found a correlation between plasma adiponectin and insulin activation of GS. This result is supported by a number of recent studies of animal models and muscle cell lines, which have shown that adiponectin augments insulin action on enzymes in the insulin signaling cascade. In contrast, we observed no differences in the abundance or activity of AMPK in obesity, type 2 diabetes, PCOS or inherited insulin resistance. This indicates that reduced insulin sensitivity in these conditions is not mediated via abnormal AMPK activity. The results from these studies demonstrate that the well-established abnormalities in insulin action on glucose uptake and glycogen synthesis are reflected by defects in insulin signaling to these cellular processes in type 2 diabetes, obesity, and PCOS, and as expected also in inherited insulin resistance caused by a mutation in INSR. In common metabolic disorders, low plasma adiponectin may contribute to insulin resistance and defects in insulin signaling, whereas in inherited insulin resistance a normal plasma adiponectin and reduced insulin clearance could contribute to maintain a sufficient activation of the insulin signaling cascade. The insight gained from these studies have improved our understanding of the molecular mechanisms underlying insulin resistance in skeletal muscle of humans, and can form the basis for further studies, which can lead to the development of treatment that more directly targets insulin resistance, and hence reduce the risk of type 2 diabetes and cardiovascular disease.

Published

2014

14. Genome-wide association study confirms BST1 and suggests a locus on 12q24 as the risk loci for Parkinson's disease in the European population

Author

Philippe Amouyel, Jean-Charles Lambert, Alexis Brice, Mark Lathrop, Diana Zelenika, Alexandra Durr, Aude Saint-Pierre, Franck Durif, Pierre Pollak, Peter A. Silburn, Mohamad Saad, Christophe Tzourio, Philippe Damier, Jean-Christophe Corvol, Alexis Elbaz, Catherine Helmer, Marie Vidailhet, François Tison, George D. Mellick, Maria Martinez, Maurice Giroud, Sylvie Forlani, Marie-Anne Loriot, Ebba Lohmann, Florence Portet, and Suzanne Lesage

Subjects

Adult, Male, Genotype, In silico, Locus (genetics), Genome-wide association study, Single-nucleotide polymorphism, GPI-Linked Proteins/genetics, Biology, GPI-Linked Proteins, Genome, Polymorphism, Single Nucleotide, Europe/epidemiology, 03 medical and health sciences, 0302 clinical medicine, ADP-ribosyl Cyclase/genetics, Antigens, CD, Risk Factors, Genetics, Humans, Genetic Predisposition to Disease, ADP-ribosyl Cyclase, Molecular Biology, Gene, Genetics (clinical), 030304 developmental biology, Aged, 0303 health sciences, Chromosomes, Human, Pair 12, Parkinson Disease/epidemiology/genetics, Antigens, CD/genetics, Brain, Genetic Variation, Parkinson Disease, General Medicine, Middle Aged, ddc:616.8, Europe, Genetic Loci, Case-Control Studies, Female, RFX4, Chromosomes, Human, Pair 4, Brain morphogenesis, 030217 neurology & neurosurgery, Genome-Wide Association Study, Transcription Factors

Abstract

We performed a three-stage genome-wide association study (GWAS) to identify common Parkinson's disease (PD) risk variants in the European population. The initial genome-wide scan was conducted in a French sample of 1039 cases and 1984 controls, using almost 500 000 single nucleotide polymorphisms (SNPs). Two SNPs at SNCA were found to be associated with PD at the genome-wide significance level (P < 3 × 10(-8)). An additional set of promising and new association signals was identified and submitted for immediate replication in two independent case-control studies of subjects of European descent. We first carried out an in silico replication study using GWAS data from the WTCCC2 PD study sample (1705 cases, 5200 WTCCC controls). Nominally replicated SNPs were further genotyped in a third sample of 1527 cases and 1864 controls from France and Australia. We found converging evidence of association with PD on 12q24 (rs4964469, combined P = 2.4 × 10(-7)) and confirmed the association on 4p15/BST1 (rs4698412, combined P = 1.8 × 10(-6)), previously reported in Japanese data. The 12q24 locus includes RFX4, an isoform of which, named RFX4_v3, encodes brain-specific transcription factors that regulate many genes involved in brain morphogenesis and intracellular calcium homeostasis.

Published

2011

15. Mutant prominin 1 found in patients with macular degeneration disrupts photoreceptor disk morphogenesis in mice

Author

Pascal Escher, Michel Michaelides, Yang Li, Changguan Wang, Kim A. Howes, Wieland B. Huttner, Haoyu Chen, Yu Zhao, Zhengya Yu, Yuhong Chen, Chao Zhao, Yali Chen, Youssef T. Al-Sheikh, David S. Williams, Shin Kamaya, Martin Klein, Jeanne M. Frederick, Zhenglin Yang, Daniel F. Schorderet, David M. Hunt, Anthony T. Moore, Chunmei Li, Denis Corbeil, Jeremy Chien, Kang Zhang, Goutam Karan, David G. Birch, F. L. Munier, Wolfgang Baehr, Yuuki Kaminoh, Samantha Johnson, D. Joshua Cameron, and Concepción Lillo

Subjects

Retinal degeneration, medicine.medical_specialty, genetic structures, Mutant, Mutation, Missense, Morphogenesis, Cadherin Related Proteins, Protocadherin, Mice, Transgenic, Nerve Tissue Proteins, Biology, Macular Degeneration, Mice, Antigens, CD, Ophthalmology, Clinical investigation, Prominin-1, Retinitis pigmentosa, Electroretinography, medicine, Animals, Humans, In patient, AC133 Antigen, 610 Medicine & health, Glycoproteins, Genetics, Cadherin, business.industry, General Medicine, Macular degeneration, Cadherins, Actin cytoskeleton, medicine.disease, eye diseases, Cell biology, Actin Cytoskeleton, Antigens, CD/genetics, Antigens, CD/metabolism, Cadherins/metabolism, Glycoproteins/genetics, Glycoproteins/metabolism, Macular Degeneration/genetics, Macular Degeneration/physiopathology, Microfilaments/metabolism, Nerve Tissue Proteins/metabolism, Peptides/genetics, Peptides/metabolism, Photoreceptor Cells, Vertebrate/metabolism, Photoreceptor Cells, Vertebrate/ultrastructure, Commentary, sense organs, Peptides, business, Corrigendum, Photoreceptor Cells, Vertebrate

Abstract

Familial macular degeneration is a clinically and genetically heterogeneous group of disorders characterized by progressive central vision loss. Here we show that an R373C missense mutation in the prominin 1 gene (PROM1) causes 3 forms of autosomal-dominant macular degeneration. In transgenic mice expressing R373C mutant human PROM1, both mutant and endogenous PROM1 were found throughout the layers of the photoreceptors, rather than at the base of the photoreceptor outer segments, where PROM1 is normally localized. Moreover, the outer segment disk membranes were greatly overgrown and misoriented, indicating defective disk morphogenesis. Immunoprecipitation studies showed that PROM1 interacted with protocadherin 21 (PCDH21), a photoreceptor-specific cadherin, and with actin filaments, both of which play critical roles in disk membrane morphogenesis. Collectively, our results identify what we believe to be a novel complex involved in photoreceptor disk morphogenesis and indicate a possible role for PROM1 and PCDH21 in macular degeneration.

Published

2009

16. The integrin antagonist cilengitide activates alphaVbeta3, disrupts VE-cadherin localization at cell junctions and enhances permeability in endothelial cells

Author

Curzio Rüegg, Gian Carlo Alghisi, and Lionel Ponsonnet

Subjects

Angiogenesis, Integrin, lcsh:Medicine, Cilengitide, Biology, Cell Biology/Cell Signaling, Permeability, Focal adhesion, chemistry.chemical_compound, Antigens, CD, Cell Adhesion, Animals, Humans, Anoikis, Cardiovascular Disorders/Vascular Biology, Pyrroles, Phosphorylation, Cell adhesion, lcsh:Science, Cells, Cultured, Integrin alphaVbeta3, Multidisciplinary, Integrin beta1, lcsh:R, Endothelial Cells, Cadherins, Antigens, CD/genetics, Antigens, CD/metabolism, Antigens, CD29/metabolism, Cadherins/genetics, Cadherins/metabolism, Cell Adhesion/drug effects, Endothelial Cells/cytology, Endothelial Cells/drug effects, Endothelium, Vascular/cytology, Enzyme Induction, Focal Adhesion Protein-Tyrosine Kinases/metabolism, Integrin alphaVbeta3/antagonists & inhibitors, Integrin alphaVbeta3/metabolism, Intercellular Junctions/drug effects, Intercellular Junctions/metabolism, Pyrimidines/metabolism, Pyrroles/metabolism, Snake Venoms/pharmacology, src-Family Kinases/antagonists & inhibitors, src-Family Kinases/metabolism, Cell biology, Fibronectin, Cell Biology/Cell Adhesion, Intercellular Junctions, Pyrimidines, src-Family Kinases, chemistry, Oncology, Focal Adhesion Protein-Tyrosine Kinases, embryonic structures, biology.protein, cardiovascular system, lcsh:Q, Endothelium, Vascular, Research Article, Snake Venoms

Abstract

Cilengitide is a high-affinity cyclic pentapeptdic alphaV integrin antagonist previously reported to suppress angiogenesis by inducing anoikis of endothelial cells adhering through alphaVbeta3/alphaVbeta5 integrins. Angiogenic endothelial cells express multiple integrins, in particular those of the beta1 family, and little is known on the effect of cilengitide on endothelial cells expressing alphaVbeta3 but adhering through beta1 integrins. Through morphological, biochemical, pharmacological and functional approaches we investigated the effect of cilengitide on alphaVbeta3-expressing human umbilical vein endothelial cells (HUVEC) cultured on the beta1 ligands fibronectin and collagen I. We show that cilengitide activated cell surface alphaVbeta3, stimulated phosphorylation of FAK (Y(397) and Y(576/577)), Src (S(418)) and VE-cadherin (Y(658) and Y(731)), redistributed alphaVbeta3 at the cell periphery, caused disappearance of VE-cadherin from cellular junctions, increased the permeability of HUVEC monolayers and detached HUVEC adhering on low-density beta1 integrin ligands. Pharmacological inhibition of Src kinase activity fully prevented cilengitide-induced phosphorylation of Src, FAK and VE-cadherin, and redistribution of alphaVbeta3 and VE-cadherin and partially prevented increased permeability, but did not prevent HUVEC detachment from low-density matrices. Taken together, these observations reveal a previously unreported effect of cilengitide on endothelial cells namely its ability to elicit signaling events disrupting VE-cadherin localization at cellular contacts and to increase endothelial monolayer permeability. These effects are potentially relevant to the clinical use of cilengitide as anticancer agent.

Published

2009

17. Critical role of Cdc42 in mediating endothelial barrier protection in vivo

Author

Ramchandran, R., Mehta, D., Vogel, S. M., Mirza, M. K., Kouklis, P., and Malik, A. B.

Subjects

Cadherins/genetics, Mutation, Missense, Antigens, CD/genetics, Mice, Transgenic, Intercellular Junctions/genetics/*metabolism/pathology, Promoter Regions, Genetic/genetics, cdc42 GTP-Binding Protein/genetics/*metabolism, Genes, Dominant/genetics, rho GTP-Binding Proteins/genetics/metabolism, Blood-Air Barrier/*metabolism/pathology, Lipopolysaccharides/toxicity, Mice, Endothelial Cells/*metabolism/pathology, Capillary Permeability/drug effects/genetics, Electric Impedance, Animals, Pulmonary Edema/chemically induced/genetics/*metabolism/pathology

Abstract

Activation of the Rho GTPase Cdc42 has been shown in endothelial cell monolayers to prevent disassembly of interendothelial junctions and the increase in endothelial permeability. Here, we addressed the in vivo role of Cdc42 activity in mediating endothelial barrier protection in lungs by generating mice expressing the dominant active mutant V12Cdc42 protein in vascular endothelial cells targeted via the VE-cadherin promoter. These mice developed normally and exhibited constitutively active GTP-bound Cdc42. The increase in lung vascular permeability and gain in tissue water content in response to intraperitoneal lipopolysaccharide challenge (7 mg/kg) were markedly attenuated in the transgenic mice. To address the basis of the protective effect, we observed that expression of V12Cdc42 mutant in endothelial monolayers reduced the decrease in transendothelial electrical resistance, a measure of opening of interendothelial junctions, thus indicating that Cdc42 activity preserved junctional integrity. RhoA activity in V12Cdc42-expressing endothelial monolayers was reduced compared with untransfected cells, suggesting that activated Cdc42 functions by counteracting the canonical RhoA-mediated mechanism of endothelial hyperpermeability. Therefore, Cdc42 activity of microvessel endothelial cells is a critical determinant of junctional barrier restrictiveness and may represent a means of therapeutically modulating increased lung vascular permeability and edema formation. Am J Physiol Lung Cell Mol Physiol

Published

2008

18. Absence of alpha 7 integrin in dystrophin-deficient mice causes a myopathy similar to Duchenne muscular dystrophy.

Author

Guo, Chun, Willem, Michael, Werner, Alexander, Raivich, Gennadij, Emerson, Michael, Neyses, Ludwig, Mayer, Ulrike, Guo, Chun, Willem, Michael, Werner, Alexander, Raivich, Gennadij, Emerson, Michael, Neyses, Ludwig, and Mayer, Ulrike

Abstract

Both the dystrophin-glycoprotein complex and alpha7beta1 integrin have critical roles in the maintenance of muscle integrity via the provision of mechanical links between muscle fibres and the basement membrane. Absence of either dystrophin or alpha7 integrin results in a muscular dystrophy. To clarify the role of alpha7 integrin and dystrophin in muscle development and function, we generated integrin alpha7/dystrophin double-mutant knockout (DKO) mice. Surprisingly, DKO mice survived post-natally and were indistinguishable from wild-type, integrin alpha7-deficient and mdx mice at birth, but died within 24-28 days. Histological analysis revealed a severe muscular dystrophy in DKO mice with endomysial fibrosis and ectopic calcification. Weight loss was correlated with the loss of muscle fibres, indicating that progressive muscle wasting in the double mutant was most likely due to inadequate muscle regeneration. The data further support that premature death of DKO mice is due to cardiac and/or respiratory failure. The integrin alpha7/dystrophin-deficient mouse model, therefore, resembles the pathological changes seen in Duchenne muscular dystrophy and suggests that the different clinical severity of dystrophin deficiency in human and mouse may be due to a fine-tuned difference in expression of dystrophin and integrin alpha7 in both species. Together, these findings indicate an essential role for integrin alpha7 in the maintenance of dystrophin-deficient muscles.

Published

2006

19. Reduced intragraft mRNA expression of matrix metalloproteinases Mmp3, Mmp12, Mmp13 and Adam8, and diminished transplant arteriosclerosis in Ccr5-deficient mice.

Author

Luckow, Bruno, Joergensen, Joanne, Chilla, Silvia, Li, Jian-Ping, Henger, Anna, Kiss, Eva, Wieczorek, Grazyna, Roth, Lukas, Hartmann, Nicole, Hoffmann, Reinhard, Kretzler, Matthias, Nelson, Peter J., Perez de Lema, Guillermo, Maier, Holger, Wurst, Wolfgang, Balling, Rudi, Pfeffer, Klaus, Grone, Hermann-Josef, Schlondorff, Detlef, Zerwes, Hans-Gunter, Luckow, Bruno, Joergensen, Joanne, Chilla, Silvia, Li, Jian-Ping, Henger, Anna, Kiss, Eva, Wieczorek, Grazyna, Roth, Lukas, Hartmann, Nicole, Hoffmann, Reinhard, Kretzler, Matthias, Nelson, Peter J., Perez de Lema, Guillermo, Maier, Holger, Wurst, Wolfgang, Balling, Rudi, Pfeffer, Klaus, Grone, Hermann-Josef, Schlondorff, Detlef, and Zerwes, Hans-Gunter

Abstract

Experimental and human organ transplant studies suggest an important role for chemokine (C-C-motif) receptor-5 (CCR5) in the development of acute and chronic allograft rejection. Because early transplant damage can predispose allografts to chronic dysfunction, we sought to identify potential pathophysiologic mechanisms leading to allograft damage by using wild-type and Ccr5-deficient mice as recipients of fully MHC-mismatched heart and carotid-artery allografts. Gene expression in rejecting heart allografts was analyzed 2 and 6 days after transplantation using Affymetrix GeneChips. Microarray analysis led to identification of four metalloproteinase genes [matrix metalloproteinase (Mmp)3, Mmp12, Mmp13 and a disintegrin and metalloprotease domain (Adam)8] with significantly diminished intragraft mRNA expression in Ccr5-deficient mice at day 6. Accordingly, allografts from Ccr5-deficient mice showed less tissue remodeling and hence better preservation of the myocardial architecture compared with allografts from wild-type recipients. Moreover, survival of cardiac allografts was significantly increased in Ccr5-deficient mice. Carotid artery allografts from Ccr5-deficient recipients showed better tissue preservation, and significant reduction of neointima formation and CD3+ T cell infiltration. Ccr5 appears to play an important role in transplant-associated arteriosclerosis that may involve metalloproteinase-mediated vessel wall remodeling. We conclude that early tissue remodeling may be a critical feature in the predisposition of allografts to the development of chronic dysfunction.

Published

2004

20. Endothelin-1 upregulates MCAM in melanocytes

Author

Mangahas, Catherine R, dela Cruz, Gelo V, Schneider, Robert J, Jamal, Sumayah, Mangahas, Catherine R, dela Cruz, Gelo V, Schneider, Robert J, and Jamal, Sumayah

Abstract

Melanoma cell adhesion molecule (MCAM) is a cell-surface adhesion molecule expressed on over 70% of metastatic melanoma cells but not expressed in normal melanocytes invivo. Protein levels of MCAM correlate with aggressive invasive behavior of melanoma cells in vitro and invivo. Here we demonstrate that endothelin-1 (ET-1) upregulates MCAM protein in primary human melanocytes. MCAM upregulation by ET-1 occurs irrespective of degree of melanocyte pigmentation and is dose-responsive. The drug BQ788 is an endothelin-B (ET(B)) receptor antagonist and inhibits upregulation of MCAM by ET-1. In addition, endothelin-3 (ET-3) and N-succinyl-[Glu9, Ala11, 15]-ET-1-1620, both selective ET(B) agonists, are potent upregulators of MCAM. These demonstrate a critical role for the ET(B) receptor in the upregulation of MCAM by ET-1 and related isoforms. MCAM mRNA abundance is also increased by ET-1 stimulation, thus the mechanism of MCAM protein upregulation may occur at the level of transcription. Our previous studies have demonstrated that ET-1 downregulates E-cadherin in melanocytes and melanoma cells. Since E-cadherin is a melanoma invasion suppressor, and MCAM is a melanoma invasion promoter, ET-1 may promote melanoma invasion and metastasis through the regulation of adhesion molecule expression.

Published

2004

21. HPA-1a phenotype-genotype discrepancy reveals a naturally occurring Arg93Gln substitution in the platelet beta 3 integrin that disrupts the HPA-1a epitope.

Author

Watkins, Nicholas A., Schaffner-Reckinger, Elisabeth, Allen, David L., Howkins, Graham J., Brons, Nicolaas H. C., Smith, Graham A., Metcalfe, Paul, Murphy, Michael F., Kieffer, Nelly, Ouwehand, Willem H., Watkins, Nicholas A., Schaffner-Reckinger, Elisabeth, Allen, David L., Howkins, Graham J., Brons, Nicolaas H. C., Smith, Graham A., Metcalfe, Paul, Murphy, Michael F., Kieffer, Nelly, and Ouwehand, Willem H.

Abstract

A single nucleotide polymorphism (SNP) at position 196 in the beta 3 integrin causes a Leu33Pro substitution in the mature protein. Alloimmunization against the beta 3Leu33 form (human platelet antigen [HPA]-1a, Pl(A1), Zw(a)) in patients who are beta 3Pro33 homozygous (HPA-1b1b, Pl(A2A2), Zw(bb)) causes neonatal alloimmune thrombocytopenia, posttransfusion purpura, or refractoriness to platelet transfusion. Studies with recombinant proteins have demonstrated that amino acids 1 to 66 and 288 to 490 of the beta 3 integrin contribute to HPA-1a epitope formation. In determining the HPA-1a status of more than 6000 donors, we identified a donor with an HPA-1a(weak) phenotype and an HPA-1a1b genotype. The platelets from this donor had normal levels of surface alpha IIb beta 3 but reacted only weakly with monoclonal and polyclonal anti-HPA-1a by whole blood enzyme-linked immunosorbent assay (ELISA), flow cytometry, and sandwich ELISA. We reasoned that an alteration in the primary nucleotide sequence of the beta 3Leu33 allele of this donor was disrupting the HPA-1a epitope. In agreement with this hypothesis, sequencing platelet RNA-derived alpha IIb and beta 3 cDNA identified a novel G/A SNP at position 376 of the beta 3 integrin that encodes for an Arg93Gln replacement in the beta 3Leu33 allele. Coexpression of the beta 3Leu33Gln93 encoding cDNA in Chinese hamster ovary cells with human alpha IIb cDNA showed that the surface-expressed alpha IIb beta 3 reacted normally with beta 3 integrin-specific monoclonal antibodies but only weakly with monoclonal anti-HPA-1a. Our results show that an Arg93Gln mutation in the beta 3Leu33 encoding allele disrupts the HPA-1a epitope, suggesting that Arg93 contributes to the formation of the HPA-1a B-cell epitope.

Published

2002

22. Genetic analysis of immunomodulating factors in sporadic Parkinson's disease.

Author

Luxembourg Centre for Systems Biomedicine (LCSB): Clinical & Experimental Neuroscience (Krüger Group) [research center], Krüger, Rejko, Hardt, C., Tschentscher, F., Jackel, S., Kuhn, W., Muller, T., Werner, J., Woitalla, D., Berg, D., Kuhnl, N., Fuchs, G. A., Santos, E. J., Przuntek, H., Epplen, J. T., Schols, L., Riess, O., Luxembourg Centre for Systems Biomedicine (LCSB): Clinical & Experimental Neuroscience (Krüger Group) [research center], Krüger, Rejko, Hardt, C., Tschentscher, F., Jackel, S., Kuhn, W., Muller, T., Werner, J., Woitalla, D., Berg, D., Kuhnl, N., Fuchs, G. A., Santos, E. J., Przuntek, H., Epplen, J. T., Schols, L., and Riess, O.

Abstract

Immunomodulating factors have been shown to play a role in the pathogenesis of Parkinson's disease (PD) by biochemical methods. In order to investigate functionally important genes of the tumor necrosis factor alpha (TNFalpha) pathway we studied the frequency of DNA polymorphisms in the interleukin 6 (IL6), the TNFalpha, and the TNFalpha receptor 1 (TNFR1) genes in 264 sporadic German PD patients and in 183 age and sex matched German healthy controls. Analyzing the TNFalpha-308 polymorphism we found heterozygous individuals carrying alleles 1 and 2 more frequently in patients with a relative risk of 1.56 (p = 0.046, p(c) = 0.13, chi2 = 3.98). In contrast, the frequency of the B/2 haplotype described by the TNFR1-609 and TNFRI+36 polymorphisms was significantly decreased in our PD patients group (p = 0.0097, p(c) = 0.048, chi2 = 6.69) with a relative risk reduced to 0.52. Our results suggest an involvement of immunomodulating factors in the pathogenesis of sporadic PD as revealed by a molecular genetic approach.

Published

2000

23. The PROM1 Mutation p. R373C Causes an Autosomal Dominant Bull's Eye Maculopathy Associated with Rod, Rod-Cone, and Macular Dystrophy

Author

Anthony T. Moore, K. Bradshaw, Kang Zhang, Matthew Bedell, Daniel F. Schorderet, Pascal Escher, Andrew R. Webster, Marie-Claire Gaillard, François-Xavier Borruat, Leila Tiab, Francis L. Munier, Michel Michaelides, David M. Hunt, Ruben Carmona, Graham E. Holder, Anthony G. Robson, Michelle E. McClements, Daniel Barthelmes, E.T. White, University of Zurich, and Michaelides, M

Subjects

Male, Fovea Centralis, genetic structures, animal diseases, 2804 Cellular and Molecular Neuroscience, Gene, Retinal Rod Photoreceptor Cells, AC133 Antigen, Age of Onset, Abnormal Fundus Autofluorescence, 610 Medicine & health, Frameshift Mutation, Genes, Dominant, Genetics, medicine.diagnostic_test, Articles, Middle Aged, Macular dystrophy, 2731 Ophthalmology, Pedigree, Bull's eye maculopathy, Phenotypes, Phenotype, Mutation (genetic algorithm), Retinal Cone Photoreceptor Cells, Female, Retinitis Pigmentosa, Tomography, Optical Coherence, 10018 Ophthalmology Clinic, Adult, medicine.medical_specialty, animal structures, Adolescent, Biology, Update, Frameshift mutation, 2809 Sensory Systems, Young Adult, Retinitis-Pigmentosa, Chromosome-4, Antigens, CD, Ophthalmology, Retinitis pigmentosa, medicine, Electroretinography, Humans, Point Mutation, Glycoproteins, Antigens, CD/genetics, Family Health, Fovea Centralis/pathology, Glycoproteins/genetics, Peptides/genetics, Retinal Cone Photoreceptor Cells/pathology, Retinal Rod Photoreceptor Cells/pathology, Retinitis Pigmentosa/ethnology, Retinitis Pigmentosa/genetics, urogenital system, Iscev Standard, medicine.disease, eye diseases, Maculopathy, Photoreceptor Degeneration, sense organs, Peptides

Abstract

PURPOSE: To characterize in detail the phenotype of five unrelated families with autosomal dominant bull's eye maculopathy (BEM) due to the R373C mutation in the PROM1 gene. METHODS: Forty-one individuals of five families of Caribbean (family A), British (families B, D, E), and Italian (family C) origin, segregating the R373C mutation in PROM1, were ascertained. Electrophysiological assessment, fundus autofluorescence (FAF) imaging, fundus fluorescein angiography (FFA), and optical coherence tomography (OCT) were performed in available subjects. Mutation screening of PROM1 was performed. RESULTS: The R373C mutant was present heterozygously in all affected patients. The age at onset was variable and ranged between 9 and 58 years, with most of the individuals presenting with reading difficulties. Subjects commonly had a mild to moderate reduction in visual acuity except for members of family C who experienced markedly reduced central vision. The retinal phenotype was characterized by macular dystrophy, with retinal pigment epithelial mottling in younger subjects, progressing to typical BEM over time, with the development of macular atrophy in older patients. In addition, all members of family C had typical features of RP. The electrophysiological findings were variable both within and between families. CONCLUSIONS: Mutations in PROM1 have been described to cause a severe form of autosomal recessive RP in two families of Indian and Pakistani descent. The results of this study have demonstrated that a distinct redundant PROM1 mutation (R373C) can also produce an autosomal dominant, fully penetrant retinopathy, characterized by BEM with little inter- and intrafamilial variability, and retinal dystrophy with variable rod or rod-cone dysfunction and marked intra- and interfamilial variability, ranging from isolated maculopathy without generalized photoreceptor dysfunction to maculopathy associated with very severe rod-cone dysfunction.

24. Tolerance without clonal expansion: self-antigen-expressing B cells program self-reactive T cells for future deletion

Author

Thorsten Buch, Ari Waisman, F. Thomas Wunderlich, Tobias J. A. J. Heinen, Werner Müller, Nir Yogev, Axel Roers, Friederike Frommer, Stephen M. Anderton, Estelle Bettelli, University of Zurich, and Waisman, Ari

Subjects

T-Lymphocytes, Programmed Cell Death 1 Receptor, Autoimmunity, Antigens, CD/biosynthesis, Antigens, CD5/genetics, Autoantigens, Interleukin 21, Mice, Immunology and Allergy, Cytotoxic T cell, Homeostasis, CTLA-4 Antigen, IL-2 receptor, Antigens, Differentiation/biosynthesis, B-Lymphocytes, Antigens, CD/genetics, B-Lymphocytes/immunology, T-Lymphocytes/metabolism, Natural killer T cell, Cell biology, medicine.anatomical_structure, Homeostasis/immunology, 2723 Immunology and Allergy, Antigens, CD5/biosynthesis, Antigens, Differentiation/genetics, Antigens, CD5/immunology, T cell, Immunology, Antigens, CD/immunology, Clonal Deletion, 610 Medicine & health, chemical and pharmacologic phenomena, Mice, Transgenic, Biology, Autoantigens/biosynthesis, CD5 Antigens, Autoimmunity/physiology, Autoantigens/immunology, Antigens, CD, medicine, Animals, B-Lymphocytes/metabolism, Antigen-presenting cell, Cell Proliferation, 2403 Immunology, Antigens, Differentiation/immunology, Gene Expression Regulation/immunology, CD40, Clonal Deletion/physiology, T-Lymphocytes/immunology, Antigens, Differentiation, 10040 Clinic for Neurology, B-1 cell, Gene Expression Regulation, biology.protein

Abstract

B cells have been shown in various animal models to induce immunological tolerance leading to reduced immune responses and protection from autoimmunity. We show that interaction of B cells with naive T cells results in T cell triggering accompanied by the expression of negative costimulatory molecules such as PD-1, CTLA-4, B and T lymphocyte attenuator, and CD5. Following interaction with B cells, T cells were not induced to proliferate, in a process that was dependent on their expression of PD-1 and CTLA-4, but not CD5. In contrast, the T cells became sensitive to Ag-induced cell death. Our results demonstrate that B cells participate in the homeostasis of the immune system by ablation of conventional self-reactive T cells.

25. Differential roles of tumor necrosis factor-alpha and interferon-gamma in mouse hypermetabolic and anorectic responses induced by LPS

Author

Arsenijevic D, Garcia I, Vesin C, Vesin D, Arsenijevic Y, Seydoux J, Girardier L, Ryffel B, Abdul DULLOO, and Richard D

Subjects

Lipopolysaccharides, Male, Transcriptional Activation, Receptors, Tumor Necrosis Factor/genetics, Cytokines/biosynthesis/blood/genetics, Mice, Transgenic, ddc:616.07, Tumor Necrosis Factor-alpha/biosynthesis/genetics/ immunology, Receptors, Tumor Necrosis Factor, Energy Metabolism/drug effects, Eating, Interferon-gamma, Mice, Antigens, CD, Animals, RNA, Messenger, Lymphotoxin-alpha, Lymphotoxin-alpha/genetics/immunology, Receptors, Interferon, Mice, Knockout, Interferon-gamma/biosynthesis/ immunology, Brain/anatomy & histology/drug effects/immunology, Tumor Necrosis Factor-alpha, Evans Blue/metabolism, Receptors, Interferon/genetics, Antigens, CD/genetics, Brain, RNA, Messenger/biosynthesis, Mice, Inbred C57BL, Blood-Brain Barrier, Receptors, Tumor Necrosis Factor, Type I, Spleen/drug effects/immunology, Cytokines, Female, Lipopolysaccharides/ pharmacology, Energy Metabolism, Blood-Brain Barrier/drug effects, Spleen, Evans Blue

Abstract

Lipopolysaccharide (LPS)-induced effects on energy balance are characterized by alterations in energy expenditure (hypermetabolism) and food intake (anorexia). To study the role of tumour necrosis factor alpha (TNF-alpha) on some of these metabolic responses to endotoxin, we have used transgenic mice expressing soluble tumour necrosis factor receptor-1 IgG fusion protein (TNFR1-IgG) as well as TNF-alpha knockout (KO), lymphotoxin-alpha (LT-alpha) KO, and interferon-gamma receptor (IFN-gamma R) KO mice. The results from TNFR1-IgG transgenic mice suggest that the hypermetabolic and anorectic responses induced by LPS are independently regulated since, in the absence of TNF-alpha or LT-alpha, the LPS-induced hypermetabolism is almost prevented but not the anorexia. The anorectic response shows the strongest association with IFN-gamma since both IFN-gamma R KO mice and mice treated with anti-IFN-gamma antibody showed marked reduction in the LPS-induced anorexia compared to other mice. IFN-gamma R KO mice also have an attenuated thermogenic response to endotoxin. Anti-Asialo GM1 antibody treatment attenuated both the hypermetabolic and anorectic responses to LPS, to an extent comparable to that observed in IFN-gamma R KO mice. This finding suggests that natural killer cells (lymphocytic subsets) may be involved in IFN-gamma production and play an important role in the metabolic alterations induced by LPS. We also showed that the hypermetabolic response of control mice is associated with an upregulation of cytokine expression within the brain and an increase in permeability of the blood brain barrier. LPS-induced anorexia appears to involve peripheral cytokine expression.