Your search keyword '"Amino acid substitution"' showing total 114 results

1. [Discrepancies in FVII:C levels depending on the thromboplastin: about a case]

Author

Rémi Balluet, Marie-Odile Geay-Baillat, Alexane Bourguignon, and Sandra Le Quellec

Subjects

Adult, medicine.medical_specialty, Laboratory monitoring, Factor VII Deficiency, Mutation, Missense, Gastroenterology, Thromboplastin, chemistry.chemical_compound, Pregnancy, hemic and lymphatic diseases, Internal medicine, medicine, Humans, In patient, cardiovascular diseases, Factor VII deficiency, Blood Coagulation, Incidental Findings, Factor VII, business.industry, Pregnancy Complications, Hematologic, Infant, Newborn, General Medicine, medicine.disease, chemistry, Coagulation, Amino Acid Substitution, Female, Blood Coagulation Tests, business

Abstract

Factor VII deficiency is the most common of the rare coagulation deficiencies. A hemorrhagic syndrome may occur in patients with FVII deficiency below 20%, although no correlation exist between the plasma FVII activity level (FVII:C) and the bleeding risk. Therefore, the management of surgery in patients with FVII deficiency remains challenging. Laboratory monitoring of FVII:C level may be helpful but should be interpreted with caution, because the dosage of FVII:C level may vary depending on the origin of the thromboplastin used. Herein, we report the case of the management of a woman who had been fortuitously diagnosed during pregnancy with FVII deficiency due to FVII variant Padua, which have induced discrepant results between two different laboratories.

Published

2020

2. [When all roads lead to Africa…]

Author

J Andoni, Urtizberea, Hadil, Alrohaif, Sayed A, Gouda, and Laila, Bastaki

Subjects

Male, Adolescent, Myotonia Congenita, Siblings, DNA Mutational Analysis, Homozygote, Mutation, Missense, Saudi Arabia, Black People, High-Throughput Nucleotide Sequencing, Cleft Palate, Diagnosis, Differential, Phenotype, Amino Acid Substitution, Kuwait, Africa, Humans, Child, Malignant Hyperthermia, Qatar, Adaptor Proteins, Signal Transducing

Abstract

Congenital myopathies represent a quite heterogeneous group of neuromuscular disorders both at the clinical and genetic level. High-throughput sequencing (NGS), targeted or not, combined with muscle pathology, greatly facilitate their accurate characterization and occasionally lead to unexpected discoveries like in the case reported here in a Kuwaiti family facing a long diagnostic odyssey.Quand tous les chemins mènent à l’Afrique….Les myopathies congénitales constituent un ensemble hétérogène de maladies neuromusculaires aussi bien sur le plan clinique que génétique. Le séquençage à haut débit, ciblé ou non, couplé à l’analyse de la biopsie musculaire, facilite grandement leur caractérisation précise et conduisent parfois à des découvertes inattendues comme dans le cas rapporté ci-dessous d’une famille koweitienne en errance diagnostique depuis de nombreuses années.

Published

2019

3. [Pathogenesis of thrombosis in JAK2V617F myeloproliferative neoplasms]

Author

Alexandre, Guy and Chloé, James

Subjects

Blood Platelets, Myeloproliferative Disorders, Amino Acid Substitution, Phenylalanine, Mutation, Missense, Animals, Humans, Thrombosis, Valine, Janus Kinase 2

Abstract

BCR-ABL negative myeloproliferative neoplasms are acquired hematologic diseases characterized by blood cell proliferation and that include polycythemia vera (PV), essential thrombocytemia (ET) and primary myelofibrosis (PMF). Occurring of venous and arterial thrombosis is the main complication of these diseases. Risk factors for thrombosis are individuals older than 60 and history of thrombosis. The mechanisms leading to thrombosis are complex and involve several blood compartments, plasmatic factors and endothelial cells. Over the last years, new actors of thrombosis have been discovered.La thrombose au cours des néoplasies myéloprolifératives - Influence de la mutation JAK2V617F.Les néoplasies myéloprolifératives (NMP) sans translocation de Philadelphie sont des maladies hématologiques acquises caractérisées par la prolifération d’une ou plusieurs lignées sanguines. Elles regroupent la polyglobulie de Vaquez (PV), la thrombocytémie essentielle (TE) et la myélofibrose primitive (MFP). La survenue de thromboses artérielles ou veineuses est un risque majeur au cours de ces maladies. Les facteurs de risque reconnus actuellement sont un âge supérieur à 60 ans et un antécédent de thrombose. Les mécanismes concourant à ce risque pro-thrombotique augmenté sont cependant multiples et complexes, impliquant l’ensemble des cellules sanguines, des facteurs plasmatiques et le compartiment endothélial. Ces dernières années, de nouveaux mécanismes physiopathologiques ont été révélés.

Published

2019

4. [In silico study of a functional mutation associated with non-small cell lung cancer: G12D mutation of exon 2 in KRAS gene]

Author

Noria Bouras, Abdelkader Bousahba, T. Sahraoui, Fatima Zohra El Kebir, Florence de Fraipont, and Ahlam Megaïz

Subjects

Models, Molecular, Lung Neoplasms, In silico, DNA Mutational Analysis, Glycine, Mutation, Missense, Computational biology, Biology, medicine.disease_cause, Genome, Proto-Oncogene Mas, Proto-Oncogene Proteins p21(ras), Exon, Protein structure, Carcinoma, Non-Small-Cell Lung, Databases, Genetic, medicine, Missense mutation, Humans, Gene, Genetic Association Studies, Aspartic Acid, Computational Biology, General Medicine, Exons, Amino Acid Substitution, Algeria, Mutation (genetic algorithm), KRAS, Software

Abstract

Biology flourished during the XXth century and was profoundly disrupted during the last decade because of the transition to the post-genomic era, the spread of high-throughput biology, and the advent of a relatively new discipline, namely bioinformatics. This latter, which encompasses the collection, organization and analysis of biological data using the computer tool, has quickly become inseparable from the studies related to the genome understanding. The consequences of the different mutations that may affect our genes are responsible for a change in the protein sequence and are likely to affect, for example, the stability of the protein, its intracellular targeting, its maturation, its assembly in a multimeric structure, the essential sites for its enzymatic activity or for the interaction with ligands. Thus, a number of bioinformatic developments have made it possible to set up in silico prediction tools of the structure of a protein that is aiming at predicting the impact of local mutations on the structure of proteins. Throughout our study, we have been interested in exploring, through in silico bioinformatic study, three analytical, prediction and modeling, software, choosing as exemple the G12D mutation that affects the proto-oncogene KRAS found in numerous algerian patients with bronchopulmonary cancers cells (NSCLC). This study allowed us to integrate these bioinformatic tools into our laboratory of developmental biology and LBDD differentiation at the University of Oran 1 Ahmed Benbella, in Algeria. Thus, we have been able to conclude, even if the found mutation is predicted to be tolerated and has no deleterious effect on the entire Ras protein, that the consequence of this missense mutation depends mainly on the position in the protein and the chemical properties of the amino acid involved in the substitution and which shows a strong affinity with the GTP molecule.

Published

2019

5. [Triple hyperautofluorescent retinal ring. Pathognomonic appearance of c.166GA NR2E3-related inherited retinal degeneration]

Author

V M, Smirnov, C-M, Dhaenens, C, Vincent-Delorme, and S, Defoort-Dhellemmes

Subjects

Adolescent, Optical Imaging, Retinal Degeneration, Glycine, Arginine, Orphan Nuclear Receptors, Polymorphism, Single Nucleotide, Fluorescence, Retina, Amino Acid Substitution, Retinal Dystrophies, Humans, Female, Tomography, Optical Coherence

Published

2018

6. [Search for the T790M mutation: The need to persevere]

Author

H, Bourien, A, Lespagnol, A, Prigent, G, Leveiller, H, Lena, C, Ricordel, and R, Corre

Subjects

Male, Threonine, Lung Neoplasms, Time Factors, Biopsy, DNA Mutational Analysis, Mutation, Missense, Middle Aged, ErbB Receptors, Methionine, Amino Acid Substitution, Drug Resistance, Neoplasm, Carcinoma, Non-Small-Cell Lung, Humans, Female, Protein Kinase Inhibitors, Aged

Abstract

In cases of advanced EGFR mutation-positive non-small cell lung cancer, first or second generation EGFR-tyrosine kinase inhibitors (TKI-EGFR 1G or TKI-EGFR 2G) are recommended as first line treatment. Inexorably, progressive disease occurs and, in 50-60% of the cases, is secondary to a T790M resistant mutation. The prescription of osimertinib (TKI-EGFR3G) in second line is dependent on identification of the T790M mutation. We report 7 cases in which the identification of the T790M mutation required repeated analyses of cell free DNA and/or biopsies over a period of time. In some cases, a positive result was obtained a long time after progressive disease had been diagnosed during treatment with first or second generation EGFR-TKI. We discuss here the different modalities of screening for the T790M mutation and we encourage persevering in this search when no alternative mechanism of resistance has been identified.

Published

2017

7. [A complex case of diabetes due to LMNA mutation]

Author

C, Ambonville, M-A, Bouldouyre, P, Laforêt, P, Richard, O, Benveniste, and C, Vigouroux

Subjects

Diagnosis, Differential, Heterozygote, Phenotype, Amino Acid Substitution, Diabetes Mellitus, Type 2, Mutation, Missense, Humans, Female, Insulin Resistance, Middle Aged, Lamin Type A, Lipodystrophy, Familial Partial

Abstract

Laminopathies (diseases related to A/C mutations of lamines) are rare genetic diseases with an extensive phenotypic spectrum, including lipodystrophic syndromes-characterized by a selective loss of adipose tissue-of which the partial Dunnigan family type is the most frequent.We report on a 55-year-old woman with diabetes and long-term disabling myalgia. Her cushingoid morphotype, associated with cutaneous lipo-atrophy and muscle hypertrophy in addition to a genetic heritage, led us to the diagnosis of complex partial familial lipodystrophy heterozygous LMNA_c.82CT, p.Arg28Trp mutation.Familial partial lipodystrophic syndromes may have varied phenotypes, mainly cardio-metabolic, which could mimic a particularly severe type 2 diabetes. The diagnostic work-up of this disease has to include a careful investigation of gait troubles and paroxysmal conduction that could lead to sudden death, as well as a genetic examination. In some cases, recombinant leptin can be proposed.

Published

2017

8. Partial agonist and biased signalling properties of the synthetic enantiomers J113863/UCB35625 at chemokine receptors CCR2 and CCR5

Author

Jenny Corbisier, Marc Parmentier, Céline Galés, Alexandre Huszagh, and Jean-Yves Springael

Subjects

0301 basic medicine, CCR1, Agonist, Receptors, CCR5, Receptors, CCR2, medicine.drug_class, G protein, Mutation, Missense, Biotechnologie, CHO Cells, GTP-Binding Protein alpha Subunits, Gi-Go, Biology, Biochemistry, Partial agonist, 03 medical and health sciences, Chemokine receptor, Cricetulus, 0302 clinical medicine, Cell Movement, Cricetinae, parasitic diseases, Functional selectivity, medicine, Animals, Humans, Inverse agonist, Receptor, Molecular Biology, Cell Biology, beta-Arrestin 2, Sciences biomédicales, Cell biology, 030104 developmental biology, Amino Acid Substitution, Xanthenes, Sciences pharmaceutiques, 030217 neurology & neurosurgery, Protein Binding, Signal Transduction

Abstract

Biased agonism at G protein-coupled receptors constitutes a promising area of research for the identification of new therapeutic molecules. In this study we identified two novel biased ligands for the chemokine receptors CCR2 and CCR5 and characterized their functional properties. We showed that J113863 and its enantiomer UCB35625, initially identified as high affinity antagonists for CCR1 and CCR3, also bind with low affinity to the closely related receptors CCR2 and CCR5. Binding of J113863 and UCB35625 to CCR2 or CCR5 resulted in the full or partial activation of the three Gi proteins and the two Go isoforms. Unlike chemokines, the compounds did not activate G12. Binding of J113863 to CCR2 or CCR5 also induced the recruitment of -arrestin 2, whereas UCB35625 did not. UCB35625 induced the chemotaxis of L1.2 cells expressing CCR2 or CCR5. In contrast, J113863 induced the migration of L1.2-CCR2 cells but antagonized the chemokine-induced migration of L1.2- CCR5 cells. We also showed that replacing the phenylalanine 3.33 in CCR5 TM3 by the corresponding histidine of CCR2 converts J113863 from an antagonist for cell migration and a partial agonist in other assays to a full agonist in all assays. Further analyses indicated that F3.33H substitution strongly increased the activation of G proteins and β-arrestin 2 by J113863. These results highlight the biased nature of the J113863 and UCB35625 that act either as antagonist, partial agonist, or full agonist according to the receptor, the enantiomer, and the signaling pathway investigated., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2017

9. [Validation steps for the detection of L858R mutation in EGFR gene by real time quantitative PCR]

Author

Anne Gibeaud, Muriel Cadouot, Jean-Marc Riedinger, Astrid Brasselet, Sarab Lizard, Emeline Saitta, Vincent Goussot, Didier Bozonnet, and Marine Jourdain

Subjects

Oncology, Fastidious organism, medicine.medical_specialty, Lung Neoplasms, DNA Mutational Analysis, Mutation, Missense, Arginine, Real-Time Polymerase Chain Reaction, Sensitivity and Specificity, Egfr tki, Leucine, Limit of Detection, Internal medicine, Carcinoma, Non-Small-Cell Lung, medicine, Humans, Gene, Cells, Cultured, business.industry, Cancer, Reproducibility of Results, Amino acid substitution, General Medicine, medicine.disease, respiratory tract diseases, ErbB Receptors, Real-time polymerase chain reaction, Amino Acid Substitution, Non small lung cancer, MCF-7 Cells, business, L858r mutation

Abstract

Since January 16(th) 2010, the French legislation requires that the medical laboratories must be accredited according to ISO 15189 standards. This concerned all the biological medical technics, including molecular biology technics. In this work, we described the validation steps by real time quantitative PCR of L858R mutation in EGFR gene, frequently detected in non-small lung cancers (NSCLC). Epidermal growth factor - tyrosine kinase inhibitors (EGFR-TKIs) are authorized in Europe for the treatment of metastatic NSCLC after failure of, at least one, prior chemotherapy. Thus, in view of accreditation of this analysis, we have used the recommendation of the COFRAC (Comite francais d'accreditation) and INCa (Institut national du cancer). Several parameters have been tested, such as the primers, the limit of detection, and the sensitivity and specificity of the method. In addition, a risk study has been evaluated. Although long and fastidious, the method of validation is required to perform analysis in optimal conditions to guaranty optimal results for the patients.

Published

2016

10. [Granular dystrophy: Not always easy to classify].

Author

Memmi B, Valleix S, Bourcier T, Labetoulle M, and Rousseau A

Subjects

Adult, Amino Acid Substitution, Corneal Dystrophies, Hereditary complications, Corneal Dystrophies, Hereditary genetics, DNA Mutational Analysis, Diagnosis, Differential, Female, Humans, Mutation, Missense, Transforming Growth Factor beta1 analysis, Transforming Growth Factor beta1 genetics, Vision Disorders diagnosis, Vision Disorders etiology, Vision Disorders genetics, Corneal Dystrophies, Hereditary classification, Corneal Dystrophies, Hereditary diagnosis

Published

2020

11. [Discrepancies in FVII:C levels depending on the thromboplastin: about a case].

Author

Balluet R, Bourguignon A, Geay-Baillat MO, and Le Quellec S

Subjects

Adult, Amino Acid Substitution, Blood Coagulation genetics, Blood Coagulation Tests, Factor VII analysis, Factor VII Deficiency blood, Female, Humans, Incidental Findings, Infant, Newborn, Mutation, Missense, Pregnancy, Pregnancy Complications, Hematologic genetics, Thromboplastin analysis, Factor VII genetics, Factor VII metabolism, Factor VII Deficiency diagnosis, Factor VII Deficiency genetics, Pregnancy Complications, Hematologic diagnosis, Thromboplastin metabolism

Abstract

Factor VII deficiency is the most common of the rare coagulation deficiencies. A hemorrhagic syndrome may occur in patients with FVII deficiency below 20%, although no correlation exist between the plasma FVII activity level (FVII:C) and the bleeding risk. Therefore, the management of surgery in patients with FVII deficiency remains challenging. Laboratory monitoring of FVII:C level may be helpful but should be interpreted with caution, because the dosage of FVII:C level may vary depending on the origin of the thromboplastin used. Herein, we report the case of the management of a woman who had been fortuitously diagnosed during pregnancy with FVII deficiency due to FVII variant Padua, which have induced discrepant results between two different laboratories.

Published

2020

12. [Chronic cutaneous lesions in a 73-year-old patient]

Author

S, Abbara, C, Bachmeyer, K, Stankovic Stojanovic, S, Amselem, G, Grateau, S, Georgin-Lavialle, B, Couturier, and E, Cogan

Subjects

Diagnosis, Differential, Amino Acid Substitution, Chronic Disease, NLR Family, Pyrin Domain-Containing 3 Protein, Humans, Female, Carrier Proteins, Skin Diseases, Cryopyrin-Associated Periodic Syndromes, Aged

Published

2015

13. [Sickle cell pathophysiology]

Author

P, Renaudier

Subjects

Amino Acid Substitution, Thrombotic Microangiopathies, Hemoglobin, Sickle, Cell Adhesion, Erythrocytes, Abnormal, Humans, Pain, Anemia, Sickle Cell, Endothelium, Vascular, Erythrocyte Aging, beta-Globins, Cell Shape, Hydrophobic and Hydrophilic Interactions

Abstract

Sickle cell disease is associated with the inversion of one base pair (A = T → A = T). The sixth codon of the beta globin chain [GAA] becomes [GTA]. Accordingly, the sixth amino acid (glutamic acid, negatively charged) is replaced by valine, hydrophobic. A hydrophobic site is present on the outside of the HbS β chain. This incurs a hydrophobic bond with the phenylalanine in position 85 and leucine in position 88, in which outsource deoxy haemoglobin. Therefore, it creates a HbS polymer that deforms the red blood cell and causes vaso-occlusive crisis in the capillary venous pole. In this conventional design, the roles are added to the nitrogen monoxide and vascular tone, the increase in adhesion of red blood cells to the endothelium damage caused by red blood cells HbS: dehydration, senescence, formation of microvesicles. If these advances in our understanding of the pathophysiology have not yet had a clinical application, they will happen one day. It is therefore particularly important to pursue in France the network structure of sickle cell disease with a view to set up multicenter trials when the day comes.

Published

2014

14. [When all roads lead to Africa…].

Author

Urtizberea JA, Alrohaif H, Gouda SA, and Bastaki L

Subjects

Adolescent, Africa, Amino Acid Substitution, Black People genetics, Child, Cleft Palate genetics, DNA Mutational Analysis, Diagnosis, Differential, High-Throughput Nucleotide Sequencing, Homozygote, Humans, Kuwait, Male, Malignant Hyperthermia genetics, Myotonia Congenita pathology, Phenotype, Qatar, Saudi Arabia, Siblings, Adaptor Proteins, Signal Transducing genetics, Cleft Palate diagnosis, Malignant Hyperthermia diagnosis, Mutation, Missense, Myotonia Congenita diagnosis, Myotonia Congenita genetics

Abstract

Congenital myopathies represent a quite heterogeneous group of neuromuscular disorders both at the clinical and genetic level. High-throughput sequencing (NGS), targeted or not, combined with muscle pathology, greatly facilitate their accurate characterization and occasionally lead to unexpected discoveries like in the case reported here in a Kuwaiti family facing a long diagnostic odyssey., (© 2019 médecine/sciences – Inserm.)

Published

2019

15. [Loss of human ICOSLG results in combined immunodeficiency].

Author

Roussel L, Landekic M, Golizeh M, Gavino C, Zhong MC, Chen J, Faubert D, Blanchet-Cohen A, Dansereau L, Parent MA, Marin S, Luo J, Le C, Ford BR, Langelier M, King IL, Divangahi M, Foulkes WD, Veillette A, and Vinh DC

Subjects

Adult, Amino Acid Substitution, Antigen Presentation, Chemotaxis, Leukocyte, Golgi Apparatus chemistry, Humans, Immunogenicity, Vaccine, Inducible T-Cell Co-Stimulator Ligand chemistry, Inducible T-Cell Co-Stimulator Ligand genetics, Inducible T-Cell Co-Stimulator Ligand immunology, Inducible T-Cell Co-Stimulator Protein immunology, Infections etiology, Lymphocyte Activation, Male, Mutation, Missense, Phenotype, Protein Transport, Recurrence, Severe Combined Immunodeficiency immunology, T-Lymphocytes immunology, Inducible T-Cell Co-Stimulator Ligand deficiency, Severe Combined Immunodeficiency genetics

Published

2019

16. [Triple hyperautofluorescent retinal ring. Pathognomonic appearance of c.166G>A NR2E3-related inherited retinal degeneration].

Author

Smirnov VM, Dhaenens CM, Vincent-Delorme C, and Defoort-Dhellemmes S

Subjects

Adolescent, Amino Acid Substitution, Arginine genetics, Female, Fluorescence, Glycine genetics, Humans, Optical Imaging, Retina pathology, Retina physiology, Retinal Degeneration genetics, Retinal Dystrophies genetics, Tomography, Optical Coherence, Orphan Nuclear Receptors genetics, Polymorphism, Single Nucleotide, Retina diagnostic imaging, Retinal Degeneration diagnosis, Retinal Dystrophies diagnosis

Published

2019

17. Meeting of the WHO expert working group on surveillance of influenza antiviral susceptibility, Geneva, July 2013

Subjects

Viral Matrix Proteins, Inhibitory Concentration 50, Amino Acid Substitution, Population Surveillance, Influenza, Human, Humans, Neuraminidase, Microbial Sensitivity Tests, Orthomyxoviridae, World Health Organization, Antiviral Agents

Published

2013

18. [Cerebrotendinous xanthomatosis: a multicentric retrospective study of 15 adults, clinical and paraclinical typical and atypical aspects]

Author

C, Lionnet, C, Carra, X, Ayrignac, T, Levade, D, Gayraud, G, Castelnovo, G, Besson, G, Androdias, S, Vukusic, C, Confavreux, C, Zaenker, J, De Seze, N, Collongues, F, Blanc, C, Tranchant, D, Wallon, D, Hannequin, A, Gerdelat-Mas, D, Brassat, M, Clanet, H, Zephir, O, Outteryck, P, Vermersch, and P, Labauge

Subjects

Adult, Male, Mutation, Missense, Brain, Genes, Recessive, Xanthomatosis, Cerebrotendinous, Middle Aged, Chenodeoxycholic Acid, Magnetic Resonance Imaging, Amino Acid Substitution, Cholestanetriol 26-Monooxygenase, Humans, Female, Age of Onset, Symptom Assessment, Aged, Retrospective Studies

Abstract

Cerebrotendinous xanthomatosis, a metabolic leukodystrophy with an autosomal recessive inheritance, is secondary to deficiency of sterol 27-hydroxylase, an enzyme involved in cholesterol catabolism. Classical symptoms include clinical or infraclinical xanthomas affecting the skin and tendons, early cataracts, neurological signs and diarrhea. Brain imaging reveals involvement of the dentate nuclei and periventricular white matter hyperintensities. The diagnosis is based on an increased cholestanol level in serum, confirmed by the presence of a mutation in the CYP27A1 gene. Treatment is based on chenodeoxycholic acid.We report a retrospective multicentric study of 15 cases of cerebrotendinous xanthomatosis diagnosed in French adults. Clinical, molecular and MRI findings were recorded in all patients.The average age at diagnosis was 39years (range 27-65). Disease onset occurred in childhood in 73% of patients and in adulthood in 27%. All patients with a pediatric onset were diagnosed during adulthood (age range 28-65years). Clinical symptoms variably associated cerebellar syndrome, pyramidal syndrome, cognitive decline, epilepsy, neuropathy (sought in 10 of our patients, present in forms in 8), psychiatric disorders, cataract and xanthomas. One patient had an atypical presentation: monoparesis associated with xanthomas. Brain MRI was abnormal in all: findings consisted in T2-weighted hyperintensity of the dentate nuclei (47%), periventricular leuoencephalopathy (73%) which preferentially involved the posterior cerebral part (60%), leucoencephalopathy with a vascular pattern (7%), hyperintensity of the cortico-spinal tracts (53%), globi pallidi, corpus callosum and cerebral atrophy (33%). Serum cholestanol was elevated in 93% of patients. The most frequent mutation was 1183CT (n=5/15). Under treatment with chenodeoxycholic acid, eight patients improved initially, followed by stabilization in five of them, and worsening in the others. Four patients died.Patients with the xanthoma-neurological disorder association should be tested for cerebrotendinous xanthomatosis. The disease often begins in childhood with a diagnostic delay but also in adulthood. Involvement of the dentate nuclei is specific but not sensitive and the supratentorial leucoencephalopathy is not specific but with an antero-posterior gradient. A vascular distribution and involvement of the corpus callosum are possible. Serum cholestanol assay is very reliable: an elevated level provides the diagnosis, which must nevertheless be confirmed by molecular biology.

Published

2013

19. [Keratinisation disorders: new data]

Author

O, Dereure

Subjects

China, Chromosomes, Human, Pair 15, Heterozygote, Carcinoma, Mutation, Missense, Sequence Analysis, DNA, Endocytosis, Porokeratosis, ErbB Receptors, Adaptor Proteins, Vesicular Transport, Genetic Heterogeneity, Keratoacanthoma, Amino Acid Substitution, Scotland, Humans, Point Mutation, Exome, Collagen, Carrier Proteins, Conserved Sequence, Chromosomes, Human, Pair 8, Glycoproteins

Published

2013

20. [Myeloproliferative disorders 'Philadelphia negative' and JAK2V617F mutation: study of 15 cases in Togo]

Author

Irénée Messanh Delagnon Kueviakoe, Ahoefa Vovor, A. Y. Segbena, Kossi Agbetiafa, Ibrahima Sanogo, Koffi Amegbor, Stéphane Giraudier, Essohana Padaro, and Yao Layibo

Subjects

Adult, Male, Pediatrics, medicine.medical_specialty, Phenylalanine, Mutation, Missense, Essential Thrombocytemia, Cohort Studies, Myeloproliferative Disorders, Polycythemia vera, medicine, Humans, Philadelphia Chromosome, Jak2v617f mutation, Longitudinal Studies, Myelofibrosis, Aged, Philadelphia negative, business.industry, Valine, General Medicine, Janus Kinase 2, Middle Aged, medicine.disease, Prognosis, Middle age, Amino Acid Substitution, Togo, Female, business, Cohort study

Abstract

The goal of our study is to document the prevalence of change JAK2V617F among patients reached of myeloproliferative syndromes (MPS) in Togo in order to evaluate frequencies. This descriptive study included 15 patients followed with the CHU Campus for a SMP. The research of JAK2 change by PCR was carried out with the APHP Henri Mondor of Creteil (France). During the study period, 15 patients followed for MPS (9 cases of polycythemia Vera, 5 cases of essential thrombocytemia and a case of primitive myelofibrosis) profited from the research of JAK2 change. The Middle age of the patients was respectively of 45±18 years; of 55±6 years for the PV and the essential thrombocytemia. The patient followed for primitive myelofibrosis was 72 years old. Sex-ratio (H/F) was of 2. JAK2 Change was positive in 5 cases out of 9 (55.5%) of the polycythemia Vera, at 3 patients out of 5 (60%) followed for essential thrombocytemia but negative for patient reached of primitive myelofibrosis. In conclusion, JAK2 Change has an interest diagnosis and forecast in the MPS negative Chromosom Philadelphia and can be systematic even in Africa Sub-saharian.

Published

2012

21. [Implication of platelet-activating factor receptor A224D mutation in susceptibility to relapsing-remitting multiple sclerosis: A Tunisian population study]

Author

A, Messadi, N, Fekih-Mrissa, J, Zaouali, S, Layouni, B, Nsiri, M, Yedeas, A, Raies, R, Mrissa, and N, Gritli

Subjects

Adult, Male, Aspartic Acid, Alanine, Tunisia, Mutation, Missense, Platelet Membrane Glycoproteins, Severity of Illness Index, Receptors, G-Protein-Coupled, Young Adult, Genetics, Population, Multiple Sclerosis, Relapsing-Remitting, Amino Acid Substitution, Disease Progression, Humans, Female, Genetic Predisposition to Disease, Genetic Association Studies

Abstract

Platelet-activating factor interacts with its specific receptor and mediates leucocytes transmigration into central nervous system and expression of HLA molecules on antigens-presenting cells. These features are the major characteristics of multiple sclerosis pathology. In the present study, we investigated the role of platelet-activating factor receptor A224 mutation in the susceptibility to relapsing-remitting form of MS in a Tunisian population.Forty-seven multiple sclerosis patients and 72 healthy controls were genotyped for platelet-activating factor receptor A224D mutation using polymerase chain reaction-restriction fragment length polymorphism technique.We used three models of inheritance: the codominant, dominant and recessive models. Our results showed a predisposing effect of platelet-activating factor receptor 224D variant on susceptibility to relapsing-remitting multiple sclerosis (30% vs 48.1%, OR [IC 95%]=2.04 [1.04-3.99], P=0.023). Our results were also consistent with a dominant model of inheritance when comparing mild genotype (AA) with carriers of one or two copies of mutant allele (AD+DD) (55.7% vs 31.9%, OR [IC 95%]=2.92 [1.34-6.81], P=0.006). No effect of this mutation was shown when considering the age at disease onset, disease severity or gender.This first study reports an implication of platelet-activating factor receptor A224D mutation in the susceptibility to relapsing-remitting multiple sclerosis in Tunisian population. Further studies will be necessary to confirm the dominant role of PAFR A224D mutation and to elucidate the effect of this mutation on platelet-activating factor/platelet-activating factor receptor pathways.

Published

2010

22. [Genetic barrier to antiretroviral drug-resistance. Focus on raltegravir, the first integrase inhibitor]

Author

C, Delaugerre

Subjects

Clinical Trials as Topic, Virulence, Genetic Variation, HIV, HIV Infections, HIV Integrase, Virus Replication, Genes, pol, Pyrrolidinones, Amino Acid Substitution, Drug Resistance, Multiple, Viral, Raltegravir Potassium, Mutation, Humans, Point Mutation, Drug Interactions, Drug Therapy, Combination, HIV Integrase Inhibitors, Selection, Genetic

Abstract

The genetic barrier for the antiretroviral describes the ability to select resistant viruses to this antiretroviral when the viral replication is not controlled. This includes combining several concepts: (1) the number of nucleotide changes required for a resistance mutation, (2) the impact of this mutation on the level of susceptibility to antiretroviral (3) the impact of this mutation on viral replication capacity; all theses conditions influencing the level of resistant variants. The antiretroviral concentration impact also the emergence of resistance. Finally, combine with other molecules, the selection of resistance mutations ton an antiretroviral may differ from one treatment to another. It is recognized that the genetic barrier to lamivudine/emtricitabine, efavirenz and nevirapine is low, and is intermediate for nucleoside such as zidovudine and tenofovir. However, ritonavir boosted protease inhibitor with high plasma concentration have a high genetic barrier. For integrase inhibitors such as raltegravir, the emergence of resistance is certainly faster than the ritonavir boosted protease inhibitors, but seems slower and less systematic than for efavirenz or lamivudine. Many factors could influence the raltegravir resistance such as the level of viral load and replication duration, genetic polymorphism of HIV (integrase gene and other, viral subtype) and the plasma and/or intra- cellular raltegravir concentration.

Published

2010

23. [Association between variants of lipoprotein lipase and coronary heart disease in a Tunisian population]

Author

A, Jelassi, I, Jguirim, A, Slimani, M, Najah, K B, Hamda, F, Addad, M, Hassine, F, Maatouk, M, Varret, and M N, Slimane

Subjects

Male, Aspartic Acid, Tunisia, Genotype, Coronary Disease, Middle Aged, Polymorphism, Single Nucleotide, Lipoprotein Lipase, Genetics, Population, Amino Acid Substitution, Case-Control Studies, Serine, Humans, Female, Genetic Predisposition to Disease, Asparagine, Genetic Association Studies, Aged

Abstract

Coronary artery disease (CAD) is a complex multifactorial disease due to the interaction of multiple genes variations and environmental factors. Genetic variants of lipoprotein lipase (LPL), a key enzyme in the hydrolysis of triglyceride rich particles, may contribute to CAD. We analysed here the frequency of LPL variants (p.Asp9Asn, p.Asn291Ser and p.Ser447X) in a Tunisian population as well as their association with circulating lipid level and risk of CAD.LPL variations were investigated by PCR-RFLP and lipid parameters were measured in 135 patients and 109 controls.The frequency of the p.Asp9Asn variation was 10.37% in CAD patients versus 3.66% in controls. The frequency for the p.Ser447X variation was 8.8% in CAD patients versus 13.7% in controls. There was no significant association between these two variants and CAD. The p.Asn291Ser mutation variation was absent in this population. In healthy subjects, heterozygote carriers of the p.Asp9Asn substitution had a significant increase level of total cholesterol (4.2±0.9mmol/L vs 5.6±1.2mmol/L; P=0.01) and a decreased level of HDL-cholesterol (1.36±0.3mmol/L vs 0.93±0.1mmol/L; P=0.045).There was no significant association between genetic variants of the LPL gene and CAD in this Tunisian population. The very low frequency of the p.Asn291Ser variation may be an ethnic specificity of Tunisians.

Published

2010

24. Preliminary review of D222G amino acid substitution in the haemagglutinin of pandemic influenza A (H1N1) 2009 viruses

Subjects

Influenza A Virus, H1N1 Subtype, Amino Acid Substitution, Influenza, Human, Mutation, Humans, Hemagglutinin Glycoproteins, Influenza Virus

Published

2010

25. [McArdle disease (gycogenosis type V): analysis of clinical, biological and genetic features of five French patients]

Author

E, Delmont, S, Sacconi, J-L, Berge-Lefranc, R, Aquaron, C, Butori, and C, Desnuelle

Subjects

Adult, Male, Young Adult, Adolescent, Amino Acid Substitution, Mutation, Glycogen Phosphorylase, Muscle Form, Glycogen Storage Disease Type V, Humans, Female, France, Middle Aged, Creatine Kinase

Abstract

McArdle disease (glycogenosis type V) is an autosomal recessive metabolic myopathy. Defect in glycogen breakdown is due to mutations of the gene for myophosphorylase (PYGM). Among patients of the department, we searched for correlations between disease phenotype, biochemistry analysis of muscle samples and PYGM genotype.We included five patients whose muscle biopsy showed deposits of glycogen and negative histochemical staining for myophosphorylase.All patients exhibited exercise intolerance and high serum CK levels (mean 4400). Two of them had an acute renal insufficiency caused by rhabdomyolysis. One patient developed moderate late-onset muscle weakness of the proximal part of upper limbs. Muscle glycogen concentration was high (three times the normal). Myophosphorylase activity was undetectable in four muscle samples out of five. Two patients were homozygous and two other heterozygous for the R50X mutation of PYGM. The other one had a novel missense mutation S814N. Patients homozygous for R50X mutation had higher CK levels (8080 versus 1457, p=0.046), but disease severity and muscle glycogen concentrations were equivalent.Our patients had typical clinical and laboratory features of McArdle disease. Diagnosis was suggested by exercise intolerance with high CK levels. The R50X mutation was the most common (60% of the mutated alleles). We found no relationship between clinical severity, PYGM genotype and biochemistry analysis of muscle samples.

Published

2007

26. [Genotyping diagnosis of acyclovir resistant herpes simplex virus]

Author

E, Frobert, D, Thouvenot, B, Lina, and F, Morfin

Subjects

Amino Acid Substitution, Genotype, Drug Resistance, Viral, Mutation, Acyclovir, Humans, Simplexvirus, DNA-Directed DNA Polymerase, Herpesviridae Infections, Polymerase Chain Reaction, Thymidine Kinase, Immunity, Innate

Abstract

Herpes simplex virus resistant to acyclovir (ACV) is a major concern among immunocompromised patients. ACV resistance might be due to mutations located in one of the two genes involved in ACV mechanism of action, the thymidine kinase gene (TK, involved in 95% of the cases) and the DNA polymerase gene. TK gene mutations consist, in half of the cases, in nucleotide insertion or deletion, occurring most of the time in G or C homopolymers considered as hot spots. Half of the other cases involves nucleotide substitutions leading to amino acids substitutions. Studies of sensitive strains revealed a high degree of TK polymorphism, many mutations being not implied in ACV resistance. At the present time, resistance detection can be performed by phenotypic tests that require virus culture and results cannot be given to the physician before 7 to 10 days. Genotyping diagnosis performed directly from clinical samples would allow to detect resistance more rapidly, in order to switch quickly to an appropriate treatment by foscarnet or cidofovir.

Published

2007

27. [Biochemical and molecular diagnosis of Gaucher disease in Tunisia]

Author

A, Dandana, S, Ferchichi, S, Khedhiri, L, Chkioua, Z, Jaidane, K, Monastiri, S, Ben Khelifa, R, Ben Mansour, I, Maire, R, Froissart, V, Bonnet, S, Laradi, and A, Miled

Subjects

Adult, Male, Gaucher Disease, Tunisia, Adolescent, Amino Acid Substitution, Glucosylceramidase, Humans, Female, Exons, Middle Aged, Nuclear Family, Sequence Deletion

Abstract

Our study was carried out at a family from the Sahel (Tunisia). The father (index case) and his two children (son and daughter). The father beta-glucocerebrosidase (GCB) activity showing a deficit. These biochemical analyses are supplemented by molecular studies: enzymatic digestion and the direct sequencing. Two mutations were analysed, the p.Asn 370 Ser and the p.Leu 444 Pro. The DNA sequencing confirmed the presence of the homozygous genotype of this p.Asn 370 Ser in the father DNA and the heterozygous one in the two children DNA. It has no detection of the 55 pb deletion in exon 9 among all the specimens of DNA treated. The mutation p.Asn 370 Ser is associated with Gaucher disease type 1 correlated of a total absence of neurological involvements.

Published

2007

28. [Molecular analysis of the p.Asn 370 Ser mutation in Gaucher disease]

Author

A, Dandana, S, Ferchichi, S, Ben Khelifa, Z, Jaidane, K, Monastiri, L, Chkioua, I, Maire, R, Froissart, V, Bonnet, S, Laradi, and A, Miled

Subjects

Diagnosis, Differential, Gaucher Disease, Amino Acid Substitution, Mutation, Restriction Mapping, Serine, Glucosylceramidase, Humans, DNA, Exons, Asparagine, Polymerase Chain Reaction, DNA Primers

Abstract

Gaucher disease is one of the most prevalent lysosomal disorders. In this present study, we report a diagnostic strategy of type 1 Gaucher disease. The application of combined methods in molecular biology allowed us to analyse the p.Asn 370 Ser mutation. The affected individual activity is very low. First, we have to used the enzymatic digestion method. Then, we have to identified the mutation by the refractory mutation system technique using specific primers for the p.Asn 370 Ser mutation. These analyses are supplemented by the direct sequencing in order to seek and confirm this mutation. Finally, the absence of the 55 pb deletion in exon 9 among corroborated the presence of the homozygous genotype of this p.Asn 370 Ser in the patient DNA.

Published

2007

29. [Application of molecular modeling to new therapeutic cancer approaches]

Author

Olivier, Michielin

Subjects

Models, Molecular, Protein Conformation, Molecular Sequence Data, Receptors, Antigen, T-Cell, Membrane Proteins, T-Cell Antigen Receptor Specificity, Protein Engineering, Immunotherapy, Adoptive, Neoplasm Proteins, Structure-Activity Relationship, Amino Acid Substitution, Antigens, Neoplasm, Protein Interaction Mapping, Humans, Computer Simulation, Amino Acid Sequence, Melanoma, Sequence Alignment, Conserved Sequence, T-Lymphocytes, Cytotoxic

Abstract

Recent progress in the experimental determination of protein structures allow to understand, at a very detailed level, the molecular recognition mechanisms that are at the basis of the living matter. This level of understanding makes it possible to design rational therapeutic approaches, in which effectors molecules are adapted or created de novo to perform a given function. An example of such an approach is drug design, were small inhibitory molecules are designed using in silico simulations and tested in vitro. In this article, we present a similar approach to rationally optimize the sequence of killer T lymphocytes receptors to make them more efficient against melanoma cells. The architecture of this translational research project is presented together with its implications both at the level of basic research as well as in the clinics.

Published

2007

30. [Hereditary and acquired iron overload]

Author

Jean-Dominique, de Korwin

Subjects

Iron Overload, Amino Acid Substitution, Histocompatibility Antigens Class I, Mutation, Humans, Membrane Proteins, Hemochromatosis, Hemochromatosis Protein

Abstract

Since the discovery of HFE gene in 1996, considerable progress has been made concerning the iron-metabolism and its major abnormalities. Five types of hereditary hemochromatosis are actually known: type 1 (HFE gene), type 2A (HJV gene), type 2B (HAMP gene), type 3 (TfR2 gene), type 4 (SLC40A1 gene). The HFE C282Y +/+ mutation is responsible for the most frequent type of hemochromatosis in France. Various secondary causes can lead to iron-overload: associated genetic diseases, exogenous iron intake, thalassaemia and refractory anaemia, hepatic siderosis, alcoholic hepatitis, cutaneous porphyria and cirrhosis. The deleterious consequences of iron-overload are due to the interactions of the environmental factors. The role of HFE heterozygote mutations is still discussed. In clinical practice, the interpretation of a serum ferritin increase is a frequent problem that needs a careful evaluation based on the tranferrin saturation measurement. Significant increase of both these factors is in favour of an HFE C282Y +/+ hemochromatosis, after exclusion of a hepatocellular insufficiency or a refractory anaemia. Nevertheless, high ferritin is not always a marker of iron-overload. Thus, there are many disorders increasing the serum ferritin levels without iron overload : cytolysis (hepatic...), inflammatory or infectious syndromes, high alcohol intake, neoplasia... Looking for HFE mutations help to separate type 1 hemochromatosis from other conditions mainly hepatic siderosis (metabolic disorders). The identification of rare types of hemochromatosis (types 2-4) is only required in particular cases. The evaluation of the iron overload is now based on hepatic MRI determination rather than liver biopsy. Repeated phlebotomies remain the essential way to decrease the iron overload in HFE hemochromatosis and to prevent the occurrence of severe and irreversible complications (cirrhosis, arthropathies, cardiac failure, and diabetes). Because of the link established between the amount of iron-overload and the occurrence of complications and the mortality over-risk in HFE C282Y +/+ hemochromatosis, venesections must be started when serum ferritin is higher than 300 microg/l in man and 200 microg/l in woman, whatever the clinical manifestations are and obviously before the symptomatic phase of the disease.

Published

2007

31. [Molecular genetics of MTHFR: polymorphisms are not all benign]

Author

Daniel, Leclerc and Rima, Rozen

Subjects

Heart Defects, Congenital, Mice, Knockout, Abortion, Habitual, Fetal Growth Retardation, Polymorphism, Genetic, Apolipoprotein A-I, Cholesterol, HDL, Hyperhomocysteinemia, Mutation, Missense, Mice, Amino Acid Substitution, Gene Frequency, Pregnancy, Ethnicity, Genetics, Schizophrenia, Animals, Humans, Point Mutation, Abnormalities, Multiple, Female, Homocystinuria, Methylenetetrahydrofolate Reductase (NADPH2)

Abstract

Methylenetetrahydrofolate reductase (MTHFR) is a key regulatory enzyme in folate and homocysteine metabolism. Research performed during the past decade has clarified our understanding of MTHFR deficiencies that cause homocystinuria or mild hyperhomocysteinemia. Our cloning of the MTHFR coding sequence was initially followed by the identification of the first deleterious mutations in MTHFR, in patients with homocystinuria and marked hyperhomocysteinemia. Shortly thereafter, we identified the 677C--T variant and showed that it encoded a thermolabile enzyme with reduced activity. Currently, a total of 41 rare but deleterious mutations in MTHFR, as well as about 60 polymorphisms have been reported. The 677C--T (Ala222Val) variant has been particularly noteworthy since it has become recognized as the most common genetic cause of hyperhomocysteinemia. The disruption of homocysteine metabolism by this polymorphism influences risk for several complex disorders, including cardiovascular disease, neural tube defects and some cancers. We describe here the complex structure of the MTHFR gene, summarize the current state of knowledge on rare and common mutations in MTHFR and discuss some relevant findings in a mouse model for MTHFR deficiency.

Published

2007

32. [Phenotypic aspects of FKRP-linked muscular dystrophy type 2I in a series of eleven patients]

Author

H, Bourteel, T, Stojkovic, J M, Cuisset, C A, Maurage, P, Laforet, P, Richard, and P, Vermersch

Subjects

Adult, Cardiomyopathy, Dilated, Male, Adolescent, Genotype, Mutation, Missense, Proteins, Stroke Volume, Middle Aged, Magnetic Resonance Imaging, Phenotype, Sex Factors, Amino Acid Substitution, Muscular Dystrophies, Limb-Girdle, Child, Preschool, Humans, Point Mutation, Female, France, Pentosyltransferases, Age of Onset, Child, Muscle, Skeletal, Respiratory Insufficiency

Abstract

Limb-girdle muscular dystrophy type 2I (LGMD2I) is caused by mutations in the fukutin related protein gene (FKRP gene). This study tries to evaluate clinical, biological and mutational characteristics of LGMD2I.Eleven patients belonging to 9 families from the North of France were selected. We reported demographic data, and results of muscular testing, cardiac, and respiratory examination, as well as the histopathological features of muscle tissue and a genetic analysis of FKRP gene for each patient.There were 6 females and 5 males. Mean age at onset was 9.7 years old. Six had Duchenne like phenotype, 5 Becker like phenotype. Nine patients suffered from restrictive respiratory failure, two males had severe dilated cardiomyopathy. Ten patients had the common L276I mutation. Three mutations had not been previously identified: L322V, L489R and R275G heterozygous mutations associated with the L276I mutation.This study underlines inter and intra familial phenotypic variability in LGMD2I, preponderance of cardiomyopathy in males and restrictive respiratory insufficiency in female.

Published

2007

33. [Localised de novo dominant dystrophic epidermolysis bullosa]

Author

A-C, Bursztejn, A-L, Pinault, Y, Le Louarn, J-P, Lacour, A, Charlesworth, G, Meneguzzi, and F, Truchetet

Subjects

Diagnosis, Differential, Male, Collagen Type VII, Amino Acid Substitution, Child, Preschool, Humans, Female, Collagen, Exons, Epidermolysis Bullosa Dystrophica, Immunophenotyping, Pedigree, Skin

Abstract

Dystrophic epidermolysis bullosa is a hereditary heterogeneous blistering disease. Clinical examination and additional tests are not always sufficient to identify the subtype or mode of transmission. We describe a case of de novo dominant inherited dystrophic epidermolysis bullosa localised strictly to the knees.A 3-year-old boy presented symmetrical lesions on the anterior aspect of the knees since starting to walk. No nail, dental or mucous dystrophy was observed and the parents presented no clinical abnormalities. Optical microscopy, electron microscopy and immunofluorescence analysis suggested dystrophic epidermolysis bullosa. The genealogical tree allowed no distinction between the dominant de novo and mitis recessive forms. Genetic analysis identified a missense G 1776W mutation at exon 61 of gene COL 7A1 in the child's DNA but not the parents'.Dystrophic epidermolysis bullosa may present in generalized or localized forms and the disease may be inherited in either autosomal dominant or recessive mode. Genetic analysis shows mutations in COL 7A1. While the clinical features often allow different types to be distinguished when the parents do not have the disease (with the recessive forms being more severe), genetic analysis is essential to confirm the mode of inheritance. In the dominant forms, and more recently in recessive cases, glycine substitutions have been implicated, although the precise role of glycine substitution has yet to be clarified. Localised involvement of the skin alone, as seen in our case report, is very rare.Genetic analysis is important for genetic counselling and determination of risk of recurrence.

Published

2007

34. [Mutation of protein kinase JAK2 in polycythemia vera: new perspectives in physiopathology and therapy]

Author

I, Marie and F, Hervé

Subjects

Phenylalanine, Valine, Janus Kinase 2, Protein-Tyrosine Kinases, Piperazines, Pyrimidines, Amino Acid Substitution, Proto-Oncogene Proteins, Benzamides, Imatinib Mesylate, Humans, Point Mutation, Chromosomes, Human, Pair 9, Polycythemia Vera, Protein Kinase Inhibitors, Protein Kinases

Abstract

The pathogenic mechanisms of polyvythemia vera (PV) still remain unknown, although there is evidence that genetic parameters may play a role in the pathogenesis of the disease.In 2005, many international research groups have identified an acquired mutation in the Janus kinase (JAK2) gene of chromosome 9; the mutation is defined by a valine-to-phenylalanine substitution at amino acid position 617 (V617F) in the JAK2's pseudokinase domain. JAK2 V617F mutation has been found in as high as 65 to 97% of patients with PV. Both in vitro and in vivo functional studies have further indicated that JAK2 V617F mutation leads to dysregulation of kinase activity, explaining, in part, clinical and biochemical features of PV.These data suggest that JAK2 V617F mutation may be a novel diagnostic marker of PV. Moreover, JAK2 V617F mutation finding may permit promising therapeutic approaches in patients with PV, particularly tyrosine kinase inhibitors; preliminary series have, in fact, underscored the potential efficacy of imatinib mesylate in PV.

Published

2005

35. [Screening for HFE C282Y mutation at birth?]

Author

J, Rochette and E, Cadet

Subjects

Neonatal Screening, Amino Acid Substitution, Histocompatibility Antigens Class I, Infant, Newborn, Feasibility Studies, Humans, Membrane Proteins, Pilot Projects, Genetic Testing, Hemochromatosis, Hemochromatosis Protein

Published

2005

36. [Oculo-cerebro-renal Lowe syndrome: clinical, biochemical and molecular studies in a Moroccan patient]

Author

Chabaâ, Laïla, Monnier, Nicole, Dahri, Saloua, Jorio, M., Lunardi, Joël, Chabraoui, Layachi, Roux-Buisson, Nathalie, Laboratoire de biochimie, Hôpital d'enfants de Rabat, Laboratoire de biochimie et génétique moléculaire, CHU Grenoble, Service de pédiatrie, Ce travail a été réalisé en partie grâce au financement (NM) par le GIS-Maladies Rares et l'Association du Syndrome de Lowe., and Collaboration

Subjects

Male, MESH: Sequence Homology, Amino Acid, Molecular Sequence Data, MESH: Sequence Alignment, Mutation, Missense, MESH: Amino Acid Sequence, MESH: Base Sequence, Animals, Humans, MESH: Animals, [SDV.NEU] Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], Amino Acid Sequence, OCRL1, Sequence Deletion, MESH: Mutation, Missense, MESH: Humans, MESH: Molecular Sequence Data, Base Sequence, Sequence Homology, Amino Acid, syndrome de Lowe, Infant, MESH: Sequence Deletion, MESH: Amino Acid Substitution, MESH: Infant, MESH: Male, Phosphoric Monoester Hydrolases, Morocco, Oculocerebrorenal Syndrome, Amino Acid Substitution, MESH: Morocco, 5 biphosphate 5-phosphatase, MESH: Phosphoric Monoester Hydrolases, [SDV.NEU]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], inositol 4, mutation, Sequence Alignment, MESH: Oculocerebrorenal Syndrome

Abstract

International audience; The oculo-cerebro-renal syndrome of Lowe is a rare X-linked disorder, caused by the inositol biphosphate 5-phosphatase deficiency, localized to the Golgi complex. Several mutations were reported in patient's OCRL gene leading to enzyme deficiency. We report a Moroccan case of OCRL syndrome of Lowe with a neo mutation in exon 10. The patient aged of 19 months was referred to our medical centre because of a psychomotor retardation. He had a medical history of eye abnormalities including cataract and bilateral glaucoma, diagnosed when he was 5 weeks old. Cataract has been treated after chirurgical therapy but ocular hypertonia persisted. Physical examination revealed an axial hypotonia and walking difficulties. Laboratory tests revealed a moderate acidosis (20 mmol/L), a slight decrease of serum phosphate level (24 mg/L) and an increased serum phosphatase activity. Further studies showed mild proteinuria, urinary bicarbonates loosing and generalised hyperaminoaciduria. Based on both clinical and biological data, Lowe syndrome has been suggested. In this context, molecular investigation has been performed using dHPLC/sequencing techniques which allow identifying an original mutation c.776T>C (p.Phe259Ser), localized on the exon 10 of the OCRL gene. The mutation was not found in the probant's mother suggesting a neo mutation. Lowe syndrome is a rare hereditary X-linked disorder resulting from a variety of heterogeneous mutations of OCRL gene. Indeed, numerous mutations have been reported, variations were noted concerning their localization as well as their type. To our knowledge, this is the first report of the neo mutation c.776T>C of OCRL gene and the first published case report of the Lowe syndrome in a Moroccan patient.

Published

2005

37. [A recurrent mutation of the JAK2 gene in chronic myeloproliferative disorders]

Author

R, Berger

Subjects

Myeloproliferative Disorders, Amino Acid Substitution, Hematologic Neoplasms, Proto-Oncogene Proteins, Chronic Disease, Mutation, Humans, DNA, Janus Kinase 2, Protein-Tyrosine Kinases, Signal Transduction

Published

2005

38. [HFE hemochromatosis: pathogenic and diagnostic approach]

Author

P, Brissot, C, Le Lan, M B, Troadec, R, Lorho, M, Ropert, G, Lescoat, and O, Loréal

Subjects

Mice, Knockout, Duodenum, Iron, Macrophages, DNA Mutational Analysis, Histocompatibility Antigens Class I, Mutation, Missense, Transferrin, Membrane Proteins, Diagnosis, Differential, Mice, Phenotype, Amino Acid Substitution, Gene Expression Regulation, Hepcidins, Intestinal Absorption, Phagocytosis, Hepatocytes, Animals, Humans, Point Mutation, Chromosomes, Human, Pair 6, Hemochromatosis, Hemochromatosis Protein, Antimicrobial Cationic Peptides

Abstract

HFE hemochromatosis is the most frequent genetic iron overload disease. It is linked to the C282Y mutation of the HFE protein, protein encoded by the HFE gene, which is located on chromosome 6. The mechanisms accounting for iron excess are not only digestive hyperabsorption of iron but also excessive recycling of macrophagic iron coming from erythrophagocytosis and secreted into the blood. Both mechanisms are linked to an HFE-related hepatic failure in producing hepcidin, a key hormone of body iron regulation. The marked phenotypic variability of C282Y homozygosity expression is likely related to both genetic and environmental factors. The HFE gene discovery has rendered non invasive the positive diagnostic of HFE hemochromatosis, which is now based first on an increased level of plasma transferrin saturation leading to the request of the HFE mutation. Then, hepatic MRI is a reliable method to quantify iron overload. The HFE gene discovery has also paved the road of an enlarged field of differential diagnoses corresponding to novel entities of non-HFE related genetic iron overload syndromes.

Published

2005

39. [Search for the T790M mutation: The need to persevere].

Author

Bourien H, Lespagnol A, Prigent A, Leveiller G, Lena H, Ricordel C, and Corre R

Subjects

Aged, Amino Acid Substitution, Biopsy, Carcinoma, Non-Small-Cell Lung drug therapy, ErbB Receptors genetics, Female, Humans, Lung Neoplasms drug therapy, Male, Methionine genetics, Middle Aged, Protein Kinase Inhibitors therapeutic use, Threonine genetics, Time Factors, Carcinoma, Non-Small-Cell Lung genetics, DNA Mutational Analysis, Drug Resistance, Neoplasm genetics, Lung Neoplasms genetics, Mutation, Missense

Abstract

In cases of advanced EGFR mutation-positive non-small cell lung cancer, first or second generation EGFR-tyrosine kinase inhibitors (TKI-EGFR 1G or TKI-EGFR 2G) are recommended as first line treatment. Inexorably, progressive disease occurs and, in 50-60% of the cases, is secondary to a T790M resistant mutation. The prescription of osimertinib (TKI-EGFR3G) in second line is dependent on identification of the T790M mutation. We report 7 cases in which the identification of the T790M mutation required repeated analyses of cell free DNA and/or biopsies over a period of time. In some cases, a positive result was obtained a long time after progressive disease had been diagnosed during treatment with first or second generation EGFR-TKI. We discuss here the different modalities of screening for the T790M mutation and we encourage persevering in this search when no alternative mechanism of resistance has been identified., (Copyright © 2018 SPLF. Published by Elsevier Masson SAS. All rights reserved.)

Published

2018

40. [21 hydroxylase deficiency: new strategies emerging from molecular studies]

Author

Y, Morel, V, Tardy, J-M, Costa, M G, Forest, and M, David

Subjects

Adrenal Hyperplasia, Congenital, Genetic Carrier Screening, Genes, Recessive, Genetic Counseling, Virilism, Dexamethasone, Fetal Diseases, Amino Acid Substitution, Pregnancy, Prenatal Diagnosis, Humans, Point Mutation, Chromosomes, Human, Pair 6, Female, Steroid 21-Hydroxylase, Case Management

Published

2004

41. [Apert's syndrome: a case report]

Author

C, Doutetien, A, Laleye, S, Tchabi, O, Biaou, R, Lawani, J, Deguenon, R, Darboux, D, Gnamey, and S K, Bassabi

Subjects

Adolescent, Hemoglobin, Sickle, Ectropion, Mutation, Missense, Receptor Protein-Tyrosine Kinases, Acrocephalosyndactylia, Receptors, Fibroblast Growth Factor, Sickle Cell Trait, Amino Acid Substitution, Exophthalmos, Humans, Point Mutation, Female, Psychomotor Disorders, Receptor, Fibroblast Growth Factor, Type 2

Abstract

Apert's syndrome is a type of acrocephalosyndactylia that is from part of the great group of craniofacial synostoses. It is characterized by craniofacial dysmorphia and syndactylia on hands and feet, which differentiates it from Crouzon's disease. It is a rare affection that is often transmitted through an autosome dominant mode, but sporadic cases exist. We report the case of a 15-year-old girl who presented characteristic clinical signs of Apert's syndrome with normal karyotype without parental consanguinity. The Ser 252 Trp mutation of the FGFR2 gene was found, confirming the molecular diagnosis. This study illustrates the severity of ocular and neurological problems of untreated Apert's syndrome. The presence of hemoglobinopathy (Hb AS) is also a mark of its originality.

Published

2003

42. [Hyperhomocysteinemia: an independent risk factor or a simple marker of vascular disease? 2. Epidemiological data]

Author

J-C, Guilland, A, Favier, G, Potier de Courcy, P, Galan, and S, Hercberg

Subjects

Oxidoreductases Acting on CH-NH Group Donors, Polymorphism, Genetic, Arteriosclerosis, Hyperhomocysteinemia, Mutation, Missense, Cystathionine beta-Synthase, Confounding Factors, Epidemiologic, United States, Europe, Amino Acid Substitution, Meta-Analysis as Topic, Risk Factors, Case-Control Studies, Humans, Thrombophilia, Homocystinuria, Prospective Studies, Vascular Diseases, Biomarkers, Methylenetetrahydrofolate Reductase (NADPH2)

Abstract

Elevated plasma total homocysteine (tHcy) is considered as a risk factor for occlusive cardiovascular disease (CVD). This concept is based on the observations of premature vascular disease in patients with homocystinuria and on the association between tHcy and increased risk of CVD in prospective studies. However, some observations have raised questions about tHcy as a risk factor. First, low risk population based prospective studies tend to indicate a weak association or no association between tHcy and CVD. Second, several traditional risk factors for CVD are associated with tHcy and may confound the relation between tHcy and CVD. Third, the C667T transition of the methylenetetrahydrofolate reductase causes a moderate increase in tHcy but no or only minor increased CVD risk. Thus, only placebo-controlled intervention studies with tHcy-lowering B-vitamins and clinical endpoints can provide additional valid arguments for the debate over whether tHcy is a causal CVD risk factor.

Published

2003

43. [The active site of human glucocerebrosidase: structural predictions and experimental validations]

Author

Sylvie, Fabrega, Patrick, Durand, Jean-Paul, Mornon, and Pierre, Lehn

Subjects

Models, Molecular, Protein Folding, Binding Sites, Glycosylation, Sequence Homology, Amino Acid, Protein Conformation, Recombinant Fusion Proteins, Molecular Sequence Data, Glutamic Acid, Protein Structure, Tertiary, Mice, Structure-Activity Relationship, Amino Acid Substitution, Catalytic Domain, Animals, Glucosylceramidase, Humans, Point Mutation, Amino Acid Sequence, Hydrophobic and Hydrophilic Interactions, Protein Processing, Post-Translational, Sequence Alignment

Abstract

Gaucher disease is a lysosomal storage disorder caused by a deficiency in glucocerebrosidase which cleaves the beta-glucosidic linkage of glucosylceramide, a normal intermediate in glycolipid metabolism. Glucocerebrosidase belongs to the clan GH-A of glycoside hydrolases, a large group of enzymes which function with retention of the anomeric configuration at the hydrolysis site. Accurate three-dimensional (3D) structure data for glucocerebrosidase should help to better understand the molecular bases of Gaucher disease. As such 3D structure data were not available, we used the two-dimensional hydrophobic cluster analysis (HCA) method to make structure predictions for the catalytic domains of clan GH-A glycoside hydrolases. We found that all the enzymes of clan GH-A may share a similar catalytic domain consisting of an (alpha/beta)8 barrel with the critical acid/base and nucleophile residues located at the C-terminal ends of strands beta 4 and beta 7, respectively. In the case of glucocerebrosidase, Glu 235 was predicted to be the putative acid/base catalyst whereas the nucleophile was located at Glu 340. Next, in order to obtain experimental evidence supporting these HCA-based predictions, we used retroviral vectors to express, in murine null cells, E235A and E340A mutant proteins, in which alanine residues unable to participate in the enzymatic reaction replace the presumed critical glutamic acid residues. Both mutants were found to be catalytically inactive although they were correctly folded/processed and sorted to the lysosome. Thus, Glu 235 and Glu 340 do indeed play key roles in the active site of human glucocerebrosidase as predicted by the HCA analysis. In a broader perspective, our work points out that bioinformatics approaches may be highly useful for generating structure-function predictions based on sequence-structure interrelationships, especially in the context of a rapid increase in protein sequence information through genome sequencing.

Published

2002

44. [Fabry's disease (alpha-galactosidase-A deficiency): physiopathology, clinical signs, and genetic aspects]

Author

Dominique Paul, Germain

Subjects

Male, X Chromosome, Eye Diseases, Genotype, Genetic Carrier Screening, Trihexosylceramides, Infant, Genetic Counseling, Kidney Transplantation, Amino Acid Substitution, Cardiovascular Diseases, Pregnancy, Prenatal Diagnosis, alpha-Galactosidase, Mutation, Disease Progression, Fabry Disease, Humans, Kidney Failure, Chronic, Female

Abstract

Fabry disease (FD, OMIM 301500) is an X-linked inherited disorder of metabolism due to mutations in the gene encoding alpha-galactosidase A, a lysosomal enzyme. The enzymatic defect leads to the accumulation of neutral glycosphingolipids throughout the body, particularly within endothelial cells. Resulting narrowing and tortuosity of small blood vessels lead to tissue ischaemia and infarction. Inability to prevent the progression of glycosphingolipid deposition causes significant morbidity (acroparesthesia, angiokeratoma, autonomic dysfunction, cardiomyopathy and deafness), and mortality from early onset strokes, heart attack and renal failure in adulthood. Demonstration of alpha-galactosidase A deficiency in leukocytes or plasma is the definitive method for the diagnosis of affected hemizygous males. Most heterozygotes present with a cardiac, renal or neurological symptomatology, although to a lesser extent than what is observed in hemizygotes. Due to random X-chromosomal inactivation, enzymatic detection of carriers is often inconclusive. Molecular testing of possible carriers is therefore mandatory for accurate genetic counselling. The GLA gene has been cloned and more than 200 mutations have been identified. Medical management is symptomatic and consists of partial pain relief with analgesic drugs (gabapentin, carbamazepine), whereas renal transplantation or dialysis is available for patients experiencing end-stage renal failure. However, the ability to produce high doses of alpha-galactosidase A in vitro has opened the way to clinical studies and enzyme replacement therapy has recently been validated as a therapeutic agent for FD patients in clinical trials. Long term safety and efficacy of replacement therapy are currently being investigated.

Published

2002

45. [The acetylator polymorphism in a Khmer population: clinical consequences]

Author

Y C, Bechtel, P R, Bechtel, H, Lelouët, H, Choisy, and N R, Dy

Subjects

Xanthine Oxidase, Arylamine N-Acetyltransferase, DNA Mutational Analysis, Antitubercular Agents, Drug Resistance, Polymerase Chain Reaction, White People, Asian People, Gene Frequency, Heterocyclic Compounds, Caffeine, Ethnicity, Isoniazid, Humans, Tuberculosis, Uracil, Alleles, Biotransformation, Polymorphism, Genetic, Acetylation, Uric Acid, Phenotype, Amino Acid Substitution, Xanthines, Inactivation, Metabolic, Carcinogens, Cambodia, Chromosomes, Human, Pair 8

Abstract

The great variability of slow acetylator (SA) and/or rapid acetylator (RA) frequency is mainly due to ethnic-racial origin. Using the urinary elimination ratio of three metabolites of caffeine--acetylamino formylamino methyluracil (AFMU) to AFMU + 1-methyl urate (1U) + 1-methyl xanthine (1X)--we settled the acetylation phenotype in 54 independent subjects of Khmer and 70 independent subjects of Caucasian origin. Using DNA from peripheral leucocytes, we determined by PCR, in 32 Khmer and 122 Caucasian subjects, the frequencies of wild-type alleles (NAT-2 *4) and of mutated alleles (NAT-2 *5A, *6A, *7A). The frequency of SA was respectively 28 per cent and 61 per cent in Khmer and Caucasian subjects. The antimode of the distribution of the ratio was different in the two populations: 0.07 in Khmers and 0.18 in Caucasians showing a reduced acetylation capacity in the Khmer population in spite of a higher frequency of RA. The frequencies of alleles were also different between the two populations. Between Khmers and Caucasians respectively: *4: 48.4-23.8 per cent *5A: 15.6-44.2 per cent. *6A: 29.7-32.0 per cent. *7A: 6.3-0 per cent. These differences might be taken into account to define a therapeutic strategy in the treatment of tuberculosis by isoniazide.

Published

2001

46. [Genetic testing for cystic fibrosis: evaluation of the Elucigene CF20 kit in blood and buccal cells]

Author

D, Feldmann, C, Guittard, M D, Georges, C, Houdayer, C, Magnier, M, Claustres, and R, Couderc

Subjects

Amino Acid Substitution, Cystic Fibrosis, Mutation, Mouth Mucosa, Cystic Fibrosis Transmembrane Conductance Regulator, Humans, Reproducibility of Results, DNA, Genetic Testing, Reagent Kits, Diagnostic, Laboratories, White People, Sequence Deletion

Abstract

Routine determination of mutations in cystic fibrosis requires accurate, rapid, reliable and low-cost methods, permitting the simultaneous detection of multiple mutations. The Elucigene CF20 kit developped by Cellmark Diagnostics, uses multiplex ARMS, which allows the screening for 20 CFTR gene mutations (deltaF508, G542X, N1303K, 1717-1GA, G551D, W1282X, R553X, deltaI507, 1078delT, 2183AAG, 3849+10kbCT, R1162X, 621+1GT, R334W, R347P, 3659delC, R117H, S1251N, E60X, A455E ) in a work day without specific instrumentation. The kit distinguishes between homozygotes and heterozygotes for deltaF508, but not for rare mutations. The kit detects from 68 to 92% of defective alleles in Caucasians. We evaluate the kit in a blind study in two independent laboratories. Thirty blood samples and thirty mouthwash samples from CF patients, carriers and unaffected individuals were analysed by the Elucigene CF20 kit. All the samples were previously analysed by denaturing gradient gel electrophoresis and sequencing. The Elucigene CF20 kit consists of three multiplexes. Each mutiplex contains ARMS specific primers for six to eight mutations and two control reactions. The absence of the upper control fragment indicates that a repeat test is required. We demonstrated a first time amplification rate of 98.3%: of the 60 samples tested, one required a reamplification. Results compared with the reference method demonstrated that in all cases where one or more of the 20 mutations detected by the kit were present in the test set, the kit accurately identified them. Reproducibility was assessed by repeating the analysis of a blood and mouthwash sample five times. Cross reactivity between R117C and R117H, R117P and R117H, R347P and R347H, deltaI507 and deltaF508, G551D and R553X were evaluated. Only a cross reactivity between R347P and R347H was observed. The kit is specially useful for first line study of patients and carrier identification.

Published

2001

47. [Fabry disease. Clinical and genetic aspects. Therapeutic perspectives]

Author

D P, Germain

Subjects

Male, X Chromosome, Amino Acid Substitution, alpha-Galactosidase, Mutation, Mutation, Missense, Fabry Disease, Humans, Renal Insufficiency

Abstract

This review presents the clinical and genetic aspects of Fabry disease, along with recent advances in research.Fabry disease is an X-linked inborn error of metabolism due to a deficient activity of the lysosomal enzyme alpha-galactosidase A. The enzymatic defect leads to the systemic accumulation of neutral glycosphingolipids in plasma and tissues. Clinical manifestations in affected hemizygous males are primarily due to progressive disease of small vessels, including angiokeratoma, autonomic dysfunction, and lifelong debilitating pain. Renal failure and vasculopathy of the heart and brain lead to early demise in adulthood. Demonstration of alpha-galactosidase A deficiency in leukocytes or plasma is the definitive method for the diagnosis of affected hemizygous males. Most female carriers are clinically symptomatic, they may present isolated acroparesthesia, cardiac symptoms, or the characteristic benign corneal dystrophy. Due to random X-chromosomal inactivation, enzymatic detection of carriers is often inconclusive. A reliable molecular test for detection of heterozygosity is therefore highly desirable for accurate genetic counselling. The GLA gene has been mapped to chromosome Xq22, and cloned. Several studies have shown the molecular heterogeneity of the disease. Currently, no standard treatment exists for Fabry disease. Symptomatic treatment is provided as appropriate. In addition, renal transplantation or dialysis is available for patients experiencing end-stage renal failure.The ability to produce high doses of recombinant alpha-galactosidase A in vitro has opened the way to preclinical studies in the mouse model and led to the development of the first clinical trials with enzyme replacement therapy in patients with Fabry disease.

Published

2001

48. [Hereditary hemochromatosis]

Author

S, Durupt, I, Durieu, R, Nové-Josserand, L, Bencharif, H, Rousset, and D, Vital Durand

Subjects

Amino Acid Substitution, HLA Antigens, Histocompatibility Antigens Class I, Prevalence, Humans, Membrane Proteins, Hemochromatosis, Hemochromatosis Protein, White People

Abstract

Hereditary hemochromatosis is a fairly common disease in the Caucasian population, with a prevalence estimated at between 1.5 to 3/1,000 inhabitants. Over the past few years, its symptomatology has altered; at present, its clinical aspect with diabetes mellitus, cirrhosis, and darker skin pigmentation only constitutes 10% of new cases of this disease.In 1996, the discovery of the C282Y mutation in the HFE gene radically altered the diagnostic approach to hereditary hemochromatosis. At present, any patient admitted with an isolated case of asthenia, or with arthralgia or hypertransaminasemia should be examined via transferrin-saturation testing: if the transferrin saturation coefficient is45%, then the presence of the C282Y mutation should be investigated to confirm the diagnosis of hemochromatosis. A liver biopsy is no longer necessary to establish the diagnosis, but this is still useful in cases of possible cirrhosis, which is the main risk factor for hepatocellular carcinoma. Phlebotomy remains the sole recommended treatment, and should be undertaken in a case-specific manner. Family screening should be carried out for all first-degree relatives for every new case that is diagnosed.The discovery of the HFE gene has permitted hereditary hemochromatosis to be easily differentiated from other forms of hepatic iron overload including a new syndrome, dysmotabolic hepatosiderosis. Casos of homozygotic C282Y without hepatic iron overload have been described, but the clinical outcome of some of these cases requires further study, and adds to the controversy on whether systematic population screening should be made available.

Published

2000

49. [Molecular basis and structure-activity relationships of the Duffy blood group antigens: chemokine and Plasmodium vivax receptors]

Author

C, Tournamille

Subjects

Models, Molecular, Erythrocytes, Genotype, Protein Conformation, Recombinant Fusion Proteins, Protozoan Proteins, Antigens, Protozoan, Nerve Tissue Proteins, Receptors, Cell Surface, Polymerase Chain Reaction, Purkinje Cells, Structure-Activity Relationship, Gene Frequency, Chlorocebus aethiops, Animals, Humans, Blood Transfusion, Alleles, Cells, Cultured, Polymorphism, Genetic, Racial Groups, Protein Structure, Tertiary, Phenotype, Amino Acid Substitution, Chromosomes, Human, Pair 1, Organ Specificity, Blood Group Incompatibility, Chemokines, CC, Receptors, Chemokine, Endothelium, Vascular, Carrier Proteins, Duffy Blood-Group System, Plasmodium vivax, Chemokines, CXC, Polymorphism, Restriction Fragment Length

Abstract

Duffy blood group antigens are of major interest in clinical medicine as they are not only involved in blood transfusion risks and occasionally in neonatal hemolytic disease, but also in the invasion of red blood cells by the hemoparasitic Plasmodium vivax. The FY locus maps to chromosome 1q22-q23, and is composed of 4 alleles: FY*A and FY*B (coding for the Fya and Fyb antigens, respectively), FY*X and FY*Fy. The Duffy antigens are carried by a 336 amino-acid glycoprotein named the Duffy Antigen/Receptor for Chemokines (DARC) that can bind with high affinity selected members of the CXC and CC classes of chemokines. Today, the genetic bases of the Duffy system have been characterized. The identification of the polymorphisms associated with the 4 alleles FY*A, FY*B, FY*Fy and FY*X has led to the development of a complete genotyping of the Duffy system by PCR, which increases the safety and lessens the risk of blood transfusion, and is useful in determining feto-maternal incompatibilities and in genetic filiation analyses. DARC is not solely expressed in erythroid cells: the same polypeptide isoform is found on the surface of endothelial cells of post-capillary venules throughout the body and also on the surface of Purkinje cells in the cerebellum, although it is encoded by different RNA messengers in each case, i.e., 1.35 and 7.5 kb, respectively. The preliminary analyses of receptor-ligand interaction have shown the existence of a chemokine-binding pocket defined by the close proximity of the first and fourth transmembrane domains of the DARC protein, and also by the importance of the N-terminal extracellular region for the binding of Plasmodium vivax merozoites.

Published

2000

50. [Corticosteroid hormones: mechanisms involved in the recognition of aldosterone by mineralocorticoid receptors]

Author

C, Hellal-Levy, J, Fagart, A, Souque, and M E, Rafestin-Oblin

Subjects

Binding Sites, Receptors, Mineralocorticoid, Amino Acid Substitution, Hydrocortisone, Protein Conformation, Mineralocorticoids, Humans, Hydrogen Bonding, Aldosterone

Abstract

Aldosterone and cortisol, the major mineralocorticoid and glucocorticoid hormones in humans, are structurally very closed. Both hormones bind to the mineralocorticoid receptor (MR) with the same affinity. Nevertheless MR is preferentially activated by aldosterone, suggesting that the binding of these two hormones to MR involved some distinct contacts. We constructed a tridimensional model of the ligand-binding domain of the human MR, by taking as a template the structural data of the retinoid receptor associated with its ligand. The MR model allowed the identification of several residues involved in the interaction with aldosterone and cortisol. The residues Gln 776 and Arg 817 make hydrogen bonds with the 3-keto function and the residue Asn 770 with the C21-hydroxyl group. Analyses of the wild type and mutant MRs activities in response to corticosteroids bearing hydroxyl groups at various steroid skeleton position led to the following conclusions: 1) the interaction between the residue Asn 770 and the C21-hydroxyl group of corticosteroids is determinant for stabilizing the active MR conformation and 2) the stability of this conformation is enhanced by the 11-18 hemiketal group of aldosterone whereas it is decreased by the 11 beta- and 17 alpha-hydroxyl groups of cortisol. These results are discussed in the light of a model for the MR activation process.

Published

2000