110 results on '"Giurgea, Irina"'
Search Results
102. Overgrowth and trisomy 15q26.1-qter including the IGF1 receptor gene: report of two families and review of the literature
- Author
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Faivre, Laurence, primary, Gosset, Philippe, additional, Cormier-Daire, Valérie, additional, Odent, Sylvie, additional, Amiel, Jeanne, additional, Giurgea, Irina, additional, Nassogne, Marie-Cécile, additional, Pasquier, Laurent, additional, Munnich, Arnold, additional, Romana, Serge, additional, Prieur, Marguerite, additional, Vekemans, Michel, additional, de Blois, Marie-Christine, additional, and Turleau, Catherine, additional
- Published
- 2002
- Full Text
- View/download PDF
103. Somatic Mosaic NLRP3Mutations and Inflammasome Activation in Late-Onset Chronic Urticaria
- Author
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Assrawi, Eman, Louvrier, Camille, Lepelletier, Clémence, Georgin-Lavialle, Sophie, Bouaziz, Jean-David, Awad, Fawaz, Moinet, Florence, Moguelet, Philippe, Vignon-Pennamen, Marie Dominique, Piterboth, William, Jumeau, Claire, Cobret, Laetitia, El Khouri, Elma, Copin, Bruno, Duquesnoy, Philippe, Legendre, Marie, Grateau, Gilles, Karabina, Sonia A., Amselem, Serge, and Giurgea, Irina
- Abstract
Chronic urticaria is a common skin disorder with heterogeneous causes. In the absence of physical triggers, chronic urticarial rash is called idiopathic or spontaneous. The objective of this study was to identify the molecular and cellular bases of a disease condition displayed by two unrelated patients aged over 60 years who presented for two decades with a chronic urticaria resistant to standard therapy that occurred in the context of systemic inflammation not triggered by cold. In both patients, a targeted sequencing approach using a next generation technology identified somatic mosaic mutations in NLRP3, a gene encoding a key inflammasome component. The study of several of both patients’ cell types showed that, despite the late onset of the disease, NLRP3mutations were not found to be restricted to myelomonocytic cells. Rather, the data obtained strongly suggested that the mutational event occurred very early, during embryonic development. As shown by functional studies, the identified mutations—an in-frame deletion and a recurrent NLRP3missense mutation—have a gain-of-function effect on NLRP3-inflammasome activation. Consistently, a complete remission was obtained in both patients with anti–IL-1 receptor antagonists. This study unveils that in late-onset chronic urticaria, the search for autoinflammatory markers and somatic mosaic NLRP3mutations may have important diagnostic and therapeutic consequences.
- Published
- 2020
- Full Text
- View/download PDF
104. French practical guidelines for the diagnosis and management of AA amyloidosis.
- Author
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Georgin-Lavialle S, Savey L, Buob D, Bastard JP, Fellahi S, Karras A, Boffa JJ, Grateau G, Audard V, Bridoux F, Damade R, Deshayes S, Giurgea I, Granel B, Hachulla E, Hot A, Jaccard A, Knebelmann B, Marciano S, Pelcot F, Sarrabay G, Boursier G, Sellam J, Terre A, and Bourguiba R
- Subjects
- Male, Humans, Female, Serum Amyloid A Protein metabolism, Serum Amyloid A Protein therapeutic use, Chronic Disease, Amyloidosis diagnosis, Amyloidosis etiology, Amyloidosis therapy, Familial Mediterranean Fever complications, Renal Insufficiency complications
- Abstract
AA amyloidosis is secondary to the deposit of excess insoluble Serum Amyloid A (SAA) protein fibrils. AA amyloidosis complicates chronic inflammatory diseases, especially chronic inflammatory rheumatisms such as rheumatoid arthritis and spondyloarthritis; chronic infections such as tuberculosis, bronchectasia, chronic inflammatory bowel diseases such as Crohn's disease; and auto-inflammatory diseases including familial Mediterranean fever. This work consists of the French guidelines for the diagnosis workup and treatment of AA amyloidosis. We estimate in France between 500 and 700 cases in the whole French population, affecting both men and women. The most frequent organ impaired is kidney which usually manifests by oedemas of the lower extremities, proteinuria, and/or renal failure. Patients are usually tired and can display digestive features anf thyroid goiter. The diagnosis of AA amyloidosis is based on detection of amyloid deposits on a biopsy using Congo Red staining with a characteristic green birefringence in polarized light. Immunohistochemical analysis with an antibody directed against Serum Amyloid A protein is essential to confirm the diagnosis of AA amyloidosis. Peripheral inflammatory biomarkers can be measured such as C Reactive protein and SAA. We propose an algorithm to guide the etiological diagnosis of AA amyloidosis. The treatement relies on the etiologic treatment of the undelying chronic inflammatory disease to decrease and/or normalize Serum Amyloid A protein concentration in order to stabilize amyloidosis. In case of renal failure, dialysis or even a kidney transplant can be porposed. Nowadays, there is currently no specific treatment for AA amyloidosis deposits which constitutes a therapeutic challenge for the future., (Copyright © 2022 The Author(s). Published by Elsevier Masson SAS.. All rights reserved.)
- Published
- 2023
- Full Text
- View/download PDF
105. The recurrent TCF4 missense variant p.(Arg389Cys) causes a neurodevelopmental disorder overlapping with but not typical for Pitt-Hopkins syndrome.
- Author
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Popp B, Bienvenu T, Giurgea I, Metreau J, Kraus C, Reis A, Fischer J, Bralo MP, Tenorio-Castaño J, Lapunzina P, Almoguera B, Lopez-Grondona F, Sticht H, and Zweier C
- Subjects
- Humans, Transcription Factor 4 genetics, Facies, Hyperventilation diagnosis, Intellectual Disability genetics, Epilepsy
- Abstract
TCF4 haploinsufficiency by deletions, truncating variants or loss-of-function missense variants within the DNA-binding and protein interacting bHLH domain causes Pitt-Hopkins syndrome (PTHS). This neurodevelopmental disorder (NDD) is characterized by severe intellectual disability (ID), epilepsy, hyperbreathing and a typical facial gestalt. Only few aberrations of the N-terminus of TCF4 were associated with milder or atypical phenotypes. By personal communication and searching databases we assembled six cases with the novel, recurrent, de novo missense variant c.1165C > T, p.(Arg389Cys) in TCF4. This variant was identified by diagnostic exome or panel sequencing and is located upstream of the bHLH domain. All six individuals presented with moderate to severe ID with language impairment. Microcephaly occurred in two individuals, epilepsy only in one, and no breathing anomalies or myopia were reported. Facial gestalt showed some aspects of PTHS but was rather non-specific in most individuals. Interestingly, the variant is located within the AD2 activation domain next to a highly conserved coactivator-recruitment motif and might alter interaction with coactivator proteins independently from the bHLH domain. Our findings of a recurrent missense variant outside the bHLH domain in six individuals with an ID phenotype overlapping with but not typical for PTHS delineate a novel genotype-phenotype correlation for TCF4-related NDDs., (© 2022 The Authors. Clinical Genetics published by John Wiley & Sons Ltd.)
- Published
- 2022
- Full Text
- View/download PDF
106. Mowat Wilson syndrome and Hirschsprung disease: a retrospective study on functional outcomes.
- Author
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Dagorno C, Pio L, Capri Y, Ali L, Giurgea I, Qoshe L, Morcrette G, Julien-Marsollier F, Sommet J, Chomton M, Berrebi D, and Bonnard A
- Subjects
- DNA Mutational Analysis, Facies, Female, Follow-Up Studies, Hirschsprung Disease genetics, Hirschsprung Disease surgery, Humans, Infant, Newborn, Intellectual Disability genetics, Intellectual Disability surgery, Male, Microcephaly genetics, Microcephaly surgery, Mutation, Retrospective Studies, Treatment Outcome, Zinc Finger E-box Binding Homeobox 2 genetics, Zinc Finger E-box Binding Homeobox 2 metabolism, Zinc Fingers, Defecation physiology, Digestive System Surgical Procedures methods, Forecasting, Hirschsprung Disease physiopathology, Intellectual Disability physiopathology, Microcephaly physiopathology
- Abstract
Aim of the Study: Mowat Wilson syndrome (MWS) is a complex genetic disorder due to mutation or deletion of the ZEB2 gene (ZFHX1B), including multiple clinical features. Hirschsprung disease is associated with this syndrome with a prevalence between 43 and 57%. The aim of this study was to demonstrate the severe outcomes and the high complication rates in children with MWS, focusing on their complicated follow-up., Methods: A retrospective comparative study was conducted on patients referred to Robert-Debré Children's Hospital for MWS from 2003 to 2018. Multidisciplinary follow-up was carried out by surgeons, geneticists, gastroenterologists, and neurologists. Data regarding patient characteristics, surgical management, postoperative complications, and functional outcomes were collected., Results: Over this period of 15 years, 23 patients were diagnosed with MWS. Hirschsprung disease was associated with 10 of them (43%). Of these cases, two patients had recto-sigmoïd aganglionosis (20%), three had aganglionic segment extension to the left colic angle (30%), two to the right colic angle (20%), and three to the whole colon (30%). The median follow-up was 8.5 years (2 months-15 years). All patients had seizures and intellectual disability. Six children (60%) presented with cardiac defects. At the last follow-up, three patients still had a stoma diversion and 7 (70%) were fed orally. One patient died during the first months. Eight (80%) of these children required a second surgery due to complications. At the last follow-up, three patients reported episodes of abdominal bloating (42%), one recurrent treated constipation (14.3%), and one soiling (14.3%). Genetic analysis identified three patients with heterozygous deletions, three with codon mutations, and three with frameshift mutations., Conclusions: MWS associated with Hirschsprung disease has a high rate of immediate surgical complications but some patients may achieve bowel function comparable with non-syndromic HD patients. A multidisciplinary follow-up is required for these patients., Level of Evidence: Retrospective observational single cohort study, Level 3.
- Published
- 2020
- Full Text
- View/download PDF
107. Somatic Mosaic NLRP3 Mutations and Inflammasome Activation in Late-Onset Chronic Urticaria.
- Author
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Assrawi E, Louvrier C, Lepelletier C, Georgin-Lavialle S, Bouaziz JD, Awad F, Moinet F, Moguelet P, Vignon-Pennamen MD, Piterboth W, Jumeau C, Cobret L, El Khouri E, Copin B, Duquesnoy P, Legendre M, Grateau G, Karabina SA, Amselem S, and Giurgea I
- Subjects
- Aged, Chronic Urticaria metabolism, DNA Mutational Analysis, Female, Humans, Inflammasomes metabolism, Male, NLR Family, Pyrin Domain-Containing 3 Protein metabolism, Chronic Urticaria genetics, DNA genetics, Inflammasomes genetics, Mutation, NLR Family, Pyrin Domain-Containing 3 Protein genetics
- Abstract
Chronic urticaria is a common skin disorder with heterogeneous causes. In the absence of physical triggers, chronic urticarial rash is called idiopathic or spontaneous. The objective of this study was to identify the molecular and cellular bases of a disease condition displayed by two unrelated patients aged over 60 years who presented for two decades with a chronic urticaria resistant to standard therapy that occurred in the context of systemic inflammation not triggered by cold. In both patients, a targeted sequencing approach using a next generation technology identified somatic mosaic mutations in NLRP3, a gene encoding a key inflammasome component. The study of several of both patients' cell types showed that, despite the late onset of the disease, NLRP3 mutations were not found to be restricted to myelomonocytic cells. Rather, the data obtained strongly suggested that the mutational event occurred very early, during embryonic development. As shown by functional studies, the identified mutations-an in-frame deletion and a recurrent NLRP3 missense mutation-have a gain-of-function effect on NLRP3-inflammasome activation. Consistently, a complete remission was obtained in both patients with anti-IL-1 receptor antagonists. This study unveils that in late-onset chronic urticaria, the search for autoinflammatory markers and somatic mosaic NLRP3 mutations may have important diagnostic and therapeutic consequences., (Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.)
- Published
- 2020
- Full Text
- View/download PDF
108. NLRP3-associated autoinflammatory diseases: Phenotypic and molecular characteristics of germline versus somatic mutations.
- Author
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Louvrier C, Assrawi E, El Khouri E, Melki I, Copin B, Bourrat E, Lachaume N, Cador-Rousseau B, Duquesnoy P, Piterboth W, Awad F, Jumeau C, Legendre M, Grateau G, Georgin-Lavialle S, Karabina SA, Amselem S, and Giurgea I
- Subjects
- Child, Preschool, Crystallography, X-Ray, Female, Germ-Line Mutation genetics, HEK293 Cells, High-Throughput Nucleotide Sequencing, Humans, Inflammasomes genetics, Male, Middle Aged, NLR Family, Pyrin Domain-Containing 3 Protein chemistry, NLR Family, Pyrin Domain-Containing 3 Protein genetics, Phenotype, Protein Conformation, Severity of Illness Index, THP-1 Cells, Autoimmune Diseases genetics, Inflammasomes metabolism, Inflammation genetics, NLR Family, Pyrin Domain-Containing 3 Protein metabolism
- Abstract
Background: NLRP3-associated autoinflammatory diseases (NLRP3-AIDs) include conditions of various severities, due to germline or somatic mosaic NLRP3 mutations., Objective: To identify mosaic- versus germline-specific NLRP3 mutations' characteristics, we reinterpreted all the mutations reported in NLRP3-AIDs and performed an in-depth study of 3 novel patients., Methods: The pathogenicity of all reported mosaic/germline mutations was reassessed according to international recommendations and their location on the NLRP3 3-dimensional structure. Deep-targeted sequencing and NLRP3-inflammasome-activation assays were used to identify the disease-causing mutation in 3 patients., Results: We identified, in 3 patients, mosaic mutations affecting the same NLRP3 amino acid (Glu569). This residue belongs to 1 of the 2 mosaic mutational hot spots that face each other in the core of the NLRP3 ATPase domain. The review of the 90 NLRP3 mutations identified in 277 patients revealed that those hot spots account for 68.5% of patients (37 of 54) with mosaic mutations. Glu569 is affected in 22% of the patients (12 of 54) with mosaic mutations and in 0.4% of patients (1 of 223) with germline mutations. Only 8 of 90 mutations were found in mosaic and germinal states. All of the germline mutations were associated with a severe phenotype. These data suggest that mutations found only in mosaic state could be incompatible with life if present in germinal state. None of the 5 most frequent germline mutations was identified in mosaic state. Mutations found only in germinal state could, therefore, be asymptomatic in mosaic state., Conclusions: The phenotypic spectrum of NLRP3-AIDs appears to be related to the germinal/mosaic status and localization of the underlying mutations., (Copyright © 2019 American Academy of Allergy, Asthma & Immunology. Published by Elsevier Inc. All rights reserved.)
- Published
- 2020
- Full Text
- View/download PDF
109. Respiratory chain deficiency in a female with Aicardi-Goutières syndrome.
- Author
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Barnérias C, Giurgea I, Hertz-Pannier L, Bahi-Buisson N, Boddaert N, Rustin P, Rotig A, Desguerre I, Munnich A, and de Lonlay P
- Subjects
- Chromatography, Gas, Female, Humans, Ketone Bodies metabolism, Lactic Acid metabolism, Magnetic Resonance Imaging, Mitochondrial Diseases pathology, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, Psychomotor Disorders complications, Pyruvic Acid metabolism, Seizures complications, Syndrome, Basal Ganglia pathology, Calcinosis complications, Calcinosis pathology, Dementia, Vascular complications, Dementia, Vascular pathology, Interferon-alpha cerebrospinal fluid, Lymphocytosis cerebrospinal fluid, Lymphocytosis complications, Mitochondrial Diseases complications
- Abstract
Aicardi-Goutières syndrome (AGS) is an early-onset progressive encephalopathy characterized by calcifications of the basal ganglia, white matter abnormalities, chronic cerebrospinal fluid (CSF) lymphocytosis, and/or a raised level of CSF interferon (INF)-alpha. We report a female with mitochondrial respiratory chain deficiency fulfilling the criteria of AGS. Disease onset was in the first year of age with seizures and psychomotor regression. To date, at 4 years of age, she presents a severe encephalopathy, increased INF-alpha in the CSF, and calcifications of basal ganglia on computerized tomography. Cerebral magnetic resonance imaging showed bilateral and symmetric hypersignal of the posterior white matter. A complex I deficiency of the mitochondrial respiratory chain was found in skeletal muscle, which was associated with a complex IV deficiency in cultured skin fibroblasts. The question of whether this oxidative phosphorylation deficiency is primary or secondary in AGS is open to debate. We suggest giving consideration to systematic evaluation of the mitochondrial respiratory chain in skeletal muscle and skin fibroblasts of other AGS patients.
- Published
- 2006
- Full Text
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110. Hyperinsulinemic hypoglycemia in children.
- Author
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de Lonlay P, Giurgea I, Robert JJ, Fournet JC, Touati G, Nihoul-Fékété C, Brunelle F, Jaubert F, Rahier J, Sempoux C, Junien C, Saudubray JM, Dunne M, Otonkoski T, Ribeiro M, and Bellané-Chantelot C
- Subjects
- Child, Homeostasis, Humans, Hyperinsulinism diagnosis, Hyperinsulinism genetics, Hypoglycemia blood, Hypoglycemia genetics, Hypoglycemia physiopathology, Insulin blood, Insulin metabolism, Insulin Secretion, Hyperinsulinism physiopathology, Hypoglycemia etiology
- Published
- 2004
- Full Text
- View/download PDF
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