Your search keyword '"Camdessanché, Jean-Philippe"' showing total 10 results

1. Impact of a frequent nearsplice variant in amyotrophic lateral sclerosis: optimising genetic screening for gene therapy opportunities.

Author

Muratet, François, Teyssou, Elisa, Chiot, Aude, Boillée, Séverine, Lobsiger, Christian S., Bohl, Delphine, Gyorgy, Beata, Guegan, Justine, Marie, Yannick, Amador, Maria Del Mar, Salachas, Francois, Meininger, Vincent, Bernard, Emilien, Antoine, Jean-Christophe, Camdessanché, Jean-Philippe, Camu, William, Cazeneuve, Cécile, Fauret-Amsellem, Anne-Laure, Leguern, Eric, and Mouzat, Kevin

Subjects

AMYOTROPHIC lateral sclerosis, FRONTOTEMPORAL lobar degeneration, GENETIC testing, GENE therapy, SPINAL muscular atrophy, LYMPHOBLASTOID cell lines, RESEARCH, GENETIC mutation, SEQUENCE analysis, RESEARCH methodology, MEDICAL cooperation, EVALUATION research, COMPARATIVE studies, GENETIC techniques, GENEALOGY, PHENOTYPES

Abstract

Objective: Mutations in superoxide dismutase 1 gene (SOD1), encoding copper/zinc superoxide dismutase protein, are the second most frequent high penetrant genetic cause for amyotrophic lateral sclerosis (ALS) motor neuron disease in populations of European descent. More than 200 missense variants are reported along the SOD1 protein. To limit the production of these aberrant and deleterious SOD1 species, antisense oligonucleotide approaches have recently emerged and showed promising effects in clinical trials. To offer the possibility to any patient with SOD1-ALS to benefit of such a gene therapy, it is necessary to ascertain whether any variant of unknown significance (VUS), detected for example in SOD1 non-coding sequences, is pathogenic.Methods: We analysed SOD1 mutation distribution after SOD1 sequencing in a large cohort of 470 French familial ALS (fALS) index cases.Results: We identified a total of 27 SOD1 variants in 38 families including two SOD1 variants located in nearsplice or intronic regions of the gene. The pathogenicity of the c.358-10T>G nearsplice SOD1 variant was corroborated based on its high frequency (as the second most frequent SOD1 variant) in French fALS, the segregation analysis confirmed in eight affected members of a large pedigree, the typical SOD1-related phenotype observed (with lower limb onset and prominent lower motor neuron involvement), and findings on postmortem tissues showing SOD1 misaccumulation.Conclusions: Our results highlighted nearsplice/intronic mutations in SOD1 are responsible for a significant portion of French fALS and suggested the systematic analysis of the SOD1 mRNA sequence could become the method of choice for SOD1 screening, not to miss these specific cases. [ABSTRACT FROM AUTHOR]

Published

2021

2. TNF-α inhibitors used as steroid-sparing maintenance monotherapy in parenchymal CNS sarcoidosis.

Author

Hilezian, Frédéric, Maarouf, Adil, Boutiere, Clemence, Rico, Audrey, Demortiere, Sarah, Kerschen, Philippe, Sene, Thomas, Bensa-Koscher, Caroline, Giannesini, Claire, Capron, Jean, Mekinian, Arsene, Camdessanché, Jean-Philippe, Androdias, Géraldine, Marignier, Romain, Collongues, Nicolas, Casez, Olivier, Coclitu, Catalina, Vaillant, Mathieu, Mathey, Guillaume, and Ciron, Jonathan

Subjects

SARCOIDOSIS, COMPUTED tomography

Abstract

Objective: To assess the efficacy of tumour necrosis factor-α (TNF-α) inhibitors used as steroid-sparing monotherapy in central nervous system (CNS) parenchymal sarcoidosis.Methods: The French Multiple Sclerosis and Neuroinflammation Centers retrospectively identified patients with definite or probable CNS sarcoidosis treated with TNF-α inhibitors as steroid-sparing monotherapy. Only patients with CNS parenchymal involvement demonstrated by MRI and imaging follow-up were included. The primary outcome was the minimum dose of steroids reached that was not associated with clinical or imaging worsening during a minimum of 3 months after dosing change.Results: Of the identified 38 patients with CNS sarcoidosis treated with TNF-α inhibitors, 23 fulfilled all criteria (13 females). Treatments were infliximab (n=22) or adalimumab (n=1) for a median (IQR) of 24 (17-40) months. At treatment initiation, the mean (SD) age was 41.5 (10.5) years and median (IQR) disease duration 22 (14-49.5) months. Overall, 60% of patients received other immunosuppressive agents before a TNF-α inhibitor. The mean (SD) minimum dose of steroids was 31.5 (33) mg before TNF-α inhibitor initiation and 6.5 (5.5) mg after (p=0.001). In all, 65% of patients achieved steroids dosing <6 mg/day; 61% showed clinical improvement, 30% stability and 9% disease worsening. Imaging revealed improvement in 74% of patients and stability in 26%.Conclusion: TNF-α inhibitors can greatly reduce steroids dosing in patients with CNS parenchymal sarcoidosis, even refractory.Classification Of Evidence: This study provides Class IV evidence that TNF-α inhibitor used as steroid-sparing monotherapy is effective for patients with CNS parenchymal sarcoidosis. [ABSTRACT FROM AUTHOR]

Published

2021

3. Effect of familial clustering in the genetic screening of 235 French ALS families.

Author

Corcia, Philippe, Camu, William, Brulard, Celine, Marouillat, Sylviane, Couratier, Philippe, Camdessanché, Jean-Philippe, Cintas, Pascal, Verschueren, Annie, Soriani, Marie-Helene, Desnuelle, Claude, Fleury, Marie-Céline, Guy, Nathalie, Cassereau, Julien, Viader, Fausto, Pittion-Vouyovitch, Sophie, Danel, Veronique, Kolev, Ivan, Masson, Gwendal Le, Beltran, Stephane, and Salachas, Francois

Subjects

GENETIC testing, PHARMACOLOGY, AMYOTROPHIC lateral sclerosis, FAMILIES, MEDICAL genetics

Abstract

Objectives: To determine whether the familial clustering of amyotrophic lateral sclerosis (ALS) cases and the phenotype of the disease may help identify the pathogenic genes involved.Methods: We conducted a targeted next-generation sequencing analysis on 235 French familial ALS (FALS), unrelated probands to identify mutations in 30 genes linked to the disease. The genealogy, that is, number of cases and generations with ALS, gender, age, site of onset and the duration of the disease were analysed.Results: Regarding the number of generations, 49 pedigrees had only one affected generation, 152 had two affected generations and 34 had at least three affected generations. Among the 149 pedigrees (63.4%) for which a deleterious variant was found, an abnormal G4C2 expansion in C9orf72 was found in 98 cases as well as SOD1, TARBP or FUS mutations in 30, 9 and 7 cases, respectively. Considering pedigrees from the number of generations, abnormal G4C2 expansion in C9orf72 was more frequent in pedigrees with pairs of affected ALS cases, which represented 65.2% of our cohort. SOD1 mutation involved all types of pedigrees. No TARDBP nor FUS mutation was present in monogenerational pedigrees. TARDBP mutation predominated in bigenerational pedigrees with at least three cases and FUS mutation in multigenerational pedigrees with more than seven cases, on average, and with an age of onset younger than 45 years.Conclusion: Our results suggest that familial clustering, phenotypes and genotypes are interconnected in FALS, and thus it might be possible to target the genetic screening from the familial architecture and the phenotype of ALS cases. [ABSTRACT FROM AUTHOR]

Published

2021

4. Paraneoplastic subacute sensory neuropathy with triple positive antineuronal antibodies associated with small-cell lung cancer.

Author

Hean, Virginie, Camdessanché, Jean-Philippe, Cathébras, Pascal, and Killian, Martin

Abstract

A 67-year-old woman with a history of smoking and cardiovascular risk factors was admitted to the emergency room for uncontrolled diabetes, loss of appetite, nausea, significant weight loss and asthenia. The initial investigation, including cerebral and gastrointestinal explorations, were normal. One month later, she started presenting severe asymmetric proprioceptive ataxia of the lower extremities. She also reported paresthesia and neuropathic pain in both feet and ankles. A positron emission tomography (PET)-scanner showed a hypermetabolic nodule in the right lung. The neurological symptoms were attributed to paraneoplastic sensory and dysautonomic neuropathy, even though the bronchoscopic biopsies came back negative at first. Anti-Hu, anti-CV2/CRMP5 and anti-SOX1 antibodies were documented. Due to the severity and rapid progression of symptoms (from the lower to the upper limbs), corticosteroids, intravenous immunoglobulins and immunosuppressants were introduced prior to biopsies revealing a small-cell lung cancer. Despite these treatments and antineoplastic chemotherapy, her status deteriorated rapidly. [ABSTRACT FROM AUTHOR]

Published

2020

5. Clinical characterisation of sensory neuropathy with anti-FGFR3 autoantibodies.

Author

Tholance, Yannick, Moritz, Christian Peter, Rosier, Carole, Ferraud, Karine, Lassablière, François, Reynaud-Federspiel, Evelyne, França Jr, Marcondes C., Martinez, Alberto R. M., Camdessanché, Jean-Philippe, Antoine, Jean-Christophe, França, Marcondes C Jr, and anti-FGFR3 antibody Study Group

Subjects

AUTOANTIBODIES, FIBROBLAST growth factor receptors, NEUROPATHY, AUTOANTIBODY analysis, ELECTRODIAGNOSIS, RESEARCH, NEURONS, RESEARCH methodology, CELL receptors, EVALUATION research, MEDICAL cooperation, COMPARATIVE studies, CHARCOT-Marie-Tooth disease, RESEARCH funding, LONGITUDINAL method

Abstract

Objective: Sensory neuropathies (SNs) are often classified as idiopathic even if immunological mechanisms can be suspected. Antibodies against the intracellular domain of the fibroblast growth factor receptor 3 (FGFR3) possibly identify a subgroup of SN affecting mostly the dorsal root ganglion (DRG). The aim of this study was to identify the frequency of anti-FGFR3 antibodies and the associated clinical pattern in a large cohort of patients with SN.Methods: A prospective, multicentric, European and Brazilian study included adults with pure SN. Serum anti-FGRF3 antibodies were analysed by ELISA. Detailed clinical and paraclinical data were collected for each anti-FGFR3-positive patient and as control for anti-FGFR3-negative patients from the same centres ('center-matched').Results: Sixty-five patients out of 426 (15%) had anti-FGFR3 antibodies, which were the only identified autoimmune markers in 43 patients (66%). The neuropathy was non-length dependent in 89% and classified as sensory neuronopathy in 64%, non-length-dependent small fibre neuropathy in 17% and other neuropathy in 19%. Specific clinical features occurred after 5-6 years of evolution including frequent paresthesia, predominant clinical and electrophysiological involvement of the lower limbs, and a less frequent mixed large and small fibre involvement. Brazilians had a higher frequency of anti-FGFR3 antibodies than Europeans (36% vs 13%, p<0.001), and a more frequent asymmetrical distribution of symptoms (OR 169, 95% CI 3.4 to 8424).Conclusions: Anti-FGFR3 antibodies occur in a subgroup of SN probably predominantly affecting the DRG. Differences between Europeans and Brazilians could suggest involvement of genetic or environmental factors. [ABSTRACT FROM AUTHOR]

Published

2020

6. CLIPPERS and its mimics: evaluation of new criteria for the diagnosis of CLIPPERS.

Author

Taieb, Guillaume, Mulero, Patricia, Psimaras, Dimitri, Oosten, Bob W van, Seebach, Jörg D., Marignier, Romain, Pico, Fernando, Rigau, Valérie, Ueno, Yuji, Duflos, Claire, Fominykh, Vera, Guiraud, Vincent, Lebrun-Frénay, Christine, Camdessanché, Jean-Philippe, Kerschen, Philippe, Ahle, Guido, Téllez, Nieves, Rovira, Alex, Khe Hoang-Xuan, and Pelletier, Jean

Subjects

VASCULAR cell adhesion molecule-1, NEUROLOGICAL disorders, GLIAL fibrillary acidic protein, PERIPHERAL nervous system, HIGHLY active antiretroviral therapy, ENCEPHALITIS diagnosis, ENCEPHALITIS, BRAIN, PREDNISOLONE, DIFFERENTIAL diagnosis, MAGNETIC resonance imaging, PREDNISONE, BRAIN stem, NEURORADIOLOGY

Abstract

Objective: To evaluate the accuracy of the recently proposed diagnostic criteria for chronic lymphocytic inflammation with pontine perivascular enhancement responsive to steroids (CLIPPERS).Methods: We enrolled 42 patients with hindbrain punctate and/or linear enhancements (<3 mm in diameter) and tested the CLIPPERS criteria.Results: After a median follow-up of 50 months (IQR 25-82), 13 out of 42 patients were CLIPPERS-mimics: systemic and central nervous system lymphomas (n=7), primary central nervous system angiitis (n=4) and autoimmune gliopathies (n=2). The sensitivity and specificity of the CLIPPERS criteria were 93% and 69%, respectively. Nodular enhancement ( ≥ 3 mm in diameter), considered as a red flag in CLIPPERS criteria, was present in 4 out of 13 CLIPPERS-mimics but also in 2 out of 29 patients with CLIPPERS, explaining the lack of sensitivity. Four out of 13 CLIPPERS-mimics who initially met the CLIPPERS criteria displayed red flags at the second attack with a median time of 5.5 months (min 3, max 18), explaining the lack of specificity. One of these four patients had antimyelin oligodendrocyte glycoprotein antibodies, and the three remaining patients relapsed despite a daily dose of prednisone/prednisolone ≥ 30 mg and a biopsy targeting atypical enhancing lesions revealed a lymphoma.Conclusions: Our study highlights that (1) nodular enhancement should be considered more as an unusual finding than a red flag excluding the diagnosis of CLIPPERS; (2) red flags may occur up to 18 months after disease onset; (3) as opposed to CLIPPERS-mimics, no relapse occurs when the daily dose of prednisone/prednisolone is ≥ 30 mg; and (4) brain biopsy should target an atypical enhancing lesion when non-invasive investigations remain inconclusive. [ABSTRACT FROM AUTHOR]

Published

2019

7. Early intravenous immunoglobulin treatment in paraneoplastic neurological syndromes with onconeural antibodies.

Author

Berzero, Giulia, Karantoni, Evgenia, Dehais, Caroline, Ducray, François, Thomas, Laure, Picard, Géraldine, Rogemond, Véronique, Candelier, Gaëlle, Camdessanché, Jean-Philippe, Antoine, Jean-Christophe, De Seze, Jérôme, Liou-Schischmanoff, Amélie, Honnorat, Jérôme, Delattre, Jean-Yves, and Psimaras, Dimitri

Subjects

INTRAVENOUS immunoglobulins, THERAPEUTIC use of immunoglobulins, PARANEOPLASTIC syndromes, IMMUNOTHERAPY, TUMOR treatment, DIAGNOSIS, CLINICAL trials, COMPARATIVE studies, DRUG administration, LONGITUDINAL method, RESEARCH methodology, MEDICAL cooperation, NEUROLOGICAL disorders, RESEARCH, EVALUATION research

Published

2018

8. Anti-MAG antibodies in 202 patients: clinicopathological and therapeutic features.

Author

Svahn, Juliette, Petiot, Philippe, Antoine, Jean-Christophe, Vial, Christophe, Delmont, Emilien, Viala, Karine, Steck, Andreas J., Magot, Armelle, Cauquil, Cecile, Zarea, Aline, Echaniz-Laguna, Andoni, Ferfoglia, Ruxandra Iancu, Gueguen, Antoine, Magy, Laurent, Léger, Jean-Marc, Kuntzer, Thierry, Ferraud, Karine, Lacour, Arnaud, Camdessanché, Jean-Philippe, and Iancu Ferfoglia, Ruxandra

Subjects

MYELIN-associated glycoprotein, MONOCLONAL gammopathies, GLYCOPROTEINS, PHENOTYPES, THERAPEUTICS

Abstract

Objective: To assess the clinicopathological and therapeutic features of patients with low (≥1000 to <10 000 Bühlmann Titre Units) (BTU), medium (10 000-70 000) or high (≥70 000) anti-myelin-associated glycoprotein (anti-MAG) antibody titres.Methods: We retrospectively and prospectively analysed standardised report forms and medical records of 202 patients from 14 neuromuscular centres.Results: Mean age at onset and mean time between symptom onset to last follow-up were respectively 62.6 years (25-91.4) and 8.4 years (0.3-33.3). Anti-MAG antibody titres at diagnosis were low, medium or high in 11%, 51% and 38% of patients. Patients presented with monoclonal gammopathy of undetermined significance in 68% of cases. About 17% of patients presented with 'atypical' clinical phenotype independently of anti-MAG titres, including acute or chronic sensorimotor polyradiculoneuropathies (12.4%), and asymmetric or multifocal neuropathy (3%). At the most severe disease stage, 22.4% of patients were significantly disabled. Seventy-eight per cent of patients received immunotherapies. Transient clinical worsening was observed in 12% of patients treated with rituximab (11/92). Stabilisation after rituximab treatment during the 7-12-month follow-up period was observed in 29% of patients. Clinical response to rituximab during the 6-month and/or 7-12-month follow-up period was observed in 31.5% of patients and correlated with anti-MAG titre ≥10 000 BTU.Conclusion: Our study highlights the extended clinical spectrum of patients with anti-MAG neuropathy, which appears unrelated to antibody titre. Besides, it may also suggest beneficial use of rituximab in the early phase of anti-MAG neuropathy. [ABSTRACT FROM AUTHOR]

Published

2018

9. Antifibroblast growth factor receptor 3 antibodies identify a subgroup of patients with sensory neuropathy.

Author

Antoine, Jean-Christophe, Boutahar, Nadia, Lassablière, François, Reynaud, Evelyne, Ferraud, Karine, Rogemond, Véronique, Paul, Stéphane, Honnorat, Jérôme, and Camdessanché, Jean-Philippe

Subjects

FIBROBLAST growth factor receptors, NEUROPATHY, AUTOIMMUNE diseases, IMMUNOGLOBULINS, NEUROLOGICAL disorders, HUMAN proteins, ENZYME-linked immunosorbent assay, PERIPHERAL neuropathy diagnosis, IMMUNOGLOBULIN analysis, ANTIGEN-antibody reactions, CELL receptors, EPITHELIAL cells, IMMUNITY, NERVE tissue proteins, PERIPHERAL neuropathy, SENSORY receptors, PREDICTIVE tests, RETROSPECTIVE studies

Abstract

Background: Immunological mechanisms are suspected in sensory neuropathy (SN) occurring with systemic autoimmune diseases and in some idiopathic cases, but so far there are no antibodies (Abs) identifying these neuropathies.Methods: In the search for such specific antibodies, serum samples were collected from 106 patients with SN of these 72 fulfilled the diagnosis criteria of sensory neuronopathy (SNN) and 211 control subjects including patients with sensorimotor neuropathies, other neurological diseases (ONDs), systemic autoimmune diseases and healthy blood donors.Results: In the first step, a protein array with 8000 human proteins allowed identification of the intracellular domain of the fibroblast growth factor receptor 3 (FGFR3) as a target of Abs in 7/16 SNN and 0/30 controls. In the second step, an ELISA method was used to test the 317 patients and controls for anti-FGFR3 Abs. Abs were detected in 16/106 patients with SN and 1/211 controls (p<0.001). Among the 106 patients with SN, anti-FGFR3 Abs were found in 11/38 patients with autoimmune context, 5/46 with idiopathic neuropathy and 0/22 with neuropathy of other aetiology (p=0.006). The only control patient with anti-FGFR3 Abs had lupus and no recorded neuropathy. Sensitivity, specificity, and positive and negative predictive values of anti-FGFR3 Abs for a diagnosis of idiopathic or dysimmune SN were 19%, 99.6%, 94.1% and 77.3%, respectively. A cell-based assay confirmed serum reactivity against the intracellular domain of FGFR3. The neuropathy in patients with anti-FGF3 Abs was non-length dependent in 87% of patients and fulfilled the criteria of probable SNN in 82%. Trigeminal nerve involvement and pain were frequent features.Conclusions: A anti-FGFR3 Abs identify a subgroup of patients with SN in whom an underlying autoimmune disorder affecting sensory neurons in the dorsal root and trigeminal nerve ganglia is suspected. [ABSTRACT FROM AUTHOR]

Published

2015

10. Impact of a frequent nearsplice SOD1 variant in amyotrophic lateral sclerosis: optimising SOD1 genetic screening for gene therapy opportunities.

Author

Muratet F, Teyssou E, Chiot A, Boillée S, Lobsiger CS, Bohl D, Gyorgy B, Guegan J, Marie Y, Amador MDM, Salachas F, Meininger V, Bernard E, Antoine JC, Camdessanché JP, Camu W, Cazeneuve C, Fauret-Amsellem AL, Leguern E, Mouzat K, Guissart C, Lumbroso S, Corcia P, Vourc'h P, Grapperon AM, Attarian S, Verschueren A, Seilhean D, and Millecamps S

Subjects

Adult, Aged, Aged, 80 and over, DNA Mutational Analysis, Female, Genetic Testing, Genetic Therapy, Humans, Male, Middle Aged, Phenotype, Amyotrophic Lateral Sclerosis genetics, Mutation, Pedigree, Superoxide Dismutase-1 genetics

Abstract

Objective: Mutations in superoxide dismutase 1 gene ( SOD1) , encoding copper/zinc superoxide dismutase protein, are the second most frequent high penetrant genetic cause for amyotrophic lateral sclerosis (ALS) motor neuron disease in populations of European descent. More than 200 missense variants are reported along the SOD1 protein. To limit the production of these aberrant and deleterious SOD1 species, antisense oligonucleotide approaches have recently emerged and showed promising effects in clinical trials. To offer the possibility to any patient with SOD1-ALS to benefit of such a gene therapy, it is necessary to ascertain whether any variant of unknown significance (VUS), detected for example in SOD1 non-coding sequences, is pathogenic., Methods: We analysed SOD1 mutation distribution after SOD1 sequencing in a large cohort of 470 French familial ALS (fALS) index cases., Results: We identified a total of 27 SOD1 variants in 38 families including two SOD1 variants located in nearsplice or intronic regions of the gene. The pathogenicity of the c.358-10T>G nearsplice SOD1 variant was corroborated based on its high frequency (as the second most frequent SOD1 variant) in French fALS, the segregation analysis confirmed in eight affected members of a large pedigree, the typical SOD1-related phenotype observed (with lower limb onset and prominent lower motor neuron involvement), and findings on postmortem tissues showing SOD1 misaccumulation., Conclusions: Our results highlighted nearsplice/intronic mutations in SOD1 are responsible for a significant portion of French fALS and suggested the systematic analysis of the SOD1 mRNA sequence could become the method of choice for SOD1 screening, not to miss these specific cases., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2021. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2021