Your search keyword '"Carapito, R. (Raphaël)"' showing total 8 results

1. CD4 T cell-intrinsic STING signaling controls the differentiation and effector functions of T H 1 and T H 9 cells

Author

Benoit Lizon, I. (Isis), Jacquin, E. (Elise), Rivera Vargas, T. (Thaiz), Richard, C. (Corentin), Roussey, A. (Aurélie), Dal Zuffo, L. (Ludivine), Martin, T. (Tiffany), Melis, A. (Andréa), Vinokurova, D. (Daria), Shahoei, S. (Sayyed Hamed), Baeza Garcia, A. (Alvaro), Pignol, C. (Cassandre), Giorgiutti, S. (Stéphane), Carapito, R. (Raphaël), Boidot, R. (Romain), Végran, F. (Frédérique), Flavell, R. (Richard A), Ryffel, B. (Bernhard), Nelson, E. (Eric R), Soulas-Sprauel, P. (Pauline), Lawrence, T. (Toby), and Apetoh, L. (Lionel)

Subjects

Aucun, Sciences du Vivant [q-bio]/Immunologie

Published

2022

2. Atypical focal segmental glomerulosclerosis associated with a new PODXL nonsense variant

Author

Marx, D. (David), Caillard-Ohlmann, S. (Sophie), Olagne, J. (Jérôme), Moulin, B. (Bruno), Hannedouche, T. (Thierry), Touchard, G. (Guy), Dupuis, A. (Arnaud), Gachet, C. (Christian), Molitor, A. (Anne), Bahram, S. (Seiamak), and Carapito, R. (Raphaël)

Subjects

Sciences du Vivant [q-bio]/Immunologie, urologic and male genital diseases

Abstract

Background: Podocalyxin (PODXL) is a highly sialylated adhesion glycoprotein that plays an important role in podocyte's physiology. Recently, missense and nonsense dominant variants in the PODXL gene have been associated with focal segmental glomerulosclerosis (FSGS), a leading cause of nephrotic syndrome and kidney failure. Their histologic description, however, was superficial or absent. Methods: We performed exome sequencing on a three-generation family affected by an atypical glomerular nephropathy and characterized the disease by light and electron microscopy. Results: The disease was characterized by FSGS features and glomerular basement membrane duplication. Six family members displayed chronic proteinuria, ranging from mild manifestations without renal failure, to severe forms with end-stage renal disease. Exome sequencing of affected twin sisters, their affected mother, healthy father, and healthy maternal uncle revealed a new nonsense variant cosegregating with the disease (c.1453C>T, NM_001018111) in the PODXL gene, which is known to be expressed in the kidney and to cause nephropathy when mutated. The variant is predicted to lead to a premature stop codon (p.Q485*) that results in the loss of the intracytoplasmic tail of the protein. Conclusion: This is the first description of a peculiar association combining a PODXL stop-gain variant and both FSGS and membranoproliferative glomerulonephritis features, described by light and electron microscopy.

Published

2021

3. Bioinformatics

Author

Bertrand, F. (Frédéric), Aouadi, I. (Ismaïl), Jung, N. (Nicolas), Carapito, R. (Raphaël), Vallat, L. (Laurent), Bahram, S. (Seiamak), and Maumy-Bertrand, M. (Myriam)

Subjects

Aucun, Sciences du Vivant [q-bio]/Médecine humaine et pathologie

Abstract

Motivation: With the growth of big data, variable selection has become one of the critical challenges in statistics. Although many methods have been proposed in the literature, their performance in terms of recall (sensitivity) and precision (predictive positive value) is limited in a context where the number of variables by far exceeds the number of observations or in a highly correlated setting. Results: In this article, we propose a general algorithm, which improves the precision of any existing variable selection method. This algorithm is based on highly intensive simulations and takes into account the correlation structure of the data. Our algorithm can either produce a confidence index for variable selection or be used in an experimental design planning perspective. We demonstrate the performance of our algorithm on both simulated and real data. We then apply it in two different ways to improve biological network reverse-engineering.

Published

2021

4. Case Report: Acquired Disseminated BCG in the Context of a Delayed Immune Reconstitution After Hematological Malignancy: Acquired Disseminated BCG in the Context of a Delayed Immune Reconstitution After Hematological Malignancy

Author

Gies, V. (Vincent), Dieudonné, Y. (Yannick), Morel, F. (Florence), Sougakoff, W. (Wladimir), Carapito, R. (Raphaël), Martin, A. (Aurélie), Weingertner, N. (Noëlle), Jacquel, L. (Léa), Hubele, F. (Fabrice), Kuhnert, C. (Cornélia), Jung, S. (Sophie), Schramm, F. (Frederic), Boyer, P. (Pierre), Hansmann, Y. (Yves), Danion, F. (François), Korganow, A. (Anne-Sophie) S. (S), and Guffroy, A. (Aurelien)

Subjects

Sciences du Vivant [q-bio]/Médecine humaine et pathologie, complex mixtures

Abstract

Context Disseminated infections due to Mycobacterium bovis Bacillus Calmette-Guerin (BCG) are unusual and occur mostly in patients with inborn error of immunity (IEI) or acquired immunodeficiency. However, cases of secondary BCGosis due to intravesical BCG instillation have been described. Herein, we present a case of severe BCGosis occurring in an unusual situation. C ase Description We report one case of severe disseminated BCG disease occurring after hematological malignancy in a 48-year-old man without BCG instillation and previously vaccinated in infancy with no complication. Laboratory investigations demonstrated that he was not affected by any known or candidate gene of IEI or intrinsic cellular defect involving IFN gamma pathway. Whole genome sequencing of the BCG strain showed that it was most closely related to the M. bovis BCG Tice strain, suggesting an unexpected relationship between the secondary immunodeficiency of the patient and the acquired BCG infection.& nbsp; Conclusion This case highlights the fact that, in addition to the IEI, physicians, as well as microbiologists and pharmacists should be aware of possible acquired disseminated BCG disease in secondary immunocompromised patients treated in centers that administrate BCG for bladder cancers.

Published

2021

5. Impact of Tenascin-C on Radiotherapy in a Novel Syngeneic Oral Squamous Cell Carcinoma Model With Spontaneous Dissemination to the Lymph Nodes

Author

Spenlé, C. (Caroline), Loustau, T. (Thomas), Burckel, H. (Helene), Riegel, G. (Gilles), Abou-Faycal, C. (Cherine), Li, C. (Chengbei) B. (B), Yilmaz, A. (Alev), Petti, L. (Luciana), Steinbach, F. (Fanny), Ahowesso, C. (Constance), Jost, C. (Camille), Paul, N. (Nicodème), Carapito, R. (Raphaël), Noel, G. (Georges), Anjuere, F. (F), Salomé, N. (Nathalie), and Orend, G. (Gertraud)

Subjects

stomatognathic diseases, Sciences du Vivant [q-bio]/Cancer

Abstract

Radiotherapy, the most frequent treatment of oral squamous cell carcinomas (OSCC) besides surgery is employed to kill tumor cells but, radiotherapy may also promote tumor relapse where the immune-suppressive tumor microenvironment (TME) could be instrumental. We established a novel syngeneic grafting model from a carcinogen-induced tongue tumor, OSCC13, to address the impact of radiotherapy on OSCC. This model revealed similarities with human OSCC, recapitulating carcinogen-induced mutations found in smoking associated human tongue tumors, abundant tumor infiltrating leukocytes (TIL) and, spontaneous tumor cell dissemination to the local lymph nodes. Cultured OSCC13 cells and OSCC13-derived tongue tumors were sensitive to irradiation. At the chosen dose of 2 Gy mimicking treatment of human OSCC patients not all tumor cells were killed allowing to investigate effects on the TME. By investigating expression of the extracellular matrix molecule tenascin-C (TNC), an indicator of an immune suppressive TME, we observed high local TNC expression and TIL infiltration in the irradiated tumors. In a TNC knockout host the TME appeared less immune suppressive with a tendency towards more tumor regression than in WT conditions. Altogether, our novel syngeneic tongue OSCC grafting model, sharing important features with the human OSCC disease could be relevant for future anti-cancer targeting of OSCC by radiotherapy and other therapeutic approaches.

Published

2021

6. NCKAP1L defects lead to a novel syndrome combining immunodeficiency, lymphoproliferation and hyperinflammation Running title: NCKAP1L deficiency: NCKAP1L deficiency

Author

Castro, C. (Carla) N. (Noemi), Rosenzwajg, M. (Michelle), Carapito, R. (Raphaël), Shahrooei, M. (Mohammad), Konantz, M. (Martina), Khan, A. (Amjad), Miao, Z. (Zhichao), Gross, M. (Miriam), Tranchant, T. (Thibaud), Radosavljevic, M. (Mirjana), Paul, N. (Nicodème), Stemmelen, T. (Tristan), Pitoiset, F. (Fabien), Hirschler, A. (Aurélie), Nespola, B. (Benoit), Molitor, A. (Anne), Rolli, V. (Veronique), Pichot, A. (Angelique), Faletti, L. (Laura) E. (Eva), Rinaldi, B. (Bruno), Friant, S. (Sylvie), Mednikov, M. (Mark), Karauzum, H. (Hatice), Javad Aman, M. (M), Carapito, C. (Christine), Lengerke, C. (Claudia), Ziaee, V. (Vahid), Eyaid, W. (Wafaa), Ehl, S. (Stephan), Alroqi, F. (Fayhan), Parvaneh, N. (Nima), and Bahram, S. (Seiamak)

Subjects

hal-03024718, Aucun

Abstract

The Nck-associated protein 1-like (NCKAP1L) gene, alternatively called hematopoietic protein 1 (HEM-1), encodes a hematopoietic lineage-specific regulator of the actin cytoskeleton. Nckap1l-deficient mice have anomalies in lymphocyte development, phagocytosis, and neutrophil migration. Here we report, for the first time, NCKAP1L deficiency cases in humans. In two unrelated patients of Middle Eastern origin, recessive mutations in NCKAP1L abolishing protein expression led to immunodeficiency, lymphoproliferation, and hyperinflammation with features of hemophagocytic lymphohistiocytosis. Immunophenotyping showed an inverted CD4/CD8 ratio with a major shift of both CD4+ and CD8+ cells toward memory compartments, in line with combined RNA-seq/proteomics analyses revealing a T cell exhaustion signature. Consistent with the core function of NCKAP1L in the reorganization of the actin cytoskeleton, patients' T cells displayed impaired early activation, immune synapse morphology, and leading edge formation. Moreover, knockdown of nckap1l in zebrafish led to defects in neutrophil migration. Hence, NCKAP1L mutations lead to broad immune dysregulation in humans, which could be classified within actinopathies.

Published

2020

7. Correction to ZMIZ1 Variants Cause a Syndromic Neurodevelopmental Disorder

Author

Carapito, R. (Raphaël), Ivanova, E. (Ekaterina), Morlon, A. (Aurore), Meng, L. (Linyan), Molitor, A. (Anne), Erdmann, E. (Eva), Kieffer, B. (Bruno), Pichot, A. (Angélique), Naegely, L. (Lydie), Kolmer, A. (Aline), Paul, N. (Nicodème), Hanauer, A. (Antoine), Tran Mau-Them, F. (Frédéric), Jean-Marçais, N. (Nolwenn), Hiatt, S. (Susan), Cooper, G. (Gregory), Tvrdik, T. (Tatiana), Muir, A. (Alison), Dimartino, C. (Clémantine), Chopra, M. (Maya), Amiel, J. (Jeanne), Gordon, C. (Christopher), Dutreux, F. (Fabien), Garde, A. (Aurore), Thauvin-Robinet, C. (Christel), Wang, X. (Xia), Leduc, M. (Magalie), Phillips, M. (Meredith), Crawford, H. (Heather), Kukolich, M. (Mary), Hunt, D. (David), Harrison, V. (Victoria), Kharbanda, M. (Mira), Smigiel, R. (Robert), Gold, N. (Nina), Hung, C. (Christina), Viskochil, D. (David), Dugan, S. (Sarah), Bayrak-Toydemir, P. (Pinar), Joly-Helas, G. (Géraldine), Guerrot, A. (Anne-Marie), Schluth-Bolard, C. (Caroline), Rio, M. (Marlène), Wentzensen, Ingrid M., McWalter, K. (Kirsty), Schnur, R. (Rhonda), Lewis, A. (Andrea), Lalani, S. (Seema), Mensah-Bonsu, N. (Noël), Céraline, J. (Jocelyn), Sun, Z. (Zijie), Ploski, R. (Rafal), Bacino, C. (Carlos), Mefford, H. (Heather), Faivre, L. (Laurence), Bodamer, O. (Olaf), Chelly, J. (Jamel), Isidor, B. (Bertrand), and Bahram, S. (Seiamak)

Subjects

Sciences du Vivant [q-bio]/Neurosciences [q-bio.NC], Sciences du Vivant [q-bio]/Biotechnologies

Published

2020

8. Identical penicillin-binding domains in penicillin-binding proteins of Streptococcus pneumoniae clinical isolates with different levels of beta-lactam resistance

Author

Chesnel, L. (Laurent), Carapito, R. (Raphaël), Croizé, J. (Jacques), Dideberg, O. (Otto), Vernet, T. (Thierry), and Zapun, A. (André)

Subjects

polycyclic compounds, Aucun, bacteria, biochemical phenomena, metabolism, and nutrition

Abstract

We have sequenced the penicillin-binding domains of the complete repertoire of penicillin-binding proteins and MurM from 22 clinical isolates of Streptococcus pneumoniae that span a wide range of P-lactam resistance levels. Evidence of mosaicism was found in the genes encoding PBP 1a, PBP 2b, PBP 2x, MurM, and, possibly, PBP 2a. Five isolates were found to have identical PBP and MurM sequences, even though the MICs for penicillin G ranged from 0.25 to 2.0 mg/liter. When the sequences encoding PBP la, PBP 2b, and PBP 2x from one of these isolates were used to transform laboratory strain R6, the resulting strain had a resistance level higher than that of the less resistant isolates carrying that PBP set but lower than that of the most resistant isolates carrying that PBP set. This result demonstrates that if the R6 strain is arbitrarily defined as the standard genotype, some wild genetic backgrounds can either increase or decrease the PBP-based resistance phenotype.

Published

2005