Your search keyword '"Maria Carmina Castiello"' showing total 38 results

1. Partial correction of immunodeficiency by lentiviral vector gene therapy in mouse models carrying Rag1 hypomorphic mutations

Author

Maria Carmina Castiello, Martina Di Verniere, Elena Draghici, Elena Fontana, Sara Penna, Lucia Sereni, Alessandra Zecchillo, Denise Minuta, Paolo Uva, Marco Zahn, Irene Gil-Farina, Andrea Annoni, Silvia Iaia, Lisa M. Ott de Bruin, Luigi D. Notarangelo, Karin Pike-Overzet, Frank J. T. Staal, Anna Villa, and Valentina Capo

Subjects

RAG1 gene, gene therapy, immunodeficiency, immune dysregulation, lentiviral vectors, autoimmunity, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionRecombination activating genes (RAG) 1 and 2 defects are the most frequent form of severe combined immunodeficiency (SCID). Patients with residual RAG activity have a spectrum of clinical manifestations ranging from Omenn syndrome to delayed-onset combined immunodeficiency, often associated with granulomas and/or autoimmunity (CID-G/AI). Lentiviral vector (LV) gene therapy (GT) has been proposed as an alternative treatment to the standard hematopoietic stem cell transplant and a clinical trial for RAG1 SCID patients recently started. However, GT in patients with hypomorphic RAG mutations poses additional risks, because of the residual endogenous RAG1 expression and the general state of immune dysregulation and associated inflammation.MethodsIn this study, we assessed the efficacy of GT in 2 hypomorphic Rag1 murine models (Rag1F971L/F971L and Rag1R972Q/R972Q), exploiting the same LV used in the clinical trial encoding RAG1 under control of the MND promoter.Results and discussionStarting 6 weeks after transplant, GT-treated mice showed a decrease in proportion of myeloid cells and a concomitant increase of B, T and total white blood cells. However, counts remained lower than in mice transplanted with WT Lin- cells. At euthanasia, we observed a general redistribution of immune subsets in tissues, with the appearance of mature recirculating B cells in the bone marrow. In the thymus, we demonstrated correction of the block at double negative stage, with a modest improvement in the cortical/medullary ratio. Analysis of antigenspecific IgM and IgG serum levels after in vivo challenge showed an amelioration of antibody responses, suggesting that the partial immune correction could confer a clinical benefit. Notably, no overt signs of autoimmunity were detected, with B-cell activating factor decreasing to normal levels and autoantibodies remaining stable after GT. On the other hand, thymic enlargement was frequently observed, although not due to vector integration and insertional mutagenesis. In conclusion, our work shows that GT could partially alleviate the combined immunodeficiency of hypomorphic RAG1 patients and that extensive efficacy and safety studies with alternative models are required before commencing RAG gene therapy in thesehighly complex patients.

Published

2023

2. Thymic Epithelial Cell Alterations and Defective Thymopoiesis Lead to Central and Peripheral Tolerance Perturbation in MHCII Deficiency

Author

Francesca Ferrua, Ileana Bortolomai, Elena Fontana, Dario Di Silvestre, Rosita Rigoni, Genni Enza Marcovecchio, Elena Draghici, Francesca Brambilla, Maria Carmina Castiello, Gloria Delfanti, Despina Moshous, Capucine Picard, Tom Taghon, Victoria Bordon, Ansgar S. Schulz, Catharina Schuetz, Silvia Giliani, Annarosa Soresina, Andrew R. Gennery, Sara Signa, Blachy J. Dávila Saldaña, Ottavia M. Delmonte, Luigi D. Notarangelo, Chaim M. Roifman, Pietro Luigi Poliani, Paolo Uva, Pier Luigi Mauri, Anna Villa, and Marita Bosticardo

Subjects

thymus, thymic epithelial cells, primary immunodeficiency, MHCII, central tolerance, Immunologic diseases. Allergy, RC581-607

Abstract

Major Histocompatibility Complex (MHC) class II (MHCII) deficiency (MHCII-D), also known as Bare Lymphocyte Syndrome (BLS), is a rare combined immunodeficiency due to mutations in genes regulating expression of MHCII molecules. MHCII deficiency results in impaired cellular and humoral immune responses, leading to severe infections and autoimmunity. Abnormal cross-talk with developing T cells due to the absence of MHCII expression likely leads to defects in thymic epithelial cells (TEC). However, the contribution of TEC alterations to the pathogenesis of this primary immunodeficiency has not been well characterized to date, in particular in regard to immune dysregulation. To this aim, we have performed an in-depth cellular and molecular characterization of TEC in this disease. We observed an overall perturbation of thymic structure and function in both MHCII−/− mice and patients. Transcriptomic and proteomic profiling of murine TEC revealed several alterations. In particular, we demonstrated that impairment of lymphostromal cross-talk in the thymus of MHCII−/− mice affects mTEC maturation and promiscuous gene expression and causes defects of central tolerance. Furthermore, we observed peripheral tolerance impairment, likely due to defective Treg cell generation and/or function and B cell tolerance breakdown. Overall, our findings reveal disease-specific TEC defects resulting in perturbation of central tolerance and limiting the potential benefits of hematopoietic stem cell transplantation in MHCII deficiency.

Published

2021

3. Gene Editing of Hematopoietic Stem Cells: Hopes and Hurdles Toward Clinical Translation

Author

Samuele Ferrari, Valentina Vavassori, Daniele Canarutto, Aurelien Jacob, Maria Carmina Castiello, Attya Omer Javed, and Pietro Genovese

Subjects

gene editing, hematopoietic stem cell, CRISPR/Cas, gene therapy, hematological diseases, Biotechnology, TP248.13-248.65, Genetics, QH426-470

Abstract

In the field of hematology, gene therapies based on integrating vectors have reached outstanding results for a number of human diseases. With the advent of novel programmable nucleases, such as CRISPR/Cas9, it has been possible to expand the applications of gene therapy beyond semi-random gene addition to site-specific modification of the genome, holding the promise for safer genetic manipulation. Here we review the state of the art of ex vivo gene editing with programmable nucleases in human hematopoietic stem and progenitor cells (HSPCs). We highlight the potential advantages and the current challenges toward safe and effective clinical translation of gene editing for the treatment of hematological diseases.

Published

2021

4. Innovative Cell-Based Therapies and Conditioning to Cure RAG Deficiency

Author

Anna Villa, Valentina Capo, and Maria Carmina Castiello

Subjects

RAG genes, gene therapy, non-genotoxic conditioning, severe combined immunodeficiency, hematopoietic stem cell transplantation, Omenn syndrome, Immunologic diseases. Allergy, RC581-607

Abstract

Genetic defects in recombination activating genes (RAG) 1 and 2 cause a broad spectrum of severe immune defects ranging from early severe and repeated infections to inflammation and autoimmune manifestations. A correlation between in vitro recombination activity and immune phenotype has been described. Hematopoietic cell transplantation is the treatment of care; however, the availability of next generation sequencing and whole genome sequencing has allowed the identification of novel genetic RAG variants in immunodeficient patients at various ages, raising therapeutic questions. This review addresses the recent advances of novel therapeutic approaches for RAG deficiency. As conventional myeloablative conditioning regimens are associated with acute toxicities and transplanted-related mortality, innovative minimal conditioning regimens based on the use of monoclonal antibodies are now emerging and show promising results. To overcome shortage of compatible donors, gene therapy has been developed in various RAG preclinical models. Overall, the transplantation of autologous gene corrected hematopoietic precursors and the use of non-genotoxic conditioning will open a new era, offering a cure to an increasing number of RAG patients regardless of donor availability and severity of clinical conditions.

Published

2020

5. In Vivo Chronic Stimulation Unveils Autoreactive Potential of Wiskott–Aldrich Syndrome Protein-Deficient B Cells

Author

Anna Villa, Marita Bosticardo, Maria Carmina Castiello, Francesca Pala, Lucia Sereni, Elena Draghici, Donato Inverso, Aisha V. Sauer, Francesca Schena, Elena Fontana, Enrico Radaelli, Paolo Uva, Karla E. Cervantes-Luevano, Federica Benvenuti, Pietro L. Poliani, Matteo Iannacone, and Elisabetta Traggiai

Subjects

Wiskott–Aldrich syndrome, autoimmunity, B cells, toll-like receptors, apoptotic cells, lymphocytic choriomeningitis virus, Immunologic diseases. Allergy, RC581-607

Abstract

Wiskott–Aldrich syndrome (WAS) is a primary immunodeficiency caused by mutations in the gene encoding the hematopoietic-specific WAS protein (WASp). WAS is frequently associated with autoimmunity, indicating a critical role of WASp in maintenance of tolerance. The role of B cells in the induction of autoreactive immune responses in WAS has been investigated in several settings, but the mechanisms leading to the development of autoimmune manifestations have been difficult to evaluate in the mouse models of the disease that do not spontaneously develop autoimmunity. We performed an extensive characterization of Was−/− mice that provided evidence of the potential alteration in B cell selection, because of the presence of autoantibodies against double-stranded DNA, platelets, and tissue antigens. To uncover the mechanisms leading to the activation of the potentially autoreactive B cells in Was−/− mice, we performed in vivo chronic stimulations with toll-like receptors agonists (LPS and CpG) and apoptotic cells or infection with lymphocytic choriomeningitis virus. All treatments led to increased production of autoantibodies, increased proteinuria, and kidney tissue damage in Was−/− mice. These findings demonstrate that a lower clearance of pathogens and/or self-antigens and the resulting chronic inflammatory state could cause B cell tolerance breakdown leading to autoimmunity in WAS.

Published

2017

6. Choice of template delivery mitigates the genotoxic risk and adverse impact of editing in human hematopoietic stem cells

Author

Samuele Ferrari, Aurelien Jacob, Daniela Cesana, Marianne Laugel, Stefano Beretta, Angelica Varesi, Giulia Unali, Anastasia Conti, Daniele Canarutto, Luisa Albano, Andrea Calabria, Valentina Vavassori, Carlo Cipriani, Maria Carmina Castiello, Simona Esposito, Chiara Brombin, Federica Cugnata, Oumeya Adjali, Eduard Ayuso, Ivan Merelli, Anna Villa, Raffaella Di Micco, Anna Kajaste-Rudnitski, Eugenio Montini, Magalie Penaud-Budloo, and Luigi Naldini

Subjects

Gene Editing, Integrases, DNA, Viral, Genetics, Molecular Medicine, Humans, Cell Biology, CRISPR-Cas Systems, Tumor Suppressor Protein p53, Hematopoietic Stem Cells, DNA Damage

Abstract

Long-range gene editing by homology-directed repair (HDR) in hematopoietic stem/progenitor cells (HSPCs) often relies on viral transduction with recombinant adeno-associated viral vector (AAV) for template delivery. Here, we uncover unexpected load and prolonged persistence of AAV genomes and their fragments, which trigger sustained p53-mediated DNA damage response (DDR) upon recruiting the MRE11-RAD50-NBS1 (MRN) complex on the AAV inverted terminal repeats (ITRs). Accrual of viral DNA in cell-cycle-arrested HSPCs led to its frequent integration, predominantly in the form of transcriptionally competent ITRs, at nuclease on- and off-target sites. Optimized delivery of integrase-defective lentiviral vector (IDLV) induced lower DNA load and less persistent DDR, improving clonogenic capacity and editing efficiency in long-term repopulating HSPCs. Because insertions of viral DNA fragments are less frequent with IDLV, its choice for template delivery mitigates the adverse impact and genotoxic burden of HDR editing and should facilitate its clinical translation in HSPC gene therapy.

Published

2022

7. Correcting inborn errors of immunity: From viral mediated gene addition to gene editing

Author

Maria Carmina Castiello, Samuele Ferrari, and Anna Villa

Subjects

Immunology, Immunology and Allergy

Published

2023

8. HyperIgE in hypomorphic recombination-activating gene defects

Author

Maria Carmina Castiello, Chiara Brandas, Valentina Capo, and Anna Villa

Subjects

Immunology, Immunology and Allergy

Abstract

Increased immunogloblulin-E (IgE) levels associated with eosinophilia represent a common finding observed in Omenn syndrome, a severe immunodeficiency caused by decreased V(D)J recombination, leading to restricted T- and B-cell receptor repertoire. V(D)J recombination is initiated by the lymphoid-restricted recombination-activating gene (RAG) recombinases. The lack of RAG proteins causes a block in lymphocyte differentiation, resulting in T

Published

2023

9. Towards Clinical Translation of Hematopoietic Cell Gene Editing for Treating Hyper-IgM Type 1

Author

Eugenio Scanziani, Luigi Naldini, Luisa Albano, Aurelien Jacob, Anna Villa, Claudia Asperti, Pietro Genovese, Maria Carmina Castiello, Elisabetta Mercuri, Marina Radrizzani, Genni Enza Marcovecchio, Valentina Vavassori, Elena Fontana, and Daniele Canarutto

Subjects

Hematopoietic cell, Genome editing, Immunology, Translation (biology), Cell Biology, Hematology, Computational biology, Biology, Biochemistry

Abstract

Hyper-IgM Type 1 (HIGM1) is caused by mutations of CD40L, whose absence in CD4 T cells impairs signaling for B cell activation and Ig class-switching. Since unregulated CD40L expression leads to lymphoproliferations/lymphomas in the mouse model of the disease, gene correction must preserve the physiological regulation of the gene. Gene editing of either autologous T cells or hematopoietic stem cells (HSC) held promise for treating HIGM1. We developed a "one size fits all" editing strategy to insert a 5'-truncated corrective CD40L cDNA in the first intron of the native human gene, effectively making expression conditional to targeted insertion in the intended locus. By exploiting a protocol that preserves T stem memory cells (TSCM), we reproducibly obtained ~40% of editing efficiency in healthy donor and patients derived T cells, restoring regulated, although partial, CD40L surface expression. The reconstituted level of expression, however, was sufficient to fully restore helper function to B cells. In order to select, track and potentially deplete edited T cells, we coupled the corrective cDNA with a clinically compatible selector gene and confirmed that enriched T cells preserved their engraftment capacity in NSG mice. Unexpectedly, the presence of an IRES-linked downstream coding frame counteracted the shorter half-life of transcript from the edited locus, allowing replenishment of intracellular stores and surface translocation of physiological amounts of CD40L upon activation. We also tailored the CD40L editing strategy to human HSC, reaching up to 15-30% editing in HSC long term engrafting NSG mice, depending on the HSC source. We then modelled the therapeutic potential of both T cell and HSC gene therapy by infusing increasing proportions of WT murine cells, as surrogates of edited cells, in HIGM1 mice. Administration of functional T cells at clinically relevant doses in HIGM1 mice, preconditioned or not with different lymphodepleting regimens, achieved long term stable T cell engraftment and partial rescue of antigen specific IgG response and germinal center formation in splenic follicles after vaccination with a thymus dependent antigen. Remarkably, infusion of T cells from mice pre-exposed to the antigen, mimicking treatment of chronically infected patients, was effective even in absence of conditioning and protected the mice from a disease relevant infection induced by the opportunistic pathogen Pneumocystis murina. Transplantation of functional T cells admixed with an equal number of HIGM1 T cells resulted in lower vaccination response, indicating competition between WT and HIGM1 cells and implying that increasing the fraction of corrected cells in the graft by selection would improve immune reconstitution. Concerning HSC gene therapy, transplanting 25% WT cells along with HIGM1 ones in HIGM1 mice - mirroring the editing efficiencies achieved in human HSC - rescued antigen specific IgG response and established protection from pathogen comparably to T cell therapy. These findings suggest that autologous edited T cells can provide immediate and substantial benefits to HIGM1 patients and position T cell as competitive strategy to HSC gene therapy, because of more straightforward translation, lower safety challenges and potentially comparable clinical benefits. We thus embarked in assessing GMP compliant reagents and protocols for T cell activation, culture and editing and developed a scalable manufacturing process. Optimization of clinical grade culture conditions allowed further increasing editing efficiency, total cellular yield and maintenance of TSCM thus paving the way to the design of a clinical trial. Disclosures Naldini: Genenta Science: Consultancy, Current equity holder in publicly-traded company, Membership on an entity's Board of Directors or advisory committees, Other: Founder.

Published

2021

10. Intestinal microbiota sustains inflammation and autoimmunity induced by hypomorphic RAG defects

Author

Pietro Luigi Poliani, Rosetta Pedotti, Graziano Pesole, Paolo Vezzoni, Bruno Fosso, Rosita Rigoni, Giovanni Pacchiana, Carlo Selmi, Elena Fontana, Virginia Maina, Anna Maria D'Erchia, Simone Guglielmetti, Stefano Mantero, Barbara Cassani, Valentina Taverniti, J. Rodrigo Mora, Silvia Musio, Maria Carmina Castiello, Anna Villa, and Fabio Grassi

Subjects

0301 basic medicine, microbiome, Autoimmunity, Inbred C57BL, medicine.disease_cause, Inflammatory bowel disease, Immune tolerance, Mice, 0302 clinical medicine, Intestinal mucosa, Immunology and Allergy, Intestinal Mucosa, Research Articles, Immunodeficiency, B-Lymphocytes, Colitis, Adoptive Transfer, Anti-Bacterial Agents, 3. Good health, DNA-Binding Proteins, Omenn syndrome, Immunology, Biology, digestive system, Tropism, Article, Immunophenotyping, 03 medical and health sciences, Immune system, Immune Tolerance, medicine, Animals, Inflammation, Immunoglobulin E, Th1 Cells, Immune dysregulation, Inflammatory Bowel Diseases, medicine.disease, Bacterial Load, Gastrointestinal Microbiome, Bacterial Translocation, Mice, Inbred C57BL, Myeloid Differentiation Factor 88, Th17 Cells, 030104 developmental biology, 030215 immunology

Abstract

Rigoni et al. report that hypomorphic Rag2R229Q mutation is associated with altered microbiota composition and defects in the gut–blood barrier and suggest that intestinal microbes may play a critical role in the distinctive immune dysregulation of Omenn syndrome., Omenn syndrome (OS) is caused by hypomorphic Rag mutations and characterized by a profound immunodeficiency associated with autoimmune-like manifestations. Both in humans and mice, OS is mediated by oligoclonal activated T and B cells. The role of microbial signals in disease pathogenesis is debated. Here, we show that Rag2R229Q knock-in mice developed an inflammatory bowel disease affecting both the small bowel and colon. Lymphocytes were sufficient for disease induction, as intestinal CD4 T cells with a Th1/Th17 phenotype reproduced the pathological picture when transplanted into immunocompromised hosts. Moreover, oral tolerance was impaired in Rag2R229Q mice, and transfer of wild-type (WT) regulatory T cells ameliorated bowel inflammation. Mucosal immunoglobulin A (IgA) deficiency in the gut resulted in enhanced absorption of microbial products and altered composition of commensal communities. The Rag2R229Q microbiota further contributed to the immunopathology because its transplant into WT recipients promoted Th1/Th17 immune response. Consistently, long-term dosing of broad-spectrum antibiotics (ABXs) in Rag2R229Q mice ameliorated intestinal and systemic autoimmunity by diminishing the frequency of mucosal and circulating gut-tropic CCR9+ Th1 and Th17 T cells. Remarkably, serum hyper-IgE, a hallmark of the disease, was also normalized by ABX treatment. These results indicate that intestinal microbes may play a critical role in the distinctive immune dysregulation of OS.

Published

2019

11. Lentiviral gene therapy corrects platelet phenotype and function in patients with Wiskott-Aldrich syndrome

Author

Marco Spinelli, Chiara Brombin, Nufar Marcus, Dario Di Silvestre, Patrizia Della Valle, Lucia Piceni Sereni, Maria Ester Bernardo, Pierluigi Mauri, Francesca Ferrua, Claudio Pignata, Lorella Cattaneo, Alessandro Aiuti, Lucia Dora Notarangelo, Armando D'Angelo, Marita Bosticardo, Stefania Giannelli, Koen van Rossem, Maddalena Migliavacca, Anna Villa, Loris Pozzi, Roula Farah, Maria Carmina Castiello, Maria Pia Cicalese, Sereni, L., Castiello, M. C., Di Silvestre, D., Della Valle, P., Brombin, C., Ferrua, Paolo, Cicalese, M. P., Pozzi, L., Migliavacca, M., Bernardo, M. E., Pignata, C., Farah, R., Notarangelo, L. D., Marcus, N., Cattaneo, L., Spinelli, M., Giannelli, S., Bosticardo, M., van Rossem, K., D'Angelo, A., Aiuti, A., Mauri, P., and Villa, A.

Subjects

0301 basic medicine, Male, δ-g, Electron-dense granule, P-selectin, Wiskott–Aldrich syndrome, Genetic enhancement, sCD40L, Soluble CD40 ligand, vWF, von Willebrand factor, HSCT, Hematopoietic stem cell transplantation, LV, Lentivirus, 0302 clinical medicine, Immunology and Allergy, Medicine, MFI, Mean fluorescence intensity, Platelet, Child, platelet, biology, Wiskott-Aldrich syndrome, Hematopoietic Stem Cell Transplantation, X-linked thrombocytopenia, Phenotype, gene therapy, 3. Good health, 030220 oncology & carcinogenesis, Child, Preschool, platelets, Female, PRP, Platelet-rich plasma, Wiskott-Aldrich Syndrome Protein, Adult, Blood Platelets, BAFF, B cell–activating factor, Adolescent, Immunology, Article, ADP, Adenosine diphosphate, 03 medical and health sciences, CD62P, P-selectin, Von Willebrand factor, XLT, X-linked thrombocytopenia, Microscopy, Electron, Transmission, WASp, Wiskott-Aldrich syndrome protein, HMGB1, High-mobility group box 1, Humans, B-cell activating factor, GT, Gene therapy, business.industry, TEM, Transmission electron microscopy, Platelet Count, Lentivirus, FU, Follow-up, Infant, Genetic Therapy, medicine.disease, Platelet Activation, OCS, Open canalicular system, STAT3, Signal transducer and activator of transcription 3, 030104 developmental biology, CT, Closure time, GPX1, Glutathione peroxidase 1, Platelet-rich plasma, sCD62P, Soluble P-selectin, FERMT3, Fermitin family homolog 3, WAS, Wiskott-Aldrich syndrome, biology.protein, business, HD, Healthy donor, ROS, Reactive oxygen species

Abstract

BACKGROUND: Thrombocytopenia is a serious issue for all patients with classical Wiskott-Aldrich syndrome (WAS) and X-linked thrombocytopenia (XLT) because it causes severe and life-threatening bleeding. Lentiviral gene therapy (GT) for WAS has shown promising results in terms of immune reconstitution. However, despite the reduced severity and frequency of bleeding events, platelet counts remain low in GT-treated patients. OBJECTIVE: We carefully investigated platelet defects in terms of phenotype and function in untreated patients with WAS and assessed the effect of GT treatment on platelet dysfunction. METHODS: We analyzed a cohort of 20 patients with WAS/XLT, 15 of them receiving GT. Platelet phenotype and function were analyzed by using electron microscopy, flow cytometry, and an aggregation assay. Platelet protein composition was assessed before and after GT by means of proteomic profile analysis. RESULTS: We show that platelets from untreated patients with WAS have reduced size, abnormal ultrastructure, and a hyperactivated phenotype at steady state, whereas activation and aggregation responses to agonists are decreased. GT restores platelet size and function early after treatment and reduces the hyperactivated phenotype proportionally to WAS protein expression and length of follow-up. CONCLUSIONS: Our study highlights the coexistence of morphologic and multiple functional defects in platelets lacking WAS protein and demonstrates that GT normalizes the platelet proteomic profile with consequent restoration of platelet ultrastructure and phenotype, which might explain the observed reduction of bleeding episodes after GT. These results are instrumental also from the perspective of a future clinical trial in patients with XLT only presenting with microthrombocytopenia.

Published

2019

12. Efficacy and safety of anti-CD45–saporin as conditioning agent for RAG deficiency

Author

Lucia Piceni Sereni, Nicolò Sacchetti, Paolo Uva, Rahul Palchaudhuri, Enrica Calzoni, Maria Carmina Castiello, David T. Scadden, Marita Bosticardo, Elena Fontana, Ileana Bortolomai, Yasuhiro Yamazaki, Elena Draghici, Anna Villa, Luigi D. Notarangelo, Cristina Corsino, and Hsin-Hui Yu

Subjects

0301 basic medicine, Immunoconjugates, Transplantation Conditioning, RAG deficiency, medicine.medical_treatment, Immunology, chemical and pharmacologic phenomena, Hematopoietic stem cell transplantation, medicine.disease_cause, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, conditioning, Immunology and Allergy, Medicine, Animals, Immunodeficiency, Bone Marrow Transplantation, Homeodomain Proteins, Mice, Knockout, Severe combined immunodeficiency, business.industry, anti-CD45–saporin, Antibodies, Monoclonal, immune reconstitution, Immune dysregulation, Total body irradiation, medicine.disease, Allografts, Saporins, immunotoxin, Transplantation, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, thymic epithelial cells, hematopoietic stem cell transplantation, Leukocyte Common Antigens, Severe Combined Immunodeficiency, Bone marrow, business, engraftment

Abstract

Background: Mutations in the recombinase-activating genes cause severe immunodeficiency, with a spectrum of phenotypes ranging from severe combined immunodeficiency to immune dysregulation. Hematopoietic stem cell transplantation is the only curative option, but a high risk of graft failure and poor immune reconstitution have been observed in the absence of myeloablation. Objectives: Our aim was to improve multilineage engraftment; we tested nongenotoxic conditioning with anti-CD45 mAbs conjugated with saporin CD45 (CD45-SAP). Methods: Rag1-KO and Rag1-F971L mice, which represent models of severe combined immune deficiency and combined immune deficiency with immune dysregulation, respectively, were conditioned with CD45-SAP, CD45-SAP plus 2 Gy of total body irradiation (TBI), 2 Gy of TBI, 8 Gy of TBI, or no conditioning and treated by using transplantation with lineage-negative bone marrow cells from wild-type mice. Flow cytometry and immunohistochemistry were used to assess engraftment and immune reconstitution. Antibody responses to 2,4,6-trinitrophenyl–conjugated keyhole limpet hemocyanin were measured by ELISA, and presence of autoantibody was detected by microarray. Results: Conditioning with CD45-SAP enabled high levels of multilineage engraftment in both Rag1 mutant models, allowed overcoming of B- and T-cell differentiation blocks and thymic epithelial cell defects, and induced robust cellular and humoral immunity in the periphery. Conclusions: Conditioning with CD45-SAP allows multilineage engraftment and robust immune reconstitution in mice with either null or hypomorphic Rag mutations while preserving thymic epithelial cell homeostasis., Graphical Abstract

Published

2020

13. Autonomous role of Wiskott-Aldrich Syndrome platelet deficiency in inducing autoimmunity and inflammation

Author

Sara Motta, Pierluigi Mauri, Maria Carmina Castiello, Anna Villa, Luigi D. Notarangelo, Lucia Piceni Sereni, Marita Bosticardo, Elena Draghici, Achille Anselmo, Dario Di Silvestre, Francesco Marangoni, Adrian J. Thrasher, Silvia Giliani, Stefano Mantero, Alessandro Aiuti, Sereni, Lucia, Castiello, Maria Carmina, Marangoni, Francesco, Anselmo, Achille, di Silvestre, Dario, Motta, Sara, Draghici, Elena, Mantero, Stefano, Thrasher, Adrian J, Giliani, Silvia, Aiuti, Alessandro, Mauri, Pierluigi, Notarangelo, Luigi D, Bosticardo, Marita, and Villa, Anna

Subjects

0301 basic medicine, Allergy, Wiskott–Aldrich syndrome, autoantibodies, Autoimmunity, medicine.disease_cause, Inbred C57BL, Mice, Immunology and Allergy, 2.1 Biological and endogenous factors, Platelet, Thrombopoiesis, Aetiology, Child, Mice, Knockout, biology, Chemistry, Wiskott-Aldrich syndrome, autoimmunity, Wiskott–Aldrich syndrome protein, autoantibodie, Child, Preschool, Female, CD40 ligand, medicine.symptom, Wiskott-Aldrich Syndrome Protein, Blood Platelets, Adult, Adolescent, Knockout, CD40 Ligand, Immunology, Inflammation, macromolecular substances, platelet deficiency, Article, 03 medical and health sciences, Young Adult, Rare Diseases, Clinical Research, medicine, Animals, Humans, Preschool, Platelet-poor plasma, Platelet Count, Inflammatory and immune system, Infant, medicine.disease, Mice, Inbred C57BL, 030104 developmental biology, Platelet-rich plasma, biology.protein

Abstract

BACKGROUND: Wiskott-Aldrich syndrome (WAS) is an X-linked immunodeficiency characterized by eczema, infections, and susceptibility to autoimmunity and malignancies. Thrombocytopenia is a constant finding, but its pathogenesis remains elusive. OBJECTIVE: To dissect the basis of the WAS platelet defect, we used a novel conditional mouse model (CoWas) lacking Wiskott-Aldrich syndrome protein (WASp) only in the megakaryocytic lineage in the presence of a normal immunologic environment, and in parallel we analyzed samples obtained from patients with WAS. METHODS: Phenotypic and functional characterization of megakaryocytes and platelets in mutant CoWas mice and patients with WAS with and without autoantibodies was performed. Platelet antigen expression was examined through a protein expression profile and cluster proteomic interaction network. Platelet immunogenicity was tested by using ELISAs and B-cell and platelet cocultures. RESULTS: CoWas mice showed increased megakaryocyte numbers and normal thrombopoiesis in vitro, but WASp-deficient platelets had short lifespan and high expression of activation markers. Proteomic analysis identified signatures compatible with defects in cytoskeletal reorganization and metabolism yet surprisingly increased antigen-processing capabilities. In addition, WASp-deficient platelets expressed high levels of surface and soluble CD40 ligand and were capable of inducing B-cell activation in vitro. WASp-deficient platelets were highly immunostimulatory in mice and triggered the generation of antibodies specific for WASp-deficient platelets, even in the context of a normal immune system. Patients with WAS also showed platelet hyperactivation and increased plasma soluble CD40 ligand levels correlating with the presence of autoantibodies. CONCLUSION: Overall, these findings suggest that intrinsic defects in WASp-deficient platelets decrease their lifespan and dysregulate immune responses, corroborating the role of platelets as modulators of inflammation and immunity. (J Allergy Clin Immunol.)

Published

2018

14. Efficacy Of Lentivirus-Mediated Gene Therapy In An Omenn Syndrome Recombination-Activating Gene 2 Mouse Model Is Not Hindered By Inflammation And Immune Dysregulation

Author

Anna Villa, Paola Carrera, Marita Bosticardo, Elena Fontana, Maria Carmina Castiello, Sara Penna, Monica Zanussi, Lucia Sergi Sergi, Elena Draghici, Luigi Poliani, Nicolò Sacchetti, Gerard Wagemaker, Valentina Capo, Barbara Cassani, Luigi D. Notarangelo, Niek P. van Til, Kerry Dobbs, Rosita Rigoni, Paolo Uva, İç Hastalıkları, Hematology, Capo, V, Castiello, M, Fontana, E, Penna, S, Bosticardo, M, Draghici, E, Poliani, L, Sergi Sergi, L, Rigoni, R, Cassani, B, Zanussi, M, Carrera, P, Uva, P, Dobbs, K, Sacchetti, N, Notarangelo, L, van Til, N, Wagemaker, G, and Villa, A

Subjects

Male, 0301 basic medicine, Rag gene, Allergy, T-Lymphocytes, Genetic enhancement, Immunology, Autoimmunity, Mice, Transgenic, Article, Gene therapy, Lentiviral vector, Omenn syndrome, Rag genes, Immunology and Allergy, 03 medical and health sciences, RAG2, medicine, Animals, Lymphocyte Count, Immunodeficiency, Inflammation, B-Lymphocytes, Severe combined immunodeficiency, business.industry, Lentivirus, Genetic Therapy, medicine.disease, Autoimmune regulator, 3. Good health, DNA-Binding Proteins, Mice, Inbred C57BL, Transplantation, Disease Models, Animal, 030104 developmental biology, Primary immunodeficiency, Female, Severe Combined Immunodeficiency, business

Abstract

Background Omenn syndrome (OS) is a rare severe combined immunodeficiency associated with autoimmunity and caused by defects in lymphoid-specific V(D)J recombination. Most patients carry hypomorphic mutations in recombination-activating gene ( RAG ) 1 or 2. Hematopoietic stem cell transplantation is the standard treatment; however, gene therapy (GT) might represent a valid alternative, especially for patients lacking a matched donor. Objective We sought to determine the efficacy of lentiviral vector (LV)–mediated GT in the murine model of OS (Rag2 R229Q/R229Q ) in correcting immunodeficiency and autoimmunity. Methods Lineage-negative cells from mice with OS were transduced with an LV encoding the human RAG2 gene and injected into irradiated recipients with OS. Control mice underwent transplantation with wild-type or OS-untransduced lineage-negative cells. Immunophenotyping, T-dependent and T-independent antigen challenge, immune spectratyping, autoantibody detection, and detailed tissue immunohistochemical analyses were performed. Results LV-mediated GT allowed immunologic reconstitution, although it was suboptimal compared with that seen in wild-type bone marrow (BM)−transplanted OS mice in peripheral blood and hematopoietic organs, such as the BM, thymus, and spleen. We observed in vivo variability in the efficacy of GT correlating with the levels of transduction achieved. Immunoglobulin levels and T-cell repertoire normalized, and gene-corrected mice responded properly to challenges in vivo . Autoimmune manifestations, such as skin infiltration and autoantibodies, dramatically improved in GT mice with a vector copy number/genome higher than 1 in the BM and 2 in the thymus. Conclusions Our data show that LV-mediated GT for patients with OS significantly ameliorates the immunodeficiency, even in an inflammatory environment.

Published

2018

15. IL-10 Critically Modulates B Cell Responsiveness in Rankl−/− Mice

Author

Elisabetta Traggiai, Elena Fontana, Francesca Schena, Anna Villa, Veronica Marrella, Nadia Lo Iacono, Lucia Piceni Sereni, Paolo Vezzoni, Heiko Sic, Maria Carmina Castiello, Pietro Luigi Poliani, Cristina Sobacchi, and Barbara Cassani

Subjects

musculoskeletal diseases, medicine.medical_specialty, Knockout, Regulatory B cells, Immunology, Mice, B cell homeostasis, Internal medicine, Plasma cell differentiation, medicine, Animals, Immunology and Allergy, B cell, Mice, Knockout, B-Lymphocytes, CD40, biology, Medicine (all), RANK Ligand, Germinal center, Interleukin-10, Cell biology, B-1 cell, medicine.anatomical_structure, Endocrinology, RANKL, biology.protein

Abstract

The immune and the skeletal system are tightly interconnected, and B lymphocytes are uniquely endowed with osteo-interactive properties. In this context, receptor activator of NF-κB (RANK) ligand (RANKL) plays a pivotal role in lymphoid tissue formation and bone homeostasis. Although murine models lacking RANK or RANKL show defects in B cell number, the role of the RANKL–RANK axis on B physiology is still a matter of debate. In this study, we have characterized in detail B cell compartment in Rankl−/− mice, finding a relative expansion of marginal zone B cells, B1 cells, and plasma cells associated with increased Ig serum levels, spontaneous germinal center formation, and hyperresponse to CD40 triggering. Such abnormalities were associated with an increased frequency of regulatory B cells and augmented B cell–derived IL-10 production. Remarkably, in vivo IL-10-R blockade reduced T cell–triggered plasma cell differentiation and restrained the expansion of regulatory B cells. These data point to a novel role of the RANKL–RANK axis in the regulation of B cell homeostasis and highlight an unexpected link between IL-10 CD40 signaling and the RANKL pathway.

Published

2015

16. Platelets in Wiskott-Aldrich syndrome: Victims or executioners?

Author

Maria Carmina Castiello, Anna Villa, and Lucia Piceni Sereni

Subjects

0301 basic medicine, Blood Platelets, Cellular immunity, Synapse assembly, Wiskott–Aldrich syndrome, Immunology, Autoimmunity, Cell Biology, Immune dysregulation, Biology, medicine.disease_cause, medicine.disease, Wiskott-Aldrich Syndrome, Pathogenesis, 03 medical and health sciences, 030104 developmental biology, Immune system, medicine, Immunology and Allergy, Animals, Humans, Immunodeficiency, Signal Transduction

Abstract

Microthrombocytopenia is the clinical hallmark of WAS, a rare X-linked immunodeficiency that is characterized by eczema, autoimmunity, and cancer susceptibility. This disease is caused by mutations in the WAS gene, which is expressed in hematopoietic cells and regulates actin cytoskeleton remodeling thereby modulating various cellular functions, including motility, immunologic synapse assembly, and signaling. Despite extensive studies that have provided great insight into the relevance of this molecule to innate and cellular immunity, the exact mechanisms of microthrombocytopenia in WAS are still unknown. This review focuses on the recent progress made in dissecting the pathogenesis of platelet defects in patients with WAS and their murine counterparts. In parallel, we will provide an overview of the state-of-the art platelets as immune modulators at the interface between hemostasis and the immune system, which suggests that these cells may have a direct role in the pathogenesis of immune dysregulation in WAS.

Published

2017

17. Preclinical modeling highlights the therapeutic potential of hematopoietic stem cell gene editing for correction of SCID-X1

Author

Giulia Schiroli, Anthony Conway, Samuele Ferrari, Michael C. Holmes, Luigi Naldini, Maria Carmina Castiello, Rahul Palchaudhuri, Anna Villa, Aurelien Jacob, Francesca Sanvito, Angelo Lombardo, Valentina Capo, Tiziana Plati, David T. Scadden, Chiara Bovolenta, Luisa Albano, Pietro Genovese, Giovanni Sitia, Andrew R. Gennery, Schiroli, Giulia, Ferrari, Samuele, Conway, Anthony, Jacob, Aurelien, Capo, Valentina, Albano, Luisa, Plati, Tiziana, Castiello, Maria C., Sanvito, Francesca, Gennery, Andrew R., Bovolenta, Chiara, Palchaudhuri, Rahul, Scadden, David T., Holmes, Michael C., Villa, Anna, Sitia, Giovanni, Lombardo, Angelo, Genovese, Pietro, and Naldini, Luigi

Subjects

0301 basic medicine, Mice, SCID, Computational biology, Biology, Bioinformatics, Mice, 03 medical and health sciences, Genome editing, medicine, Animals, CRISPR, Clustered Regularly Interspaced Short Palindromic Repeats, Progenitor cell, Gene Editing, Severe combined immunodeficiency, Cas9, Medicine (all), Hematopoietic stem cell, General Medicine, Hematopoietic Stem Cells, medicine.disease, Zinc finger nuclease, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Gene Targeting, Interleukin Receptor Common gamma Subunit

Abstract

Targeted genome editing in hematopoietic stem/progenitor cells (HSPCs) is an attractive strategy for treating immunohematological diseases. However, the limited efficiency of homology-directed editing in primitive HSPCs constrains the yield of corrected cells and might affect the feasibility and safety of clinical translation. These concerns need to be addressed in stringent preclinical models and overcome by developing more efficient editing methods. We generated a humanized X-linked severe combined immunodeficiency (SCID-X1) mouse model and evaluated the efficacy and safety of hematopoietic reconstitution from limited input of functional HSPCs, establishing thresholds for full correction upon different types of conditioning. Unexpectedly, conditioning before HSPC infusion was required to protect the mice from lymphoma developing when transplanting small numbers of progenitors. We then designed a one-size-fits-all IL2RG (interleukin-2 receptor common γ-chain) gene correction strategy and, using the same reagents suitable for correction of human HSPC, validated the edited human gene in the disease model in vivo, providing evidence of targeted gene editing in mouse HSPCs and demonstrating the functionality of the IL2RG-edited lymphoid progeny. Finally, we optimized editing reagents and protocol for human HSPCs and attained the threshold of IL2RG editing in long-term repopulating cells predicted to safely rescue the disease, using clinically relevant HSPC sources and highly specific zinc finger nucleases or CRISPR (clustered regularly interspaced short palindromic repeats)/Cas9 (CRISPR-associated protein 9). Overall, our work establishes the rationale and guiding principles for clinical translation of SCID-X1 gene editing and provides a framework for developing gene correction for other diseases.

Published

2017

18. Wiskott-Aldrich syndrome protein-mediated actin dynamics control type-I interferon production in plasmacytoid dendritic cells

Author

Elisa Bonomi, Ulrich Kalinke, Stefania Gobessi, Anna Villa, Marco Catucci, Ayse Metin, Luigi D. Notarangelo, Francesca Prete, Sophie Hambleton, Maria Carmina Castiello, William Vermi, Robbert G. M. Bredius, Mayrel Labrada, Mirjam van der Burg, Federica Benvenuti, Caterina Cancrini, Alessandro Aiuti, Immunology, International Centre for Genetic Engineering and Biotechnology, Padriciano 99, 34149 Trieste, Italy., Prete, Francesca, Catucci, Marco, Labrada, Mayrel, Gobessi, Stefania, Castiello Maria, Carmina, Bonomi, Elisa, Aiuti, Alessandro, Vermi, William, Cancrini, Caterina, Metin, Ayse, Hambleton, Sophie, Bredius, Robbert, Notarangelo Luigi, Daniele, van der Burg, Mirjam, Kalinke, Ulrich, Villa, Anna, and Benvenuti, Federica

Subjects

Male, Wiskott–Aldrich syndrome, Autoimmunity, Plasmacytoid dendritic cell, Receptor, Interferon alpha-beta, Mice, 0302 clinical medicine, immune system diseases, Interferon, hemic and lymphatic diseases, Immunology and Allergy, Mice, Knockout, 0303 health sciences, biology, Wiskott–Aldrich syndrome protein, hemic and immune systems, Endocytosis, Cell biology, Wiskott-Aldrich Syndrome, 3. Good health, Interferon Type I, Female, Wiskott-Aldrich Syndrome Protein, medicine.drug, Signal Transduction, congenital, hereditary, and neonatal diseases and abnormalities, Immunology, macromolecular substances, Article, 03 medical and health sciences, medicine, Animals, Humans, RNA, Messenger, 030304 developmental biology, Innate immune system, Base Sequence, TLR9, Interferon-alpha, Dendritic Cells, Cell Biology, medicine.disease, Type I interferon production, Actins, Immunity, Innate, Mice, Inbred C57BL, Disease Models, Animal, Toll-Like Receptor 9, biology.protein, Interferon type I, 030215 immunology

Abstract

Wiskott-Aldrich Syndrome protein (WASp)–mediated actin polymerization controls intracellular trafficking and compartmentalization of TLR9 ligands in plasmacytoid dendritic cells., Mutations in Wiskott-Aldrich syndrome (WAS) protein (WASp), a regulator of actin dynamics in hematopoietic cells, cause WAS, an X-linked primary immunodeficiency characterized by recurrent infections and a marked predisposition to develop autoimmune disorders. The mechanisms that link actin alterations to the autoimmune phenotype are still poorly understood. We show that chronic activation of plasmacytoid dendritic cells (pDCs) and elevated type-I interferon (IFN) levels play a role in WAS autoimmunity. WAS patients display increased expression of type-I IFN genes and their inducible targets, alteration in pDCs numbers, and hyperresponsiveness to TLR9. Importantly, ablating IFN-I signaling in WASp null mice rescued chronic activation of conventional DCs, splenomegaly, and colitis. Using WASp-deficient mice, we demonstrated that WASp null pDCs are intrinsically more responsive to multimeric agonist of TLR9 and constitutively secrete type-I IFN but become progressively tolerant to further stimulation. By acute silencing of WASp and actin inhibitors, we show that WASp-mediated actin polymerization controls intracellular trafficking and compartmentalization of TLR9 ligands in pDCs restraining exaggerated activation of the TLR9–IFN-α pathway. Together, these data highlight the role of actin dynamics in pDC innate functions and imply the pDC–IFN-α axis as a player in the onset of autoimmune phenomena in WAS disease.

Published

2013

19. Neutrophils drive type I interferon production and autoantibodies in patients with Wiskott-Aldrich syndrome

Author

Giulia Maria Piperno, Federica Benvenuti, Genni Enza Marcovecchio, Asma Naseem, Maria Carmina Castiello, Maria Pia Cicalese, Anna Villa, Elena Fontana, Luigi D. Notarangelo, Karla E Cervantes-Luevano, Marita Bosticardo, Alessandro Aiuti, Nicoletta Caronni, and Paolo Uva

Subjects

Adult, Male, 0301 basic medicine, Adolescent, Neutrophils, Immunology, Gene Expression, Plasmacytoid dendritic cell, Granulocyte, medicine.disease_cause, Extracellular Traps, Article, Autoimmunity, Young Adult, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Immunology and Allergy, B-cell activating factor, Autoantibodies, Mice, Knockout, B-Lymphocytes, biology, business.industry, Infant, Dendritic Cells, Neutrophil extracellular traps, Type I interferon production, Wiskott-Aldrich Syndrome, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Child, Preschool, Neutrophil elastase, Myeloperoxidase, Interferon Type I, biology.protein, Female, business, 030215 immunology

Abstract

Background Wiskott-Aldrich syndrome (WAS) is a rare primary immunodeficiency caused by mutations in Wiskott-Aldrich syndrome protein (WASp), a key regulator of cytoskeletal dynamics in hematopoietic cells. A high proportion of patients experience autoimmunity caused by a breakdown in T- and B-cell tolerance. Moreover, excessive production of type I interferon (IFN-I) by plasmacytoid dendritic cells (pDCs) contributes to autoimmune signs; however, the factors that trigger excessive innate activation have not been defined. Objective Neutrophil extracellular traps (NETs) emerged as major initiating factors in patients with diseases such as systemic lupus erythematosus and rheumatoid arthritis. In this study we explored the possible involvement of aberrant neutrophil functions in patients with WAS. Methods We evaluated the expression of a set of granulocyte genes associated with NETs in a cohort of patients with WAS and the presence of NET inducers in sera. Using a mouse model of WAS, we analyzed NET release by WASp-null neutrophils and evaluated the composition and homeostasis of neutrophils in vivo . By using depletion experiments, we assessed the effect of neutrophils in promoting inflammation and reactivity against autoantigens. Results Transcripts of genes encoding neutrophil enzymes and antimicrobial peptides were increased in granulocytes of patients with WAS, and serum-soluble factors triggered NET release. WASp-null neutrophils showed increased spontaneous NETosis, induced IFN-I production by pDCs, and activated B cells through B-cell activating factor. Consistently, their depletion abolished constitutive pDC activation, normalized circulating IFN-I levels, and, importantly, abolished production of autoantibodies directed against double-stranded DNA, nucleosomes, and myeloperoxidase. Conclusions These findings reveal that neutrophils are involved in the pathogenic loop that causes excessive activation of innate cells and autoreactive B cells, thus identifying novel mechanisms that contribute to the autoimmunity of WAS.

Published

2018

20. Lentiviral-mediated gene therapy restores B cell tolerance in Wiskott-Aldrich syndrome patients

Author

Marita Bosticardo, Samantha Scaramuzza, Nicolas Chamberlain, Jean Nicolas Schickel, Neil Romberg, Henner Morbach, Salomé Glauzy, Eric Meffre, Fabio Candotti, Alessandro Aiuti, Maria Carmina Castiello, Francesca Pala, Barbara Cassani, and Anna Villa

Subjects

Adult, Male, Wiskott–Aldrich syndrome, Recombinant Fusion Proteins, Molecular Sequence Data, B-cell receptor, Naive B cell, Genetic Vectors, Clonal Deletion, Receptors, Antigen, B-Cell, medicine.disease_cause, T-Lymphocytes, Regulatory, Clonal deletion, Immune tolerance, Autoimmunity, 03 medical and health sciences, 0302 clinical medicine, Bone Marrow, medicine, Immune Tolerance, Humans, Amino Acid Sequence, Child, B cell, 030304 developmental biology, 0303 health sciences, B-Lymphocytes, biology, Lentivirus, Wiskott–Aldrich syndrome protein, General Medicine, Genetic Therapy, medicine.disease, Clone Cells, 3. Good health, Wiskott-Aldrich Syndrome, medicine.anatomical_structure, Child, Preschool, Immunology, Commentary, biology.protein, Wiskott-Aldrich Syndrome Protein, 030215 immunology, Research Article

Abstract

Wiskott-Aldrich syndrome (WAS) is an X-linked immunodeficiency characterized by microthrombocytopenia, eczema, and high susceptibility to developing tumors and autoimmunity. Recent evidence suggests that B cells may be key players in the pathogenesis of autoimmunity in WAS. Here, we assessed whether WAS protein deficiency (WASp deficiency) affects the establishment of B cell tolerance by testing the reactivity of recombinant antibodies isolated from single B cells from 4 WAS patients before and after gene therapy (GT). We found that pre-GT WASp-deficient B cells were hyperreactive to B cell receptor stimulation (BCR stimulation). This hyperreactivity correlated with decreased frequency of autoreactive new emigrant/transitional B cells exiting the BM, indicating that the BCR signaling threshold plays a major role in the regulation of central B cell tolerance. In contrast, mature naive B cells from WAS patients were enriched in self-reactive clones, revealing that peripheral B cell tolerance checkpoint dysfunction is associated with impaired suppressive function of WAS regulatory T cells. The introduction of functional WASp by GT corrected the alterations of both central and peripheral B cell tolerance checkpoints. We conclude that WASp plays an important role in the establishment and maintenance of B cell tolerance in humans and that restoration of WASp by GT is able to restore B cell tolerance in WAS patients.

Published

2015

21. 481. Targeted Genome Editing in Mouse Hematopoietic Stem/Progenitor Cells (HSPC) To Model Gene Correction of SCID-X1

Author

Maria Carmina Castiello, Pietro Genovese, Philip D. Gregory, Valentina Capo, Luigi Naldini, Anna Villa, Angelo Lombardo, Giovanni Sitia, Michael C. Holmes, and Giulia Schiroli

Subjects

Pharmacology, Transgene, Genetic enhancement, Gene targeting, Transfection, Biology, Molecular biology, Cell biology, Haematopoiesis, medicine.anatomical_structure, Drug Discovery, medicine, Genetics, Molecular Medicine, Lymphopoiesis, Progenitor cell, Molecular Biology, B cell

Abstract

Targeted genome editing by artificial nucleases has brought the goal of gene correction within the reach of gene therapy. A candidate disease for HSPC gene correction is SCID-X1, because gene therapy with early generation integrating vectors showed robust clinical efficacy even from few corrected cells but also the occurrence of adverse events due to insertional mutagenesis and unregulated transgene expression. We recently reported a strategy that enabled targeted integration of a corrective cDNA into the IL2RG gene in 6% of human HSPC with high specificity. Gene corrected HSPC generated polyclonal lymphoid cells that express the IL2RG protein and have a selective growth advantage over those carrying disruptive IL2RG mutations (Genovese, Nature, 2014). Here, to model SCID-X1 disease correction, we developed a mouse model carrying the IL2RG human gene including a common disease-causing mutation in place of the murine Il2rg gene, allowing to use the same reagents utilized for gene correction of human cells. These mice have impairment in lymphoid development which phenocopies that reported for Il2rg-/- mice. To assess the minimal level of corrected HSPC required to achieve immune reconstitution we first performed competitive transplants with wild-type (WT) and Il2rg-/- HSPC and found that 1% of WT cells are sufficient to reconstitute at least in part the T and B cell compartments. We then developed a protocol to obtain gene correction in murine Lin- HSPC based on the delivery of donor DNA template by IDLVs followed by transfection of ZFN mRNAs. This protocol was associated with high on-target nuclease activity (40%) and a mean of 6% transgene integration by HDR, but also with high levels of acute cytotoxicity (65% cell loss). The surviving cells remained capable of expansion in culture and preserved their clonogenic potential. Importantly, upon transplant into lethally irradiated mice, only the gene corrected cells were able to generate lymphoid lineages (B and T cells), showing a clear selective advantage over un-corrected cells. These data indicate functional correction of the IL2RG gene by our strategy. Yet, measuring percentage of correction within myeloid cells at long-term we found that it was almost undetectable. Despite the lack of HSC marking, gene corrected lymphoid cells stably persisted in the mice up to 7 months post transplantation within all the hematopoietic organs. Furthermore, upon challenging the transplanted mice with a murine pathogen (LCMV Arm.) we observed viral-specific γIFN production by CD8+ gene corrected cells at a similar extent as for WT mice, proving in vivo the functionality of corrected T cells. These results suggest that our protocol achieves biologically relevant levels of gene correction in progenitors that sustain long-term lymphopoiesis but is limited in multipotent HSC. Ongoing studies aim to improve murine HSC gene targeting and to compare safety and efficacy of gene correction vs gene replacement in our disease model.

Published

2015

22. B-cell development and functions and therapeutic options in adenosine deaminase-deficient patients

Author

Miriam Casiraghi, Mirjam van der Burg, Maria Grazia Roncarolo, Aisha V. Sauer, Maria Pia Cicalese, Alessandro Aiuti, Stefania Giannelli, Davide Montin, Klaus Müller, Maria Carmina Castiello, Lucia Dora Notarangelo, Joris M. van Montfrans, Samantha Scaramuzza, Barbara H. Barendregt, Immacolata Brigida, Jennifer M. Puck, Jacques J.M. van Dongen, Elisabetta Traggiai, Chiara Brombin, Valentina Pistoia, Francesca Ferrua, Brigida, I, Sauer, Av, Ferrua, F, Giannelli, S, Scaramuzza, S, Pistoia, V, Castiello, Mc, Barendregt, Bh, Cicalese, Mp, Casiraghi, M, Brombin, Chiara, Puck, J, Müller, K, Notarangelo, Ld, Montin, D, van Montfrans, Jm, Roncarolo, Mg, Traggiai, E, van Dongen, Jj, van der Burg, M, Aiuti, Alessandro, Pediatrics, and Immunology

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Allergy, Adenosine Deaminase, adenosine deaminase–deficient severe combined immunodeficiency, Genetic enhancement, B-cell receptor, Immunology, Biology, Regenerative Medicine, Article, Adenosine deaminase, Gene therapy, B-Cell Activating Factor, medicine, Genetics, Immunology and Allergy, 2.1 Biological and endogenous factors, Humans, antibodies, Enzyme Replacement Therapy, Aetiology, Child, Preschool, B cell, Pediatric, Severe combined immunodeficiency, Transplantation, B-Lymphocytes, CD40, 5.2 Cellular and gene therapies, B-cell development, Inflammatory and immune system, Hematopoietic Stem Cell Transplantation, Hematopoietic stem cell, nutritional and metabolic diseases, Infant, Genetic Therapy, medicine.disease, Stem Cell Research, 3. Good health, adenosine deaminase-deficient severe combined immunodeficiency, medicine.anatomical_structure, Child, Preschool, biology.protein, Stem Cell Research - Nonembryonic - Non-Human, Bone marrow, Development of treatments and therapeutic interventions

Abstract

BACKGROUND:Adenosine deaminase (ADA) deficiency causes severe cellular and humoral immune defects and dysregulation because of metabolic toxicity. Alterations in B-cell development and function have been poorly studied. Enzyme replacement therapy (ERT) and hematopoietic stem cell (HSC) gene therapy (GT) are therapeutic options for patients lacking a suitable bone marrow (BM) transplant donor. OBJECTIVE: We sought to study alterations in B-cell development in ADA-deficient patients and investigate the ability of ERT and HSC-GT to restore normal B-cell differentiation and function. METHODS:Flow cytometry was used to characterize B-cell development in BM and the periphery. The percentage of gene-corrected B cells was measured by using quantitative PCR. B cells were assessed for their capacity to proliferate and release IgM after stimulation. RESULTS:Despite the severe peripheral B-cell lymphopenia, patients with ADA-deficient severe combined immunodeficiency showed a partial block in central BM development. Treatment with ERT or HSC-GT reverted most BM alterations, but ERT led to immature B-cell expansion. In the periphery transitional B cells accumulated under ERT, and the defect in maturation persisted long-term. HSC-GT led to a progressive improvement in B-cell numbers and development, along with increased levels of gene correction. The strongest selective advantage for ADA-transduced cells occurred at the transition from immature to naive cells. B-cell proliferative responses and differentiation to immunoglobulin secreting IgM after B-cell receptor and Toll-like receptor triggering were severely impaired after ERT and improved significantly after HSC-GT. CONCLUSIONS:ADA-deficient patients show specific defects in B-cell development and functions that are differently corrected after ERT and HSC-GT.

Published

2014

23. Wiskott-Aldrich syndrome protein deficiency in natural killer and dendritic cells affects antitumor immunity

Author

Marita Bosticardo, Anna Villa, Marco Catucci, Francesca Granucci, Daniela Cesana, Ivan Zanoni, Massimo Venturini, Elena Draghici, Eugenio Montini, Maria Carmina Castiello, Maurilio Ponzoni, Catucci, M, Zanoni, I, Draghici, E, Bosticardo, M, Castiello, M, Venturini, M, Cesana, D, Montini, E, Ponzoni, M, Granucci, F, Villa, A, Castiello, Mc, Ponzoni, Maurilio, and Villa, A.

Subjects

Lung Neoplasms, Wiskott–Aldrich syndrome, Immunology, Cell, Melanoma, Experimental, Kaplan-Meier Estimate, Lymphocyte Activation, DC, Pathogenesis, Interferon-gamma, Mice, Immune system, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Immunology and Allergy, NK cell, Cells, Cultured, Cyclin-Dependent Kinase Inhibitor p16, Bone Marrow Transplantation, Mice, Knockout, biology, Wiskott-Aldrich syndrome, Wiskott–Aldrich syndrome protein, Dendritic Cells, Flow Cytometry, medicine.disease, In vitro, Tumor Burden, Killer Cells, Natural, Mice, Inbred C57BL, Immune surveillance, medicine.anatomical_structure, biology.protein, Primary immunodeficiency, Antitumor immunity, Wiskott-Aldrich Syndrome Protein

Abstract

Wiskott-Aldrich syndrome (WAS) is a primary immunodeficiency caused by reduced or absent expression of the WAS protein (WASP). WAS patients are affected by microthrombocytopenia, recurrent infections, eczema, autoimmune diseases, and malignancies. Although immune deficiency has been proposed to play a role in tumor pathogenesis, there is little evidence on the correlation between immune cell defects and tumor susceptibility. Taking advantage of a tumor-prone model, we show that the lack of WASP induces early tumor onset because of defective immune surveillance. Consistently, the B16 melanoma model shows that tumor growth and the number of lung metastases are increased in the absence of WASP. We then investigated the in vivo contribution of Was(-/-) NK cells and DCs in controlling B16 melanoma development. We found fewer B16 metastases developed in the lungs of Was(-/-) mice that had received WT NK cells as compared with mice bearing Was(-/-) NK cells. Furthermore, we demonstrated that Was(-/-) DCs were less efficient in inducing NK-cell activation in vitro and in vivo. In summary, for the first time, we demonstrate in in vivo models that WASP deficiency affects resistance to tumor and causes impairment in the antitumor capacity of NK cells and DCs.

Published

2014

24. Wiskott-Aldrich Syndrome protein deficiency pertubs the homeostatis of B-cell compartment in humans

Author

Maria Carmina Castiello, Eric Meffre, Gertjan J. Driessen, Małgorzata Pac, Mirjam van der Burg, Samantha Scaramuzza, Elisabetta Traggiai, Francesca Pala, Nicolas Chamberlain, Aisha V. Sauer, Anna Villa, Marco Catucci, Menno C. van Zelm, Marita Bosticardo, Ewa Bernatowska, Alessandro Aiuti, Immunology, and Pediatrics

Subjects

Immunoglobulin gene, Wiskott–Aldrich syndrome, Immunology, Gene Expression, Somatic hypermutation, Autoimmunity, Article, Wiskott–Aldrich Syndrome, 03 medical and health sciences, 0302 clinical medicine, Immune system, Bone Marrow, Cell Movement, B-Cell Activating Factor, medicine, Homeostasis, Humans, Immunology and Allergy, Immunodeficiency, B cell, 030304 developmental biology, B-Lymphocytes, 0303 health sciences, Primary immunodeficiency, B lymphocyte, biology, B-cell activating factor (BAFF), Wiskott–Aldrich syndrome protein, Cell Differentiation, medicine.disease, Chemokine CXCL12, Wiskott-Aldrich Syndrome, 3. Good health, medicine.anatomical_structure, Immunoglobulin repertoire, biology.protein, Receptors, Complement 3d, Disease Susceptibility, Immunoglobulin Heavy Chains, Immunologic Memory, Wiskott-Aldrich Syndrome Protein, 030215 immunology

Abstract

Wiskott–Aldrich Syndrome protein (WASp) regulates the cytoskeleton in hematopoietic cells and mutations in its gene cause the Wiskott–Aldrich Syndrome (WAS), a primary immunodeficiency with microthrombocytopenia, eczema and a higher susceptibility to develop tumors. Autoimmune manifestations, frequently observed in WAS patients, are associated with an increased risk of mortality and still represent an unsolved aspect of the disease. B cells play a crucial role both in immune competence and self-tolerance and defects in their development and function result in immunodeficiency and/or autoimmunity. We performed a phenotypical and molecular analysis of central and peripheral B-cell compartments in WAS pediatric patients. We found a decreased proportion of immature B cells in the bone marrow correlating with an increased presence of transitional B cells in the periphery. These results could be explained by the defective migratory response of WAS B cells to SDF-1α, essential for the retention of immature B cells in the BM. In the periphery, we observed an unusual expansion of CD21low B-cell population and increased plasma BAFF levels that may contribute to the high susceptibility to develop autoimmune manifestations in WAS patients. WAS memory B cells were characterized by a reduced in vivo proliferation, decreased somatic hypermutation and preferential usage of IGHV4-34, an immunoglobulin gene commonly found in autoreactive B cells. In conclusion, our findings demonstrate that WASp-deficiency perturbs B-cell homeostasis thus adding a new layer of immune dysregulation concurring to the increased susceptibility to develop autoimmunity in WAS patients., Highlights • WASp-deficiency affects both central and peripheral B-cell development. • An early egress of immature B cells leads to an increase of transitional B cells in periphery. • Reduced maturation status of WAS memory B cells. • Altered selection of both protective and autoreactive Ig gene families in WAS patients. • Potentially autoreactive CD21low B cells are expanded in WAS patients.

Published

2014

25. Preclinical Safety and Efficacy of Human CD34(+) Cells Transduced With Lentiviral Vector for the Treatment of Wiskott-Aldrich Syndrome

Author

Maria G. Roncarolo, Robbert G. M. Bredius, Maria Carmina Castiello, Marita Bosticardo, Anna Villa, Monica Salomoni, Marco Ranzani, Mariana Loperfido, Elisa Vicenzi, Anna Ripamonti, Raisa Jofra Hernandez, Luca Biasco, Christof von Kalle, Samantha Scaramuzza, Fabrizio Benedicenti, Alessandra Biffi, Manfred Schmidt, Alessandro Aiuti, Elena Draghici, Luigi Naldini, Eugenio Montini, Andrea Finocchi, Cynthia C. Bartholomae, Marina Radrizzani, Scaramuzza, S1, Biasco, L, Ripamonti, A, Castiello, Mc, Loperfido, M, Draghici, E, Hernandez, Rj, Benedicenti, F, Radrizzani, M, Salomoni, M, Ranzani, M, Bartholomae, Cc, Vicenzi, E, Finocchi, A, Bredius, R, Bosticardo, M, Schmidt, M, von Kalle, C, Montini, E, Biffi, A, Roncarolo, MARIA GRAZIA, Naldini, Luigi, Villa, A, and Aiuti, A.

Subjects

Wiskott–Aldrich syndrome, Genetic enhancement, Knockout, Genetic Vectors, CD34, Bone Marrow Cells, Biology, Viral vector, 03 medical and health sciences, Mice, Transduction, 0302 clinical medicine, Genetic, Drug Discovery, medicine, Genetics, Animals, Progenitor cell, Antigens, Molecular Biology, 030304 developmental biology, Interleukin 3, Bone Marrow Transplantation, Pharmacology, 0303 health sciences, Antigens, CD34, Lentivirus, Mice, Knockout, Wiskott-Aldrich Syndrome, Transduction, Genetic, medicine.disease, 3. Good health, Haematopoiesis, medicine.anatomical_structure, Settore MED/03 - Genetica Medica, 030220 oncology & carcinogenesis, Immunology, Molecular Medicine, Original Article, Bone marrow

Abstract

"Gene therapy with ex vivo-transduced hematopoietic stem/progenitor cells may represent a valid therapeutic option for monogenic immunohematological disorders such as Wiskott-Aldrich syndrome (WAS), a primary immunodeficiency associated with thrombocytopenia. We evaluated the preclinical safety and efficacy of human CD34+ cells transduced with lentiviral vectors (LV) encoding WAS protein (WASp). We first set up and validated a transduction protocol for CD34+ cells derived from bone marrow (BM) or mobilized peripheral blood (MPB) using a clinical grade, highly purified LV. Robust transduction of progenitor cells was obtained in normal donors and WAS patients' cells, without evidence of toxicity. To study biodistribution of human cells and exclude vector release in vivo, LV-transduced CD34+ cells were transplanted in immunodeficient mice, showing a normal engraftment and differentiation ability towards transduced lymphoid and myeloid cells in hematopoietic tissues. Vector mobilization to host cells and transmission to germline cells of the LV were excluded by different molecular assays. Analysis of vector integrations showed polyclonal integration patterns in vitro and in human engrafted cells in vivo. In summary, this work establishes the preclinical safety and efficacy of human CD34+ cells gene therapy for the treatment of WAS."

Published

2013

26. Lentiviral hematopoietic stem cell gene therapy in patients with Wiskott-Aldrich syndrome

Author

Maria Grazia Valsecchi, Fabio Ciceri, Jason P. Gardner, Anne Galy, Andrea Finocchi, Clelia Di Serio, Anna Villa, Alessandro Aiuti, Danilo Pellin, Paolo Rizzardi, David J. Dow, Marita Bosticardo, Jordan S. Orange, Maria Pia Cicalese, Stefania Giannelli, Pinaki P. Banerjee, Maria Grazia Roncarolo, Luigi Naldini, Victor Neduva, Luca Biasco, Ayse Metin, Roberto Miniero, Alessandra Biffi, Francesca Ferrua, Stefania Galimberti, Manfred G. Schmidt, Samantha Scaramuzza, Sara Di Nunzio, Maria Carmina Castiello, Miriam Casiraghi, Francesca Dionisio, Luciano Callegaro, Cristina Baricordi, Andrea Assanelli, Nalini Mehta, Eugenio Montini, Andrea Calabria, Claudia Benati, Christof von Kalle, Costanza Evangelio, Aiuti, Alessandro, Biasco, L, Scaramuzza, S, Ferrua, F, Cicalese, Mp, Baricordi, C, Dionisio, F, Calabria, A, Giannelli, S, Castiello, Mc, Bosticardo, M, Evangelio, C, Assanelli, A, Casiraghi, M, Di Nunzio, S, Callegaro, L, Benati, C, Rizzardi, P, Pellin, D, DI SERIO, Mariaclelia, Schmidt, M, Von Kalle, C, Gardner, J, Mehta, N, Neduva, V, Dow, Dj, Galy, A, Miniero, R, Finocchi, A, Metin, A, Banerjee, Pp, Orange, J, Galimberti, S, Valsecchi, Mg, Biffi, A, Montini, E, Villa, A, Ciceri, Fabio, Roncarolo, MARIA GRAZIA, Naldini, Luigi, IRCCS San Raffaele Scientific Institute [Milan, Italie], Hematology and BMT Unit, San Raffaele Scientific Institute, Unit of Lymphoid Malignancies, CHU Necker - Enfants Malades [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Immunologie moléculaire et biothérapies innovantes (IMBI), École Pratique des Hautes Études (EPHE), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Université d'Évry-Val-d'Essonne (UEVE)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Généthon, Ospedale San Raffaele, École pratique des hautes études (EPHE), Biasco, Luca, Scaramuzza, Samantha, Ferrua, Francesca, Cicalese, Maria Pia, Baricordi, Cristina, Dionisio, Francesca, Calabria, Andrea, Giannelli, Stefania, Castiello, Maria Carmina, Bosticardo, Marita, Evangelio, Costanza, Assanelli, Andrea, Casiraghi, Miriam, Di Nunzio, Sara, Callegaro, Luciano, Benati, Claudia, Rizzardi, Paolo, Pellin, Danilo, Di Serio, Clelia, Schmidt, Manfred, Von Kalle, Christof, Gardner, Jason, Mehta, Nalini, Neduva, Victor, Dow, David J., Galy, Anne, Miniero, Roberto, Finocchi, Andrea, Metin, Ayse, Banerjee, Pinaki P., Orange, Jordan S., Galimberti, Stefania, Valsecchi, Maria Grazia, Biffi, Alessandra, Montini, Eugenio, Villa, Anna, Roncarolo, Maria Grazia, Aiuti, A, Cicalese, M, Castiello, M, Di Serio, C, Dow, D, Banerjee, P, Valsecchi, M, Ciceri, F, Roncarolo, M, Naldini, L, and Généthon

Subjects

Male, Wiskott–Aldrich syndrome, medicine.medical_treatment, Genetic enhancement, Hematopoietic Stem Cells/*metabolism, [SDV]Life Sciences [q-bio], Hematopoietic stem cell transplantation, Genetic Therapy/*methods, 0302 clinical medicine, Transduction, Genetic, Child, 0303 health sciences, Multidisciplinary, biology, Wiskott–Aldrich syndrome protein, Hematopoietic Stem Cell Transplantation, Hematopoietic stem cell, Gene Therapy, 3. Good health, Wiskott-Aldrich Syndrome, Haematopoiesis, medicine.anatomical_structure, 030220 oncology & carcinogenesis, [SDV.IMM]Life Sciences [q-bio]/Immunology, Genetic Vector, Wiskott-Aldrich Syndrome Protein, Human, Virus Integration, Genetic Vectors, Wiskott-Aldrich Syndrome/*therapy, Wiskott-Aldrich Syndrome Protein/*genetics, Lentiviru, Viral vector, 03 medical and health sciences, Transduction, Genetic, medicine, Humans, Progenitor cell, 030304 developmental biology, Settore MED/38 - Pediatria Generale e Specialistica, business.industry, Lentivirus, Hematopoietic Stem Cell, Genetic Therapy, medicine.disease, Hematopoietic Stem Cells, Immunology, biology.protein, business

Abstract

Next-Generation Gene Therapy Few disciplines in contemporary clinical research have experienced the high expectations directed at the gene therapy field. However, gene therapy has been challenging to translate to the clinic, often because the therapeutic gene is expressed at insufficient levels in the patient or because the gene delivery vector integrates near protooncogenes, which can cause leukemia (see the Perspective by Verma ). Biffi et al. ( 1233158 , published online 11 July) and Aiuti et al. ( 1233151 ; published online 11 July) report progress on both fronts in gene therapy trials of three patients with metachromatic leukodystrophy (MLD), a neurodegenerative disorder, and three patients with Wiskott-Aldrich syndrome (WAS), an immunodeficiency disorder. Optimized lentiviral vectors were used to introduce functional MLD or WAS genes into the patients' hematopoietic stem cells (HSCs) ex vivo, and the transduced cells were then infused back into the patients, who were then monitored for up to 2 years. In both trials, the patients showed stable engraftment of the transduced HSC and high expression levels of functional MLD or WAS genes. Encouragingly, there was no evidence of lentiviral vector integration near proto-oncogenes, and the gene therapy treatment halted disease progression in most patients. A longer follow-up period will be needed to further validate efficacy and safety.

Published

2013

27. Corrigendum to 'Preclinical Safety and Efficacy of Human CD34+ Cells Transduced With Lentiviral Vector for the Treatment of Wiskott-Aldrich Syndrome'

Author

Elisa Vicenzi, Monica Salomoni, Raisa Jofra Hernandez, Marco Ranzani, Maria Grazia Roncarolo, Mariana Loperfido, Anna Villa, Manfred G. Schmidt, Luca Biasco, Marita Bosticardo, Cynthia C. Bartholomae, Maria Carmina Castiello, Christof von Kalle, Anna Ripamonti, Eugenio Montini, Robbert G. M. Bredius, Andrea Finocchi, Marina Radrizzani, Elena Draghici, Luigi Naldini, Samantha Scaramuzza, Alessandro Aiuti, Fabrizio Benedicenti, and Alessandra Biffi

Subjects

Mice, Knockout, Pharmacology, Wiskott–Aldrich syndrome, business.industry, Cd34 cells, Genetic Vectors, Lentivirus, Antigens, CD34, Bone Marrow Cells, medicine.disease, Virology, Molecular therapy, Wiskott-Aldrich Syndrome, Viral vector, Mice, Transduction, Genetic, Drug Discovery, Genetics, medicine, Animals, Molecular Medicine, Corrigendum, business, Molecular Biology, Bone Marrow Transplantation

Abstract

Gene therapy with ex vivo-transduced hematopoietic stem/progenitor cells may represent a valid therapeutic option for monogenic immunohematological disorders such as Wiskott-Aldrich syndrome (WAS), a primary immunodeficiency associated with thrombocytopenia. We evaluated the preclinical safety and efficacy of human CD34(+) cells transduced with lentiviral vectors (LV) encoding WAS protein (WASp). We first set up and validated a transduction protocol for CD34(+) cells derived from bone marrow (BM) or mobilized peripheral blood (MPB) using a clinical grade, highly purified LV. Robust transduction of progenitor cells was obtained in normal donors and WAS patients' cells, without evidence of toxicity. To study biodistribution of human cells and exclude vector release in vivo, LV-transduced CD34(+) cells were transplanted in immunodeficient mice, showing a normal engraftment and differentiation ability towards transduced lymphoid and myeloid cells in hematopoietic tissues. Vector mobilization to host cells and transmission to germline cells of the LV were excluded by different molecular assays. Analysis of vector integrations showed polyclonal integration patterns in vitro and in human engrafted cells in vivo. In summary, this work establishes the preclinical safety and efficacy of human CD34(+) cells gene therapy for the treatment of WAS.

Published

2016

28. 280. Lentiviral-Mediated Gene Therapy Restores B Cell Homeostasis and Tolerance in Wiskott-Aldrich Syndrome Patients

Author

Mirjam van der Burg, Eric Meffre, Fabio Candotti, Neil Romberg, Luigi Naldini, Maria Carmina Castiello, Francesca Ferrua, Nicolas Chamberlain, Marita Bosticardo, Francesca Pala, Samantha Scaramuzza, Anna Villa, Henner Morbach, Jean-Nicolas Schickel, and Alessandro Aiuti

Subjects

Pharmacology, Wiskott–Aldrich syndrome, Genetic enhancement, Naive B cell, Hematopoietic stem cell, Biology, medicine.disease, B-1 cell, medicine.anatomical_structure, B cell homeostasis, Drug Discovery, Immunology, Genetics, medicine, Molecular Medicine, Progenitor cell, Molecular Biology, B cell

Abstract

Wiskott-Aldrich Syndrome (WAS) is a severe X-linked primary immunodeficiency characterized by micro-thrombocytopenia, eczema and increased risk of infections, autoimmunity and tumors. Allogeneic hematopoietic stem cell (HSC) transplantation is a recognized curative treatment for WAS, but when a matched donor is not available, administration of WAS gene-corrected autologous HSCs represents a valid alternative therapeutic approach. Since alterations of WAS protein (WASp)-deficient B lymphocytes contribute to immunodeficiency and autoimmunity in WAS, we followed the B cell reconstitution in 4 WAS patients treated by lentiviral vector-gene therapy (GT) after a reduced-intensity conditioning regimen combined with anti-CD20 administration. We analyzed the B cell subset distribution in the bone marrow and peripheral blood by flow cytometry and the autoantibody profile by a high-throughput autoantigen microarray platform before and after GT. Lentiviral vector-transduced progenitor cells were able to repopulate the B cell compartment with a normal distribution of transitional, naive and memory B cells. The reduction in the proportion of autoimmune-associated CD21low B cells and in the plasma levels of B cell-activating factor was associated with the decreased autoantibody production in WAS patients after GT. Then, we evaluated the functionality of B cell tolerance checkpoints by testing the reactivity of recombinant antibodies isolated from single B cells. Before GT, we found a decreased frequency of autoreactive new emigrant/transitional B cells in WAS patients, suggesting a hyperfunctional central B cell checkpoint in the absence of WASp. In contrast, high frequency of polyreactive and Hep2 reactive clones were found in mature naive B cells of WAS patients, indicating a defective peripheral B cell checkpoint. Both central and peripheral B cell tolerance checkpoints were restored after GT, further supporting the qualitative efficacy of this treatment. In conclusion, WASp plays an important role in the regulation of B cell homeostasis and in the establishment of B cell tolerance in humans and lentiviral-mediated GT is able to ameliorate the functionality of B cell compartment contributing to the clinical and immunological improvement in WAS patients.

Published

2016

29. Dendritic cell functional improvement in a preclinical model of lentiviral-mediated gene therapy for Wiskott-Aldrich syndrome

Author

Federica Benvenuti, Francesca Prete, Maria Carmina Castiello, Maria Grazia Roncarolo, Marita Bosticardo, Alessandro Aiuti, Anna Villa, Marco Catucci, Michela Locci, Elena Draghici, Catucci, M, Prete, F, Bosticardo, M, Castiello, M, Draghici, E, Locci, M, Roncarolo, MARIA GRAZIA, Aiuti, Alessandro, Benvenuti, F, and Villa, A.

Subjects

dendritic cell, Lymphoid Tissue, Genetic enhancement, gene-corrected cell therapy, Bone Marrow Cells, Article, Viral vector, Transduction, Mice, Gene therapy, Genetic, Phagocytosis, In vivo, Transduction, Genetic, Cell Movement, Models, Genetics, Animals, Dendritic Cells, Humans, Genetic Therapy, Wiskott-Aldrich Syndrome Protein, Wiskott-Aldrich Syndrome, Lentivirus, Models, Genetic, Molecular Biology, Settore MED/38 - Pediatria Generale e Specialistica, biology, Wiskott–Aldrich syndrome protein, Dendritic cell, Ovalbumin, Haematopoiesis, Wiskott -- Aldrich syndrome, Immunology, biology.protein, Cancer research, Molecular Medicine, Stem cell

Abstract

Wiskott-Aldrich syndrome (WAS) is a rare X-linked primary immunodeficiency caused by the defective expression of the WAS protein (WASP) in hematopoietic cells. It has been shown that dendritic cells (DCs) are functionally impaired in WAS patients and was(-/-) mice. We have previously demonstrated the efficacy and safety of a murine model of WAS gene therapy (GT), using stem cells transduced with a lentiviral vector (LV). The aim of this study was to investigate whether GT can correct DC defects in was(-/-) mice. As DCs expressing WASP were detected in the secondary lymphoid organs of the treated mice, we tested the in vitro and in vivo function of bone marrow-derived DCs (BMDCs). The BMDCs showed efficient in vitro uptake of latex beads and Salmonella typhimurium. When BMDCs from the treated mice (GT BMDCs) and the was(-/-) mice were injected into wild-type hosts, we found a higher number of cells that had migrated to the draining lymph nodes compared with mice injected with was(-/-) BMDCs. Finally, we found that ovalbumin (OVA)-pulsed GT BMDCs or vaccination of GT mice with anti-DEC205 OVA fusion protein can efficiently induce antigen-specific T-cell activation in vivo. These findings show that WAS GT significantly improves DC function, thus adding new evidence of the preclinical efficacy of LV-mediated WAS GT.

Published

2012

30. SOCS1 gene transfer accelerates the transition to heart failure through the inhibition of the gp130/JAK/STAT pathway

Author

Gianluigi Condorelli, Alberto M. Marra, Matthew J. During, Maria Chiara Monti, Valentina Petrillo, Luigi Saccà, Antonio Cittadini, Alfonso Baldi, Eduardo Bossone, Maria Carmina Castiello, Lavinia Saldamarco, Guido Iaccarino, Salvatore Longobardi, Cittadini, Antonio, Monti, MARIA GAIA, Iaccarino, G., Castiello, M. C., Baldi, A., Bossone, E., Longobardi, S., Marra, ALBERTO MARIA, Petrillo, V., Saldamarco, Lavinia, During, M. J., Sacca', Luigi, Condorelli, G., Cittadini, A, Monti, Mg, Iaccarino, Gennarfrancesco, Castiello, Mc, Baldi, Alfonso, Bossone, E, Longobardi, S, Marra, Am, Petrillo, V, Saldamarco, L, During, Mj, and Saccà, L

Subjects

Male, Vascular Endothelial Growth Factor A, Time Factors, Physiology, medicine.medical_treatment, Messenger, Left, Wistar, Apoptosis, Suppressor of Cytokine Signaling Proteins, Ventricular Function, Left, Cytokine Receptor gp130, Ventricular Function, SOCS3, Phosphorylation, Ultrasonography, Janus kinase 1, Gene Transfer Techniques, JAK-STAT signaling pathway, Dependovirus, SOCS, Left Ventricular, Up-Regulation, Angiopoietin-2, Animals, Disease Models, Animal, Disease Progression, Genetic Vectors, Heart Failure, Hemodynamics, Hypertrophy, Left Ventricular, Janus Kinase 1, Myocardium, RNA, Messenger, Rats, Rats, Wistar, STAT3 Transcription Factor, Signal Transduction, Cardiac hypertrophy, Cytokine, Cardiology and Cardiovascular Medicine, medicine.medical_specialty, Biology, Gene therapy, Suppressor of Cytokine Signaling 1 Protein, Physiology (medical), Internal medicine, medicine, Pressure overload, Suppressor of cytokine signaling 1, Animal, Original Articles, Hypertrophy, Glycoprotein 130, Suppressor of Cytokine Signaling 3 Protein, Endocrinology, Disease Models, Cancer research, RNA, Janus kinase

Abstract

Aims The suppressors of cytokine signalling (SOCS) are identified inhibitors of cytokine and growth factor signalling that act via the Janus kinase (JAK) signal transducers and activators of transcription (STAT) pathways. Aberrant JAK/STAT signalling promotes progression from hypertrophy to heart failure. Little information is available concerning the role of SOCS in the transition from hypertrophy to heart failure. To this aim, we investigated the effects of SOCS1 overexpression obtained by in vivo adeno-associated gene transfer using an aortopulmonary cross-clamping technique in a chronic pressure-overload cardiac rat model. Methods and results Rats were randomized into four groups: sham-operated ( n = 18), aortic banding (AB) ( n = 18), AB + viral vector encoding for haemoagglutinin (AB + HA, n = 16), and AB + viral vector encoding for SOCS1 (AB + SOCS1, n = 18). Echocardiographic and haemodynamic measurements were performed 15 weeks after banding. While SOCS3 was upregulated during the hypertrophic phase, SOCS1 transcript levels increased significantly between 15 and 20 weeks. Remodelling was markedly worse in AB + SOCS1, showed larger left ventricular internal dimensions (+16%), higher end-diastolic pressures (+57%) and wall stress (+45%), and reduced fractional shortening (−32%) compared with AB + HA; apoptotic rate was increased three­fold and the gp130 pathway was inhibited. Ex vivo experiments showed that mechanical stretch upregulated SOCS1 expression, which was in turn attenuated by tumour necrosis factor-α (TNF-α) inhibition. Conclusion Enhanced SOCS1 myocardial signalling is associated with accelerated transition from hypertrophy to failure in an established model of pressure overload. SOCS1 may represent an attractive target for the prevention of heart failure progression.

Published

2012

31. Lentiviral-mediated gene therapy leads to improvement of B-cell functionality in a murine model of Wiskott-Aldrich syndrome

Author

Elisabetta Traggiai, Elena Fontana, Maria Grazia Roncarolo, Marita Bosticardo, Pietro Luigi Poliani, Aisha V. Sauer, Francesca Schena, Maria Carmina Castiello, Alessandro Aiuti, Anna Villa, Marco Catucci, Elena Draghici, Luigi Naldini, Michela Locci, Bosticardo, M, Draghici, E, Schena, F, Sauer, Av, Fontana, E, Castiello, Mc, Catucci, M, Locci, M, Naldini, Luigi, Aiuti, Alessandro, Roncarolo, MARIA GRAZIA, Poliani, Pl, Traggiai, E, and Villa, A.

Subjects

Wiskott–Aldrich syndrome, Genetic enhancement, Genetic Vectors, Immunology, Gene Expression, B-cell, Biology, Viral vector, murine model, Mice, medicine, Animals, Humans, Immunology and Allergy, B cell, Autoantibodies, Bone Marrow Transplantation, Mice, Knockout, B-Lymphocytes, Wiskott-Aldrich syndrome, Lentivirus, Hematopoietic stem cell, Genetic Therapy, medicine.disease, Antigens, T-Independent, Molecular biology, gene therapy, Recombinant Proteins, Mice, Inbred C57BL, Transplantation, Disease Models, Animal, medicine.anatomical_structure, Bone marrow, Stem cell, Wiskott-Aldrich Syndrome Protein

Abstract

"\"Background: Wiskott-Aldrich syndrome (WAS) is an X-linked primary immunodeficiency characterized by thrombocytopenia, eczema, infections, autoimmunity, and lymphomas. Transplantation of hematopoietic stem cells from HLA-identical donors is curative, but it is not available to all patients. We have developed a gene therapy (GT) approach for WAS by using a lentiviral vector encoding for human WAS promoter\\\/cDNA (w1.6W) and demonstrated its preclinical efficacy and safety. Objective: To evaluate B-cell reconstitution and correction of B-cell phenotype in GT-treated mice. Methods: We transplanted Was(-\\\/-) mice sublethally irradiated (700 rads) with lineage marker-depleted bone marrow wild-type cells, Was(-\\\/-) cells untransduced or transduced with the w1.6W lentiviral vector and analyzed B-cell reconstitution in bone marrow, spleen, and peritoneum. Results: Here we show that WAS protein(+) B cells were present in central and peripheral B-cell compartments from GT-treated mice and displayed the strongest selective advantage in the splenic marginal zone and peritoneal B1 cell subsets. After GT, splenic architecture was improved and B-cell functions were restored, as demonstrated by the improved antibody response to pneumococcal antigens and the reduction of serum IgG autoantibodies. Conclusion: WAS GT leads to improvement of B-cell functions, even in the presence of a mixed chimerism, further validating the clinical application of the w1.6W lentiviral vector. (J Allergy Clin Immunol 2011;127:1376-84.)\"" BACKGROUND: Wiskott-Aldrich syndrome (WAS) is an X-linked primary immunodeficiency characterized by thrombocytopenia, eczema, infections, autoimmunity, and lymphomas. Transplantation of hematopoietic stem cells from HLA-identical donors is curative, but it is not available to all patients. We have developed a gene therapy (GT) approach for WAS by using a lentiviral vector encoding for human WAS promoter/cDNA (w1.6W) and demonstrated its preclinical efficacy and safety. OBJECTIVE: To evaluate B-cell reconstitution and correction of B-cell phenotype in GT-treated mice. METHODS: We transplanted Was(-/-) mice sublethally irradiated (700 rads) with lineage marker-depleted bone marrow wild-type cells, Was(-/-) cells untransduced or transduced with the w1.6W lentiviral vector and analyzed B-cell reconstitution in bone marrow, spleen, and peritoneum. RESULTS: Here we show that WAS protein(+) B cells were present in central and peripheral B-cell compartments from GT-treated mice and displayed the strongest selective advantage in the splenic marginal zone and peritoneal B1 cell subsets. After GT, splenic architecture was improved and B-cell functions were restored, as demonstrated by the improved antibody response to pneumococcal antigens and the reduction of serum IgG autoantibodies. CONCLUSION: WAS GT leads to improvement of B-cell functions, even in the presence of a mixed chimerism, further validating the clinical application of the w1.6W lentiviral vector.

Published

2011

32. Revertant T lymphocytes in a patient with Wiskott-Aldrich syndrome: analysis of function and distribution in lymphoid organs

Author

Sara Trifari, Marita Bosticardo, Ronan Calvez, William Vermi, Robert Chiesa, Maurilio Ponzoni, Luca Mollica, Maria Grazia Roncarolo, Fanny Lafouresse, Loïc Dupré, Daniela Medicina, Francesco Marangoni, Maurizio Caniglia, Anna Villa, Marco Catucci, Maria Carmina Castiello, Claudio Doglioni, Federica Cattaneo, Samantha Scaramuzza, Alessandro Aiuti, Trifari, S, Scaramuzza, S, Catucci, M, Ponzoni, Maurilio, Mollica, L, Chiesa, R, Cattaneo, F, Lafouresse, F, Calvez, R, Vermi, W, Medicina, D, Castiello, Mc, Marangoni, F, Bosticardo, M, Doglioni, Claudio, Caniglia, M, Aiuti, Alessandro, Villa, A, Roncarolo, MARIA GRAZIA, and Dupre, L.

Subjects

Adult, Male, Wiskott–Aldrich syndrome, Lymphoid Tissue, T-Lymphocytes, Immunology, Blotting, Western, DNA Mutational Analysis, Molecular Sequence Data, Cell Separation, medicine.disease_cause, Polymerase Chain Reaction, Immune system, Germline mutation, medicine, Immunology and Allergy, Humans, Amino Acid Sequence, Immunodeficiency, Settore MED/38 - Pediatria Generale e Specialistica, Mutation, Microscopy, Confocal, biology, Base Sequence, Mosaicism, Wiskott–Aldrich syndrome protein, medicine.disease, Flow Cytometry, Wiskott-Aldrich Syndrome, Lymphatic system, biology.protein, Primary immunodeficiency, Wiskott-Aldrich Syndrome Protein

Abstract

Background: The Wiskott-Aldrich syndrome (WAS) is a rare genetic disease characterized by thrombocytopenia, immunodeficiency, autoimmunity, and hematologic malignancies. Secondary mutations leading to re-expression of WAS protein (WASP) are relatively frequent in patients with WAS. Objective: The tissue distribution and function of revertant cells were investigated in a novel case of WAS gene secondary mutation. Methods: A vast combination of approaches was used to characterize the second-site mutation, to investigate revertant cell function, and to track their distribution over a 18-year clinical follow-up. Results: The WAS gene secondary mutation was a 4-nucleotide insertion, 4 nucleotides downstream of the original deletion. This somatic mutation allowed the T-cell-restricted expression of a stable, full-length WASP with a 3-amino acid change compared with the wild-type protein. WASP(+) T cells appeared early in the spleen (age 10 years) and were highly enriched in a mesenteric lymph node at a later time (age 23 years). Revertant T cells had a diversified T-cell-receptor repertoire and displayed in vitro and in vivo selective advantage. They proliferated and produced cytokines normally on T-cell-receptor stimulation. Consistently, the revertant WASP correctly localized to the immunologic synapse and to the leading edge of migrating T cells. Conclusion: Despite the high proportion of functional revertant T cells, the patient still has severe infections and autoimmune disorders, suggesting that re-expression of WASP in T cells is not sufficient to normalize immune functions fully in patients with WAS. (J Allergy Clin Immunol 2010;125:439-48.) Background: The Wiskott-Aldrich syndrome (WAS) is a rare genetic disease characterized by thrombocytopenia, immunodeficiency, autoimmunity, and hematologic malignancies. Secondary mutations leading to re-expression of WAS protein (WASP) are relatively frequent in patients with WAS. Objective: The tissue distribution and function of revertant cells were investigated in a novel case of WAS gene secondary mutation. Methods: A vast combination of approaches was used to characterize the second-site mutation, to investigate revertant cell function, and to track their distribution over a 18-year clinical follow-up. Results: The WAS gene secondary mutation was a 4-nucleotide insertion, 4 nucleotides downstream of the original deletion. This somatic mutation allowed the T-cell-restricted expression of a stable, full-length WASP with a 3-amino acid change compared with the wild-type protein. WASP(+) T cells appeared early in the spleen (age 10 years) and were highly enriched in a mesenteric lymph node at a later time (age 23 years). Revertant T cells had a diversified T-cell-receptor repertoire and displayed in vitro and in vivo selective advantage. They proliferated and produced cytokines normally on T-cell-receptor stimulation. Consistently, the revertant WASP correctly localized to the immunologic synapse and to the leading edge of migrating T cells. Conclusion: Despite the high proportion of functional revertant T cells, the patient still has severe infections and autoimmune disorders, suggesting that re-expression of WASP in T cells is not sufficient to normalize immune functions fully in patients with WAS. (J Allergy Clin Immunol 2010;125:439-48.) BACKGROUND: The Wiskott-Aldrich syndrome (WAS) is a rare genetic disease characterized by thrombocytopenia, immunodeficiency, autoimmunity, and hematologic malignancies. Secondary mutations leading to re-expression of WAS protein (WASP) are relatively frequent in patients with WAS. OBJECTIVE: The tissue distribution and function of revertant cells were investigated in a novel case of WAS gene secondary mutation. METHODS: A vast combination of approaches was used to characterize the second-site mutation, to investigate revertant cell function, and to track their distribution over a 18-year clinical follow-up. RESULTS: The WAS gene secondary mutation was a 4-nucleotide insertion, 4 nucleotides downstream of the original deletion. This somatic mutation allowed the T-cell-restricted expression of a stable, full-length WASP with a 3-amino acid change compared with the wild-type protein. WASP(+) T cells appeared early in the spleen (age 10 years) and were highly enriched in a mesenteric lymph node at a later time (age 23 years). Revertant T cells had a diversified T-cell-receptor repertoire and displayed in vitro and in vivo selective advantage. They proliferated and produced cytokines normally on T-cell-receptor stimulation. Consistently, the revertant WASP correctly localized to the immunologic synapse and to the leading edge of migrating T cells. CONCLUSION: Despite the high proportion of functional revertant T cells, the patient still has severe infections and autoimmune disorders, suggesting that re-expression of WASP in T cells is not sufficient to normalize immune functions fully in patients with WAS. Copyright 2010 American Academy of Allergy, Asthma & Immunology. Published by Mosby, Inc. All rights reserved.

Published

2009

33. Safety and Clinical Benefit of Lentiviral Hematopoietic Stem Cell Gene Therapy for Wiskott-Aldrich Syndrome

Author

Francesca Ferrua, Maria Carmina Castiello, Marita Bosticardo, Anna Villa, Jordan S. Orange, Stefania Giannelli, Miriam Casiraghi, Luigi Naldini, Ayse Metin, Maria Grazia Roncarolo, Fabio Ciceri, Andrea Finocchi, Michael H. Albert, Marcella Facchini, Maria Pia Cicalese, Carmen Petrescu, Francesca Dionisio, Maria Grazia Valsecchi, Alessandro Aiuti, Roberta Pajno, Koen van Rossem, Stefania Galimberti, Samantha Scaramuzza, Luca Biasco, and Chris Dott

Subjects

medicine.medical_specialty, Myeloid, business.industry, Wiskott–Aldrich syndrome, medicine.medical_treatment, Immunology, Cell Biology, Hematology, Hematopoietic stem cell transplantation, medicine.disease, Biochemistry, Gastroenterology, Fludarabine, Transplantation, medicine.anatomical_structure, Platelet transfusion, Internal medicine, Medicine, Bone marrow, business, Busulfan, medicine.drug

Abstract

Wiskott-Aldrich Syndrome (WAS) is an X-linked primary immunodeficiency characterized by thrombocytopenia, recurrent infections, eczema, autoimmunity and increased susceptibility to malignancies. Allogeneic hematopoietic stem cell transplantation (HSCT) is a recognized curative treatment for WAS, but is still associated with transplant-related complications and long-term morbidity, particularly in the absence of fully matched donors. In April 2010, we initiated a phase I/II clinical trial with hematopoietic stem cell (HSC) gene therapy (GT) for WAS. The investigational medicinal product (IMP) consists of autologous CD34+ HSC engineered with a lentiviral vector (LV) driving the expression of WAS cDNA from an endogenous 1.6 kb human WAS promoter (LV-WAS), infused after a reduced intensity conditioning (RIC) based on anti-CD20 mAb, targeted busulfan and fludarabine. We previously reported early follow up (FU) results from the first 3 patients (Aiuti et al., Science 2013). Seven patients (Zhu score ≥3) have now been treated at a median age of 1.9 years (1.1 - 11.1). As of May 2015, all patients are alive with a median FU of 3.2 years (0.7 - 5.0). CD34+ cell source was bone marrow (BM) (n=5), mobilized peripheral blood (MPB) (n=1) or both (n=1). IMP dose ranged between 7.0 and 14.1 x106 CD34+/kg, containing on average 94.4 ± 3.5% transduced clonogenic progenitors and a mean vector copy number (VCN)/genome in bulk CD34+ cells of 2.7 ± 0.8. No adverse reactions were observed after IMP infusion and RIC was well tolerated. Median duration of severe neutropenia was 19 days; granulocyte-colony stimulating factor was administered to 1 patient. In the first 6 treated patients with FU >2 years, we observed robust and persistent engraftment of gene corrected cells. At the most recent FU, transduced BM progenitors ranged between 20.7 and 59.7%, and LV-transduced cells were detected in multiple lineages, including PB granulocytes (VCN 0.34 - 0.93) and lymphocytes (VCN 1.18 - 2.73). WAS protein expression, measured by flow-cytometry, was detected in the majority of PB platelets [mean ± standard deviation (SD), 71.4 ± 14.0%], monocytes (63.3 ± 18.5%) and lymphocytes (78.9 ± 14.9%). Lymphocyte subset counts were normal in most patients and proliferative response to anti-CD3 mAb was in the normal range in all 6 patients. After immune reconstitution, a marked reduction in the annualized estimated rate of severe infections was observed, as compared with baseline (figure 1A). The first 6 treated patients discontinued anti-infective prophylaxis and no longer require a protected environment. Four patients stopped immunoglobulin supplementation and 2 of them developed specific antibodies after vaccination. Eczema resolved in 4 patients and remains mild in 2. No clinical manifestations of autoimmunity were observed ≥1 year after GT in accordance with improved B-cell development and decreased autoantibody production. All patients became platelet transfusion independent at a median of 4 months after GT (range: 1.0 - 8.7). Mean platelet counts progressively increased after treatment (mean ± SD: before GT, 13.4 ± 7.8 x109/l; 24-30 month FU, 45.8 ± 22.0 x109/l; 36-42 month FU, 57.0 ± 18.7 x109/l). The frequency and the severity of bleeding events decreased after the 1st year of FU. No severe bleedings were recorded after treatment (figure 1B). Quality of life improved in all patients after GT. From the 2nd year of FU, the number of hospitalizations for infections decreased and no hospitalizations due to bleeding were observed after treatment. The seventh patient treated, who received MPB derived CD34+ cells only, showed the fastest platelet recovery with the highest level of transduced myeloid cell engraftment, and is clinically well. No Serious Adverse Events (SAE) related to the IMP were observed. The most frequent SAE were related to infections (85%), occuring mainly during the 1st year of FU. Importantly, no evidence of abnormal clonal proliferations emerged after GT and the LV integration profile show a polyclonal pattern, with no skewing for proto-oncogenes. In conclusion, this updated report in 7 WAS patients show that GT is well tolerated and leads to a sustained clinical benefit. The high level of gene transfer obtained with LV-WAS results in robust engraftment of transduced HSC, even when combined with RIC. Prolonged FU will provide additional information on the long-term safety and clinical efficacy of this treatment. Figure 1. Figure 1. Disclosures Villa: Fondazione Telethon: Research Funding. Dott:GlaxoSmithKline: Consultancy. van Rossem:GlaxoSmithKline: Employment. Naldini:Salk Institute: Patents & Royalties: Lentiviral vectors; San Raffaele Telethon Institute: Patents & Royalties: Lentiviral vector technology; GlaxoSmithKline: Other: GSK licensed gene therapies developed at my Institute and the Institute receives milestone payments; Sangamo Biosciences: Research Funding; Biogen: Research Funding; Genenta Sciences: Equity Ownership, Membership on an entity's Board of Directors or advisory committees. Aiuti:GlaxoSmithKline (GSK): Other: PI of clinical trial which is financially sponsored by GSK; Fondazione Telethon: Research Funding.

Published

2015

34. 447. Lentiviral Gene Therapy in a Preclinical Model of Omenn Syndrome

Author

Niek P. van Til, Maria Carmina Castiello, Gerard Wagemaker, Virginia Maina, Elena Draghici, Valentina Capo, Anna Villa, and Marita Bosticardo

Subjects

Pharmacology, Severe combined immunodeficiency, T cell, Lymphocyte, Genetic enhancement, Hematopoietic stem cell, Biology, medicine.disease, Omenn syndrome, Viral vector, Multiplicity of infection, medicine.anatomical_structure, Drug Discovery, Immunology, Genetics, medicine, Cancer research, Molecular Medicine, Molecular Biology

Abstract

Patients with Omenn syndrome (OS), carrying hypomorphic recombination activating genes (RAG) mutations, develop a peculiar severe combined immunodeficiency associated with autoimmune-like manifestations. RAG1 and RAG2 genes play an essential role in the generation of antigen receptors during lymphocyte development. HLA-matched bone marrow transplantation is curative, however, hematopoietic stem cell gene therapy (GT) could represent an alternative treatment for patients lacking a suitable donor. The aim of the present study was to investigate the efficacy of GT in a knock-in murine model carrying the Rag2 R229Q mutation that mimics most of the symptoms of human OS. To this aim, we are testing a lentiviral vector encoding for codon optimized human RAG2 (hRAG2co-LV vector) under the control of the ubiquitous chromatin opening element (UCOE).We initially measured the efficiency of transduction of Rag2R229Q/R229Q lineage negative (lin-) cells by testing the presence of the integrated viral vector by real-time PCR in lin- cells transduced at a multiplicity of infection (MOI) 5 and 10 and in vitro cultured for 8 days. We observed that the hRAG2co-LV vector transduced Rag2R229Q/R229Q lin- cells very efficiently at MOI 5. Then, we tested the in vivo efficacy of hRAG2co-LV-mediated GT infusing transduced lin- BM cells isolated from male Rag2R229Q/R229Q mice in lethally irradiated females. Control Rag2R229Q/R229Q mice received wild-type (BMT-WT) or untransduced (BMT-OS) lin- BM cells. Analysis of immune cells in peripheral blood was evaluated overtime starting from six weeks after the treatment. GT-treated mice showed the appearance and progressive increase of B cells and amelioration of T cell frequency and absolute count as compared to BMT-OS mice. In parallel, the frequency of myeloid cells started to decrease 13 weeks after GT indicating a normalization of peripheral immune cell distribution. Our preliminary data demonstrate the feasibility of GT in the preclinical model of OS. Additional experiments aimed at evaluating long-term efficacy and safety are ongoing.

Published

2015

35. B-cell reconstitution after lentiviral vector-mediated gene therapy in patients with Wiskott-Aldrich syndrome

Author

Paolo Uva, Mirjam van der Burg, Anna Villa, Immacolata Brigida, Francesca Ferrua, Lucia Piceni Sereni, Michael H. Albert, Giorgio Ottaviano, Marita Bosticardo, Alessandro Aiuti, Maria Carmina Castiello, Francesca Pala, Maria Grazia Roncarolo, Luigi Naldini, Samantha Scaramuzza, Castiello, Mc, Scaramuzza, S, Pala, F, Ferrua, F, Uva, P, Brigida, I, Sereni, L, van der Burg, M, Ottaviano, G, Albert, Mh, Grazia Roncarolo, M, Naldini, Luigi, Aiuti, Alessandro, Villa, A, Bosticardo, M., and Immunology

Subjects

Male, VCN, Vector copy number, Transplantation Conditioning, Wiskott–Aldrich syndrome, medicine.medical_treatment, Gene Expression, Hematopoietic stem cell transplantation, Bone Marrow, Transduction, Genetic, B-Cell Activating Factor, Immunology and Allergy, Child, BM, Bone marrow, B cell, Wiskott-Aldrich syndrome, Hematopoietic Stem Cell Transplantation, Hematopoietic stem cell, gene therapy, 3. Good health, medicine.anatomical_structure, Child, Preschool, SDF-1α, Stromal cell–derived factor 1α, Stem cell, Wiskott-Aldrich Syndrome Protein, BAFF, B cell–activating factor, Recombinant Fusion Proteins, Genetic Vectors, Immunology, B-Lymphocyte Subsets, Immunoglobulins, Biology, primary immunodeficiency, Transplantation, Autologous, CD19, Immunophenotyping, Immune Deficiencies, Infection, and Systemic Immune Disorders, WASp, Wiskott-Aldrich syndrome protein, medicine, Humans, Progenitor cell, Autoantibodies, IVIg, Intravenous immunoglobulin, GT, Gene therapy, Gene Expression Profiling, Lentivirus, lentiviral vector, Infant, PB, Peripheral blood, Genetic Therapy, HSC, Hematopoietic stem cell, Hematopoietic Stem Cells, medicine.disease, WAS, Wiskott-Aldrich syndrome, biology.protein, Bone marrow, HD, Healthy donor

Abstract

Background Wiskott-Aldrich syndrome (WAS) is a severe X-linked immunodeficiency characterized by microthrombocytopenia, eczema, recurrent infections, and susceptibility to autoimmunity and lymphomas. Hematopoietic stem cell transplantation is the treatment of choice; however, administration of WAS gene–corrected autologous hematopoietic stem cells has been demonstrated as a feasible alternative therapeutic approach. Objective Because B-cell homeostasis is perturbed in patients with WAS and restoration of immune competence is one of the main therapeutic goals, we have evaluated reconstitution of the B-cell compartment in 4 patients who received autologous hematopoietic stem cells transduced with lentiviral vector after a reduced-intensity conditioning regimen combined with anti-CD20 administration. Methods We evaluated B-cell counts, B-cell subset distribution, B cell–activating factor and immunoglobulin levels, and autoantibody production before and after gene therapy (GT). WAS gene transfer in B cells was assessed by measuring vector copy numbers and expression of Wiskott-Aldrich syndrome protein. Results After lentiviral vector-mediated GT, the number of transduced B cells progressively increased in the peripheral blood of all patients. Lentiviral vector-transduced progenitor cells were able to repopulate the B-cell compartment with a normal distribution of B-cell subsets both in bone marrow and the periphery, showing a WAS protein expression profile similar to that of healthy donors. In addition, after GT, we observed a normalized frequency of autoimmune-associated CD19 + CD21 − CD35 − and CD21 low B cells and a reduction in B cell–activating factor levels. Immunoglobulin serum levels and autoantibody production improved in all treated patients. Conclusions We provide evidence that lentiviral vector-mediated GT induces transgene expression in the B-cell compartment, resulting in ameliorated B-cell development and functionality and contributing to immunologic improvement in patients with WAS.

Published

2015

36. Characterization of B cell function in Wiskott Aldrich Syndrome (143.37)

Author

Maria Carmina Castiello, Marita Bosticardo, Elena Draghici, Aisha Sauer, Francesca Schena, Ursula Schenk, Barbara Cassani, Alessandro Aiuti, Maria Grazia Roncarolo, Fabio Grassi, Elisabetta Traggiai, and Anna Villa

Subjects

Immunology, Immunology and Allergy

Abstract

Wiskott-Aldrich Syndrome (WAS) is an X-linked immunodeficiency caused by mutations of the gene encoding for WASp, a protein involved in cytoskeletal reorganization of hematopoietic cells. WAS is characterized by microthrombocytopenia, eczema, infections, tumors and high rate of autoimmunity. WASp negative T cells have been extensively studied, while the role of WASp in B cells has been less characterized. Analysis of serum from adult was-/- mice showed increased level of Igs as compared to wt mice, in particular in IgG2a subclass. This result was further confirmed by ELISpot assays performed on sorted Marginal Zone (MZ) and Follicular (FO) B cells from wt and was-/- mice. The presence of autoreactive B cells was supported by the high titers of autoantibodies against dsDNA and tissue Ags in was-/- mice. In in vitro proliferation assays, was-/- B cells are hyper-proliferating to BCR-dependent (IgM) and Toll Like Receptors (TLRs)-dependent stimuli (LPS, CpG) in comparison to wt B cells, although no difference in the expression of TLRs was found. Preliminary results on Ca2+ flux upon CpG stimulus revealed increased Ca2+ mobilization in was-/- MZ B cell as compared to wt MZ B cells. Our data suggest that WASp absence affects B cell function and further studies are ongoing to better characterize BCR and TLR signaling pathways and intracellular trafficking in order to understand the contribution of B cells in autoimmune manifestations found in WAS patients.

Published

2010

37. Gene Editing of Hematopoietic Stem Cells: Hopes and Hurdles Toward Clinical Translation

Author

Samuele Ferrari, Valentina Vavassori, Daniele Canarutto, Aurelien Jacob, Maria Carmina Castiello, Attya Omer Javed, and Pietro Genovese

Subjects

0301 basic medicine, lcsh:QH426-470, lcsh:Biotechnology, Genetic enhancement, Computational biology, Review, Biology, 03 medical and health sciences, 0302 clinical medicine, CRISPR/Cas, Genome editing, lcsh:TP248.13-248.65, medicine, CRISPR, Genome Editing, Progenitor cell, Gene, Cas9, gene editing, hematological diseases, Hematopoietic stem cell, gene therapy, lcsh:Genetics, 030104 developmental biology, medicine.anatomical_structure, hematopoietic stem cell, Stem cell, 030217 neurology & neurosurgery

Abstract

In the field of hematology, gene therapies based on integrating vectors have reached outstanding results for a number of human diseases. With the advent of novel programmable nucleases, such as CRISPR/Cas9, it has been possible to expand the applications of gene therapy beyond semi-random gene addition to site-specific modification of the genome, holding the promise for safer genetic manipulation. Here we review the state of the art of ex vivo gene editing with programmable nucleases in human hematopoietic stem and progenitor cells (HSPCs). We highlight the potential advantages and the current challenges toward safe and effective clinical translation of gene editing for the treatment of hematological diseases.

38. Modeling, optimization, and comparable efficacy of T cell and hematopoietic stem cell gene editing for treating hyper‐IgM syndrome

Author

Giulia Schiroli, Elisabetta Mercuri, Andrea Cappelleri, Anna Villa, Genni Enza Marcovecchio, Maria Kanariou, Vassilios Lougaris, Frank Buquicchio, Maria Carmina Castiello, Valentina Vavassori, Carrie M Margulies, Cecilia Cotta-Ramusino, Luigi Naldini, Francesca Ferrua, Stefano Beretta, Eugenio Scanziani, Alessandro Plebani, Arjan C. Lankester, Ivan Merelli, Luisa Albano, Paola Mv Rancoita, Pietro Genovese, Elena Fontana, Vavassori, V., Mercuri, E., Marcovecchio, G. E., Castiello, M. C., Schiroli, G., Albano, L., Margulies, C., Buquicchio, F., Fontana, E., Beretta, S., Merelli, I., Cappelleri, A., Rancoita, P. M. V., Lougaris, V., Plebani, A., Kanariou, M., Lankester, A., Ferrua, F., Scanziani, E., Cotta-Ramusino, C., Villa, A., Naldini, L., Genovese, P., Vavassori, V, Mercuri, E, Marcovecchio, G, Castiello, M, Schiroli, G, Albano, L, Margulies, C, Buquicchio, F, Fontana, E, Beretta, S, Merelli, I, Cappelleri, A, Rancoita, P, Lougaris, V, Plebani, A, Kanariou, M, Lankester, A, Ferrua, F, Scanziani, E, Cotta-Ramusino, C, Villa, A, Naldini, L, and Genovese, P

Subjects

0301 basic medicine, Adoptive cell transfer, Medicine (General), truncated EGFR, T-Lymphocytes, Genetic enhancement, T cell, Immunology, QH426-470, Hyper-IgM Immunodeficiency Syndrome, Article, T-cell therapy, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, CRISPR‐Cas gene editing, R5-920, medicine, Genetics, Animals, Humans, Progenitor cell, CRISPR-Cas gene editing, hematopoietic stem cells, X-linked hyper-IgM Syndrome, Gene Editing, CD40, biology, Hyper-IgM Immunodeficiency Syndrome, Type 1, T‐cell therapy, Hematopoietic stem cell, Articles, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, biology.protein, Cancer research, Molecular Medicine, hematopoietic stem cell, Genetics, Gene Therapy & Genetic Disease, X‐linked hyper‐IgM Syndrome, 030217 neurology & neurosurgery

Abstract

Precise correction of the CD40LG gene in T cells and hematopoietic stem/progenitor cells (HSPC) holds promise for treating X‐linked hyper‐IgM Syndrome (HIGM1), but its actual therapeutic potential remains elusive. Here, we developed a one‐size‐fits‐all editing strategy for effective T‐cell correction, selection, and depletion and investigated the therapeutic potential of T‐cell and HSPC therapies in the HIGM1 mouse model. Edited patients’ derived CD4 T cells restored physiologically regulated CD40L expression and contact‐dependent B‐cell helper function. Adoptive transfer of wild‐type T cells into conditioned HIGM1 mice rescued antigen‐specific IgG responses and protected mice from a disease‐relevant pathogen. We then obtained ~ 25% CD40LG editing in long‐term repopulating human HSPC. Transplanting such proportion of wild‐type HSPC in HIGM1 mice rescued immune functions similarly to T‐cell therapy. Overall, our findings suggest that autologous edited T cells can provide immediate and substantial benefits to HIGM1 patients and position T‐cell ahead of HSPC gene therapy because of easier translation, lower safety concerns and potentially comparable clinical benefits., Here we report a comprehensive set of preclinical studies, performed both in vitro on X‐linked hyper‐IgM syndrome (HIGM1) patient‐derived cells and in vivo in HIGM1 mice, which uncovers crucial guiding principles towards clinical translation of CD40LG targeted gene correction in T cells or hematopoietic stem cells (HSC) for the treatment of HIGM1.