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1. Evidence for a pathogenic role of extrafollicular, IL-10–producing CCR6⁺B helper T cells in systemic lupus erythematosus

Author

Facciotti, F., Larghi, P., Bosotti, R., Vasco, C., Gagliani, N., Cordiglierif, C., Mazzarag, S., Ranzani, V., Rottoli, E., Curti, S., Penatti, A., Karnani, B., Kobayashi, Y., Crosti, M., Bombaci, M., van Hamburg, J. P., Rossetti, G., Gualtierotti, R., Gerosa, M., Gatti, S., Torretta, S., Pignataro, L., Tas, S. W., Abrignani, S., Pagani, M., Grassi, F., Meroni, P. L., Flavell, R. A., and Geginat, J.

Published
2020

2. Chronic cholesterol administration to the brain supports complete and long-lasting cognitive and motor amelioration in Huntington's disease

Author

Birolini, G, Valenza, M, Ottonelli, I, Talpo, F, Minoli, L, Cappelleri, A, Bombaci, M, Caccia, C, Canevari, C, Trucco, A, Leoni, V, Passoni, A, Favagrossa, M, Nucera, M, Colombo, L, Paltrinieri, S, Bagnati, R, Duskey, J, Caraffi, R, Vandelli, M, Taroni, F, Salmona, M, Scanziani, E, Biella, G, Ruozi, B, Tosi, G, Cattaneo, E, Birolini G., Valenza M., Ottonelli I., Talpo F., Minoli L., Cappelleri A., Bombaci M., Caccia C., Canevari C., Trucco A., Leoni V., Passoni A., Favagrossa M., Nucera M. R., Colombo L., Paltrinieri S., Bagnati R., Duskey J. T., Caraffi R., Vandelli M. A., Taroni F., Salmona M., Scanziani E., Biella G., Ruozi B., Tosi G., Cattaneo E., Birolini, G, Valenza, M, Ottonelli, I, Talpo, F, Minoli, L, Cappelleri, A, Bombaci, M, Caccia, C, Canevari, C, Trucco, A, Leoni, V, Passoni, A, Favagrossa, M, Nucera, M, Colombo, L, Paltrinieri, S, Bagnati, R, Duskey, J, Caraffi, R, Vandelli, M, Taroni, F, Salmona, M, Scanziani, E, Biella, G, Ruozi, B, Tosi, G, Cattaneo, E, Birolini G., Valenza M., Ottonelli I., Talpo F., Minoli L., Cappelleri A., Bombaci M., Caccia C., Canevari C., Trucco A., Leoni V., Passoni A., Favagrossa M., Nucera M. R., Colombo L., Paltrinieri S., Bagnati R., Duskey J. T., Caraffi R., Vandelli M. A., Taroni F., Salmona M., Scanziani E., Biella G., Ruozi B., Tosi G., and Cattaneo E.

Abstract

Evidence that Huntington's disease (HD) is characterized by impaired cholesterol biosynthesis in the brain has led to strategies to increase its level in the brain of the rapidly progressing R6/2 mouse model, with a positive therapeutic outcome. Here we tested the long-term efficacy of chronic administration of cholesterol to the brain of the slowly progressing zQ175DN knock-in HD mice in preventing (“early treatment”) or reversing (“late treatment”) HD symptoms. To do this we used the most advanced formulation of cholesterol loaded brain-permeable nanoparticles (NPs), termed hybrid-g7-NPs-chol, which were injected intraperitoneally. We show that one cycle of treatment with hybrid-g7-NPs-chol, administered in the presymptomatic (“early treatment”) or symptomatic (“late treatment”) stages is sufficient to normalize cognitive defects up to 5 months, as well as to improve other behavioral and neuropathological parameters. A multiple cycle treatment combining both early and late treatments (“2 cycle treatment”) lasting 6 months generates therapeutic effects for more than 11 months, without severe adverse reactions. Sustained cholesterol delivery to the brain of zQ175DN mice also reduces mutant Huntingtin aggregates in both the striatum and cortex and completely normalizes synaptic communication in the striatal medium spiny neurons compared to saline-treated HD mice. Furthermore, through a meta-analysis of published and current data, we demonstrated the power of hybrid-g7-NPs-chol and other strategies able to increase brain cholesterol biosynthesis, to reverse cognitive decline and counteract the formation of mutant Huntingtin aggregates. These results demonstrate that cholesterol delivery via brain-permeable NPs is a therapeutic option to sustainably reverse HD-related behavioral decline and neuropathological signs over time, highlighting the therapeutic potential of cholesterol-based strategies in HD patients. Data availability: This study does not include data deposit

Published
2023

3. Corrigendum: The Impact of Anti-rheumatic Drugs on the Seroprevalence of Anti-SARS-CoV-2 Antibodies in a Cohort of Patients With Inflammatory Arthritis: The MAINSTREAM Study(Front. Med., (2022), 9, (850858), 10.3389/fmed.2022.850858)

Author

Favalli E. G., Favalli, E, Gobbini, A, Bombaci, M, Maioli, G, Biggioggero, M, Pesce, E, Favalli, A, Martinovic, M, Fabbris, T, Marchisio, E, Bandera, A, Gori, A, Abrignani, S, Grifantini, R, Caporali, R, Favalli E. G., Gobbini A., Bombaci M., Maioli G., Biggioggero M., Pesce E., Favalli A., Martinovic M., Fabbris T., Marchisio E., Bandera A., Gori A., Abrignani S., Grifantini R., Caporali R., Favalli E. G., Favalli, E, Gobbini, A, Bombaci, M, Maioli, G, Biggioggero, M, Pesce, E, Favalli, A, Martinovic, M, Fabbris, T, Marchisio, E, Bandera, A, Gori, A, Abrignani, S, Grifantini, R, Caporali, R, Favalli E. G., Gobbini A., Bombaci M., Maioli G., Biggioggero M., Pesce E., Favalli A., Martinovic M., Fabbris T., Marchisio E., Bandera A., Gori A., Abrignani S., Grifantini R., and Caporali R.

Abstract

[This corrects the article DOI: 10.3389/fmed.2022.850858.]

Published
2022

4. Integrated longitudinal immunophenotypic, transcriptional and repertoire analyses delineate immune responses in COVID-19 patients

Author

Notarbartolo, S, Ranzani, V, Bandera, A, Gruarin, P, Bevilacqua, V, Putignano, A, Gobbini, A, Galeota, E, Manara, C, Bombaci, M, Pesce, E, Zagato, E, Favalli, A, Sarnicola, M, Curti, S, Crosti, M, Martinovic, M, Fabbris, T, Marini, F, Donnici, L, Lorenzo, M, Mancino, M, Ungaro, R, Lombardi, A, Mangioni, D, Muscatello, A, Aliberti, S, Blasi, F, De Feo, T, Prati, D, Manganaro, L, Granucci, F, Lanzavecchia, A, De Francesco, R, Gori, A, Grifantini, R, Abrignani, S, Notarbartolo S., Ranzani V., Bandera A., Gruarin P., Bevilacqua V., Putignano A. R., Gobbini A., Galeota E., Manara C., Bombaci M., Pesce E., Zagato E., Favalli A., Sarnicola M. L., Curti S., Crosti M., Martinovic M., Fabbris T., Marini F., Donnici L., Lorenzo M., Mancino M., Ungaro R., Lombardi A., Mangioni D., Muscatello A., Aliberti S., Blasi F., De Feo T., Prati D., Manganaro L., Granucci F., Lanzavecchia A., De Francesco R., Gori A., Grifantini R., Abrignani S., Notarbartolo, S, Ranzani, V, Bandera, A, Gruarin, P, Bevilacqua, V, Putignano, A, Gobbini, A, Galeota, E, Manara, C, Bombaci, M, Pesce, E, Zagato, E, Favalli, A, Sarnicola, M, Curti, S, Crosti, M, Martinovic, M, Fabbris, T, Marini, F, Donnici, L, Lorenzo, M, Mancino, M, Ungaro, R, Lombardi, A, Mangioni, D, Muscatello, A, Aliberti, S, Blasi, F, De Feo, T, Prati, D, Manganaro, L, Granucci, F, Lanzavecchia, A, De Francesco, R, Gori, A, Grifantini, R, Abrignani, S, Notarbartolo S., Ranzani V., Bandera A., Gruarin P., Bevilacqua V., Putignano A. R., Gobbini A., Galeota E., Manara C., Bombaci M., Pesce E., Zagato E., Favalli A., Sarnicola M. L., Curti S., Crosti M., Martinovic M., Fabbris T., Marini F., Donnici L., Lorenzo M., Mancino M., Ungaro R., Lombardi A., Mangioni D., Muscatello A., Aliberti S., Blasi F., De Feo T., Prati D., Manganaro L., Granucci F., Lanzavecchia A., De Francesco R., Gori A., Grifantini R., and Abrignani S.

Abstract

To understand how a protective immune response against SARS-CoV-2 develops over time, we integrated phenotypic, transcriptional and repertoire analyses on PBMCs from mild and severe COVID-19 patients during and after infection, and compared them to healthy donors (HD). A type I IFN-response signature marked all the immune populations from severe patients during the infection. Humoral immunity was dominated by IgG production primarily against the RBD and N proteins, with neutralizing antibody titers increasing post infection and with disease severity. Memory B cells, including an atypical FCRL5+ T-BET+ memory subset, increased during the infection, especially in patients with mild disease. A significant reduction of effector memory, CD8+T cells frequency characterized patients with severe disease. Despite such impairment, we observed robust clonal expansion of CD8+T lymphocytes, while CD4+T cells were less expanded and skewed toward TCMand TH2-like phenotypes. MAIT cells were also expanded, but only in patients with mild disease. Terminally differentiated CD8+GZMB+effector cells were clonally expanded both during the infection and post-infection, while CD8+GZMK+lymphocytes were more expanded post-infection and represented bona fide memory precursor effector cells. TCR repertoire analysis revealed that only highly proliferating T cell clonotypes, which included SARS-CoV-2-specific cells, were maintained post-infection and shared between the CD8+GZMB+and GZMK+subsets. Overall, this study describes the development of immunity against SARS-CoV-2 and identifies an effector CD8+T cell population with memory precursor-like features.

Published
2021

5. Insights into kinetics, release, and behavioral effects of brain-targeted hybrid nanoparticles for cholesterol delivery in Huntington's disease

Author

Birolini, G, Valenza, M, Ottonelli, I, Passoni, A, Favagrossa, M, Duskey, J, Bombaci, M, Vandelli, M, Colombo, L, Bagnati, R, Caccia, C, Leoni, V, Taroni, F, Forni, F, Ruozi, B, Salmona, M, Tosi, G, Cattaneo, E, Birolini G., Valenza M., Ottonelli I., Passoni A., Favagrossa M., Duskey J. T., Bombaci M., Vandelli M. A., Colombo L., Bagnati R., Caccia C., Leoni V., Taroni F., Forni F., Ruozi B., Salmona M., Tosi G., Cattaneo E., Birolini, G, Valenza, M, Ottonelli, I, Passoni, A, Favagrossa, M, Duskey, J, Bombaci, M, Vandelli, M, Colombo, L, Bagnati, R, Caccia, C, Leoni, V, Taroni, F, Forni, F, Ruozi, B, Salmona, M, Tosi, G, Cattaneo, E, Birolini G., Valenza M., Ottonelli I., Passoni A., Favagrossa M., Duskey J. T., Bombaci M., Vandelli M. A., Colombo L., Bagnati R., Caccia C., Leoni V., Taroni F., Forni F., Ruozi B., Salmona M., Tosi G., and Cattaneo E.

Abstract

Supplementing brain cholesterol is emerging as a potential treatment for Huntington's disease (HD), a genetic neurodegenerative disorder characterized, among other abnormalities, by inefficient brain cholesterol biosynthesis. However, delivering cholesterol to the brain is challenging due to the blood-brain barrier (BBB), which prevents it from reaching the striatum, especially, with therapeutically relevant doses. Here we describe the distribution, kinetics, release, and safety of novel hybrid polymeric nanoparticles made of PLGA and cholesterol which were modified with an heptapeptide (g7) for BBB transit (hybrid-g7-NPs-chol). We show that these NPs rapidly reach the brain and target neural cells. Moreover, deuterium-labeled cholesterol from hybrid-g7-NPs-chol is released in a controlled manner within the brain and accumulates over time, while being rapidly removed from peripheral tissues and plasma. We confirm that systemic and repeated injections of the new hybrid-g7-NPs-chol enhanced endogenous cholesterol biosynthesis, prevented cognitive decline, and ameliorated motor defects in HD animals, without any inflammatory reaction. In summary, this study provides insights about the benefits and safety of cholesterol delivery through advanced brain-permeable nanoparticles for HD treatment.

Published
2021

6. Evidence for a pathogenic role of extrafollicular, IL-10-producing CCR6+B helper T cells in systemic lupus erythematosus

Author

Facciotti, F, Larghi, P, Bosotti, R, Vasco, C, Gagliani, N, Cordiglieri, C, Mazzara, S, Ranzani, V, Rottoli, E, Curti, S, Penatti, A, Karnani, B, Kobayashi, Y, Crosti, M, Bombaci, M, van Hamburg, J, Rossetti, G, Gualtierotti, R, Gerosa, M, Gatti, S, Torretta, S, Pignataro, L, Tas, S, Abrignani, S, Pagani, M, Grassi, F, Meroni, P, Flavell, R, Geginat, J, Facciotti F, Larghi P, Bosotti R, Vasco C, Gagliani N, Cordiglieri C, Mazzara S, Ranzani V, Rottoli E, Curti S, Penatti A, Karnani B, Kobayashi Y, Crosti M, Bombaci M, van Hamburg JP, Rossetti G, Gualtierotti R, Gerosa M, Gatti S, Torretta S, Pignataro L, Tas SW, Abrignani S, Pagani M, Grassi F, Meroni PL, Flavell RA, Geginat J, Facciotti, F, Larghi, P, Bosotti, R, Vasco, C, Gagliani, N, Cordiglieri, C, Mazzara, S, Ranzani, V, Rottoli, E, Curti, S, Penatti, A, Karnani, B, Kobayashi, Y, Crosti, M, Bombaci, M, van Hamburg, J, Rossetti, G, Gualtierotti, R, Gerosa, M, Gatti, S, Torretta, S, Pignataro, L, Tas, S, Abrignani, S, Pagani, M, Grassi, F, Meroni, P, Flavell, R, Geginat, J, Facciotti F, Larghi P, Bosotti R, Vasco C, Gagliani N, Cordiglieri C, Mazzara S, Ranzani V, Rottoli E, Curti S, Penatti A, Karnani B, Kobayashi Y, Crosti M, Bombaci M, van Hamburg JP, Rossetti G, Gualtierotti R, Gerosa M, Gatti S, Torretta S, Pignataro L, Tas SW, Abrignani S, Pagani M, Grassi F, Meroni PL, Flavell RA, and Geginat J

Abstract

Interleukin 10 (IL-10) is an antiinflammatory cytokine, but also promotes B cell responses and plays a pathogenic role in systemic lupus erythematosus (SLE). CD4+CCR6+IL-7R+T cells from human tonsils produced IL-10 following stimulation by naïve B cells, which promoted B cell immunoglobulin G (IgG) production. These tonsillar CCR6+B helper T cells were phenotypically distinct from follicular helper T (TFH) cells and lacked BCL6 expression. In peripheral blood, a CCR6+T cell population with similar characteristics was identified, which lacked Th17- and TFH-associated gene signatures and differentiation-associated surface markers. CD4+CCR6+T cells expressing IL-10, but not IL-17, were also detectable in the spleens of cytokine reporter mice. They provided help for IgG production in vivo, and expanded systemically in pristane-induced lupus-like disease. In SLE patients, CD4+CCR6+IL-7R+T cells were associated with the presence of pathogenic anti-dsDNA (doublestranded DNA) antibodies, and provided spontaneous help for autoantibody production ex vivo. Strikingly, IL-10-producing CCR6+T cells were highly abundant in lymph nodes of SLE patients, and colocalized with B cells at the margins of follicles. In conclusion, we identified a previously uncharacterized population of extrafollicular B helper T cells, which produced IL-10 and could play a prominent pathogenic role in SLE.

Published
2020

7. POS0254 IMMUNE RESPONSE TO SARS-CoV-2 INFECTION IN PATIENTS WITH RHEUMATIC MUSCULOSKELETAL DISEASES: THE MAINSTREAM STUDY

Author

Favalli, E. G., primary, Favalli, A., additional, Andrea, G., additional, Maioli, G., additional, Zagato, E., additional, Bombaci, M., additional, Pesce, E., additional, Donnici, L., additional, Gruarin, P., additional, Biggioggero, M., additional, Curti, S., additional, Manganaro, L., additional, Marchisio, E., additional, Bevilacqua, V., additional, Martinovic, M., additional, Fabbris, T., additional, Sarnicola, M. L., additional, Crosti, M., additional, Marongiu, L., additional, Granucci, F., additional, Notabartolo, S., additional, Bandera, A., additional, Gori, A., additional, De Francesco, R., additional, Abrignani, S., additional, Caporali, R., additional, and Grifantini, R., additional

Published
2022
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8. Novel biomarkers for primary biliary cholangitis to improve diagnosis and understand underlying regulatory mechanisms

Author

Bombaci, M, Pesce, E, Torri, A, Carpi, D, Crosti, M, Lanzafame, M, Cordiglieri, C, Sinisi, A, DEL MORO, L, Bernuzzi, F, Gerussi, A, Geginat, J, Muratori, L, Terracciano, L, Invernizzi, P, Abrignani, S, Grifantini, R, Bombaci M., Pesce E., Torri A., Carpi D., Crosti M., Lanzafame M., Cordiglieri C., Sinisi A., DEL MORO, LILIA ANNA PAOLA MARIA, Bernuzzi F., Gerussi A., Geginat J., Muratori L., Terracciano L. M., Invernizzi P., Abrignani S., Grifantini R., Bombaci, M, Pesce, E, Torri, A, Carpi, D, Crosti, M, Lanzafame, M, Cordiglieri, C, Sinisi, A, DEL MORO, L, Bernuzzi, F, Gerussi, A, Geginat, J, Muratori, L, Terracciano, L, Invernizzi, P, Abrignani, S, Grifantini, R, Bombaci M., Pesce E., Torri A., Carpi D., Crosti M., Lanzafame M., Cordiglieri C., Sinisi A., DEL MORO, LILIA ANNA PAOLA MARIA, Bernuzzi F., Gerussi A., Geginat J., Muratori L., Terracciano L. M., Invernizzi P., Abrignani S., and Grifantini R.

Abstract

Background and aims: Primary biliary cholangitis is an autoimmune biliary disease characterized by injury of bile ducts, eventually leading to cirrhosis and death. In most cases, anti-mitochondrial antibodies and persistently elevated serum alkaline phosphatase are the basis for the serological diagnosis. Anti-nuclear antibodies are also useful and may indicate a more aggressive diseases course. In patients in which anti-mitochondrial antibodies are not detected, an accurate diagnosis requires liver histology. This study aims at identifying specific biomarkers for the serological diagnosis of primary biliary cholangitis. Methods: Sera from patients affected by primary biliary cholangitis, primary sclerosing cholangitis, hepatitis C virus (with and without cryoglobulinemia), hepatocarcinoma and healthy donors were tested on a protein array representing 1658 human proteins. The most reactive autoantigens were confirmed by DELFIA analysis on expanded cohorts of the same mentioned serum classes, and on autoimmune hepatitis sera, using anti-PDC-E2 as reference biomarker. Results: Two autoantigens, SPATA31A3 and GARP, showed high reactivity with primary biliary cholangitis sera, containing or not anti-mitochondrial antibodies. Their combination with PDC-E2 allowed to discriminate primary biliary cholangitis from all tested control classes with high sensitivity and specificity. We found that GARP expression is upregulated upon exposure to biliary salts in human cholangiocytes, an event involving EGFR and insulin pathways. GARP expression was also detected in biliary duct cells of PBC patients. Conclusions: This study highlighted SPATA31A3 and GARP as new biomarkers for primary biliary cholangitis and unravelled molecular stimuli underlying GARP expression in human cholangiocytes

Published
2019

9. Structure, immunoreactivity, and in silico epitope determination of SmSPI S. mansoni serpin for immunodiagnostic application

Author

De Benedetti S., Di Pisa F., Fassi E.M.A., Cretich M., Musico A., Frigerio R., Mussida A., Bombaci M., Grifantini R., Colombo G., Bolognesi M., Grande R., Zanchetta N., Gismondo M.R., Mileto D., Mancon A., and Gourlay L.J.

Subjects
crystal structure, Serine protease inhibitor, Neglected Tropical Disease, immunodiagnostics, circulating antigen, schistosomiasis, parasitic diseases, in silico epitope predictions
Abstract

The human parasitic disease Schistosomiasis is caused by the Schistosoma trematode flatworm that infects freshwaters in tropical regions of the world, particularly in Sub-Saharan Africa, South America, and the Far-East. It has also been observed as an emerging disease in Europe, due to increased immigration. In addition to improved therapeutic strategies, it is imperative to develop novel, rapid, and sensitive diagnostic tests that can detect the Schistosoma parasite, allowing timely treatment. Present diagnosis is difficult and involves microscopy-based detection of Schistosoma eggs in the feces. In this context, we present the 3.22 Å resolution crystal structure of the circulating antigen Serine protease inhibitor from S. mansoni (SmSPI), and we describe it as a potential serodiagnostic marker. Moreover, we identify three potential immunoreactive epitopes using in silico-based epitope mapping methods. Here, we confirm effective immune sera reactivity of the recombinant antigen, suggesting the further investigation of the protein and/or its predicted epitopes as serodiagnostic Schistosomiasis biomarkers.

Published
2021

10. POS0048 SEROPREVALENCE OF ANTI-SARS-COV-2 ANTIBODIES IN RHEUMATIC PATIENTS TREATED WITH BIOLOGICAL AND TARGETED THERAPY LIVING IN LOMBARDY, ITALY (MAINSTREAM PROJECT)

Author

Favalli, E. G., primary, Maioli, G., additional, Bombaci, M., additional, Biggioggero, M., additional, Favalli, A., additional, Agape, E., additional, Andrea, G., additional, Pesce, E., additional, Zagato, E., additional, Fabbris, T., additional, Martinovic, M., additional, Marchisio, E., additional, Abrignani, S., additional, Grifantini, R., additional, and Caporali, R., additional

Published
2021
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11. THU0221 EVIDENCE FOR A PATHOGENIC ROLE OF EXTRA-FOLLICULAR, IL-10 PRODUCING CCR6+B-HELPER T-CELLS IN SYSTEMIC LUPUS ERYTHEMATOSUS

Author

Gerosa, M., primary, Facciotti, F., additional, Larghi, P., additional, Bosotti, R., additional, Vasco, C., additional, Gagliani, N., additional, Cordiglieri, C., additional, Rottoli, E., additional, Penatti, A. E., additional, Argolini, L. M., additional, Karnani, B., additional, Kobayashi, Y., additional, Bombaci, M., additional, Van Hamburg, J. P., additional, Gualtierotti, R., additional, Gatti, S., additional, Torretta, S., additional, Pignataro, L., additional, Tas, S. W., additional, Caporali, R., additional, Abrignani, S., additional, Pagani, M., additional, Grassi, F., additional, Meroni, P. L., additional, Flavell, R., additional, and Geginat, J., additional

Published
2020
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12. Evidence for a pathogenic role of extrafollicular, IL-10–producing CCR6 + B helper T cells in systemic lupus erythematosus

Author

Facciotti, F., primary, Larghi, P., additional, Bosotti, R., additional, Vasco, C., additional, Gagliani, N., additional, Cordiglieri, C., additional, Mazzara, S., additional, Ranzani, V., additional, Rottoli, E., additional, Curti, S., additional, Penatti, A., additional, Karnani, B., additional, Kobayashi, Y., additional, Crosti, M., additional, Bombaci, M., additional, van Hamburg, J. P., additional, Rossetti, G., additional, Gualtierotti, R., additional, Gerosa, M., additional, Gatti, S., additional, Torretta, S., additional, Pignataro, L., additional, Tas, S. W., additional, Abrignani, S., additional, Pagani, M., additional, Grassi, F., additional, Meroni, P. L., additional, Flavell, R. A., additional, and Geginat, J., additional

Published
2020
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13. Evidence for a pathogenic role of extrafollicular, IL-10-producing CCR6+B helper T cells in systemic lupus erythematosus.

Author

Facciotti, F., Larghi, P., Bosotti, R., Vasco, C., Gagliani, N., Cordiglieri, C., Mazzara, S., Ranzani, V., Rottoli, E., Curti, S., Penatti, A., Karnani, B., Kobayashi, Y., Crosti, M., Bombaci, M., van Hamburg, J. P., Rossetti, G., Gualtierotti, R., Gerosa, M., and Gatti, S.

Subjects
T helper cells, SYSTEMIC lupus erythematosus, B cells, CELL populations, IMMUNOGLOBULIN G
Abstract

Interleukin 10 (IL-10) is an antiinflammatory cytokine, but also promotes B cell responses and plays a pathogenic role in systemic lupus erythematosus (SLE). CD4+CCR6+IL-7R+T cells from human tonsils produced IL-10 following stimulation by naïve B cells, which promoted B cell immunoglobulin G (IgG) production. These tonsillar CCR6+B helper T cells were phenotypically distinct from follicular helper T (TFH) cells and lacked BCL6 expression. In peripheral blood, a CCR6+T cell population with similar characteristics was identified, which lacked Th17- and TFH-associated gene signatures and differentiation-associated surface markers. CD4+CCR6+T cells expressing IL-10, but not IL-17, were also detectable in the spleens of cytokine reporter mice. They provided help for IgG production in vivo, and expanded systemically in pristane-induced lupus-like disease. In SLE patients, CD4+CCR6+IL-7R+T cells were associated with the presence of pathogenic anti-dsDNA (doublestranded DNA) antibodies, and provided spontaneous help for autoantibody production ex vivo. Strikingly, IL-10-producing CCR6+T cells were highly abundant in lymph nodes of SLE patients, and colocalized with B cells at the margins of follicles. In conclusion, we identified a previously uncharacterized population of extrafollicular B helper T cells, which produced IL-10 and could play a prominent pathogenic role in SLE. [ABSTRACT FROM AUTHOR]

Published
2020
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15. Immunoprotective cryptococcal proteins

Author

Teti, Giuseppe, Biondo, Carmelo, Mancuso, Giuseppe, Midiri, A, Messina, L, Bombaci, M, Garufi, G, Tuscano, G, Genovese, K, and Felici, F.

Published
2005

36. Novel biomarkers for primary biliary cholangitis to improve diagnosis and understand underlying regulatory mechanisms

Author

Pietro Invernizzi, Alessio Gerussi, Luigi Muratori, Anna Torri, Sergio Abrignani, Antonia Sinisi, Jens Geginat, Mariacristina Crosti, Francesca Bernuzzi, Donatella Carpi, Monica Moro, Chiara Cordiglieri, Elisa Pesce, Renata Grifantini, Mauro Bombaci, Manuela Lanzafame, Luigi Terracciano, Bombaci, M, Pesce, E, Torri, A, Carpi, D, Crosti, M, Lanzafame, M, Cordiglieri, C, Sinisi, A, DEL MORO, L, Bernuzzi, F, Gerussi, A, Geginat, J, Muratori, L, Terracciano, L, Invernizzi, P, Abrignani, S, Grifantini, R, Bombaci M., Pesce E., Torri A., Carpi D., Crosti M., Lanzafame M., Cordiglieri C., Sinisi A., Moro M., Bernuzzi F., Gerussi A., Geginat J., Muratori L., Terracciano L.M., Invernizzi P., Abrignani S., and Grifantini R.

Subjects
Adult, Male, Cirrhosis, Hepatitis C virus, Autoimmune hepatitis, medicine.disease_cause, Autoantigens, primary biliary cholangiti, Serology, Primary sclerosing cholangitis, Biliary disease, 03 medical and health sciences, Young Adult, GARP, 0302 clinical medicine, medicine, Humans, protein array, Aged, Autoantibodies, Aged, 80 and over, Hepatology, business.industry, Liver Cirrhosis, Biliary, Membrane Proteins, Middle Aged, medicine.disease, Cryoglobulinemia, Mitochondria, liver autoimmune disease, 030220 oncology & carcinogenesis, Immunology, biomarker, Biomarker (medicine), 030211 gastroenterology & hepatology, Female, business, Biomarkers
Abstract

Background and aims: Primary biliary cholangitis is an autoimmune biliary disease characterized by injury of bile ducts, eventually leading to cirrhosis and death. In most cases, anti-mitochondrial antibodies and persistently elevated serum alkaline phosphatase are the basis for the serological diagnosis.Anti-nuclear antibodies are also useful and may indicate a more aggressive diseases course. In patients in which anti-mitochondrial antibodies are not detected, an accurate diagnosis requires liver histology. This study aims at identifying specific biomarkers for the serological diagnosis of primary biliary cholangitis. Methods: Sera from patients affected by primary biliary cholangitis, primary sclerosing cholangitis, hepatitis C virus (with and without cryoglobulinemia), hepatocarcinoma and healthy donors were tested on a protein array representing 1658 human proteins. The most reactive autoantigens were confirmed by DELFIA analysis on expanded cohorts of the same mentioned serum classes, and on autoimmune hepatitis sera, using anti-PDC-E2 as reference biomarker. Results: Two autoantigens, SPATA31A3 and GARP, showed high reactivity with primary biliary cholangitis sera, containing or not anti-mitochondrial antibodies. Their combination with PDC-E2 allowed to discriminate primary biliary cholangitis from all tested control classes with high sensitivity and specificity. We found that GARP expression is upregulated upon exposure to biliary salts in human cholangiocytes, an event involving EGFR and insulin pathways. GARP expression was also detected in biliary duct cells of PBC patients. Conclusions: This study highlighted SPATA31A3 and GARP as new biomarkers for primary biliary cholangitis and unravelled molecular stimuli underlying GARP expression in human cholangiocytes.

Published
2019

37. Immunosuppressant Treatment in Rheumatic Musculoskeletal Diseases Does Not Inhibit Elicitation of Humoral Response to SARS-CoV-2 Infection and Preserves Effector Immune Cell Populations

Author

Andrea Favalli, Ennio Giulio Favalli, Andrea Gobbini, Elena Zagato, Mauro Bombaci, Gabriella Maioli, Elisa Pesce, Lorena Donnici, Paola Gruarin, Martina Biggioggero, Serena Curti, Lara Manganaro, Edoardo Marchisio, Valeria Bevilacqua, Martina Martinovic, Tanya Fabbris, Maria Lucia Sarnicola, Mariacristina Crosti, Laura Marongiu, Francesca Granucci, Samuele Notarbartolo, Alessandra Bandera, Andrea Gori, Raffaele De Francesco, Sergio Abrignani, Roberto Caporali, Renata Grifantini, Favalli, A, Favalli, E, Gobbini, A, Zagato, E, Bombaci, M, Maioli, G, Pesce, E, Donnici, L, Gruarin, P, Biggioggero, M, Curti, S, Manganaro, L, Marchisio, E, Bevilacqua, V, Martinovic, M, Fabbris, T, Sarnicola, M, Crosti, M, Marongiu, L, Granucci, F, Notarbartolo, S, Bandera, A, Gori, A, De Francesco, R, Abrignani, S, Caporali, R, and Grifantini, R

Subjects
DMARD, SARS-CoV-2, Antirheumatic Agents, Rheumatic Diseases, Immunology, Humans, COVID-19, Immunology and Allergy, rheumatic musculoskeletal disease, Immunosuppressive Agents, immune response, COVID-19 Drug Treatment, inflammatory arthriti
Abstract

COVID-19 has proven to be particularly serious and life-threatening for patients presenting with pre-existing pathologies. Patients affected by rheumatic musculoskeletal disease (RMD) are likely to have impaired immune responses against SARS-CoV-2 infection due to their compromised immune system and the prolonged use of disease-modifying anti-rheumatic drugs (DMARDs), which include conventional synthetic (cs) DMARDs or biologic and targeted synthetic (b/ts) DMARDs. To provide an integrated analysis of the immune response following SARS-CoV-2 infection in RMD patients treated with different classes of DMARDs we carried out an immunological analysis of the antibody responses toward SARS-CoV-2 nucleocapsid and RBD proteins and an extensive immunophenotypic analysis of the major immune cell populations. We showed that RMD individuals under most DMARD treatments mount a sustained antibody response to the virus, with neutralizing activity. In addition, they displayed a sizable percentage of effector T and B lymphocytes. Among b-DMARDs, we found that anti-TNFα treatments are more favorable drugs to elicit humoral and cellular immune responses as compared to CTLA4-Ig and anti-IL6R inhibitors. This study provides a whole picture of the humoral and cellular immune responses in RMD patients by reassuring the use of DMARD treatments during COVID-19. The study points to TNF-α inhibitors as those DMARDs permitting elicitation of functional antibodies to SARS-CoV-2 and adaptive effector populations available to counteract possible re-infections.

Published
2022

38. Insights into kinetics, release, and behavioral effects of brain-targeted hybrid nanoparticles for cholesterol delivery in Huntington's disease

Author

Alice Passoni, Claudio Caccia, Renzo Bagnati, Flavio Forni, Mario Salmona, Valerio Leoni, Marta Valenza, Giovanni Tosi, Laura Colombo, Mauro Bombaci, Franco Taroni, Monica Favagrossa, Ilaria Ottonelli, Maria Angela Vandelli, Giulia Birolini, Jason T. Duskey, Elena Cattaneo, Barbara Ruozi, Birolini, G, Valenza, M, Ottonelli, I, Passoni, A, Favagrossa, M, Duskey, J, Bombaci, M, Vandelli, M, Colombo, L, Bagnati, R, Caccia, C, Leoni, V, Taroni, F, Forni, F, Ruozi, B, Salmona, M, Tosi, G, and Cattaneo, E

Subjects
Huntington, Kinetics, Pharmaceutical Science, Endogeny, 02 engineering and technology, Striatum, Pharmacology, Blood–brain barrier, 03 medical and health sciences, chemistry.chemical_compound, Nanoparticle, Huntington's disease, medicine, Animals, Distribution (pharmacology), Cognitive decline, Blood-brain barrier, 030304 developmental biology, 0303 health sciences, Cholesterol, Nanoparticles, Chemistry, technology, industry, and agriculture, Brain, 021001 nanoscience & nanotechnology, medicine.disease, PLGA, Huntington Disease, medicine.anatomical_structure, lipids (amino acids, peptides, and proteins), 0210 nano-technology
Abstract

Supplementing brain cholesterol is emerging as a potential treatment for Huntington’s disease (HD), a genetic neurodegenerative disorder characterized, among other abnormalities, by inefficient brain cholesterol biosynthesis. However, delivering cholesterol to the brain is challenging due to the bloodbrain barrier (BBB), which prevents it from reaching the striatum, especially, with therapeutically relevant doses.Here we describe the distribution, kinetics, release, and safety of novel hybrid polymeric nanoparticles made of PLGA and cholesterol which were modified with an heptapeptide (g7) for BBB transit (hybrid-g7-NPs-chol). We show that these NPs rapidly reach the brain and target neural cells. Moreover, deuterium-labeled cholesterol from hybrid-g7-NPs-chol is released in a controlled manner within the brain and accumulates over time, while being rapidly removed from peripheral tissues and plasma. We confirm that systemic and repeated injections of the new hybrid-g7-NPs-chol enhanced endogenous cholesterol biosynthesis, prevented cognitive decline, and ameliorated motor defects in HD animals, without any inflammatory reaction.In summary, this study provides insights about the benefits and safety of cholesterol delivery through advanced brain-permeable nanoparticles for HD treatment.

Published
2021

39. Integrated longitudinal immunophenotypic, transcriptional and repertoire analyses delineate immune responses in COVID-19 patients

Author

Samuele, Notarbartolo, Valeria, Ranzani, Alessandra, Bandera, Paola, Gruarin, Valeria, Bevilacqua, Anna Rita, Putignano, Andrea, Gobbini, Eugenia, Galeota, Cristina, Manara, Mauro, Bombaci, Elisa, Pesce, Elena, Zagato, Andrea, Favalli, Maria Lucia, Sarnicola, Serena, Curti, Mariacristina, Crosti, Martina, Martinovic, Tanya, Fabbris, Federico, Marini, Lorena, Donnici, Mariangela, Lorenzo, Marilena, Mancino, Riccardo, Ungaro, Andrea, Lombardi, Davide, Mangioni, Antonio, Muscatello, Stefano, Aliberti, Francesco, Blasi, Tullia, De Feo, Daniele, Prati, Lara, Manganaro, Francesca, Granucci, Antonio, Lanzavecchia, Raffaele, De Francesco, Andrea, Gori, Renata, Grifantini, Sergio, Abrignani, Notarbartolo, S, Ranzani, V, Bandera, A, Gruarin, P, Bevilacqua, V, Putignano, A, Gobbini, A, Galeota, E, Manara, C, Bombaci, M, Pesce, E, Zagato, E, Favalli, A, Sarnicola, M, Curti, S, Crosti, M, Martinovic, M, Fabbris, T, Marini, F, Donnici, L, Lorenzo, M, Mancino, M, Ungaro, R, Lombardi, A, Mangioni, D, Muscatello, A, Aliberti, S, Blasi, F, De Feo, T, Prati, D, Manganaro, L, Granucci, F, Lanzavecchia, A, De Francesco, R, Gori, A, Grifantini, R, and Abrignani, S

Subjects
Adult, Male, Cell Plasticity, T-Lymphocyte Subset, Antibodies, Viral, Immunophenotyping, Clonal Evolution, T-Lymphocyte Subsets, Humans, Lymphocyte Count, Aged, B-Lymphocytes, SARS-CoV-2, Gene Expression Profiling, B-Lymphocyte, COVID-19, Biomarker, Middle Aged, Immunoglobulin Isotypes, Host-Pathogen Interaction, Immunoglobulin Isotype, Host-Pathogen Interactions, Leukocytes, Mononuclear, Female, Transcriptome, Immunologic Memory, Biomarkers, Human
Abstract

To understand how a protective immune response against SARS-CoV-2 develops over time, we integrated phenotypic, transcriptional and repertoire analyses on PBMCs from mild and severe COVID-19 patients during and after infection, and compared them to healthy donors (HD). A type I IFN-response signature marked all the immune populations from severe patients during the infection. Humoral immunity was dominated by IgG production primarily against the RBD and N proteins, with neutralizing antibody titers increasing post infection and with disease severity. Memory B cells, including an atypical FCRL5+ T-BET+ memory subset, increased during the infection, especially in patients with mild disease. A significant reduction of effector memory, CD8+T cells frequency characterized patients with severe disease. Despite such impairment, we observed robust clonal expansion of CD8+T lymphocytes, while CD4+T cells were less expanded and skewed toward TCMand TH2-like phenotypes. MAIT cells were also expanded, but only in patients with mild disease. Terminally differentiated CD8+GZMB+effector cells were clonally expanded both during the infection and post-infection, while CD8+GZMK+lymphocytes were more expanded post-infection and represented bona fide memory precursor effector cells. TCR repertoire analysis revealed that only highly proliferating T cell clonotypes, which included SARS-CoV-2-specific cells, were maintained post-infection and shared between the CD8+GZMB+and GZMK+subsets. Overall, this study describes the development of immunity against SARS-CoV-2 and identifies an effector CD8+T cell population with memory precursor-like features.

Published
2021

40. A Structurally Simple Vaccine Candidate Reduces Progression and Dissemination of Triple-Negative Breast Cancer

Author

Amedei, Amedeo, Asadzadeh, Fatemeh, Papi, Francesco, Vannucchi, Maria Giuliana, Ferrucci, Veronica, Bermejo, Iris A., Fragai, Marco, De Almeida, Carolina Vieira, Cerofolini, Linda, Giuntini, Stefano, Bombaci, Mauro, Pesce, Elisa, Niccolai, Elena, Natali, Francesca, Guarini, Eleonora, Gabel, Frank, Traini, Chiara, Catarinicchia, Stefano, Ricci, Federica, Orzalesi, Lorenzo, Berti, Francesco, Corzana, Francisco, Zollo, Massimo, Grifantini, Renata, Nativi, Cristina, 0000-0002-2143-046X, 0000-0001-8864-4852, 0000-0002-0795-9594, 0000-0002-1631-4624, 0000-0001-5597-8127, 0000-0002-6312-3230, Amedei, A., Asadzadeh, F., Papi, F., Vannucchi, M. G., Ferrucci, V., Bermejo, I. A., Fragai, M., De Almeida, C. V., Cerofolini, L., Giuntini, S., Bombaci, M., Pesce, E., Niccolai, E., Natali, F., Guarini, E., Gabel, F., Traini, C., Catarinicchia, S., Ricci, F., Orzalesi, L., Berti, F., Corzana, F., Zollo, M., Grifantini, R., and Nativi, C.

Subjects
0301 basic medicine, Immunology, 02 engineering and technology, Medical Biochemistry, Article, 03 medical and health sciences, Breast cancer, Immune system, Antigen, Tn antigen, medicine, lcsh:Science, Triple-negative breast cancer, Cancer, Multidisciplinary, biology, business.industry, 021001 nanoscience & nanotechnology, medicine.disease, 030104 developmental biology, Tumor progression, Cancer cell, biology.protein, Cancer research, lcsh:Q, Antibody, 0210 nano-technology, business, Vaccine
Abstract

Summary The Tn antigen is a well-known tumor-associated carbohydrate determinant, often incorporated in glycopeptides to develop cancer vaccines. Herein, four copies of a conformationally constrained mimetic of the antigen TnThr (GalNAc-Thr) were conjugated to the adjuvant CRM197, a protein licensed for human use. The resulting vaccine candidate, mime[4]CRM elicited a robust immune response in a triple-negative breast cancer mouse model, correlated with high frequency of CD4+ T cells and low frequency of M2-type macrophages, which reduces tumor progression and lung metastasis growth. Mime[4]CRM-mediated activation of human dendritic cells is reported, and the proliferation of mime[4]CRM-specific T cells, in cancer tissue and peripheral blood of patients with breast cancer, is demonstrated. The locked conformation of the TnThr mimetic and a proper presentation on the surface of CRM197 may explain the binding of the conjugate to the anti-Tn antibody Tn218 and its efficacy to fight cancer cells in mice., Graphical Abstract, Highlights • Structurally simple vaccine candidate reduces BC tumor size and delays lung metastasis • TnThr mimetic, fused to CRM197 adjuvant, is able to elicit T and B immune responses • TnThr mimetic-based vaccine candidate able to activate human DCs • The vaccine candidate recruits T helper CD4+ in the tumor microenvironment, Medical Biochemistry; Immunology; Cancer

Published
2020
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41. MyD88 and TLR2, but not TLR4, are required for host defense againstCryptococcus neoformans

Author

Maria Rosaria Catania, Luciano Messina, Mauro Bombaci, Giuseppe Mancuso, Gabriella Garufi, Francesco Tomasello, Concetta Beninati, Angelina Midiri, Carmelo Biondo, Giuseppe Teti, Biondo, C, Midiri, A, Messina, L, Tomasello, F, Garufi, G, Catania, MARIA ROSARIA, Bombaci, M, Beninati, C, Teti, G, and Mancuso, G.

Subjects
Immunology, Mutant, Receptors, Cell Surface, Microbiology, Interferon-gamma, Mice, Antigen, medicine, Cryptococcus neoformans, Pathogenic yeasts, Animals, Immunology and Allergy, RNA, Messenger, Receptors, Immunologic, Receptor, Adaptor Proteins, Signal Transducing, Innate immune system, biology, Reverse Transcriptase Polymerase Chain Reaction, Tumor Necrosis Factor-alpha, Cryptococcosis, biology.organism_classification, medicine.disease, Antigens, Differentiation, Interleukin-12, Toll-Like Receptor 2, Toll-Like Receptor 4, TLR2, Myeloid Differentiation Factor 88, Macrophages, Peritoneal, TLR4
Abstract

We investigated here the potential role of Toll-like receptors (TLR) and the adaptor protein MyD88 in innate immunity responses to Cryptococcus neoformans, a pathogenic encapsulated yeast. Peritoneal macrophages from MyD88(-/-) or TLR2(-/-) mice released significantly less TNF-alpha, compared with wild-type controls, after in vitro stimulation with whole yeasts. In contrast, no differences in TNF-alpha release were noted between macrophages from C3H/HeJ mice, which have a loss of function mutation in TLR4, relative to C3H/HeN controls. When MyD88- or TLR2-deficient mice were infected with low doses of the H99 serotype A strain, all of the control animals, but none of MyD88(-/-) and only 38% of the TLR2(-/-) animals survived, in association with higher fungal burden in the mutant mice. Both MyD88(-/-) and TLR2(-/-) animals showed decreased TNF-alpha, IL-12p40 and/or IFN-gamma expression in various organs during infection. No difference in susceptibility to experimental cryptococcosis was found between C3H/HeJ mice and C3H/HeN controls. In conclusion, our data indicate that TLR2 and MyD88, but not TLR4, critically contribute to anti-cryptococcal defenses through the induction of increased TNF-alpha, IL-12 and IFN-gamma expression.

Published
2005

42. Identification of new autoantigens by protein array indicates a role for IL4 neutralization in autoimmune hepatitis

Author

Antonella Sinisi, Mariacristina Crosti, Renzo Nogarotto, Massimiliano Pagani, Paolo Muratori, Anna Linda Zignego, Milena Arigò, Jens Geginat, Elisa Sugliano, Francesco Marabita, Chiara Zingaretti, Luigi Muratori, Maurizio Marconi, Pietro Invernizzi, Cristina Cheroni, Raoul J. P. Bonnal, Paolo Marcatili, Piero Colombatto, Sergio Abrignani, Monica Moro, Raffaele De Francesco, Maurizia Rossana Brunetto, Angela Cardaci, Mauro Bombaci, Ferruccio Bonino, Zingaretti C, Arigo' M, Cardaci A, Moro M, Crosti M, Sinisi A, Sugliano E, Cheroni C, Marabita F, Nogarotto R, Bonnal RJ, Marcatili P, Marconi M, Zignego A, Muratori P, Invernizzi P, Colombatto P, Brunetto M, Bonino F, De Francesco R, Geginat J, Pagani M, Muratori L, Abrignani S, and Bombaci M.

Subjects
Microarray, Protein Array Analysis, Autoimmune hepatitis, Biology, Autoantigens, Biochemistry, Analytical Chemistry, law.invention, immune system diseases, law, medicine, Humans, Phosphorylation, Receptor, Molecular Biology, Interleukin 4, Autoantibodies, Autoimmune Hepatitis, Hepatitis B Virus, Hepatitis C Virus, Healthy Donor, Interleukin-4 receptor, Interleukin-4 receptor Fibronectin Type III domain, Mean Fluorescence Intensity, Viral Hepatitis, Research, Autoantibody, Interleukin-4 Receptor alpha Subunit, medicine.disease, Antibodies, Neutralizing, Molecular biology, Recombinant Proteins, digestive system diseases, Protein Structure, Tertiary, Hepatitis, Autoimmune, Liver, AUTOIMMUNE HEPATITIS, Immunology, Protein microarray, Recombinant DNA, Interleukin-4, STAT6 Transcription Factor, Biomarkers, Immunostaining, Signal Transduction
Abstract

Autoimmune hepatitis (AIH) is an unresolving inflammation of the liver of unknown cause. Diagnosis requires the exclusion of other conditions and the presence of characteristic features such as specific autoantibodies. Presently, these autoantibodies have relatively low sensitivity and specificity and are identified via immunostaining of cells or tissues; therefore, there is a diagnostic need for better and easy-to-assess markers. To identify new AIH-specific autoantigens, we developed a protein microarray comprising 1626 human recombinant proteins, selected in silico for being secreted or membrane associated. We screened sera from AIH patients on this microarray and compared the reactivity with that of sera from healthy donors and patients with chronic viral hepatitis C. We identified six human proteins that are specifically recognized by AIH sera. Serum reactivity to a combination of four of these autoantigens allows identification of AIH patients with high sensitivity (82%) and specificity (92%). Of the six autoantigens, the interleukin-4 (IL4) receptor fibronectin type III domain of the IL4 receptor (CD124), which is expressed on the surface of both lymphocytes and hepatocytes, showed the highest individual sensitivity and specificity for AIH. Remarkably, patients' sera inhibited STAT6 phosphorylation induced by IL4 binding to CD124, demonstrating that these autoantibodies are functional and suggesting that IL4 neutralization has a pathogenetic role in AIH.

Published
2012

43. Identification and cloning of a cryptococcal deacetylase that produces protective immune responses

Author

Marco R. Oggioni, Demetrio Delfino, Giuseppe Tomaselli, Mauro Bombaci, Giuseppe Mancuso, Angelina Midiri, Carmelo Biondo, Giuseppe Teti, Concetta Beninati, Biondo C, Beninati C, Delfino D, Oggioni M, Mancuso G, Midiri A, Bombaci M, Tomaselli G, and Teti G

Subjects
Cellular immunity, pathogenesi, Antigens, Fungal, Immunology, Molecular Sequence Data, Microbiology, law.invention, Amidohydrolases, Immune system, Antigen, law, vaccine, medicine, Hypersensitivity, Delayed, Amino Acid Sequence, Cloning, Molecular, Cryptococcus neoformans, Fungal vaccine, biology, Base Sequence, biology.organism_classification, medicine.disease, immunity, Molecular Weight, Infectious Diseases, Delayed hypersensitivity, Cryptococcosis, Recombinant DNA, Parasitology, Immunization, Fungal and Parasitic Infections, Fungal Vaccines
Abstract

Cell-mediated immunity plays a crucial role in host defenses againstCryptococcus(Filobasidiella)neoformans. Therefore, the identification of cryptococcal antigens capable of producing T-cell-mediated responses, such as delayed-type hypersensitivity (DTH) reactions, may be useful in the development of immune-based strategies to control cryptococcosis. In order to characterize DTH-producing antigens, culture supernatants from the unencapsulated Cap-67 strain were separated by anion-exchange chromatography. After further fractionation by preparative sodium dodecyl sulfate-polyacrylamide gel electrophoresis, a purified protein with an apparent molecular mass of 25 kDa was found to produce DTH, as evidenced by increased footpad swelling in mice immunized with culture supernatants, relative to unimmunized mice. The 20-amino-acid N-terminal sequence of the 25-kDa protein was used to search data of theC. neoformansGenome Project. Based on the genomic DNA sequence, a DNA probe was used to screen a λ cDNA library prepared from strain B3501. Clones were isolated containing the full-length gene (d25), which showed homology with a number of polysaccharide deacetylases from fungi and bacteria. The recombinant d25 protein expressed inEscherichia coliwas similar to the natural one in DTH-producing activity. Moreover, immunization with either the natural or the recombinant protein prolonged survival and decreased fungal burden in mice challenged with the highly virulentC. neoformansstrain H99. In conclusion, we have described the first cryptococcal gene whose product, a 25-kDa extracellular polysaccharide deacetylase, has been shown to induce protective immunity responses.

Published
2002

44. Surface Interactome in Streptococcus pyogenes

Author

Barbara Lelli, Fabiana Falugi, Silvia Pileri, Luisa Bracci, Emiliano Chiarot, Guido Grandi, Elia Bove, Alfredo Pezzicoli, Nathalie Norais, Sergio Balloni, Vittorio Tedde, Cesira Galeotti, Renata Grifantini, Mauro Bombaci, Marco Soriani, Renzo Nogarotto, Galeotti CL, Bove E, Pezzicoli A, Nogarotto R, Norais N, Pileri S, Lelli B, Falugi F, Balloni S, Tedde V, Chiarot E, Bombaci M, Soriani M, Bracci L, Grandi G, and Grifantini R

Subjects
Streptococcus pyogenes, Research, Protein Array Analysis, Plasma protein binding, Biology, medicine.disease_cause, Biochemistry, Interactome, Analytical Chemistry, Microbiology, Protein–protein interaction, Cell biology, Bacterial Proteins, Chlorides, Zinc Compounds, medicine, Protein microarray, Protein folding, Molecular Biology, Function (biology), Protein Binding
Abstract

Very few studies have so far been dedicated to the systematic analysis of protein interactions occurring between surface and/or secreted proteins in bacteria. Such interactions are expected to play pivotal biological roles that deserve investigation. Taking advantage of the availability of a detailed map of surface and secreted proteins in Streptococcus pyogenes (group A Streptococcus (GAS)), we used protein array technology to define the "surface interactome" in this important human pathogen. Eighty-three proteins were spotted on glass slides in high density format, and each of the spotted proteins was probed for its capacity to interact with any of the immobilized proteins. A total of 146 interactions were identified, 25 of which classified as "reciprocal," namely, interactions that occur irrespective of which of the two partners was immobilized on the chip or in solution. Several of these interactions were validated by surface plasmon resonance and supported by confocal microscopy analysis of whole bacterial cells. By this approach, a number of interesting interactions have been discovered, including those occurring between OppA, DppA, PrsA, and TlpA, proteins known to be involved in protein folding and transport. These proteins, all localizing at the septum, might be part, together with HtrA, of the recently described ExPortal complex of GAS. Furthermore, SpeI was found to strongly interact with the metal transporters AdcA and Lmb. Because SpeI strictly requires zinc to exert its function, this finding provides evidence on how this superantigen, a major player in GAS pathogenesis, can acquire the metal in the host environment, where it is largely sequestered by carrier proteins. We believe that the approach proposed herein can lead to a deeper knowledge of the mechanisms underlying bacterial invasion, colonization, and pathogenesis.

Published
2012

45. Bifunctional heterobimetallic 3d-4f [Co(II)-RE, RE = Dy, Eu, and Y] ionic complexes: modulation of the magnetic-luminescence behaviour.

Author

Bombaci M, Lo Presti F, Pellegrino AL, Lippi M, Rossi P, Tacconi L, Sorace L, and Malandrino G

Abstract

This work reports the engineering and functional properties of an emerging class of heterobimetallic 3d-4f ionic complexes designed with cobalt and rare-earth (RE) metals. We present a comprehensive examination of the structural, magnetic, optical, and thermal properties of the heterobimetallic ionic complexes with the general formula [Co(hfa) 3 ] - [RE(hfa) 2 tetraglyme] + (RE = Dy, Eu, and Y), where the metal centres are coordinated by hexafluoroacetylacetonate (Hhfa = 1,1,1,5,5,5-hexafluoro-2,4-pentanedione), β-diketone and tetraglyme (2,5,8,11,14-pentaoxapentadecane) polyether. Structural analysis reveals an octahedral coordination geometry enveloping the cobalt(II) centre, characterized by inherent symmetry properties consistent across the derivatives, while a capped square-antiprism coordination polyhedron is observed for the RE ions. Electron paramagnetic resonance (EPR) spectroscopy confirms the constancy of the electronic structure of the cobalt(II) moiety and the significant contribution of the lanthanide ions to the magnetic properties of the compounds. The non-trivial single-ion magnetic properties of cobalt(II), dysprosium(III), and europium(III) centres, and the effect of their interactions are investigated by a detailed static and dynamic magnetic susceptibility study. Moreover, optical analyses have been carried out showing the π-π* intraligand (IL) transition of the β-diketonate ligand and the d-d cobalt(II) transitions. Luminescence characterization of dysprosium(III) and europium(III) derivatives exhibits their characteristic emission bands, indicative of the unique photophysical properties conferred by the lanthanide ions. Thermal studies using thermogravimetric analysis (TGA) and differential scanning calorimetry (DSC) reveal good thermal stability and volatility properties, underscoring the interesting nature of these ionic complexes for potential deposition on suitable substrates. In summary, these heterobimetallic complexes show intriguing optical and magnetic properties with potential implications across diverse scientific disciplines, including molecular magnetism, optoelectronics, and materials science.

Published
2024
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46. Macrophages producing chondroitin sulfate proteoglycan-4 induce neuro-cardiac junction impairment in Duchenne muscular dystrophy.

Author

Milan M, Maiullari F, Chirivì M, Ceraolo MG, Zigiotto R, Soluri A, Maiullari S, Landoni E, Silvestre DD, Brambilla F, Mauri P, De Paolis V, Fratini N, Crosti MC, Cordiglieri C, Parisi C, Calogero A, Seliktar D, Torrente Y, Lanzuolo C, Dotti G, Toccafondi M, Bombaci M, De Falco E, Bearzi C, and Rizzi R

Abstract

Duchenne muscular dystrophy (DMD) is caused by the absence of the full form of the dystrophin protein, which is essential for maintaining the structural integrity of muscle cells, including those in the heart and respiratory system. Despite progress in understanding the molecular mechanisms associated with DMD, myocardial insufficiency persists as the primary cause of mortality, and existing therapeutic strategies remain limited. This study investigates the hypothesis that a dysregulation of the biological communication between infiltrating macrophages (MPs) and neurocardiac junctions exists in dystrophic cardiac tissue. In a mouse model of DMD (mdx), this phenomenon is influenced by the over-release of chondroitin sulfate proteoglycan-4 (CSPG4), a key inhibitor of nerve sprouting and a modulator of the neural function, by MPs infiltrating the cardiac tissue and associated with dilated cardiomyopathy, a hallmark of DMD. Givinostat, the histone deacetylase inhibitor under current development as a clinical treatment for DMD, is effective at both restoring a physiological microenvironment at the neuro-cardiac junction and cardiac function in mdx mice in addition to a reduction in cardiac fibrosis, MP-mediated inflammation, and tissue CSPG4 content. This study provides novel insight into the pathophysiology of DMD in the heart, identifying potential new biological targets. © 2024 The Author(s). The Journal of Pathology published by John Wiley & Sons Ltd on behalf of The Pathological Society of Great Britain and Ireland., (© 2024 The Author(s). The Journal of Pathology published by John Wiley & Sons Ltd on behalf of The Pathological Society of Great Britain and Ireland.)

Published
2024
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47. High-throughput peptide array analysis and computational techniques for serological profiling of flavivirus infections: Implications for diagnostics and vaccine development.

Author

Bombaci M, Fassi EMA, Gobbini A, Mileto D, Cassaniti I, Pesce E, Casali E, Mancon A, Sammartino J, Ferrari A, Percivalle E, Grande R, Marchisio E, Gismondo MR, Abrignani S, Baldanti F, Colombo G, and Grifantini R

Subjects
Humans, Peptides immunology, Vaccine Development, Computational Biology methods, Dengue diagnosis, Dengue immunology, Dengue blood, Dengue Virus immunology, Dengue Virus genetics, High-Throughput Screening Assays methods, Serologic Tests methods, Biomarkers blood, Viral Proteins immunology, Adult, Antibodies, Viral blood, Middle Aged, Male, Female, Zika Virus immunology, Flavivirus Infections diagnosis, Flavivirus Infections immunology, Flavivirus immunology, Protein Array Analysis methods
Abstract

Arthropod-borne viruses, such as dengue virus (DENV), pose significant global health threats, with DENV alone infecting around 400 million people annually and causing outbreaks beyond endemic regions. This study aimed to enhance serological diagnosis and discover new drugs by identifying immunogenic protein regions of DENV. Utilizing a comprehensive approach, the study focused on peptides capable of distinguishing DENV from other flavivirus infections through serological analyses. Over 200 patients with confirmed arbovirus infection were profiled using high-density pan flavivirus peptide arrays comprising 6253 peptides and the computational method matrix of local coupling energy (MLCE). Twenty-four peptides from nonstructural and structural viral proteins were identified as specifically recognized by individuals with DENV infection. Six peptides were confirmed to distinguish DENV from Zika virus (ZIKV), West Nile virus (WNV), Yellow Fever virus (YFV), Usutu virus (USUV), and Chikungunya virus (CHIKV) infections, as well as healthy controls. Moreover, the combination of two immunogenic peptides emerged as a potential serum biomarker for DENV infection. These peptides, mapping to highly accessible regions on protein structures, show promise for diagnostic and prophylactic strategies against flavivirus infections. The described methodology holds broader applicability in the serodiagnosis of infectious diseases., (© 2024 Wiley Periodicals LLC.)

Published
2024
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48. Identification of two autoantigens recognised by circulating autoantibodies as potential biomarkers for diagnosing giant cell arteritis.

Author

Pesce E, Bombaci M, Croci S, Bonacini M, Marvisi C, Ricordi C, Monti S, Muratore F, Abrignani S, Caporali R, Borghi MO, Salvarani C, Villiger PM, Grifantini R, and Meroni PL

Subjects
Humans, Female, Aged, Male, Middle Aged, Case-Control Studies, Takayasu Arteritis immunology, Takayasu Arteritis blood, Takayasu Arteritis diagnosis, Predictive Value of Tests, Protein Array Analysis, Enzyme-Linked Immunosorbent Assay, Giant Cell Arteritis immunology, Giant Cell Arteritis blood, Giant Cell Arteritis diagnosis, Autoantibodies blood, Biomarkers blood, Autoantigens immunology
Abstract

Objectives: Giant cell arteritis (GCA) is a common vasculitis affecting patients aged 50 and older. GCA leads to chronic inflammation of large/medium-sized vessel walls with complications such as permanent vision loss and risk of stroke and aortic aneurysms. Early diagnosis is crucial and relies on temporal artery biopsy (TAB) and ultrasound imaging of temporal and axillary arteries. However, these methods have limitations. Serum biomarkers as autoantibodies have been reported but with inconclusive data for their use in the clinical setting. Additionally, C-reactive protein and erythrocyte sedimentation rate are non-specific and limited in reflecting disease activity, particularly in patients treated with IL-6 inhibitors. This study aimed to identify serum autoantibodies as new diagnostic biomarkers for GCA using a human protein array., Methods: One commercial and one proprietary human protein array were used for antibody profiling of sera from patients with GCA (n=55), Takayasu (TAK n=7), and Healthy Controls (HC n=28). The identified candidate autoantigens were purified and tested for specific autoantibodies by ELISA., Results: Antibodies against two proteins, VSIG10L (V-Set and Immunoglobulin Domain Containing 10 Like) and DCBLD1 (discoidin), were identified and found to be associated with GCA, with an overall prevalence of 43-57%, respectively, and high specificity as individual antibodies. A control series of TAK sera tested negative., Conclusions: Detecting GCA-specific autoantibodies may offer a new, non-invasive tool for improving our diagnostic power in GCA. Even though cell-mediated immune responses are crucial for GCA pathogenesis, this finding opens the way for investigating the additional role of humoral immune responses in the disease.

Published
2024
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49. Tracking the immune response profiles elicited by the BNT162b2 vaccine in COVID-19 unexperienced and experienced individuals.

Author

Galeota E, Bevilacqua V, Gobbini A, Gruarin P, Bombaci M, Pesce E, Favalli A, Lombardi A, Vincenti F, Ongaro J, Fabbris T, Curti S, Martinovic M, Toccafondi M, Lorenzo M, Critelli A, Clemente F, Crosti M, Sarnicola ML, Martinelli M, La Sala L, Espadas A, Donnici L, Borghi MO, De Feo T, De Francesco R, Prati D, Meroni PL, Notarbartolo S, Geginat J, Gori A, Bandera A, Abrignani S, and Grifantini R

Subjects
Humans, BNT162 Vaccine, SARS-CoV-2, Pandemics, Vaccination, Antibodies, Neutralizing, Antibodies, Viral, COVID-19 prevention & control, Vaccines
Abstract

Multiple vaccines have been approved to control COVID-19 pandemic, with Pfizer/BioNTech (BNT162b2) being widely used. We conducted a longitudinal analysis of the immune response elicited after three doses of the BNT162b2 vaccine in individuals who have previously experienced SARS-CoV-2 infection and in unexperienced ones. We conducted immunological analyses and single-cell transcriptomics of circulating T and B lymphocytes, combined to CITE-seq or LIBRA-seq, and VDJ-seq. We found that antibody levels against SARS-CoV-2 Spike, NTD and RBD from wild-type, delta and omicron VoCs show comparable dynamics in both vaccination groups, with a peak after the second dose, a decline after six months and a restoration after the booster dose. The antibody neutralization activity was maintained, with lower titers against the omicron variant. Spike-specific memory B cell response was sustained over the vaccination schedule. Clonal analysis revealed that Spike-specific B cells were polyclonal, with a partial clone conservation from natural infection to vaccination. Spike-specific T cell responses were oriented towards effector and effector memory phenotypes, with similar trends in unexperienced and experienced individuals. The CD8 T cell compartment showed a higher clonal expansion and persistence than CD4 T cells. The first two vaccinations doses tended to induce new clones rather than promoting expansion of pre-existing clones. However, we identified a fraction of Spike-specific CD8 T cell clones persisting from natural infection that were boosted by vaccination and clones specifically induced by vaccination. Collectively, our observations revealed a moderate effect of the second dose in enhancing the immune responses elicited after the first vaccination. Differently, we found that a third dose was necessary to restore comparable levels of neutralizing antibodies and Spike-specific T and B cell responses in individuals who experienced a natural SARS-CoV-2 infection., Competing Interests: Declaration of competing interest Author Renata Grifantini is currently employed by CheckmAb Srl. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024. Published by Elsevier Inc.)

Published
2024
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50. SARS-COV-2 specific t-cells in patients with thyroid disorders related to COVID-19 are enriched in the thyroid and acquire a tissue-resident memory phenotype.

Author

Silvestri Y, Clemente F, Moschetti G, Maioli S, Carelli E, Espadas de Arias A, Torelli R, Longhi E, De Feo T, Crosti M, Sarnicola ML, Salvi M, Mantovani G, Arosio M, Bombaci M, Pesce E, Grifantini R, Abrignani S, Geginat J, and Muller I

Subjects
Humans, SARS-CoV-2, RNA, Viral, Phenotype, Antibodies, Thyroid Gland, COVID-19
Abstract

Background: SARS-CoV-2 infections have been associated with the onset of thyroid disorders like classic subacute thyroiditis (SAT) or atypical SAT upon severe COVID disease (COV-A-SAT). Little is known about thyroid anti-viral immune responses., Objectives: To define the role of T-cells in COV-A-SAT., Methods: T-cells from COV-A-SAT patients were analyzed by multi-dimensional flow cytometry, UMAP and DiffusionMap dimensionality reduction and FlowSOM clustering. T-cells from COVID-naïve healthy donors, patients with autoimmune thyroiditis (ATD) and with SAT following COVID vaccination were analyzed as controls. T-cells were analyzed four and eight months post-infection in peripheral blood and in thyroid specimen obtained by ultrasound-guided fine needle aspiration. SARS-COV2-specific T-cells were identified by cytokine production induced by SARS-COV2-derived peptides and with COVID peptide-loaded HLA multimers after HLA haplotyping., Results: COV-A-SAT was associated with HLA-DRB1*13 and HLA-B*57. COV-A-SAT patients contained activated Th1- and cytotoxic CD4+ and CD8+ effector cells four months post-infection, which acquired a quiescent memory phenotype after eight months. Anti-SARS-CoV-2-specific T-cell responses were readily detectable in peripheral blood four months post-infection, but were reduced after eight months. CD4+ and CD8+ tissue-resident memory cells (TRM) were present in the thyroid, and circulating CXCR3+T-cells identified as their putative precursors. SARS-CoV-2-specific T-cells were enriched in the thyroid, and acquired a TRM phenotype eight months post-infection., Conclusions: The association of COV-A-SAT with specific HLA haplotypes suggests a genetic predisposition and a key role for T-cells. COV-A-SAT is characterized by a prolonged systemic anti-viral effector T-cell response and the late generation of COVID-specific TRM in the thyroid target tissue., Competing Interests: Declaration of Competing Interest We declare no conflict of interest., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2023
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