Your search keyword '"Camponeschi C"' showing total 18 results

1. Recovering or Persisting: The Immunopathological Features of SARS-CoV-2 Infection in Children

Author

Buonsenso, Danilo, Valentini, Piero, De Rose, Cristina, Tredicine, Maria, Pereyra Boza, Maria Del Carmen, Camponeschi, C., Morello, Rosa, Zampino, Giuseppe, Brooks, A. E. S., Rende, M., Ria, Francesco, Sanguinetti, Maurizio, Delogu, Giovanni, Sali, Michela, Di Sante, Gabriele, Buonsenso D., Valentini P. (ORCID:0000-0001-6095-9510), De Rose C., Tredicine M., Pereyra Boza M. D. C., Morello R., Zampino G. (ORCID:0000-0003-3865-3253), Ria F. (ORCID:0000-0002-8444-0307), Sanguinetti M. (ORCID:0000-0002-9780-7059), Delogu G. (ORCID:0000-0003-0182-8267), Sali M. (ORCID:0000-0003-3609-2990), Di Sante G. (ORCID:0000-0001-6608-3388), Buonsenso, Danilo, Valentini, Piero, De Rose, Cristina, Tredicine, Maria, Pereyra Boza, Maria Del Carmen, Camponeschi, C., Morello, Rosa, Zampino, Giuseppe, Brooks, A. E. S., Rende, M., Ria, Francesco, Sanguinetti, Maurizio, Delogu, Giovanni, Sali, Michela, Di Sante, Gabriele, Buonsenso D., Valentini P. (ORCID:0000-0001-6095-9510), De Rose C., Tredicine M., Pereyra Boza M. D. C., Morello R., Zampino G. (ORCID:0000-0003-3865-3253), Ria F. (ORCID:0000-0002-8444-0307), Sanguinetti M. (ORCID:0000-0002-9780-7059), Delogu G. (ORCID:0000-0003-0182-8267), Sali M. (ORCID:0000-0003-3609-2990), and Di Sante G. (ORCID:0000-0001-6608-3388)

Abstract

Background. The profile of cellular immunological responses of children across the spectrum of COVID-19, ranging from acute SARS-CoV-2 infection to full recovery or Long COVID, has not yet been fully investigated. Methods. We examined and compared cytokines in sera and cell subsets in peripheral blood mononuclear cells (B and regulatory T lymphocytes) collected from four distinct groups of children, distributed as follows: younger than 18 years of age with either acute SARS-CoV-2 infection (n = 49); fully recovered from COVID-19 (n = 32); with persistent symptoms (Long COVID, n = 51); and healthy controls (n = 9). Results. In the later stages after SARS-CoV-2 infection, the cohorts of children, both with recovered and persistent symptoms, showed skewed T and B subsets, with remarkable differences when compared with children at the onset of the infection and with controls. The frequencies of IgD+CD27− naïve B cells, IgD+IgM+ and CD27−IgM+CD38dim B cells were higher in children with recent infection than in those with an older history of disease (p < 0.0001 for all); similarly, the total and natural Tregs compartments were more represented in children at onset when compared with Long COVID (p < 0.0001 and p = 0.0005, respectively). Despite the heterogeneity, partially due to age, sex and infection incidence, the susceptibility of certain children to develop persistent symptoms after infection appeared to be associated with the imbalance of the adaptive immune response. Following up and comparing recovered versus Long COVID patients, we analyzed the role of circulating naïve and switched B and regulatory T lymphocytes in counteracting the evolution of the symptomatology emerged, finding an interesting correlation between the amount and ability to reconstitute the natural Tregs component with the persistence of symptoms (linear regression, p = 0.0026). Conclusions. In this study, we suggest that children affected by Long COVID may have a compromised ability to s

Published

2022

2. Study of the effects of Lemna minor extracts on human immune cell populations

Author

Catelani Cardoso, C., Miraldi, E., Ceccarini, M. R., Naureen, Z., Baini, G., Manara, E., Anpilogov, K., Camilleri, G., Dhuli, K., Paolacci, S., Ria, Francesco, Di Sante, Gabriele, Camponeschi, C., Tredicine, Maria, Zanlari, A., Chiurazzi, Pietro, Beccari, T., Bertelli, M., Ria F. (ORCID:0000-0002-8444-0307), Di Sante G. (ORCID:0000-0001-6608-3388), Tredicine M., Chiurazzi P. (ORCID:0000-0001-5104-1521), Catelani Cardoso, C., Miraldi, E., Ceccarini, M. R., Naureen, Z., Baini, G., Manara, E., Anpilogov, K., Camilleri, G., Dhuli, K., Paolacci, S., Ria, Francesco, Di Sante, Gabriele, Camponeschi, C., Tredicine, Maria, Zanlari, A., Chiurazzi, Pietro, Beccari, T., Bertelli, M., Ria F. (ORCID:0000-0002-8444-0307), Di Sante G. (ORCID:0000-0001-6608-3388), Tredicine M., and Chiurazzi P. (ORCID:0000-0001-5104-1521)

Abstract

OBJECTIVE: Lemna minor is a plant with a huge repertoire of secondary metabolites. The literature indicates that extracts of Lemna minor have antioxidant, antiradical, immunomodulatory and anti-inflammatory properties. The objective of the present study was to find a suitable technique to extract active compounds from this plant and verify whether these extracts have immunomodulatory activity. MATERIALS AND METHODS: We grew L. minor on a standard medium with Gamborg B5 and vitamins. We extracted compounds from the plant by maceration and decoction. The phytochemical profile of the extracts was characterized by chromatography, spectrophotometry, and spectroscopy. The extracts were tested on cultures of mononuclear cells from four human subjects. These cells were pulsed with carboxyfluorescein succinimidyl ester, grown in triplicate in standard culture medium without (control) and with increasing concentrations of Lemna extracts. Flow cytometry was used to evaluate cell death and proliferation of the total mononuclear cell population and of CD4+, CD8+, B cell and monocyte populations. RESULTS: The Lemna extracts were not cytotoxic and did not cause cell necrosis or apoptosis in immune cells. At low concentrations, they induced very limited proliferation of CD4+ cells within 48 hours. At high concentrations, they induced proliferation of CD8+ cells and B lymphocytes within 48 hours. CONCLUSIONS: Unfortunately, we failed to confirm any immunomodulatory activity of Lemna extracts. Growth and death rates of human immune cells were not significantly affected by adding Lemna extracts to the culture medium.

Published

2021

3. S100B protein as a therapeutic target in multiple sclerosis: The S100B inhibitor arundic acid protects from chronic experimental autoimmune encephalomyelitis

Author

Camponeschi, C., De Carluccio, M., Amadio, S., Clementi, Maria Elisabetta, Sampaolese, B., Volonte, C., Tredicine, Maria, Spica, V. R., Di Liddo, R., Ria, Francesco, Michetti, Fabrizio, Di Sante, Gabriele, Clementi M. E., Tredicine M., Ria F. (ORCID:0000-0002-8444-0307), Michetti F. (ORCID:0000-0003-2546-0532), Di Sante G. (ORCID:0000-0001-6608-3388), Camponeschi, C., De Carluccio, M., Amadio, S., Clementi, Maria Elisabetta, Sampaolese, B., Volonte, C., Tredicine, Maria, Spica, V. R., Di Liddo, R., Ria, Francesco, Michetti, Fabrizio, Di Sante, Gabriele, Clementi M. E., Tredicine M., Ria F. (ORCID:0000-0002-8444-0307), Michetti F. (ORCID:0000-0003-2546-0532), and Di Sante G. (ORCID:0000-0001-6608-3388)

Abstract

S100B is an astrocytic protein behaving at high concentration as a damage-associated molecular pattern molecule. A direct correlation between the increased amount of S100B and inflammatory processes has been demonstrated, and in particular, the inhibitor of S100B activity pentamidine has been shown to ameliorate clinical scores and neuropathologic-biomolecular parameters in the relapsing-remitting experimental autoimmune encephalomyelitis mouse model of multiple sclerosis. This study investigates the effect of arundic acid (AA), a known inhibitor of astrocytic S100B synthesis, in the chronic experimental autoimmune encephalomyelitis, which is another mouse model of multiple sclerosis usually studied. By the daily evaluation of clinical scores and neuropathologic-molecular analysis performed in the spinal cord, we observed that the AA-treated group showed lower severity compared to the vehicle-treated mice, particularly in the early phase of disease onset. We also observed a significant reduction of astrocytosis, demyelination, immune infiltrates, proinflammatory cytokines expression and enzymatic oxidative reactivity in the AA-treated group. Overall, our results reinforce the involvement of S100B in the development of animal models of multiple sclerosis and propose AA targeting the S100B protein as a focused potential drug to be considered for multiple sclerosis treatment.

Published

2021

4. Study of the effects of Lemna minor extracts on human immune cell populations.

Author

CARDOSO, C. CATELANI, MIRALDI, E., CECCARINI, M. R., NAUREEN, Z., BAINI, G., MANARA, E., ANPILOGOV, K., CAMILLERI, G., DHULI, K., PAOLACCI, S., RIA, F., DI SANTE, G., CAMPONESCHI, C., TREDICINE, M., ZANLARI, A., CHIURAZZI, P., BECCARI, T., and BERTELLI, M.

Abstract

OBJECTIVE: Lemna minor is a plant with a huge repertoire of secondary metabolites. The literature indicates that extracts of Lemna minor have antioxidant, antiradical, immunomodulatory and anti-inflammatory properties. The objective of the present study was to find a suitable technique to extract active compounds from this plant and verify whether these extracts have immunomodulatory activity. MATERIALS AND METHODS: We grew L. minor on a standard medium with Gamborg B5 and vitamins. We extracted compounds from the plant by maceration and decoction. The phytochemical profile of the extracts was characterized by chromatography, spectrophotometry, and spectroscopy. The extracts were tested on cultures of mononuclear cells from four human subjects. These cells were pulsed with carboxyfluorescein succinimidyl ester, grown in triplicate in standard culture medium without (control) and with increasing concentrations of Lemna extracts. Flow cytometry was used to evaluate cell death and proliferation of the total mononuclear cell population and of CD4+, CD8+, B cell and monocyte populations. RESULTS: The Lemna extracts were not cytotoxic and did not cause cell necrosis or apoptosis in immune cells. At low concentrations, they induced very limited proliferation of CD4+ cells within 48 hours. At high concentrations, they induced proliferation of CD8+ cells and B lymphocytes within 48 hours. CONCLUSIONS: Unfortunately, we failed to confirm any immunomodulatory activity of Lemna extracts. Growth and death rates of human immune cells were not significantly affected by adding Lemna extracts to the culture medium. [ABSTRACT FROM AUTHOR]

Published

2021

5. Potential of Energy Saving of Propane Heat Pump as replacement of gas boilers with low and high temperature emitters

Author

Camponeschi Corrado, Goni Maurizio, Cioffi Francesca, Dongellini Matteo, Naldi Claudia, Morini Gian Luca, Germano Luca, Genovese Filippo, Cervellati Andrea, Casolari Alessandro, Corsaro Federico, Ciancamerla Matteo, and Ballotta Luca

Subjects

air-source heat pumps, r290 (propane), global warming potential, energy efficiency, environmental impact, Environmental sciences, GE1-350

Abstract

This work deals with the analysis of the energy performance and the environmental impact of a Heating, Ventilation and Air Conditioning (HVAC) system based on an innovative Air-to-Water electrical Heat Pump (AWHP) using propane (R290) as the refrigerant. A building of the University of Bologna located in Forlì (North of Italy) is considered for replacing a condensing gas boiler and a conventional chiller with an AWHP using R290. To evaluate the efficiency of the existing heating system and the potential savings linked to the adoption of the propane AWHP, the building energy model was created and calibrated by collecting monthly thermal and electrical consumptions as a function of the actual climate data. In this paper, the main features of the R290-based AWHP are described in detail by emphasising the device performance as a function of the operating conditions (i.e., air and water temperature and speed of the scroll compressor). A series of scenarios have been studied to evaluate the energy performance of the propane AWHP with respect to the reference scenario under various operating conditions. The results show that while the total primary energy demand increases adopting the propane AWHP with respect to the case of a gas boiler, the non-renewable primary energy fraction decreases significantly, with a dramatic increase in the renewable quote. From an economic point of view, lower annual costs are obtained by adopting a propane AWHP coupled to fan coils, mainly when the electrical heat pump is used in a thermally insulated building in which a photovoltaic system is installed.

Published

2024

6. A TLR/CD44 axis regulates T cell trafficking in experimental and human multiple sclerosis

Author

Maria Tredicine, Chiara Camponeschi, Davide Pirolli, Matteo Lucchini, Mariagrazia Valentini, Maria Concetta Geloso, Massimiliano Mirabella, Marco Fidaleo, Benedetta Righino, Camilla Moliterni, Ezio Giorda, Mario Rende, Maria Cristina De Rosa, Maria Foti, Gabriela Constantin, Francesco Ria, Gabriele Di Sante, Tredicine, M, Camponeschi, C, Pirolli, D, Lucchini, M, Valentini, M, Geloso, M, Mirabella, M, Fidaleo, M, Righino, B, Moliterni, C, Giorda, E, Rende, M, De Rosa, M, Foti, M, Constantin, G, Ria, F, and Di Sante, G

Subjects

Settore BIO/16 - ANATOMIA UMANA, Cell biology, Multidisciplinary, Settore MED/04 - PATOLOGIA GENERALE, Molecular biology, Science, Immunology, Molecular modeling, CD44, multiple sclerosis, Article

Abstract

Summary In the pathogenesis of autoimmune disorders, the modulation of leukocytes′ trafficking plays a central role, still poorly understood. Here, we focused on the effect of TLR2 ligands in trafficking of T helper cells through reshuffling of CD44 isoforms repertoire. Concurrently, strain background and TLR2 haplotype affected Wnt/β-catenin signaling pathway and expression of splicing factors. During EAE, mCD44v9-v10 was specifically enriched in the forebrain and showed an increased ability to bind stably to osteopontin. Similarly, we observed that hCD44v7 was highly enriched in cells of cerebrospinal fluid from MS patients with active lesions. Moreover, TLRs engagement modulated the composition of CD44 variants also in human T helper cells, supporting the hypothesis that pathogens or commensals, through TLRs, in turn modulate the repertoire of CD44 isoforms, thereby controlling the distribution of lesions in the CNS. The interference with this mechanism(s) represents a potential tool for prevention and treatment of autoimmune relapses and exacerbations., Graphical abstract Host-Pathogen interaction modulating T cell trafficking and tissue infiltration through CD44 variants (CD44v). Circulating T cells through lymphoid and non-lymphoid organs, regulate homeostasis of immune system. The environment could lead an imbalance, also acting on the ability of T cells to move. The expression of certain CD44 isoforms can explain the ability of T cells to infiltrate into the CNS of patients affected by multiple sclerosis, crossing the blood brain barrier. This effect seems to be associated with microbial products, able to modulate CD44 splicing on T cells, that regulate their ability to move (Vestweber, 2015). Created with Biorender.com., Highlights • Environment and genetic are both involved in the regulation of T cell motility • Pathogens and commensals impact on T cell trafficking through a TLRs/CD44v axis • Regulation of CD44 isoforms by TLRs is a new pathogenetic mechanism of autoimmunity • Modulation of CD44 isoform can be a new target for therapy of multiple sclerosis, Molecular biology; Immunology; Cell biology

Published

2022

7. Seeing COVID-19 through an urban lens

Author

Michele Acuto, Roger Keil, Shaun Larcom, Chiara Camponeschi, Susan Parnell, Tom Lindsay, Mehrnaz Ghojeh, Acuto, M [0000-0003-4320-0531], Larcom, S [0000-0003-0029-3264], Keil, R [0000-0002-1904-4623], Camponeschi, C [0000-0002-9905-2921], Parnell, S [0000-0002-5702-1684], and Apollo - University of Cambridge Repository

Subjects

Global and Planetary Change, 2019-20 coronavirus outbreak, Ecology, Coronavirus disease 2019 (COVID-19), Renewable Energy, Sustainability and the Environment, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), fungi, Geography, Planning and Development, food and beverages, Lens (geology), Environmental ethics, social sciences, Management, Monitoring, Policy and Law, 41 Environmental Sciences, Urban Studies, Environmental studies, Pandemic, 11 Sustainable Cities and Communities, population characteristics, 10 Reduced Inequalities, human activities, Nature and Landscape Conservation, Food Science, 40 Engineering

Abstract

COVID-19 has changed the face of cities and recast urban life globally. In turn, cities have become the major theatres of the crisis for a once-in-a-century test to global resilience. Global health governance has thus far struggled to face up to the urban character of the pandemic. The UN Secretary General recently called for a better appreciation of how COVID-19 is unfolding in “an urban world” if we are to rebuild more sustainably. We argue it is imperative do so by attending to urban inequalities that underpin the crisis, and by understanding the fundamental inclusive development opportunity at play here if we allow urban expertise, and cities, closer to the heart of the global response. Under the presumptive ‘new normal’ of COVID-19, multiple intersecting policy agendas have come to the fore not just in the shape of health concerns but also with regards to environmental sustainability and ‘green’ economic recovery. Much of this has had to do with recasting the ways we live in cities. The UN has already stressed that approximately 95% of COVID-19 cases have taken place in urban settlements, with over 1,500 cities affected worldwide. Many have made the case that post-pandemic planning discussion must transcend dualistic framings pitting ‘health’ versus ‘environmental’ concerns, whilst not giving in to simplistic economic growth approaches. By far and large that implies radical changes to our cities and urban livelihoods. Yet these are rarely at the centre of the multilateral debate. We urgently need to attend to the urban socio-economic crisis underpinning COVID-19 that unfolds amidst the most vulnerable in cities both at the inter- and intra-urban scale.

Published

2020

8. Prediction of CD44 Structure by Deep Learning-Based Protein Modeling.

Author

Camponeschi C, Righino B, Pirolli D, Semeraro A, Ria F, and De Rosa MC

Subjects

Carrier Proteins metabolism, Deep Learning, Extracellular Matrix metabolism, Hyaluronic Acid chemistry, Molecular Dynamics Simulation, Receptors, Cell Surface metabolism, Humans, Animals, Hyaluronan Receptors chemistry, Hyaluronan Receptors metabolism

Abstract

CD44 is a cell surface glycoprotein transmembrane receptor that is involved in cell-cell and cell-matrix interactions. It crucially associates with several molecules composing the extracellular matrix, the main one of which is hyaluronic acid. It is ubiquitously expressed in various types of cells and is involved in the regulation of important signaling pathways, thus playing a key role in several physiological and pathological processes. Structural information about CD44 is, therefore, fundamental for understanding the mechanism of action of this receptor and developing effective treatments against its aberrant expression and dysregulation frequently associated with pathological conditions. To date, only the structure of the hyaluronan-binding domain (HABD) of CD44 has been experimentally determined. To elucidate the nature of CD44s, the most frequently expressed isoform, we employed the recently developed deep-learning-based tools D-I-TASSER, AlphaFold2, and RoseTTAFold for an initial structural prediction of the full-length receptor, accompanied by molecular dynamics simulations on the most promising model. All three approaches correctly predicted the HABD, with AlphaFold2 outperforming D-I-TASSER and RoseTTAFold in the structural comparison with the crystallographic HABD structure and confidence in predicting the transmembrane helix. Low confidence regions were also predicted, which largely corresponded to the disordered regions of CD44s. These regions allow the receptor to perform its unconventional activity.

Published

2023

9. Publisher Correction: Virtual screening and molecular dynamics simulations provide insight into repurposing drugs against SARS-CoV-2 variants Spike protein/ACE2 interface.

Author

Pirolli D, Righino B, Camponeschi C, Ria F, Di Sante G, and De Rosa MC

Published

2023

10. Virtual screening and molecular dynamics simulations provide insight into repurposing drugs against SARS-CoV-2 variants Spike protein/ACE2 interface.

Author

Pirolli D, Righino B, Camponeschi C, Ria F, Di Sante G, and De Rosa MC

Subjects

Humans, Angiotensin-Converting Enzyme 2, Drug Repositioning, Molecular Docking Simulation, SARS-CoV-2, Spike Glycoprotein, Coronavirus, Protein Binding, Molecular Dynamics Simulation, COVID-19

Abstract

After over two years of living with Covid-19 and hundreds of million cases worldwide there is still an unmet need to find proper treatments for the novel coronavirus, due also to the rapid mutation of its genome. In this context, a drug repositioning study has been performed, using in silico tools targeting Delta Spike protein/ACE2 interface. To this aim, it has been virtually screened a library composed by 4388 approved drugs through a deep learning-based QSAR model to identify protein-protein interactions modulators for molecular docking against Spike receptor binding domain (RBD). Binding energies of predicted complexes were calculated by Molecular Mechanics/Generalized Born Surface Area from docking and molecular dynamics simulations. Four out of the top twenty ranking compounds showed stable binding modes on Delta Spike RBD and were evaluated also for their effectiveness against Omicron. Among them an antihistaminic drug, fexofenadine, revealed very low binding energy, stable complex, and interesting interactions with Delta Spike RBD. Several antihistaminic drugs were found to exhibit direct antiviral activity against SARS-CoV-2 in vitro, and their mechanisms of action is still debated. This study not only highlights the potential of our computational methodology for a rapid screening of variant-specific drugs, but also represents a further tool for investigating properties and mechanisms of selected drugs., (© 2023. The Author(s).)

Published

2023

11. Liposome-based nanoparticles impact on regulatory and effector phenotypes of macrophages and T cells in multiple Sclerosis patients.

Author

Tredicine M, Ria F, Poerio N, Lucchini M, Bianco A, De Santis F, Valentini M, De Arcangelis V, Rende M, Stabile AM, Pistilli A, Camponeschi C, Nociti V, Mirabella M, Fraziano M, and Di Sante G

Subjects

Humans, Liposomes metabolism, Phosphatidylserines, Macrophages metabolism, Phenotype, Multiple Sclerosis drug therapy, Nanoparticles

Abstract

Current available treatments of Multiple Sclerosis (MS) reduce neuroinflammation acting on different targets on the immune system, but potentially lead to severe side effects and have a limited efficacy in slowing the progression of the disease. Here, we evaluated in vitro the immunomodulatory potential of a new class of nanoparticles - liposomes, constituted by a double-layer of phosphatidylserine (PSCho/PS), and double-faced, with an outer layer of phosphatidylserine and an inner layer of phosphatidic acid (PSCho/PA), either alone or in the presence of the myelin basic protein (MBP) peptide (residues 85-99) (PSCho/PS-MBP and PSCho/PA-MBP). Results showed that PSCho/PS are equally and efficiently internalized by pro- and anti-inflammatory macrophages (M1 and M2 respectively), while PSCho/PA were internalized better by M2 than M1. PSCho/PS liposomes were able to inhibit the secretion of innate pro-inflammatory cytokine IL-1β. PSCho/PS liposomes expanded Tregs, reducing Th1 and Th17 cells, while PSCho/PA liposomes were unable to dampen pro-inflammatory T cells and to promote immune-regulatory phenotype (Treg). The ability of PSCho/PS liposomes to up-regulate Treg cells was more pronounced in MS patients with high basal expression of M2 markers. PSCho/PS liposomes were more effective in decreasing Th1 (but not Th17) cells in MS patients with a disease duration >3 months. On the other hand, down-modulation of Th17 cells was evident in MS patients with active, Gadolinium enhancing lesions at MRI and in MS patients with a high basal expression of M1-associated markers in the monocytes. The same findings were observed for the modulation of MBP-driven Th1/Th17/Treg responses. These observations suggest that early MS associate to a hard-wired pro-Th1 phenotype of M1 that is lost later during disease course. On the other hand, acute inflammatory events reflect a temporary decrease of M2 phenotype that however is amenable to restauration upon treatment with PSCho/PS liposomes. Thus, together these data indicate that monocytes/macrophages may play an important regulatory function during MS course and suggest a role for PSCho/PS and PSCho/PS-MBP as new therapeutic tools to dampen the pro-inflammatory immune responses and to promote its regulatory branch., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests:Gabriele Di Sante reports financial support was provided by Fondazione Cassa di Risparmio di Perugia. Francesco Ria reports financial support was provided by Italian Multiple Sclerosis Association. Maurizio Fraziano reports financial support was provided by Italian Multiple Sclerosis Association. Francesco Ria reports financial support was provided by Università Cattolica del Sacro Cuore., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2023

12. Recovering or Persisting: The Immunopathological Features of SARS-CoV-2 Infection in Children.

Author

Buonsenso D, Valentini P, De Rose C, Tredicine M, Pereyra Boza MDC, Camponeschi C, Morello R, Zampino G, Brooks AES, Rende M, Ria F, Sanguinetti M, Delogu G, Sali M, Di Sante G, and On Behalf Of The Gemelli-Pediatric Covid-Team

Abstract

Background. The profile of cellular immunological responses of children across the spectrum of COVID-19, ranging from acute SARS-CoV-2 infection to full recovery or Long COVID, has not yet been fully investigated. Methods. We examined and compared cytokines in sera and cell subsets in peripheral blood mononuclear cells (B and regulatory T lymphocytes) collected from four distinct groups of children, distributed as follows: younger than 18 years of age with either acute SARS-CoV-2 infection (n = 49); fully recovered from COVID-19 (n = 32); with persistent symptoms (Long COVID, n = 51); and healthy controls (n = 9). Results. In the later stages after SARS-CoV-2 infection, the cohorts of children, both with recovered and persistent symptoms, showed skewed T and B subsets, with remarkable differences when compared with children at the onset of the infection and with controls. The frequencies of IgD+CD27− naïve B cells, IgD+IgM+ and CD27−IgM+CD38dim B cells were higher in children with recent infection than in those with an older history of disease (p < 0.0001 for all); similarly, the total and natural Tregs compartments were more represented in children at onset when compared with Long COVID (p < 0.0001 and p = 0.0005, respectively). Despite the heterogeneity, partially due to age, sex and infection incidence, the susceptibility of certain children to develop persistent symptoms after infection appeared to be associated with the imbalance of the adaptive immune response. Following up and comparing recovered versus Long COVID patients, we analyzed the role of circulating naïve and switched B and regulatory T lymphocytes in counteracting the evolution of the symptomatology emerged, finding an interesting correlation between the amount and ability to reconstitute the natural Tregs component with the persistence of symptoms (linear regression, p = 0.0026). Conclusions. In this study, we suggest that children affected by Long COVID may have a compromised ability to switch from the innate to the adaptive immune response, as supported by our data showing a contraction of naïve and switched B cell compartment and an unstable balance of regulatory T lymphocytes occurring in these children. However, further prospective immunological studies are needed to better clarify which factors (epigenetic, diet, environment, etc.) are involved in the impairment of the immunological mechanisms in the Long COVID patients., Competing Interests: The authors declare no conflict of interest.

Published

2022

13. Immunopathology of SARS-CoV-2 Infection: A Focus on T Regulatory and B Cell Responses in Children Compared with Adults.

Author

Di Sante G, Buonsenso D, De Rose C, Tredicine M, Palucci I, De Maio F, Camponeschi C, Bonadia N, Biasucci D, Pata D, Chiaretti A, Valentini P, Ria F, Sanguinetti M, and Sali M

Abstract

While the clinical impact of COVID-19 on adults has been massive, the majority of children develop pauci-symptomatic or even asymptomatic infection and only a minority of the latter develop a fatal outcome. The reasons of such differences are not yet established. We examined cytokines in sera and Th and B cell subpopulations in peripheral blood mononuclear cells (PBMC) from 40 children (<18 years old), evaluating the impact of COVID-19 infection during the pandemic’s first waves. We correlated our results with clinical symptoms and compared them to samples obtained from 16 infected adults and 7 healthy controls. While IL6 levels were lower in SARS-CoV-2+ children as compared to adult patients, the expression of other pro-inflammatory cytokines such as IFNγ and TNFα directly correlated with early age infection and symptoms. Th and B cell subsets were modified during pediatric infection differently with respect to adult patients and controls and within the pediatric group based on age. Low levels of IgD− CD27+ memory B cells correlated with absent/mild symptoms. On the contrary, high levels of FoxP3+/CD25high T-Regs associated with a moderate−severe clinical course in the childhood. These T and B cells subsets did not associate with severity in infected adults, with children showing a predominant expansion of immature B lymphocytes and natural regulatory T cells. This study shows differences in immunopathology of SARS-CoV-2 infection in children compared with adults. Moreover, these data could provide information that can drive vaccination endpoints for children.

Published

2022

14. A TLR/CD44 axis regulates T cell trafficking in experimental and human multiple sclerosis.

Author

Tredicine M, Camponeschi C, Pirolli D, Lucchini M, Valentini M, Geloso MC, Mirabella M, Fidaleo M, Righino B, Moliterni C, Giorda E, Rende M, De Rosa MC, Foti M, Constantin G, Ria F, and Di Sante G

Abstract

In the pathogenesis of autoimmune disorders, the modulation of leukocytes' trafficking plays a central role, still poorly understood. Here, we focused on the effect of TLR2 ligands in trafficking of T helper cells through reshuffling of CD44 isoforms repertoire. Concurrently, strain background and TLR2 haplotype affected Wnt/β-catenin signaling pathway and expression of splicing factors. During EAE, m CD44 v9- v 10 was specifically enriched in the forebrain and showed an increased ability to bind stably to osteopontin. Similarly, we observed that h CD44 v7 was highly enriched in cells of cerebrospinal fluid from MS patients with active lesions. Moreover, TLRs engagement modulated the composition of CD44 variants also in human T helper cells, supporting the hypothesis that pathogens or commensals, through TLRs, in turn modulate the repertoire of CD44 isoforms, thereby controlling the distribution of lesions in the CNS. The interference with this mechanism(s) represents a potential tool for prevention and treatment of autoimmune relapses and exacerbations., Competing Interests: The authors declare no conflict of interest. The funders had no role in the design of the study; in the collection, analyses, or interpretation of data; in the writing of the manuscript, or in the decision to publish the results., (© 2022 The Authors.)

Published

2022

15. S100B Protein as a Therapeutic Target in Multiple Sclerosis: The S100B Inhibitor Arundic Acid Protects from Chronic Experimental Autoimmune Encephalomyelitis.

Author

Camponeschi C, De Carluccio M, Amadio S, Clementi ME, Sampaolese B, Volonté C, Tredicine M, Romano Spica V, Di Liddo R, Ria F, Michetti F, and Di Sante G

Subjects

Animals, Caprylates pharmacology, Disease Models, Animal, Encephalomyelitis, Autoimmune, Experimental metabolism, Female, Mice, Mice, Inbred C57BL, Molecular Targeted Therapy, Multiple Sclerosis metabolism, S100 Calcium Binding Protein beta Subunit metabolism, Caprylates therapeutic use, Encephalomyelitis, Autoimmune, Experimental drug therapy, Multiple Sclerosis drug therapy, S100 Calcium Binding Protein beta Subunit antagonists & inhibitors

Abstract

S100B is an astrocytic protein behaving at high concentration as a damage-associated molecular pattern molecule. A direct correlation between the increased amount of S100B and inflammatory processes has been demonstrated, and in particular, the inhibitor of S100B activity pentamidine has been shown to ameliorate clinical scores and neuropathologic-biomolecular parameters in the relapsing-remitting experimental autoimmune encephalomyelitis mouse model of multiple sclerosis. This study investigates the effect of arundic acid (AA), a known inhibitor of astrocytic S100B synthesis, in the chronic experimental autoimmune encephalomyelitis, which is another mouse model of multiple sclerosis usually studied. By the daily evaluation of clinical scores and neuropathologic-molecular analysis performed in the spinal cord, we observed that the AA-treated group showed lower severity compared to the vehicle-treated mice, particularly in the early phase of disease onset. We also observed a significant reduction of astrocytosis, demyelination, immune infiltrates, proinflammatory cytokines expression and enzymatic oxidative reactivity in the AA-treated group. Overall, our results reinforce the involvement of S100B in the development of animal models of multiple sclerosis and propose AA targeting the S100B protein as a focused potential drug to be considered for multiple sclerosis treatment.

Published

2021

16. Study of the effects of Lemna minor extracts on human immune cell populations.

Author

Catelani Cardoso C, Miraldi E, Ceccarini MR, Naureen Z, Baini G, Manara E, Anpilogov K, Camilleri G, Dhuli K, Paolacci S, Ria F, Di Sante G, Camponeschi C, Tredicine M, Zanlari A, Chiurazzi P, Beccari T, and Bertelli M

Subjects

Cells, Cultured, Humans, Phytochemicals genetics, Phytochemicals isolation & purification, Phytochemicals pharmacology, Plant Extracts genetics, Plant Extracts isolation & purification, Araceae genetics, Immunomodulation drug effects, Immunomodulation immunology, Leukocytes, Mononuclear drug effects, Leukocytes, Mononuclear immunology, Plant Extracts pharmacology

Abstract

Objective: Lemna minor is a plant with a huge repertoire of secondary metabolites. The literature indicates that extracts of Lemna minor have antioxidant, antiradical, immunomodulatory and anti-inflammatory properties. The objective of the present study was to find a suitable technique to extract active compounds from this plant and verify whether these extracts have immunomodulatory activity., Materials and Methods: We grew L. minor on a standard medium with Gamborg B5 and vitamins. We extracted compounds from the plant by maceration and decoction. The phytochemical profile of the extracts was characterized by chromatography, spectrophotometry, and spectroscopy. The extracts were tested on cultures of mononuclear cells from four human subjects. These cells were pulsed with carboxyfluorescein succinimidyl ester, grown in triplicate in standard culture medium without (control) and with increasing concentrations of Lemna extracts. Flow cytometry was used to evaluate cell death and proliferation of the total mononuclear cell population and of CD4+, CD8+, B cell and monocyte populations., Results: The Lemna extracts were not cytotoxic and did not cause cell necrosis or apoptosis in immune cells. At low concentrations, they induced very limited proliferation of CD4+ cells within 48 hours. At high concentrations, they induced proliferation of CD8+ cells and B lymphocytes within 48 hours., Conclusions: Unfortunately, we failed to confirm any immunomodulatory activity of Lemna extracts. Growth and death rates of human immune cells were not significantly affected by adding Lemna extracts to the culture medium.

Published

2021

17. Haemophilus parasuis ( Glaesserella parasuis ) as a Potential Driver of Molecular Mimicry and Inflammation in Rheumatoid Arthritis.

Author

Di Sante G, Gremese E, Tolusso B, Cattani P, Di Mario C, Marchetti S, Alivernini S, Tredicine M, Petricca L, Palucci I, Camponeschi C, Aragon V, Gambotto A, Ria F, and Ferraccioli G

Abstract

Background: Haemophilus parasuis ( Hps ; now Glaesserella parasuis ) is an infectious agent that causes severe arthritis in swines and shares sequence similarity with residues 261-273 of collagen type 2 (Coll 261-273 ), a possible autoantigen in rheumatoid arthritis (RA). Objectives/methods: We tested the presence of Hps sequencing 16S ribosomal RNA in crevicular fluid, synovial fluids, and tissues in patients with arthritis (RA and other peripheral arthritides) and in healthy controls. Moreover, we examined the cross-recognition of Hps by Coll 261-273 -specific T cells in HLA-DRB1 * 04 pos RA patients, by T-cell receptor (TCR) beta chain spectratyping and T-cell phenotyping. Results: Hps DNA was present in 57.4% of the tooth crevicular fluids of RA patients and in 31.6% of controls. Anti- Hps IgM and IgG titers were detectable and correlated with disease duration and the age of the patients. Peripheral blood mononuclear cells (PBMCs) were stimulated with Hps virulence-associated trimeric autotransporter peptide (VtaA10 755-766 ), homologous to human Coll 261-273 or co-cultured with live Hps . In both conditions, the expanded TCR repertoire overlapped with Coll 261-273 and led to the production of IL-17. Discussion: We show that the DNA of an infectious agent ( Hps ), not previously described as pathogen in humans, is present in most patients with RA and that an Hps peptide is able to activate T cells specific for Coll 261-273 , likely inducing or maintaining a molecular mimicry mechanism. Conclusion: The cross-reactivity between VtaA10 755-766 of a non-human infectious agent and human Coll 261-273 suggests an involvement in the pathogenesis of RA. This mechanism appears emphasized in predisposed individuals, such as patients with shared epitope., Competing Interests: The 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 © 2021 Di Sante, Gremese, Tolusso, Cattani, Di Mario, Marchetti, Alivernini, Tredicine, Petricca, Palucci, Camponeschi, Aragon, Gambotto, Ria and Ferraccioli.)

Published

2021

18. Synergistic antiproliferative and differentiating effect of 2,4-monofurfurylidene-tetra-O-methylsorbitol and 4,6-dimethyl-2-(3,4,5-trimethoxyphenylamino)pyrimidine on primary and immortalized keratinocytes.

Author

Serafino A, Nicotera G, Andreola F, Giovannini D, Zonfrillo M, Sferrazza G, Calcaterra A, De Angelis C, Camponeschi C, and Pierimarchi P

Subjects

Adult, Anti-Inflammatory Agents, Non-Steroidal chemistry, Biomarkers metabolism, Cell Cycle Checkpoints drug effects, Cell Line, Transformed, Cell Proliferation drug effects, Cell Shape drug effects, Cell Survival drug effects, Cells, Cultured, Cyclohexylamines chemistry, Dermatologic Agents chemistry, Drug Synergism, Humans, Keratinocytes cytology, Psoriasis drug therapy, Pyrimidines chemistry, Reactive Oxygen Species metabolism, Sorbitol chemistry, Sorbitol pharmacology, Tissue Donors, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cell Differentiation drug effects, Cyclohexylamines pharmacology, Dermatologic Agents pharmacology, Keratinocytes drug effects, Pyrimidines pharmacology, Sorbitol analogs & derivatives

Abstract

Psoriasis is one of the most common chronic autoinflammatory skin disease, associated with hyperproliferation and abnormal differentiation of keratinocytes, inflammation, and angiogenesis. The available treatments for psoriasis are not curative and may have numerous side effects, and topical administration is preferred over systemic therapy due to the reduced systemic burden of the drug. Thus, novel and more efficacious formulations of anti-inflammatory and/or differentiating compounds for topical application could be very useful for the disease management and for improving the quality of life of the patients. Here we evaluated the potential as anti-psoriatic of an equimolar mixture of two compounds, 2,4-Monofurfurylidene-tetra-O-methylsorbitol (Compound A) and 4,6-dimethyl-2-(3,4,5-trimethoxyphenylamino)pyrimidine (Compound B), that, used individually, are known to possess immunomodulating properties (Compound A) and keratolitic and anti-inflammatory activity (Compound B). Human immortalized keratinocyte cell line (HaCaT cells) and primary human keratinocyte cells from adult donor (HEKa) were used as in vitro experimental models. We show that the mix A + B exhibits antiproliferative activity and induces terminal differentiation more efficiently than compounds A and B used individually. We confirm that the compound B is the active ingredient of the mixture and the mainly responsible for anti-psoriatic activity, but the mix A + B is more effective and possesses lower cytotoxicity than the compound B alone. This could be ascribable to the association with compound A, that is known to possess, in addition to the immunomodulating ability, antioxidant and antiradical action. Our results indicate that mix A + B could be a suitable candidate for a new cosmeceutical formulation for topical treatment of psoriasis., (Copyright © 2018 Elsevier Masson SAS. All rights reserved.)

Published

2018