Your search keyword '"Cammarata, Ilenia"' showing total 7 results

1. CD8+ T cells specific to apoptosis‐associated epitopes are expanded in patients with chronic HBV infection and fibrosis.

Author

Pacella, Ilenia, Cammarata, Ilenia, Martire, Carmela, Brancaccio, Giuseppina, Gaeta, Giovanni Battista, Barnaba, Vincenzo, and Piconese, Silvia

Subjects

*T cells, *SUPPRESSOR cells, *CHRONIC hepatitis B, *TRANSVERSE electromagnetic cells, *EPITOPES

Abstract

Background & Aims: During chronic viral infections, the apoptosis of activated T cell elicits a CD8+ T cell response directed to those cryptic epitopes that emerge from caspase‐cleaved structural proteins. Such response directed to apoptosis‐associated epitopes (AEs) contributes to the amplification of immunopathology. Methods: Here, we have analysed through flow cytometry AE‐specific CD8+ T cells in patients with chronic hepatitis B virus (HBV) infection, naïve‐to‐treatment or undergoing nucleos(t)ide‐analogue (NUC) therapy. Results: We found that AE‐specific CD8+ T cell frequencies were significantly increased only in those NUC‐treated patients who also presented advanced hepatic fibrosis. Regulatory T cells were also expanded in those patients, and AE‐specific, but not HBV‐specific, CD8+ T cell frequency positively correlated with Treg percentages. Through multiparameter flow cytometry, multidimensionality reduction and unsupervised clustering analysis, we could identify novel subpopulations among effector memory (em) and emCD45RA+ T cell (Tem and Temra) subsets. CD8+ T cells with distinct specificities differentially populated the subpopulation map: while HBV‐specific were mostly contained in the Tem subset, AE‐specific CD8+ T cells encompassed naïve, as well as T central memory, Tem and Temra cells. Conclusion: All together, these findings indicate a link between AE‐specific CD8+ T cells and advanced liver fibrosis in patients with chronic HBV infection, and suggest that virus‐specific and AE‐specific CD8+ T cells exhibit distinct differentiation states and contribute in distinct ways to immunopathology. [ABSTRACT FROM AUTHOR]

Published

2021

2. In adult X-CGD patients, regulatory T cells are expanded while activated T cells display a NOX2-independent ROS increase.

Author

Cammarata, Ilenia, Pinna, Valeria, Pacella, Ilenia, Rotella, Ivano, Soresina, Annarosa, Badolato, Raffaele, Plebani, Alessandro, Pignata, Claudio, Cirillo, Emilia, Zicari, Anna Maria, Violi, Francesco, Carnevale, Roberto, Loffredo, Lorenzo, and Piconese, Silvia

Subjects

*REGULATORY T cells, *T cells, *CHRONIC granulomatous disease, *ADULTS, *AUTOIMMUNE diseases

Abstract

• Adult X-CGD patient have increased Treg percentages. • Tregs from X-CGD respond more to in vitro activation. • ROS content in T cells is activation-related and NOX2-independent. • Activated T cells from X-CGD contain more ROS than controls. • Tconvs from X-CGD produce more TNF. The X-linked chronic granulomatous disease (X-CGD), a rare genetic disease characterised by recurrent infections, is caused by mutations of NOX2. Significant proportions of X-CGD patients display signs of immune dysregulation. Regulatory T cells (Tregs) are CD4+ T lymphocytes that expand in active inflammation and prevent autoimmune disorders. Here we asked whether X-CGD is associated to Treg dysfunctions in adult patients. To this aim, the frequency of Tregs was analysed through intracellular flow cytometry in a cohort of adult X-CGD patients, carriers and controls. We found that Tregs were significantly expanded and activated in blood of adult X-CGD patients, and this was associated with activation of conventional CD4+ T cells (Tconvs). T cell activation was characterised by accumulation of intracellular ROS, not derived from NOX2 but likely produced by cellular metabolism. The higher TNF production by Tconvs in X-CGD patients might contribute to the expansion of Tregs through the TNFR2 receptor. In summary, our data indicate that Tregs expand in adult X-CGD in response to immune activation, and that the increase of NOX2-independent ROS content is a feature of activated T cells. [ABSTRACT FROM AUTHOR]

Published

2024

3. Combination of chemotherapy and PD-1 blockade induces T cell responses to tumor non-mutated neoantigens.

Author

Grimaldi, Alessio, Cammarata, Ilenia, Martire, Carmela, Focaccetti, Chiara, Piconese, Silvia, Buccilli, Marta, Mancone, Carmine, Buzzacchino, Federica, Berrios, Julio Rodrigo Giron, D'Alessandris, Nicoletta, Tomao, Silverio, Giangaspero, Felice, Paroli, Marino, Caccavale, Rosalba, Spinelli, Gian Paolo, Girelli, Gabriella, Peruzzi, Giovanna, Nisticò, Paola, Spada, Sheila, and Panetta, Mariangela

Subjects

*CANCER treatment, *CANCER chemotherapy, *T cells, *CANCER immunotherapy, *CD4 antigen, *CD8 antigen

Abstract

Here, we developed an unbiased, functional target-discovery platform to identify immunogenic proteins from primary non-small cell lung cancer (NSCLC) cells that had been induced to apoptosis by cisplatin (CDDP) treatment in vitro, as compared with their live counterparts. Among the multitude of proteins identified, some of them were represented as fragmented proteins in apoptotic tumor cells, and acted as non-mutated neoantigens (NM-neoAgs). Indeed, only the fragmented proteins elicited effective multi-specific CD4+ and CD8+ T cell responses, upon a chemotherapy protocol including CDDP. Importantly, these responses further increased upon anti-PD-1 therapy, and correlated with patients' survival and decreased PD-1 expression. Cross-presentation assays showed that NM-neoAgs were unveiled in apoptotic tumor cells as the result of caspase-dependent proteolytic activity of cellular proteins. Our study demonstrates that apoptotic tumor cells generate a repertoire of immunogenic NM-neoAgs that could be potentially used for developing effective T cell-based immunotherapy across multiple cancer patients. Grimaldi and Cammarata et al. develop a proteomics-based, target discovery platform to identify immunogenic proteins specific to apoptotic tumor cells. This study highlights the importance of protein modifications in apoptotic tumor cells as a mechanism of generating immunogenic neoantigens that can be targeted for T cell-based immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2020

4. Counter-regulation of regulatory T cells by autoreactive CD8+ T cells in rheumatoid arthritis.

Author

Cammarata, Ilenia, Martire, Carmela, Citro, Alessandra, Raimondo, Domenico, Fruci, Doriana, Melaiu, Ombretta, D'Oria, Valentina, Carone, Chiara, Peruzzi, Giovanna, Cerboni, Cristina, Santoni, Angela, Sidney, John, Sette, Alessandro, Paroli, Marino, Caccavale, Rosalba, Milanetti, Edoardo, Riminucci, Mara, Timperi, Eleonora, Piconese, Silvia, and Manzo, Antonio

Subjects

*T cells, *CYTOTOXIC T cells, *RHEUMATOID arthritis, *TUMOR necrosis factors, *CONDITIONED response

Abstract

The mechanisms whereby autoreactive T cells escape peripheral tolerance establishing thus autoimmune diseases in humans remain an unresolved question. Here, we demonstrate that autoreactive polyfunctional CD8+ T cells recognizing self-antigens (i.e., vimentin, actin cytoplasmic 1, or non-muscle myosin heavy chain 9 epitopes) with high avidity, counter-regulate Tregs by killing them, in a consistent percentage of rheumatoid arthritis (RA) patients. Indeed, these CD8+ T cells express a phenotype and gene profile of effector (eff) cells and, upon antigen-specific activation, kill Tregs indirectly in an NKG2D-dependent bystander fashion in vitro. This data provides a mechanistic basis for the finding showing that AE-specific (CD107a+) CD8+ T killer cells correlate, directly with the disease activity score, and inversely with the percentage of activated Tregs, in both steady state and follow-up studies in vivo. In addition, multiplex immunofluorescence imaging analyses of inflamed synovial tissues in vivo show that a remarkable number of CD8+ T cells express granzyme-B and selectively contact FOXP3+ Tregs, some of which are in an apoptotic state, validating hence the possibility that CD8+ Teff cells can counteract neighboring Tregs within inflamed tissues, by killing them. Alternatively, the disease activity score of a different subset of patients is correlated with the expansion of a peculiar subpopulation of autoreactive low avidity, partially-activated (pa)CD8+ T cells that, despite they conserve the conventional naïve (N) phenotype, produce high levels of tumor necrosis factor (TNF)-α and exhibit a gene expression signature of a progressive activation state. Tregs directly correlate with the expansion of this autoreactive (low avidity) paCD8+ TN cell subset in vivo , and efficiently control their differentiation rather their proliferation in vitro. Interestingly, autoreactive high avidity CD8+ Teff cells or low avidity paCD8+ TN cells are significantly expanded in RA patients who would become non-responders or patients who would become responders to TNF-α inhibitor therapy, respectively. These data provide evidence of a previously undescribed role of such mechanisms in the progression and therapy of RA. • Autoreactive CD8+ TN or eff cells differently affect Tregs to their vantage in RA. • Autoreactive low avidity CD8+ TN cells producing TNF-α are sustained by Tregs. • Autoreactive high avidity CD8+ Teff cells resist Tregs by killing them. • These distinctive mechanisms condition the response to anti-TNF therapy. • They could contribute for designing innovative therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2019

5. Viral hepatitis, inflammation, and cancer: A lesson for autoimmunity.

Author

Piconese, Silvia, Cammarata, Ilenia, and Barnaba, Vincenzo

Subjects

*TUMORS, *IMMUNOPATHOLOGY, *IMMUNOREGULATION, *AUTOIMMUNITY, *LIVER diseases

Abstract

Abstract In the present review, we analyzed the various overlapping and non-mutually exclusive mechanisms that intersect and form complex and highly flexible immunological networks allowing the defense against liver infections and tumors. Liver immunity results from the combination of the skills of systemic and local immune system(s) to sense and recognize pathogen or tumor antigens, to sensitize a wide range of innate and adaptive immune cells, and to clear the "invaders", through the establishment of a transient liver immunopathology state undergoing resolution/control of infections or tumors, and memory development. Then, a special emphasis is placed on discussing about the capacity of the immune system(s) to develop a state of chronic low-level immunopathology adapting through the intervention of simultaneous immunoregulatory mechanisms, when the liver is infected by highly mutable viruses (e.g., hepatitis B or C viruses [HBV or HCV]) capable to escape from the immune recognition. The establishment of chronic inflammation represents an advantage for the species survival, because it guarantees the long-term survival of human hosts despite the virus persistence. However, chronic inflammation, in the long run, can evolve towards severe consequences (decompensated cirrhosis and hepatocellular carcinoma) in some individuals, finding requiring the impelling need of discovering new therapeutic anti-viral and immunostimulatory agents addressed, in combination, to fight especially HBV that, in contrast to HCV, lacks antivirals capable to eradicate the virus. Finally, we discussed the concept proposing that the divergent immunoregulatory mechanisms that develop in persisting infections or tumors, on the one hand, and autoimmunity, on the other hand, are the mirror image of each other, whose understanding is also relevant for preparing novel immunotherapeutic approaches in autoimmune diseases. Highlights • Protective liver immunity eliminates the « invaders » by transient immunopathology. • Chronic low-level inflammation guarantees host survival despite virus persistence. • T cell inhibitory checkpoints and Tregs contribute to maintain this condition. • In the long run, the host-virus compromise may evolve into cirrhosis and cancer. • Immunoregulation in infections and tumors is the mirror image of autoimmunity. [ABSTRACT FROM AUTHOR]

Published

2018

6. ANGPTL3 deficiency associates with the expansion of regulatory T cells with reduced lipid content.

Author

Pinzon Grimaldos, Alessandra, Pacella, Ilenia, Bini, Simone, Tucci, Gloria, Cammarata, Ilenia, Di Costanzo, Alessia, Minicocci, Ilenia, D'Erasmo, Laura, Arca, Marcello, and Piconese, Silvia

Subjects

*REGULATORY T cells, *T cells, *LIPID metabolism, *LIPIDS, *LIPOPROTEINS, *CARDIOVASCULAR diseases

Abstract

Angiopoietin-like 3 (ANGPTL3) regulates lipid and glucose metabolism. Loss-of-function mutations in its gene, leading to ANGPTL3 deficiency, cause in humans the familial combined hypolipidemia type 2 (FHBL2) phenotype, characterized by very low concentrations of circulating lipoproteins and reduced risk of atherosclerotic cardiovascular disease. Whether this condition is accompanied by immune dysfunctions is unknown. Regulatory T cells (Tregs) are CD4 T lymphocytes endowed with immune suppressive and atheroprotective functions and sensitive to metabolic signals. By investigating FHBL2, we explored the hypothesis that Tregs expand in response to extreme hypolipidemia, through a modulation of the Treg-intrinsic lipid metabolism. Treg frequency, phenotype, and intracellular lipid content were assessed ex vivo from FHBL2 subjects and age- and sex-matched controls, through multiparameter flow cytometry. The response of CD4 T cells from healthy controls to marked hypolipidemia was tested in vitro in low-lipid culture conditions. The ex vivo analysis revealed that FHBL2 subjects showed higher percentages of Tregs with a phenotype undistinguishable from controls and with a lower lipid content, which directly correlated with the concentrations of circulating lipoproteins. In vitro , lipid restriction induced the upregulation of genes of the mevalonate pathway, including those involved in isoprenoid biosynthesis, and concurrently increased the expression of the Treg markers FOXP3 and Helios. The latter event was found to be prenylation-dependent, and likely related to increased IL-2 production and signaling. Our study demonstrates that FHBL2 is characterized by high Treg frequencies, a feature which may concur to the reduced atherosclerotic risk in this condition. Mechanistically, hypolipidemia may directly favor Treg expansion, through the induction of the mevalonate pathway and the prenylation of key signaling proteins. [Display omitted] • In ANGPTL3 deficiency, hypolipidemia correlates with Treg expansion. • Tregs from these individuals contain less intracellular lipids. • In vitro, lipid deprivation induces the mevalonate pathway and Treg markers. • Such event is prenylation-dependent and IL-2/CD25-related. [ABSTRACT FROM AUTHOR]

Published

2022

7. Thyroid Hormone Protects from Fasting-Induced Skeletal Muscle Atrophy by Promoting Metabolic Adaptation.

Author

Ucci, Sarassunta, Renzini, Alessandra, Russi, Valentina, Mangialardo, Claudia, Cammarata, Ilenia, Cavioli, Giorgia, Santaguida, Maria Giulia, Virili, Camilla, Centanni, Marco, Adamo, Sergio, Moresi, Viviana, and Verga-Falzacappa, Cecilia

Subjects

*SKELETAL muscle, *THYROID hormones, *TRIIODOTHYRONINE, *ATROPHY, *METABOLIC regulation, *MUSCLE mass, *PROTEOLYSIS, *LYSOSOMES

Abstract

Thyroid hormones regulate a wide range of cellular responses, via non-genomic and genomic actions, depending on cell-specific thyroid hormone transporters, co-repressors, or co-activators. Skeletal muscle has been identified as a direct target of thyroid hormone T3, where it regulates stem cell proliferation and differentiation, as well as myofiber metabolism. However, the effects of T3 in muscle-wasting conditions have not been yet addressed. Being T3 primarily responsible for the regulation of metabolism, we challenged mice with fasting and found that T3 counteracted starvation-induced muscle atrophy. Interestingly, T3 did not prevent the activation of the main catabolic pathways, i.e., the ubiquitin-proteasome or the autophagy-lysosomal systems, nor did it stimulate de novo muscle synthesis in starved muscles. Transcriptome analyses revealed that T3 mainly affected the metabolic processes in starved muscle. Further analyses of myofiber metabolism revealed that T3 prevented the starvation-mediated metabolic shift, thus preserving skeletal muscle mass. Our study elucidated new T3 functions in regulating skeletal muscle homeostasis and metabolism in pathological conditions, opening to new potential therapeutic approaches for the treatment of skeletal muscle atrophy. [ABSTRACT FROM AUTHOR]

Published

2019