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1. OP0011 INVESTIGATING THE ROLE OF ENDOTHELIAL DYSFUNCTION IN ANTIPHOSPHOLIPID SYNDROME BY USING PATIENT-SPECIFIC ENDOTHELIAL COLONY-FORMING CELLS

Author

Calcaterra, F., primary, Gerosa, M., additional, Ciceri, R., additional, Bacci, M., additional, Cancellara, A., additional, Tumminello, F., additional, Saresini, A., additional, Iannone, C., additional, Argolini, L. M., additional, Donadini, M. P., additional, Della Bella, S., additional, Lodigiani, C., additional, Mavilio, D., additional, and Caporali, R. F., additional

Published
2024
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2. Transcriptomic profile of TNFhigh MAIT cells is linked to B cell response following SARS-CoV-2 vaccination

Author

Marzano, P, Balin, S, Terzoli, S, Della Bella, S, Cazzetta, V, Piazza, R, Sandrock, I, Ravens, S, Tan, L, Prinz, I, Calcaterra, F, Di Vito, C, Cancellara, A, Calvi, M, Carletti, A, Franzese, S, Frigo, A, Darwish, A, Voza, A, Mikulak, J, Mavilio, D, Marzano P., Balin S., Terzoli S., Della Bella S., Cazzetta V., Piazza R., Sandrock I., Ravens S., Tan L., Prinz I., Calcaterra F., Di Vito C., Cancellara A., Calvi M., Carletti A., Franzese S., Frigo A., Darwish A., Voza A., Mikulak J., Mavilio D., Marzano, P, Balin, S, Terzoli, S, Della Bella, S, Cazzetta, V, Piazza, R, Sandrock, I, Ravens, S, Tan, L, Prinz, I, Calcaterra, F, Di Vito, C, Cancellara, A, Calvi, M, Carletti, A, Franzese, S, Frigo, A, Darwish, A, Voza, A, Mikulak, J, Mavilio, D, Marzano P., Balin S., Terzoli S., Della Bella S., Cazzetta V., Piazza R., Sandrock I., Ravens S., Tan L., Prinz I., Calcaterra F., Di Vito C., Cancellara A., Calvi M., Carletti A., Franzese S., Frigo A., Darwish A., Voza A., Mikulak J., and Mavilio D.

Abstract

Introduction: Higher frequencies of mucosal-associated invariant T (MAIT) cells were associated with an increased adaptive response to mRNA BNT162b2 SARS-CoV-2 vaccine, however, the mechanistic insights into this relationship are unknown. In the present study, we hypothesized that the TNF response of MAIT cells supports B cell activation following SARS-CoV-2 immunization. Methods: To investigate the effects of repeated SARS-CoV-2 vaccinations on the peripheral blood mononuclear cells (PBMCs), we performed a longitudinal single cell (sc)RNA-seq and scTCR-seq analysis of SARS-CoV-2 vaccinated healthy adults with two doses of the Pfizer-BioNTech BNT162b2 mRNA vaccine. Collection of PBMCs was performed 1 day before, 3 and 17 days after prime vaccination, and 3 days and 3 months following vaccine boost. Based on scRNA/TCR-seq data related to regulatory signals induced by the vaccine, we used computational approaches for the functional pathway enrichment analysis (Reactome), dynamics of the effector cell-polarization (RNA Velocity and CellRank), and cell-cell communication (NicheNet). Results: We identified MAIT cells as an important source of TNF across circulating lymphocytes in response to repeated SARS-CoV-2 BNT162b2 vaccination. The TNFhigh signature of MAIT cells was induced by the second administration of the vaccine. Notably, the increased TNF expression was associated with MAIT cell proliferation and efficient anti-SARS-CoV-2 antibody production. Finally, by decoding the ligand-receptor interactions and incorporating intracellular signaling, we predicted TNFhigh MAIT cell interplay with different B cell subsets. In specific, predicted TNF-mediated activation was selectively directed to conventional switched memory B cells, which are deputed to high-affinity long-term memory. Discussion: Overall, our results indicate that SARS-CoV-2 BNT162b2 vaccination influences MAIT cell frequencies and their transcriptional effector profile with the potential to promote B cell

Published
2023

3. PB1411 Study of Endothelial Dysfunction in Patients with Unprovoked Venous Thromboembolism through Endothelial Colony-Forming Cell In Vitro Characterization

Author

Cancellara, A., primary, Bacci, M., additional, Ciceri, R., additional, Romualdi, E., additional, Pessi, V., additional, Tumminello, F., additional, Fantuzzi, M., additional, Lodigiani, C., additional, Donadini, M., additional, Della Bella, S., additional, Calcaterra, F., additional, and Mavilio, D., additional

Published
2023
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7. APOL1 polymorphism modulates sphingolipid profile of human podocytes

Author

Valsecchi, M, Cazzetta, V, Oriolo, F, Lan, X, Piazza, R, Saleem, M, Singhal, P, Mavilio, D, Mikulak, J, Aureli, M, Valsecchi M., Cazzetta V., Oriolo F., Lan X., Piazza R., Saleem M. A., Singhal P. C., Mavilio D., Mikulak J., Aureli M., Valsecchi, M, Cazzetta, V, Oriolo, F, Lan, X, Piazza, R, Saleem, M, Singhal, P, Mavilio, D, Mikulak, J, Aureli, M, Valsecchi M., Cazzetta V., Oriolo F., Lan X., Piazza R., Saleem M. A., Singhal P. C., Mavilio D., Mikulak J., and Aureli M.

Abstract

Apolipoprotein L1 (APOL1) wild type (G0) plays a role in the metabolism of sphingolipids, glycosphingolipids, sphingomyelin and ceramide, which constitute bioactive components of the lipid rafts (DRM). We asked whether APOL1 variants (APOL1-Vs) G1 and G2 carry the potential to alter the metabolism of sphingolipids in human podocytes. The sphingolipid pattern in HPs overexpressing either APOL1G0 or APOL1-Vs was analysed by using a thin mono- and bi-dimensional layer chromatography, mass-spectrometry and metabolic labelling with [1-3H]sphingosine. HP G0 and G1/G2-Vs exhibit a comparable decrease in lactosylceramide and an increase in the globotriaosylceramide content. An analysis of the main glycohydrolases activity involved in glycosphingolipid catabolism showed an overall decrease in the activeness of the tested enzymes, irrespective of the type of APOL1-Vs expression. Similarly, the high throughput cell live-based assay showed a comparable increased action of the plasma membrane glycosphingolipid-glycohydrolases in living cells independent of the genetic APOL1 expression profile. Importantly, the most significative modification of the sphingolipid pattern induced by APOL1-Vs occurred in DRM resulted with a drastic reduction of radioactivity associated with sphingolipids. G1/G2-Vs present a decrease amount of globotriaosylceramide and globopentaosylceramide compared to G0. Additionally, ceramide at the DRM site and lactosylceramide in general, showed a greatest fall in G1/G2 in comparison with G0. Additionally, the levels of glucosylceramide decreased only in the DRM of human podocytes overexpressing G1/G2-Vs. These findings suggest that altered sphingolipidsprofiles may contribute to the deranged functionality of the plasma membrane in APOL1 risk milieu.

Published
2020

9. Development of Human ILCs and Impact of Unconventional Cytotoxic Subsets in the Pathophysiology of Inflammatory Diseases and Cancer

Author

Calvi, M., Di Vito, C., Frigo, A., Trabanelli, S., Jandus, C., and Mavilio, D.

Subjects
Antineoplastic Agents, Humans, Immunity, Innate, Killer Cells, Natural, Lymphoid Tissue, Neoplasms, T-Lymphocytes, Helper-Inducer, ILC-poiesis, cancer, cytotoxicity, inflammation, innate lymphoid cells (ILCs), natural killer (NK) cells, unconventional subsets
Abstract

Innate lymphoid cells (ILCs) were firstly described by different independent laboratories in 2008 as tissue-resident innate lymphocytes mirroring the phenotype and function of T helper cells. ILCs have been subdivided into three distinct subgroups, ILC1, ILC2 and ILC3, according to their cytokine and transcriptional profiles. Subsequently, also Natural Killer (NK) cells, that are considered the innate counterpart of cytotoxic CD8 T cells, were attributed to ILC1 subfamily, while lymphoid tissue inducer (LTi) cells were attributed to ILC3 subgroup. Starting from their discovery, significant advances have been made in our understanding of ILC impact in the maintenance of tissue homeostasis, in the protection against pathogens and in tumor immune-surveillance. However, there is still much to learn about ILC ontogenesis especially in humans. In this regard, NK cell developmental intermediates which have been well studied and characterized prior to the discovery of helper ILCs, have been used to shape a model of ILC ontogenesis. Herein, we will provide an overview of the current knowledge about NK cells and helper ILC ontogenesis in humans. We will also focus on the newly disclosed circulating ILC subsets with killing properties, namely unconventional CD56 dim NK cells and cytotoxic helper ILCs, by discussing their possible role in ILC ontogenesis and their contribution in both physiological and pathological conditions.

Published
2022

10. The challenges of primary biliary cholangitis: What is new and what needs to be done

Author

Terziroli Beretta-Piccoli, B, Mieli-Vergani, G, Vergani, D, Vierling, J, Adams, D, Alpini, G, Banales, J, Beuers, U, Bjornsson, E, Bowlus, C, Carbone, M, Chazouilleres, O, Dalekos, G, De Gottardi, A, Harada, K, Hirschfield, G, Invernizzi, P, Jones, D, Krawitt, E, Lanzavecchia, A, Lian, Z, Ma, X, Manns, M, Mavilio, D, Quigley, E, Sallusto, F, Shimoda, S, Strazzabosco, M, Swain, M, Tanaka, A, Trauner, M, Tsuneyama, K, Zigmond, E, Gershwin, M, Terziroli Beretta-Piccoli B., Mieli-Vergani G., Vergani D., Vierling J. M., Adams D., Alpini G., Banales J. M., Beuers U., Bjornsson E., Bowlus C., Carbone M., Chazouilleres O., Dalekos G., De Gottardi A., Harada K., Hirschfield G., Invernizzi P., Jones D., Krawitt E., Lanzavecchia A., Lian Z. -X., Ma X., Manns M., Mavilio D., Quigley E. M., Sallusto F., Shimoda S., Strazzabosco M., Swain M., Tanaka A., Trauner M., Tsuneyama K., Zigmond E., Gershwin M. E., Terziroli Beretta-Piccoli, B, Mieli-Vergani, G, Vergani, D, Vierling, J, Adams, D, Alpini, G, Banales, J, Beuers, U, Bjornsson, E, Bowlus, C, Carbone, M, Chazouilleres, O, Dalekos, G, De Gottardi, A, Harada, K, Hirschfield, G, Invernizzi, P, Jones, D, Krawitt, E, Lanzavecchia, A, Lian, Z, Ma, X, Manns, M, Mavilio, D, Quigley, E, Sallusto, F, Shimoda, S, Strazzabosco, M, Swain, M, Tanaka, A, Trauner, M, Tsuneyama, K, Zigmond, E, Gershwin, M, Terziroli Beretta-Piccoli B., Mieli-Vergani G., Vergani D., Vierling J. M., Adams D., Alpini G., Banales J. M., Beuers U., Bjornsson E., Bowlus C., Carbone M., Chazouilleres O., Dalekos G., De Gottardi A., Harada K., Hirschfield G., Invernizzi P., Jones D., Krawitt E., Lanzavecchia A., Lian Z. -X., Ma X., Manns M., Mavilio D., Quigley E. M., Sallusto F., Shimoda S., Strazzabosco M., Swain M., Tanaka A., Trauner M., Tsuneyama K., Zigmond E., and Gershwin M. E.

Abstract

Primary Biliary Cholangitis (PBC) is an uncommon, chronic, cholangiopathy of autoimmune origin and unknown etiology characterized by positive anti-mitochondrial autoantibodies (AMA), female preponderance and progression to cirrhosis if left untreated. The diagnosis is based on AMA- or PBC-specific anti-nuclear antibody (ANA)-positivity in the presence of a cholestatic biochemical profile, histologic confirmation being mandatory only in seronegative cases. First-line treatment is ursodeoxycholic acid (UDCA), which is effective in preventing disease progression in about two thirds of the patients. The only approved second-line treatment is obeticholic acid. This article summarizes the most relevant conclusions of a meeting held in Lugano, Switzerland, from September 23rd-25th 2018, gathering basic and clinical scientists with various background from around the world to discuss the latest advances in PBC research. The meeting was dedicated to Ian Mackay, pioneer in the field of autoimmune liver diseases. The role of liver histology needs to be reconsidered: liver pathology consistent with PBC in AMA-positive individuals without biochemical cholestasis is increasingly reported, raising the question as to whether biochemical cholestasis is a reliable disease marker for both clinical practice and trials. The urgent need for new biomarkers, including more accurate markers of cholestasis, was also widely discussed during the meeting. Moreover, new insights in interactions of bile acids with biliary epithelia in PBC provide solid evidence of a role for impaired epithelial protection against potentially toxic hydrophobic bile acids, raising the fundamental question as to whether this bile acid-induced epithelial damage is the cause or the consequence of the autoimmune attack to the biliary epithelium. Strategies are needed to identify difficult-to-treat patients at an early disease stage, when new therapeutic approaches targeting immunologic pathways, in addition to bile acid

Published
2019

15. Cancer immunotherapy by blocking immune checkpoints on innate lymphocytes

Author

Pesce, S., Trabanelli, S., Di Vito, C., Greppi, M., Obino, V., Guolo, F., Minetto, P., Bozzo, M., Calvi, M., Zaghi, E., Candiani, S., Lemoli, R.M., Jandus, C., Mavilio, D., and Marcenaro, E.

Subjects
KIR, NKG2A, PD-1, immune checkpoint, immune escape, immunotherapy, innate immunity, innate lymphoid cells, miRNA, natural killer cells, animal diseases, bacteria, chemical and pharmacologic phenomena, biochemical phenomena, metabolism, and nutrition, ddc:616.07
Abstract

Immune checkpoints refer to a plethora of inhibitory pathways of the immune system that play a crucial role in maintaining self-tolerance and in tuning the duration and amplitude of physiological immune responses to minimize collateral tissue damages. The breakdown of this delicate balance leads to pathological conditions, including cancer. Indeed, tumor cells can develop multiple mechanisms to escape from immune system defense, including the activation of immune checkpoint pathways. The development of monoclonal antibodies, targeting inhibitory immune checkpoints, has provided an immense breakthrough in cancer therapy. Immune checkpoint inhibitors (ICI), initially developed to reverse functional exhaustion in T cells, recently emerged as important actors in natural killer (NK)-cell-based immunotherapy. Moreover, the discovery that also helper innate lymphoid cells (ILCs) express inhibitory immune checkpoints, suggests that these molecules might be targeted on ILCs, to modulate their functions in the tumor microenvironment. Recently, other strategies to achieve immune checkpoint blockade have been developed, including miRNA exploiting systems. Herein, we provide an overview of the current knowledge on inhibitory immune checkpoints on NK cells and ILCs and we discuss how to target these innate lymphocytes by ICI in both solid tumors and hematological malignancies.

Published
2020

16. Human liver-resident CD56bright/CD16neg NK cells are retained within hepatic sinusoids via the engagement of CCR5 and CXCR6 pathways

Author

Hudspeth, K, Donadon, M, Cimino, M, Pontarini, E, Tentorio, P, Preti, M, Hong, M, Bertoletti, A, Bicciato, S, Invernizzi, P, Lugli, E, Torzilli, G, Gershwin, M, Mavilio, D, INVERNIZZI, PIETRO, Mavilio, D., Hudspeth, K, Donadon, M, Cimino, M, Pontarini, E, Tentorio, P, Preti, M, Hong, M, Bertoletti, A, Bicciato, S, Invernizzi, P, Lugli, E, Torzilli, G, Gershwin, M, Mavilio, D, INVERNIZZI, PIETRO, and Mavilio, D.

Abstract

Rationale: The liver-specific natural killer (NK) cell population is critical for local innate immune responses, but the mechanisms that lead to their selective homing and the definition of their functionally relevance remain enigmatic. Objectives: We took advantage of the availability of healthy human liver to rigorously define the mechanisms regulating the homing of NK cells to liver and the repertoire of receptors that distinguish liver-resident NK (lr-NK) cells from circulating counterparts. Findings: Nearly 50% of the entire liver NK cell population is composed of functionally relevant CD56bright lr-NK cells that localize within hepatic sinusoids. CD56bright lr-NK cells express CD69, CCR5 and CXCR6 and this unique repertoire of chemokine receptors is functionally critical as it determines selective migration in response to the chemotactic stimuli exerted by CCL3, CCL5 and CXCL16. Here, we also show that hepatic sinusoids express CCL3pos Kupffer cells, CXCL16pos endothelial cells and CCL5pos T and NK lymphocytes. The selective presence of these chemokines in sinusoidal spaces creates a unique tissue niche for lr-CD56bright NK cells that constitutively express CCR5 and CXCR6. CD56bright lr-NK cells co-exist with CD56dim conventional NK (c-NK) cells that are, interestingly, transcriptionally and phenotypically similar to their peripheral circulating counterparts. Indeed, CD56dim c-NK cells lack expression of CD69, CCR5, and CXCR6 but express selectins, integrins and CX3CR1. Conclusion: Our findings disclosing the phenotypic and functional differences between lr-Nk cells and c-NK cells are critical to distinguish liver-specific innate immune responses. Hence, any therapeutic attempts at modifying the large population of CD56bright lr-NK cells will require modification of hepatic CCR5 and CXCR6.

Published
2016

17. Human innate lymphoid cells (ILCs): Toward a uniform immune-phenotyping

Author

Trabanelli, S., Gomez-Cadena, A., Salomé, B., Michaud, K., Mavilio, D., Landis, B.N., Jandus, P., and Jandus, C.

Subjects
body regions, skin and connective tissue diseases, Animals, Flow Cytometry/methods, Humans, Immunity, Innate/immunology, Immunologic Factors/immunology, Immunophenotyping/methods, Lymphocytes/immunology, allergy, flow cytometry, immune monitoring, innate lymphoid cells, leukemia, phenotype
Abstract

Helper innate lymphoid cells (ILCs), the most recently identified population of the ILC family, play a fundamental role in the restoration of tissue integrity, in the protection against infiltrating pathogens as well as in tumor immune-surveillance. ILCs have been divided into three main subsets, ILC1, ILC2, and ILC3, that can be specifically activated by different signals coming either indirectly from pathogens or from other cell populations, including cancer cells. Following activation, ILCs are in turn able to promptly secrete a wide range of soluble mediators that modulate effector cell functions. The discovery and the study of these immune cells is now offering important opportunities for innovative therapies of allergic airway diseases, inflammatory disorders and might be crucial for the discovery of new targets for the therapy of cancer. It is therefore fundamental that the scientific community establishes harmonized guidelines to obtain a consensus in the identification and phenotypical and functional characterization of ILCs. © 2018 International Clinical Cytometry Society.

Published
2018

20. Proceedings from the Second Haploidentical Stem Cell Transplantation Symposium-Haplo2014, San Francisco, California, December 4, 2014

Author

Al Malki, M. M., Horowitz, M., Handgretinger, R., Leung, W., Roy, D. -C., Huang, X. -J., Fuchs, E., Locatelli, Franco, Blaise, D., Mineishi, S., Martelli, M., Miller, J., June, C., Ai, H. -S., Luznik, L., Mavilio, D., Lugli, E., van den Brink, M. R. M., Champlin, R. E., Ciurea, S. O., Locatelli F. (ORCID:0000-0002-7976-3654), Al Malki, M. M., Horowitz, M., Handgretinger, R., Leung, W., Roy, D. -C., Huang, X. -J., Fuchs, E., Locatelli, Franco, Blaise, D., Mineishi, S., Martelli, M., Miller, J., June, C., Ai, H. -S., Luznik, L., Mavilio, D., Lugli, E., van den Brink, M. R. M., Champlin, R. E., Ciurea, S. O., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Significant progress has been made over the past decade in haploidentical transplantation, with the development of novel methods to control intense alloreactive reactions generated in the major HLA-mismatched setting. Application of post-transplantation cyclophosphamide has gained worldwide acceptance as an effective and low-cost way to perform this type of transplantation, with outcomes now similar to those from HLA-matched unrelated donors. These advances have resulted in improved treatment-related mortality, whereas disease relapse has emerged as the most common cause of treatment failure. In addition, improvements in immunologic reconstitution after transplantation are much needed, not only in haploidentical transplantation but in all forms of stem cell transplantation. This symposium has focused on some of the most promising methods to control alloreactivity in this form of transplantation and application of cellular therapy to prevent disease relapse after transplantation, as well as understanding immunologic reconstitution and foreseeable approaches to improve immune recovery after transplantation.

Published
2016

21. Expression variability and function of the RET gene in adult peripheral blood mononuclear cells

Author

Rusmini, Marta, Griseri, P, Matera, I, Pontarini, E, Ravazzolo, Roberto, Mavilio, D, and Ceccherini, I.

Subjects
Adult, Glial Cell Line-Derived Neurotrophic Factor Receptors, Gene Expression Regulation, Carcinogenesis, T-Lymphocytes, Interleukin-8, Proto-Oncogene Proteins c-ret, Leukocytes, Mononuclear, Humans, Nerve Growth Factors, RNA, Messenger
Abstract

RET is a gene playing a key role during embryogenesis and in particular during the enteric nervous system development. High levels of RET gene expression are maintained in different human tissues also in adulthood, although their physiological role remains unclear. In particular, collected evidences of a RET contribution in the development and maintenance of the immune system prompted us to investigate its levels of surface expression on peripheral blood mononuclear cells (PBMCs) from adult healthy donors. Despite variability among samples, RET expression was conserved at similar levels in the different immune cell subsets, with higher correlations in similar lymphocyte populations (i.e. CD4(+) and CD8(+) T cells). Conversely, no correlation was found between the amount of RET receptor, the expression of its putative ligands and co-receptors and the genotypes at the RET locus. Moreover, we investigated the RET-associated inflammatory pathways in PBMCs from healthy donors both in resting conditions and upon glial cell derived neurotrophic factor (GDNF) and GPI-linked co-receptors alpha 1 (GFRα1) mediated RET activation. RET mRNA levels positively correlated with the transcript amount of interleukin-8 (IL-8), a cytokine produced by monocytes and macrophages, though we could not demonstrate its direct effect on RET expression by in vitro experiments on THP1 human monocytic cells. These results imply that RET expression might be influenced by either cis- and/or trans-factors, which together would account for its high variability within the general population, and suggest a putative functional role of the RET gene in modulating immune cell responses during inflammation and carcinogenesis.

Published
2013

22. Consensus guidelines for the detection of immunogenic cell death

Author

Kepp, O., Senovilla, L., Vitale, I., Vacchelli, E., Adjemian, S., Agostinis, P., Apetoh, L., Aranda, F., Barnaba, V., Bloy, N., Bracci, L., Breckpot, K., Brough, D., Buqué, A., Castro, Mg, Cirone, M., Colombo, Mi, Cremer, I., Demaria, S., Dini, L., Eliopoulos, A., Faggioni, A., Formenti, Sc, Fu??íková, J., Gabriele, L., Gaipl, Us, Galon, J., Garg, A., Ghiringhelli, F., Giese, Na, Guo, Zs, Hemminki, A., Herrmann, M., Hodge, Jw, Holdenrieder, S., Honeychurch, J., Hm, Hu, Huang, X., Illidge, Tm, Kono, K., Korbelik, M., Krysko, Dv, Loi, S., Lowenstein, Pr, Lugli, E., Ma, Y., Madeo, F., Manfredi, Aa, Martins, I., Matzinger, P., Mavilio, D., Menger, L., Merendino, N., Michaud, M., Mignot, G., Mossman, Kl, Multhoff, G., Oehler, R., Palombo, F., Panaretakis, T., Pol, J., Proietti, E., Ricci, Je, Riganti, Chiara, Rovere Querini, P., Rubartelli, A., Sistigu, A., Smyth, Mj, Sonnemann, J., Spisek, R., Stagg, J., Sukkurwala, Aq, Tartour, E., Thorburn, A., Thorne, Sh, Vandenabeele, P., Velotti, F., Workenhe, Sr, Yang, H., Zong, Wx, Zitvogel, L., Kroemer, G., Galluzzi, L., Medicine and Pharmacy academic/administration, Basic (bio-) Medical Sciences, Laboratory of Molecullar and Cellular Therapy, Chemistry, Kepp, Oliver, Senovilla, Laura, Vitale, Ilio, Vacchelli, Erika, Adjemian, Sandy, Agostinis, Patrizia, Apetoh, Lionel, Aranda, Fernando, Barnaba, Vincenzo, Bloy, Norma, Bracci, Laura, Breckpot, Karine, Brough, David, Buqué, Aitziber, Castro, Maria G, Cirone, Mara, Colombo, Maria I, Cremer, Isabelle, Demaria, Sandra, Dini, Luciana, Eliopoulos, Aristides G, Faggioni, Alberto, Formenti, Silvia C, Fučíková, Jitka, Gabriele, Lucia, Gaipl, Udo S, Galon, Jérôme, Garg, Abhishek, Ghiringhelli, Françoi, Giese, Nathalia A, Guo, Zong Sheng, Hemminki, Akseli, Herrmann, Martin, Hodge, James W, Holdenrieder, Stefan, Honeychurch, Jamie, Hu, Hong Min, Huang, Xing, Illidge, Tim M, Kono, Koji, Korbelik, Mladen, Krysko, Dmitri V, Loi, Sherene, Lowenstein, Pedro R, Lugli, Enrico, Ma, Yuting, Madeo, Frank, Manfredi, Angelo A, Martins, Isabelle, Mavilio, Domenico, Menger, Laurie, Merendino, Nicolò, Michaud, Michael, Mignot, Gregoire, Mossman, Karen L, Multhoff, Gabriele, Oehler, Rudolf, Palombo, Fabio, Panaretakis, Theochari, Pol, Jonathan, Proietti, Enrico, Ricci, Jean Ehrland, Riganti, Chiara, Rovere Querini, Patrizia, Rubartelli, Anna, Sistigu, Antonella, Smyth, Mark J, Sonnemann, Juergen, Spisek, Radek, Stagg, John, Sukkurwala, Abdul Qader, Tartour, Eric, Thorburn, Andrew, Thorne, Stephen H, Vandenabeele, Peter, Velotti, Francesca, Workenhe, Samuel T, Yang, Haining, Zong, Wei Xing, Zitvogel, Laurence, Kroemer, Guido, Galluzzi, Lorenzo, Kepp, O, Senovilla, L, Vitale, I, Vacchelli, E, Adjemian, S, Agostinis, P, Apetoh, L, Aranda, F, Barnaba, V, Bloy, N, Bracci, L, Breckpot, K, Brough, D, Buque, A, Castro, Mg, Cirone, M, Colombo, Mi, Cremer, I, Demaria, S, Dini, L, Eliopoulos, Ag, Faggioni, A, Formenti, Sc, Fucikova, J, Gabriele, L, Gaipl, U, Galon, J, Garg, A, Ghiringhelli, F, Giese, Na, Guo, Z, Hemminki, A, Herrmann, M, Hodge, Jw, Holdenrieder, S, Honeychurch, J, Hu, Hm, Huang, X, Illidge, Tm, Kono, K, Korbelik, M, Krysko, Dv, Loi, S, Lowenstein, Pr, Lugli, E, Ma, Yt, Madeo, F, Manfredi, ANGELO ANDREA M. A., Martins, I, Mavilio, D, Menger, L, Merendino, N, Michaud, M, Mignot, G, Mossman, Kl, Multhoff, G, Oehler, R, Palombo, F, Panaretakis, T, Pol, J, Proietti, E, Ricci, Je, Riganti, C, ROVERE QUERINI, Patrizia, Rubartelli, A, Sistigu, A, Smyth, Mj, Sonnemann, J, Spisek, R, Stagg, J, Sukkurwala, Aq, Tartour, E, Thorburn, A, Thorne, Sh, Vandenabeele, P, Velotti, F, Workenhe, St, Yang, Hn, Zong, Wx, Zitvogel, L, Kroemer, G, and Galluzzi, L.

Subjects
HSV-1, herpes simplex virus type I, Δψm, mitochondrial transmembrane potential, medicine.medical_treatment, DAMP, damage-associated molecular pattern, detection, FLT3LG, fms-related tyrosine kinase 3 ligand, Review, member 3, calreticulin, Eukaryotic translation initiation factor 2A, RFP, red fluorescent protein, 0302 clinical medicine, MOMP, mitochondrial outer membrane permeabilization, Immunology and Allergy, GFP, green fluorescent protein, HMGB1, 0303 health sciences, education.field_of_study, Toll-like receptor, BAK1, BCL2-antagonist/killer 1, H2B, histone 2B, endoplasmic reticulum stre, 3. Good health, BAX, BCL2-associated X protein, XBP1, X-box binding protein 1, cell death, Oncology, PDIA3, protein disulfide isomerase family A, 030220 oncology & carcinogenesis, endoplasmic reticulum stress, Immunogenic cell death, HSP, heat shock protein, immunotherapy, TLR, Toll-like receptor, autophagy, ATF6, activating transcription factor 6, Immunology, ICD, immunogenic cell death, EIF2A, eukaryotic translation initiation factor 2A, Guidelines, Biology, BCL2, B-cell CLL/lymphoma 2 protein, ER, endoplasmic reticulum, PI, propidium iodide, ATP release, 03 medical and health sciences, Immune system, immunogenic, medicine, IFN, interferon, Antigen-presenting cell, education, 030304 developmental biology, CALR, calreticulin, Damage-associated molecular pattern, Immunotherapy, CTL, cytotoxic T lymphocyte, HMGB1, high mobility group box 1, IL, interleukin, G3BP1, GTPase activating protein (SH3 domain) binding protein 1, APC, antigen-presenting cell, Cancer cell, DiOC6(3), 3,3′-dihexyloxacarbocyanine iodide, DAPI, 4′,6-diamidino-2-phenylindole
Abstract

Apoptotic cells have long been considered as intrinsically tolerogenic or unable to elicit immune responses specific for dead cell-associated antigens. However, multiple stimuli can trigger a functionally peculiar type of apoptotic demise that does not go unnoticed by the adaptive arm of the immune system, which we named "immunogenic cell death" (ICD). ICD is preceded or accompanied by the emission of a series of immunostimulatory damage-associated molecular patterns (DAMPs) in a precise spatiotemporal configuration. Several anticancer agents that have been successfully employed in the clinic for decades, including various chemotherapeutics and radiotherapy, can elicit ICD. Moreover, defects in the components that underlie the capacity of the immune system to perceive cell death as immunogenic negatively influence disease outcome among cancer patients treated with ICD inducers. Thus, ICD has profound clinical and therapeutic implications. Unfortunately, the gold-standard approach to detect ICD relies on vaccination experiments involving immunocompetent murine models and syngeneic cancer cells, an approach that is incompatible with large screening campaigns. Here, we outline strategies conceived to detect surrogate markers of ICD in vitro and to screen large chemical libraries for putative ICD inducers, based on a high-content, high-throughput platform that we recently developed. Such a platform allows for the detection of multiple DAMPs, like cell surface-exposed calreticulin, extracellular ATP and high mobility group box 1 (HMGB1), and/or the processes that underlie their emission, such as endoplasmic reticulum stress, autophagy and necrotic plasma membrane permeabilization. We surmise that this technology will facilitate the development of next-generation anticancer regimens, which kill malignant cells and simultaneously convert them into a cancer-specific therapeutic vaccine. peerreview_statement: The publishing and review policy for this title is described in its Aims & Scope. aims_and_scope_url: http://www.tandfonline.com/action/journalInformation?show=aimsScope&journalCode=koni20 ispartof: OncoImmunology vol:3 issue:9 pages:12472-124508 ispartof: location:United States status: published

Published
2014

25. B-cell reconstitution recapitulates B-cell lymphopoiesis following haploidentical BM transplantation and post-transplant CY

Author

Roberto, A, primary, Castagna, L, additional, Gandolfi, S, additional, Zanon, V, additional, Bramanti, S, additional, Sarina, B, additional, Crocchiolo, R, additional, Todisco, E, additional, Carlo-Stella, C, additional, Tentorio, P, additional, Timofeeva, I, additional, Santoro, A, additional, Bella, S Della, additional, Roederer, M, additional, Mavilio, D, additional, and Lugli, E, additional

Published
2014
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30. Safety of MF59-Adjuvanted Influenza Vaccination in the Elderly: Results of a Comparative Study of MF59-Adjuvanted Vaccine Versus Nonadjuvanted Influenza Vaccine in Northern Italy

Author

Villa, M., primary, Black, S., additional, Groth, N., additional, Rothman, K. J., additional, Apolone, G., additional, Weiss, N. S., additional, Aquino, I., additional, Boldori, L., additional, Caramaschi, F., additional, Gattinoni, A., additional, Malchiodi, G., additional, Crucitti, A., additional, Della Cioppa, G., additional, Scarpini, E., additional, Mavilio, D., additional, and Mannino, S., additional

Published
2013
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40. APOL1 polymorphism modulates sphingolipid profile of human podocytes

Author

Xiqian Lan, Pravin C. Singhal, Manuela Valsecchi, Joanna Mikulak, Moin A. Saleem, Valentina Cazzetta, Massimo Aureli, Ferdinando Oriolo, Domenico Mavilio, Rocco Piazza, Valsecchi, M, Cazzetta, V, Oriolo, F, Lan, X, Piazza, R, Saleem, M, Singhal, P, Mavilio, D, Mikulak, J, and Aureli, M

Subjects
Ceramide, Glycoside Hydrolases, 030232 urology & nephrology, Globotriaosylceramide, APOL1 polymorphism, Podocyte, Biochemistry, Sphingolipid, 03 medical and health sciences, chemistry.chemical_compound, Lactosylceramide, 0302 clinical medicine, Humans, APOL1, music, Molecular Biology, Lipid raft, Lipid rafts, 030304 developmental biology, Sphingolipids, 0303 health sciences, Polymorphism, Genetic, music.instrument, Sphingosine, Podocytes, Cell Membrane, Wild type, Cell Biology, Apolipoprotein L1, Cell biology, Metabolism, Gene Expression Regulation, chemistry, Original Article, lipids (amino acids, peptides, and proteins), Sphingomyelin, HIVAN, Plasma membrane
Abstract

Apolipoprotein L1 (APOL1) wild type (G0) plays a role in the metabolism of sphingolipids, glycosphingolipids, sphingomyelin and ceramide, which constitute bioactive components of the lipid rafts (DRM). We asked whether APOL1 variants (APOL1-Vs) G1 and G2 carry the potential to alter the metabolism of sphingolipids in human podocytes. The sphingolipid pattern in HPs overexpressing either APOL1G0 or APOL1-Vs was analysed by using a thin mono- and bi-dimensional layer chromatography, mass-spectrometry and metabolic labelling with [1-3H]sphingosine. HP G0 and G1/G2-Vs exhibit a comparable decrease in lactosylceramide and an increase in the globotriaosylceramide content. An analysis of the main glycohydrolases activity involved in glycosphingolipid catabolism showed an overall decrease in the activeness of the tested enzymes, irrespective of the type of APOL1-Vs expression. Similarly, the high throughput cell live-based assay showed a comparable increased action of the plasma membrane glycosphingolipid-glycohydrolases in living cells independent of the genetic APOL1 expression profile. Importantly, the most significative modification of the sphingolipid pattern induced by APOL1-Vs occurred in DRM resulted with a drastic reduction of radioactivity associated with sphingolipids. G1/G2-Vs present a decrease amount of globotriaosylceramide and globopentaosylceramide compared to G0. Additionally, ceramide at the DRM site and lactosylceramide in general, showed a greatest fall in G1/G2 in comparison with G0. Additionally, the levels of glucosylceramide decreased only in the DRM of human podocytes overexpressing G1/G2-Vs. These findings suggest that altered sphingolipidsprofiles may contribute to the deranged functionality of the plasma membrane in APOL1 risk milieu. Electronic supplementary material The online version of this article (10.1007/s10719-020-09944-w) contains supplementary material, which is available to authorized users.

Published
2020

41. NKG2A expression identifies a subset of human Vδ2 T cells exerting the highest antitumor effector functions

Author

Sara Terzoli, Rocco Piazza, Domenico Supino, Elena Bruni, Guido Torzilli, Eric Vivier, Claudia Carenza, Likai Tan, Domenico Mavilio, Matteo Simonelli, Joanna Mikulak, Sarina Ravens, Matteo Cimino, Matteo Donadon, Silvia Della Bella, Sara Franzese, Federico Colombo, Enrico Lugli, Emanuela Marcenaro, Anna Villa, Immo Prinz, Valentina Cazzetta, Paolo Marzano, Lorenzo Bello, DUMENIL, Anita, Università degli Studi di Milano = University of Milan (UNIMI), Istituto Clinico Humanitas [Milan] (IRCCS Milan), Humanitas University [Milan] (Hunimed), San Raffaele Scientific Institute, Vita-Salute San Raffaele University and Center for Translational Genomics and Bioinformatics, Hannover Medical School [Hannover] (MHH), Università degli studi di Genova = University of Genoa (UniGe), Centre d'Immunologie de Marseille - Luminy (CIML), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Hôpital de la Timone [CHU - APHM] (TIMONE), Cazzetta, V, Bruni, E, Terzoli, S, Carenza, C, Franzese, S, Piazza, R, Marzano, P, Donadon, M, Torzilli, G, Cimino, M, Simonelli, M, Bello, L, Villa, A, Tan, L, Ravens, S, Prinz, I, Supino, D, Colombo, F, Lugli, E, Marcenaro, E, Vivier, E, Della Bella, S, Mikulak, J, and Mavilio, D

Subjects
Cytotoxicity, Immunologic, Male, QH301-705.5, immune education, [SDV]Life Sciences [q-bio], Human leukocyte antigen, Biology, Inhibitory postsynaptic potential, Lymphocyte Activation, General Biochemistry, Genetics and Molecular Biology, Transcriptome, Lymphocytes, Tumor-Infiltrating, NKG2A immune checkpoint, Vδ2 T cells, cancer, cancer immune-therapy, hyper-reactivity, Neoplasms, medicine, Humans, Cell Self Renewal, Biology (General), Intraepithelial Lymphocytes, Vδ2 T cell, Aged, Cell Proliferation, Mechanism (biology), Effector, Cancer, Infant, Receptors, Antigen, T-Cell, gamma-delta, Middle Aged, medicine.disease, Phenotype, Coculture Techniques, Immunity, Innate, Gene Expression Regulation, Neoplastic, [SDV] Life Sciences [q-bio], Hepatocellular carcinoma, Case-Control Studies, Cancer research, Cytokines, Female, K562 Cells, NK Cell Lectin-Like Receptor Subfamily C, Signal Transduction
Abstract

International audience; Human Vδ2 cells are innate-like γδ T effectors performing potent immune surveillance against tumors. The constitutive expression of NKG2A identifies a subset of Vδ2 T cells licensed with an intrinsic hyper-responsiveness against cancer. Indeed, the transcriptomic profiles of NKG2A+ and NKG2A- cells characterize two distinct "intralineages" of Vδ2 T lymphocytes that appear early during development, keep their phenotypes, and show self-renewal capabilities in adult life. The hyper-responsiveness of NKG2A+ Vδ2 T cells is counterbalanced by the inhibitory signaling delivered by human leukocyte antigen E (HLA-E) expressed on malignant cells as a tumor-escape mechanism. However, either masking or knocking out NKG2A restores the capacity of Vδ2 T cells to exert the highest effector functions even against HLA-E+ tumors. This is highly relevant in the clinic, as the different degrees of engagement of the NKG2A-HLA-E checkpoint in hepatocellular carcinoma, glioblastoma, and non-small cell lung cancer directly impact patients' overall survival. These findings open avenues for developing combined cellular and immunologic anticancer therapies.

Published
2021

42. High-dimensional single cell analysis identifies stem-like cytotoxic CD8+ T cells infiltrating human tumors

Author

Joanna Mikulak, Andrea Grilli, Marco Alloisio, Emilia Maria Cristina Mazza, Giulia Veronesi, Enrico Lugli, Federico Colombo, Francesco Ferrari, Pierluigi Novellis, Egesta Lopci, Jolanda Brummelman, Giorgia Alvisi, Domenico Mavilio, Brummelman, J, Mazza, Emc, Alvisi, G, Colombo, F, Grilli, A, Mikulak, J, Mavilio, D, Alloisio, M, Ferrari, F, Lopci, E, Novellis, P, Veronesi, G, and Lugli, E

Subjects
0301 basic medicine, Male, Receptors, CXCR5, Lung Neoplasms, medicine.medical_treatment, T cell, Immunology, Biology, CD8-Positive T-Lymphocytes, Article, Transcriptome, 03 medical and health sciences, Mice, 0302 clinical medicine, TIGIT, Single-cell analysis, medicine, Immunology and Allergy, Cytotoxic T cell, Animals, Humans, Receptors, Immunologic, Receptor, Hepatitis A Virus Cellular Receptor 2, Research Articles, Stem Cells, Immunotherapy, Neoplasm Proteins, Tumor Necrosis Factor Receptor Superfamily, Member 7, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cancer research, Female, CD8
Abstract

CD8+ T cells infiltrating tumors are largely dysfunctional. Brummelman and Mazza et al. identify partially exhausted CXCR5+ TIM-3– CD8+ T cells with enhanced stem-like properties and cytotoxicity infiltrating human solid tumors. These cells express candidate immunotherapeutic targets (PD-1, TIGIT and CD27) for their reinvigoration., CD8+ T cells infiltrating tumors are largely dysfunctional, but whether a subset maintains superior functionality remains ill defined. By high-dimensional single cell analysis of millions of CD8+ T cells from 53 individuals with lung cancer, we defined those subsets that are enriched in tumors compared with cancer-free tissues and blood. Besides exhausted and activated cells, we identified CXCR5+ TIM-3– CD8+ T cells with a partial exhausted phenotype, while retaining gene networks responsible for stem-like plasticity and cytotoxicity, as revealed by single cell sequencing of the whole transcriptome. Ex vivo, CXCR5+ TIM-3– CD8+ T cells displayed enhanced self-renewal and multipotency compared with more differentiated subsets and were largely polyfunctional. Analysis of inhibitory and costimulatory receptors revealed PD-1, TIGIT, and CD27 as possible targets of immunotherapy. We thus demonstrate a hierarchy of differentiation in the context of T cell exhaustion in human cancer similar to that of chronically infected mice, which is further shown to disappear with disease progression., Graphical Abstract

Published
2018

43. Are human Vδ2(pos) T cells really resistant to aging and Human Cytomegalovirus infection?()

Author

Francesco Dieli, Domenico Mavilio, Joanna Mikulak, Mikulak J., Dieli F., and Mavilio D.

Subjects
Human cytomegalovirus, Cytomegalovirus Infection, Letter, Congenital cytomegalovirus infection, Cytomegaloviru, Cytomegalovirus, T-Lymphocyte Subset, Receptors, Antigen, T-Cell, gamma-delta, General Medicine, Biology, medicine.disease, Virology, General Biochemistry, Genetics and Molecular Biology, T-Lymphocyte Subsets, Cytomegalovirus Infections, Host-Pathogen Interactions, medicine, Humans, Cytomegalovirus infections, Lymphocyte subsets, Human, Disease Resistance
Abstract

In their recent paper, Weili Xu et al. [1] described the different behaviors of Vδ1pos and Vδ2pos T cell subsets in response to lifelong stress and claimed that Vδ2pos T cells are not affected by aging and Human Cytomegalovirus (HCMV) infection. While we agree that these two γδ T cell subsets diverge both in phenotype/function and in tissue distribution, we are somewhat surprised that authors did not take into account the several previously published and contradictory experimental evidence in regards to senescence of Vδ2pos T cells [2,3]. These latter studies reported that HCMV infection not only induces a clonal expansion of a distinct Vγ9neg/Vδ2pos T cell subset, but also determines a concomitant adaptive differentiation from CD27high naïve cells to CD27low/neg terminal-effectors. However, Weili Xu et al. argued that the expression and kinetics of both CD27 and CD45RA surface markers do not change and follow the homeostatic changes of Vδ2pos T cells. This statement goes in the opposite direction to previously reported findings as the CD27/CD45RA phenotype has been shown to mark the maturation and differentiation (TNaïve, TCentral-Memory, Teffector-Memory and TEffectory-Memory RA) of Vδ2pos T cells. Indeed, the different surface expression of both CD27 and CD45 parallel the progressive decrease of telomere length, the proliferative capacity as well as the different effector-functions and resistance to death of Vδ2+ T cells in response to antigens and homeostatic cytokines [4,5]. Hence, we believe that these controversial issues require further discussion beyond the unilateral conclusion given by the study of Weili Xu et al.

Published
2019

44. The challenges of primary biliary cholangitis: What is new and what needs to be done

Author

John M. Vierling, Edward L. Krawitt, Gianfranco Alpini, Shinji Shimoda, Mark G. Swain, Mario Strazzabosco, M. Eric Gershwin, Pietro Invernizzi, George N. Dalekos, David H. Adams, Diego Vergani, Atsushi Tanaka, Koichi Tsuneyama, Andrea De Gottardi, Kenichi Harada, Gideon M. Hirschfield, Christopher L. Bowlus, Olivier Chazouillères, Marco Carbone, Eamonn Martin Quigley, Xiong Ma, Michael Trauner, David Jones, Antonio Lanzavecchia, Benedetta Terziroli Beretta-Piccoli, Ehud Zigmond, Michael Manns, Einar Bjornsson, Giorgina Mieli-Vergani, Ulrich Beuers, Federica Sallusto, Zhe-Xiong Lian, Jesus M. Banales, Domenico Mavilio, Terziroli Beretta-Piccoli, B, Mieli-Vergani, G, Vergani, D, Vierling, J, Adams, D, Alpini, G, Banales, J, Beuers, U, Bjornsson, E, Bowlus, C, Carbone, M, Chazouilleres, O, Dalekos, G, De Gottardi, A, Harada, K, Hirschfield, G, Invernizzi, P, Jones, D, Krawitt, E, Lanzavecchia, A, Lian, Z, Ma, X, Manns, M, Mavilio, D, Quigley, E, Sallusto, F, Shimoda, S, Strazzabosco, M, Swain, M, Tanaka, A, Trauner, M, Tsuneyama, K, Zigmond, E, and Gershwin, M

Subjects
0301 basic medicine, Cholagogues and Choleretics, Histology, Cirrhosis, medicine.drug_class, Biliary epithelial cell, Immunology, Bile acid, Disease, Chenodeoxycholic Acid, Bioinformatics, Autoimmune Diseases, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cholestasis, MED/12 - GASTROENTEROLOGIA, medicine, Humans, Immunology and Allergy, 030203 arthritis & rheumatology, Liver Cirrhosis, Biliary, business.industry, Primary biliary cholangitis, Ursodeoxycholic Acid, Autoantibody, Obeticholic acid, Biomarker, Congresses as Topic, medicine.disease, Personalized medicine, Ursodeoxycholic acid, 030104 developmental biology, Liver, chemistry, Antibodies, Antinuclear, Etiology, Female, business, medicine.drug
Abstract

Primary Biliary Cholangitis (PBC) is an uncommon, chronic, cholangiopathy of autoimmune origin and unknown etiology characterized by positive anti-mitochondrial autoantibodies (AMA), female preponderance and progression to cirrhosis if left untreated. The diagnosis is based on AMA- or PBC-specific anti-nuclear antibody (ANA)-positivity in the presence of a cholestatic biochemical profile, histologic confirmation being mandatory only in seronegative cases. First-line treatment is ursodeoxycholic acid (UDCA), which is effective in preventing disease progression in about two thirds of the patients. The only approved second-line treatment is obeticholic acid. This article summarizes the most relevant conclusions of a meeting held in Lugano, Switzerland, from September 23rd-25th 2018, gathering basic and clinical scientists with various background from around the world to discuss the latest advances in PBC research. The meeting was dedicated to Ian Mackay, pioneer in the field of autoimmune liver diseases. The role of liver histology needs to be reconsidered: liver pathology consistent with PBC in AMA-positive individuals without biochemical cholestasis is increasingly reported, raising the question as to whether biochemical cholestasis is a reliable disease marker for both clinical practice and trials. The urgent need for new biomarkers, including more accurate markers of cholestasis, was also widely discussed during the meeting. Moreover, new insights in interactions of bile acids with biliary epithelia in PBC provide solid evidence of a role for impaired epithelial protection against potentially toxic hydrophobic bile acids, raising the fundamental question as to whether this bile acid-induced epithelial damage is the cause or the consequence of the autoimmune attack to the biliary epithelium. Strategies are needed to identify difficult-to-treat patients at an early disease stage, when new therapeutic approaches targeting immunologic pathways, in addition to bile acid-based therapies, may be effective. In conclusion, using interdisciplinary approaches, groundbreaking advances can be expected before long in respect to our understanding of the etiopathogenesis of PBC, with the ultimate aim of improving its treatment.

Published
2019

45. MFSD2A Promotes Endothelial Generation of Inflammation-resolving Lipid Mediators and Reduces Colitis in Mice

Author

Alberto Malesci, Silvio Danese, Antonino Spinelli, Federica Furfaro, Stefania Vetrano, Paola Antonia Corsetto, Luciana Petti, Luca Massimino, Angela Maria Rizzo, Silvia D'Alessio, Laurent Peyrin-Biroulet, Gionata Fiorino, Carlotta Tacconi, Domenico Mavilio, Philippe Fonteyne, Federica Ungaro, F. Calcaterra, Andrea Piontini, Valeria Garzarelli, Silvia Della Bella, Carmen Correale, Krishna Rao Maddipati, Michele Carvello, Ungaro, F., Tacconi, C., Massimino, L., Corsetto, P., Correale, C., Fonteyne, P., Piontini, A., Garzarelli, V., Calcaterra, F., Della Bella, S., Spinelli, A., Carvello, M., Rizzo, A., Vetrano, S., Petti, L., Fiorino, G., Furfaro, F., Mavilio, D., Maddipati, K., Malesci, A., Peyrin-Biroulet, L., D’Alessio, S., and Danese, S.

Subjects
0301 basic medicine, Endothelium, Docosahexaenoic Acids, Angiogenesis, Colon, IBD, Mice, Nude, Inflammation, Biology, gut vasculature, Transfection, Inflammatory bowel disease, 03 medical and health sciences, angiogenesis, Cytochrome P-450 Enzyme System, inflammatory bowel disease, medicine, Animals, Humans, Oxylipins, Progenitor cell, Colitis, Cells, Cultured, Endothelial Progenitor Cells, Hepatology, Symporters, Tumor Necrosis Factor-alpha, Tumor Suppressor Proteins, Dextran Sulfate, Gastroenterology, Membrane Transport Proteins, Lipid metabolism, medicine.disease, Ulcerative colitis, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Immunology, Cancer research, Epoxy Compounds, RNA Interference, medicine.symptom, Signal Transduction
Abstract

Background & Aims Alterations in signaling pathways that regulate resolution of inflammation (resolving pathways) contribute to pathogenesis of ulcerative colitis (UC). The resolution process is regulated by lipid mediators, such as those derived from the ω-3 docosahexaenoic acid (DHA), whose esterified form is transported by the major facilitator superfamily domain containing 2A (MFSD2A) through the endothelium of brain, retina, and placenta. We investigated if and how MFSD2A regulates lipid metabolism of gut endothelial cells to promote resolution of intestinal inflammation. Methods We performed lipidomic and functional analyses of MFSD2A in mucosal biopsies and primary human intestinal microvascular endothelial cells (HIMECs) isolated from surgical specimens from patients with active, resolving UC and healthy individuals without UC (controls). MFSD2A was knocked down in HIMECs with small hairpin RNAs or overexpressed from a lentiviral vector. Human circulating endothelial progenitor cells that overexpress MFSD2A were transferred to CD1 nude mice with dextran sodium sulfate–induced colitis, with or without oral administration of DHA. Results Colonic biopsies from patients with UC had reduced levels of inflammation-resolving DHA-derived epoxy metabolites compared to healthy colon tissues or tissues with resolution of inflammation. Production of these metabolites by HIMECs required MFSD2A, which is required for DHA retention and metabolism in the gut vasculature. In mice with colitis, transplanted endothelial progenitor cells that overexpressed MFSD2A not only localized to the inflamed mucosa but also restored the ability of the endothelium to resolve intestinal inflammation, compared with mice with colitis that did not receive MFSD2A-overexpressing endothelial progenitors. Conclusions Levels of DHA-derived epoxides are lower in colon tissues from patients with UC than healthy and resolving mucosa. Production of these metabolites by gut endothelium requires MFSD2A; endothelial progenitor cells that overexpress MFSD2A reduce colitis in mice. This pathway might be induced to resolve intestinal inflammation in patients with colitis.

Published
2017

46. Editorial: Activation, functions, and generation of immunological memory in γδ T lymphocytes: lessons from nonhuman primates

Author

Francesco Dieli, Domenico Mavilio, Dieli, F, and Mavilio, D

Subjects
TRAIL, T cell, Lymphocyte, Immunology, Population, Major histocompatibility complex, Antigen, T-Lymphocyte Subsets, medicine, Animals, Immunology and Allergy, Cytotoxic T cell, Listeriosis, education, Lung, Antigens, Bacterial, education.field_of_study, Tumor, biology, Effector, T-cell receptor, Cell Biology, gamma delta cell, Listeria monocytogenes, Organophosphates, Cell biology, medicine.anatomical_structure, Bacterial Vaccines, biology.protein, Spotlight on Leading Edge Research, Immunization, Immunologic Memory
Abstract

T cells constitute an unconventional lymphocyte population with distinct functions complementary to those of CD4 and CD8 T cells. As such, they have both adaptive features, such as expression of the TCR, and innate-like functions reminiscent of NK cells, with whom they share extensive repertoires of activating and inhibitory receptors [1, 2]. Although most antigens recognized by murine T cells remain obscure, advances have been made in identifying ligands for human T cells. The majority of circulating human T lymphocytes expresses a TCR formed by the preferentially-paired V 9 and V 2 chains (here and thereafter, called V 9V 2 T cells). Instead of binding peptides associated with molecules belonging to the MHC, V 9V 2 T cells recognize pyrophosphate intermediates of the microbial or eukaryotic isoprenoid synthesis pathways, called PAgs [3, 4]. Isoprenoids are produced by one of two major pathways: the classical mevalonate pathway and the alternative deoxyxylulose (nonmevalonate) pathway of isoprenoids synthesis that is used by numerous bacterial species and by some highly significant eukaryotic pathogens but not by vertebrate cells. IPP is an intermediate metabolite that is present in both pathways, whereas HMBPP is only produced in the nonmevalonate pathway by certain microbes, including Mycobacterium tuberculosis and Listeria monocytogenes. Given this cross-reactivity between human V 9V 2 T cells and microbial and self-PAgs, there is a great interest in the scientific community of elucidating how TCR signaling can be induced by such small molecules. PAgs can directly activate V 9V 2 T cells, but such activation is greatly enhanced by monocytes and/or DCs. Hence, either PAgs are presented as cargo to the reactive TCR or their cellular processing somehow sensitizes cell recognition through the engagement of V 9V 2 TCR (i.e., by stabilizing surface expression of TCR-binding molecules) [3, 4]. A candidate molecule involved in intracellular PAg processing is the F1-ATPase, which was reported to bind directly the V 9V 2 TCR and to also interact with IPP conjugated to AMP, an adenosine derivative of IPP [5]. Thus, V 9V 2 T cells may collectively monitor multiple components of pathways regulating cholesterol biosynthesis that are altered by infection or other forms of stress. In this regard, it was found recently that PAg-induced V 9V 2 T cell activation also involves the participation of BTN3A1, a widely expressed member of the Ig superfamily [6]. Therefore, production of exogenous HMBPP or up-regulation of endogenous IPP in human cells in response to infections or noninfective immune dysregulation provokes V 9V 2 T cell reactivity, albeit at substantially different sensitivity. Although IPP was isolated from Mycobacterium smegmatis as the first natural ligand for human T cells, it soon became clear that the amounts of IPP present in bacterial extracts do not reach the minimum threshold required for inducing V 9V 2 T cell activation in several experimental systems in vitro. HMBPP is more potent than IPP in the context of in vitro activation of V 9V 2 T cells, active at picoto nanomolar concentrations, whereas IPP requires 3-log higher concentrations within micromolar ranges. Such high concentrations are not produced in physiological conditions but are reached during the course of pathologic metabolisms of stressed or infected cells. V 9V 2 T cells evolved to detect stressed cells and microbial pathogens, although only if the local amounts of IPP released from damaged tissues are at least 10,000-fold higher than the HMBPP concentrations reached during bacterial infections. This explains the different bioactivities of these two compounds [7]. The finding that V 9V 2 T cells respond differentially in vitro to increasing concentrations of structurally related PAgs indicates that such ligands constitute agonists for the TCR at different strengths. Indeed, experimental approaches aiming to define the underlying molecular basis of T lymphocyte activation demonstrate that V 9V 2 TCR can discriminate between subtle differences of substrates. By analyzing early cellular events and late effector responses of V 9V 2 T cells, it has also been reported that IPP induces a timeand dose-dependent down-modulation of the reactive TCR, whereas HMBPP induces little or no TCR

Published
2014

47. Full-length soluble urokinase plasminogen activator receptor down-modulates nephrin expression in podocytes

Author

Massimo Alfano, Guido Giusti, Silvio Danese, Silvia D'Alessio, Marco Genua, Maria Pia Rastaldi, Paola Cinque, Pravin C. Singhal, Federica Portale, Domenico Mavilio, Manuela Lo Porto, Silvia Proietti, Manuela Nebuloni, Joanna Mikulak, Moin A. Saleem, Alfano, M, Cinque, P, Giusti, G, Proietti, S, Nebuloni, M, Danese, S, D'Alessio, S, Genua, M, Portale, F, Lo Porto, M, Singhal, Pc, Rastaldi, Mp, Saleem, Ma, Mavilio, D, and Mikulak, J

Subjects
medicine.medical_specialty, Down-Regulation, urologic and male genital diseases, Article, Receptors, Urokinase Plasminogen Activator, Nephrin, Mice, 03 medical and health sciences, 0302 clinical medicine, Focal segmental glomerulosclerosis, Downregulation and upregulation, Internal medicine, medicine, Animals, Humans, Promoter Regions, Genetic, WT1 Proteins, Receptor, 030304 developmental biology, Mice, Knockout, 0303 health sciences, Integrin alphaVbeta3, Multidisciplinary, biology, Podocytes, urogenital system, Genetic Variation, Membrane Proteins, medicine.disease, female genital diseases and pregnancy complications, 3. Good health, Urokinase receptor, Proteinuria, Endocrinology, Gene Expression Regulation, SuPAR, 030220 oncology & carcinogenesis, biology.protein, Plasminogen activator, Protein Binding
Abstract

Increased plasma level of soluble urokinase-type plasminogen activator receptor (suPAR) was associated recently with focal segmental glomerulosclerosis (FSGS). In addition, different clinical studies observed increased concentration of suPAR in various glomerular diseases and in other human pathologies with nephrotic syndromes such as HIV and Hantavirus infection, diabetes and cardiovascular disorders. Here, we show that suPAR induces nephrin down-modulation in human podocytes. This phenomenon is mediated only by full-length suPAR, is time-and dose-dependent and is associated with the suppression of Wilms’ tumor 1 (WT-1) transcription factor expression. Moreover, an antagonist of αvβ3 integrin RGDfv blocked suPAR-induced suppression of nephrin. These in vitro data were confirmed in an in vivo uPAR knock out Plaur−/− mice model by demonstrating that the infusion of suPAR inhibits expression of nephrin and WT-1 in podocytes and induces proteinuria. This study unveiled that interaction of full-length suPAR with αvβ3 integrin expressed on podocytes results in down-modulation of nephrin that may affect kidney functionality in different human pathologies characterized by increased concentration of suPAR.

Published
2015

48. Human liver-resident CD56bright/CD16neg NK cells are retained within hepatic sinusoids via the engagement of CCR5 and CXCR6 pathways

Author

Guido Torzilli, Matteo Donadon, Antonio Bertoletti, Matteo Cimino, Michelle Hong, Elena Pontarini, Max Preti, Domenico Mavilio, Kelly Hudspeth, Silvio Bicciato, Enrico Lugli, M. Eric Gershwin, Pietro Invernizzi, Paolo Tentorio, Hudspeth, K, Donadon, M, Cimino, M, Pontarini, E, Tentorio, P, Preti, M, Hong, M, Bertoletti, A, Bicciato, S, Invernizzi, P, Lugli, E, Torzilli, G, Gershwin, M, and Mavilio, D

Subjects
0301 basic medicine, Antigens, Differentiation, T-Lymphocyte, Chemokine, T-Lymphocytes, Interleukin 21, 0302 clinical medicine, MED/12 - GASTROENTEROLOGIA, Cell Movement, Lectins, Receptors, Receptors, Viru, Killer Cells, 2.1 Biological and endogenous factors, Immunology and Allergy, Aetiology, Endothelial Cell, C-Type, biology, Liver immunology, Liver Disease, Janus kinase 3, Homing of hepatic NK cells, hemic and immune systems, Cherokees Chemokine receptor, CD56 Antigen, Virus, CD, Cell biology, Killer Cells, Natural, Liver, Differentiation, Natural, Interleukin 12, Receptors, Virus, Receptors, Chemokine, Kupffer Cell, Human, Signal Transduction, Adult, Receptors, CCR5, IgG, Kupffer Cells, 1.1 Normal biological development and functioning, Immunology, Antigens, CD56, CCL5, Article, 03 medical and health sciences, Underpinning research, Antigens, CD, Homing of hepatic NK cell, Cherokees Chemokine receptors, Humans, Lectins, C-Type, Antigens, CXCL16, Receptors, CXCR6, Innate immune system, Receptors, IgG, Endothelial Cells, CXCR6, 030104 developmental biology, T-Lymphocyte, biology.protein, Digestive Diseases, CCR5, 030215 immunology, Homing (hematopoietic)
Abstract

Rationale The liver-specific natural killer (NK) cell population is critical for local innate immune responses, but the mechanisms that lead to their selective homing and the definition of their functionally relevance remain enigmatic. Objectives We took advantage of the availability of healthy human liver to rigorously define the mechanisms regulating the homing of NK cells to liver and the repertoire of receptors that distinguish liver-resident NK (lr-NK) cells from circulating counterparts. Findings Nearly 50% of the entire liver NK cell population is composed of functionally relevant CD56 bright lr-NK cells that localize within hepatic sinusoids. CD56 bright lr-NK cells express CD69, CCR5 and CXCR6 and this unique repertoire of chemokine receptors is functionally critical as it determines selective migration in response to the chemotactic stimuli exerted by CCL3, CCL5 and CXCL16. Here, we also show that hepatic sinusoids express CCL3 pos Kupffer cells, CXCL16 pos endothelial cells and CCL5 pos T and NK lymphocytes. The selective presence of these chemokines in sinusoidal spaces creates a unique tissue niche for lr-CD56 bright NK cells that constitutively express CCR5 and CXCR6. CD56 bright lr-NK cells co-exist with CD56 dim conventional NK (c-NK) cells that are, interestingly, transcriptionally and phenotypically similar to their peripheral circulating counterparts. Indeed, CD56 dim c-NK cells lack expression of CD69, CCR5, and CXCR6 but express selectins, integrins and CX 3 CR1. Conclusion Our findings disclosing the phenotypic and functional differences between lr-Nk cells and c-NK cells are critical to distinguish liver-specific innate immune responses. Hence, any therapeutic attempts at modifying the large population of CD56 bright lr-NK cells will require modification of hepatic CCR5 and CXCR6.

Published
2015

49. Dendritic cells/natural killer cross-talk: a novel target for human immunodeficiency virus type-1 protease inhibitors

Author

Domenico Mavilio, Luigi Racioppi, Manuela Fogli, Maria Letizia Giardino Torchia, Elena Ciaglia, Laura Vitiello, Anna Maria Masci, Andrea la Sala, Giardino Torchia, M., Ciaglia, Elena, Masci, A. M., Vitiello, Laura, Fogli, M., la Sala, A., Mavilio, D., and Racioppi, Luigi

Subjects
Immunology, Immunology/Innate Immunity, Immunology/Immunomodulation, lcsh:Medicine, Enzyme-Linked Immunosorbent Assay, Biology, Immunophenotyping, Immune system, HIV Protease, medicine, Humans, HIV Protease Inhibitor, lcsh:Science, Cell Proliferation, CD86, Multidisciplinary, lcsh:R, Dendritic Cells, HIV Protease Inhibitors, Dendritic cell, Flow Cytometry, Killer Cells, Natural, Cell killing, Nelfinavir, Interleukin 15, Immunology/Immune Response, Interleukin 12, lcsh:Q, Research Article, medicine.drug
Abstract

Background HIV-1 Protease Inhibitors, namely PIs, originally designed to inhibit HIV-1 aspartic protease, can modulate the immune response by mechanisms largely unknown, and independent from their activity on viral replication. Here, we analyzed the ability of PIs to interfere with differentiation program of monocytes toward dendritic cell (DCs) lineage, a key process in the inflammatory response. Methodology/Principal Findings Monocytes from healthy donors were isolated and induced to differentiate in vitro in the presence or absence of saquinavir, ritonavir, nelfinavir, indinavir or amprenavir (sqv, rtv, nlfv, idv, apv, respectively). These drugs demonstrated a differential ability to sustain the generation of immature DCs (iDCs) with an altered phenotype, including low levels of CD1a, CD86, CD36 and CD209. DCs generated in the presence of rtv also failed to acquire the typical phenotype of mature DCs (mDCs), and secreted lower amounts of IL-12 and IL-15. Accordingly, these aberrant mDCs failed to support activation of autologous Natural Killer (NK) cells, and resulted highly susceptible to NK cell-mediated cytotoxicity. Conclusions/Significance Our findings uncover novel functional properties of PIs within the DC-NK cell cross-talk, unveiling the heterogeneous ability of members of this class drugs to drive the generation of atypical monocyte-derived DCs (MDDCs) showing an aberrant phenotype, a failure to respond appropriately to bacterial endotoxin, a weak ability to prime autologous NK cells, and a high susceptibility to NK cell killing. These unexpected properties might contribute to limit inflammation and viral spreading in HIV-1 infected patients under PIs treatment, and open novel therapeutical perspectives for this class drugs as immunomodulators in autoimmunity and cancer.

Published
2010

50. Protocol for differentiation of monocytes and macrophages from human induced pluripotent stem cells.

Author

Emmerich K, Calcaterra F, Tang X, Chen G, Pontarini E, Ciceri R, Yang D, Joseph B, Della Bella S, Varea I, Mavilio D, and Boehm M

Subjects
Humans, Cell Culture Techniques methods, Hematopoietic Stem Cells cytology, Cells, Cultured, Induced Pluripotent Stem Cells cytology, Monocytes cytology, Macrophages cytology, Cell Differentiation physiology
Abstract

Study of disease-relevant immune cells, namely monocytes and macrophages, is limited based on availability of primary tissue, a limitation that can be remedied using human induced pluripotent stem cell (hiPSC) technology. Here, we present a protocol for differentiation of monocytes and macrophages from hiPSCs. We describe steps for hiPSC maintenance, mesoderm lineage induction, hematopoietic progenitor cells (HPCs) commitment and expansion, and myeloid lineage induction. We then detail procedures for monocyte formation and functional macrophage formation and polarization. For complete details on the use and execution of this protocol, please refer to Chen et al. 1 ., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2024
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