Your search keyword '"Abrignani S"' showing total 12 results

1. Pulmonary Langerhans Cell Histiocytosis and Lymphangioleiomyomatosis Have Circulating Cells With Loss of Heterozygosity of the TSC2 Gene.

Author

Elia D, Torre O, Vasco C, Geginat J, Abrignani S, Bulgheroni E, Carelli E, Cassandro R, Pacheco-Rodriguez G, Steagall WK, Moss J, and Harari S

Subjects

Humans, Loss of Heterozygosity, Tuberous Sclerosis Complex 2 Protein genetics, Tumor Suppressor Proteins genetics, Histiocytosis, Langerhans-Cell genetics, Lung Diseases genetics, Lymphangioleiomyomatosis

Abstract

Background: Lymphangioleiomyomatosis (LAM) and pulmonary Langerhans cell histiocytosis (PLCH) are cystic lung diseases in which a neoplastic cell is thought to be responsible for disease pathogenesis. The neoplastic LAM cell has mutations in the TSC genes, TSC1 or TSC2, whereas the neoplastic PLCH cell may have mutations in several genes (eg, BRAF, NRAS, MAP2K1). These mutations are not specific for PLCH and have been described in multiple cancers. TSC1 or TSC2 mutations and loss of heterozygosity (LOH) have also been described in cancers., Research Question: Is TSC2 LOH specific to LAM or is it also found in PLCH?, Study Design and Methods: We recruited patients with LAM (n = 53) and healthy volunteers (n = 22) and compared the presence of cells with TSC2 LOH with patients with PLCH (n = 12). Blood and urine samples were collected for analysis. Fluorescence-activated cell sorting (FACS) was used to identify subpopulations of cells from blood and urine samples. We isolated CD45-CD235a-, CD45-CD235a+, and CD45+CD235a- cells from blood after density gradient separation. Cells were screened for TSC2 LOH at five microsatellites markers (ie, kg8, D16S3395, D16S3024, D16S521, D16S291). We obtained four cell subpopulations from urine (ie, CD44v6+CD9+, CD44v6+CD9-, CD44v6-CD9+, CD44v6-CD9-)., Results: Using FACS, cells were isolated from blood and urine from patients with PLCH that showed TSC2 LOH. Healthy volunteers did not have cells with TSC2 LOH. As a control, cells isolated from blood and urine from patients with LAM gave results similar to those reported previously. These data show that TSC2 LOH is found in patients with cystic lung diseases with potential neoplastic characteristics, and in patients with cancer., Interpretation: The presence of TSC2 LOH in circulating cells is not specific for LAM. The data suggest that chromosomal abnormalities affecting the TSC2 gene are found in other diseases associated with cells having cancer-like neoplastic cells., (Copyright © 2022. Published by Elsevier Inc.)

Published

2022

2. Why is it so difficult to develop a hepatitis C virus preventive vaccine?

Author

Zingaretti C, De Francesco R, and Abrignani S

Subjects

Animals, Antiviral Agents therapeutic use, Clinical Trials, Phase I as Topic, Clinical Trials, Phase II as Topic, Disease Models, Animal, Hepacivirus, Hepatitis C, Chronic drug therapy, Humans, Randomized Controlled Trials as Topic, Hepatitis C, Chronic prevention & control, Viral Hepatitis Vaccines therapeutic use

Abstract

With an estimated 3% of the world's population chronically infected, hepatitis C virus (HCV) represents a major health problem for which an efficient vaccination strategy would be highly desirable. Indeed, chronic hepatitis C is recognized as one of the major causes of cirrhosis, hepatocarcinoma and liver failure worldwide and it is the most common indication for liver transplantation, accounting for 40-50% of liver transplants. Much progress has been made in the prevention of HCV transmission and in therapeutic intervention. However, even if a new wave of directly acting antivirals promise to overcome the problems of low efficacy and adverse effects observed for the current standard of care, which include interferon-α and ribavirin, an effective vaccine would be the only means to definitively eradicate infection and to diminish the burden of HCV-related diseases at affordable costs. Although there is strong evidence that the goal of a prophylactic vaccine could be achieved, there are huge development issues that have impeded reaching this goal and that still have to be addressed. In this article we address the question of whether an HCV vaccine is needed, whether it will eventually be feasible, and why it is so difficult to produce.

Published

2014

3. Human CD1c+ dendritic cells secrete high levels of IL-12 and potently prime cytotoxic T-cell responses.

Author

Nizzoli G, Krietsch J, Weick A, Steinfelder S, Facciotti F, Gruarin P, Bianco A, Steckel B, Moro M, Crosti M, Romagnani C, Stölzel K, Torretta S, Pignataro L, Scheibenbogen C, Neddermann P, De Francesco R, Abrignani S, and Geginat J

Subjects

Animals, Antigen Presentation, CD4-Positive T-Lymphocytes cytology, CD8-Positive T-Lymphocytes cytology, Cell Proliferation, Cell Separation, Cytokines metabolism, Dendritic Cells metabolism, Humans, Immunologic Memory, Interferon-alpha metabolism, Interferon-gamma metabolism, Lymphocyte Activation, Mice, Phenotype, Toll-Like Receptors metabolism, Antigens, CD1 metabolism, Dendritic Cells cytology, Glycoproteins metabolism, Interleukin-12 metabolism, T-Lymphocytes, Cytotoxic cytology

Abstract

Dendritic cells (DC) have the unique capacities to induce primary T-cell responses. In mice, CD8α(+)DC are specialized to cross-prime CD8(+) T cells and produce interleukin-12 (IL-12) that promotes cytotoxicity. Human BDCA-3(+)DC share several relevant characteristics with CD8α(+)DC, but the capacities of human DC subsets to induce CD8(+) T-cell responses are incompletely understood. Here we compared CD1c(+) myeloid DC (mDC)1, BDCA-3(+)mDC2, and plasmacytoid DC (pDC) in peripheral blood and lymphoid tissues for phenotype, cytokine production, and their capacities to prime cytotoxic T cells. mDC1 were surprisingly the only human DC that secreted high amounts of IL-12p70, but they required combinational Toll-like receptor (TLR) stimulation. mDC2 and pDC produced interferon-λ and interferon-α, respectively. Importantly, mDC1 and mDC2 required different combinations of TLR ligands to cross-present protein antigens to CD8(+) T cells. pDC were inefficient and also expressed lower levels of major histocompatibility complex and co-stimulatory molecules. Nevertheless, all DC induced CD8(+) memory T-cell expansions upon licensing by CD4(+) T cells, and primed naive CD8(+) T cells following appropriate TLR stimulation. However, because mDC1 produced IL-12, they induced the highest levels of cytotoxic molecules. In conclusion, CD1c(+)mDC1 are the relevant source of IL-12 for naive T cells and are fully equipped to cross-prime cytotoxic T-cell responses.

Published

2013

4. A novel polyclonal antibody library for expression profiling of poorly characterized, membrane and secreted human proteins.

Author

Grifantini R, Pagani M, Pierleoni A, Grandi A, Parri M, Campagnoli S, Pileri P, Cattaneo D, Canidio E, Pontillo A, De Camilli E, Bresciani A, Marinoni F, Pedrazzoli E, Nogarotto R, Abrignani S, Viale G, Sarmientos P, and Grandi G

Subjects

Animals, Antibodies genetics, Breast Neoplasms chemistry, Escherichia coli metabolism, Female, Gene Library, Humans, Immunohistochemistry methods, Male, Membrane Proteins biosynthesis, Mice, Prostatic Neoplasms chemistry, Protein Array Analysis, Antibodies immunology, Biomarkers, Tumor analysis, Gene Expression Profiling methods, Membrane Proteins immunology, Peptide Library, Recombinant Proteins immunology

Abstract

The YOMICS™ antibody library (http://www.yomics.com/) presented in this article is a new collection of 1559 murine polyclonal antibodies specific for 1287 distinct human proteins. This antibody library is designed to target marginally characterized membrane-associated and secreted proteins. It was generated against human proteins annotated as transmembrane or secreted in GenBank, EnsEMBL, Vega and Uniprot databases, described in no or very few dedicated PubMed-linked publications. The selected proteins/protein regions were expressed in E. coli, purified and used to raise antibodies in the mouse. The capability of YOMICS™ antibodies to specifically recognize their target proteins either as recombinant form or as expressed in cells and tissues was confirmed through several experimental approaches, including Western blot, confocal microscopy and immunohistochemistry (IHC). Moreover, to show the applicability of the library for biomarker investigation by IHC, five antibodies against proteins either known to be expressed in some cancers or homologous to tumor-associated proteins were tested on tissue microarrays carrying tumor and normal tissues from breast, colon, lung, ovary and prostate. A consistent differential expression in cancer was observed. Our results indicate that the YOMICS™ antibody library is a tool for systematic protein expression profile analysis that nicely complements the already available commercial antibody collections., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published

2011

5. NKT-cell help to B lymphocytes can occur independently of cognate interaction.

Author

Tonti E, Galli G, Malzone C, Abrignani S, Casorati G, and Dellabona P

Subjects

Adjuvants, Immunologic pharmacology, Animals, Antibody Formation drug effects, Antigen Presentation drug effects, Antigen-Presenting Cells immunology, Antigens, CD1d genetics, Antigens, CD1d immunology, Bone Marrow Transplantation, CD40 Antigens genetics, CD40 Antigens immunology, Cell Communication drug effects, Cell Communication physiology, Galactosylceramides pharmacology, Histocompatibility Antigens Class II genetics, Histocompatibility Antigens Class II immunology, Immunity, Innate drug effects, Immunization, Mice, Mice, Knockout, T-Lymphocytes, Helper-Inducer immunology, Transplantation Chimera genetics, Transplantation Chimera immunology, Antibody Formation physiology, Antigen Presentation physiology, B-Lymphocytes immunology, Galactosylceramides immunology, Immunity, Innate physiology, Natural Killer T-Cells immunology

Abstract

CD4(+) T (Th)-cell help to B lymphocytes requires cognate interaction and CD40 engagement. Invariant natural killer T (iNKT) cells are innate-like T lymphocytes that recognize alphagalactosylceramide (alphaGalCer) presented by CD1d, and can help B-cell responses. We asked whether alphaGalCer-activated iNKT cells help B lymphocytes through cognate interaction, or indirectly, via enhancement of Th-B-cell interaction. After immunization with protein Ags and alphaGalCer, antibody titers were assessed in wild-type or splenectomized mice, and in bone marrow radiation chimeras lacking CD1d or CD40 expression on B lymphocytes, or expressing CD1d or MHC II disjointly on antigen-presenting cells (APCs). We find that alphaGalCer-dependent enhancement of B-cell response (1) can occur when B cells do not express CD1d but express CD40; (2) requires that iNKT and Th cells interact with the same APCs that coexpress both CD1d and MHC-II; and (3) takes place without spleen. These findings demonstrate alphaGalCer-induced help for antibody responses can occur without cognate iNKT/B-cell interaction, and suggest this help entails activation of APCs by iNKT cells, which in turn activate Th cells and their helper functions for B cells. Thus, the alphaGalCer-induced help recapitulates the function of classical adjuvants that stimulate the innate immune system to support adaptive immune responses.

Published

2009

6. Intracellular accumulation of hepatitis C virus proteins in a human hepatoma cell line.

Author

Brazzoli M, Crotta S, Bianchi A, Bagnoli F, Monaghan P, Wileman T, Abrignani S, and Merola M

Subjects

Base Sequence, Carcinoma, Hepatocellular virology, Cell Line, Tumor, DNA, Viral genetics, Endoplasmic Reticulum virology, Gene Expression, Genome, Viral, Hepacivirus genetics, Humans, Liver Neoplasms virology, Multiprotein Complexes, Replicon, Subcellular Fractions virology, Viral Envelope Proteins chemistry, Viral Envelope Proteins genetics, Viral Envelope Proteins metabolism, Viral Nonstructural Proteins chemistry, Viral Nonstructural Proteins genetics, Viral Nonstructural Proteins metabolism, Viral Proteins chemistry, Viral Proteins genetics, Virus Replication, Hepacivirus physiology, Viral Proteins metabolism

Abstract

Background/aims: The establishment of HCV replicon systems strongly improved the research on the replication processes but poorly advanced our knowledge on the subcellular localization of the structural glycoproteins, mainly due to their low expression. We sought to verify whether reinforcing E1E2 expression in the context of both HCV genomic and subgenomic replicon from either homologous or heterologous strains leads to formation of supramolecular structures including structural and nonstructural proteins., Methods: Robust expression of HCV glycoproteins was achieved by stable expression of E1E2p7 from genotype 1a and 1b., Results: In these cells, E1 and E2 triggered the formation of dot-like structures in which they co-localized with core and the nonstructural proteins NS3 and NS5A. Confocal microscopy analyses suggested that accumulation of HCV proteins occurs in an ER-derived subcompartment. Moreover, by labeling de novo-synthesized HCV RNA, we showed that these structures constitute a site of viral RNA synthesis., Conclusions: Expression in trans of HCV glycoproteins in the context of replicative viral genome or subgenome generates accumulation of structural and nonstructural viral proteins in peculiar cytoplasmic structures. The simultaneous presence of viral RNA, structural and nonstructural protein suggests that these complexes represent not only sites of HCV replication but also potential places of viral pre-budding.

Published

2007

7. Comparable functions of plasmacytoid and monocyte-derived dendritic cells in chronic hepatitis C patients and healthy donors.

Author

Piccioli D, Tavarini S, Nuti S, Colombatto P, Brunetto M, Bonino F, Ciccorossi P, Zorat F, Pozzato G, Comar C, Abrignani S, and Wack A

Subjects

Adult, Aged, Blood Donors, Female, Humans, Interferon-alpha biosynthesis, Lymphocyte Culture Test, Mixed, Male, Middle Aged, Monocytes cytology, Plasma Cells cytology, Tumor Necrosis Factor-alpha biosynthesis, Dendritic Cells physiology, Hepatitis C, Chronic immunology

Abstract

Background/aims: Dendritic cells (DCs) play a key role in immune responses through antigen presentation and cytokine secretion. Hepatitis C virus (HCV) is able to escape elimination by the immune system and often establishes a chronic infection. To investigate whether DC dysfunction is involved in this process, we have studied monoycte-derived DCs (Mo-DCs) and plasmacytoid DCs (pDCs), which produce large amounts of IFN-alpha, from chronic HCV patients and healthy donors., Methods: We have assessed TNF-alpha and IFN-alpha production by pDCs using intracellular staining after total PBMCs stimulation with unmethylated CG dinucleotides (CpGs). The induction of allogeneic T cell proliferation by immature Mo-DCs was measured using the MLR assay. The up-regulation of maturation markers and the production of TNF-alpha in response to LPS were analyzed using flow cytometry and ELISA, respectively., Results: We have detected comparable frequencies of pDCs producing TNF-alpha and IFN-alpha in both chronic HCV patients and healthy donors and we have found that immature Mo-DCs from both patients and donors similarly induce allogeneic T cell proliferation and mature and secrete TNF-alpha in response to LPS., Conclusions: Our results demonstrate that both pDC and Mo-DCs are not impaired in HCV infected patients.

Published

2005

8. Molecular analysis of V(H)I+ B lymphocytes in hepatitis C patients.

Author

Galli-Stampino L, Pasqualini A, Pozzato G, Bonino F, Filipponi F, Mosca M, Masciopinto F, Abrignani S, and Uematsu Y

Subjects

B-Lymphocytes immunology, Case-Control Studies, Clone Cells immunology, DNA Primers, Female, Humans, Immunoglobulin Heavy Chains immunology, Male, Middle Aged, Reverse Transcriptase Polymerase Chain Reaction, Sequence Analysis, RNA, B-Lymphocytes virology, Hepatitis C, Chronic genetics, Hepatitis C, Chronic immunology, Immunoglobulin Heavy Chains genetics

Abstract

Background and Aims: Hepatitis C virus infection is often associated with lymphoproliferative disorders such as essential mixed cryoglobulinemia and B-cell non-Hodgkin lymphoma, which show preferential expression of VHI family products. By analyzing immunoglobulin heavy chain usage, we addressed the question of whether or not clonal B-cell expansion occurrs in patients free of essential mixed cryoglobulinemia or non-Hodgkin lymphoma., Patients and Methods: Four hepatitis C virus-positive patients, all undergoing liver transplantation, were studied. Peripheral blood, intra-hepatic, and lymph node lymphocytes were used as a source of B cells. A patient with hepatocellular carcinoma and fresh blood from four healthy donors were used as negative controls. VHI family sequences were cloned and analyzed by reverse transcription-polymerase chain reaction., Results: Immunoglobulin heavy chain sequences from clonally expanded B lymphocytes were identified in three out of four hepatitis C virus-infected patients. The clonally expanded B lymphocyte populations showed a broad spectra of immunoglobulin heavy chain gene usage., Conclusions: HCV infection can induce B-cell expansion with larger clonal variation. The restricted V gene usage in hepatitis C virus-associated non-Hodgkin lymphoma suggests that there may be selection mechanisms to develop non-Hodgkin lymphoma from non-malignant, clonally expanded B-cell populations in hepatitis C virus-infected patients.

Published

2003

9. Perspectives for a vaccine against hepatitis C virus.

Author

Abrignani S, Houghton M, and Hsu HH

Subjects

Animals, DNA, Disease Models, Animal, Hepatitis C immunology, Humans, Hepatitis C prevention & control, Viral Hepatitis Vaccines immunology

Abstract

There is no vaccine for HCV and the only available treatment, IFNalpha alone or in combination with ribavirin, has proven efficacious in less than 50% of patients. Given that approximately 200 million chronic HCV infections have been estimated worldwide, there is a pressing need to develop vaccination strategies aimed at preventing and possibly eradicating HCV infection. However, several major practical and scientific problems arise in designing an HCV vaccine. First, HCV is only readily detected as RNA by PCR. Second, the only species that can be infected by HCV are humans and chimpanzees. Third, the virus does not replicate efficiently in vitro. Fourth, some viral proteins have very high mutability. Last, there is little information on correlates of immunity. Although an ideal vaccine should protect from infection, in that it should elicit sterilizing immunity, this is quite an ambitious goal in the PCR era. In the case of HCV, where acute HCV infection is a very limited health problem and infection can only be assessed by PCR, a more realistic goal might be to look for vaccines capable of protecting from chronic infection. We have preliminary evidence in chimpanzees that an HCV vaccine consisting of recombinant envelope proteins can elicit antibodies and inflammatory CD4+ T cell responses which can prevent chronic infection in the majority of vaccinees. Although the scientific and clinical challenges that need to be addressed are still substantial, advances in recombinant protein technology, novel adjuvants, and DNA vaccines, will be key in developing strategies to generate protective immunity against chronic HCV infection.

Published

1999

10. Role of macrophages in bypassing the inhibitory activity of Newcastle disease virus on the T-suppressor-cell circuit which regulates contact sensitivity to picryl chloride.

Author

Dieli F, Abrignani S, Lio D, and Salerno A

Subjects

Animals, Immunization, Passive, Mice, Newcastle Disease immunology, Picryl Chloride, Spleen immunology, Suppressor Factors, Immunologic physiology, Dermatitis, Contact immunology, Immune Tolerance, Macrophages physiology, Newcastle disease virus immunology, T-Lymphocytes immunology, T-Lymphocytes, Regulatory immunology

Abstract

The interaction between the paramyxovirus of Newcastle disease virus (NDV) and the T-suppressor-cell circuit which regulates the expression phase of contact sensitivity reaction to picryl chloride was investigated. NDV infection impairs the T-acceptor-cell (Tacc) activity, as demonstrated by the failure of Tacc from mice infected with NDV both on Day 0 and on Day 3 to release the nonspecific inhibitor of the passive transfer of contact sensitivity. Tacc from NDV-infected mice fail to bind appreciable amounts of exogenous T suppressor factor, so indicating that the virus eliminates this T-cell population. However, macrophages from mice infected with NDV are able to release a nonspecific inhibitor of the passive transfer of contact sensitivity, indicating that the inhibition of Tacc activity in mice infected with NDV is bypassed by macrophages, so that the T-suppressor circuit is functionally active in NDV-infected mice. The mechanism of the selective inhibition of the Tacc activity by NDV is discussed.

Published

1988

11. Infection of mice with Newcastle disease virus inhibits the T suppressor afferent cell circuit which regulates contact sensitivity to picryl chloride.

Author

Dieli F, Colonna Romano G, Abrignani S, Colizzi V, and Salerno A

Subjects

Animals, DNA biosynthesis, Mice, Picryl Chloride immunology, Dermatitis, Contact immunology, Newcastle Disease immunology, Newcastle disease virus immunology, T-Lymphocytes, Regulatory immunology

Abstract

The interaction between Newcastle disease virus (NDV) and the suppressor cell circuit which regulates the induction phase of contact sensitivity reaction to picryl chloride (Pcl) was investigated. NDV infection impairs the activity of the T suppressor afferent cells (Ts-aff) which inhibit DNA synthesis in the draining lymph nodes of mice specifically sensitized with Pcl and the development of contact sensitivity. The inhibitory effect of NDV was evident when the virus was administered up to 2 days before or at the same time as the injection of picrylsulfonic acid; this effect required infectious virus, as NDV inactivated by ultraviolet irradiation failed to inhibit Ts-aff activity. Taken together with the previous finding that the T suppressor efferent cell is unaffected by NDV, the present results support the view that contact sensitivity reaction to picryl chloride is regulated by two distinct T-suppressor-cell circuits.

Published

1985

12. Complement activation by cell-associated immune complexes in contact sensitivity.

Author

Salerno A, Brai M, Dieli F, Colonna Romano G, Abrignani S, Colizzi V, and Asherson GL

Subjects

Animals, Lymph Nodes immunology, Male, Mice, Mice, Inbred CBA, Mice, Inbred Strains, Oxazolone, Picryl Chloride, Antigen-Antibody Complex immunology, Complement Activation, Complement Pathway, Classical, Dermatitis, Contact immunology, Immunity, Cellular, Lymphocytes immunology

Abstract

Lymph node cells collected 4 days after painting the skin with picryl chloride activate the first components of the classical pathway of complement cascade, as shown by consumption of C4 of rabbit complement with total sparing of C5 and factor B activity. In contrast, lymph node cells collected 1 or 6 days after sensitization fail to do so. The ability of "4-day" cells to activate complement is inhibited by treating the cells with specific low-molecular-weight hapten, which is known to dissociate the immune complex present on the cell surface. When mouse serum was used as source of complement, a different behavior in complement activation between CBA/J and B10.D2-New/SnJ serum was observed: "4-day" cells failed to consume CBA/J serum whereas a normal complement activation was detected when B10.D2-New/SnJ serum was used. Using these two sera which differ in the level of C4, an inverse relationship between the ability of "4-day" cells to activate complement and their capacity to induce contact sensitivity when injected into the footpad of normal recipients was reported. Experiments performed using sera from C5 genetically deficient mice demonstrate that only the early complement components are involved, suggesting that membrane immune complexes are solubilized as a result of complement activation; on the other hand, membrane bound activated complement components could alter the immunizing potential of "4-day" cells.

Published

1984