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1. Immunoregulatory molecule expression on extracellular microvesicles in people living with HIV

Author

Neyrinck-Leglantier, Deborah, primary, Tamagne, Marie, additional, Ben Rayana, Raida, additional, Many, Souganya, additional, Vingert, Paul, additional, LeGagneux, Julie, additional, Delorme, Adèle Silane, additional, Andrieu, Muriel, additional, Boilard, Eric, additional, Cognasse, Fabrice, additional, Hamzeh-Cognasse, Hind, additional, Perez-Patrigeon, Santiago, additional, Lelievre, Jean-Daniel, additional, Pirenne, France, additional, Gallien, Sébastien, additional, and Vingert, Benoît, additional

Published
2024
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3. Immune interactions and regulation with CD39+ extracellular vesicles from platelet concentrates.

Author

Delorme, Adèle Silane, Laguide, Alexandra, Tamagne, Marie, Pinheiro, Marion Klea, Cagnet, Léonie, Neyrinck-Leglantier, Deborah, Khelfa, Mehdi, Cleophax, Sabine, Pirenne, France, and Vingert, Benoît

Subjects
EXTRACELLULAR vesicles, BLOOD platelets, B cells, BLOOD platelet transfusion, T cells
Abstract

Introduction: CD39 plays an important role in the immunoregulation and inhibition of effector cells. It is expressed on immune cells, including Tregs, and on extracellular vesicles (EVs) budding from the plasma membrane. Platelet transfusion may induce alloimmunization against HLA-I antigens, leading to refractoriness to platelet transfusion with severe consequences for patients. Tregs may play a key role in determining whether alloimmunization occurs in patients with hematologic disorders. We hypothesized that CD39+ EVs might play an immunoregulatory role, particularly in the context of platelet transfusions in patients with hematologic disorders. Such alloimmunization leads to the production of alloantibodies and is sensitive to the regulatory action of CD39. Methods: We characterized CD39+ EVs in platelet concentrates by flow cytometry. The absolute numbers and cellular origins of CD39+ EVs were evaluated. We also performed functional tests to evaluate interactions with immune cells and their functions. Results: We found that CD39+ EVs from platelet concentrates had an inhibitory phenotype that could be transferred to the immune cells with which they interacted: CD4+ and CD8+ T lymphocytes (TLs), dendritic cells, monocytes, and B lymphocytes (BLs). Moreover, the concentration of CD39+ EVs in platelet concentrates varied and was very high in 10% of concentrates. The number of these EVs present was determinant for EV-cell interactions. Finally, functional interactions were observed with BLs, CD4+ TLs and CD39+ EVs for immunoglobulin production and lymphoproliferation, with potential implications for the immunological management of patients. [ABSTRACT FROM AUTHOR]

Published
2024
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4. Divergent CD4+ T-cell profiles are associated with anti-HLA alloimmunization status in platelet-transfused AML patients

Author

Khelfa, Mehdi, primary, Leclerc, Mathieu, additional, Kerbrat, Stéphane, additional, Boudjemai, Yakout Nait Sidenas, additional, Benchouaia, Médine, additional, Neyrinck-Leglantier, Déborah, additional, Cagnet, Léonie, additional, Berradhia, Lylia, additional, Tamagne, Marie, additional, Croisille, Laure, additional, Pirenne, France, additional, Maury, Sébastien, additional, and Vingert, Benoît, additional

Published
2023
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6. Divergent CD4+ T-cell profiles are associated with anti-HLA alloimmunization status in platelet-transfused AML patients.

Author

Khelfa, Mehdi, Leclerc, Mathieu, Kerbrat, Stéphane, Sidenas Boudjemai, Yakout Nait, Benchouaia, Médine, Neyrinck-Leglantier, Déborah, Cagnet, Léonie, Berradhia, Lylia, Tamagne, Marie, Croisille, Laure, Pirenne, France, Maury, Sébastien, and Vingert, Benoît

Subjects
ACUTE myeloid leukemia, T cells, BLOOD platelet transfusion, HUMORAL immunity
Abstract

Introduction: Acute myeloid leukemia (AML) is one of the commonest hematologic disorders. Due to the high frequency of disease- or treatment-related thrombocytopenia, AML requires treatment with multiple platelet transfusions, which can trigger a humoral response directed against platelets. Some, but not all, AML patients develop an anti-HLA immune response after multiple transfusions. We therefore hypothesized that different immune activation profiles might be associated with anti-HLA alloimmunization status. Methods: We tested this hypothesis, by analyzing CD4+ T lymphocyte (TL) subsets and their immune control molecules in flow cytometry and single-cell multi-omics. Results: A comparison of immunological status between anti-HLA alloimmunized and non-alloimmunized AML patients identified differences in the phenotype and function of CD4+ TLs. CD4+ TLs from alloimmunized patients displayed features of immune activation, with higher levels of CD40 and OX40 than the cells of healthy donors. However, the most notable differences were observed in non-alloimmunized patients. These patients had lower levels of CD40 and OX40 than alloimmunized patients and higher levels of PD1. Moreover, the Treg compartment of non-alloimmunized patients was larger and more functional than that in alloimmunized patients. These results were supported by a multi-omics analysis of immune response molecules in conventional CD4+ TLs, Tfh circulating cells, and Tregs. Discussion: Our results thus reveal divergent CD4+ TL characteristics correlated with anti-HLA alloimmunization status in transfused AML patients. These differences, characterizing CD4+ TLs independently of any specific antigen, should be taken into account when considering the immune responses of patients to infections, vaccinations, or transplantations. [ABSTRACT FROM AUTHOR]

Published
2023
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9. Platelet EVs contain an active proteasome involved in protein processing for antigen presentation via MHC-I molecules

Author

Marcoux, Genevieve, primary, Laroche, Audrée, additional, Hasse, Stephan, additional, Bellio, Marie, additional, Mbarik, Maroua, additional, Tamagne, Marie, additional, Allaeys, Isabelle, additional, Zufferey, Anne, additional, Lévesque, Tania, additional, Rebetz, Johan, additional, Karakeussian-Rimbaud, Annie, additional, Turgeon, Julie, additional, Bourgoin, Sylvain G., additional, Hamzeh-Cognasse, Hind, additional, Cognasse, Fabrice, additional, Kapur, Rick, additional, Semple, John W., additional, Hébert, Marie-Josée, additional, Pirenne, France, additional, Overkleeft, Herman S., additional, Florea, Bogdan I., additional, Dieude, Mélanie, additional, Vingert, Benoît, additional, and Boilard, Eric, additional

Published
2021
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10. Autologous blood extracellular vesicles and specific CD4+ T-cell co-activation.

Author

Neyrinck-Leglantier, Déborah, Tamagne, Marie, L'honoré, Sasha, Cagnet, Léonie, Pakdaman, Sadaf, Marchand, Alexandre, Pirenne, France, and Vingert, Benoît

Subjects
EXTRACELLULAR vesicles, T cells, COMMUNICABLE diseases, IMMUNE system
Abstract

Extracellular vesicles (EVs), which are generated by cell membrane budding in diverse cells, are present in variable numbers in the blood. An immunoregulatory role has been demonstrated principally for heterologous EVs, but the function of the EVs present naturally in blood remains unknown. We hypothesize that these autologous EVs might also modulate the phenotype and function of immune system cells, especially CD4+ T lymphocytes (TLs), as previously described for heterologous EVs. Several membranes and soluble immunoregulatory molecules were studied after the treatment of CD4+ TLs with autologous EVs. No direct activation was detected with autologous EVs, contrasting with the findings for heterologous EVs. However, following treatment with autologous EVs, a soluble form of CD27 (sCD27) was detected. sCD27 is strongly associated with lymphoproliferation. Autologous EVs have been shown to increase TL proliferation only after T-cell receptor (TcR) engagement due to polyclonal or specific-antigen stimulation. Our results therefore suggest that the EVs present in the blood have an immunomodulatory role different from that of heterologous EVs. These findings should be taken into account in future studies, particularly those focusing on infectious diseases, autotransfusion or doping practices. [ABSTRACT FROM AUTHOR]

Published
2022
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13. Fetal Hemoglobin Measurement per Red Blood Cell Provides Biological and Clinical Protective Thresholds

Author

Hebert, Nicolas, primary, Marie Georgine, Rakotoson, additional, Bodivit, Gwellaouen, additional, Audureau, Etienne, additional, Oubaya, Nadia, additional, Pakdaman, Sadaf, additional, Sakka, Mehdi, additional, Di Liberto, Gaetana, additional, Chadebech, Philippe, additional, Vingert, Benoît, additional, Pirenne, France, additional, Galactéros, Frédéric, additional, Cambot, Marie, additional, and Bartolucci, Pablo, additional

Published
2019
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14. CD4 responses in HIV controllers

Author

Potter, Simon J, Lacabaratz, Christine, Lambotte, Olivier, Perez-Patrigeon, Santiago, Vingert, Benoît, Sinet, Martine, Colle, Jean-Hervé, Urrutia, Alejandra, Scott-Algara, Daniel, Boufassa, Faroudy, Delfraissy, Jean-François, Thèze, Jacques, Venet, Alain, Chakrabarti, Lisa A, Immunogénétique Cellulaire, Institut Pasteur [Paris], Immunologie antivirale systémique et cérébrale, Université Paris-Sud - Paris 11 (UP11)-IFR93-Institut National de la Santé et de la Recherche Médicale (INSERM), Service de médecine interne et maladies infectieuses, Université Paris-Sud - Paris 11 (UP11)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpital Bicêtre, Régulation des Infections Rétrovirales, Santé reproductive, sexualité, infection à VIH - épidémiologie, démographie, sciences sociales, Institut national d'études démographiques (INED)-Université Paris-Sud - Paris 11 (UP11)-Institut National de la Santé et de la Recherche Médicale (INSERM), and Institut Pasteur [Paris] (IP)

Subjects
CD4+ T cell, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, HIV, HIV controllers, central memory
Abstract

International audience; Human immunodeficiency virus (HIV) controllers are rare individuals who spontaneously control HIV type 1 replication for 10 years or more in the absence of antiretroviral treatment. In the present study, HIV controllers (n = 11) maintained potent HIV-specific CD4 responses in spite of very low antigenic loads. Their CD4(+) central memory T (T(CM)) cells were characterized by near-normal numbers and preserved interleukin-2 (IL-2) secretion in response to HIV antigens and uniformly high expression of the survival receptor IL-7 receptor alpha (IL-7Ralpha). Controllers expressed CCR7 at higher levels than uninfected controls, suggesting differences in T(CM)-cell homing patterns. CD4(+) effector memory T (T(EM))-cell responses were polyfunctional in HIV controllers, while IL-2 secretion was lost in viremic patients. Cytokine production was three times higher in controllers than in treated patients with undetectable viral loads, suggesting an intrinsically more efficient response in the former group. The total CD4(+) T(EM)-cell pool underwent immune activation in controllers, as indicated by increased HLA-DR expression, decreased IL-7Ralpha expression, a bias towards gamma interferon production upon polyclonal stimulation, and increased macrophage inflammatory protein 1beta secretion associated with chronic CCR5 down-regulation. Thus, HIV controllers showed a preserved CD4(+) T(CM)-cell compartment and signs of potent functional activation in the CD4(+) T(EM)-cell compartment. While controllers did not show the generalized immune activation pattern associated with disease progression, they had signs of immune activation restricted to the effector compartment. These findings suggest the induction of an efficient, nondetrimental type of immune activation in patients who spontaneously control HIV.

Published
2007

16. HIV Controllers Maintain a Population of Highly Efficient Th1 Effector Cells in Contrast to Patients Treated in the Long Term

Author

Vingert, Benoît, primary, Benati, Daniela, additional, Lambotte, Olivier, additional, de Truchis, Pierre, additional, Slama, Laurence, additional, Jeannin, Patricia, additional, Galperin, Moran, additional, Perez-Patrigeon, Santiago, additional, Boufassa, Faroudy, additional, Kwok, William W., additional, Lemaître, Fabrice, additional, Delfraissy, Jean-François, additional, Thèze, Jacques, additional, and Chakrabarti, Lisa A., additional

Published
2012
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17. Preserved Central Memory and Activated Effector Memory CD4 + T-Cell Subsets in Human Immunodeficiency Virus Controllers: an ANRS EP36 Study

Author

Potter, Simon J., primary, Lacabaratz, Christine, additional, Lambotte, Olivier, additional, Perez-Patrigeon, Santiago, additional, Vingert, Benoît, additional, Sinet, Martine, additional, Colle, Jean-Hervé, additional, Urrutia, Alejandra, additional, Scott-Algara, Daniel, additional, Boufassa, Faroudy, additional, Delfraissy, Jean-François, additional, Thèze, Jacques, additional, Venet, Alain, additional, and Chakrabarti, Lisa A., additional

Published
2007
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19. HIV Controller CD4+ T Cells Respond to Minimal Amounts of Gag Antigen Due to High TCR Avidity.

Author

Vingert, Benoît, Perez-Patrigeon, Santiago, Jeannin, Patricia, Lambotte, Olivier, Boufassa, Faroudy, Lemaître, Fabrice, Kwok, William W., Theodorou, Ioannis, Delfraissy, Jean-François, Thèze, Jacques, and Chakrabarti, Lisa A.

Subjects
*IMMUNE response, *CELL proliferation, *ANTIGEN presenting cells, *ANTIRETROVIRAL agents, *PEPTIDE synthesis, *T cells
Abstract

HIV controllers are rare individuals who spontaneously control HIV replication in the absence of antiretroviral treatment. Emerging evidence indicates that HIV control is mediated through very active cellular immune responses, though how such responses can persist over time without immune exhaustion is not yet understood. To investigate the nature of memory CD4+ T cells responsible for long-term anti-HIV responses, we characterized the growth kinetics, Vβ repertoire, and avidity for antigen of patient-derived primary CD4+ T cell lines. Specific cell lines were obtained at a high rate for both HIV controllers (16/17) and efficiently treated patients (19/20) in response to the immunodominant Gag293 peptide. However, lines from controllers showed faster growth kinetics than those of treated patients. After normalizing for growth rates, IFN-γ responses directed against the immunodominant Gag293 peptide showed higher functional avidity in HIV controllers, indicating differentiation into highly efficient effector cells. In contrast, responses to Gag161, Gag263, or CMV peptides did not differ between groups. Gag293-specific CD4+ T cells were characterized by a diverse Vβ repertoire, suggesting that multiple clones contributed to the high avidity CD4+ T cell population in controllers. The high functional avidity of the Gag293-specific response could be explained by a high avidity interaction between the TCR and the peptide-MHC complex, as demonstrated by MHC class II tetramer binding. Thus, HIV controllers harbor a pool of memory CD4+ T cells with the intrinsic ability to recognize minimal amounts of Gag antigen, which may explain how they maintain an active antiviral response in the face of very low viremia. [ABSTRACT FROM AUTHOR]

Published
2010
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20. Preserved Central Memory and Activated Effector Memory CD4+ T-Cell Subsets in Human Immunodeficiency Virus Controllers: an ANRS EP36 Study.

Author

Potter, Simon J., Lacabaratz, Christine, Lambotte, Olivier, Perez-Patrigeon, Santiago, Vingert, Benoît, Sinet, Martine, Colle, Jean-Hervé, Urrutia, Alejandra, Scott-Algara, Daniel, Boufassa, Faroudy, Delfraissy, Jean-François, Thèze, Jacques, Venet, Alain, and Chakrabarti, Lisa A.

Subjects
*HIV, *VIRAL replication, *ANTIRETROVIRAL agents, *CD4 antigen, *T cells, *CYTOKINES
Abstract

Human immunodeficiency virus (HIV) controllers are rare individuals who spontaneously control HIV type 1 replication for 10 years or more in the absence of antiretroviral treatment. In the present study, HIV controllers (n = 11) maintained potent HIV-specific CD4 responses in spite of very low antigenic loads. Their CD4+ central memory T (TCM) cells were characterized by near-normal numbers and preserved interleukin-2 (IL-2) secretion in response to HIV antigens and uniformly high expression of the survival receptor IL-7 receptor α (IL-7R α ). Controllers expressed CCR7 at higher levels than uninfected controls, suggesting differences in TCM-cell homing patterns. CD4+ effector memory T (TEM)-cell responses were polyfunctional in HIV controllers, while IL-2 secretion was lost in viremic patients. Cytokine production was three times higher in controllers than in treated patients with undetectable viral loads, suggesting an intrinsically more efficient response in the former group. The total CD4+ TEM-cell pool underwent immune activation in controllers, as indicated by increased HLA-DR expression, decreased IL-7R α expression, a bias towards gamma interferon production upon polyclonal stimulation, and increased macrophage inflammatory protein 1β secretion associated with chronic CCR5 down-regulation. Thus, HIV controllers showed a preserved CD4+ TCM-cell compartment and signs of potent functional activation in the CD4+ TEM-cell compartment. While controllers did not show the generalized immune activation pattern associated with disease progression, they had signs of immune activation restricted to the effector compartment. These findings suggest the induction of an efficient, nondetrimental type of immune activation in patients who spontaneously control HIV. [ABSTRACT FROM AUTHOR]

Published
2007
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21. Immune interactions and regulation with CD39 + extracellular vesicles from platelet concentrates.

Author

Delorme AS, Laguide A, Tamagne M, Pinheiro MK, Cagnet L, Neyrinck-Leglantier D, Khelfa M, Cleophax S, Pirenne F, and Vingert B

Subjects
Humans, Cell Communication immunology, Platelet Transfusion, Female, B-Lymphocytes immunology, B-Lymphocytes metabolism, Male, Apyrase metabolism, Apyrase immunology, T-Lymphocytes, Regulatory immunology, T-Lymphocytes, Regulatory metabolism, Antigens, CD, Extracellular Vesicles immunology, Extracellular Vesicles metabolism, Blood Platelets immunology, Blood Platelets metabolism, Tetraspanin 29 metabolism
Abstract

Introduction: CD39 plays an important role in the immunoregulation and inhibition of effector cells. It is expressed on immune cells, including Tregs, and on extracellular vesicles (EVs) budding from the plasma membrane. Platelet transfusion may induce alloimmunization against HLA-I antigens, leading to refractoriness to platelet transfusion with severe consequences for patients. Tregs may play a key role in determining whether alloimmunization occurs in patients with hematologic disorders. We hypothesized that CD39 + EVs might play an immunoregulatory role, particularly in the context of platelet transfusions in patients with hematologic disorders. Such alloimmunization leads to the production of alloantibodies and is sensitive to the regulatory action of CD39., Methods: We characterized CD39 + EVs in platelet concentrates by flow cytometry. The absolute numbers and cellular origins of CD39 + EVs were evaluated. We also performed functional tests to evaluate interactions with immune cells and their functions., Results: We found that CD39 + EVs from platelet concentrates had an inhibitory phenotype that could be transferred to the immune cells with which they interacted: CD4 + and CD8 + T lymphocytes (TLs), dendritic cells, monocytes, and B lymphocytes (BLs). Moreover, the concentration of CD39 + EVs in platelet concentrates varied and was very high in 10% of concentrates. The number of these EVs present was determinant for EV-cell interactions. Finally, functional interactions were observed with BLs, CD4 + TLs and CD39 + EVs for immunoglobulin production and lymphoproliferation, with potential implications for the immunological management of patients., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 Delorme, Laguide, Tamagne, Pinheiro, Cagnet, Neyrinck-Leglantier, Khelfa, Cleophax, Pirenne and Vingert.)

Published
2024
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22. Divergent CD4 + T-cell profiles are associated with anti-HLA alloimmunization status in platelet-transfused AML patients.

Author

Khelfa M, Leclerc M, Kerbrat S, Boudjemai YNS, Benchouaia M, Neyrinck-Leglantier D, Cagnet L, Berradhia L, Tamagne M, Croisille L, Pirenne F, Maury S, and Vingert B

Subjects
Humans, Blood Platelets, T-Lymphocytes, Helper-Inducer, CD4-Positive T-Lymphocytes, CD40 Antigens, Thrombocytopenia, Anemia, Hemolytic, Autoimmune, Leukemia, Myeloid, Acute therapy
Abstract

Introduction: Acute myeloid leukemia (AML) is one of the commonest hematologic disorders. Due to the high frequency of disease- or treatment-related thrombocytopenia, AML requires treatment with multiple platelet transfusions, which can trigger a humoral response directed against platelets. Some, but not all, AML patients develop an anti-HLA immune response after multiple transfusions. We therefore hypothesized that different immune activation profiles might be associated with anti-HLA alloimmunization status., Methods: We tested this hypothesis, by analyzing CD4+ T lymphocyte (TL) subsets and their immune control molecules in flow cytometry and single-cell multi-omics., Results: A comparison of immunological status between anti-HLA alloimmunized and non-alloimmunized AML patients identified differences in the phenotype and function of CD4+ TLs. CD4+ TLs from alloimmunized patients displayed features of immune activation, with higher levels of CD40 and OX40 than the cells of healthy donors. However, the most notable differences were observed in non-alloimmunized patients. These patients had lower levels of CD40 and OX40 than alloimmunized patients and higher levels of PD1. Moreover, the Treg compartment of non-alloimmunized patients was larger and more functional than that in alloimmunized patients. These results were supported by a multi-omics analysis of immune response molecules in conventional CD4+ TLs, Tfh circulating cells, and Tregs., Discussion: Our results thus reveal divergent CD4+ TL characteristics correlated with anti-HLA alloimmunization status in transfused AML patients. These differences, characterizing CD4+ TLs independently of any specific antigen, should be taken into account when considering the immune responses of patients to infections, vaccinations, or transplantations., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Khelfa, Leclerc, Kerbrat, Boudjemai, Benchouaia, Neyrinck-Leglantier, Cagnet, Berradhia, Tamagne, Croisille, Pirenne, Maury and Vingert.)

Published
2023
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23. CD27 + microparticle interactions and immunoregulation of CD4 + T lymphocytes.

Author

Cagnet L, Neyrinck-Leglantier D, Tamagne M, Berradhia L, Khelfa M, Cleophax S, Pirenne F, and Vingert B

Subjects
Lymphocyte Activation, Phenotype, CD4-Positive T-Lymphocytes, T-Lymphocytes, Cytokines metabolism
Abstract

Introduction: Aplasia and hematological malignancies are treated with platelet transfusions, which can have major immunomodulatory effects. Platelet concentrates (PCs) contain many immunomodulatory elements, including the platelets themselves, residual leukocytes, extracellular vesicles, such as microparticles (MPs), cytokines and other soluble elements. Two of these components, MPs and a soluble form of CD27 (sCD27), have been shown to play a particularly important role in immune system modulation. The loss of CD27 expression is an irreversible marker of terminal effector CD3 + T-lymphocyte (TL) differentiation, and the CD27 + MPs present in PCs may maintain CD27 expression on the surface of TLs, and, thus, the activation of these cells., Methods: In this study, we phenotyped the CD27-expressing MPs present in PCs by microscale flow cytometry and investigated the interaction of these particles with CD4 + TLs. We cocultured MPs and PBMCs and determined the origin of the CD27 expressed on the surface of CD4 + TLs with the aid of two fluorochromes (BV510 for CD27 originating from MPs and BV786 for cellular CD27)., Results: We showed that the binding of CD27- expressing MPs involved the CD70 molecule, which was also present on these MPs. Finally, the maintenance of CD27 expression on the surface of TLs by sorted CD27 + MPs led to activation levels lower than those observed with other types of MPs., Discussion: These results for CD27-expressing MPs and their CD70-mediated targeting open up new possibilities for immunotherapy based on the use of MPs to maintain a phenotype or to target immune cells, for example. Moreover, decreasing the levels of CD27-expressing MPs in transfused platelets might also increase the chances of success for anti-CD27 monoclonal immunotherapy., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Cagnet, Neyrinck-Leglantier, Tamagne, Berradhia, Khelfa, Cleophax, Pirenne and Vingert.)

Published
2023
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24. Autologous blood extracellular vesicles and specific CD4 + T-cell co-activation.

Author

Neyrinck-Leglantier D, Tamagne M, L'honoré S, Cagnet L, Pakdaman S, Marchand A, Pirenne F, and Vingert B

Subjects
CD4-Positive T-Lymphocytes, Immunomodulation, Lymphocyte Activation, T-Lymphocytes, Extracellular Vesicles metabolism
Abstract

Extracellular vesicles (EVs), which are generated by cell membrane budding in diverse cells, are present in variable numbers in the blood. An immunoregulatory role has been demonstrated principally for heterologous EVs, but the function of the EVs present naturally in blood remains unknown. We hypothesize that these autologous EVs might also modulate the phenotype and function of immune system cells, especially CD4 + T lymphocytes (TLs), as previously described for heterologous EVs. Several membranes and soluble immunoregulatory molecules were studied after the treatment of CD4 + TLs with autologous EVs. No direct activation was detected with autologous EVs, contrasting with the findings for heterologous EVs. However, following treatment with autologous EVs, a soluble form of CD27 (sCD27) was detected. sCD27 is strongly associated with lymphoproliferation. Autologous EVs have been shown to increase TL proliferation only after T-cell receptor (TcR) engagement due to polyclonal or specific-antigen stimulation. Our results therefore suggest that the EVs present in the blood have an immunomodulatory role different from that of heterologous EVs. These findings should be taken into account in future studies, particularly those focusing on infectious diseases, autotransfusion or doping practices., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Neyrinck-Leglantier, Tamagne, L’honoré, Cagnet, Pakdaman, Marchand, Pirenne and Vingert.)

Published
2022
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25. Red blood cell alloimmunization is influenced by the delay between Toll-like receptor agonist injection and transfusion.

Author

Elayeb R, Tamagne M, Bierling P, Noizat-Pirenne F, and Vingert B

Subjects
Animals, Antibodies metabolism, Antigen Presentation, Antigens, CD genetics, Antigens, CD immunology, CD4-Positive T-Lymphocytes cytology, CD4-Positive T-Lymphocytes drug effects, Dendritic Cells cytology, Dendritic Cells drug effects, Erythrocyte Transfusion, Erythrocytes chemistry, Erythrocytes drug effects, Gene Expression, Humans, Immunity, Humoral, Interleukin-12 immunology, Interleukin-12 metabolism, Mice, Mice, Transgenic, Muramidase administration & dosage, Muramidase genetics, Peptides administration & dosage, Peptides genetics, Peptides immunology, Poly I-C pharmacology, Spleen immunology, Time Factors, Toll-Like Receptor 3 genetics, Toll-Like Receptor 3 immunology, Transgenes, CD4-Positive T-Lymphocytes immunology, Dendritic Cells immunology, Erythrocytes immunology, Immunization, Muramidase immunology, Toll-Like Receptor 3 agonists
Abstract

Murine models of red blood cell transfusion show that inflammation associated with viruses or methylated DNA promotes red blood cell alloimmunization. In vaccination studies, the intensity of antigen-specific responses depends on the delay between antigen and adjuvant administration, with a short delay limiting immune responses. In mouse models of alloimmunization, the delay between the injection of Toll-like receptor agonists and transfusion is usually short. In this study, we hypothesized that the timing of Toll-like receptor 3 agonist administration affects red blood cell alloimmunization. Poly(I:C), a Toll-like receptor 3 agonist, was administered to B10BR mice at various time points before the transfusion of HEL-expressing red blood cells. For each time point, we measured the activation of splenic HEL-presenting dendritic cells, HEL-specific CD4(+) T cells and anti-HEL antibodies in serum. The phenotype of activated immune cells depended on the delay between transfusion and Toll-like receptor-dependent inflammation. The production of anti-HEL antibodies was highest when transfusion occurred 7 days after agonist injection. The proportion of HEL-presenting CD8α(+) dendritic cells producing interleukin-12 was highest in mice injected with poly(I:C) 3 days before transfusion. Although the number of early-induced HEL-specific CD4(+) T cells was similar between groups, a high proportion of these cells expressed CD134, CD40 and CD44 in mice injected with poly(I:C) 7 days before transfusion. This study clearly shows that the delay between transfusion and Toll-like receptor-induced inflammation influences the immune response to transfused red blood cells., (Copyright© Ferrata Storti Foundation.)

Published
2016
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26. [Role of CD4 lymphocytes in the efficient immune response of HIV controllers].

Author

Thèze J, Chakrabarti L, Vingert B, Lambotte O, and Delfraissy JF

Subjects
HIV Long-Term Survivors, Humans, Viral Load, CD4-Positive T-Lymphocytes immunology, HIV Infections immunology, HIV Infections virology
Abstract

More than 30 million people are infected by HIV worldwide. The rate of progression to AIDS is variable. A newly identified category of patients, so-called HIV controllers, spontaneously control HIV replication for long periods. HIV controllers are defined as infected patients whose viral load remains below 400 RNA copies/ml of blood, without treatment, for at least five years. We have studied the immune system of these patients, and particularly their CD4 lymphocytes, that participate in the induction, intensity, quality and duration of immune responses. CD4 lymphocytes in patients who progress to AIDS are directly targeted by the virus and participate in the activation that leads to immune deficiency. Central memory CD4 cells exhibit unusual properties in HIV controllers. Apart from the fact that they persist in large numbers and secrete large amounts of interleukin-2, which serves as an autocrine factor for their own growth, central memory CD4 cells overexpress the CCR7 homing molecule that allows them to leave capillaries and rapidly enter lymph nodes, the site of effective immune responses. These CD4 lymphocytes also men multiply rapidly, and some of them express receptors with very high antigen avidity. The presence of these central memory CD4 cells and their characteristic properties may explain the remarkable stability observed in HIV controllers. We suspect that these lymphocytes react very rapidly and efficiently to any breakthrough in viral replication. The putative relationship between HIV controllers and patients who remain asymptomatic and uninfected despite repeated exposure to the virus is discussed. Our new findings should help to guide antiretroviral therapy and vaccination strategies.

Published
2011

27. Preserved central memory and activated effector memory CD4+ T-cell subsets in human immunodeficiency virus controllers: an ANRS EP36 study.

Author

Potter SJ, Lacabaratz C, Lambotte O, Perez-Patrigeon S, Vingert B, Sinet M, Colle JH, Urrutia A, Scott-Algara D, Boufassa F, Delfraissy JF, Thèze J, Venet A, and Chakrabarti LA

Subjects
Adult, Aged, CD4 Lymphocyte Count, CD4-Positive T-Lymphocytes classification, Cytokines metabolism, Female, HIV Infections virology, HIV-1 immunology, Humans, Male, Middle Aged, CD4-Positive T-Lymphocytes immunology, HIV Infections immunology, HIV Long-Term Survivors, Immunologic Memory immunology, Lymphocyte Activation immunology
Abstract

Human immunodeficiency virus (HIV) controllers are rare individuals who spontaneously control HIV type 1 replication for 10 years or more in the absence of antiretroviral treatment. In the present study, HIV controllers (n = 11) maintained potent HIV-specific CD4 responses in spite of very low antigenic loads. Their CD4+ central memory T (T(CM)) cells were characterized by near-normal numbers and preserved interleukin-2 (IL-2) secretion in response to HIV antigens and uniformly high expression of the survival receptor IL-7 receptor alpha (IL-7Ralpha). Controllers expressed CCR7 at higher levels than uninfected controls, suggesting differences in T(CM)-cell homing patterns. CD4+ effector memory T (T(EM))-cell responses were polyfunctional in HIV controllers, while IL-2 secretion was lost in viremic patients. Cytokine production was three times higher in controllers than in treated patients with undetectable viral loads, suggesting an intrinsically more efficient response in the former group. The total CD4+ T(EM)-cell pool underwent immune activation in controllers, as indicated by increased HLA-DR expression, decreased IL-7Ralpha expression, a bias towards gamma interferon production upon polyclonal stimulation, and increased macrophage inflammatory protein 1beta secretion associated with chronic CCR5 down-regulation. Thus, HIV controllers showed a preserved CD4+ T(CM)-cell compartment and signs of potent functional activation in the CD4+ T(EM)-cell compartment. While controllers did not show the generalized immune activation pattern associated with disease progression, they had signs of immune activation restricted to the effector compartment. These findings suggest the induction of an efficient, nondetrimental type of immune activation in patients who spontaneously control HIV.

Published
2007
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