Your search keyword '"Allard‐Chamard Hugues"' showing total 6 results

1. SARS-CoV-2 spike antigenspecific B cell and antibody responses in pre-vaccination period COVID-19 convalescent males and females with or without post-covid condition.

Author

Limoges, Marc-André, Irmine Quenum, Akouavi Julite, Hussain Chowdhury, Mohammad Mobarak, Rexhepi, Fjolla, Namvarpour, Mozhdeh, Ali Akbari, Sara, Rioux-Perreault, Christine, Nandi, Madhuparna, Lucier, Jean-François, Lemaire-Paquette, Samuel, Premkumar, Lakshmanane, Durocher, Yves, Cantin, André, Lévesque, Simon, Dionne, Isabelle J., Menendez, Alfredo, Ilangumaran, Subburaj, Allard-Chamard, Hugues, Piché, Alain, and Ramanathan, Sheela

Subjects

ANTIBODY formation, B cells, COVID-19 pandemic, COVID-19, SARS-CoV-2

Abstract

Background: Following SARS-CoV-2 infection a significant proportion of convalescent individuals develop the post-COVID condition (PCC) that is characterized by wide spectrum of symptoms encompassing various organs. Even though the underlying pathophysiology of PCC is not known, detection of viral transcripts and antigens in tissues other than lungs raise the possibility that PCC may be a consequence of aberrant immune response to the viral antigens. To test this hypothesis, we evaluated B cell and antibody responses to the SARS-CoV-2 antigens in PCC patients who experienced mild COVID-19 disease during the pre-vaccination period of COVID-19 pandemic. Methods: The study subjects included unvaccinated male and female subjects who developed PCC or not (No-PCC) after clearing RT-PCR confirmed mild COVID-19 infection. SARS-CoV-2 D614G and omicron RBD specific B cell subsets in peripheral circulation were assessed by flow cytometry. IgG, IgG3 and IgA antibody titers toward RBD, spike and nucleocapsid antigens in the plasma were evaluated by ELISA. Results: The frequency of the B cells specific to D614G-RBD were comparable in convalescent groups with and without PCC in both males and females. Notably, in females with PCC, the anti-D614G RBD specific double negative (IgD-CD27-) B cells showed significant correlation with the number of symptoms at acute of infection. Anti-spike antibody responses were also higher at 3 months postinfection in females who developed PCC, but not in the male PCC group. On the other hand, the male PCC group also showed consistently high anti-RBD IgG responses compared to all other groups. Conclusions: The antibody responses to the spike protein, but not the anti-RBD B cell responses diverge between convalescent males and females who develop PCC. Our findings also suggest that sex-related factors may also be involved in the development of PCC via modulating antibody responses to the SARS-CoV-2 antigens. [ABSTRACT FROM AUTHOR]

Published

2023

2. SARS-CoV-2 mRNA vaccine-induced immune responses in rheumatoid arthritis.

Author

Limoges, Marc-André, Lortie, Audrey, Demontier, Élodie, Quenum, Akouavi Julite Irmine, Lessard, Félix, Drouin, Zacharie, Carrier, Nathalie, Nguimbus, Leopold Mbous, Beaulieu, Marie-Claude, Boire, Gilles, Piché, Alain, Allard-Chamard, Hugues, Ramanathan, Sheela, and Roux, Sophie

Subjects

MONONUCLEAR leukocytes, RHEUMATOID arthritis, IMMUNE response, HUMORAL immunity, B cells

Abstract

Our objective was to characterize T and B cell responses to vaccination with SARS-CoV-2 antigens in immunocompromised rheumatoid arthritis (RA) patients. In 22 RA patients, clinical and biological variables were analyzed before and 4 weeks after each of 3 messenger RNA (mRNA) vaccine doses and compared with unmatched healthy individuals. Sequentially sampled peripheral blood mononuclear cells and sera were collected to determine immune profiles and to analyze the T cell response to a spike peptide pool and B cell specificity to the receptor-binding domain (RBD). Anti-spike antibodies were detectable in 6 of 22 RA patients after 1 dose of vaccine with increasing titers after each booster dose, although the overall response was lower compared with that in healthy control individuals. Responding patients after the first dose were more likely to have RA antibodies and a higher baseline proportion of circulating follicular B cells. In RA patients, the mRNA vaccine elicited a robust CD4+ T response to a spike peptide pool following the first and second doses. Consistent with the serologies, RBD-specific B cells exhibited a modest increase after the first dose and the second dose resulted in marked increases only in a fraction of the RA patients to both ancestral and omicron RBD. Our results highlight the importance of multidose COVID-19 vaccination in RA patients to develop a protective humoral response. However, these patients rapidly develop specific T CD4+ responses, despite delayed B cell responses. [ABSTRACT FROM AUTHOR]

Published

2023

3. B1a and B2 cells are characterized by distinct CpG modification states at DNMT3A-maintained enhancers.

Author

Mahajan, Vinay S., Mattoo, Hamid, Sun, Na, Viswanadham, Vinayak, Yuen, Grace J., Allard-Chamard, Hugues, Ahmad, Maimuna, Murphy, Samuel J. H., Cariappa, Annaiah, Tuncay, Yesim, and Pillai, Shiv

Subjects

FETAL liver cells, B cells, GENES, BONE marrow, PROGENITOR cells

Abstract

The B1 and B2 lineages of B cells contribute to protection from pathogens in distinct ways. The role of the DNA CpG methylome in specifying these two B-cell fates is still unclear. Here we profile the CpG modifications and transcriptomes of peritoneal B1a and follicular B2 cells, as well as their respective proB cell precursors in the fetal liver and adult bone marrow from wild-type and CD19-Cre Dnmt3a floxed mice lacking DNMT3A in the B lineage. We show that an underlying foundational CpG methylome is stably established during B lineage commitment and is overlaid with a DNMT3A-maintained dynamic methylome that is sculpted in distinct ways in B1a and B2 cells. This dynamic DNMT3A-maintained methylome is composed of novel enhancers that are closely linked to lineage-specific genes. While DNMT3A maintains the methylation state of these enhancers in both B1a and B2 cells, the dynamic methylome undergoes a prominent programmed demethylation event during B1a but not B2 cell development. We propose that the methylation pattern of DNMT3A-maintained enhancers is determined by the coincident recruitment of DNMT3A and TET enzymes, which regulate the developmental expression of B1a and B2 lineage-specific genes. B cell progenitors differentiate into multiple subsets with distinct functions. Here the authors analyze the epigenetic landscapes of sorted B cell subsets using multiple platforms and show that the epigenetic regulator, DNMT3A, is essential for modulating the activity of enhancers critical for B1 and B2 lineage-determining genes. [ABSTRACT FROM AUTHOR]

Published

2021

4. Induction of metabolic quiescence defines the transitional to follicular B cell switch.

Author

Farmer, Jocelyn R., Allard-Chamard, Hugues, Sun, Na, Ahmad, Maimuna, Bertocchi, Alice, Mahajan, Vinay S., Aicher, Toby, Arnold, Johan, Benson, Mark D., Morningstar, Jordan, Barmettler, Sara, Yuen, Grace, Murphy, Samuel J. H., Walter, Jolan E., Ghebremichael, Musie, Shalek, Alex K., Batista, Facundo, Gerszten, Robert, and Pillai, Shiv

Subjects

ADENOSINES, B cell differentiation, T helper cells, B cells, CELL analysis, PROTEIN kinases, CELL membranes

Abstract

AMPing up B cell maturation: Glycolysis provides an important energy source during B cell activation. In contrast, Farmer et al. found that metabolic quiescence was important for the development of human follicular B cells from transitional B cell precursors. In comparison to transitional B cells, mouse and human follicular B cells had reduced expression of genes involved in aerobic respiration, increased AMPK activation, and greater amounts of the cell surface ectoenzymes CD39 and CD73, which generate extracellular adenosine. Transitional human B cells that expressed CD73 or were treated with an AMPK agonist preferentially acquired a follicular B cell phenotype. These data identify a previously uncharacterized metabolic checkpoint in B cell development. Transitional B cells must actively undergo selection for self-tolerance before maturing into their resting follicular B cell successors. We found that metabolic quiescence was acquired at the follicular B cell stage in both humans and mice. In follicular B cells, the expression of genes involved in ribosome biogenesis, aerobic respiration, and mammalian target of rapamycin complex 1 (mTORC1) signaling was reduced when compared to that in transitional B cells. Functional metabolism studies, profiling of whole-cell metabolites, and analysis of cell surface proteins in human B cells suggested that this transition was also associated with increased extracellular adenosine salvage. Follicular B cells increased the abundance of the cell surface ectonucleotidase CD73, which coincided with adenosine 5′-monophosphate–activated protein kinase (AMPK) activation. Differentiation to the follicular B cell stage in vitro correlated with surface acquisition of CD73 on human transitional B cells and was augmented with the AMPK agonist, AICAR. Last, individuals with gain-of-function PIK3CD (PI3Kδ) mutations and increased pS6 activation exhibited a near absence of circulating follicular B cells. Together, our data suggest that mTORC1 attenuation may be necessary for human follicular B cell development. These data identify a distinct metabolic switch during human B cell development at the transitional to follicular stages, which is characterized by an induction of extracellular adenosine salvage, AMPK activation, and the acquisition of metabolic quiescence. [ABSTRACT FROM AUTHOR]

Published

2019

5. T peripheral helper (Tph) cells, a marker of immune activation in cancer and autoimmune disorders.

Author

del Carmen Crespo Oliva, Celia, Labrie, Marilyne, and Allard-Chamard, Hugues

Subjects

*T helper cells, *IMMUNE response, *BIOMARKERS, *B cells, *RHEUMATOID arthritis

Abstract

T peripheral helper (Tph) cells are a newly discovered subtype of CD4+ T cells that have emerged as the counterpart of T follicular helper (Tfh) cells in the peripheral tissues. These two cell types share some common characteristics, such as high levels of PD1 and CXCL13 expression, but differ in the expression of transcription factors and chemokine receptors. Tph cells have been studied in relation to B cells' effector functions, including cytokines production and antibody-mediated immune responses. However, their role in the inflammatory-mediated development of malignancies remains poorly understood. Tph cells were initially identified in the synovium of rheumatoid arthritis patients and have since been found to be expanded in several autoimmune diseases. They have been linked to a worse prognosis in autoimmune conditions, but intriguingly, their presence has been correlated with better outcomes in certain types of cancer. The functions of Tph cells are still being investigated, but recent data suggests their involvement in the assembly of tertiary lymphoid structures (TLS). Furthermore, their interaction with B cells, which have been mainly described as possessing a memory phenotype, promotes their development. In this review, we explore the role of Tph cells in peripheral immune responses during cancer and autoimmune disorders. • Tph cells have been implicated in the induction of ectopic lymphoid structures. • Increasing data suggest a transition from Tfh into Tph cells. • Upon antigen stimulation, Tph cell activation is regulated by concomitant PD-1 signaling. • Pathways controlled by Tph activation have been characterized in the early stages of ADs as a leading contributor to the perpetuation of chronic inflammation. Hence it would be rational to address Tph cells as putative targets in preventing ADs establishment in its early stages. • Triggering TLS neogenesis and promoting humoral responses is a pivotal antitumoral function of Tph cells; however, recent studies on breast cancer suggest an alternative antitumoral role of Tph based on limiting Treg expansion. [ABSTRACT FROM AUTHOR]

Published

2024

6. Loss of Bcl-6-Expressing T Follicular Helper Cells and Germinal Centers in COVID-19.

Author

Kaneko, Naoki, Kuo, Hsiao-Hsuan, Boucau, Julie, Farmer, Jocelyn R., Allard-Chamard, Hugues, Mahajan, Vinay S., Piechocka-Trocha, Alicja, Lefteri, Kristina, Osborn, Matthew, Bals, Julia, Bartsch, Yannic C., Bonheur, Nathalie, Caradonna, Timothy M., Chevalier, Josh, Chowdhury, Fatema, Diefenbach, Thomas J., Einkauf, Kevin, Fallon, Jon, Feldman, Jared, and Finn, Kelsey K.

Subjects

*GERMINAL centers, *COVID-19, *T helper cells, *HUMORAL immunity, *T cell differentiation, *FOLLICULAR dendritic cells, *B cells

Abstract

Humoral responses in coronavirus disease 2019 (COVID-19) are often of limited durability, as seen with other human coronavirus epidemics. To address the underlying etiology, we examined post mortem thoracic lymph nodes and spleens in acute SARS-CoV-2 infection and observed the absence of germinal centers and a striking reduction in Bcl-6+ germinal center B cells but preservation of AID+ B cells. Absence of germinal centers correlated with an early specific block in Bcl-6+ T FH cell differentiation together with an increase in T-bet+ T H1 cells and aberrant extra-follicular TNF-α accumulation. Parallel peripheral blood studies revealed loss of transitional and follicular B cells in severe disease and accumulation of SARS-CoV-2-specific "disease-related" B cell populations. These data identify defective Bcl-6+ T FH cell generation and dysregulated humoral immune induction early in COVID-19 disease, providing a mechanistic explanation for the limited durability of antibody responses in coronavirus infections, and suggest that achieving herd immunity through natural infection may be difficult. • Germinal centers are lost in lymph nodes and spleens in acute COVID-19 • Bcl-6+ GC B cells and Bcl-6+ T follicular helper cells are markedly diminished • Abundant T H1 cells and aberrant TNF-α production are seen in COVID-19 lymph nodes • SARS-CoV-2-specific activated B cells accumulate in the blood of patients Shiv Pillai and colleagues show that in acute COVID-19, there is a striking loss of germinal centers in lymph nodes and spleens and depletion of Bcl-6+ B cells but preservation of AID+ B cells. A specific block in germinal center type Bcl-6+ T follicular helper cell differentiation may explain the loss of germinal centers and the accumulation of non-germinal-center-derived activated B cells. These data suggest an underlying basis for the lower quality and lack of durability of humoral immune responses observed during natural infection with SARS-CoV-2 and have significant implications for expectations of herd immunity. [ABSTRACT FROM AUTHOR]

Published

2020