Your search keyword '"atypical B cells"' showing total 8 results

1. Regulation of B‐cell function and expression of CD11c, T‐bet, and FcRL5 in response to different activation signals.

Author

Kleberg, Linn, Courey‐Ghaouzi, Alan‐Dine, Lautenbach, Maximilian Julius, Färnert, Anna, and Sundling, Christopher

Subjects

PLASMA cells, B cells, CELL differentiation, MALARIA, SECRETION

Abstract

CD11c, FcRL5, or T‐bet are commonly expressed by B cells expanding during inflammation, where they can make up >30% of mature B cells. However, the association between the proteins and differentiation and function in the host response remains largely unclear. We have assessed the co‐expression of CD11c, T‐bet, and FcRL5 in an in vitro B‐cell culture system to determine how stimulation via the BCR, toll‐like receptor 9 (TLR9), and different cytokines influence CD11c, T‐bet, and FcRL5 expression. We observed different expression dynamics for all markers, but a largely overlapping regulation of CD11c and FcRL5 in response to BCR and TLR9 activation, while T‐bet was strongly dependent on IFN‐γ signaling. Investigating plasma cell differentiation and APC functions, there was no association between marker expression and antibody secretion or T‐cell help. Rather the functions were associated with TLR9‐signalling and B‐cell‐derived IL‐6 production, respectively. These results suggest that the expression of CD11c, FcRL5, and T‐bet and plasma cell differentiation and improved APC functions occur in parallel and are regulated by similar activation signals, but they are not interdependent. [ABSTRACT FROM AUTHOR]

Published

2024

2. Unravelling B cell heterogeneity: insights into flow cytometrygated B cells from single-cell multi-omics data.

Author

Pernes, Jane I., Alsayah, Atheer, Tucci, Felicia, and Bashford-Rogers, Rachael J. M.

Subjects

B cells, MULTIOMICS, CELL populations, CELL physiology, HETEROGENEITY

Abstract

Introduction: B cells play a pivotal role in adaptive immunity which has been extensively characterised primarily via flow cytometry-based gating strategies. This study addresses the discrepancies between flow cytometry-defined B cell subsets and their high-confidence molecular signatures using single-cell multiomics approaches. Methods: By analysing multi-omics single-cell data from healthy individuals and patients across diseases, we characterised the level and nature of cellular contamination within standard flow cytometric-based gating, resolved some of the ambiguities in the literature surrounding unconventional B cell subsets, and demonstrated the variable effects of flow cytometric-based gating cellular heterogeneity across diseases. Results: We showed that flow cytometric-defined B cell populations are heterogenous, and the composition varies significantly between disease states thus affecting the implications of functional studies performed on these populations. Importantly, this paper draws caution on findings about B cell selection and function of flow cytometric-sorted populations, and their roles in disease. As a solution, we developed a simple tool to identify additional markers that can be used to increase the purity of flow-cytometric gated immune cell populations based on multi-omics data (AlliGateR). Here, we demonstrate that additional non-linear CD20, CD21 and CD24 gating can increase the purity of both naïve and memory populations. Discussion: These findings underscore the need to reconsider B cell subset definitions within the literature and propose leveraging single-cell multi-omics data for refined characterisation. We show that single-cell multi-omics technologies represent a powerful tool to bridge the gap between surface marker-based annotations and the intricate molecular characteristics of B cell subsets. [ABSTRACT FROM AUTHOR]

Published

2024

3. Acquisition of complement fixing antibodies targeting Plasmodium falciparum merozoites in infants and their mothers in Uganda.

Author

Mortazavi, Susanne E., Lugaajju, Allan, Nylander, Maria, Danielsson, Lena, Tijani, Muyideen Kolapo, Beeson, James G., and Persson, Kristina E. M.

Subjects

PLASMODIUM falciparum, IMMUNOLOGIC memory, MEROZOITES, CORD blood, IMMUNOGLOBULINS, CRYING

Abstract

Background: Antibody-mediated complement fixation has previously been associated with protection against malaria in naturally acquired immunity. However, the process of early-life development of complement-fixing antibodies in infants, both in comparison to their respective mothers and to other immune parameters, remains less clear. Results: We measured complement-fixing antibodies in newborns and their mothers in a malaria endemic area over 5 years follow-up and found that infants’ complement-fixing antibody levels were highest at birth, decreased until six months, then increased progressively until they were similar to birth at five years. Infants with high levels at birth experienced a faster decay of complement-fixing antibodies but showed similar levels to the low response group of newborns thereafter. No difference was observed in antibody levels between infant cord blood and mothers at delivery. The same result was found when categorized into high and low response groups, indicating placental transfer of antibodies. Complement-fixing antibodies were positively correlated with total schizont-specific IgG and IgM levels in mothers and infants at several time points. At nine months, complement-fixing antibodies were negatively correlated with total B cell frequency and osteopontin concentrations in the infants, while positively correlated with atypical memory B cells and P. falciparum-positive atypical memory B cells. Conclusion: This study indicates that complement-fixing antibodies against P. falciparum merozoites are produced in the mothers and placentally-transferred, and they are acquired in infants over time during the first years of life. Understanding early life immune responses is crucial for developing a functional, long lasting malaria vaccine. [ABSTRACT FROM AUTHOR]

Published

2023

4. BAFF system expression in double negative 2, activated naive and activated memory B cells in systemic lupus erythematosus.

Author

Álvarez Gómez, Jhonatan Antonio, Salazar-Camarena, Diana Celeste, Román-Fernández, Ilce Valeria, Ortiz-Lazareno, Pablo César, Cruz, Alvaro, Muñoz-Valle, José Francisco, Marín-Rosales, Miguel, Espinoza-García, Noemí, Sagrero-Fabela, Nefertari, and Palafox-Sánchez, Claudia Azucena

Subjects

IMMUNOLOGIC memory, SYSTEMIC lupus erythematosus, B cell receptors, B cells, ENZYME-linked immunosorbent assay

Abstract

Introduction: B cell activating factor (BAFF) has an important role in normal B cell development. The aberrant expression of BAFF is related with the autoimmune diseases development like Systemic Lupus Erythematosus (SLE) for promoting self-reactive B cells survival. BAFF functions are exerted through its receptors BAFF-R (BR3), transmembrane activator calcium modulator and cyclophilin ligand interactor (TACI) and B cell maturation antigen (BCMA) that are reported to have differential expression on B cells in SLE. Recently, atypical B cells that express CD11c have been associated with SLE because they are prone to develop into antibody-secreting cells, however the relationship with BAFF remains unclear. This study aims to analyze the BAFF system expression on CXCR5-CD11c+ atypical B cell subsets double negative 2 (DN2), activated naive (aNAV), switched memory (SWM) and unswitched memory (USM) B cells. Methods: Forty-five SLE patients and 15 healthy subjects (HS) were included. Flow cytometry was used to evaluate the expression of the receptors in the B cell subpopulations. Enzyme-linked immunosorbent assay (ELISA) was performed to quantify the soluble levels of BAFF (sBAFF) and IL-21. Results: We found increased frequency of CXCR5- CD11c+ atypical B cell subpopulations DN2, aNAV, SWM and USM B cells in SLE patients compared to HS. SLE patients had increased expression of membrane BAFF (mBAFF) and BCMA receptor in classic B cell subsets (DN, NAV, SWM and USM). Also, the CXCR5+ CD11c-DN1, resting naive (rNAV), SWM and USM B cell subsets showed higher mBAFF expression in SLE. CXCR5- CD11c+ atypical B cell subpopulations DN2, SWM and USM B cells showed strong correlations with the expression of BAFF receptors. The atypical B cells DN2 in SLE showed significant decreased expression of TACI, which correlated with higher IL-21 levels. Also, lower expression of TACI in atypical B cell DN2 was associated with high disease activity. Discussion: These results suggest a participation of the BAFF system in CXCR5- CD11c+ atypical B cell subsets in SLE patients. Decreased TACI expression on atypical B cells DN2 correlated with high disease activity in SLE patients supporting the immunoregulatory role of TACI in autoimmunity. [ABSTRACT FROM AUTHOR]

Published

2023

5. Autoantibodies during infectious diseases: Lessons from malaria applied to COVID-19 and other infections.

Author

Rivera-Correa, Juan and Rodriguez, Ana

Subjects

COMMUNICABLE diseases, AUTOANTIBODIES, COVID-19, MALARIA, B cells

Abstract

Autoimmunity is a common phenomenon reported in many globally relevant infections, including malaria and COVID-19. These and other highly inflammatory diseases have been associated with the presence of autoantibodies. The role that these autoantibodies play during infection has been an emerging topic of interest. The vast numbers of studies reporting a range of autoantibodies targeting cellular antigens, such as dsDNA and lipids, but also immune molecules, such as cytokines, during malaria, COVID-19 and other infections, underscore the importance that autoimmunity can play during infection. During both malaria and COVID-19, the presence of autoantibodies has been correlated with associated pathologies such as malarial anemia and severe COVID-19. Additionally, high levels of Atypical/Autoimmune B cells (ABCs and atypical B cells) have been observed in both diseases. The growing literature of autoimmune B cells, age-associated B cells and atypical B cells in Systemic Lupus erythematosus (SLE) and other autoimmune disorders has identified recent mechanistic and cellular targets that could explain the development of autoantibodies during infection. These new findings establish a link between immune responses during infection and autoimmune disorders, highlighting shared mechanistic insights. In this review, we focus on the recent evidence of autoantibody generation during malaria and other infectious diseases and their potential pathological role, exploring possible mechanisms that may explain the development of autoimmunity during infections. [ABSTRACT FROM AUTHOR]

Published

2022

6. Generation of plasma cells and CD27−IgD− B cells during hantavirus infection is associated with distinct pathological findings.

Author

Kerkman, Priscilla F, Dernstedt, Andy, Tadala, Lalitha, Mittler, Eva, Dannborg, Mirjam, Sundling, Christopher, Maleki, Kimia T, Tauriainen, Johanna, Tuiskunen‐Bäck, Anne, Wigren Byström, Julia, Ocaya, Pauline, Thunberg, Therese, Jangra, Rohit K, Román‐Sosa, Gleyder, Guardado‐Calvo, Pablo, Rey, Felix A, Klingström, Jonas, Chandran, Kartik, Puhar, Andrea, and Ahlm, Clas

Subjects

HANTAVIRUS diseases, B cells, HEMORRHAGIC fever with renal syndrome, PLASMA cells, PLASMA production

Abstract

Objective: Human hantavirus infections can cause haemorrhagic fever with renal syndrome (HFRS). The pathogenic mechanisms are not fully understood, nor if they affect the humoral immune system. The objective of this study was to investigate humoral immune responses to hantavirus infection and to correlate them to the typical features of HFRS: thrombocytopenia and transient kidney dysfunction. Methods: We performed a comprehensive characterisation of longitudinal antiviral B‐cell responses of 26 hantavirus patients and combined this with paired clinical data. In addition, we measured extracellular adenosine triphosphate (ATP) and its breakdown products in circulation and performed in vitro stimulations to address its effect on B cells. Results: We found that thrombocytopenia was correlated to an elevated frequency of plasmablasts in circulation. In contrast, kidney dysfunction was indicative of an accumulation of CD27−IgD− B cells and CD27−/low plasmablasts. Finally, we provide evidence that high levels of extracellular ATP and matrix metalloproteinase 8 can contribute to shedding of CD27 during human hantavirus infection. Conclusion: Our findings demonstrate that thrombocytopenia and kidney dysfunction associate with distinctly different effects on the humoral immune system. Moreover, hantavirus‐infected individuals have significantly elevated levels of extracellular ATP in circulation. [ABSTRACT FROM AUTHOR]

Published

2021

7. Deep Phenotyping of CD11c+ B Cells in Systemic Autoimmunity and Controls.

Author

Rincon-Arevalo, Hector, Wiedemann, Annika, Stefanski, Ana-Luisa, Lettau, Marie, Szelinski, Franziska, Fuchs, Sebastian, Frei, Andreas Philipp, Steinberg, Malte, Kam-Thong, Tony, Hatje, Klas, Keller, Baerbel, Warnatz, Klaus, Radbruch, Andreas, Lino, Andreia C., Schrezenmeier, Eva, and Dörner, Thomas

Subjects

B cells, SYSTEMIC lupus erythematosus, AUTOIMMUNITY, BLOOD cells, KI-67 antigen, PSYCHONEUROIMMUNOLOGY

Abstract

Circulating CD11c+ B cells are a key phenomenon in certain types of autoimmunity but have also been described in the context of regular immune responses (i.e., infections, vaccination). Using mass cytometry to profile 46 different markers on individual immune cells, we systematically initially confirmed the presence of increased CD11c+ B cells in the blood of systemic lupus erythematosus (SLE) patients. Notably, significant differences in the expression of CD21, CD27, and CD38 became apparent between CD11c− and CD11c+ B cells. We observed direct correlation of the frequency of CD21−CD27− B cells and CD21−CD38− B cells with CD11c+ B cells, which were most pronounced in SLE compared to primary Sjögren's syndrome patients (pSS) and healthy donors (HD). Thus, CD11c+ B cells resided mainly within memory subsets and were enriched in CD27−IgD−, CD21−CD27−, and CD21−CD38− B cell phenotypes. CD11c+ B cells from all donor groups (SLE, pSS, and HD) showed enhanced CD69, Ki-67, CD45RO, CD45RA, and CD19 expression, whereas the membrane expression of CXCR5 and CD21 were diminished. Notably, SLE CD11c+ B cells showed enhanced expression of the checkpoint molecules CD86, PD1, PDL1, CD137, VISTA, and CTLA-4 compared to HD. The substantial increase of CD11c+ B cells with a CD21− phenotype co-expressing distinct activation and checkpoint markers, points to a quantitative increased alternate (extrafollicular) B cell activation route possibly related to abnormal immune regulation as seen under the striking inflammatory conditions of SLE which shows a characteristic PD-1/PD-L1 upregulation. [ABSTRACT FROM AUTHOR]

Published

2021

8. Challenges and Opportunities for Consistent Classification of Human B Cell and Plasma Cell Populations.

Author

Sanz, Ignacio, Wei, Chungwen, Jenks, Scott A., Cashman, Kevin S., Tipton, Christopher, Woodruff, Matthew C., Hom, Jennifer, and Lee, F. Eun-Hyung

Subjects

PLASMA cells, B cells, CELL populations, IMMUNE response, CLASSIFICATION

Abstract

The increasingly recognized role of different types of B cells and plasma cells in protective and pathogenic immune responses combined with technological advances have generated a plethora of information regarding the heterogeneity of this human immune compartment. Unfortunately, the lack of a consistent classification of human B cells also creates significant imprecision on the adjudication of different phenotypes to well-defined populations. Additional confusion in the field stems from: the use of non-discriminatory, overlapping markers to define some populations, the extrapolation of mouse concepts to humans, and the assignation of functional significance to populations often defined by insufficient surface markers. In this review, we shall discuss the current understanding of human B cell heterogeneity and define major parental populations and associated subsets while discussing their functional significance. We shall also identify current challenges and opportunities. It stands to reason that a unified approach will not only permit comparison of separate studies but also improve our ability to define deviations from normative values and to create a clean framework for the identification, functional significance, and disease association with new populations. [ABSTRACT FROM AUTHOR]

Published

2019