Profiling the specificity of clonally expanded plasma cells during chronic viral infection by single‐cell analysis

Lau

2022

Preprint

Antibody-secreting cells (ASCs) are key contributors to humoral immunity through immunoglobulin production and the potential to be long-lived. ASCs have been recently identified in the thymus (THY) which is of interest as autoreactive THY B cells regulate T cell tolerance. Here, we showed that the young female THY was skewed towards higher production of ASCs relative to males. However, these differences disappeared with age. Intravenous labeling combined with blockade of CD154(CD40L) suggested that THY ASCs were generated in situ in a T cell dependent fashion. Single cell RNA-sequencing revealed that THY ASCs possessed a transcriptional signature indicative of interferon signaling and activation. Flow cytometry confirmed that THY ASCs had increased levels of Toll-like receptor 7 as well as the activation markers CD69 and major histocompatibility class II. Overall, THY ASCs are a unique population that require further investigation to fully appreciate their biological significance.

Section: Discussionmentioning

confidence: 99%

Thymus Antibody-Secreting Cells Represent a Tissue Specific Population That Possess an Activated Cellular Phenotype

Lau

2022

Preprint

“…Selected antibodies were produced in PnP-mRuby hybridoma cells as previously described (Parola et al, 2019) and validated using normalized supernatant ELISAs against purified LCMV clone 13 NP, LCMV clone 13 GP, DNP-OVA, insulin (Sigma, I5500), mouse genomic DNA (Sigma, 692339), MOG (Sigma, 692339) as previously described (Neumeier et al 2021). An anti-mouse IgG-HRP (Sigma, A2554) was employed at 1:1500 and used for detection.…”

Section: Methodsmentioning

confidence: 99%

“…For single-cell sequencing, brain B cells (CD19+ CD3-CD45.1+) were FACS-sorted from STOP:GP, aCD8-GFAP:GP and GFAP:GP mice 7 days after start of TAM, and from MOG:GP mice 47 days after i.c infection. Combined single-cell transcriptome and immune repertoire sequencing was performed using the 10x Genomics Chromium Single Cell V(D)J Reagents Kit (CG000166 Rev A) according to established methods (Neumeier et al 2021). Single cells together with gel beads (10x Genomics, 1000006) were encapsulated in gel emulsion microdroplets using 4 lanes of one Chromium Single Cell A Chip (10x Genomics, 1000009) with a target loading of 13,000 cells per reaction.…”

Section: Single-cell Immune Repertoire Sequencing Of Murine B Cellsmentioning

confidence: 99%

“…Recent advancements in sequencing and microfluidic techniques have enabled comprehensive profiling of B cells and their corresponding antibody repertoires (Yermanos, Agrafiotis, et al 2021; Neumeier et al 2021; Agrafiotis et al 2021; Horns, Dekker, and Quake 2020). Current iterations of this technology provide both single-cell antibody repertoires (full-length, paired heavy and light chain antibody sequences) and single-cell transcriptomes (Csepregi et al 2020).…”

Section: Introductionmentioning

confidence: 99%

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Persistent virus-specific and clonally expanded antibody secreting cells respond to induced self antigen in the CNS

Agrafiotis

Dizerens

Vincenti

et al. 2022

Preprint

Self Cite

B cells contribute to the pathogenesis of both cellular- and humoral-mediated central nervous system (CNS) inflammatory diseases through a variety of mechanisms. In such conditions, B cells may enter the CNS parenchyma and contribute to local tissue destruction. It remains unexplored, however, how infection and autoimmunity drive transcriptional phenotypes, repertoire features, and antibody functionality. Here, we profiled B cells from the CNS of murine models of intracranial (i.c.) viral infections and autoimmunity. We identified a population of clonally expanded, antibody secreting cells (ASCs) that had undergone class-switch recombination and extensive somatic hypermutation following i.c. infection with attenuated lymphocytic choriomeningitis virus (rLCMV). Recombinant expression and characterisation of these antibodies revealed specificity to viral antigens (LCMV glycoprotein GP), correlating with ASC persistence in the brain weeks after resolved infection. Furthermore, these virus-specific ASCs upregulated proliferation and expansion programs in response to the conditional and transient induction of the LCMV GP as a neo-self antigen by astrocytes. This class-switched, clonally expanded, and mutated population persisted and was even more pronounced when peripheral B cells were depleted prior to autoantigen induction in the CNS. In contrast, the most expanded B cell clones in mice with persistent expression of LCMV GP in the CNS did not exhibit neo-self antigen specificity, potentially a consequence of local tolerance induction. Finally, a comparable population of clonally expanded, class-switched, proliferating ASCs was detected in the cerebrospinal fluid of multiple sclerosis patients. Taken together, our findings support the existence of B cells that populate the CNS and are capable of responding to locally encountered autoantigens.

“…Additionally, the emergence of single-cell sequencing (scSeq) technologies has made it possible to identify endogenously paired variable heavy (VH) and variable light chain (VL) regions from single B cells at high-throughput, which can be used to subsequently reconstruct antibodies for experimental testing (DeKosky et al 2013; DeKosky et al 2015) . For example, our group recently performed scSeq of plasma cells following immunization or viral infection in mice, and subsequent expression and screening of antibodies from highly expanded clones was shown to correlate with antigen-specificity (Neumeier et al 2022; Neumeier, Yermanos, et al 2021). A similar approach was applied to plasma cells isolated from convalescent Covid-19 individuals and led to the discovery of a panel of antibodies, including potent neutralizing antibodies against SARS-CoV-2 (Ehling et al 2022).…”

Section: Introductionmentioning

confidence: 99%

Generation of a single-cell B cell atlas of antibody repertoires and transcriptomes to identify signatures associated with antigen-specificity

Agrafiotis

Neumeier

Hong

et al. 2021

Preprint

Self Cite

Aging of the humoral immune response has been shown to affect its critical role in defending the host from a variety of pathogens. Technical limitations have nevertheless made it challenging to investigate the relationship between genotype and phenotype of antibody repertoires in the context of aging. We therefore performed single-cell sequencing of over 95,000 B cells to simultaneously investigate B cell receptor (BCR) repertoires and gene expression profiles in the bone marrow and spleens of young and old mice following immunizations with a protein antigen. We discovered the presence of clonally expanded B cells in both young and old mice, which had distinct transcriptional phenotypes and exhibited age-associated gene signatures relating to plasma cell differentiation and protein folding and stabilization genes. Recombinant expression of 227 monoclonal antibodies revealed that clonally expanded B cells were frequently antigen-specific in young mice but not in old mice. Furthermore, we detected clonal convergence across different mice which was correlated with antigen-specificity. Although isotype- and expansion-specific transcriptional phenotypes could be detected, there was little correlation with antigen-specificity and transcriptional signatures. Together, our work provides an age-resolved single-cell repertoire resource that further relates antibody specificity, repertoire features, and whole transcriptomes.