Allergen-specific IgG Memory B Cells Are Temporally Linked to IgE Memory Responses

Overview

Journal J Allergy Clin Immunol

Specialty Allergy & Immunology

Date 2019 Dec 30

PMID 31883847

Citations 21

Authors

Ilka Hoof

Veronique Schulten

Janice A Layhadi

Thomas Stranzl

Lars H Christensen

Sara Herrera de la Mata

Gregory Seumois

Pandurangan Vijayanand

Claus Lundegaard

Kristoffer Niss

Anders Lund

Johanne Ahrenfeldt

Jens Holm

Esther Steveling

Hanisah Sharif

Stephen R Durham

Bjorn Peters

Mohamed H Shamji

Peter S Andersen

Affiliations

Soon will be listed here.

Abstract

Background: IgE is the least abundant immunoglobulin and tightly regulated, and IgE-producing B cells are rare. The cellular origin and evolution of IgE responses are poorly understood.

Objective: The cellular and clonal origin of IgE memory responses following mucosal allergen exposure by sublingual immunotherapy (SLIT) were investigated.

Methods: In a randomized double-blind, placebo-controlled, time course SLIT study, PBMCs and nasal biopsy samples were collected from 40 adults with seasonal allergic rhinitis at baseline and at 4, 8, 16, 28, and 52 weeks. RNA was extracted from PBMCs, sorted B cells, and nasal biopsy samples for heavy chain variable gene repertoire sequencing. Moreover, mAbs were derived from single B-cell transcriptomes.

Results: Combining heavy chain variable gene repertoire sequencing and single-cell transcriptomics yielded direct evidence of a parallel boost of 2 clonally and functionally related B-cell subsets of short-lived IgE plasmablasts and IgG memory B cells. Mucosal grass pollen allergen exposure by SLIT resulted in highly diverse IgE and IgG repertoires. These were extensively mutated and appeared relatively stable as per heavy chain isotype, somatic hypermutations, and clonal composition. Single IgG memory B-cell and IgE preplasmablast transcriptomes encoded antibodies that were specific for major grass pollen allergens and able to elicit basophil activation at very low allergen concentrations.

Conclusion: For the first time, we have shown that on mucosal allergen exposure, human IgE memory resides in allergen-specific IgG memory B cells. These cells rapidly switch isotype, expand into short-lived IgE plasmablasts, and serve as a potential target for therapeutic intervention.

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