Recruitment of plasma cells from IL-21-dependent and IL-21-independent immune reactions to the bone marrow

Author:

Ferreira-Gomes MartaORCID,Chen YidanORCID,Durek Pawel,Rincon-Arevalo HectorORCID,Heinrich FrederikORCID,Bauer LauraORCID,Szelinski FranziskaORCID,Guerra Gabriela Maria,Stefanski Ana-LuisaORCID,Niedobitek Antonia,Wiedemann Annika,Bondareva Marina,Ritter JacobORCID,Lehmann Katrin,Hardt Sebastian,Hipfl Christian,Hein SaschaORCID,Hildt EberhardORCID,Matz Mareen,Mei Henrik E.ORCID,Cheng Qingyu,Dang Van Duc,Witkowski MarioORCID,Lino Andreia C.ORCID,Kruglov Andrey,Melchers Fritz,Perka Carsten,Schrezenmeier Eva V.,Hutloff AndreasORCID,Radbruch AndreasORCID,Dörner Thomas,Mashreghi Mir-FarzinORCID

Abstract

AbstractBone marrow plasma cells (BMPC) are the correlate of humoral immunity, consistently releasing antibodies into the bloodstream. It remains unclear if BMPC reflect different activation environments or maturation of their precursors. Here we define human BMPC heterogeneity and track the recruitment of antibody-secreting cells (ASC) from SARS-CoV-2 vaccine immune reactions to the bone marrow (BM). Trajectories based on single-cell transcriptomes and repertoires of peripheral and BM ASC reveal sequential colonisation of BMPC compartments. In activated B cells, IL-21 suppresses CD19 expression, indicating that CD19low-BMPC are derived from follicular, while CD19high-BMPC originate from extrafollicular immune reactions. In primary immune reactions, both CD19low- and CD19high-BMPC compartments are populated. In secondary immune reactions, most BMPC are recruited to CD19high-BMPC compartments, reflecting their origin from extrafollicular reactivations of memory B cells. A pattern also observable in vaccinated-convalescent individuals and upon diphtheria/tetanus/pertussis recall-vaccination. Thus, BMPC diversity reflects the evolution of a given humoral immune response.

Funder

Bundesministerium für Bildung und Forschung

Publisher

Springer Science and Business Media LLC

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