Single-cell transcriptome mapping identifies a local, innate B cell population driving chronic rejection after lung transplantation
Natalia F. Smirnova, Kent Riemondy, Marta Bueno, Susan Collins, Pavan Suresh, Xingan Wang, Kapil N. Patel, Carlyne Cool, Melanie Königshoff, Nirmal S. Sharma, Oliver Eickelberg
Natalia F. Smirnova, Kent Riemondy, Marta Bueno, Susan Collins, Pavan Suresh, Xingan Wang, Kapil N. Patel, Carlyne Cool, Melanie Königshoff, Nirmal S. Sharma, Oliver Eickelberg
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Resource and Technical Advance Pulmonology Transplantation

Single-cell transcriptome mapping identifies a local, innate B cell population driving chronic rejection after lung transplantation

Abstract

Bronchiolitis obliterans syndrome (BOS) is the main reason for poor outcomes after lung transplantation (LTx). We and others have recently identified B cells as major contributors to BOS after LTx. The extent of B cell heterogeneity and the relative contributions of B cell subpopulations to BOS, however, remain unclear. Here, we provide a comprehensive analysis of cell population changes and their gene expression patterns during chronic rejection after orthotopic LTx in mice. Of 11 major cell types, Mzb1-expressing plasma cells (PCs) were the most prominently increased population in BOS lungs. These findings were validated in 2 different cohorts of human BOS after LTx. A Bhlhe41, Cxcr3, and Itgb1 triple-positive B cell subset, also expressing classical markers of the innate-like B-1 B cell population, served as the progenitor pool for Mzb1+ PCs. This subset accounted for the increase in IgG2c production within BOS lung grafts. A genetic lack of Igs decreased BOS severity after LTx. In summary, we provide a detailed analysis of cell population changes during BOS. IgG+ PCs and their progenitors — an innate B cell subpopulation — are the major source of local Ab production and a significant contributor to BOS after LTx.

Authors

Natalia F. Smirnova, Kent Riemondy, Marta Bueno, Susan Collins, Pavan Suresh, Xingan Wang, Kapil N. Patel, Carlyne Cool, Melanie Königshoff, Nirmal S. Sharma, Oliver Eickelberg

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Figure 2

MZB1+ cells are associated with BOS in mouse and human transplanted lungs.

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MZB1+ cells are associated with BOS in mouse and human transplanted lung...
(A) UMAP representation of the cell populations detected in murine lung grafts by condition (HLA→B6 and B6→B6). (B) Proportion of each cell type in control versus BOS mouse lung graft samples. (C) Immunofluorescence and quantification of Mzb1+ cells in mouse native lungs and lung grafts. Data analyzed with 2-way ANOVA and Tukey’s multiple comparisons posttest. Scale bars, 1 mm. (D) IHC and quantification for MZB1 on explants from healthy donors and patients who developed BOS after LTx (samples from the University of Colorado collection). Scale bars, 2 mm and 200 μm in inserts. Data are expressed as mean ± SEM and analyzed with a Mann-Whitney 2-tailed test. *P < 0.05, **P < 0.01; alv, alveolar; mac, macrophages; OB, obliterative bronchiolitis; pneumo, pneumocytes; ROI, region of interest; LB, lymphocytic bronchiolitis.