IL-21–producing effector Tfh cells promote B cell alloimmunity in lymph nodes and kidney allografts
Hengcheng Zhang, … , Bruce R. Blazar, Peter T. Sage
Hengcheng Zhang, … , Bruce R. Blazar, Peter T. Sage
Published October 23, 2023
Citation Information: JCI Insight. 2023;8(20):e169793. https://doi.org/10.1172/jci.insight.169793.
View: Text | PDF
Research Article Immunology Transplantation

IL-21–producing effector Tfh cells promote B cell alloimmunity in lymph nodes and kidney allografts

Abstract

Follicular helper T (Tfh) cells have been implicated in controlling rejection after allogeneic kidney transplantation, but the precise subsets, origins, and functions of Tfh cells in this process have not been fully characterized. Here we show that a subset of effector Tfh cells marked by previous IL-21 production is potently induced during allogeneic kidney transplantation and is inhibited by immunosuppressive agents. Single-cell RNA-Seq revealed that these lymph node (LN) effector Tfh cells have transcriptional and clonal overlap with IL-21–producing kidney-infiltrating Tfh cells, implicating common origins and developmental trajectories. To investigate the precise functions of IL-21–producing effector Tfh cells in LNs and allografts, we used a mouse model to selectively eliminate these cells and assessed allogeneic B cell clonal dynamics using a single B cell culture system. We found that IL-21–producing effector Tfh cells were essential for transplant rejection by regulating donor-specific germinal center B cell clonal dynamics both systemically in the draining LN and locally within kidney grafts. Thus, IL-21–producing effector Tfh cells have multifaceted roles in Ab-mediated rejection after kidney transplantation by promoting B cell alloimmunity.

Authors

Hengcheng Zhang, Cecilia B. Cavazzoni, Manuel A. Podestà, Elsa D. Bechu, Garyfallia Ralli, Pragya Chandrakar, Jeong-Mi Lee, Ismail Sayin, Stefan G. Tullius, Reza Abdi, Anita S. Chong, Bruce R. Blazar, Peter T. Sage

×

Figure 4

Transplant immunosuppression attenuates IL-21–producing Tfh cell development in LNs and grafts.

Options: View larger image (or click on image) Download as PowerPoint
Transplant immunosuppression attenuates IL-21–producing Tfh cell develop...
(A) Schematic of CTLA-4Ig or anti-CD20 administration after allogeneic kidney transplantation. (B) Frequency of B cells in dLNs of recipient mice. (C) Gating strategy (left) and quantification (right) of Tfr (gated as CD4+CD19CXCR5+ICOS+GITR+) and Tfh (gated as CD4+CD19CXCR5+ICOS+GITR) cells. (D) Quantification of IL-21–expressing Tfh cells in dLNs as a percentage of all CD4+ cells or as a total number. (E) Frequency (left) and total number (right) of IL-21–producing CD4+ T cells within kidney grafts. (F) Gating strategy (left) and frequency (right) of GC B cells from dLNs. (G) DSA IgG measurements from serum of transplanted mice. (H) Histological images of transplanted kidneys including H&E staining (top) and IF staining for C4d (bottom). Scale bars: 100 μm; original magnification: ×100. Data are combined from 2 independent experiments, n = 3–4 mice replicates per group. Student’s 2-tailed unpaired t test for 2-group comparisons for F and G, 1-way ANOVA with Tukey’s for multiple comparison for BE. *P < 0.05; **P < 0.01; ***P < 0.001.