Stem cell transplantation impairs dendritic cell trafficking and herpesvirus immunity
Carol A. Wilke, … , Bethany B. Moore, Xiaofeng Zhou
Carol A. Wilke, … , Bethany B. Moore, Xiaofeng Zhou
Published September 3, 2019
Citation Information: JCI Insight. 2019;4(18):e130210. https://doi.org/10.1172/jci.insight.130210.
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Research Article Immunology Inflammation

Stem cell transplantation impairs dendritic cell trafficking and herpesvirus immunity

Abstract

Long-term survivors after hematopoietic stem cell transplantation are at high risk of infection, which accounts for one-third of all deaths related to stem cell transplantation. Little is known about the cause of inferior host defense after immune cell reconstitution. Here, we exploited a murine syngeneic BM transplantation (BMT) model of late infection with murine gammaherpesvirus 68 (MHV-68) to determine the role of conventional DC (cDC) trafficking in adaptive immunity in BMT mice. After infection, the expression of chemokine Ccl21 in the lung is reduced and the migration of cDCs into lung draining lymph nodes (dLNs) is impaired in BMT mice, limiting the opportunity for cDCs to prime Th cells in the dLNs. While cDC subsets are redundant in priming Th1 cells, Notch2 functions in cDC2s are required for priming increased Th17 responses in BMT mice, and cDC1s can lessen this activity. Importantly, Th17 cells can be primed both in the lungs and dLNs, allowing for increased Th17 responses without optimum cDC trafficking in BMT mice. Taken together, impaired cDC trafficking in BMT mice reduces protective Th1 responses and allows increased pathogenic Th17 responses. Thus, we have revealed a previously unknown mechanism for BMT procedures to cause long-term inferior immune responses to herpes viral infection.

Authors

Carol A. Wilke, Mathew M. Chadwick, Paul R. Chan, Bethany B. Moore, Xiaofeng Zhou

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Figure 3

Th cell differentiation and cellularity in dLNs are correlated with DC migration phenotypes in non-BMT or BMT mice.

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Th cell differentiation and cellularity in dLNs are correlated with DC m...
(A) Absolute numbers IFN-γ+ Th1 cells per dLN and percent of Th1 cells among CD4+ T cells (pregated for CD45+CD90.2+CD3+CD4+). (B) Absolute numbers of IL-17A+ Th17 cells per dLN and percent of Th17 cells among CD4+ T cells. (C) Total cell numbers of dLNs of non-BMT or BMT mice at 7 dpi with MHV-68 were determined by hemocytometer counting. The absolute numbers of mDCs, CD4+ Th, CD8+ T, and B cells per dLN were determined by total dLN cell numbers and percentage of flow cytometry based on cell surface markers. Mean ± SEM is shown for all panels and n = 5 for each group. Similar results were obtained in 2 additional experiments. Symbols represent individual mouse data points. ***P < 0.001; ****P < 0.0001, Student’s t test (2 tailed). BMT, BM transplantation; dLN, draining lymph node; mDC, migratory DC.