Lymphatic drainage from bronchus-associated lymphoid tissue in tolerant lung allografts promotes peripheral tolerance
Wenjun Li, … , Andrew E. Gelman, Daniel Kreisel
Wenjun Li, … , Andrew E. Gelman, Daniel Kreisel
Published November 16, 2020
Citation Information: J Clin Invest. 2020;130(12):6718-6727. https://doi.org/10.1172/JCI136057.
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Research Article Vascular biology

Lymphatic drainage from bronchus-associated lymphoid tissue in tolerant lung allografts promotes peripheral tolerance

Abstract

Tertiary lymphoid organs are aggregates of immune and stromal cells including high endothelial venules and lymphatic vessels that resemble secondary lymphoid organs and can be induced at nonlymphoid sites during inflammation. The function of lymphatic vessels within tertiary lymphoid organs remains poorly understood. During lung transplant tolerance, Foxp3+ cells accumulate in tertiary lymphoid organs that are induced within the pulmonary grafts and are critical for the local downregulation of alloimmune responses. Here, we showed that tolerant lung allografts could induce and maintain tolerance of heterotopic donor-matched hearts through pathways that were dependent on the continued presence of the transplanted lung. Using lung retransplantation, we showed that Foxp3+ cells egressed from tolerant lung allografts via lymphatics and were recruited into donor-matched heart allografts. Indeed, survival of the heart allografts was dependent on lymphatic drainage from the tolerant lung allograft to the periphery. Thus, our work indicates that cellular trafficking from tertiary lymphoid organs regulates immune responses in the periphery. We propose that these findings have important implications for a variety of disease processes that are associated with the induction of tertiary lymphoid organs.

Authors

Wenjun Li, Jason M. Gauthier, Alice Y. Tong, Yuriko Terada, Ryuji Higashikubo, Christian C. Frye, Margaret S. Harrison, Kohei Hashimoto, Amit I. Bery, Jon H. Ritter, Ruben G. Nava, Varun Puri, Brian W. Wong, Kory J. Lavine, Ankit Bharat, Alexander S. Krupnick, Andrew E. Gelman, Daniel Kreisel

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Figure 3

Peripheral tolerance is associated with exit of Foxp3+ cells from tolerant lung allograft.

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Peripheral tolerance is associated with exit of Foxp3+ cells from tolera...
(A) Schematic diagram depicting experimental transplant model. Intravital 2-photon imaging of (B) BALB/c cardiac allograft (n = 3) and (C) retransplanted (Retxp) tolerant BALB/c lung allograft (n = 3) 6 days after transplantation of BALB/c heart into B6 mouse into which a tolerant BALB/c lung was retransplanted at least 21 days prior (Foxp3+ cells: green; quantum dot–labeled [q-dot–labeled] vessels: red; second harmonic generation [SHG]: blue). The BALB/c lung had been originally transplanted into a B6 Foxp3 IRES-GFP mouse (treated with perioperative costimulatory blockade) at least 30 days before the retransplant procedure. (D) Kaplan-Meier survival curves of BALB/c hearts (▲) that were transplanted into B6 recipients that received perioperative costimulatory blockade (n = 5) or (●) that were transplanted into nonimmunosuppressed B6 mice that received tolerant BALB/c pulmonary allografts at least 21 days before cardiac transplantation (n = 7). The BALB/c lungs had been originally engrafted into B6 mice that received perioperative costimulatory blockade and then retransplanted at least 30 days later. (E) Histological appearance (H&E) of long-term-surviving BALB/c hearts after transplantation into B6 mice into which a tolerant BALB/c lung allograft was retransplanted at least 21 days prior. Scale bars: 30 μm (B and C) and 100 μm (E).