Mechanisms that mediate allograft tolerance differ between organs. We have previously shown that Foxp3+ T cell-enriched bronchus-associated lymphoid tissue (BALT) is induced in tolerant murine lung allografts and that these Foxp3+ cells suppress alloimmune responses locally and systemically. Here, we demonstrated that Foxp3+ cells that reside in tolerant lung allografts differed phenotypically and transcriptionally from those in the periphery and were clonally expanded. Using a mouse lung retransplant model, we showed that recipient Foxp3+ cells were continuously recruited to the BALT within tolerant allografts. We identified distinguishing features of graft-resident and newly recruited Foxp3+ cells and showed that graft-infiltrating Foxp3+ cells acquired transcriptional profiles resembling those of graft-resident Foxp3+ cells over time. Allografts underwent combined antibody-mediated rejection and acute cellular rejection when recruitment of recipient Foxp3+ cells was prevented. Finally, we showed that local administration of IL-33 could expand and activate allograft-resident Foxp3+ cells, providing a platform for the design of tolerogenic therapies for lung transplant recipients. Our findings establish graft-resident Foxp3+ cells as critical orchestrators of lung transplant tolerance and highlight the need to develop lung-specific immunosuppression.
Maintenance of graft tissue-resident Foxp3+ cells is necessary for lung transplant tolerance in mice.
维持移植组织中驻留的 Foxp3+ 细胞对于小鼠肺移植耐受性是必要的
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作者:Li Wenjun, Terada Yuriko, Bai Yun Zhu, Yokoyama Yuhei, Shepherd Hailey M, Amrute Junedh M, Bery Amit I, Liu Zhiyi, Gauthier Jason M, Terekhova Marina, Bharat Ankit, Ritter Jon H, Puri Varun, Hachem Ramsey R, Turnquist HÄth R, Sage Peter T, Alessandrini Alessandro, Artyomov Maxim N, Lavine Kory J, Nava Ruben G, Krupnick Alexander S, Gelman Andrew E, Kreisel Daniel
| 期刊: | Journal of Clinical Investigation | 影响因子: | 13.600 |
| 时间: | 2025 | 起止号: | 2025 Mar 18; 135(10):e178975 |
| doi: | 10.1172/JCI178975 | 研究方向: | 细胞生物学 |
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