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Donor bone marrow together with recipient regulatory T cells induces chimerism without irradiation in kidney transplantation

免疫抑制 医学 移植 肾移植 贝拉塔克普 免疫学 T细胞 骨髓 细胞疗法 细胞 临床试验 免疫系统 B细胞 体外 多克隆抗体 移植嵌合体 癌症研究 组织相容性试验 免疫耐受 骨髓移植 受体 T淋巴细胞 免疫原性 移植排斥反应
作者
Thomas Wekerle,Moritz Muckenhuber,Andreas Heinzel,Anna Marianne Weijler,Ana F. David,Verena Kainz,Karin Hu,Jasmin Mucha,Konstantinos Mengrelis,Roman Reindl‐Schwaighofer,Georg A. Böhmig,Bruno Watschinger,Georg Gyöeri,Thomas Soliman,Andreas Salat,Christoph Schwarz,Marlena Muhm,Georg Heinze,Michael Wolzt,Nina Worel
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science]
卷期号:18 (854)
标识
DOI:10.1126/scitranslmed.aee6850
摘要

Cotransplantation of donor bone marrow (BM) has yielded a therapeutic benefit in clinical trials of kidney transplantation by inducing chimerism-based tolerance, but this was dependent on unfavorable recipient irradiation. Additional regulatory T (T reg ) cell administration can overcome the need for myelosuppression, but this has been demonstrated only in mice so far. Here, we conducted a controlled, phase 1/2a trial of combined BM and T reg cell therapy in HLA-mismatched living-donor kidney transplantation (NCT03867617). Six patients received polyclonal recipient T reg cells and donor BM cells (BMCs) immediately posttransplant. Immunosuppression consisted of thymoglobulin, belatacept, sirolimus, steroids, and short-course tocilizumab. The control group received no T reg cells, BMCs, or tocilizumab. Total leukocyte donor chimerism was detected across all patients in the study group posttransplantation. This was not observed in any patient belonging to the control group, consequently meeting the primary end point of higher chimerism levels in the study versus control groups ( P = 0.001). Chimerism was observed across multiple lineages, with up to 4% in T cells. For three patients in the study group, immunosuppression could be minimized to belatacept monotherapy. Antidonor reactivity was decreased in in vitro T cell proliferation assays, suggesting specific downmodulation of the antidonor T cell response. In addition, expansion of antidonor T cell clones was shown by T cell receptor sequencing analysis to be dampened in the study versus control groups. This trial serves as a proof of concept for a combination cell therapy that induces chimerism-based immunomodulation in kidney transplantation without the need for irradiation.

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