TY - JOUR
T1 - Phase I trial of donor-derived modified immune cell infusion in kidney transplantation
AU - Morath, Christian
AU - Schmitt, Anita
AU - Kleist, Christian
AU - Daniel, Volker
AU - Opelz, Gerhard
AU - Süsal, Caner
AU - Ibrahim, Eman
AU - Kälble, Florian
AU - Speer, Claudius
AU - Nusshag, Christian
AU - da Silva, Luiza Pego
AU - Sommerer, Claudia
AU - Wang, Lei
AU - Ni, Ming
AU - Hückelhoven-Krauss, Angela
AU - Czock, David
AU - Merle, Uta
AU - Mehrabi, Arianeb
AU - Sander, Anja
AU - Hackbusch, Matthes
AU - Eckert, Christoph
AU - Waldherr, Rüdiger
AU - Schnitzler, Paul
AU - Müller-Tidow, Carsten
AU - Hoheisel, Jörg D.
AU - Mustafa, Shakhawan A.
AU - Alhamdani, Mohamed S.S.
AU - Bauer, Andrea S.
AU - Reiser, Jochen
AU - Zeier, Martin
AU - Schmitt, Michael
AU - Schaier, Matthias
AU - Terness, Peter
N1 - Publisher Copyright:
Copyright: © 2020, American Society for Clinical Investigation.
PY - 2020/5/1
Y1 - 2020/5/1
N2 - BACKGROUND. Preclinical experiments have shown that donor blood cells, modified in vitro by an alkylating agent (modified immune cells [MICs]), induced long-term specific immunosuppression against the allogeneic donor. METHODS. In this phase I trial, patients received either 1.5 × 106 MICs per kg BW on day -2 (n = 3, group A), or 1.5 × 108 MICs per kg BW on day -2 (n = 3, group B) or day -7 (n = 4, group C) before living donor kidney transplantation in addition to post-transplantation immunosuppression. The primary outcome measure was the frequency of adverse events (AEs) until day 30 (study phase) with follow-up out to day 360. RESULTS. MIC infusions were extremely well tolerated. During the study phase, 10 treated patients experienced a total of 69 AEs that were unlikely to be related or not related to MIC infusion. No donor-specific human leukocyte antigen Abs or rejection episodes were noted, even though the patients received up to 1.3 × 1010 donor mononuclear cells before transplantation. Group C patients with low immunosuppression during follow-up showed no in vitro reactivity against stimulatory donor blood cells on day 360, whereas reactivity against third-party cells was still preserved. Frequencies of CD19+CD24hiCD38hi transitional B lymphocytes (Bregs) increased from a median of 6% before MIC infusion to 20% on day 180, which was 19- and 68-fold higher, respectively, than in 2 independent cohorts of transplanted controls. The majority of Bregs produced the immunosuppressive cytokine IL-10. MIC-treated patients showed the Immune Tolerance Network operational tolerance signature. CONCLUSION. MIC administration was safe and could be a future tool for the targeted induction of tolerogenic Bregs. TRIAL REGISTRATION. EudraCT number: 2014-002086-30; ClinicalTrials.gov identifier: NCT02560220.
AB - BACKGROUND. Preclinical experiments have shown that donor blood cells, modified in vitro by an alkylating agent (modified immune cells [MICs]), induced long-term specific immunosuppression against the allogeneic donor. METHODS. In this phase I trial, patients received either 1.5 × 106 MICs per kg BW on day -2 (n = 3, group A), or 1.5 × 108 MICs per kg BW on day -2 (n = 3, group B) or day -7 (n = 4, group C) before living donor kidney transplantation in addition to post-transplantation immunosuppression. The primary outcome measure was the frequency of adverse events (AEs) until day 30 (study phase) with follow-up out to day 360. RESULTS. MIC infusions were extremely well tolerated. During the study phase, 10 treated patients experienced a total of 69 AEs that were unlikely to be related or not related to MIC infusion. No donor-specific human leukocyte antigen Abs or rejection episodes were noted, even though the patients received up to 1.3 × 1010 donor mononuclear cells before transplantation. Group C patients with low immunosuppression during follow-up showed no in vitro reactivity against stimulatory donor blood cells on day 360, whereas reactivity against third-party cells was still preserved. Frequencies of CD19+CD24hiCD38hi transitional B lymphocytes (Bregs) increased from a median of 6% before MIC infusion to 20% on day 180, which was 19- and 68-fold higher, respectively, than in 2 independent cohorts of transplanted controls. The majority of Bregs produced the immunosuppressive cytokine IL-10. MIC-treated patients showed the Immune Tolerance Network operational tolerance signature. CONCLUSION. MIC administration was safe and could be a future tool for the targeted induction of tolerogenic Bregs. TRIAL REGISTRATION. EudraCT number: 2014-002086-30; ClinicalTrials.gov identifier: NCT02560220.
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U2 - 10.1172/JCI133595
DO - 10.1172/JCI133595
M3 - Article
C2 - 31990685
AN - SCOPUS:85084114261
SN - 0021-9738
VL - 130
SP - 2364
EP - 2376
JO - Journal of Clinical Investigation
JF - Journal of Clinical Investigation
IS - 5
ER -