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Efficacy of intracellular immune checkpoint-silenced DC vaccine

BACKGROUND. DC-based tumor vaccines have had limited clinical success thus far. SOCS1, a key inhibitor of inflammatory cytokine signaling, is an immune checkpoint regulator that limits DC immunopotency. METHODS. We generated a genetically modified DC (gmDC) vaccine to perform immunotherapy. The aden...

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Autores principales: Wang, Danhong, Huang, Xue F., Hong, Bangxing, Song, Xiao-Tong, Hu, Liangding, Jiang, Min, Zhang, Bin, Ning, Hongmei, Li, Yuhang, Xu, Chen, Lou, Xiao, Li, Botao, Yu, Zhiyong, Hu, Jiangwei, Chen, Jianlin, Yang, Fan, Gao, Haiyan, Ding, Guoliang, Liao, Lianming, Rollins, Lisa, Jones, Lindsey, Chen, Si-Yi, Chen, Hu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Clinical Investigation 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5821183/
https://www.ncbi.nlm.nih.gov/pubmed/29415891
http://dx.doi.org/10.1172/jci.insight.98368
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author Wang, Danhong
Huang, Xue F.
Hong, Bangxing
Song, Xiao-Tong
Hu, Liangding
Jiang, Min
Zhang, Bin
Ning, Hongmei
Li, Yuhang
Xu, Chen
Lou, Xiao
Li, Botao
Yu, Zhiyong
Hu, Jiangwei
Chen, Jianlin
Yang, Fan
Gao, Haiyan
Ding, Guoliang
Liao, Lianming
Rollins, Lisa
Jones, Lindsey
Chen, Si-Yi
Chen, Hu
author_facet Wang, Danhong
Huang, Xue F.
Hong, Bangxing
Song, Xiao-Tong
Hu, Liangding
Jiang, Min
Zhang, Bin
Ning, Hongmei
Li, Yuhang
Xu, Chen
Lou, Xiao
Li, Botao
Yu, Zhiyong
Hu, Jiangwei
Chen, Jianlin
Yang, Fan
Gao, Haiyan
Ding, Guoliang
Liao, Lianming
Rollins, Lisa
Jones, Lindsey
Chen, Si-Yi
Chen, Hu
author_sort Wang, Danhong
collection PubMed
description BACKGROUND. DC-based tumor vaccines have had limited clinical success thus far. SOCS1, a key inhibitor of inflammatory cytokine signaling, is an immune checkpoint regulator that limits DC immunopotency. METHODS. We generated a genetically modified DC (gmDC) vaccine to perform immunotherapy. The adenovirus (Ad-siSSF) delivers two tumor-associated antigens (TAAs), survivin and MUC1; secretory bacterial flagellin for DC maturation; and an RNA interference moiety to suppress SOCS1. A 2-stage phase I trial was performed for patients with relapsed acute leukemia after allogenic hematopoietic stem cell transplantation: in stage 1, we compared the safety and efficacy between gmDC treatment (23 patients) and standard donor lymphocyte infusion (25 patients); in stage 2, we tested the efficacy of the gmDC vaccine for 12 acute myeloid leukemia (AML) patients with early molecular relapse. RESULTS. gmDCs elicited potent TAA-specific CTL responses in vitro, and the immunostimulatory activity of gmDC vaccination was demonstrated in rhesus monkeys. A stage 1 study established that this combinatory gmDC vaccine is safe in acute leukemia patients and yielded improved survival rate. In stage 2, we observed a complete remission rate of 83% in 12 relapsed AML patients. Overall, no grade 3 or grade 4 graft-versus-host disease incidence was detected in any of the 35 patients enrolled. CONCLUSIONS. This study, with combinatory modifications in DCs, demonstrates the safety and efficacy of SOCS1-silenced DCs in treating relapsed acute leukemia. TRIAL REGISTRATION. ClinicalTrials.gov NCT01956630. FUNDING. National Institute of Health (R01CA90427); the Key New Drug Development and Manufacturing Program of the “Twelfth Five-Year Plan” of China (2011ZX09102-001-29); and Clinical Application Research of Beijing (Z131107002213148).
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spelling pubmed-58211832018-03-09 Efficacy of intracellular immune checkpoint-silenced DC vaccine Wang, Danhong Huang, Xue F. Hong, Bangxing Song, Xiao-Tong Hu, Liangding Jiang, Min Zhang, Bin Ning, Hongmei Li, Yuhang Xu, Chen Lou, Xiao Li, Botao Yu, Zhiyong Hu, Jiangwei Chen, Jianlin Yang, Fan Gao, Haiyan Ding, Guoliang Liao, Lianming Rollins, Lisa Jones, Lindsey Chen, Si-Yi Chen, Hu JCI Insight Clinical Medicine BACKGROUND. DC-based tumor vaccines have had limited clinical success thus far. SOCS1, a key inhibitor of inflammatory cytokine signaling, is an immune checkpoint regulator that limits DC immunopotency. METHODS. We generated a genetically modified DC (gmDC) vaccine to perform immunotherapy. The adenovirus (Ad-siSSF) delivers two tumor-associated antigens (TAAs), survivin and MUC1; secretory bacterial flagellin for DC maturation; and an RNA interference moiety to suppress SOCS1. A 2-stage phase I trial was performed for patients with relapsed acute leukemia after allogenic hematopoietic stem cell transplantation: in stage 1, we compared the safety and efficacy between gmDC treatment (23 patients) and standard donor lymphocyte infusion (25 patients); in stage 2, we tested the efficacy of the gmDC vaccine for 12 acute myeloid leukemia (AML) patients with early molecular relapse. RESULTS. gmDCs elicited potent TAA-specific CTL responses in vitro, and the immunostimulatory activity of gmDC vaccination was demonstrated in rhesus monkeys. A stage 1 study established that this combinatory gmDC vaccine is safe in acute leukemia patients and yielded improved survival rate. In stage 2, we observed a complete remission rate of 83% in 12 relapsed AML patients. Overall, no grade 3 or grade 4 graft-versus-host disease incidence was detected in any of the 35 patients enrolled. CONCLUSIONS. This study, with combinatory modifications in DCs, demonstrates the safety and efficacy of SOCS1-silenced DCs in treating relapsed acute leukemia. TRIAL REGISTRATION. ClinicalTrials.gov NCT01956630. FUNDING. National Institute of Health (R01CA90427); the Key New Drug Development and Manufacturing Program of the “Twelfth Five-Year Plan” of China (2011ZX09102-001-29); and Clinical Application Research of Beijing (Z131107002213148). American Society for Clinical Investigation 2018-02-08 /pmc/articles/PMC5821183/ /pubmed/29415891 http://dx.doi.org/10.1172/jci.insight.98368 Text en http://creativecommons.org/licenses/by/4.0/ This work is licensed under the Creative Commons Attribution 4.0 International License. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/.
spellingShingle Clinical Medicine
Wang, Danhong
Huang, Xue F.
Hong, Bangxing
Song, Xiao-Tong
Hu, Liangding
Jiang, Min
Zhang, Bin
Ning, Hongmei
Li, Yuhang
Xu, Chen
Lou, Xiao
Li, Botao
Yu, Zhiyong
Hu, Jiangwei
Chen, Jianlin
Yang, Fan
Gao, Haiyan
Ding, Guoliang
Liao, Lianming
Rollins, Lisa
Jones, Lindsey
Chen, Si-Yi
Chen, Hu
Efficacy of intracellular immune checkpoint-silenced DC vaccine
title Efficacy of intracellular immune checkpoint-silenced DC vaccine
title_full Efficacy of intracellular immune checkpoint-silenced DC vaccine
title_fullStr Efficacy of intracellular immune checkpoint-silenced DC vaccine
title_full_unstemmed Efficacy of intracellular immune checkpoint-silenced DC vaccine
title_short Efficacy of intracellular immune checkpoint-silenced DC vaccine
title_sort efficacy of intracellular immune checkpoint-silenced dc vaccine
topic Clinical Medicine
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5821183/
https://www.ncbi.nlm.nih.gov/pubmed/29415891
http://dx.doi.org/10.1172/jci.insight.98368
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