Literature DB >> 26970668

Modulation of human allogeneic and syngeneic pluripotent stem cells and immunological implications for transplantation.

S D Sackett1, M E Brown1, D M Tremmel1, T Ellis2, W J Burlingham1, J S Odorico3.   

Abstract

Tissues derived from induced pluripotent stem cells (iPSCs) are a promising source of cells for building various regenerative medicine therapies; from simply transplanting cells to reseeding decellularized organs to reconstructing multicellular tissues. Although reprogramming strategies for producing iPSCs have improved, the clinical use of iPSCs is limited by the presence of unique human leukocyte antigen (HLA) genes, the main immunologic barrier to transplantation. In order to overcome the immunological hurdles associated with allogeneic tissues and organs, the generation of patient-histocompatible iPSCs (autologous or HLA-matched cells) provides an attractive platform for personalized medicine. However, concerns have been raised as to the fitness, safety and immunogenicity of iPSC derivatives because of variable differentiation potential of different lines and the identification of genetic and epigenetic aberrations that can occur during the reprogramming process. In addition, significant cost and regulatory barriers may deter commercialization of patient specific therapies in the short-term. Nonetheless, recent studies provide some evidence of immunological benefit for using autologous iPSCs. Yet, more studies are needed to evaluate the immunogenicity of various autologous and allogeneic human iPSC-derived cell types as well as test various methods to abrogate rejection. Here, we present perspectives of using allogeneic vs. autologous iPSCs for transplantation therapies and the advantages and disadvantages of each related to differentiation potential, immunogenicity, genetic stability and tumorigenicity. We also review the current literature on the immunogenicity of syngeneic iPSCs and discuss evidence that questions the feasibility of HLA-matched iPSC banks. Finally, we will discuss emerging methods of abrogating or reducing host immune responses to PSC derivatives.
Copyright © 2016 Elsevier Inc. All rights reserved.

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Year:  2016        PMID: 26970668      PMCID: PMC4859756          DOI: 10.1016/j.trre.2016.02.001

Source DB:  PubMed          Journal:  Transplant Rev (Orlando)        ISSN: 0955-470X            Impact factor:   3.943


  122 in total

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4.  A model for personalized in vivo analysis of human immune responsiveness.

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6.  Promotion of rat cardiac allograft survival by intrathymic inoculation of donor splenocytes.

Authors:  J S Odorico; A M Posselt; A Naji; J F Markmann; C F Barker
Journal:  Transplantation       Date:  1993-05       Impact factor: 4.939

7.  Induced pluripotent stem cell-derived neural cells survive and mature in the nonhuman primate brain.

Authors:  Marina E Emborg; Yan Liu; Jiajie Xi; Xiaoqing Zhang; Yingnan Yin; Jianfeng Lu; Valerie Joers; Christine Swanson; James E Holden; Su-Chun Zhang
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Journal:  Nature       Date:  2013-01-09       Impact factor: 49.962

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Authors:  Yizhong Peng; Xiangcheng Qing; Hongyang Shu; Shuo Tian; Wenbo Yang; Songfeng Chen; Hui Lin; Xiao Lv; Lei Zhao; Xi Chen; Feifei Pu; Donghua Huang; Xu Cao; Zengwu Shao
Journal:  Biomater Transl       Date:  2021-06-28

Review 3.  Endogenous repair theory enriches construction strategies for orthopaedic biomaterials: a narrative review.

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Review 4.  Report of the Key Opinion Leaders Meeting on Stem Cell-derived Beta Cells.

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Journal:  Transplantation       Date:  2018-08       Impact factor: 4.939

Review 5.  Pluripotent-Stem-Cell-Derived Hepatic Cells: Hepatocytes and Organoids for Liver Therapy and Regeneration.

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6.  Biodegradable Poly-ε-Caprolactone Scaffolds with ECFCs and iMSCs for Tissue-Engineered Heart Valves.

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7.  Development of a liver-specific Tet-off AAV8 vector for improved safety of insulin gene therapy for diabetes.

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  7 in total

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