Autoimmunity As a Target for Chimeric Immune Receptor Therapy: A New Vision to Therapeutic Potential

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Autoimmunity As a Target for Chimeric Immune Receptor Therapy: A New Vision to Therapeutic Potential Publisher Pubmed

Haddadi MH^{1, 5} ; Hajizadehsaffar E⁵ ; Khosravimaharlooei M² ; Basiri M³ ; Negahdari B¹ ; Baharvand H^{3, 4}

Show Affiliations

1. Department of Medical Biotechnology, School of Advanced Technologies in Medicine, Tehran University of Medical Sciences, Tehran, Iran
2. Columbia Center for Translational Immunology, Department of Medicine, Columbia University College of Physicians and Surgeons, New York, NY, United States
3. Department of Stem Cells and Developmental Biology, Cell Science Research Center, Royan Institute for Stem Cell Biology and Technology, ACECR, Tehran, Iran
4. Department of Developmental Biology, University of Science and Culture, Tehran, Iran
5. Department of Regenerative Medicine, Cell Science Research Center, Royan Institute for Stem Cell Biology and Technology, ACECR, Tehran, Iran

Source: Blood Reviews Published:2020

Abstract

Chimeric immune receptors (CIRs) are functionally pleiotropic because they are artificially expressed on diverse cell types, which gives specificity to their function to anergize, kill, or protect cognate target cells. CIRs consist of chimeric antigen receptors (CARs) and B-cell antibody receptor (BAR) or chimeric autoantibody receptors (CAARs). Approval of CAR-T cell therapy by the Food and Drug Administration (FDA) has encouraged investigators to search for autoimmune therapies that are CIR-based. Both T effector cells, particularly CD8+, and T CD4+ regulatory cells (Tregs) can be engineered through CIR expression. Recently, natural killer cells have been included to increase efficiency. Unwanted antibody producer B cells are effectively prevented by CAAR-T cells, B-cell antibody receptor (BAR)-T CD8+, and BAR-Treg, which represents an advantage in antibody-mediated diseases such as pemphigus vulgaris (PV) and hemophilia A. Although CAAR and BAR-T cells may have curative benefits for autoantibody-mediated immune diseases, verification of long-term efficacy and safety are a priority before clinical use. Effective CIR-T cell therapy largely depends on the reliability and stability of the receptor. Based on CIR functionality, factors that explicitly determine effectiveness of the treatment should be considered. These factors include antigen/autoantibody specificity, single chain variable fragment (scFv) affinity, and autoantibody masking. Herein, we review the current evidence of CIR therapy with a focus on their therapeutic potential for autoimmune diseases and their challenges. © 2019 Elsevier Ltd

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Style	Citing Format
MLA	Haddadi MH, et al.. "Autoimmunity As a Target for Chimeric Immune Receptor Therapy: A New Vision to Therapeutic Potential." Blood Reviews, vol. 41, no. , 2020, pp. -.
APA	Haddadi MH, Hajizadehsaffar E, Khosravimaharlooei M, Basiri M, Negahdari B, Baharvand H (2020). Autoimmunity As a Target for Chimeric Immune Receptor Therapy: A New Vision to Therapeutic Potential. Blood Reviews, 41(), -.
Chicago	Haddadi MH, Hajizadehsaffar E, Khosravimaharlooei M, Basiri M, Negahdari B, Baharvand H. "Autoimmunity As a Target for Chimeric Immune Receptor Therapy: A New Vision to Therapeutic Potential." Blood Reviews 41, no. (2020): -.
Harvard	Haddadi MH et al. (2020) 'Autoimmunity As a Target for Chimeric Immune Receptor Therapy: A New Vision to Therapeutic Potential', Blood Reviews, 41(), pp. -.
Vancouver	Haddadi MH, Hajizadehsaffar E, Khosravimaharlooei M, Basiri M, Negahdari B, Baharvand H. Autoimmunity As a Target for Chimeric Immune Receptor Therapy: A New Vision to Therapeutic Potential. Blood Reviews. 2020;41():-.
BibTex	@article{ author = {Haddadi MH and Hajizadehsaffar E and Khosravimaharlooei M and Basiri M and Negahdari B and Baharvand H}, title = {Autoimmunity As a Target for Chimeric Immune Receptor Therapy: A New Vision to Therapeutic Potential}, journal = {Blood Reviews}, volume = {41}, number = {}, pages = {-}, year = {2020} }
RIS	TY - JOUR AU - Haddadi MH AU - Hajizadehsaffar E AU - Khosravimaharlooei M AU - Basiri M AU - Negahdari B AU - Baharvand H TI - Autoimmunity As a Target for Chimeric Immune Receptor Therapy: A New Vision to Therapeutic Potential JO - Blood Reviews VL - 41 IS - SP - EP - PY - 2020 ER -

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