Literature DB >> 32987195

CD4+ T cells engineered with FVIII-CAR and murine Foxp3 suppress anti-factor VIII immune responses in hemophilia a mice.

Richard Y Fu1, Alex C Chen1, Meghan J Lyle1, Chun-Yu Chen1, Chao Lien Liu1, Carol H Miao2.   

Abstract

Although protein replacement therapy provides effective treatment for hemophilia A patients, about a third of severe patients develop neutralizing inhibitor antibodies to factor VIII. Adoptive transfer of regulatory T cells (Tregs) has shown promise in treating unwanted immune responses. In previous studies, transferred polyclonal Tregs ameliorated the anti-factor VIII immune responses in hemophilia A mice. In addition, factor VIII-primed Tregs demonstrated increased suppressive function. However, antigen-specific Tregs are a small fraction of the total lymphocyte population. To generate large numbers of factor VIII-specific Tregs, the more abundant murine primary CD4+ T cells were lentivirally transduced ex vivo to express Foxp3 and a chimeric antigen receptor specific to factor VIII (F8CAR). Transduced cells significantly inhibited the proliferation of factor VIII-specific effector T cells in suppression assays. To monitor the suppressive function of the transduced chimeric antigen receptor expressing T cells in vivo, engineered CD4+CD25+Foxp3+F8CAR-Tregs were sorted and adoptively transferred into hemophilia A mice that are treated with hydrodynamically injected factor VIII plasmid. Mice receiving engineered F8CAR-Tregs showed maintenance of factor VIII clotting activity and did not develop anti-factor VIII inhibitors, while control CD4+T cell or PBS recipient mice developed inhibitors and had a sharp decrease in factor VIII activity. These results show that CD4+ cells lentivirally transduced to express Foxp3 and F8CAR can promote factor VIII tolerance in a murine model. With further development and testing, this approach could potentially be applied to human hemophilia patients.
Copyright © 2020 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  Adoptive cell therapy; Anti-factor VIII inhibitors; Antibody response; CAR-Tregs; Chimeric antigen receptor; Factor VIII; Hemophilia A; Regulatory T cells; Tolerance induction

Mesh:

Substances:

Year:  2020        PMID: 32987195      PMCID: PMC7655680          DOI: 10.1016/j.cellimm.2020.104216

Source DB:  PubMed          Journal:  Cell Immunol        ISSN: 0008-8749            Impact factor:   4.868


  49 in total

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Journal:  Blood       Date:  2001-02-15       Impact factor: 22.113

4.  Donor CD19 CAR T cells exert potent graft-versus-lymphoma activity with diminished graft-versus-host activity.

Authors:  Arnab Ghosh; Melody Smith; Scott E James; Marco L Davila; Enrico Velardi; Kimon V Argyropoulos; Gertrude Gunset; Fabiana Perna; Fabiana M Kreines; Emily R Levy; Sophie Lieberman; Hillary V Jay; Andrea Z Tuckett; Johannes L Zakrzewski; Lisa Tan; Lauren F Young; Kate Takvorian; Jarrod A Dudakov; Robert R Jenq; Alan M Hanash; Ana Carolina F Motta; George F Murphy; Chen Liu; Andrea Schietinger; Michel Sadelain; Marcel R M van den Brink
Journal:  Nat Med       Date:  2017-01-09       Impact factor: 53.440

5.  In vivo expansion of regulatory T cells with IL-2/IL-2 mAb complexes prevents anti-factor VIII immune responses in hemophilia A mice treated with factor VIII plasmid-mediated gene therapy.

Authors:  Chao-Lien Liu; Peiqing Ye; Benjamin C Yen; Carol H Miao
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Authors:  Alex C Chen; Xiaohe Cai; Chong Li; Liliane Khoryati; Marc A Gavin; Carol H Miao
Journal:  Front Immunol       Date:  2020-04-28       Impact factor: 7.561

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Journal:  Front Immunol       Date:  2021-03-29       Impact factor: 7.561

3.  CAR- and TRuC-redirected regulatory T cells differ in capacity to control adaptive immunity to FVIII.

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Review 4.  Driving CARs to BARs: The Winding Road to Specific Regulatory T Cells for Tolerance.

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Journal:  Front Immunol       Date:  2021-09-06       Impact factor: 7.561

Review 5.  CAR-T Regulatory (CAR-Treg) Cells: Engineering and Applications.

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Review 6.  Regulatory CAR-T cells in autoimmune diseases: Progress and current challenges.

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Review 7.  Emerging translational strategies and challenges for enhancing regulatory T cell therapy for graft-versus-host disease.

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  7 in total

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