Literature DB >> 30768842

Characterization, biology, and expansion of regulatory T cells in the Cynomolgus macaque for preclinical studies.

Paula Alonso-Guallart1, Jonah S Zitsman1, Jeffrey Stern1, Sigal B Kofman1, David Woodland1, Siu-Hong Ho1, Hugo P Sondermeijer1,2, Leo Bühler3, Adam Griesemer1,4, Megan Sykes1,4,5, Raimon Duran-Struuck1,6.   

Abstract

Reliable in vitro expansion protocols of regulatory T cells (Tregs) are needed for clinical use. We studied the biology of Mauritian Cynomolgus macaque (MCM) Tregs and developed four in vitro Treg expansion protocols for translational studies. Tregs expanded 3000-fold when artificial antigen presenting cells (aAPCs) expressing human CD80, CD58 and CD32 were used throughout the culture. When donor peripheral blood mononuclear cells (PBMCs) were used as the single source of APCs followed by aAPCs, Tregs expanded 2000-fold. Tregs from all protocols suppressed the proliferation of anti-CD2CD3CD28 bead-stimulated autologous PBMCs albeit with different potencies, varying from 1:2-1:4 Treg:PBMC ratios, up to >1:32. Reculture of cryopreserved Tregs permitted reexpansion with improved suppressive activity. Occasionally, CD8 contamination was observed and resolved by resorting. Specificity studies showed greater suppression of stimulation by anti-CD2CD3CD28 beads of PBMCs from the same donor used for stimulation during the Treg cultures and of autologous cells than of third-party PBMC responders. Similar to humans, the Treg-specific demethylated region (TSDR) within the Foxp3 locus correlated with suppressive activity and expression of Foxp3. Contrary to humans, FoxP3 expression did not correlate with CD45RA or CD127 expression. In summary, we have characterized MCM Tregs and developed four Treg expansion protocols that can be used for preclinical applications.
© 2019 The American Society of Transplantation and the American Society of Transplant Surgeons.

Entities:  

Keywords:  animal models: nonhuman primate; basic (laboratory) research/science; cellular transplantation (nonislet); graft survival; immune regulation; immunobiology; immunosuppression/immune modulation; tolerance: chimerism; translational research/science

Year:  2019        PMID: 30768842      PMCID: PMC6658340          DOI: 10.1111/ajt.15313

Source DB:  PubMed          Journal:  Am J Transplant        ISSN: 1600-6135            Impact factor:   8.086


  38 in total

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5.  Large-scale in vitro expansion of polyclonal human CD4(+)CD25high regulatory T cells.

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Review 7.  The role of IL-10 and TGF-beta in the differentiation and effector function of T regulatory cells.

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9.  Human cd25(+)cd4(+) t regulatory cells suppress naive and memory T cell proliferation and can be expanded in vitro without loss of function.

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10.  The role of regulatory T cells in antigen-induced arthritis: aggravation of arthritis after depletion and amelioration after transfer of CD4+CD25+ T cells.

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