Haploidentical mixed chimerism cures autoimmunity in established type 1 diabetic mice
Yuqing Liu, Xiaoqi Wang, Yongping Zhu, Mingfeng Zhang, Ubaydah Nasri, Sharne S. Sun, Stephen J. Forman, Arthur D. Riggs, Xi Zhang, Defu Zeng
Yuqing Liu, Xiaoqi Wang, Yongping Zhu, Mingfeng Zhang, Ubaydah Nasri, Sharne S. Sun, Stephen J. Forman, Arthur D. Riggs, Xi Zhang, Defu Zeng
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Research Article Autoimmunity

Haploidentical mixed chimerism cures autoimmunity in established type 1 diabetic mice

Abstract

Clinical trials are currently testing whether induction of haploidentical mixed chimerism (Haplo-MC) induces organ transplantation tolerance. Whether Haplo-MC can be used to treat established autoimmune diseases remains unknown. Here, we show that established autoimmunity in euthymic and adult-thymectomized NOD (H-2g7) mice was cured by induction of Haplo-MC under a non-myeloablative anti-thymocyte globulin–based conditioning regimen and infusion of CD4+ T cell–depleted hematopoietic graft from H-2b/g7 F1 donors that expressed autoimmune-resistant H-2b or from H-2s/g7 F1 donors that expressed autoimmune-susceptible H-2s. The cure was associated with enhanced thymic negative selection, increased thymic Treg (tTreg) production, and anergy or exhaustion of residual host-type autoreactive T cells in the periphery. The peripheral tolerance was accompanied by expansion of donor- and host-type CD62L–Helios+ tTregs as well as host-type Helios–Nrp1+ peripheral Tregs (pTregs) and PD-L1hi plasmacytoid DCs (pDCs). Depletion of donor- or host-type Tregs led to reduction of host-type PD-L1hi pDCs and recurrence of autoimmunity, whereas PD-L1 deficiency in host-type DCs led to reduction of host-type pDCs and Helios–Nrp1+ pTregs. Thus, induction of Haplo-MC reestablished both central and peripheral tolerance through mechanisms that depend on allo-MHC+ donor-type DCs, PD-L1hi host-type DCs, and the generation and persistence of donor- and host-type tTregs and pTregs.

Authors

Yuqing Liu, Xiaoqi Wang, Yongping Zhu, Mingfeng Zhang, Ubaydah Nasri, Sharne S. Sun, Stephen J. Forman, Arthur D. Riggs, Xi Zhang, Defu Zeng

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Figure 11

Percentage and surface receptor changes of donor- or host-type Tregs after depletion of host- or donor-type Tregs.

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Percentage and surface receptor changes of donor- or host-type Tregs aft...
Three weeks after depletion of Tregs by DT injection as described in Figure 9, percentage and surface receptors of donor- or host-type Tregs in the spleen (SPL) and PancLNs of NOD mice with H-2b/g7 Haplo-MC were measured. (A and B) Representative pattern and mean ± SEM of percentage of host-type Tregs among host-type CD4+ Tcon cells as well as expression levels of CTLA-4, ICOS, and GITR on host-type Tregs in the spleen and PancLNs of Haplo-MC NOD mice with or without depletion of donor-type Tregs (n = 6–9). (C and D) Representative pattern and mean ± SEM of percentage of donor-type Tregs among donor-type CD4+ Tcon cells as well as expression levels of CTLA-4, ICOS, and GITR on donor-type Tregs in spleen and PancLNs of Haplo-MC NOD mice with or without depletion of host-type Treg depletion (n = 6–9). P values were calculated using unpaired 2-tailed Student’s t tests; *P < 0.05, **P < 0.01.