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Novel Function of CD4+ T Cell DEPTOR in Treg Homeostasis and Alloimmunity.

J. Wedel,1,2 S. Bruneau,1,2 K. Liu,1,2 N. Kochupurakkal,1,2 M. Laplante,3 D. Briscoe.1,2

1Division of Nephrology, Boston Children's Hospital, Boston, MA
2Transplant Research Program, Harvard Medical School, Boston, MA
3CRIUCPQ, Université
Laval, Quebec, Canada.

Meeting: 2016 American Transplant Congress

Abstract number: 568

Keywords: Lymphocytes, Mice, Rejection, T cells

Session Information

Session Name: Joint Plenary Session IV

Session Type: Plenary

Date: Wednesday, June 15, 2016

Session Time: 8:30am-10:00am

 Presentation Time: 9:00am-9:15am

Location: Veterans Auditorium

DEPTOR, a recently described modulator of PI-3K/mTOR signaling, is expressed by CD4+ T cells, and functions to modulate CD4+ Teff cell differentiation. Upon CD4+ T cell activation, intrinsic DEPTOR is degraded, which in turn decreases its negative regulation of Teff responses. We also find that forced overexpression of DEPTOR in CD4+ cells stabilizes Foxp3 expression and increases Treg function in vitro.

Here, we used a doxycycline (dox)-inducible DEPTOR transgenic mouse (rtTA+/+DEPTOR+/+, iDEP) to evaluate its effect on alloimmune Teff/Treg responses. Fully MHC mismatched BALB/c (H-2d) hearts were transplanted into C57BL/6 or iDEP recipients (both H-2b). Administration of dox to iDEP recipients resulted in a marked overexpression of DEPTOR within CD4+ cells, and was associated with a significant (p<0.001) prolongation of graft survival (MST 35 days, n=5) vs. WT recipients (MST 7 days, n=14). iDEP recipients (day 6) had a lower frequency of CD4+ TEM cells (CD44highCD62Llow) and increased numbers of CD4+Foxp3+ Tregs vs. WT recipients. CD4+ T cells from iDEP transgenic mice were also adoptively transferred into BALB/c heart transplanted Rag2-/-IL2Rγ-/- mice (H-2b) two days post-transplant. Treatment of iDEP recipients with dox again resulted in a significant prolongation of graft survival (MST 37 days, n=5 vs. 16 days in controls, n=6; p<0.01). These findings indicate that overexpression of DEPTOR in CD4+cells is immunosuppressive. We next administered anti-CD25 (PC-61, 250[micro]g on d-5, d-2 and d+2) to iDEP recipients which results in >70% depletion of CD4+Foxp3+ Tregs and evaluated graft survival. Surprisingly, the graft prolonging effect of forced DEPTOR overexpression was completely abrogated in these Treg-depleted recipients (MST 9 days, n=5). Finally, we treated recipients of fully MHC mismatched allografts (BALB/c into C57BL/6) with MLN4924 (60 mg/kg BID x 5 days) as a pharmacologic agent to inhibit DEPTOR degradation and found a similar prolongation of graft survival (MST 18 days, n=5 vs. 7 days in controls, n=3; p<0.01).

Collectively, these findings identify DEPTOR as a novel cell intrinsic immunomodulatory protein in CD4+ T cells that enhances T regulatory cell function following transplantation. These findings provide for the intriguing possibility that targeting DEPTOR degradation has promise as a future therapeutic.

CITATION INFORMATION: Wedel J, Bruneau S, Liu K, Kochupurakkal N, Laplante M, Briscoe D. Novel Function of CD4+ T Cell DEPTOR in Treg Homeostasis and Alloimmunity. Am J Transplant. 2016;16 (suppl 3).

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To cite this abstract in AMA style:

Wedel J, Bruneau S, Liu K, Kochupurakkal N, Laplante M, Briscoe D. Novel Function of CD4+ T Cell DEPTOR in Treg Homeostasis and Alloimmunity. [abstract]. Am J Transplant. 2016; 16 (suppl 3). https://atcmeetingabstracts.com/abstract/novel-function-of-cd4-t-cell-deptor-in-treg-homeostasis-and-alloimmunity/. Accessed May 11, 2025.

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