Literature DB >> 11544341

An antagonist IL-15/Fc protein prevents costimulation blockade-resistant rejection.

S Ferrari-Lacraz1, X X Zheng, Y S Kim, Y Li, W Maslinski, X C Li, T B Strom.   

Abstract

IL-15 is a powerful T cell growth factor (TCGF) with particular importance for the maintenance of CD8(+) T cells. Because costimulation blockade does not result in universal tolerance, we hypothesized that "escape" from costimulation blockade might represent a CD8(+) and IL-15/IL-15R(+)-dependent process. For this analysis, we have used an IL-15 mutant/Fcgamma2a protein, a potentially cytolytic protein that is also a high-affinity receptor site specific antagonist for the IL-15Ralpha receptor protein, as a therapeutic agent. The IL-15-related fusion protein was used as monotherapy or in combination with CTLA4/Fc in murine islet allograft models. As monotherapies, CTLA4/Fc and an IL-15 mutant/Fcgamma2a were comparably effective in a semiallogeneic model system, and combined treatment with IL-15 mutant/Fcgamma2a plus CTLA4/Fc produced universal permanent engraftment. In a fully MHC-mismatched strain combination known to be refractory to costimulation blockade treatment, combined treatment with both fusion proteins proved to be highly effective; >70% of recipients were tolerized. The analysis revealed that the IL-15 mutant/Fc treatment confers partial protection from both CD4(+) and CD8(+) T cell graft infiltration. In rejections occurring despite CTLA4/Fc treatment, concomitant treatment with the IL-15 mutant/Fcgamma2a protein blocked a CD8(+) T cell-dominated rejection processes. This protection was linked to a blunted proliferative response of alloreactive T cells as well silencing of CTL-related gene expression events. Hence, we have demonstrated that targeting the IL-15/IL-15R pathway represents a new and potent strategy to prevent costimulation blockade-resistant CD8(+) T cell-driven rejection.

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Year:  2001        PMID: 11544341      PMCID: PMC3806296          DOI: 10.4049/jimmunol.167.6.3478

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  37 in total

1.  CD40 ligand blockade induces CD4+ T cell tolerance and linked suppression.

Authors:  K Honey; S P Cobbold; H Waldmann
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Authors:  J Trambley; A W Bingaman; A Lin; E T Elwood; S Y Waitze; J Ha; M M Durham; M Corbascio; S R Cowan; T C Pearson; C P Larsen
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Authors:  Y Li; X C Li; X X Zheng; A D Wells; L A Turka; T B Strom
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Authors:  K A Newell; G He; Z Guo; O Kim; G L Szot; I Rulifson; P Zhou; J Hart; J R Thistlethwaite; J A Bluestone
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5.  IL-2 and IL-4 double knockout mice reject islet allografts: a role for novel T cell growth factors in allograft rejection.

Authors:  X C Li; P Roy-Chaudhury; W W Hancock; R Manfro; M S Zand; Y Li; X X Zheng; P W Nickerson; J Steiger; T R Malek; T B Strom
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6.  Targeting the IL-15 receptor with an antagonist IL-15 mutant/Fc gamma2a protein blocks delayed-type hypersensitivity.

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Review 7.  CD40 and CD154 in cell-mediated immunity.

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8.  Treatment of allograft recipients with donor-specific transfusion and anti-CD154 antibody leads to deletion of alloreactive CD8+ T cells and prolonged graft survival in a CTLA4-dependent manner.

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10.  Secondary but not primary T cell responses are enhanced in CTLA-4-deficient CD8+ T cells.

Authors:  C A Chambers; T J Sullivan; T Truong; J P Allison
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3.  Eomesodermin(lo) CTLA4(hi) Alloreactive CD8+ Memory T Cells Are Associated With Prolonged Renal Transplant Survival Induced by Regulatory Dendritic Cell Infusion in CTLA4 Immunoglobulin-Treated Nonhuman Primates.

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5.  CD8(+) T cells resistant to costimulatory blockade are controlled by an antagonist interleukin-15/Fc protein.

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Review 6.  Cellular therapies for type 1 diabetes.

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7.  IL-15 induces alloreactive CD28(-) memory CD8 T cell proliferation and CTLA4-Ig resistant memory CD8 T cell activation.

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8.  Prolonged survival of allogeneic islets in cynomolgus monkeys after short-term triple therapy.

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Review 9.  Targeting cytokines beyond tumor necrosis factor-alpha and interleukin-1 in rheumatoid arthritis.

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10.  Molecular characterization and functional activity of an IL-15 antagonist MutIL-15/Fc human fusion protein.

Authors:  Xiaoyi Yang; Abraham Kallarakal; Nirmala Saptharishi; Hengguang Jiang; Zhiwen Yang; Yueqing Xie; George Mitra; Xin Xiao Zheng; Terry B Strom; Gopalan Soman
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