Modified amino acid copolymers suppress myelin basic protein 85–99-induced encephalomyelitis in humanized mice through different effects on T cells

Illés, Zsolt; Stern, Joel N. H.; Reddy, Jay; Waldner, Hanspeter; Mycko, Marcin P.; Brosnan, Celia F.; Ellmerich, Stéphan; Altmann, Daniel M.; Santambrogio, Laura; Strominger, Jack L.; Kuchroo, Vijay K.

doi:10.1073/pnas.0403833101

Cited by 37 publications

(45 citation statements)

References 37 publications

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“…2A Left). Likewise, in the mice immunized with J3 or J5 alone a lower response was induced suggesting, by analogy to responses to copolymers (30), that the non-tg, endogenous T cells (that represent Ϸ70% of the T cells in the humanized mice) might have responded to these peptides presented by HLA-DR2. However, a negligible response to J2 (that bound weakly) was seen.…”

Section: Inhibition By Synthetic Peptide 15-mers Of Il-2 Secretion By Anmentioning

confidence: 99%

“…Proliferative responses were measured as described in refs. 17 (17,29,30), peptide synthesis (13), isolation of empty HLA-DR2 (12,13), inhibition by peptide 15-mers of MBP 85-99 binding to HLA-DR2 (DRA͞DRB1*1501) (13,17), sorting of tg and endogenous (non-tg) T cells from humanized mice by flow cytometry (30), cytokine measurement by ELISA (30), and detection of PLP 139-151-reactive CD4 ϩ T cells by using I-A s ͞PLP 139-151 tetramers (31,32). (11,17).…”

Section: Methodsmentioning

confidence: 99%

“…As a negative control, Nase 101-120 peptide, which also binds I-A s , was used. To determine the proliferative response of transgenic (tg) T cells expressing the HLA-DR2-restricted͞MBP 85-99-specific TCR (hV␤2 ϩ CD4 ϩ ) and non-tg T cells (hV␤2 Ϫ CD4 ϩ ), splenocytes were fractionated from double-tg humanized mice that express both HLA-DR2 and a MBP 85-99-specific hV␤2 T cell receptor from an MS patient (30) by flow cytometry and seeded into a 96-well U-bottom microtiter plate in complete medium at 4 ϫ 10 5 cells per well. Irradiated splenocytes of humanized mice, also expressing HLA-DR2, were used as antigen-presenting cells.…”

Section: Methodsmentioning

confidence: 99%

“…Cop1 binds to several human HLA-DR molecules, including HLA-DR2, and blocks modestly the presentation of MBP 85-99 (27,28). The effectiveness of amino acid copolymers with in vitro and in vivo assays was greatly improved by modifications that enhanced their binding to HLA-DR2 (29,30). We hypothesized that by similarly improving the binding of synthetic peptide mimetics (13,29,30), their effectiveness might also be greatly enhanced.…”

mentioning

confidence: 99%

“…The effectiveness of amino acid copolymers with in vitro and in vivo assays was greatly improved by modifications that enhanced their binding to HLA-DR2 (29,30). We hypothesized that by similarly improving the binding of synthetic peptide mimetics (13,29,30), their effectiveness might also be greatly enhanced. Thus, T cell recognition of MBP 85-99 might be more effectively inhibited and͞or additional immunosuppressive functions of the copolymers might be enhanced by the peptide mimetics.…”

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confidence: 99%

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Peptide 15-mers of defined sequence that substitute for random amino acid copolymers in amelioration of experimental autoimmune encephalomyelitis

Stern

Illés

Reddy

et al. 2005

Proc. Natl. Acad. Sci. U.S.A.

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Myelin basic protein (MBP) is a major candidate autoantigen in multiple sclerosis (MS).Cop1 ͉ HLA-DR ͉ multiple sclerosis ͉ T cells M ultiple sclerosis (MS), an autoimmune inflammatory disease of the CNS, is associated with the HLA-DR2 haplotype (DRA*0101, DRB1*1501, DQA1*0102, DQB1*0602) (1-3). Myelin basic protein (MBP) is one of the major candidate autoantigens in the pathogenesis of MS. Particularly, T cell reactivity to the immunodominant MBP 85-99 epitope is found in subjects carrying human leukocyte antigen (HLA)-DR2, a genetic marker for susceptibility to MS. HLA-DR2-restricted MBP-specific T cells are clonally expanded and activated in MS patients (4-9). Furthermore, HLA-DR2͞MBP 85-99 complexes have been detected in the CNS plaques of these patients (10). Critical residues for binding to HLA-DR2 and for T cell antigen receptor (TCR) recognition of the MBP 85-99 epitope have been defined (11,12).Several therapeutic approaches to MS have been attempted by using cytokines, copolymers, dimers of class II major histocompatibility complex-peptide complexes, peptide antigens that induce anergy, vaccination with TCR, and an altered peptide ligand (13)(14)(15)(16)(17)(18)(19). Many of these studies aimed to interfere with the MBP 85-99-specific T cell recognition and͞or to deviate the T cell response from the Th1 to the Th2 phenotype. Copolymer 1 [Cop1, Copaxone, Glatiramer Acetate, poly(Y, E, A, K)n], the only approved drug known to reduce MBP-specific T cell responses, reduces the relapse rate by Ϸ30% in relapsingremitting forms of MS (20-26). Cop1 binds to several human HLA-DR molecules, including HLA-DR2, and blocks modestly the presentation of MBP 85-99 (27, 28). The effectiveness of amino acid copolymers with in vitro and in vivo assays was greatly improved by modifications that enhanced their binding to HLA-DR2 (29, 30). We hypothesized that by similarly improving the binding of synthetic peptide mimetics (13, 29, 30), their effectiveness might also be greatly enhanced. Thus, T cell recognition of MBP 85-99 might be more effectively inhibited and͞or additional immunosuppressive functions of the copolymers might be enhanced by the peptide mimetics. In this paper we report generation of three peptide inhibitors based on the binding motif of MBP 85-99 to HLA-DR2 with improved functions in inhibiting T cell responses and experimental autoimmune encephalomyelitis (EAE). These 15-mers (J2, J3, and J5) competed with MBP 85-99 for binding to HLA-DR2, inhibited IL-2 secretion by MBP 85-99-specific T cell clones and induced production of Th2 cytokines by splenocytes. Additionally they did not crossreact with MBP 85-99-or PLP 139-151-specific T cells. They also suppressed EAE in two different murine disease models in a manner equivalent to that achieved by using the modified random amino acid copolymers. Materials and MethodsGeneration of Peptide-Specific Short-Term T Cell Lines and Proliferative Responses to Peptides. Mice were immunized with proteolipid protein (PLP) 139-151 or peptide 15-mers (100 g per mouse) em...

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Section: Inhibition By Synthetic Peptide 15-mers Of Il-2 Secretion By Anmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Peptide 15-mers of defined sequence that substitute for random amino acid copolymers in amelioration of experimental autoimmune encephalomyelitis

Stern

Illés

Reddy

et al. 2005

Proc. Natl. Acad. Sci. U.S.A.

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The Design of Polyvalent Therapeutics

Joshi

Vance

Rai

et al. 2008

Chemistry A European J

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Copolymer effects on microglia and T cells in the central nervous system of humanized mice

et al. 2005

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The random amino acid copolymers FYAK and VWAK ameliorate EAE in a humanized mouse model expressing both a human transgenic myelin basic protein (MBP)85-99-specific T cell receptor and HLA-DR2. Here we show that microglia isolated from the central nervous system (CNS) of humanized mice with EAE induced by MBP85-99 and treated with these copolymers had reduced expression of HLA-DR, and thus reduced capacity to present MBP85-99 and activate transgenic T cells. In vitro microglia upregulated empty HLA-DR2 upon activation with GM-CSF with or without LPS or IFN-c, but not with IL-4 or IL-10. Correspondingly, gene chip arrays showed that the CNS of untreated and YFAK-treated mice differentially expressed pro-and anti-inflammatory molecules during MBP85-99-induced EAE. Interestingly, microglia expressed the fulllength cb and ab subunits of the tetrameric adaptor protein complexes AP-1 and AP-2 respectively, but after treatment with GM-CSF these complexes were cleaved, as had been found in immature dendritic cells derived from bone marrow. Strikingly, in vivo the perivascular lymphocyte infiltration seen in untreated mice immunized with MBP85-99 was composed of equal numbers of hVb2 + MPB85-99-specific transgenic and hVb2 -endogenous T cells, while the much smaller infiltration seen after treatment with YFAK was composed predominantly of hVb2 -endogenous T cells.

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Modified amino acid copolymers suppress myelin basic protein 85–99-induced encephalomyelitis in humanized mice through different effects on T cells

Cited by 37 publications

References 37 publications

Peptide 15-mers of defined sequence that substitute for random amino acid copolymers in amelioration of experimental autoimmune encephalomyelitis

Peptide 15-mers of defined sequence that substitute for random amino acid copolymers in amelioration of experimental autoimmune encephalomyelitis

The Design of Polyvalent Therapeutics

Copolymer effects on microglia and T cells in the central nervous system of humanized mice

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