High Frequency of Autoreactive Myelin Proteolipid Protein–Specific T Cells in the Periphery of Naive Mice

Anderson, Ana C.; Nicholson, Lindsay B.; Legge, Kevin L.; Turchin, Vadim; Zaghouani, Habib; Kuchroo, Vijay K.

doi:10.1084/jem.191.5.761

Cited by 251 publications

(221 citation statements)

References 42 publications

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“…The lesser magnitude in the generation of PLP 139-151-specific T cells in ACA 83-95-immunized could lead to the generation of cross-reactive T cells both in periphery and locally within the CNS. Myelin antigens such as MBP and PLP can be expressed in thymus and peripheral lymphoid tissues and aberrant expression of PLP transcripts importantly DM20, an isoform of PLP lacking PLP 139-151 motif contribute to the endogenous generation of PLP 139-151 reactive T cells by escaping central tolerance (Anderson et al, 2000;Klein et al, 2000;Voskuhl, 1998). Furthermore, healthy humans including MS patients react to MBP or PLP suggestive of the existence of endogenous myelin reactive T cell repertoires and the resident dendritic cells and microglia can present antigens locally within CNS (Bailey et al, 2007;Pette et al, 1990;Wucherpfennig and Strominger, 1995).…”

Section: Discussionmentioning

confidence: 99%

An epitope from Acanthamoeba castellanii that cross-react with proteolipid protein 139-151-reactive T cells induces autoimmune encephalomyelitis in SJL mice

Massilamany

Steffen

Reddy

2010

Journal of Neuroimmunology

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Epitope from Acanthamoeba castellanii That Cross-React with Proteolipid Protein 139-151-Reactive T Cells Induces Autoimmune Encephalomyelitis in SJL Mice" (2010). Jay Reddy Publications. 17. https://digitalcommons.unl.edu/vbsjayreddy/17 tein databases. This search resulted in the identification of one novel peptide spanning aa 83-95 of rhodanese-related sulfurtransferase in Acanthamoeba castellanii (ACA) and it induces EAE similar to that of PLP 139-151. Materials and methods MiceFour to six-week-old female SJL/J (H-2 s ) mice were obtained from the Jackson Laboratory (Bar Harbor, Maine). The mice were maintained in accordance with the animal protocol guidelines of the University of Nebraska-Lincoln, Lincoln, Nebraska. Peptide synthesis and immunization proceduresPLP 139-151 (HSLGKWLGHPDKF), ACA 83-95 (YFLLKWLGH-PNVS) and neuraminidase (NASE) 101-120 (EALVRQGLAKVAY-VYKPNNT) were synthesized on 9-fluorenylmethyloxycarbonyl chemistry (Neopeptide, Cambridge, Massachusetts). All peptides were HPLC-purified (N90%) and confirmed by mass spectroscopy. To measure recall responses 100 µg of each peptide emulsified in CFA was administered subcutaneously in the flank. For disease induction, Mycobacterium tuberculosis (MTB) H37RA extract (Difco Laboratories, Detroit, Michigan) was added as an additional component to a final concentration of 5 mg/ml. Pertussis toxin (List Biological Laboratories, Campbell, California) was administered (100 ng per mouse) intraperitoneally on day 0 and day 2 postimmunization. Identification of microbial peptides that mimic PLP 139-151PLP 139-151 is an immunodominant epitope in which the critical residues required for major histocompatibility complex (MHC) class II and T cell receptor (TCR)-binding have been well-characterized (Figure 1). By using PLP 139-151 as a putative antigen, we performed pattern search using the prosite scan of the Bioinformatics Toolkit

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Section: Discussionmentioning

confidence: 99%

An epitope from Acanthamoeba castellanii that cross-react with proteolipid protein 139-151-reactive T cells induces autoimmune encephalomyelitis in SJL mice

Massilamany

Steffen

Reddy

2010

Journal of Neuroimmunology

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“…However, for lymphocytes that escaped central tolerance, peripheral tolerance mechanisms would operate to protect against destructive auto-immunity through active suppression by regulatory cells or via a mechanism called clonal ignorance [37,38]. Of particular interest, prior studies have revealed that central tolerance is operative for so-called "sequestered" antigens such as PLP [24,25]. In fact, a splice variant of PLP is promiscuously expressed in the thymus and would play some role in shaping the T cell repertoire.…”

Section: Discussionmentioning

confidence: 99%

“…Moreover, it has been proven that a splice variant of myelin proteolipid protein (PLP), an encephalitogenic antigen causing EAE, is promiscuously expressed in the thymus and plays a role in shaping the autoimmune T cell repertoire [24,25]. Given this information together with our experimental data, an attractive hypothesis was that self-tolerance to P0 might be defective in P0-deficient mice owing to a lower expression of P0 in the thymus, a place for establishing self-tolerance to P0.…”

Section: Transcription Levels Of P0 In the Thymus Inversely Correlatementioning

confidence: 99%

“…Recent studies demonstrate that a number of autoantigens, including those that were believed to be secluded from the immune system, are actually expressed in the thymus [19][20][21][22][23][24][25][26][27]. Furthermore, experiments have proven that such a promiscuous expression of autoantigen would contribute to eliminating pathogenic autoimmune T cells from the T cell repertoire [24,25]. We found that the P0 gene is also transcribed in the thymus, but the transcription level is reduced in P0 +/-mice as compared to wild-type mice.…”

Section: Introductionmentioning

confidence: 99%

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Heterozygous null mutation of myelin P0 protein enhances susceptibility to autoimmune neuritis targeting P0 peptide

et al. 2003

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Mice with a heterozygous null mutation in myelin protein zero (P0 +/-) develop late-onset clinical paralysis associated with inflammatory pathology in the peripheral nerves. Although the development of this illness is known to require T cells and macrophages, little is understood regarding the immunological defect in the mice. Here we report that young P0 +/-mice, free from clinical manifestations, have a defect in central tolerance to P0, and are more prone to induction of experimental autoimmune neuritis (EAN) by sensitization against P0 180-199 peptide. Notably, we found that the P0 gene is transcribed in the thymus of wild-type and the P0 +/-mice in an amount proportional to the gene dosage. We then replaced the thymus of wild-type mice with that of the P0-deficient mice and vice versa. Immunization of these mice with P0 [180][181][182][183][184][185][186][187][188][189][190][191][192][193][194][195][196][197][198][199] revealed that a lower thymic P0 transcript would be associated with the higher recall T cell response to P0 [180][181][182][183][184][185][186][187][188][189][190][191][192][193][194][195][196][197][198][199] , thus accounting for the higher susceptibility of the P0 +/-mice to P0-induced EAN. These results imply that a heterozygous mutation in an autoantigen could cause defective central tolerance to the autoantigen. As such, autoimmune T cells may play some role in "genetic" diseases caused by a heterozygous gene defect.

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“…This appears to be due to the high frequency of PLP 139-151-reactive T cells observed in these mice. 54 In this article we now examine a second epitope, MBP 89-101, in order to determine whether our protocol is PLPspecific or is more generally applicable. We show that by inducing disease with MBP protein (instead of MSCH) we can ameliorate disease using transduced fibroblasts secreting either the MBP 89-101 or PLP 139-151 epitope.…”

Section: Discussionmentioning

confidence: 99%

Cell-based gene therapy experiments in murine experimental autoimmune encephalomyelitis

Louie

Weiner

et al. 2005

Gene Ther

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With the ultimate goal of developing a novel treatment for multiple sclerosis (MS), we have developed a cell-based gene therapy protocol for the treatment of murine experimental autoimmune encephalomyelitis (EAE), a powerful animal model for MS. We have determined that transduced fibroblasts secreting encephalogenic epitopes, when injected into mice with EAE, cause a striking abrogation of disease. Both myelin basic protein (MBP) and proteolipid protein mini-gene constructs expressed in syngeneic fibroblast cells were capable of ameliorating ongoing EAE induced by MBP protein. These experiments are crucial since they suggest that not all encephalogenic epitopes need be secreted for the control of disease. We also demonstrate the success of this protocol when transduced syngeneic, and most importantly, allogeneic cells are sequestered within an implantable chamber. Furthermore, we find that through modifying antigen expression by changing the signal sequence of the mini-gene construct, we were able to significantly reduce the dose of cells required for treatment. These improvements to the minigene delivery system are critical for the eventual translation of our protocol to the clinic.

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High Frequency of Autoreactive Myelin Proteolipid Protein–Specific T Cells in the Periphery of Naive Mice

Cited by 251 publications

References 42 publications

An epitope from Acanthamoeba castellanii that cross-react with proteolipid protein 139-151-reactive T cells induces autoimmune encephalomyelitis in SJL mice

An epitope from Acanthamoeba castellanii that cross-react with proteolipid protein 139-151-reactive T cells induces autoimmune encephalomyelitis in SJL mice

Heterozygous null mutation of myelin P0 protein enhances susceptibility to autoimmune neuritis targeting P0 peptide

Cell-based gene therapy experiments in murine experimental autoimmune encephalomyelitis

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