Critical Relationships Between Constituents of the Antigen-Adjuvant Emulsion Affecting Experimental Allergic Encephalomyelitis in a Completely Susceptible Mouse Genotype

Lee, Johanna M.; Schneider, Howard A.

doi:10.1084/jem.115.1.157

Cited by 31 publications

(23 citation statements)

References 9 publications

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“…A role for this type of pathogen has been suggested by studies from Harkiolaki et al (5), showing that peptides derived by microbial pathogens stimulate a T cells from a mouse transgenic for a TCR specific for DR2-MBP85-99. In the present report, we show that a self-reactive disease of the CNS can develop after a transient infection with a nonpathogenic Mycobacterium in the periphery, which results in appropriate stimuli leading to the development of the encephalitogenic phenotype in responding T cells (15).…”

Section: Discussionmentioning

confidence: 57%

“…Average duration of disease remission (calculated from the first day in which disease score was 1 point below the maximum value reached during the acute bout to the first day in which disease score had gained 1 point above the lowest value observed during remission) was 17. Induction of EAE by immunization with peptide depends on the dose of both peptide and adjuvant (15). To examine the effect of dose of infecting bacterium on the development of EAE, we conducted a second experiment with three groups of SJL mice, infected with 10 6 (6 mice) or 4 3 10 6 (six mice) or 4 3 10 7 (five mice) CFU of rMS p139 .…”

Section: Infection With Live Rmsmentioning

confidence: 99%

“…In the SJL mouse, EAE follows immunization with p139 alone without administration of pertussis toxin, indicating that p139-specific T cells primed in the periphery acquire a phenotype sufficient for homing into the CNS without need for alteration of the BBB. The development of EAE is critically dependent on the presence and amount of Mycobacterium tuberculosis products in the adjuvant (15) that provide nonantigenic moieties, thereby determining the encephalitogenic phenotype during priming. We therefore wondered whether infection with nonpathogenic mycobacteria carrying a determinant cross-reactive to CNS would trigger EAE, without need for presence of the infectious agent in the CNS.…”

mentioning

confidence: 99%

“…Therefore, M. smegmatis has been used as vaccine vector, because it activates DCs and induces CD8-mediated immune responses (22)(23)(24)(25). Finally, killed M. smegmatis has been shown to provide the same adjuvant activity of M. tuberculosis during induction of EAE (15).…”

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confidence: 99%

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Mycobacterium smegmatisExpressing a Chimeric Protein MPT64-Proteolipid Protein (PLP) 139–151 Reorganizes the PLP-Specific T Cell Repertoire Favoring a CD8-Mediated Response and Induces a Relapsing Experimental Autoimmune Encephalomyelitis

Nicolò¹,

Sali

Sante³

et al. 2009

The Journal of Immunology

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We infected SJL mice with a recombinant Mycobacterium smegmatis expressing a chimeric protein containing the self-epitope of proteolipid protein 139–151 (p139) fused to MPT64, a secreted protein of Mycobacterium tuberculosis (rMSp139). Infected mice developed a relapsing experimental autoimmune encephalomyelitis (EAE), showing a prevailing demyelination of the CNS, and disease severity was significantly lower in comparison with the one that follows immunization with p139. rMSp139 was not detected in lymph node or spleen in the course of clinical disease development or in the CNS during relapse. Infection with rMSp139 modified the p139-specific T cell repertoire, recruiting the spontaneous p139-specific repertoire and activating CD4+ T cells carrying the BV4 semiprivate rearrangement. T cells carrying the public BV10 rearrangement that are consistently found in the CNS during flares of disease were not activated by infection with rMSp139 because lymph node APCs infected with rMSp139 selectively fail to present the epitope for which BV10 cells are specific. Simultaneously, rMSp139 expanded p139-specific CD8+ cells more efficiently than immunization with peptide in adjuvant. SJL mice vaccinated against the CDR3 sequence of the BV10 public rearrangement reduced usage of the BV10 cells and displayed reduced symptoms during bouts of EAE. Thus, transient peripheral infection with a CNS-cross–reactive nonpathogenic Mycobacterium induces a relapsing EAE that continues long after clearance of the infectious agent. The composition of the self-reactive repertoire activated determines severity and histology of the resulting disease.

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Section: Discussionmentioning

confidence: 57%

Section: Infection With Live Rmsmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Mycobacterium smegmatisExpressing a Chimeric Protein MPT64-Proteolipid Protein (PLP) 139–151 Reorganizes the PLP-Specific T Cell Repertoire Favoring a CD8-Mediated Response and Induces a Relapsing Experimental Autoimmune Encephalomyelitis

Nicolò¹,

Sali

Sante³

et al. 2009

The Journal of Immunology

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“…The fact that tuberculin sensitivity is also suppressed by scurvy is consistent with the autoimmune theory of EAE development. The recovery of tuberculin sensitivity following restitution of vitamin C, however, may indicate only that the mechanisms underlying tuberculin sensitivity are much cruder than those underlying the development of EAE, which depends upon a rather fine balance between concentrations of CNS and mycobacteria (4,9).…”

Section: Discussionmentioning

confidence: 99%

Prevention of Experimental Allergic Encephalomyelitis (Eae) by Vitamin C Deprivation

Kies

Alvord

Shaw

1962

The Journal of Experimental Medicine

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Scorbutic guinea pigs injected with CNS and mycobacterium to induce experimental allergic encephalomyelitis (EAE) showed no clear-cut neurological signs and failed to show histological evidence of central nervous system damage. The degree of protection afforded by vitamin C deprivation was related directly to the duration of the scorbutogenic diet and inversely to the strength of the CNS challenge. Vitamin C deprivation also abolished tuberculin sensitivity as measured by the PPD skin reaction. Upon restoration of vitamin C, the animals recovered their sensitivity to PPD but did not develop EAE. It was further demonstrated that these effects of vitamin C deprivation were not related to inanition or to the endogenous levels of 17-hydroxycorticosteroids.

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Studies on adjuvant‐induced polyarthritis in rats. I. Adjuvant composition, route of injection, and removal of depot site

Ward

Jones

1962

Arthritis & Rheumatism

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The composition and quantity of Freund-type adjuvant injected, the route of injection, and reaction at the depot site were studied for their roles in producing polyarthritis in rats. The intradermal injection of Myobacterium butyricum in oil induced arthritis with much higher frequency than the subcutaneous or intravenous route. The minimal effective intradermal dose was 0.06 mg. M . butyricum in 0.02 ml. oil; 0.6 mg. mycobacteria in 0.1 ml. oil was required to produce polyarthritis in 100 per cent of rats. Wax fractions of mycobacteria did not induce arthritis. Neither a depot of adjuvant nor inflammation at the injection site was important as polyarthritis developed, even though amputation of the tail to remove the depot of injected adjuvant was performed within 2 hours after injection. While the mechanism of adjuvant-induced polyarthritis remains unknown, the joint disease appeared dependent upon specific sites of dissemination of the adjuvant, Le composition e le quantitate de adjuvante typo Freund, le via de injection usate, e le reaction a1 sito del deposito esseva studiate con respecto a lor rolos in le production de polyarthritis in rattos. Le injection intradermal de Mycobacterium butyricum in oleo induceva arthritis multo plus frequentemente que le injection subcutanee o intravenose del mesme preparato. Le minime efficace dose intradermal esseva 0,06 mg de M . butyricum in 0,02 ml de oleo. Pro producer polyarthritis in 100 pro cento del rattos, 0,6 mg de M . butyricum in 0,l ml de oleo esseva requirite. Fractiones de cera de mycobacterios non induceva arthritis. Ni un deposito de adjuvante ni inflammation a1 sito del injection esseva importante. Polyarthritis se disveloppava mesmo quando le cauda esseva amputate (pro eliminar le deposito del injicite adjuvante) intra 2 horas post le injection. Ben que le mechanism0 del induction de polyarthritis per un adjuvante remane incognoscite, il pareva que le occurrentia de morbo articular dependeva de specific sitos de dissemination del adjuvante.REUND ADJUVANTS have been used extensively to enhance antibody

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Critical Relationships Between Constituents of the Antigen-Adjuvant Emulsion Affecting Experimental Allergic Encephalomyelitis in a Completely Susceptible Mouse Genotype

Cited by 31 publications

References 9 publications

Mycobacterium smegmatisExpressing a Chimeric Protein MPT64-Proteolipid Protein (PLP) 139–151 Reorganizes the PLP-Specific T Cell Repertoire Favoring a CD8-Mediated Response and Induces a Relapsing Experimental Autoimmune Encephalomyelitis

Mycobacterium smegmatisExpressing a Chimeric Protein MPT64-Proteolipid Protein (PLP) 139–151 Reorganizes the PLP-Specific T Cell Repertoire Favoring a CD8-Mediated Response and Induces a Relapsing Experimental Autoimmune Encephalomyelitis

Prevention of Experimental Allergic Encephalomyelitis (Eae) by Vitamin C Deprivation

Studies on adjuvant‐induced polyarthritis in rats. I. Adjuvant composition, route of injection, and removal of depot site

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