Involvement of antibody production quantitative trait loci in the susceptibility to pristane-induced arthritis in the mouse

Jensen, José Ricardo; Peters, L C; Borrego, Andrea; Ribeiro, Orlando; Cabrera, Wafa Hanna Koury; Starobinas, Nancy; Siqueira, Maria; Ibañez, Olga M.; Franco, Marcelo De

doi:10.1038/sj.gene.6364271

Cited by 23 publications

(32 citation statements)

References 27 publications

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“…In mice, several loci were identified in different models of experimental arthritis. The involvement of acute inflammation 14 and antibody production QTL 27 were demonstrated in PIA development, as well as many other QTL in arthritis models such as those induced by Borrelia burgdorferi, 28 PGIA 29 and CIA. 30 Rheumatoid arthritis is a chronic inflammatory and autoimmune disease characterized by cell accumulation in the sinovium, complement deposition and the production of several proinflammatory cytokines.…”

Section: Discussionmentioning

confidence: 99%

“…Spleen cells from phosphate-buffered saline (PBS)-or pristane-treated mice were evaluated for IL-6, IL-12, IL-4 and IFNgspecific spot-forming cells. The cytokine ELISPOT assay was performed according to Jensen et al 27 Multiscreen HA 96-well nitrocellulose-based plates (Millipore Corp., Molsheim, France) were coated overnight with capture monoclonal antibodies (mAb) anti-IL-6, IL-12, IL-4 or IFNg (5 mg/ml in PBS). After blocking with RPMI plus 5% fetal calf serum (FCS) for 1 h at room temperature, spleen cells were isolated from PBS-or pristane-treated mice 10, 20, and 75 days after the first injection and incubated (5 Â 10 5 and 10 6 cells/well in duplicate) for 20 h at 371C in a CO 2 incubator.…”

Section: Pristane-induced Arthritismentioning

confidence: 99%

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Slc11a1 (formerly NRAMP1) gene modulates both acute inflammatory reactions and pristane-induced arthritis in mice

et al. 2006

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Mice selected for the maximum acute inflammatory reaction (AIRmax) are highly susceptible to pristane-induced arthritis (PIA), whereas mice selected for the minimum response (AIRmin) are resistant. These lines show distinct patterns of leukocyte infiltration and R and S allele frequency disequilibrium of the solute carrier family 11a member 1 (Slc11a1) gene. In order to study the interactions of the Slc11a1 R and S alleles with the inflammation modulating Quantitative Trait Loci (QTL) during PIA development, homozygous AIRmax RR , AIRmax SS , AIRmin RR and AIRmin SS lines were produced by genotype-assisted breedings. These mice received two intraperitoneal injections of 0.5 ml pristane at 60-day intervals, and the subsequent development of arthritis was assessed for 210 days. Cytokine-secreting cell profiles were investigated using enzyme-linked immunospot. Arthritis incidence in AIRmax RR mice reached 29%, whereas PIA incidence in AIRmax SS mice was 70% by day 180. AIRmin RR mice were resistant, whereas 13.3% of AIRmin SS mice became arthritic. The presence of the defective S allele also increased arthritis severity, although acute inflammation was higher in mice bearing the R allele. A predominant Th0/Th2-type response in Slc11a1 SS mice was observed. These results indicate that Slc11a1 is a strong candidate for the QTL modulating acute inflammation and for PIA.

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Section: Discussionmentioning

confidence: 99%

Section: Pristane-induced Arthritismentioning

confidence: 99%

Slc11a1 (formerly NRAMP1) gene modulates both acute inflammatory reactions and pristane-induced arthritis in mice

et al. 2006

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“…H III and L III mice, both genders, presented slightly higher production of IgG2a anti-Hsp65 and anti-DNA related to the IgG1 isotype. This balance towards a Th1 response may indicate a natural pro-inflammatory status in these strains which is confirmed by the relative easy way to induce adjuvant arthritis in H III mice [53]. The time-course analyses of immunoglobulin production did not show significant intragroup differences, which might be related to the absence of a strong specific response to these proteins demonstrated by the low antibody titers even 30 days after the protein inoculation and because this is not an immunization process.…”

Section: Discussionmentioning

confidence: 93%

Mycobacterium leprae Hsp65 administration reduces the lifespan of aged high antibody producer mice

et al. 2014

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BackgroundAging process may result in immune modifications that lead to disruption of innate and acquired immunity mechanisms that may induce chronic-degenerative events. The heat shock proteins (Hsp), phylogeneticaly conserved among organisms, present as main function the ability of folding and refolding proteins, but they also are associated with chronic-degenerative disorders. Here were evaluated the role of M. leprae native Hsp65 (WT) and its point-mutated (K409A) on survival and anti-DNA and anti-Hsp65 antibody production of aged genetically selected mice for high (HIII) and low (LIII) antibody production; data from 120- and 270-days old mice (named “adult” or “aged”, respectively) were compared.ResultsWT Hsp65 administration induces reduction in the mean survival time of adult and aged female HIII mice, this effect being stronger in aged individuals. Surprisingly, the native protein administration increased the survival of aged female LIII when compared to K409A and control groups. No survival differences were observed in aged male mice after Hsp65 proteins inoculation. We observed increase in IgG1 anti-Hsp65 in WT and K409A aged HIII female mice groups and no marked changes in the anti-DNA (adult and aged HIII) and anti-Hsp65 IgG1 or IgG2a isotypes production in adult HIII female and aged male mice. LIII male mice presented increased anti-DNA and anti-Hsp65 IgG2a isotype production after WT or K409A injection, and LIII female groups showed no alterations.ConclusionsThe results revealed that the WT Hsp65 interferes with survival of aged HIII female mice without involvement of a remarkable IgG1 and IgG2a anti-DNA and anti-Hsp65 antibodies production. The deleterious effects of Hsp65 on survival time in aged HIII female mice could be linked to a gender-effect and are in agreement with those previously reported in lupus-prone mice.

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“…H III and L III lines also show extreme divergence in other phenotypes, such as skin carcinogenesis [31] and pristane induced arthritis—PIA. Our group successfully detected a PIA-susceptibility QTL on chromosome 3 by examining the cosegregation of the most significant Ab QTL markers with arthritis phenotypes [32]. …”

Section: Introductionmentioning

confidence: 99%

Trypanosoma cruziInfection in Genetically Selected Mouse Lines: Genetic Linkage with Quantitative Trait Locus Controlling Antibody Response

Vorraro

Cabrera

Ribeiro

et al. 2014

Mediators of Inflammation

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Trypanosoma cruzi infection was studied in mouse lines selected for maximal (AIRmax) or minimal (AIRmin) acute inflammatory reaction and for high (HIII) or low (LIII) antibody (Ab) responses to complex antigens. Resistance was associated with gender (females) and strain—the high responder lines AIRmax and HIII were resistant. The higher resistance of HIII as compared to LIII mice extended to higher infective doses and was correlated with enhanced production of IFN-γ and nitric oxide production by peritoneal and lymph node cells, in HIII males and females. We also analyzed the involvement of previously mapped Ab and T. cruzi response QTL with the survival of Selection III mice to T. cruzi infections in a segregating backcross [F1(HIII×LIII) ×LIII] population. An Ab production QTL marker mapping to mouse chromosome 1 (34.8 cM) significantly cosegregated with survival after acute T. cruzi infections, indicating that this region also harbors genes whose alleles modulate resistance to acute T. cruzi infection.

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Involvement of antibody production quantitative trait loci in the susceptibility to pristane-induced arthritis in the mouse

Cited by 23 publications

References 27 publications

Slc11a1 (formerly NRAMP1) gene modulates both acute inflammatory reactions and pristane-induced arthritis in mice

Slc11a1 (formerly NRAMP1) gene modulates both acute inflammatory reactions and pristane-induced arthritis in mice

Mycobacterium leprae Hsp65 administration reduces the lifespan of aged high antibody producer mice

Trypanosoma cruziInfection in Genetically Selected Mouse Lines: Genetic Linkage with Quantitative Trait Locus Controlling Antibody Response

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