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Phenotype conversion from rheumatoid arthritis to systemic lupus erythematosus by introduction of Y aa mutation into F c[gamma] RIIB -deficient C 57 BL /6 mice
We previously established an I g G F c receptor IIB ( F c[gamma] RIIB )-deficient C 57 BL /6 ( B 6)-congenic mouse strain ( KO 1), which spontaneously develops rheumatoid arthritis ( RA ), but not systemic lupus erythematosus ( SLE ). Here, we show that when Y chromosome-linked autoimmune accelerati...
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| Published in: | European journal of immunology 2013-03, Vol.43 (3), p.770-778 |
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| Main Authors: | , , , , , , , , , , , |
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| Language: | English |
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| container_end_page | 778 |
| container_issue | 3 |
| container_start_page | 770 |
| container_title | European journal of immunology |
| container_volume | 43 |
| creator | Kawano, Shinya Lin, Qingshun Amano, Hirofumi Kaneko, Toshiyuki Nishikawa, Keiko Tsurui, Hiromichi Tada, Norihiro Nishimura, Hiroyuki Takai, Toshiyuki Shirai, Toshikazu Takasaki, Yoshinari Hirose, Sachiko |
| description | We previously established an I g G F c receptor IIB ( F c[gamma] RIIB )-deficient C 57 BL /6 ( B 6)-congenic mouse strain ( KO 1), which spontaneously develops rheumatoid arthritis ( RA ), but not systemic lupus erythematosus ( SLE ). Here, we show that when Y chromosome-linked autoimmune acceleration ( Y aa) mutation was introduced in KO 1 strain ( KO 1. Y aa), the majority of KO 1. Y aa mice did not develop RA , but instead did develop SLE . This phenotype conversion did not depend on autoantibody specificity, since KO 1. Y aa mice, compared with KO 1, showed a marked increase in serum levels of both lupus-related and RA -related autoantibodies. The increase in frequencies of CD 69 super(+) activated B cells and T cells, and the spontaneous splenic GC formation with T follicular helper cell generation were manifest early in life of KO 1. Y aa, but not KO 1 and B 6. Y aa, mice. Activated CD 4 super(+) T cells from KO 1. Y aa mice showed upregulated production of IL -21 and IL -10, compared with the finding in KO 1 mice, indicating the possibility that this aberrant cytokine milieu relates to the disease phenotype conversion. Thus, our model is useful to clarify the shared and the disease-specific mechanisms underlying the clinically distinct systemic autoimmune diseases RA and SLE . |
| doi_str_mv | 10.1002/eji.201243057 |
| format | article |
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Here, we show that when Y chromosome-linked autoimmune acceleration ( Y aa) mutation was introduced in KO 1 strain ( KO 1. Y aa), the majority of KO 1. Y aa mice did not develop RA , but instead did develop SLE . This phenotype conversion did not depend on autoantibody specificity, since KO 1. Y aa mice, compared with KO 1, showed a marked increase in serum levels of both lupus-related and RA -related autoantibodies. The increase in frequencies of CD 69 super(+) activated B cells and T cells, and the spontaneous splenic GC formation with T follicular helper cell generation were manifest early in life of KO 1. Y aa, but not KO 1 and B 6. Y aa, mice. Activated CD 4 super(+) T cells from KO 1. Y aa mice showed upregulated production of IL -21 and IL -10, compared with the finding in KO 1 mice, indicating the possibility that this aberrant cytokine milieu relates to the disease phenotype conversion. Thus, our model is useful to clarify the shared and the disease-specific mechanisms underlying the clinically distinct systemic autoimmune diseases RA and SLE .</abstract><doi>10.1002/eji.201243057</doi></addata></record> |
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| title | Phenotype conversion from rheumatoid arthritis to systemic lupus erythematosus by introduction of Y aa mutation into F c[gamma] RIIB -deficient C 57 BL /6 mice |
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