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正常和狼疮易感小鼠的自身抗体库分析。

Autoantibody repertoire analysis in normal and lupus-prone mice.

作者信息

Starobinski M, Lacour M, Reininger L, Izui S

机构信息

Department of Pathology, University of Geneva, Switzerland.

出版信息

J Autoimmun. 1989 Oct;2(5):657-74. doi: 10.1016/s0896-8411(89)80005-8.

Abstract

We have analyzed at the clonal level (limiting dilution assay) the repertoire of lipopolysaccharide (LPS)-responsive murine B cells committed to the production of autoantibodies characteristic of systemic lupus erythematous (SLE), i.e. anti-single-stranded DNA (ssDNA), anti-double-stranded DNA, anti-Sm and rheumatoid factors (RF). Our results demonstrated that: (1) the frequency of precursor B cells producing each lupus autoantibody (approximately 1 in every 100-400 LPS-responding B cell) was similar in two non-autoimmune (C57BL/6 and BALB/c) and four SLE-prone (NZB, (NZB x NZW)F1, MRL/MpJ and BXSB/MpJ) mice despite the marked differences in autoimmune responses in the different SLE-prone mice, and (2) the relative frequency of autoantibody-secreting precursor B cells was constant throughout life, and equally distributed among activated and resting B-cell populations and among B cells from the peritoneal cavity and spleen. The lack of association of anti-ssDNA secretion with anti-Sm or RF secretion in cultures set up with a smaller number of B cells ruled out the possibility that the similar frequency of different autoantibody-secreting cell precursors is due to the poly-specificity of IgM autoantibodies. Notably, the frequencies of autoantibody-secreting precursor cells were significantly lower, approximately 4 and 10 times, than those of anti-tetanus toxoid and anti-dinitrophenyl antibody-producing precursor B cells, respectively. The similar frequency of precursor B cells producing four different lupus autoantibodies on the one hand and the considerable variation in each autoimmune response among SLE-prone mice on the other, support the hypothesis that specific stimulatory mechanisms may govern each autoimmune response in different SLE strains of mice.

摘要

我们已在克隆水平(有限稀释分析)分析了对脂多糖(LPS)有反应、致力于产生系统性红斑狼疮(SLE)特征性自身抗体的小鼠B细胞库,即抗单链DNA(ssDNA)、抗双链DNA、抗Sm和类风湿因子(RF)。我们的结果表明:(1)尽管不同SLE易感小鼠的自身免疫反应存在显著差异,但在两种非自身免疫小鼠(C57BL/6和BALB/c)和四种SLE易感小鼠(NZB、(NZB×NZW)F1、MRL/MpJ和BXSB/MpJ)中,产生每种狼疮自身抗体的前体B细胞频率(每100 - 400个对LPS有反应的B细胞中约有1个)相似;(2)分泌自身抗体的前体B细胞的相对频率在整个生命过程中保持恒定,并且在活化和静止的B细胞群体之间以及来自腹腔和脾脏的B细胞之间均匀分布。在使用较少数量B细胞建立的培养物中,抗ssDNA分泌与抗Sm或RF分泌缺乏相关性,排除了不同自身抗体分泌细胞前体频率相似是由于IgM自身抗体多特异性的可能性。值得注意的是,分泌自身抗体的前体细胞频率分别比产生抗破伤风类毒素和抗二硝基苯基抗体的前体B细胞频率显著低约4倍和10倍。一方面,产生四种不同狼疮自身抗体的前体B细胞频率相似,另一方面,SLE易感小鼠之间每种自身免疫反应存在相当大的差异,这支持了特定刺激机制可能控制不同SLE品系小鼠中每种自身免疫反应的假设。

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