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CpG DNA刺激骨髓中的自身反应性未成熟B细胞。

CpG DNA stimulates autoreactive immature B cells in the bone marrow.

作者信息

Azulay-Debby Hilla, Edry Efrat, Melamed Doron

机构信息

Department of Immunology, Bruce Rappaport Faculty of Medicine, Technion-Israel Institute of Technology, Haifa, Israel.

出版信息

Eur J Immunol. 2007 Jun;37(6):1463-75. doi: 10.1002/eji.200636878.

Abstract

Polyclonal activation of developing B cells is an injurious process, because most of these cells are nontolerant and express autoreactive receptors. CpG DNA is a polyclonal activator of mature B cells, but its effect on developing B cells is unclear. We tested whether developing, nontolerant B cells are responsive to mitogenic stimulation by CpG DNA and whether such a stimulus can interfere with the establishment of central tolerance. We found that developing B cells express Toll-like receptor 9 and undergo a polyclonal response to CpG DNA stimulation, as revealed by proliferation and differentiation to antibody-producing cells. In vitro and ex vivo experiments revealed that stimulation with CpG DNA protects immature B cells from negative selection imposed by apoptosis and receptor editing and results in the production of autoantibodies. Finally, we found that in vivo administration of CpG DNA activates immature B cells in the bone marrow and suppresses the expression of recombination-activating genes in a mouse model of central tolerance and receptor editing. These results suggest that mitogenic signals provided by CpG DNA stimulate nontolerant immature B cells in the bone marrow and have the potential to interfere with central tolerance.

摘要

发育中B细胞的多克隆激活是一个有害过程,因为这些细胞中的大多数是未耐受的,并且表达自身反应性受体。CpG DNA是成熟B细胞的多克隆激活剂,但其对发育中B细胞的影响尚不清楚。我们测试了发育中的未耐受B细胞是否对CpG DNA的促有丝分裂刺激有反应,以及这种刺激是否会干扰中枢耐受的建立。我们发现发育中的B细胞表达Toll样受体9,并对CpG DNA刺激产生多克隆反应,这通过增殖和分化为抗体产生细胞得以揭示。体外和体内实验表明,CpG DNA刺激可保护未成熟B细胞免受凋亡和受体编辑所施加的阴性选择,并导致自身抗体的产生。最后,我们发现在中枢耐受和受体编辑的小鼠模型中,体内给予CpG DNA可激活骨髓中的未成熟B细胞,并抑制重组激活基因的表达。这些结果表明,CpG DNA提供的促有丝分裂信号刺激骨髓中未耐受的未成熟B细胞,并有可能干扰中枢耐受。

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