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自身反应性B细胞的体内存活:长寿B细胞的特征

In vivo survival of autoreactive B cells: characterization of long-lived B cells.

作者信息

Morris S C, Moroldo M, Giannini E H, Orekhova T, Finkelman F D

机构信息

Division of Immunology, University of Cincinnati College of Medicine, Cincinnati, OH 45267, USA.

出版信息

J Immunol. 2000 Mar 15;164(6):3035-46. doi: 10.4049/jimmunol.164.6.3035.

Abstract

To determine the effects of chronic Ag stimulation on B cell survival and phenotype, we compared survival and surface markers of hen egg lysozyme (HEL)-specific B cells in Ig transgenic (Tgn) mice, which lack HEL, and in HEL-Ig transgenic mice, which express soluble HEL. Serum HEL levels were maximized in HEL-Ig Tgn mice by feeding them zinc, which activates the metallothionein promoter that regulates HEL expression. B cell age was characterized by expression of heat-stable Ag, and B220 and B cell survival was studied by evaluating changes in B cell number when lymphopoiesis was suppressed with anti-IL-7 mAb and by identifying newly generated B cells through 5-bromo-2'-deoxyuridine incorporation. Our observations show that the mean B cell life span is considerably reduced in HEL-Ig Tgn compared with Ig Tgn mice, but also demonstrate that some HEL-Ig Tgn B cells survive to maturity. Some of these surviving B cells have undergone receptor editing (substitution of an endogenous Ig light chain for the transgenic Ig light chain), so that their ability to bind HEL is decreased or absent. Surviving HEL-Ig Tgn B cells that retain HEL specificity express decreased mIgD and little or no mIgM. mIgD expression progressively decreases with increasing HEL-Ig Tgn B cell age. These observations suggest that self Ag-specific B cells can survive in the presence of soluble self Ag by down-regulating mIg expression, which should limit B cell signaling by Ag that might otherwise cause deletion of these cells.

摘要

为了确定慢性抗原刺激对B细胞存活和表型的影响,我们比较了缺乏卵清溶菌酶(HEL)的Ig转基因(Tgn)小鼠和表达可溶性HEL的HEL-Ig转基因小鼠中HEL特异性B细胞的存活情况和表面标志物。通过给HEL-Ig Tgn小鼠喂食锌来最大化血清HEL水平,锌可激活调节HEL表达的金属硫蛋白启动子。通过热稳定抗原、B220的表达来表征B细胞年龄,通过用抗IL-7单克隆抗体抑制淋巴细胞生成时评估B细胞数量的变化以及通过5-溴-2'-脱氧尿苷掺入来鉴定新生成的B细胞,研究B细胞存活情况。我们的观察结果表明,与Ig Tgn小鼠相比,HEL-Ig Tgn小鼠中B细胞的平均寿命显著缩短,但也表明一些HEL-Ig Tgn B细胞可存活至成熟。这些存活的B细胞中有一些经历了受体编辑(用内源性Ig轻链替代转基因Ig轻链),因此它们结合HEL的能力降低或丧失。保留HEL特异性的存活HEL-Ig Tgn B细胞表达的mIgD减少,mIgM很少或不表达。随着HEL-Ig Tgn B细胞年龄的增加,mIgD表达逐渐降低。这些观察结果表明,自身抗原特异性B细胞可以通过下调mIg表达在可溶性自身抗原存在的情况下存活,这应该会限制可能导致这些细胞缺失的抗原对B细胞的信号传导。

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