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TEPC-15种系特异性的晚期克隆选择与扩增。

Late clonal selection and expansion of the TEPC-15 germ-line specificity.

作者信息

Fung J, Köhler H

出版信息

J Exp Med. 1980 Nov 1;152(5):1262-73. doi: 10.1084/jem.152.5.1262.

Abstract

The maturation of the antibody response to phosphorylcholine (PC) in neonatal BALB/c mice was studied. A T cell-independent class 1 1 PC-antigen, 3-(p-azophenyl phosphorylcholine)-N-acetyl-L-tyrosylglycylglycine lipopolysaccharide, was synthesized and used to immunize neonatal mice of different ages. The earliest anti-PC hemolytic plaque-forming response could be induced in 1-d-old neonates. Idiotype analysis on these early anti-PC antibodies showed that the response was not TEPC-15 dominant although TEPC-15-positive plaque-forming cells were detected. However, idiotype analysis of the anti-PC-LPS response in 7 d or older animals indicated that clonal dominance had been established. Similar results were obtained in splenic fragment culture with cells from neonatal livers and spleens. PC-specific precursors were detected in the liver of 1-d-old neonates, whereas the spleen of those animals contained no precursors for PC. Precursors for PC residing in the neonatal liver are not TEPC-15 dominant, whereas the splenic PC precursors of 5- to 6-day-old animals express the TEPC-15 idiotype dominatly. These findings demonstrate that during ontogeny PC-specific B cells appear before the TEPC-15 clone becomes dominant. Thus clonal dominance in the adult anti-PC response and late acquisition of the TEPC-15 specificity during ontogeny do not signify a particularly unique or direct relationship to the expression of genes encoded in the germline.

摘要

研究了新生BALB/c小鼠对磷酸胆碱(PC)抗体反应的成熟过程。合成了一种非T细胞依赖性1类PC抗原,即3-(对偶氮苯基磷酸胆碱)-N-乙酰-L-酪氨酰甘氨酰甘氨酸脂多糖,并用于免疫不同年龄的新生小鼠。最早在1日龄的新生小鼠中可诱导出抗PC溶血空斑形成反应。对这些早期抗PC抗体的独特型分析表明,尽管检测到TEPC-15阳性空斑形成细胞,但该反应并非以TEPC-15为主。然而,对7日龄及以上动物抗PC-LPS反应的独特型分析表明,克隆优势已经确立。用新生小鼠肝脏和脾脏细胞进行脾片段培养也得到了类似结果。在1日龄新生小鼠的肝脏中检测到PC特异性前体细胞,而这些动物的脾脏中不含PC前体细胞。新生小鼠肝脏中的PC前体细胞并非以TEPC-15为主,而5至6日龄动物脾脏中的PC前体细胞则主要表达TEPC-15独特型。这些发现表明,在个体发育过程中,PC特异性B细胞在TEPC-15克隆占主导地位之前就已出现。因此,成年抗PC反应中的克隆优势以及个体发育过程中TEPC-15特异性的后期获得并不意味着与种系中编码基因的表达存在特别独特或直接的关系。

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