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单个胎鼠脾脏的特异性抗原结合细胞群体:库组成、大小和遗传控制。

The specific antigen-binding cell populations of individual fetal mouse spleens: repertoire composition, size, and genetic control.

作者信息

Cohen J E, D'Eustachio P, Edelman G M

出版信息

J Exp Med. 1977 Aug 1;146(2):394-411. doi: 10.1084/jem.146.2.394.

Abstract

In order to analyze the genetic and physiological basis of controls affecting the generation of the repertoire of antigen-binding cells in fetal mice, we have measured the numbers of spleen cells specific for each of four antigens as a function of the total numbers of nucleated and Ig-bearing cells in inbred, hybrid, and random bred fetuses. For each of the two inbred strains BALB/c and CBA/J, the proportion of nucleated cells specific for a given antigen was the same for all individuals of the strain at the 18th day of gestation. The proportion did vary from antigen to antigen, however, and for each antigen the proportion of specific cells observed in CBA/J fetuses was approximately four times that observed in BALB/c fetuses. This difference appeared to be due to a difference between the two strains in the relative size of the repertoire of antigen-binding spleen cells at this stage of development, inasmuch as the frequency of Ig-bearing spleen cells in CBA/J fetuses was likewise approximately four times that observed in BALB/c fetuses. In random bred Swiss-L fetal mice at the 18th day of gestation, the proportion of cells specific for a given antigen varied significantly from one individual to the next. The ratio of proportions of the two antigens observed was constant from individual to individual, however, and this constant ratio differed significantly from the ratio observed for the same two antigens in fetal BALB/c and CBA/J inbred mice. These data suggest that the ontogeny of the repertoire of antigen-binding cells in fetal mice is subject to at least two independent sets of controls, one affecting the relative size of the repertoire in the spleen, and the other affecting the distribution of antigen-binding specificities within that repertoire. Analysis of repertoire size and composition in the spleens of hybrid fetuses confirmed the observation that the two parameters are controlled independently, and suggested further that the control of repertoire size in these fetuses is due to the action of one or a few closely-linked autosomal Mendelian genes. These data are consistent with models for the origin of antibody diversity in which the genes coding for the full repertoire of antibodies are generated somatically from a small number of germ-line genes early in development and in the absence of any strong positive or negative selection with respect to antigenic specificity.

摘要

为了分析影响胎鼠抗原结合细胞库产生的调控的遗传和生理基础,我们测定了四种抗原各自特异性的脾细胞数量,作为近交系、杂交系和随机繁殖胎鼠中有核细胞和含免疫球蛋白细胞总数的函数。对于两个近交系BALB/c和CBA/J中的每一个,在妊娠第18天时,特定抗原特异性的有核细胞比例在该品系的所有个体中是相同的。然而,该比例因抗原而异,并且对于每种抗原,在CBA/J胎鼠中观察到的特异性细胞比例约为在BALB/c胎鼠中观察到的四倍。这种差异似乎是由于在发育的这个阶段,两个品系在抗原结合脾细胞库的相对大小上存在差异,因为CBA/J胎鼠中含免疫球蛋白脾细胞的频率同样约为在BALB/c胎鼠中观察到的四倍。在妊娠第18天的随机繁殖瑞士-L胎鼠中,特定抗原特异性的细胞比例在不同个体之间有显著差异。然而,观察到的两种抗原比例的比值在个体之间是恒定的,并且这个恒定比值与在胎鼠BALB/c和CBA/J近交系中观察到的相同两种抗原的比值有显著差异。这些数据表明,胎鼠抗原结合细胞库的个体发生至少受到两组独立的调控,一组影响脾中细胞库的相对大小,另一组影响该细胞库内抗原结合特异性的分布。对杂交胎鼠脾脏中细胞库大小和组成的分析证实了这两个参数是独立控制的这一观察结果,并进一步表明这些胎鼠中细胞库大小的控制是由于一个或几个紧密连锁的常染色体孟德尔基因的作用。这些数据与抗体多样性起源的模型一致,在该模型中,编码全部抗体库的基因在发育早期从少数种系基因中体细胞产生,并且在没有任何关于抗原特异性的强烈正选择或负选择的情况下。

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The somatic generation of immune recognition.免疫识别的体细胞产生
Eur J Immunol. 1971 Jan;1(1):1-9. doi: 10.1002/eji.1830010102.
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Maturation of the humoral immune response in mice.小鼠体液免疫反应的成熟
J Exp Med. 1974 Feb 1;139(2):249-63. doi: 10.1084/jem.139.2.249.

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