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正常和T15独特型抑制的BALB/c小鼠中针对PC-KLH的I组和II组抗体反应的特征分析。

Characterization of the group I and group II antibody response against PC-KLH in normal and T15 idiotype-suppressed BALB/c mice.

作者信息

Bruderer U, Aebersold R, Blaser K, Heusser C H

机构信息

Pharmaceuticals Research Laboratories, Ciba-Geigy Ltd, Basel, Switzerland.

出版信息

Immunology. 1988 Jul;64(3):385-90.

Abstract

The memory response of BALB/c mice to phosphocholine-keyhole limpet haemocyanin (PC-KLH) consists of two antibody populations, designated Group I and Group II, that differ in their fine specificity, as determined by hapten inhibition using phosphocholine (PC) and p-nitrophenylphosphocholine (NPPC). It is known that Group I response is dominated by T15 idiotype-positive antibodies that utilize the VH1 heavy-chain gene in combination with V kappa 22 light-chain gene. In this paper we show that Group II serum antibodies of BALB/c mice are also highly restricted in their heterogeneity, as determined by N-terminal amino acid sequence analysis. Furthermore, we demonstrate that the Group II response is not affected by neonatally induced T15 suppression, whereas the Group I response in these mice consists of T15-negative antibodies. This suggests that the expression of the two antibody populations is regulated independently. Finally, we show that the isotype distributions within a fine specificity are the same in normal and T15-suppressed mice. Interestingly this is true not only for the Group II but also for the Group I antibodies. Because the isolated Group I antibodies from normal mice differ in structure from those of T15-suppressed mice, i.e. different light chains, our data indicate that the isotype distribution of these two populations is associated with their fine specificity in addition to their clonal origin.

摘要

BALB/c小鼠对磷酸胆碱-钥孔戚血蓝蛋白(PC-KLH)的记忆反应由两个抗体群体组成,分别命名为I组和II组,通过使用磷酸胆碱(PC)和对硝基苯基磷酸胆碱(NPPC)进行半抗原抑制测定,它们在精细特异性上有所不同。已知I组反应主要由利用VH1重链基因与Vκ22轻链基因组合的T15独特型阳性抗体主导。在本文中,我们表明,通过N端氨基酸序列分析确定,BALB/c小鼠的II组血清抗体在其异质性方面也受到高度限制。此外,我们证明II组反应不受新生期诱导的T15抑制的影响,而这些小鼠中的I组反应由T15阴性抗体组成。这表明这两个抗体群体的表达是独立调节的。最后,我们表明在正常小鼠和T15抑制小鼠中,精细特异性内的同种型分布是相同的。有趣的是,不仅II组如此,I组抗体也是如此。由于从正常小鼠中分离的I组抗体在结构上与T15抑制小鼠的不同,即轻链不同,我们的数据表明,除了它们的克隆起源外,这两个群体的同种型分布还与其精细特异性相关。

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