首页> 外文期刊>The Journal of Experomental Medicine >Immunological unresponsiveness to thymus-independent antigens: two fundamentally different genetic mechanisms of B-cell unresponsiveness to dextran
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Immunological unresponsiveness to thymus-independent antigens: two fundamentally different genetic mechanisms of B-cell unresponsiveness to dextran

机译:对胸腺无抗原的免疫无响应:B细胞对葡聚糖的两个基本不同的遗传机制

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The immune response of mice to the α-l-6 epitope of dextran (Dx) B512 was found to be under genetic control. The congenic mouse strains A, A.CA, A.SW, A.TH, and A.TL exhibited a specific defect in their response to α-l-6. Also strain CBA/N was unresponsive to α-1-6, but the mechanism of unresponsiveness was found to be different. Unresponsiveness to α-l-6 in congenic A strains was not due to suppressor cells. Although these strains failed to respond to the α-l-6 epitope, they responded strongly to the hapten Fluorescein isothiocyanate (FITC) conjugated to Dx, indicating that the Dx can function as an efficient carrier in these strains. Dx was a potent polyclonal B-cell activator in congenic A strains as well as in high responder strains. Polyclonally-activating concentrations of lipopolysaccharide (LPS) failed to induce the synthesis of anti-α- l-6 antibodies in congenic A strains, although antibodies of all other specificities studied were produced. However, in high responder strains, LPS induced the synthesis of anti-α-l-6 antibodies. It was concluded that congenic A strains do not express V genes coding for antibodies against α-l-6. In contrast, strain CBA/N failed to respond to both the α-l-6 and FITC epitope on Dx, whereas they could respond to FITC conjugated to horse erythrocytes. Dx induced a very small, if any, polyclonal antibody response in B cells from CBA/N mice or male CBA/N x DBA hybrids, whereas Dx was a very potent polyclonal B-cell activator in female hybrids. It is concluded that CBA/N mice are nonresponders to Dx or haptenated Dx, because the cell population that can respond to the polyclonal B-cell activating properties of Dx is severely depleted.
机译:发现小鼠对葡聚糖(DX)B512的α-L-6表位的免疫应答受到遗传控制。先生小鼠菌株A,A.Ca,A.sw,A.Th和A.TL在α-L-6的响应中表现出特定的缺陷。菌株CBA / N对α-1-6没有响应,但发现没有反应的机制是不同的。对α-L-6的α-L-6在ConciC中的α-L-6没有抑制细胞。虽然这些菌株未能应对α-L-6表位,但它们强烈地反应到与DX缀合的Hapten荧光素异硫氰酸酯(FITC),表明DX可以用作这些菌株中的有效载体。 DX是一种有效的多克隆B细胞活化剂,其菌株以及高响应菌株。脂多糖(LPS)的多克隆活化浓度未能诱导在ConciC A株中的抗α-L-6抗体的合成,尽管所研究的所有其他特异性的抗体。然而,在高响应者菌株中,LPS诱导抗α-L-6抗体的合成。结论是,Congenic A株不会表达编码抗体α-L-6的抗体的V基因。相反,菌株CBA / n未能响应DX上的α-L-6和FITC表位,而它们可以响应与马红细胞缀合的FITC。 DX诱导来自CBA / N小鼠或雄性CBA / N X DBA杂种的B细胞中的非常小,如果有多克隆抗体反应,而DX是在雌性杂交物中是一个非常有效的多克隆B细胞活化剂。得出结论,CBA / N小鼠对DX或Haptenated DX无反应,因为可以响应DX的多克隆B细胞活化性能的细胞群被严重耗尽。

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