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甲萘醌(维生素K3)和2,4-二硝基苯基配体与一种骨髓瘤蛋白及一些传统抗体的奇特交叉反应。

The strange cross-reaction of menadione (vitamin K3) and 2,4-dinitrophenyl ligands with a myeloma protein and some conventional antibodies.

作者信息

Michaelides M C, Eisen H N

出版信息

J Exp Med. 1974 Sep 1;140(3):687-702. doi: 10.1084/jem.140.3.687.

Abstract

To explore the possibility that the affinity of some myeloma proteins for 2,4-dinitrophenyl (DNP) ligands is the consequence of a "strange" (i.e., unexpected) cross-reaction for more natural ligands, a variety of substances (primarily derivatives of purines, pyrimidines, naphthaquinone) were tested for ability to block the binding of [(3)H]-epsilon-DNP-L-lysine by protein 315, an IgA mouse myeloma protein with high affinity for DNP ligands. The most impressive inhibiting activity was observed with 2-methyl-1,4-napthaquinone (menadione, vitamin K(3)). The affinity (intrinsic association constant) of protein 315 for menadione was 5 x 10(5) L/M (at 4 degrees C). Because the same affinity was measured in direct-binding assays (e.g., equilibrium dialysis) and in an indirect one based on the assumption of competitive binding with DNP-lysine, it is likely that menadione and DNP bind at overlapping sites in the protein's combining region. This conclusion is supported by molecular models which reveal some common structural features in these ligands. Hence it is not surprising that antinitrophenyl antibody preparations, raised by conventional immunization procedures (anti-2,4-DNP; anti-2,6-DNP; anti-2,4,6-TNP) also bind menadione with considerable affinity. As with DNP ligands, when menadione binds to protein 315 or to conventional antinitrophenyl antibodies, some of the protein's tryptophan fluorescence is quenched, there is a change in the ligand's absorption spectrum (hypochromia and/or red shift), and the binding is temperature-dependent (exothermal).

摘要

为了探究某些骨髓瘤蛋白对2,4 -二硝基苯基(DNP)配体的亲和力是否是对更天然配体产生“奇怪”(即意外)交叉反应的结果,测试了多种物质(主要是嘌呤、嘧啶、萘醌的衍生物)阻断蛋白315(一种对DNP配体具有高亲和力的IgA小鼠骨髓瘤蛋白)与[(3)H]-ε-DNP-L-赖氨酸结合的能力。观察到2-甲基-1,4-萘醌(甲萘醌,维生素K(3))具有最显著的抑制活性。蛋白315对甲萘醌的亲和力(内在缔合常数)为5×10(5) L/M(在4℃时)。因为在直接结合测定(如平衡透析)和基于与DNP-赖氨酸竞争结合假设的间接测定中测得相同的亲和力,所以甲萘醌和DNP可能在蛋白质结合区域的重叠位点结合。分子模型支持了这一结论,该模型揭示了这些配体中的一些共同结构特征。因此,通过常规免疫程序制备的抗硝基苯基抗体制剂(抗-2,4-DNP;抗-2,6-DNP;抗-2,4,6-TNP)也以相当高的亲和力结合甲萘醌就不足为奇了。与DNP配体一样,当甲萘醌与蛋白315或常规抗硝基苯基抗体结合时,蛋白质的一些色氨酸荧光会猝灭,配体的吸收光谱会发生变化(减色和/或红移),并且结合是温度依赖性的(放热)。

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