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抗独特型抗体介导的抗原-抗体结合亲和力增强。

Enhanced antigen-antibody binding affinity mediated by an anti-idiotypic antibody.

作者信息

Sawutz D G, Koury R, Homcy C J

机构信息

Harvard Medical School, Boston, Massachusetts.

出版信息

Biochemistry. 1987 Aug 25;26(17):5275-82. doi: 10.1021/bi00391a010.

Abstract

We previously described the production of four monoclonal antibodies to the beta-adrenergic receptor antagonist alprenolol. One of these antibodies, 5B7 (IgG2a, kappa), was used to raise anti-idiotypic antisera in rabbits. In contrast to the expected results, one of the anti-idiotypic antisera (R9) promotes [125I]iodocyanopindolol (ICYP) binding to antibody 5B7. In the presence of R9, the dissociation constant decreases 100-fold from 20 to 0.3 nM. This increase in binding affinity of antibody 5B7 for ICYP is not observed in the presence of preimmune, rabbit anti-mouse or anti-idiotypic antisera generated to a monoclonal antibody of a different specificity. Furthermore, R9 in the absence of 5B7 does not bind ICYP. The F(ab) fragments of 5B7 and R9 behaved in a similar manner, and the soluble complex responsible for the high-affinity interaction with ICYP can be identified by gel filtration chromatography. The elution position of the complex is consistent with a 5B7 F(ab)-R9 F(ab) dimer, indicating that polyvalency is not responsible for the enhanced ligand binding. Kinetic analysis of ICYP-5B7 binding revealed that the rate of ICYP dissociation from 5B7 in the presence of R9 is approximately 100 times slower than in the absence of R9 [k-1(+R9) = 0.025 min-1 vs. k-1(-R9) = 2.04 min-1], consistent with the 100-fold change in binding affinity of 5B7 for ICYP. The available data best fit a model in which an anti-idiotypic antibody binds at or near the binding site of the idiotype participating in the formation of a hybrid ligand binding site.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

我们之前描述了针对β-肾上腺素能受体拮抗剂烯丙洛尔产生的四种单克隆抗体。其中一种抗体5B7(IgG2a,κ)被用于在兔体内产生抗独特型抗血清。与预期结果相反,其中一种抗独特型抗血清(R9)促进[125I]碘氰吲哚洛尔(ICYP)与抗体5B7结合。在R9存在的情况下,解离常数从20 nM降至0.3 nM,降低了100倍。在存在免疫前血清、兔抗小鼠血清或针对不同特异性单克隆抗体产生的抗独特型抗血清时,未观察到抗体5B7对ICYP结合亲和力的这种增加。此外,在没有5B7的情况下,R9不结合ICYP。5B7和R9的F(ab)片段表现出相似的行为,并且负责与ICYP高亲和力相互作用的可溶性复合物可通过凝胶过滤色谱法鉴定。该复合物的洗脱位置与5B7 F(ab)-R9 F(ab)二聚体一致,表明多价性不是增强配体结合的原因。ICYP-5B7结合的动力学分析表明,在R9存在的情况下,ICYP从5B7解离的速率比不存在R9时慢约100倍[k-1(+R9) = 0.025 min-1 vs. k-1(-R9) = 2.04 min-1],这与5B7对ICYP结合亲和力的100倍变化一致。现有数据最符合一种模型,即抗独特型抗体在参与形成杂合配体结合位点的独特型结合位点处或附近结合。(摘要截断于250字)

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