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具有影响Clq和高亲和力Fc受体结合的单氨基酸取代的重组小鼠单克隆抗体在BALB/c小鼠中具有相同的血清半衰期。

Recombinant mouse monoclonal antibodies with single amino acid substitutions affecting Clq and high affinity Fc receptor binding have identical serum half-lives in the BALB/c mouse.

作者信息

Wawrzynczak E J, Denham S, Parnell G D, Cumber A J, Jones P T, Winter G

机构信息

Drug Targeting and Immunophysiology Laboratories, Institute of Cancer Research, Sutton, Surrey, U.K.

出版信息

Mol Immunol. 1992 Feb;29(2):221-7. doi: 10.1016/0161-5890(92)90103-5.

Abstract

The serum half-lives of three recombinant mouse monoclonal antibodies, differing radically in their ability to bind to Clq or FcRI but only minimally in structure, were determined in the BALB/c mouse following intravenous administration. The wild-type antibody, a chimaeric antibody comprising variable domains binding 3-iodo-4-hydroxy-5-nitrophenylacetate and constant domains of the mouse IgG2b isotype, was eliminated from the bloodstream with biphasic kinetics: alpha-phase, 0.5 days; beta-phase, 7.0 days. The alpha- and beta-phase half-lives of mutant recombinant antibodies with single amino acid substitutions, either Glu 235-Leu allowing binding to the mouse FcRI, or Lys 322-Ala reducing Clq binding 30-fold, were indistinguishable from those of the wild-type antibody demonstrating that the biological half-life of intact mouse IgG is independent of the ability to bind Clq or FcRI. The major implication of the present study is that IgG molecules which have been genetically engineered to eliminate interaction with other components of the immune system should retain the long half-life typical of natural antibodies.

摘要

在BALB/c小鼠静脉注射后,测定了三种重组小鼠单克隆抗体的血清半衰期。这三种抗体在与Clq或FcRI结合的能力上有很大差异,但结构上差异极小。野生型抗体是一种嵌合抗体,其可变区结合3-碘-4-羟基-5-硝基苯乙酸,恒定区为小鼠IgG2b同种型,从血液中消除呈现双相动力学:α相半衰期为0.5天;β相半衰期为7.0天。单氨基酸取代的突变重组抗体,即允许与小鼠FcRI结合的Glu 235-Leu取代,或使Clq结合减少30倍的Lys 322-Ala取代,其α相和β相半衰期与野生型抗体无差异,表明完整小鼠IgG的生物学半衰期与结合Clq或FcRI的能力无关。本研究的主要意义在于,经过基因工程改造以消除与免疫系统其他成分相互作用的IgG分子应保留天然抗体典型的长半衰期。

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