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能够在内体中低pH值条件下释放白喉毒素的抗体。

Antibodies capable of releasing diphtheria toxin in response to the low pH found in endosomes.

作者信息

Raso V, Brown M, McGrath J, Liu S, Stafford W F

机构信息

Boston Biomedical Research Institute, Boston, Massachusetts 02114, USA.

出版信息

J Biol Chem. 1997 Oct 31;272(44):27618-22. doi: 10.1074/jbc.272.44.27618.

Abstract

Diphtheria toxin (DT) undergoes a rapid conformational change in response to the acidity encountered within endosomes. That transition is integral to the passage of its catalytic domain into the cytosol and thus its lethal action. The importance of this translocation mechanism led us to develop several monoclonal antibodies that bind DT at neutral pH but spontaneously release the toxin when critical epitopes denature or unfold upon lowering the pH to 4.5-5.5. Hybridomas were selected using a microtiter plate assay that measured the pH-dependent detachment of antibody from immobilized toxin. The acid-sensitive epitopes involved were on the catalytic, transmembrane, and receptor binding domains of DT. This pH-induced disruption of the binding of toxin to these monoclonal antibodies was analyzed by sedimentation velocity ultracentrifugation. Antibody combining sites were fully occupied at pH 5.5, partially bound at pH 5.0, and totally empty at pH 4.5. It was estimated that the Ka for antibody-toxin binding was approximately 1000-fold lower at pH 5.0 than at neutral pH. This novel acid-triggered release mechanism provides a basis for delivery of antibody-bound toxin into cells accompanied by its immediate dissociation as the complex enters acidic vesicles.

摘要

白喉毒素(DT)会因内体中遇到的酸性环境而迅速发生构象变化。这种转变对于其催化结构域进入细胞质从而发挥致死作用至关重要。这种转运机制的重要性促使我们开发了几种单克隆抗体,这些抗体在中性pH值下与DT结合,但当pH值降至4.5 - 5.5时,关键表位变性或展开,抗体就会自发释放毒素。使用微量滴定板分析法筛选杂交瘤,该方法可测量抗体从固定化毒素上的pH依赖性解离。所涉及的酸敏感表位位于DT的催化、跨膜和受体结合结构域上。通过沉降速度超速离心法分析了pH诱导的毒素与这些单克隆抗体结合的破坏情况。在pH 5.5时抗体结合位点被完全占据,在pH 5.0时部分结合,在pH 4.5时完全空出。据估计,在pH 5.0时抗体与毒素结合的Ka值比中性pH值时低约1000倍。这种新型的酸触发释放机制为将抗体结合的毒素递送至细胞提供了基础,当复合物进入酸性囊泡时,毒素会立即解离。

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