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调整下一代马来酰亚胺交联剂的水解稳定性可获得白蛋白-抗体片段偶联物和三 scFv。

Tuning the Hydrolytic Stability of Next Generation Maleimide Cross-Linkers Enables Access to Albumin-Antibody Fragment Conjugates and tri-scFvs.

机构信息

Department of Chemistry, University College London , 20 Gordon Street, London, WC1H OAJ, United Kingdom.

Cancer Institute, University College London , 72 Huntley Street, London, WC1E 6BT, United Kingdom.

出版信息

Bioconjug Chem. 2018 Feb 21;29(2):486-492. doi: 10.1021/acs.bioconjchem.7b00795. Epub 2018 Jan 31.

Abstract

We describe investigations to expand the scope of next generation maleimide cross-linkers for the construction of homogeneous protein-protein conjugates. Diiodomaleimides are shown to offer the ideal properties of rapid bioconjugation with reduced hydrolysis, allowing the cross-linking of even sterically hindered systems. The optimized linkers are exploited to link human serum albumin to antibody fragments (Fab or scFv) as a prospective half-life extension platform, with retention of antigen binding and robust serum stability. Finally, a triprotein conjugate is formed, by linking scFv antibody fragments targeting carcinoembryonic antigen. This tri-scFv is shown to infer a combination of greater antigen avidity and increased in vivo half-life, representing a promising platform for antibody therapeutic development.

摘要

我们描述了扩展下一代马来酰亚胺交联剂范围的研究,用于构建均一的蛋白质-蛋白质缀合物。二碘马来酰亚胺被证明具有快速生物缀合和减少水解的理想特性,允许甚至空间位阻系统的交联。优化的连接子被用于将人血清白蛋白与抗体片段(Fab 或 scFv)连接,作为一种有前途的半衰期延长平台,保留抗原结合和稳健的血清稳定性。最后,通过连接针对癌胚抗原的 scFv 抗体片段,形成三聚体缀合物。该三聚体 scFv 表现出更高的抗原亲和力和体内半衰期的增加,代表了抗体治疗开发的有前途的平台。

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