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首页> 外文期刊>Journal of biosciences >Homology modelling and bivalent single-chain Fv construction of anti-HepG2 single-chain immunoglobulin Fv fragments from a phage display library
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Homology modelling and bivalent single-chain Fv construction of anti-HepG2 single-chain immunoglobulin Fv fragments from a phage display library

机译:噬菌体展示文库中抗HepG2单链免疫球蛋白Fv片段的同源性建模和二价单链Fv构建

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We prepared single-chain immunoglobulin Fv fragments (scFv) SLH10 specific for the HepG2 cell line after biopanning from a large human-na?ˉve phage display library (Griffin. 1 Library). The three-dimensional (3D) structure of SLH10 was modelled by the Insight II molecule simulation software. The structure was refined using the molecular dynamics method. The structures with the least steric clashes and lowest energy were determined finally. The optimized structures of heavy (VH) and light (VL) variable chains of SLH10 scFv were obtained. Then SLH10 bivalent single-chain Fv (BsFv) was constructed that would be suitable for high-affinity targeting. SLH10 BsFv was generated by linking scFvs together and identified by sequencing. Its expression products were confirmed by western blot analysis. The relative molecular masses of scFv and BsFv were approximately 30 kDa and 60 kDa, respectively. Flow cytometry revealed that SLH10 BsFv bound the selected cell lines with greater signal intensity than the parental scFv. The improved antigen binding of SLH10 BsFv may be useful for immunodiagnostics or targeted gene therapy for liver cancer.
机译:我们从一个大型人幼稚噬菌体展示文库(Griffin。1文库)进行生物淘选后,制备了对HepG2细胞系特异的单链免疫球蛋白Fv片段(scFv)SLH10。 SLH10的三维(3D)结构由Insight II分子模拟软件建模。使用分子动力学方法精制结构。最终确定了具有最小空间碰撞和最低能量的结构。获得了SLH10 scFv的重链(VH)和轻链(VL)的优化结构。然后构建适合高亲和力靶向的SLH10二价单链Fv(BsFv)。通过将scFv连接在一起生成SLH10 BsFv,并通过测序进行鉴定。通过Western印迹分析证实其表达产物。 scFv和BsFv的相对分子质量分别约为30 kDa和60 kDa。流式细胞仪显示SLH10 BsFv以比亲本scFv更大的信号强度结合选定的细胞系。 SLH10 BsFv的改进的抗原结合可用于肝癌的免疫诊断或靶向基因治疗。

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