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Construction of a Fluorescein-Responsive Chimeric Receptor With Strict Ligand Dependency

机译:严格配体依赖性的荧光素反应性嵌合受体的构建

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Since many cell functions are regulated by members of the cytokine receptor superfamily, the artificial mimicry of the cytokine receptor system would be attractive for cellular engineering. We previously showed that an antibody/cytokine receptor chimera can transduce a growth signal in response to non-natural ligands, such as fluorescein-conjugated BSA. However, considerable background of cell proliferation was observed without antigen. Therefore, we redesigned chimeric receptor constructs with different combinations of domains containing anti-fluorescein single chain Fv (ScFv), extracellular D1/D2 as well as transmembrane domains of erythropoietin receptor (EpoR), and the intracellular domain of glycoprotein 130 (gp130), to obtain strictly fluorescein-dependent chimeric receptors. When interleukin-3-dependent Ba/F3 cells were transduced with retroviral vectors encoding individual chimeric receptors, the chimeras either with both D I and D2 domains or without any EpoR extracellular domain attained a strict ligand-dependent ON/OFF regulation.
机译:由于许多细胞功能受细胞因子受体超家族成员的调节,因此细胞因子受体系统的人工模拟对于细胞工程将具有吸引力。我们先前显示,抗体/细胞因子受体嵌合体可以响应非天然配体(例如荧光素偶联的BSA)转导生长信号。然而,在没有抗原的情况下,观察到相当大的细胞增殖背景。因此,我们重新设计了具有不同结构域组合的嵌合受体构建体,这些结构域包含抗荧光素单链Fv(ScFv),细胞外D1 / D2以及促红细胞生成素受体(EpoR)的跨膜结构域和糖蛋白130(gp130)的细胞内结构域,获得严格的荧光素依赖性嵌合受体。用编码单个嵌合受体的逆转录病毒载体转导白介素3依赖性Ba / F3细胞时,具有D I和D2结构域或没有任何EpoR细胞外结构域的嵌合体均达到严格的配体依赖性ON / OFF调节。

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