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通过在包膜糖蛋白受体结合区插入单链抗体可变结构域,将逆转录病毒靶向至表达突变型表皮生长因子受体的癌细胞。

Targeting retrovirus to cancer cells expressing a mutant EGF receptor by insertion of a single chain antibody variable domain in the envelope glycoprotein receptor binding lobe.

作者信息

Lorimer I A, Lavictoire S J

机构信息

Ottawa Regional Cancer Centre, Cancer Research Group, 501 Smyth Road, Ottawa, Ontario, Canada, K1H 8L6.

出版信息

J Immunol Methods. 2000 Apr 3;237(1-2):147-57. doi: 10.1016/s0022-1759(99)00219-7.

Abstract

We have investigated targeting of retroviral vectors to a mutant EGF receptor (EGFRvIII) that is expressed in cancers of the brain, breast, lung and ovary, but is not found in any normal tissues. An expression plasmid was made in which a single chain Fv antibody specific for EGFRvIII was inserted at a novel position within a disulphide-bonded surface loop near the native receptor binding site of the Moloney leukemia virus ecotropic envelope glycoprotein. This fusion protein was expressed and incorporated into retroviral particles as efficiently as normal envelope glycoprotein. Retroviral vectors made with the fusion protein were able to bind peptide antigen and EGFRvIII expressed on the surface of human glioblastoma cells. The retroviral vectors had normal levels of infectivity on mouse cells, showing that the envelope glycoprotein tolerated a large insertion at this site, but did not show significant infectivity to human cells expressing EGFRvIII. Thus we were able to redirect retrovirus binding to this tumour-specific target without perturbing the normal function of the ecotropic envelope glycoprotein, but this was not sufficient to mediate infectivity via this receptor.

摘要

我们研究了将逆转录病毒载体靶向一种突变型表皮生长因子受体(EGFRvIII),该受体在脑癌、乳腺癌、肺癌和卵巢癌中表达,但在任何正常组织中均未发现。构建了一种表达质粒,其中对EGFRvIII具有特异性的单链Fv抗体被插入到莫洛尼白血病病毒嗜亲性包膜糖蛋白天然受体结合位点附近的一个二硫键连接的表面环内的一个新位置。这种融合蛋白能够表达,并与正常包膜糖蛋白一样高效地整合到逆转录病毒颗粒中。用该融合蛋白制备的逆转录病毒载体能够结合人胶质母细胞瘤细胞表面表达的肽抗原和EGFRvIII。这些逆转录病毒载体对小鼠细胞具有正常水平的感染性,表明包膜糖蛋白在该位点能够耐受较大的插入,但对表达EGFRvIII的人细胞没有显著的感染性。因此,我们能够将逆转录病毒的结合重定向到这个肿瘤特异性靶点,而不干扰嗜亲性包膜糖蛋白的正常功能,但这不足以通过该受体介导感染性。

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