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Effects of spatial configuration on tumor cellstransgene expression

机译:空间构型对肿瘤细胞转基因表达的影响

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We investigated the impact of the multicellular architecture on transgene expression of LM05e and LM3 spontaneous Balb/c-mammary adenocarcinoma and HEp-2 human laryngeal squamous carcinoma cell lines. When transferred from monolayers to spheroids, tumor cells strongly enhanced transient transgene expression, which surprisingly was still detectable 75 days after lipofection. The cytomegalovirus immediate early promoter (CMVie) yielded a very high β-galactosidase (βgal) transgene expression, which resulted 8-, 6- and 3-fold greater in LM05e, LM3 and HEp-2 spheroids than the corresponding monolayers. The SV40 early promoter displayed both, a lower spheroids/monolayers ratio and about 10% of βgal expression driven by CMVie. Cis-addition of Epstein Barr virus EBNA-1/oriP cassette enhanced the CMVie-driven transgene expression only in human HEp-2. Deletion of a 325 bp 5’ fragment of the CMVie promoter dropped spheroids βgal expression to 5%. This effect was restored to 10-25% or 25-60% by the insertion of one KCS (18 bp) or four myc-max consensus sequences (67 bp). Whenspheroids disassembled and grew as monolayers, βgal activity dropped accordingly
机译:我们调查了多细胞架构对LM05e和LM3自发Balb / c-乳腺腺癌和HEp-2人喉鳞状细胞癌细胞系转基因表达的影响。当从单层转移到球体时,肿瘤细胞强烈增强了瞬时转基因表达,令人惊讶的是,在脂质转染后75天仍可检测到。巨细胞病毒立即早期启动子(CMVie)产生了非常高的β-半乳糖苷酶(βgal)转基因表达,与相应的单层相比,LM05e,LM3和HEp-2球体的表达分别高8、6和3倍。 SV40早期启动子显示出较低的球状体/单层比率和CMVie驱动的βgal表达的约10%。顺式添加爱泼斯坦巴尔病毒EBNA-1 / oriP盒仅在人HEp-2中增强了CMVie驱动的转基因表达。 CMVie启动子的325 bp 5'片段的缺失使球体βgal的表达降至5%。通过插入一个KCS(18 bp)或四个myc-max共有序列(67 bp),可以将该效果恢复到10-25%或25-60%。当球体分解并以单层形式生长时,βgal活性相应下降

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