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Creation of Golden Gate constructs for gene doctoring

机译:基因译者的Golden Gate构造的创建

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摘要

Construction of pDOC-GG and its use to produce Gene Doctoring donor plasmids and perform chromosomal modifications. The first three stages describe the production of pDOC-GG. 1) Three DNA fragments (brown arrows) were designed, based on pDOC-K, to form the backbone of pDOC-GG. Significant features of pDOC-K are displayed. White boxes represent multiple cloning sites (MCS) 1 and 2; dark green arrows represent PCR primers sacB_GA_F and sacB_GA_R used to obtain fragment pDOC_sacB. Other fragments were produced by chemical synthesis. 2) Full features of the three fragments designed from pDOC-K and two further fragments to introduce new genetic elements. Light green arrows represent promoters. 3) Significant features of pDOC-GG, which was produced by Gibson assembly of the five fragments. The last three stages describe the construction of mutagenesis cassettes in pDOC-GG, and use of the resulting donor plasmid for Gene Doctoring. 4) BsaI overhangs (coloured boxes) for homologous regions (HR) 1 and 2 should be complementary to the CTAC and ACGA overhangs generated on pDOC-GG. Multiple intervening parts (Pt. A – X) are assembled sequentially by design of appropriate complementary BsaI overhangs. 5) and 6) The donor plasmid is used for Gene Doctoring as described by Lee et al. [1]
机译:PDOC-GG的构建及其用于生产基因培养给运动质粒并进行染色体修饰。前三个阶段描述了PDOC-GG的生产。 1)基于PDOC-K设计了三种DNA片段(棕色箭头),以形成PDOC-GG的骨架。显示PDOC-K的显着特征。白色盒子代表多个克隆网站(MCS)1和2;深绿色箭头代表PCR引物SACB_GA_F和SACB_GA_R用于获得片段PDOC_SACB。其他碎片是通过化学合成产生的。 2)三个片段的完整特征,由Pdoc-k和另外两片碎片引入新的遗传元素。浅绿色箭头代表启动子。 3)PDOC-GG的显着特征,由五个片段的Gibson组装生产。最后三个阶段描述了PDOC-GG中诱变盒的构建,并使用所得供体质粒进行基因博士。 4)同源地区(HR)1和2的BSAI悬垂(色盒)应与PDOC-GG产生的CTAC和ACGA悬垂互补。通过设计适当的互补bsai悬垂来顺序组装多个介入部分(Pt.A-X)。 5)和6)如Lee等人所述,供体质粒用于基因译者。 [1]

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