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高效反向(5'→3')合成复杂 DNA 微阵列。

High-Efficiency Reverse (5'→3') Synthesis of Complex DNA Microarrays.

机构信息

Institute of Inorganic Chemistry, Faculty of Chemistry, University of Vienna, Vienna, Austria.

Department of Physiological Chemistry, Christian Doppler Laboratory for Bioactive Aroma Compounds, Faculty of Chemistry, University of Vienna, Vienna, Austria.

出版信息

Sci Rep. 2018 Oct 10;8(1):15099. doi: 10.1038/s41598-018-33311-3.

Abstract

DNA microarrays are important analytical tools in genetics and have recently found multiple new biotechnological roles in applications requiring free 3' terminal hydroxyl groups, particularly as a starting point for enzymatic extension via DNA or RNA polymerases. Here we demonstrate the highly efficient reverse synthesis of complex DNA arrays using a photolithographic approach. The method is analogous to conventional solid phase synthesis but makes use of phosphoramidites with the benzoyl-2-(2-nitrophenyl)-propoxycarbonyl (BzNPPOC) photolabile protecting group on the 3'-hydroxyl group. The use of BzNPPOC, with more than twice the photolytic efficiency of the 2-(2-nitrophenyl)-propoxycarbonyl (NPPOC) previously used for 5'→3' synthesis, combined with additional optimizations to the coupling and oxidation reactions results in an approximately 3-fold improvement in the reverse synthesis efficiency of complex arrays of DNA oligonucleotides. The coupling efficiencies of the reverse phosphoramidites are as good as those of regular phosphoramidites, resulting in comparable yields. Microarrays of DNA surface tethered on the 5' end and with free 3' hydroxyl termini can be synthesized quickly and with similarly high stepwise coupling efficiency as microarrays using conventional 3'→5' synthesis.

摘要

DNA 微阵列是遗传学中重要的分析工具,最近在需要游离 3'末端羟基的多种新生物技术应用中发现了多个新的作用,特别是作为通过 DNA 或 RNA 聚合酶进行酶延伸的起始点。在这里,我们展示了使用光刻技术高效地反向合成复杂 DNA 微阵列。该方法类似于传统的固相合成,但利用在 3'羟基上带有苯甲酰基-2-(2-硝基苯基)-丙氧羰基(BzNPPOC)光不稳定保护基的亚磷酰胺。BzNPPOC 的使用效率比以前用于 5'→3'合成的 2-(2-硝基苯基)-丙氧羰基(NPPOC)高两倍多,与偶联和氧化反应的额外优化相结合,导致复杂 DNA 寡核苷酸反向合成效率提高了约 3 倍。反向亚磷酰胺的偶联效率与常规亚磷酰胺一样好,因此产量相当。5'端连接的 DNA 表面微阵列和游离 3'末端羟基可以快速合成,并且与使用常规 3'→5'合成的微阵列一样具有类似的高逐步偶联效率。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a3ea/6180089/14394a399b9b/41598_2018_33311_Fig1_HTML.jpg

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