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首页> 外文期刊>Chemistry: A European journal >Liquid-Phase Synthesis of 2-Methyl-RNA on a Homostar Support through Organic-Solvent Nanofiltration
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Liquid-Phase Synthesis of 2-Methyl-RNA on a Homostar Support through Organic-Solvent Nanofiltration

机译:通过有机溶剂纳米过滤,在Homostar载体上液相合成2-甲基RNA

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Due to the discovery of RNAi, oligonucleotides (oligos) have re-emerged as a major pharmaceutical target that may soon be required in ton quantities. However, it is questionable whether solid-phase oligo synthesis (SPOS) methods can provide a scalable synthesis. Liquid-phase oligo synthesis (LPOS) is intrinsically scalable and amenable to standard industrial batch synthesis techniques. However, most reported LPOS strategies rely upon at least one precipitation per chain extension cycle to separate the growing oligonucleotide from reaction debris. Precipitation can be difficult to develop and control on an industrial scale and, because many precipitations would be required to prepare a therapeutic oligonucleotide, we contend that this approach is not viable for large-scale industrial preparation. We are developing an LPOS synthetic strategy for 2-methyl RNA phosphorothioate that is more amenable to standard batch production techniques, using organic solvent nanofiltration (OSN) as the critical scalable separation technology. We report the first LPOS-OSN preparation of a 2-Me RNA phosphorothioate 9-mer, using commercial phosphoramidite monomers, and monitoring all reactions by HPLC, (PNMR)-P-31 spectroscopy and MS.
机译:由于RNAi的发现,寡核苷酸(寡核苷酸)已重新出现,成为可能很快需要大量使用的主要药物靶标。但是,固相齐聚物合成(SPOS)方法能否提供可扩展的合成方法值得怀疑。液相低聚合成(LPOS)本质上可扩展,并且符合标准的工业批量合成技术。但是,大多数报道的LPOS策略每个链延伸周期至少依赖一个沉淀来将生长的寡核苷酸与反应碎片分离。沉淀可能难以在工业规模上发展和控制,而且由于制备治疗性寡核苷酸需要许多沉淀,因此我们认为这种方法不适用于大规模工业制备。我们正在开发一种使用有机溶剂纳米过滤(OSN)作为关键的可扩展分离技术的,适用于标准批量生产技术的2-甲基RNA硫代磷酸酯LPOS合成策略。我们报道了使用商业亚磷酰胺单体并通过HPLC,(PNMR)-P-31光谱和MS监测所有反应的第一个LPOS-OSN制备的2-Me RNA硫代磷酸酯9-mer。

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