School of Applied and Interdisciplinary Sciences, Indian Association for the Cultivation of Science, Kolkata, India.
Curr Protoc. 2023 Feb;3(2):e686. doi: 10.1002/cpz1.686.
Phosphorodiamidate morpholino oligonucleotides (PMOs) are a successful class of antisense reagents that efficiently modulate gene expression. Because PMOs do not follow standard phosphoramidite chemistry, optimized synthetic protocols for these compounds are relatively scarce in the literature. This paper presents detailed protocols for synthesizing full-length PMOs using chlorophosphoramidate chemistry by manual solid-phase synthesis. We first describe the synthesis of Fmoc-protected morpholino hydroxyl monomers, and the corresponding chlorophosphoramidate monomers, from commercially available protected ribonucleosides. The new Fmoc chemistry necessitates the use of a milder base, such as N-ethylmorpholine (NEM), and coupling reagent, such as 5-(ethylthio)-1H-tetrazole (ETT), which are also tolerated for acid-sensitive trityl chemistry. These chlorophosphoramidate monomers are then employed for PMO synthesis in a manual solid-phase procedure using four sequential steps. The synthetic cycle for each nucleotide incorporation consists of (a) deblocking of the 3'-N protecting group using an acidic deblocking cocktail for trityl and base deblocking for Fmoc, (b) neutralization, (c) coupling in the presence of ETT and NEM, and (d) capping of the unreacted morpholine ring-amine. The method uses safe, stable, and inexpensive reagents, and the process is expected to be scalable. After full-length PMO synthesis and ammonia-mediated cleavage from the solid support and deprotection, a range of PMOs with different lengths can be obtained conveniently and efficiently with reproducible good yields. © 2023 Wiley Periodicals LLC. Basic Protocol 1: Synthesis of the novel Fmoc-protected morpholino monomers Basic Protocol 2: Synthesis of the phosphorylating reagent (N,N-dimethylphosphoramic dichloride) required for chlorophosphoramidate monomer synthesis Basic Protocol 3: Synthesis of chlorophosphoramidate monomers of Fmoc-protected morpholino monomers Basic Protocol 4: Solution-phase standardization of dimer and trimer PMO synthesis using Fmoc chemistry Basic Protocol 5: Solid-phase synthesis, purification, and characterization of full-length (25-mer) no-tail PMO using both trityl and Fmoc chemistry.
磷酰胺酯吗啉寡核苷酸 (PMO) 是一类成功的反义试剂,可有效调节基因表达。由于 PMO 不遵循标准的亚磷酰胺化学,因此这些化合物的优化合成方案在文献中相对较少。本文介绍了使用氯磷酰胺化学通过手动固相合成合成全长 PMO 的详细方案。我们首先描述了从商业上可获得的保护核苷中合成 Fmoc 保护的吗啉羟基单体和相应的氯磷酰胺单体。新的 Fmoc 化学需要使用更温和的碱,如 N-乙基吗啉 (NEM) 和偶联试剂,如 5-(乙基硫代)-1H-四唑 (ETT),它们也可耐受酸敏感的三苯甲基化学。然后,这些氯磷酰胺单体用于手动固相程序中的 PMO 合成,共进行四个连续步骤。每个核苷酸掺入的合成循环包括:(a) 使用酸性脱保护剂混合物脱保护 3'-N 保护基团,用于三苯甲基脱保护和 Fmoc 碱基脱保护,(b) 中和,(c) 在 ETT 和 NEM 存在下偶联,以及 (d) 封闭未反应的吗啉环-胺。该方法使用安全、稳定且廉价的试剂,预计该过程可规模化。全长 PMO 合成完成后,通过氨介导从固相载体上切割并脱保护,可方便、高效地获得不同长度的一系列 PMO,产率重现性良好。© 2023 Wiley Periodicals LLC. 基本方案 1:新型 Fmoc 保护的吗啉单体的合成 基本方案 2:用于氯磷酰胺单体合成的磷酰化试剂(N,N-二甲基磷酰胺二氯)的合成 基本方案 3:Fmoc 保护的吗啉单体的氯磷酰胺单体的合成 基本方案 4:使用 Fmoc 化学进行二聚体和三聚体 PMO 合成的溶液相标准化 基本方案 5:使用三苯甲基和 Fmoc 化学通过固相合成、纯化和表征全长(25 -mer)无尾 PMO。
