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寡核苷酸合成过程中的酸结合与脱三苯甲基反应。

Acid binding and detritylation during oligonucleotide synthesis.

作者信息

Paul C H, Royappa A T

机构信息

PerSeptive Biosystems, Framingham, MA 01701, USA.

出版信息

Nucleic Acids Res. 1996 Aug 1;24(15):3048-52. doi: 10.1093/nar/24.15.3048.

Abstract

Under the conditions normally used for detritylation in oligonucleotide synthesis, the haloacetic acid binds strongly to the oligonucleotide. Acetonitrile also forms a complex with the deblocking acid, in competition with the oligonucleotide, and drastically slows detritylation. Incomplete removal of acetonitrile during the deblock step may slow the kinetics enough to result in incomplete detritylation of the oligonucleotide. Acid binding to the growing oligonucleotide causes striking chromatographic effects in the presence of high oligonucleotide mass densities. In packed-bed column reactors, at low linear velocities, the acid binding almost completely depletes free acid from the deblocking solution. This results in an advancing zone within which the oligonucleotide is saturated with acid. Detritylation occurs mostly in a narrow band at the front of the advancing saturated zone. Increasing the DCA concentration in order to achieve quick saturation can give faster and more complete detritylation while minimizing the exposure time of the oligonucleotide to acid.

摘要

在寡核苷酸合成中通常用于脱三苯甲基化的条件下,卤代乙酸会与寡核苷酸强烈结合。乙腈也会与去保护酸形成复合物,与寡核苷酸竞争,从而极大地减缓脱三苯甲基化反应。在去保护步骤中,如果乙腈没有完全去除,可能会使反应动力学足够慢,导致寡核苷酸脱三苯甲基化不完全。在高寡核苷酸质量密度存在的情况下,酸与生长中的寡核苷酸结合会产生显著的色谱效应。在填充床柱反应器中,在低线性流速下,酸结合几乎会使去保护溶液中的游离酸完全耗尽。这会导致一个前进区,在该区内寡核苷酸被酸饱和。脱三苯甲基化主要发生在前进的饱和区前端的一个窄带内。增加二氯乙酸(DCA)浓度以实现快速饱和,可以使脱三苯甲基化更快、更完全,同时将寡核苷酸与酸的接触时间降至最低。

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