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序列编码吗啉代寡核苷酸的设计与合成

Conception and Synthesis of Sequence-Coded Morpholinos.

作者信息

Pousse Benoit, Al Ouahabi Abdelaziz, Baxter Paul N W, Charles Laurence, Lutz Jean-François

机构信息

CNRS, ISIS, Université de Strasbourg, 8 allée Gaspard Monge, Strasbourg, 67000, France.

CNRS, Institut Charles Sadron UPR22, Université de Strasbourg, 23 rue du Loess Cedex 2, Strasbourg, 67034, France.

出版信息

Chemistry. 2025 May 22;31(29):e202501161. doi: 10.1002/chem.202501161. Epub 2025 Apr 29.

Abstract

Solid-phase morpholino chemistry was explored as a new route to synthesize abiological sequence-defined oligomers. Two comonomers, 0 and 1 containing (i) a chlorophosphoramidate reactive function, (ii) a trityl-protected morpholine, and (iii) a coding substituent (H or CH for 0 and 1, respectively) on the morpholine ring were first synthesized and characterized. This binary alphabet was afterwards tested for the synthesis of digitally-encoded oligomers with different lengths and sequences. The oligomers were prepared on a modified polystyrene resin, cleaved, and characterized by liquid chromatography mass spectrometry. When using a repetitive cycle containing only morpholino coupling and trityl deprotection steps, the formed oligomers were not uniform. Thus, an additional capping step was added. In these conditions, uniform coded sequences were prepared in most cases. Furthermore, the oligomers were analyzed by tandem mass spectrometry. In the studied collision-induced dissociation conditions, the repeat units of the oligomers undergo two main-chain fragmentations and full sequence coverage was observed for all studied sequences. Therefore, the binary messages stored in the oligomers could be decoded and retrieved in all cases.

摘要

探索了固相吗啉化学作为合成无生物序列定义低聚物的新途径。首先合成并表征了两种共聚单体0和1,它们含有:(i) 氯代磷酰胺活性官能团;(ii) 三苯甲基保护的吗啉;(iii) 吗啉环上的编码取代基(分别为0和1的H或CH)。之后对这个二元字母表进行了测试,用于合成不同长度和序列的数字编码低聚物。在改性聚苯乙烯树脂上制备低聚物,进行切割,并通过液相色谱-质谱进行表征。当使用仅包含吗啉偶联和三苯甲基脱保护步骤的重复循环时,形成的低聚物不均匀。因此,添加了一个额外的封端步骤。在这些条件下,大多数情况下都制备出了均匀的编码序列。此外,通过串联质谱对低聚物进行了分析。在所研究的碰撞诱导解离条件下,低聚物的重复单元经历两种主链断裂,并且对所有研究序列都观察到了完整的序列覆盖。因此,在所有情况下,存储在低聚物中的二元信息都可以被解码和检索。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b51d/12099184/39968a54e39e/CHEM-31-e202501161-g007.jpg

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