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电喷雾串联质谱快速区分核苷酸磷酰胺非对映异构体。

Rapid differentiation of nucleotide phosphoramidate diastereomers by electrospray ionization tandem mass spectrometry.

机构信息

Pharmasset, Inc., 303A College Road East, Princeton, NJ 08540, USA.

出版信息

Rapid Commun Mass Spectrom. 2012 Aug 30;26(16):1887-92. doi: 10.1002/rcm.6307.

DOI:10.1002/rcm.6307
PMID:22777791
Abstract

RATIONALE

Nucleotide phosphoramidates are prodrugs which effectively deliver the active nucleotide to target tissues. It was shown that the individual phosphoramidate diastereomers have different antiviral activity, although the active nucleotide is the same. Therefore, a fast and simple analytical method is needed to characterize the individual diastereomeric phosphoramidate prodrugs.

METHODS

Stock solutions of diastereomeric nucleotide phosphoramidate prodrugs, i.e., 5'-phosphate derivatives of the β-D-2'-deoxy-2'-α-fluoro-2'-β-C-methyluridine nucleotide, were made in 25% acetonitrile to achieve a final concentration of 10 µg/mL. The samples were studied using high-performance liquid chromatography (HPLC) coupled with electrospray ionization tandem mass spectrometry (ESI-MS/MS).

RESULTS

The MS/MS spectra of diastereomeric pairs showed substantial differences in the relative abundances of a characteristic ion in negative mode, which is proposed to be a cyclic phosphoramidate ion. Results were confirmed by the MS/MS spectrum of an analog without the NH proton and deuterium exchange experiment. Furthermore, the diastereomer-specific fragmentation behavior in negative ESI-MS was used to characterize a series of nucleotide phosphoramidates with different amino acid and aromatic substituents.

CONCLUSIONS

An HPLC/MS/MS method was developed for the differentiation of the diastereomers of phosphoramidate prodrugs. In negative mode MS/MS spectra, the cyclic phosphoramidate ions yielded unambiguous distinction. This method presented a rapid and simple way for the characterization of nucleotide phosphoramidates.

摘要

理由

核苷酸膦酸酯是前药,可有效地将活性核苷酸递送到靶组织。研究表明,尽管活性核苷酸相同,但单个膦酸酯非对映异构体具有不同的抗病毒活性。因此,需要一种快速简单的分析方法来表征单个非对映异构体膦酸酯前药。

方法

将非对映异构体核苷酸膦酸酯前药的储备溶液,即β-D-2'-脱氧-2'-α-氟-2'-β-C-甲基尿苷核苷酸的 5'-磷酸酯衍生物,在 25%乙腈中制成终浓度为 10μg/mL 的溶液。使用高效液相色谱(HPLC)与电喷雾串联质谱(ESI-MS/MS)联用对样品进行研究。

结果

非对映异构体对的 MS/MS 光谱在负模式下特征离子的相对丰度上存在显着差异,该离子被提议为环状膦酸酯离子。通过无 NH 质子的 MS/MS 光谱和氘交换实验对结果进行了确认。此外,负 ESI-MS 中对映体特异性的碎裂行为用于表征一系列具有不同氨基酸和芳基取代基的核苷酸膦酸酯。

结论

开发了一种用于区分膦酸酯前药非对映异构体的 HPLC/MS/MS 方法。在负模式 MS/MS 光谱中,环状膦酸酯离子产生了明确的区分。该方法为核苷酸膦酸酯的表征提供了一种快速简单的方法。

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