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建立电荷反转衍生化策略以提高利马前列素的电离效率,并通过专属中性丢失和存活产率法研究利马前列素衍生物的裂解模式。

Establishment of a Charge Reversal Derivatization Strategy to Improve the Ionization Efficiency of Limaprost and Investigation of the Fragmentation Patterns of Limaprost Derivatives Via Exclusive Neutral Loss and Survival Yield Method.

作者信息

Sun Dong, Meng Xiangjun, Ren Tianming, Fawcett John Paul, Wang Hualu, Gu Jingkai

机构信息

Research Center for Drug Metabolism, Jilin University, Changchun, 130012, People's Republic of China.

Beijing Xiuzheng Innovation Medicine Research Institute Co. Ltd., Beijing, 102209, People's Republic of China.

出版信息

J Am Soc Mass Spectrom. 2018 Jul;29(7):1365-1375. doi: 10.1007/s13361-018-1924-z. Epub 2018 Apr 9.

DOI:10.1007/s13361-018-1924-z
PMID:29633222
Abstract

Sensitivity is generally an issue in bioassays of prostaglandins and their synthetic analogs due to their extremely low concentration in vivo. To improve the ionization efficiency of limaprost, an oral prostaglandin E1 (PGE1) synthetic analog, we investigated a charge reversal derivatization strategy in electrospray ionization mass spectrometry (ESI-MS). We established that the cholamine derivative exhibits much greater signal intensity in the positive-ion mode compared with limaprost in the negative ion mode. Collision-induced dissociation (CID) involved exclusive neutral mass loss and positive charge migration to form stable cationic product ions with the positive charge on the limaprost residue rather than on the modifying group. This has the effect of maintaining the efficiency and specificity of multiple reaction monitoring (MRM) and avoiding cross talk. CID fragmentation patterns of other limaprost derivatives allowed us to relate the dissociation tendency of different neutral leaving groups to an internal energy distribution scale based on the survival yield method. Knowledge of the energy involved in the production of stabilized positive ions will potentially assist the selection of suitable derivatization reagents for the analysis of a wide variety of lipid acids. Graphical Abstract ᅟ.

摘要

由于前列腺素及其合成类似物在体内的浓度极低,其灵敏度在生物测定中通常是一个问题。为了提高利马前列素(一种口服前列腺素E1(PGE1)合成类似物)的电离效率,我们在电喷雾电离质谱(ESI-MS)中研究了一种电荷反转衍生化策略。我们发现,与负离子模式下的利马前列素相比,胆碱衍生物在正离子模式下表现出更高的信号强度。碰撞诱导解离(CID)涉及唯一的中性质量损失和正电荷迁移,以形成稳定的阳离子产物离子,正电荷位于利马前列素残基上而非修饰基团上。这有助于维持多反应监测(MRM)的效率和特异性,并避免串扰。其他利马前列素衍生物的CID裂解模式使我们能够基于存活产率法将不同中性离去基团的解离趋势与内能分布尺度联系起来。了解稳定正离子产生过程中涉及的能量可能有助于为各种脂肪酸的分析选择合适的衍生化试剂。图形摘要ᅟ。

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