| 5-乙酰(苯甲酰)基-4-芳基-3,4-二氢嘧啶-2(1H)-酮的质谱裂解规律 |
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| 引用本文: | 李前荣,沙里海,丁毅,尹浩,郭庆祥.5-乙酰(苯甲酰)基-4-芳基-3,4-二氢嘧啶-2(1H)-酮的质谱裂解规律[J].化学物理学报,2005,18(4):577-584. |
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| 作者姓名: | 李前荣 沙里海 丁毅 尹浩 郭庆祥 |
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| 作者单位: | 中国科学技术大学结构分析重点实验室,中国科学技术大学化学系,安徽大学现代实验技术中心,中国科学技术大学结构分析重点实验室,中国科学技术大学化学系 合肥230026,合肥230026,伊朗科学技术研究部,德黑兰158756186,伊朗,合肥230039,合肥230026,合肥230026 |
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| 基金项目: | ProjectsupportedbytheNationalNaturalScienceFoundationofChina(20332020) |
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| 摘 要: | 利用飞行时间质谱仪的高分辨本领和离子阱串联质谱技术研究了5乙酰(苯甲酰)基4芳基3,4二氢嘧啶2(1H)酮(1-5)的电子轰击质谱的裂解规律.将所有质谱离子的精确质量数据经OpenLynx软件导出其分子离子和碎片离子的元素组成.根据质谱裂解规律,主要质谱离子得到了归属,并经离子阱串联质谱技术加以证实.化合物1-3的质谱出现了丰度很强的分子离子峰,其中1和3的分子离子为基峰,证明此类化合物的结构相当稳定.但4和5的分子离子峰却很弱(相对丰度在4%以下),这是由于嘧啶环4位上的苯环分别含有强吸电子基团-NO2(在苯环的间位才有此效应)和-Cl(苯环的2和4位均含有氯)所致.化合物1-5的主要裂解包括:分子离子失去芳基形成丰度很高的阳离子(M-Ar)+;分子离子失去羰基形成中等强度的阳离子(M-RCO)+;分子离子失去氢原子所产生的(M-H)+峰,以及消除中性分子NH=C=X的嘧啶环破裂裂解.此外,所有化合物在低质量区都发现明显的苯基阳离子Ph+(m/z77).并且还提出个别化合物的几个额外裂解过程为:化合物4(分子中苯环的3位上含有硝基)出现的基峰(M-OH)+;化合物5(分子中苯环的2和4位上都含有氯原子)出现了的基峰(M-Cl)+;化合物3和5分别出现了m/z238(16%)和m/z241(29%)的特征离子峰,它们由相应的离子消除中性分子四员内酰胺生成查耳酮离子,该离子具有共轭大Π键而稳定存在.
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| 关 键 词: | 二氢嘧啶酮 飞行时间质谱 离子阱串联质谱 电子轰击 裂解途径 |
| 收稿时间: | 4/1/2004 12:00:00 AM |
Fragmentation Regularity of 5-Acetyl(Benzoyl)-4-aryl-3,4-dihydropyrimidin-2(1H)-ones by Mass Spectrometry |
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| Li Qianrong,Salehi Hojatollah,Ding Yi,Yin Hao and Guo Qingxiang.Fragmentation Regularity of 5-Acetyl(Benzoyl)-4-aryl-3,4-dihydropyrimidin-2(1H)-ones by Mass Spectrometry[J].Chinese Journal of Chemical Physics,2005,18(4):577-584. |
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| Authors: | Li Qianrong Salehi Hojatollah Ding Yi Yin Hao and Guo Qingxiang |
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| Institution: | Li Qianrong~a**,Salehi Hojatollah~b,c,Ding Yi~d,Yin Hao~a,Guo Qingxiang~b |
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| Abstract: | Using high resolution capabilities of a time-of-flight instrument and ion trap tandem technique, electron impact mass spectra of 5-acetyl (benzoyl)-4-aryl-3,4-dihydropyrimidin-2(1H)-ones ST5HZ1-5 were studied. The molecular ion (M) peaks for 1-3ST5BZ can be found in the spectra with high abundances, but very weak for 4 and 5, in which strong electron-attracting substituents are attached to the benzene ring. The main fragmentation pathways for 1-5 include the cleavage of (M-Ar)~+ with high intensity, (M-RCO)~+ with moderate abundance, (M-H)~+ with high intensity for the compounds without strong electron-attracting substituent in the aromatic ring, and the pyrimidine ring cleavage (loss of neutral NH=C=X). In addition, a prominent cation (Ph~+, m/z 77) can be found in the low mass region of the spectra for all the compounds, which give rise by different pathways between 1-2 and 3-5. Several additional fragmentations for individual compounds are proposed. |
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| Keywords: | Dihydropyrimidinones Time of flight mass spectrometry Ion trap tandem mass spectrometry Electron impact Fragmentation pathways |
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