电场辐照前后某些中药有效成分的质谱分析

利用快原子轰击质谱（ＦＡＢＭＳ）及解吸电子轰击质谱（ＤＥＩＭＳ）方法，分析了电场辐照前后的５种中药有效成分，证明电场辐照灭菌并不改变其化学结构，讨论了底物效应及正，负快原子轰击质谱的差异，以及与电吸电子轰击质谱的不同断裂规律，同时利用Ｂ／Ｅ联动扫描（亚稳离子测定）进行了验证。     

质谱及色谱-质谱联用技术在多糖结构分析中的应用

综述了从1968-2010年间质谱及色谱-质谱联用分析法在多糖结构分析中的应用,包括电子轰击质谱、化学电离质谱、快原子轰击质谱、电喷雾质谱、基质辅助激光解吸离子化质谱、气相色谱-质谱、液相色谱-质谱和毛细管电泳-质谱法(引用文献42篇)。     

2,3-二烷氧基-5-烷氧羰基苄基胺羧酰胺螯合剂的快原子轰击质谱研究

本文报道了运用快原子轰击电离以及快原子轰击-联动扫描方法对2,3-二烷氧基-5-烷氧羰基苄基胺羧酰胺螯合剂的质谱研究, 阐明了它们的裂解途径, 并以此对它和铁离子相螯合后螯合部位进行推测. 结果表明快原子轰击电离方法为金属配合物的研究提供了一种新的手段.     

2,3-二烷氧基-5-烷氧羰基苄基胺羧酰胺螯合剂的快原子轰击质谱研究

本文报道了运用快原子轰击电离以及快原子轰击-联动扫描方法对2,3-二烷氧基-5-烷氧羰基苄基胺羧酰胺螯合剂的质谱研究,阐明了它们的裂解途径,井以此对它和铁离子相螯合后螯合部位进行推测。结果表明快原子轰击电离方法为金属配合物的研究提供了一种新的手段。     

质谱技术在糖类结构分析中的应用

综述了电子轰击、化学电离、快原子轰击、电喷雾离子化、基质辅助激光解吸、串联质谱等质谱技术在糖类结构分析中的应用。引用文献共53篇。     

质谱联用技术在生物大分子分析中的应用

本文评述了近年来质谱联用技术在生物大分子分析应用中的最新进展。着重评述了由于ESI接口的出现而推动的高效液相色谱一连续流动快速原子轰击质谱(HPLC-cfFABMS )、高效取代色谱一连续流动快速原子轰击质谱(HPDC-cfFABMS ) ,凝胶渗透色谱一诱导祸合等离子体质谱(GPC-1CPMS )、毛细管电泳一质谱(CE-MS )和毛细管电泳一飞行时间质谱(CE-TOFMS)等方面近两年的动向及成果。本文较广泛地展示了质谱联用技术在生物大分子分析中的重要作用和独特的地位。     

有机磷化合物的快原子轰击质谱研究 Ⅶ.N-对甲苯磺酰基-N''''-异丙基-N-取代-S-丙基磷酰二胺酯

本文讨论一类新合成的磷酰二胺酯的质谱特征。其电子轰击质谱(EIMS)分子离子峰很弱(<1%),我们采用快原子轰击质谱(FABMS),讨论其PFABMS与NFABMS的区别、取代基的影响,PFABMS与NFABMS的主要离子产生机理。     

如何看EI-MS质谱图

电子轰击源质谱(EI-MS)是质谱测定中经常使用、也是提供质谱结构信息最丰富的技术之一。面对一张完全未知化合物质谱图中的任意一个峰,能马上回答出是奇质量、偶质量、奇电荷、偶电荷峰,是分子峰、碎片峰、重排峰,含奇数氮、偶数氮(包括不含氮),含碳原子、硫原子、氯原子、溴原子数目等系列质谱结构信息,是质谱结构分析的基本功。     

冠醚稀土络合物的快原子轰击质谱

本文报道十余个冠醚稀土络合物的快原子轰击质谱(FABMS)。通过分析FABMS的特征及亚稳离子分解讨论了溶液中的反应和络合性质。     

芳香环状低聚体的结构表征

综述了芳香环状低聚体结构表征的发展过程及最新进展,以高效液相色谱、快原子（离子）轰击质谱、激光质谱、电喷雾质谱为主结合其他辅助方法分别做以介绍并比较了各种表征方法的特点及应用范围。     

Identification of phosphoramide mustard/DNA adducts using tandem mass spectrometry

The reaction pathway of alkylating agents is often exploited in the design of bifunctional anti-cancer drugs. These drugs form mono-DNA adducts as well as inter- and intra-strand cross-linked adducts, notably by reaction at DNA bases, including the N-7-position of guanine (G). A positive-ion fast-atom bombardment (FAB) mass spectrum of an in vitro preparation of DNA alkylated with phosphoramide mustard (the active metabolite of the anti-cancer drug cyclophosphamide) indicated the presence of the two mono-DNA adducts N-(2-chloroethyl)-N-[2-(7-guaninyl)ethyl] amine, designated NOR-G, and N-(2-hydroxyethyl)-N-[2-(7-guaninyl)ethyl] amine, designated NOR-G-OH, (MH+ 257/259 and 239, respectively) but not the presence of the cross-linked adduct N,N-bis-[2-(7-guaninyl)ethyl] amine, designated G-NOR-G (MH+ 372). Using synthetic standards, daughter-ion spectra of NOR-G, NOR-G-OH and G-NOR-G were obtained (matrix 0.2 M p-toluene sulphonic acid in glycerol) by positive-ion FAB tandem mass spectrometry (FAB-MS/MS). The daughter-ion spectra of both mono-DNA adducts NOR-G and NOR-G-OH contained a fragment ion at m/z 152 [G + H]+, whereas the cross-linked adduct, G-NOR-G, showed an ion at m/z 221, [MH-G]+. Evidence for the presence of NOR-G, NOR-G-OH and G-NOR-G in the in vitro preparation was obtained by performing a double parent-ion scan on m/z 152 and 221. The presence of G-NOR-G was further supported by performing a single parent-ion scan on m/z 221.(ABSTRACT TRUNCATED AT 250 WORDS)     

二十种混合氨基酸的质谱鉴定 直接磷酰化物的正负离子FAB-MS分析

将二十种天然氨基酸按等摩尔量混合后,用二异丙基亚磷酸酯直接磷酰化,可以高选择性(96%)地获得N-磷酰氨基酸衍生物的混合物,负离子FAB-MS可以原位检出混合物中全部N-磷酰氨基酸,且准分子离子峰较高,可发展为混合氨基酸衍生物全分析的有效手段.正离子FAB-MS则对碱性磷酰化氨基酸的检出更有利     

The early glycation products of the Maillard reaction: mass spectrometric characterization of novel imidazolidinones derived from an opioid pentapeptide and glucose

Glucose-substituted imidazolidinones related to the endogenous opioid peptide leucine-enkephalin have been investigated using fast atom bombardment tandem mass spectrometry (FAB-MS/MS) and electrospray ionization tandem mass spectrometry (ESI-MS/MS). In addition to Amadori compounds, the studied imidazolidinones represent a novel type of the early glycation products formed in the Maillard reaction. To obtain insight into the fragmentation behavior of these carbohydrate-peptide adducts, we also studied synthetic precursors of the glucose-substituted imidazolidinones as well as the corresponding isopropylidene derivatives. The collision-induced dissociation (CID) spectra of [M + H](+) ions of all these imidazolidinones have been compared. Detailed analysis showed that fragmentation of each compound generates two ions at m/z 566 and m/z 598 which are characteristic and undoubtedly confirm the imidazolidinone-type structure. These two significant ions were identified as the M + 10 and M + 42 modifications of the N-terminus of the parent opioid pentapeptide effected by the carbohydrate moiety. Furthermore, the ion at m/z 178 is identified as the M + 42 modification of the immonium ion of the N-terminal amino acid (tyrosine) also effected by the carbohydrate moiety. They can be used as diagnostic ions for imidazolidinone-type compounds in studying the Maillard reaction. Thus, we have demonstrated the utility of FAB-MS/MS and ESI-MS/MS in the structural determination and identification of such novel peptide-carbohydrate adducts, useful in understanding the details of the mechanism of non-enzymatic glycation in vivo.     

Detection and characterization by mass spectrometry of radical adducts produced by linoleic acid oxidation

The formation of linoleic acid radical species under the oxidative conditions of the Fenton reaction (using hydrogen peroxide and Fe (II)) was monitored by FAB-MS and ES-MS using the spin trap 5,5-dimethyl-1-pyrrolidine-N-oxide, DMPO. Both the FAB and ES mass spectra were very similar and showed the presence of ions corresponding to carbon- and oxygen centered spin adducts (DMPO/L*, DMPO/LO*, and DMPO/LOO*). Cyclic structures, formed between the DMPO oxygen and the neighboring carbon of the fatty acid, were also observed. Electrospray tandem mass spectrometry of these ions was performed to confirm the proposed structure of these adducts. All MS/MS spectra showed an ion at m/z 114, correspondent to the [DMPO + H]+, and a fragment ion due to loss of DMPO (loss of 113 Da), confirming that they are DMPO adducts. ES-MS/MS spectra of alkoxyl radical adducts (DMPO/LO*) showed an additional ion at m/z 130 [DMPO - O + H]+, while ES MS/MS of peroxyl radical adducts (DMPO/LOO*) showed a fragment ion at m/z 146 [DMPO - OO + H]+, confirming both structures. Other fragment ions were observed, such as alkyl acylium radical ions, formed by cleavage of the alkyl chain after loss of water and the DMPO molecule. The identification of fragment ions observed in the MS/MS spectra of the different DMPO adducts suggests the occurrence of structural isomers containing the DMPO moiety both at C9 and C13. The use of ES tandem mass spectrometry, associated with spin trapping experiments, has been shown to be a valuable tool for the structural characterization of carbon and oxygen-centered spin adducts of lipid radicals.     

Atmospheric pressure matrix-assisted laser desorption/ionisation ion trap mass spectrometry of synthetic polymers: a comparison with vacuum matrix-assisted laser desorption/ionisation time-of-flight mass spectrometry

Atmospheric pressure matrix-assisted laser desorption/ionisation quadrupole ion trap (AP-MALDI/QIT) mass spectrometry has been investigated for the analysis of polyethylene glycol (PEG 1500) and a hyperbranched polymer (polyglycidol) in the presence of alkali-metal salts. Mass spectra of PEG 1500 obtained at atmospheric pressure showed dimetallated matrix/analyte adducts, in addition to the expected alkali-metal/PEG ions, for all matrix/alkali-metal salt combinations. The relative intensities of the desorbed ions were dependent on the matrix, the alkali-metal salt added to aid cationisation and the ion trap interface conditions [capillary temperature, in-source collisionally-induced dissociation (CID)]. These data indicate that the adducts are rapidly stabilised by collisional cooling enabling them to be transferred into the ion trap. Experiments using identical sample preparation conditions were carried out on a vacuum MALDI time-of-flight (ToF) mass spectrometer. In all cases, vacuum MALDI-ToF spectra showed only alkali-metal/PEG ions and no matrix/analyte adducts. The tandem mass spectrometry (MS/MS) capability of the ion trap has been demonstrated for a lithiated polyglycol yielding a rich fragment-ion spectrum. Analysis of the hyperbranched polymer polyglycidol by AP-MALDI/QIT reveals the characteristic ion series for these polymers as also observed under vacuum MALDI-ToF conditions.     

烷基苯磺酸盐的电喷雾离子化质谱和碰撞活化解离质谱－质谱分析

用正,负电喷雾电离（ESI）并结合碰撞活化解离（CAD）质谱法对烷基苯磺酸盐（ABS）进行鉴定,无论正,负离子化过程中均不出现快原子轰击质谱常见的碎片峰,由于没有复杂碎片峰的干扰,ESI－MS对分析ABS试样大为有利,正离子ESI－MS对支化ABS鉴定的灵敏度远低于负离子ESI－MS,用CAD－MS对ESI－ME谱各主要峰进行了归属,线型与支化ABS相对含量可以用负离子ESI－MS求出,负离子化ESI－MS是快速,有效和可靠的鉴定,ABS的方法。     

Production and fragmentation of negative ions from neutral N-linked carbohydrates ionized by matrix-assisted laser desorption/ionization

Although negative ion fragmentation mass spectra of neutral N-linked carbohydrates (those attached to Asn in glycoproteins) provide much more structural information than spectra recorded in positive ion mode, neutral carbohydrates are reluctant to form negative ions by matrix-assisted laser desorption/ionization (MALDI) unless ionized from specific matrices such as nor-harmane or adducted with anions such as chloride. This paper reports the results of experiments to optimize negative ion formation from adducts of N-linked glycans with respect to ion abundance and fragment ion production. The best results were obtained with 2,4,6-trihydroxyacetophenone (THAP) as the matrix with added ammonium nitrate as the salt providing the anion. This approach is demonstrated to be applicable for a wide range of N-linked glycan structures. Phosphate adducts, analogous to those that are usually encountered in electrospray spectra from N-glycans released by protein N-glycosidase F, were produced by addition of ammonium phosphate to the matrix but in relatively low yield allowing competitive ionization of endogenous anionic compounds leading to complex spectra. Fragmentation of the nitrate adducts, which were formed in higher yield, generally paralleled that seen by collision-induced dissociation following ionization by electrospray, with the first stage of the dissociation being the elimination of the nitrate with a proton from one of the hydroxyl groups of the sugar. The spectra of the resulting [M-H](-) species displayed very specific fragment ions, mainly cross-ring and C-type glycosidic cleavage products, that revealed more structural (linkage and branching) information of the compounds than the mainly glycosidic cleavage products that dominated the positive ion spectra.     

Negative ion production from peptides and proteins by matrix‐assisted laser desorption/ionization time‐of‐flight mass spectrometry

Negative ion production from peptides and proteins was investigated by matrix‐assisted laser desorption/ionization time‐of‐flight (MALDI‐TOF) mass spectrometry. Although most research on peptide and protein identification with ionization by MALDI has involved the detection of positive ions, for some acidic peptides protonated molecules are not easily formed because the side chains of acidic residues are more likely to lose a proton and form a deprotonated species. After investigating more than 30 peptides and proteins in both positive and negative ion modes, [M–H]⁻ ions were detected in the negative ion mode for all peptides and proteins although the matrix used was 2,5‐dihydroxybenzoic acid (DHB), which is a good proton donor and favors the positive ion mode production of [M+H]⁺ ions. Even for highly basic peptides without an acidic site, such as myosin kinase inhibiting peptide and substance P, good negative ion signals were observed. Conversely, gastrin I (1‐14), a peptide without a highly basic site, will form positive ions. In addition, spectra obtained in the negative ion mode are usually cleaner due to absence of alkali metal adducts. This can be useful during precursor ion isolation for MS/MS studies. Copyright © 2008 John Wiley & Sons, Ltd.     

Chiral recognition of cellulose tris(5-fluoro-2-methylpheylcarbamate) toward (R)- and (S)-1,1′-bi-2-naphthol detected by negative ion fast-atom bombardment mass spectrometry

Chiral recognition between cellulose tris(5-fluoro-2-methylphenylcarbamate) (MW > 120,000) as a host compound and (R,S)-1,1′-binaphthol (MW 286) as a guest compound was investigated by fast-atom bombardment mass spectrometry (FAB-MS). The use of negative ion FAB-MS made it possible to obtain a very simple mass spectrum of the guest compound with a high signal-to-noise ratio. Additionally, when nitrophenyl octyl ether, which has no OH group, was utilized as matrix, chiral recognition between the host and the guest compounds was unequivocally detected. Copyright © 1999 John Wiley & Sons, Ltd.     

Study of structural characteristic features of phenanthriondolizidine alkaloids by fast atom bombardment with tandem mass spectrometry

The mass spectrometric behavior of phenanthroindolizidine alkaloids has been investigated in detail by positive ion fast atom bombardment tandem mass spectrometry (FAB-MS/MS) combined with collision-induced dissociation (CID). The fragmentation has been correlated with the skeleton structure and positions of substituents. The product ions arising from retro-Diels-Alder cleavages differ clearly for compounds with different skeletons. The substituents at C-14 were observed to markedly influence the fragmentation pathway of [M + H](+) ions. A diversity of dissociation behavior initiated by the variation of substituents on the aromatic ring was also observed in the CID spectra. Product ions resulting from loss of CH(4) were obtained for compounds in which both C-6 and C-7 are occupied by methoxy groups. FAB-MS/MS spectra can reflect the connection between the fragmentation behavior and structural features of these phenanthroindolizidine alkaloids rapidly and effectively, and should prove to be a powerful method to determine the structures of related compounds.