抗抑郁化合物SIPI5358与环糊精形成的非共价复合物

用电喷雾电离质谱(ESI-MS)和串级质谱(MS/MS),并结合紫外光谱、荧光光谱等方法,研究一种芳烷醇哌嗪类抗抑郁化合物SIPI5358与α-、β-、γ-环糊精(CD)制备得到的非共价复合物.质谱分析结果显示,SIPI5358分子可以和α-CD生成配合比为1∶1的非共价复合物,而与β-、γ-CD生成不同配合比的非共价复合物.串级质谱的结果进一步验证β-CD与SIPI5358非共价复合物的组成.用紫外光谱和荧光光谱实验对液相中非共价复合物的形成进行了辅助研究,结果均再次验证了非共价复合物的生成.荧光光谱实验测得SIPI5358与β-CD反应的生成常数Kf=3.45×103 mol.L-1.     

关于中药质量控制与体内代谢研究的思考

质量控制是保证中药安全、有效的重要基础。体内代谢研究可以为阐明中药的治病机制提供依据。本文以蟾酥为例,讨论了当前中药质量控制及体内代谢研究存在的主要问题和解决办法:认为把中药指纹图谱的全面指认与多指标成分定量相结合是有效控制中药质量的可行途径;液相色谱-质谱联用技术(LC/MS)将在中药化学研究、体内代谢研究等方面发挥重要作用;中药的化学指纹图谱应与药理活性相关联,从而建立合理的中药质量评价体系;结构修饰对基于天然产物的新药发现具有重要意义。     

基于直接注射-多级质谱全扫描技术的人血红蛋白快速肽图分析

利用液相色谱–串联质谱法(LC-MS/MS)进行肽图分析,是目前单克隆抗体等蛋白类药物质量控制的主要方法,然而,LC-MS/MS分析具有费时、费溶剂和成本高等缺点。本研究以人血红蛋白(Human hemoglobin, Hb)为例,考察利用直接注射–多级质谱全扫描技术(DI-MS/MS^ALL)进行肽图分析的可行性。Hb经胰蛋白酶水解后,多肽样品通过流动注射泵直接注入QTOF-MS离子源,采用MS/MS^ALL记录MS¹谱图以及每个单位质荷比窗口(1 Da)的MS²谱图信息,所获得的质谱信息与Skyline软件给出的21个理论肽段质谱信息进行匹配,初步指认了20个肽段。常规的LC-MS/MS肽图分析检测出了所有21个理论肽段。DI-MS/MSALL的MS¹图谱与LC-MS/MS的平均MS¹图谱相近,主要为各肽段带电荷数1～4的准分子离子信号,以双电荷为主,而MS²图谱均以y⁺离子为主。因此,DI-MS/MS^...     

数字离子阱质谱仪低质量截止值的改进方法

本研究在实验室自制的线形数字离子阱质量分析器上,通过改变数码电源的频率扫描方式,在CID过程中,通过扫描数字束缚方波电源的频率和数字激发方波的频率实现母体解离。例如对于利血平母体离子,当将离子数字束缚方波频率从500 kHz扫描到560 kHz,可以测量到低质荷比的碎片离子,成功实现了串级质谱分析的低质量碎片离子的分析。通过与利血平三重四极质谱串级质谱分析实验结果的比较,发现可以在数字离子阱质谱仪上获得与三重四极质谱相同的串级质谱测量结果。结果表明,本方法可以用于低质量离子的测量,克服了传统离子阱质谱进行串级质谱分析的一个主要难点,显著提高数字离子阱质谱的性能。     

含有28个氨基酸的复杂多肽的串级质谱全序列分析研究

利用MALDI-TOF/TOF MS和ESI-MS/MS对一种含有多达28个氨基酸的复杂合成多肽成功进行了全序列测定. 通过调节激光强度、碰撞诱导解离(CID)能量等质谱参数以及依据不同序列分析软件, 获得了涵盖所有b型和y型碎片离子的串级质谱图. 结果显示这种方法可以有效地解决de novo测序方法遇到的谱峰过于复杂导致运算死机等问题. 通过讨论如何对含有超过20个氨基酸片断的多肽进行合格串级质谱实验, 为蛋白质组学肽段序列测定提供了新的方法和思路.     

利用三级质谱与二级质谱匹配策略鉴定丹参中酚酸类成分

多级质谱信息(MS/MS information)可提供鉴定化合物结构的关键线索,多级质谱(MS/MS)图谱到结构的转换(MS/MS spectrum to structure)是精准鉴定化合物结构的重要过程。本研究提出了化合物的三级质谱(MS³)图谱与其结构单元的二级质谱(MS²)图谱匹配策略,实现了化合物结构的精准鉴定。首先,利用三重四极杆复合线性离子阱质谱仪(Qtrap-MS)的双碰撞池,采集酯类化合物酯基质谱裂解产生的特征碎片离子(c^–和y^–)在线性离子阱(LIT)内经第二次碰撞诱导解离(Collision-induced dissociation, CID)后的MS³图谱,并同步采集其结构单元化合物([M–H]^–)在LIT中经碰撞诱导解离后的MS²图谱,结果表明,酯类化合物特征碎片离子的MS³图谱与结构单元化合物的MS²图谱匹配。最后,采用HR-MS/MS对丹参总酚酸(Total ...     

离子阱GC-MS-MS检测鼠药中的毒鼠强

建立了离子阱气相色谱-串级质谱（MS—MS）检测鼠药中毒鼠强的方法。测定毒鼠强的线性范围为0．2～5．0mg／L,线性相关系数为0．9984,检出限为0．0013mg／kg,回收率为76．1％～116．7％,测定结果的相对标准偏差为6．1％（n=6）。同时利用二级质谱分析了毒鼠强裂解规律,该法对毒鼠强具有良好的确证性。     

毛细管色谱法分析糠醛中组分

选择最佳GC／MS分析条件，对工业级和分析级糠醛所含各组分进行分离和检测，通过质谱谱库的计算机检索，结合图谱解析和参考文献定性，鉴定出了十个主要组分。在气相色谱仪上，采用内标法对各组分进行定量，取得了满意的分析结果。     

EPA甲酯和DHA甲酯标准样品的制备和结构解析

从鱼油中分离制备得到二十碳五烯酸（EPA）甲酯和二十二碳六烯酸（DHA）甲酯,采用红外光谱、质谱、核磁共振波谱等手段对EPA甲酯和DHA甲酯的结构进行表征,提供了不饱和脂肪酸甲酯标准物质研制基础。样品的红外光谱（IR）、质谱（MS）、核磁共振谱图（1HNMR、13CNMR）所给出的结构信息与EPA甲酯和DHA甲酯的化学结构式相符,并通过DEPT谱和I3C-1H COSY化学位移相关谱（HMBC）对各共振峰进行了指认,样品的谱图数据与文献报道基本一致。     

串级质谱法鉴定食品中苏丹红一号

利用气相色谱串级质谱(GC/MS/MS)法定性定量鉴定食品中染料苏丹红一号,建立了离子阱气相色谱-质谱联用仪分析食品中苏丹红一号染料的方法。结果表明,苏丹红一号在0.045~0.90 mg.L-1浓度范围内呈线性关系,相关系数为0.999 0,检测下限为0.004 5 mg.kg-1,回收率在83.1%~103.2%之间。方法具有样品预处理简单、灵敏度高、检出限低于现行国家标准水平,确证能力强等特点,满足食品中苏丹红一号的定性定量监测。     

LC-ESI MS/MS测定蜜胺餐具中三聚氰胺的迁移量

建立了液相色谱串联电喷雾正离子源质谱(LC-ESI MS/MS)检测蜜胺餐具中三聚氰胺迁移量的方法.采用强阳离子交换柱,流动相为乙腈-10 mmol/L乙酸铵/乙酸缓冲溶液(pH 4.0)(40:60,体积比),以多反应离子监测对三聚氰胺做定性定量分析.在水、3%乙酸、10%乙醇模拟物中,三聚氰胺在3.00～130.0...     

乳腺癌代谢物组模式特征发现方法及HPLC/M S/M S分析

提出一种基于单独最优特征组合和BP神经网络的代谢物组模式特征发现方法,并用其寻找到尿样中与乳腺癌最为相关的4种核苷,组成一组特异性检测参数.经HPLC/MS/MS联用法鉴定,它们是乳清酸核苷、1-甲酰化腺苷、S-腺苷-L-蛋氨酸及N²-甲酰化鸟苷.将这4种核苷作为输入变量,用BP神经分类网络建立乳腺癌诊断模型.留一法交叉验证和独立验证结果表明,该模型预测准确率达到90%以上.     

GC/MS和ESI/MS/MS同位素内标法检测甲基丙二酸血症

以甲基丙二酸血症为对象,分别用GC/MS和ESI/MS/MS方法对该疾病进行了定性和定量检测.通过对样品前处理和分离条件的改善,对疾病的标识化合物之一甲基丙二酸进行了定量测定,其稳定性、精密度和回收率结果很好.同时比较了GC/MS和ESI/MS/MS两种方法的特点,发现两种方法的结合不仅可满足新生儿代谢疾病筛查的要求,同时还可对高危人群进行诊断.     

液相色谱-串联质谱法测定地表水中的丙烯酰胺

建立了地表水中丙烯酰胺残留的液相色谱-串联质谱联用测定方法。结果表明,该法的检出限0．1μg,线性范围0．1～100．0μg/L,加标回收率81．7％～86．4％。     

Determinations of geniposide using LC/MS/MS methods via forming ammonium and acetate adducts

In this paper, we report method development work to determine geniposide using LC/MS/MS via the formation of positive and negative ion adducts. Geniposide, which has been recognized to have choleretic effects, is the major iridoid glycoside component of Gardenia herbs. To enhance the sensitivity of LC/MS detection of geniposide, a small amount of volatile additives such as ammonium acetate and acetic acid are added into mobile phase solvents to form positive and negative adducts, which can then ionize via electrospray processes. The formation of positive adducts is due to the complexation between geniposide and ammonium ions ([M + NH₄]⁺). The formation of anionic adducts [M + CH₃COO]⁻ is believed to occur via hydrogen bonds bridging acetate ions and glucose groups on the geniposide molecule. Mobile phase solvents containing acetonitrile and aqueous solution (0.2 mM ammonium acetate or 0.1% acetic acid) at the ratio 15: 85 are employed to elute geniposide using C8 reverse phase liquid chromatography columns with electrospray tandem mass spectrometry determinations. Using geniposide standards, the methods are validated at the concentration ranges of 5 to 1000 ng/mL and 20 to 5000 ng/mL using ammonium and acetate adducts respectively. The correlation coefficients of the standard curves are 0.9999 using both ammonium and acetate adducts. The detection limits of using ammonium and acetate adducts are 1 and 5 ng/mL respectively. The measurement accuracy and precision of using ammonium adducts are within 12% and 3% respectively, whereas the accuracy and precision are within 6 and 11% respectively using acetate adducts. When the validated calibration curves of the ammonium adduct of geniposide are used to determine spiked control samples in rat blood dialysates, the determination errors of accuracy and precision are within 12% and 10% respectively.     

红景天苷及其酯化产物的ESI MS和MS/MS裂解途径

糖苷广泛存在于自然界中,常以糖苷酯形式存在,这有效地提高了它们的酯溶性,增加它们在肠内和胞内的吸收[1-3]。红景天苷是一种具有抗疲劳、抗辐射、抗缺氧、提高记忆、延缓衰老等药理活性的天然糖苷[4-8],在此先导化合物的基础上合成了各种红景天苷酯。本文对这类红景天苷酯的E     

粮食中磺酰脲类除草剂的UPLC/MS/MS测定方法

建立了多类粮食作物中15种磺酰脲类除草剂的超高效液相色谱-串联质谱联用仪(UPLC/MS/MS)多离子监测(MRM)的多残留检测方法。样品经乙腈提取,乙腈饱和的正己烷液-液分配,石墨化碳氨基小柱净化,采用UPLC-MS/MS(ESI+)测定。方法中各种磺酰脲类除草剂在5～200μg/L浓度范围内线性良好,相关系数在0.9995～0.9999。在5～100μg/kg范围内,平均加标回收率在71.6%～115.3%之间,相对标准偏差不大于15%。各种药物的定量限(S/N≥10)均可达到5μg/kg。该方法可同时满足大豆、大米、玉米等多种粮食中磺酰脲类除草剂的检测需求。     

MS／MS Study of Deoxydinucleotides Bound with Alkali—metal Ions Using ESI—MS

Positive ion ESI-MS has been used to examine the fragmentation pathways of the complex ions of deoxydinucleotides with H^ ,Na^ ,K^ by LCQ instrument.It had been found that the dissociation Varied markedly due to the differences of the base sequence.The alkali-metal ion binding site and the charcaterization of dissociation were directed by the size of metal ion,the sequesce of base and the steric hindrance.     

Detection of flavonoids from Spinacia oleracea leaves using HPLC-ESI-QTOF-MS/MS and UPLC-QqQLIT-MS/MS techniques

Spinacia oleracea L. (Spinach) is a leafy vegetable which is considered to have a high nutritional value. Flavonoids in spinach were reported to act as antimutagenic property. Rapid detection of these flavonoids in Spinach was achieved by using HPLC-ESI-QTOF-MS/MS. Thirty six compounds were tentatively identified based on their retention times, accurate mass and MS/MS spectra. The fragmentation patterns of known compounds were applied to elucidate the structure of their corresponding derivatives having the same basic skeleton. Out of thirty six peaks, three peaks were assigned as patuletin and six peaks were assigned as spinacetin derivatives. Twelve compounds were first time identified following the fragmentation pattern of known compounds. Five of the identified compounds i.e., spinacetin, 5,3′,4′-trihydroxy-3-methoxy-6,7-methylenedioxyflavone, protocatechuic acid, ferulic acid and coumaric acid were simultaneously quantified in spinach leaves by a validated UPLC-ESI-MS/MS method under MRM mode.     

Characterization of major degradation products of an adenosine A2A receptor antagonist under stressed conditions by LC‐MS and FT tandem MS analysis

Parkinson's disease (PD) is a very serious neurological disorder, and current methods of treatment fail to achieve long‐term control. SCH 420814 is a potent, selective and orally active adenosine A_2A receptor antagonist discovered by Schering‐Plough. Stability testing provides evidence of the quality of a bulk drug when exposed to the influence of environmental factors. Understanding the drug degradation profiles is critical to the safety and potency assessment of the drug candidate for clinical trials. As a result, identification of degradation products has taken an important role in drug development process. In this study, a rapid and sensitive method was developed for the structural determination of the degradation products of SCH 420814 formed under different forced conditions. The study utilizes a combination of liquid chromatography–tandem‐mass spectrometry (LC‐MS/MS) and Fourier Transform (FT) MS techniques to obtain complementary information for structure elucidation of the unknowns. This combination approach has significant impact on degradation product identification. A total of ten degradation products of SCH 420814 were characterized using the developed method. Copyright © 2009 John Wiley & Sons, Ltd.