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首页> 外文期刊>Journal of biomolecular screening: The official journal of the Society for Biomolecular Screening >Coupling Laser Diode Thermal Desorption with Acoustic Sample Deposition to Improve Throughput of Mass Spectrometry-Based Screening
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Coupling Laser Diode Thermal Desorption with Acoustic Sample Deposition to Improve Throughput of Mass Spectrometry-Based Screening

机译:激光二极管热脱附与声样品沉积的耦合,以提高基于质谱的筛选的通量

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摘要

The move toward label-free screening in drug discovery has increased the demand for mass spectrometry (MS)-based analysis. Here we investigated the approach of coupling acoustic sample deposition (ASD) with laser diode thermal desorption (LDTD)-tandem mass spectrometry (MS/MS). We assessed its use in a cytochrome P450 (CYP) inhibition assay, where a decrease in metabolite formation signifies CYP inhibition. Metabolite levels for 3 CYP isoforms were measured as CYP3A4-1'-OH-midazolam, CYP2D6-dextrorphan, and CYP2C9-4'-OH-diclofenac. After incubation, samples (100 nL) were acoustically deposited onto a stainless steel 384-LazWell plate, then desorbed by an infrared laser directly from the plate surface into the gas phase, ionized by atmospheric pressure chemical ionization (APCI), and analyzed by MS/MS. Using this method, we achieved a sample analysis speed of 2.14 s/well, with bioanalytical performance comparable to the current online solid-phase extraction (SPE)-based MS method. An even faster readout speed was achieved when postreaction sample multiplexing was applied, where three reaction samples, one for each CYP, were transferred into the same well of the LazWell plate. In summary, LDTD coupled with acoustic sample deposition and multiplexing significantly decreased analysis time to 0.7 s/sample, making this MS-based approach feasible to support high-throughput screening (HTS) assays.
机译:在药物发现中向无标记筛选的发展增加了对基于质谱(MS)的分析的需求。在这里,我们研究了耦合声样品沉积(ASD)与激光二极管热脱附(LDTD)-串联质谱(MS / MS)的方法。我们评估了其在细胞色素P450(CYP)抑制测定中的用途,其中代谢物形成的减少表示CYP抑制。测定了3种CYP亚型的代谢物水平,分别为CYP3A4-1'-OH-咪达唑仑,CYP2D6-右旋芬和CYP2C9-4'-OH-双氯芬酸。孵育后,将样品(100 nL)声学沉积到384-LazWell不锈钢板上,然后通过红外激光直接从板表面解吸到气相中,通过大气压化学电离(APCI)进行电离,并通过MS分析/多发性硬化症。使用这种方法,我们实现了2.14 s /孔的样品分析速度,其生物分析性能可与当前基于在线固相萃取(SPE)的MS方法相媲美。当应用反应后样品多路复用时,可以实现更快的读出速度,其中将三个反应样品(每个CYP一个)转移到LazWell板的同一孔中。总而言之,LDTD与声学样品沉积和多路复用相结合,将分析时间显着减少至0.7 s /样品,这使得这种基于MS的方法可用于支持高通量筛选(HTS)分析。

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