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直接定量细胞色素 P450 和药物转运蛋白——组织和细胞培养裂解物的快速、靶向质谱免疫分析试剂盒。

Direct Quantification of Cytochromes P450 and Drug Transporters-A Rapid, Targeted Mass Spectrometry-Based Immunoassay Panel for Tissues and Cell Culture Lysates.

机构信息

NMI Natural and Medical Sciences Institute at the University of Tübingen, Reutlingen, Germany (F.W., H.S.H., H.P., T.O.J., O.P.); SIGNATOPE GmbH, Reutlingen, Germany (F.W., H.S.H., H.P., T.O.J., O.P.); Dr. Margarete Fischer-Bosch-Institute of Clinical Pharmacology, Stuttgart, Germany (K.K., U.M.Z.); Department of Clinical Pharmacology, University of Tuebingen, Tübingen, Germany (K.K., U.M.Z.); Departments of Surgical Sciences (A.N.) and Pharmacy (C.W., P.A.), Uppsala University, Uppsala, Sweden; and Cardiovascular and Metabolic Diseases, Innovative Medicines and Early Development Biotech Unit, Mölndal, Sweden (C.W.).

NMI Natural and Medical Sciences Institute at the University of Tübingen, Reutlingen, Germany (F.W., H.S.H., H.P., T.O.J., O.P.); SIGNATOPE GmbH, Reutlingen, Germany (F.W., H.S.H., H.P., T.O.J., O.P.); Dr. Margarete Fischer-Bosch-Institute of Clinical Pharmacology, Stuttgart, Germany (K.K., U.M.Z.); Department of Clinical Pharmacology, University of Tuebingen, Tübingen, Germany (K.K., U.M.Z.); Departments of Surgical Sciences (A.N.) and Pharmacy (C.W., P.A.), Uppsala University, Uppsala, Sweden; and Cardiovascular and Metabolic Diseases, Innovative Medicines and Early Development Biotech Unit, Mölndal, Sweden (C.W.)

出版信息

Drug Metab Dispos. 2018 Apr;46(4):387-396. doi: 10.1124/dmd.117.078626. Epub 2018 Jan 17.

Abstract

The quantification of drug metabolizing enzymes and transporters has recently been revolutionized on the basis of targeted proteomic approaches. Isotope-labeled peptides are used as standards for the quantification of the corresponding proteins in enzymatically fragmented samples. However, hurdles in these approaches are low throughput and tedious sample prefractionation steps prior to mass spectrometry (MS) readout. We have developed an assay platform using sensitive and selective immunoprecipitation coupled with mass spectrometric readout allowing the quantification of proteins directly from whole cell lysates using less than 20,000 cells per analysis. Peptide group-specific antibodies (triple X proteomics antibodies) enable the enrichment of proteotypic peptides sharing a common terminus. These antibodies were employed to establish a MS-based immunoassay panel for the quantification of 14 cytochrome P450 (P450) enzymes and nine transporters. We analyzed the P450 enzyme and transporter levels in genotyped liver tissue homogenates and microsomes, and in samples from a time course induction experiment in human hepatocytes addressing different induction pathways. For the analysis of P450 enzymes and transporters only a minute amount of sample is required and no prefractionation is necessary, thus the assay platform bears the potential to bridge cell culture model experiments and results from whole organ tissue studies.

摘要

基于靶向蛋白质组学方法,药物代谢酶和转运体的定量分析最近取得了重大突破。同位素标记肽被用作在酶解样品中定量相应蛋白质的标准。然而,这些方法存在一些障碍,如高通量和在质谱(MS)读取之前繁琐的样品预分级步骤。我们开发了一种使用敏感和选择性免疫沉淀结合质谱读取的检测平台,允许使用少于每个分析 20,000 个细胞直接从全细胞裂解物中定量蛋白质。肽组特异性抗体(三重 X 蛋白质组学抗体)能够富集具有共同末端的蛋白质型肽。这些抗体被用于建立基于 MS 的免疫分析试剂盒,用于定量 14 种细胞色素 P450(P450)酶和 9 种转运体。我们分析了基因分型肝组织匀浆和微粒体中的 P450 酶和转运体水平,以及人肝细胞中不同诱导途径的时间过程诱导实验中的样品。对于 P450 酶和转运体的分析,只需要少量的样品,并且不需要预分级,因此该检测平台有可能将细胞培养模型实验和整个器官组织研究的结果联系起来。

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