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Resolution of co-eluting isomers of anti-inflammatory drugs conjugated to carbonic anhydrase inhibitors from plasma in liquid chromatography by energy-resolved tandem mass spectrometry

机译:通过能量分辨串联质谱法从液相色谱中血浆中与碳酸酐酶抑制剂缀合的碳酸酐酶抑制剂缀合的共同洗脱异构体的分辨率

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摘要

Rheumatoid arthritis (RA) is a chronic inflammatory disease caused by a faulty autoimmune response. Recently, it was reported that some human carbonic anhydrases (CAs) isoforms are overexpressed in inflamed synovium of RA patients. New CA inhibitors (CAIs) incorporating CA-binding moiety and the cyclooxygenase inhibitor tail (nonsteroidal anti-inflammatory drug [NSAID] type) were studied. The aim of this work is the evaluation of the chemical stability of NSAID − CAI hybrids towards spontaneous or enzymatic hydrolysis by LC-MS/MS. The analytes are isomer pairs of 6- or 7-hydroxycoumarin, their different fragment ions abundances allowed the development of a mathematical tool (LEDA) to distinguish them. LEDA reliability at ng mL−1 level was checked (>90%), being proved the effectiveness in the correct assignment of the isomer present in the sample. The hybrids resulted stable in all tested matrices allowing us to conclude that these compounds reach the target tissues unmodified, opening perspectives for their development in the treatment of inflammation.
机译:类风湿性关节炎(RA)是一种慢性炎症性疾病,由缺陷的自身免疫反应引起。最近,据报道,一些人碳酸酐酶(CAS)同种型在发炎的RA患者的发炎僵局中过表达。研究了掺入Ca结合部分和环氧氧酶抑制剂尾(非甾体类抗炎药[NSAID]型)的新CA抑制剂(CAIS)。这项工作的目的是评价NSAID - CAI杂交物的化学稳定性朝向LC-MS / MS的自发性或酶水解。分析物是6-或7-羟基苏格林的异构体对,其不同的片段离子丰富允许开发数学工具(LEDA)来区分它们。检查了Ng ML-1水平的LEDA可靠性(> 90%),在样品中存在的正确分配的有效性。所有测试基质中的杂种导致杂交稳定,允许我们得出结论,这些化合物未经修改的靶组织未经修改,打开其在治疗炎症时开放的观点。

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