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Mass spectrometry of selective androgen receptor modulators

机译:选择性雄激素受体调节剂的质谱

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Nonsteroidal selective androgen receptor modulators (SARMs) are an emerging class of drugs for treatment of various diseases including osteoporosis and muscle wasting as well as the correction of age-related functional decline such as muscle strength and power. Several SARMs, which have advanced to preclinical and clinical trials, are composed of diverse chemical structures including arylpropionamide-, bicyclic hydantoin-, quinoline-, and tetrahydroquinoline-derived nuclei. Since January 2008, SARMs have been categorized as anabolic agents and prohibited by the World Anti-Doping Agency (WADA). Suitable detection methods for these low-molecular weight drugs were based on mass spectrometric approaches, which necessitated the elucidation of dissociation pathways in order to characterize and identify the target analytes in doping control samples as well as potential metabolic products and synthetic analogs. Fragmentation patterns of representatives of each category of SARMs after electrospray ionization (ESI) and collision-induced dissociation (CID) as well as electron ionization (EI) are summarized. The complexity and structural heterogeneity of these drugs is a daunting challenge for detection methods.
机译:非体内选择性雄激素受体调节剂(SARMS)是一种用于治疗各种疾病的新出现的药物,包括骨质疏松症和肌肉浪费以及肌肉力量和力量等年龄相关功能下降的校正。几种已经前进至临床前和临床试验的群体由不同的化学结构组成,包括芳基咪唑 - ,双环氰基,喹啉和喹啉和四氢喹啉衍生的细胞核。自2008年1月以来,SARM已被分类为合成代理人,并受到世界反兴奋剂机构(WADA)的禁止。这些低分子量药物的合适检测方法基于质谱方法,这需要阐明解离途径,以表征和鉴定掺杂对照样品中的靶分析物以及潜在的代谢产物和合成类似物。总结了电喷雾电离(ESI)和碰撞诱导的解离(CID)之后每类SARM的代表的碎片模式以及电子电离(EI)。这些药物的复杂性和结构性异质性是一种令人生畏的检测方法挑战。

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