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Bioactivation of drugs in the skin: relationship to cutaneous adverse drug reactions

机译:皮肤中药物的生物活化:皮肤不良药物的关系

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摘要

Drug-induced skin rashes are poorly understood idiosyncratic reactions, and current methods cannot predict their occurrence. Most idiosyncratic drug reactions are thought to be caused by chemically reactive metabolites, and the skin is a frequent site of idiosyncratic reactions; however, the skin has a very limited capacity to metabolize drugs. To balance this, the skin represents a protective barrier with a very active immune response against pathogens and other types of skin injury. Therefore its response to reactive metabolites is quite different from that of the liver. The purpose of this review is to integrate emerging findings into proposed mechanisms of drug and carcinogen metabolism in the skin that are likely responsible for rashes and other immune responses of the skin. Current evidence suggests the skin possesses significant sulfotransferase and flavin monooxygenases activities, but very low cytochromes P450 activity. However, there are skin-specific P450s that are not present in the liver. The manner in which the skin responds to neoantigens through local antigen presentation and innate immune sensing is reviewed with a focus on insights gained from the contact hypersensitivity (CHS) field. The roles of keratinocytes and Langerhans cells, and the emerging function of NOD-like receptors, are highlighted.
机译:药物诱导的皮疹是理解的特质不良,目前的方法无法预测其发生。据认为,大多数特质药物反应是由化学反应性代谢物引起的,并且皮肤是一种频繁的特质性反应部位;然而,皮肤具有非常有限的来代谢药物能力。为了平衡这一点,皮肤代表一种保护屏障,具有非常活跃的免疫应答,免受病原体和其他类型的皮肤损伤。因此,对反应性代谢物的反应与肝脏的反应完全不同。本次审查的目的是将新出现的结果整合到可能对皮疹和其他免疫应答的皮肤上的药物和致癌物质代谢的提出机制中。目前的证据表明皮肤具有显着的磺基转移酶和黄蛋白单氧基酶活性,但是细胞变色为P450活性非常低。然而,存在肝脏中不存在的皮肤特异性P450。通过局部抗原呈现和先天免疫感应对皮肤对新抗原作出反应的方式进行审阅,重点是从接触超敏反应(CHS)场中获得的见解。突出的角质形成细胞和朗格汉斯细胞的作用以及点状受体的新出现功能。

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