Trends in hypersensitivity drug reactions: more drugs, more response patterns, more heterogeneity.

医学 血管性水肿 免疫球蛋白E 免疫学 药品 抗体 莫西沙星 免疫系统 左氧氟沙星 过敏反应 药理学 抗生素 过敏 微生物学 生物
作者
Inmaculada Doña,Ester Barrionuevo,Natalia Blanca‐López,MJ Torres,Tahía D. Fernández,Cristobalina Mayorga,G. Canto,M. Blanca
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期刊:PubMed 卷期号:24 (3): 143-53; quiz 1 p following 153 被引量:83
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Hypersensitivity drug reactions (HDRs) vary over time in frequency, drugs involved, and clinical entities. Specific reactions are mediated by IgE, other antibody isotypes (IgG or IgM), and T cells. Nonspecific HDRs include those caused by nonsteroidal anti-inflammatory drugs (NSAIDs). beta-Lactams--the most important of which are amoxicillin and clavulanic acid--are involved in specific immunological mechanisms. Fluoroquinolones (mainly moxifloxacin, followed by ciprofloxacin and levofloxacin) can also induce HDRs mediated by IgE and T cells. In the case of radio contrast media, immediate reactions have decreased, while nonimmediate reactions, mediated by T cells, have increased. There has been a substantial rise in hypersensitivity reactions to antibiotics and latex in perioperative allergic reactions to anesthetics. NSAIDs are the most frequent drugs involved in HDRs. Five well-defined clinical entities, the most common of which is NSAID-induced urticaria/angioedema, have been proposed in a new consensus classification. Biological agents are proteins including antibodies that have been humanized in order to avoid adverse reactions. Reactions can be mediated by IgE or T cells or they may be due to an immunological imbalance. Chimeric antibodies are still in use and may have epitopes that are recognized by the immune system, resulting in allergic reactions.

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