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HLA and drug-induced toxicity

机译:HLA和药物引起的毒性

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摘要

The discovery of new associations between drug toxicities and specifc HLA alleles has been facilitated by the use of DNA-based molecular techniques and the introduction of higher-resolution HLA typing, which have replaced serological typing in this feld of study. Drug toxicity/HLA associations have been best documented for immunologically mediated reactions, such as drug hypersensitivity reactions associated with the use of abacavir, and severe cutaneous adverse drug reactions, such as Stevens-Johnson syndrome and toxic epidermal necrolysis induced by carbamazepine and allopurinol use, respectively. The implementation of HLA-B*5701 screening for the prevention of abacavir hypersensitivity syndrome (ABC HSR) has provided a model approach that can be applied to the screening of other drugs. High-level clinical evidence supporting HLA-B*5701 screening for ABC HSR has converged with experimental fndings characterizing the CD8+T-cell HLA-B*5701-restricted immune response triggered by abacavir. This has been followed by the successful development of simplifed inexpensive and quality-assured laboratory tests for HLA-B*5701 and ongoing quality assurance programs, resulting in a paradigm both for the implementation of HLA-B*5701 screening for HIV providers as well as for the broader successful implementation of pharmacogenetic screening in the clinic.
机译:通过使用基于DNA的分子技术和引入更高分辨率的HLA分型,已促进了药物毒性与特定HLA等位基因之间新关联的发现,在此研究领域中已取代了血清分型。药物毒性/ HLA关联在免疫介导的反应(例如与使用阿巴卡韦相关的药物超敏反应)以及严重的皮肤不良药物反应(例如史蒂文斯-约翰逊综合征和卡马西平和别嘌呤醇诱导的毒性表皮坏死)方面得到了最好的记录,分别。 HLA-B * 5701筛查用于预防阿巴卡韦超敏反应综合征(ABC HSR)的实施提供了一种可用于筛查其他药物的模型方法。支持针对ABC HSR的HLA-B * 5701筛查的高级临床证据已与实验结果相融合,这些实验结果表征了由阿巴卡韦触发的CD8 + T细胞HLA-B * 5701限制性免疫反应。随后,成功开发了针对HLA-B * 5701的简化的廉价且具有质量保证的实验室测试,以及正在进行的质量保证计划,从而形成了为HIV提供者以及对HIV提供者实施HLA-B * 5701筛查的范例在临床上更广泛地成功实施药物遗传学筛查。

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