Givosiran, a novel treatment for acute hepatic porphyrias

Manish Thapar, S. Rudnick, H. Bonkovsky
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引用次数: 11

Abstract

ABSTRACT Introduction Acute hepatic porphyrias (AHPs) are a group of rare genetic disorders that affect the enzymes of the heme biosynthetic pathway. Patients have a varied presentation, but attacks of severe abdominal pain are the cardinal feature. Until recently, IV hemin was the only definitive treatment option available. Areas covered We summarize salient features of AHP and the work leading to clinical studies of givosiran and to its approval by the US FDA and the EMA. Givosiran is a novel siRNA therapeutic agent that targets hepatic 5-aminolevulinic acid (ALA) synthase-1, the first and rate limiting enzyme in the heme biosynthetic pathway. It has been effective in decreasing the levels of hepatic ALA synthase-1 mRNA, levels of ALA, which likely is the chief neurotoxin, and the composite attack rates in patients with AHP. The drug can cause elevated liver enzymes, elevations in serum creatinine, and injection site reactions. Single doses, given to asymptomatic persons with AIP who are chronic high excretors of ALA and porphobilinogen, caused decreases in CYP1A2 and CYP2D6 activity, raising concern for drug interactions. Expert opinion Givosiran is expensive; insurance plans are likely to limit its availability to patients with well-documented AHP and frequent and severe acute attacks.
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吉沃西兰治疗急性肝卟啉的新方法
摘要引言急性肝卟啉(AHPs)是一组罕见的影响血红素生物合成途径酶的遗传疾病。患者有不同的表现,但严重腹痛发作是主要特征。直到最近,静脉注射血红素是唯一确定的治疗选择。涵盖的领域我们总结了AHP的显著特征以及吉沃西兰临床研究的工作,并获得了美国食品药品监督管理局和欧洲药品管理局的批准。吉沃西兰是一种新型siRNA治疗剂,靶向肝脏5-氨基乙酰丙酸(ALA)合成酶-1,这是血红素生物合成途径中的第一种限速酶。它可以有效降低AHP患者肝脏ALA合成酶-1mRNA的水平、可能是主要神经毒素的ALA的水平以及复合攻击率。该药物可引起肝酶升高、血清肌酐升高和注射部位反应。无症状AIP患者是ALA和卟啉原的慢性高排泄物,单次给药会导致CYP1A2和CYP2D6活性下降,引起人们对药物相互作用的担忧。专家意见Givosiran价格昂贵;保险计划可能会将其限制在有充分记录的AHP和频繁严重急性发作的患者身上。
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来源期刊
CiteScore
2.30
自引率
0.00%
发文量
9
期刊介绍: Expert Review of Precision Medicine and Drug Development publishes primarily review articles covering the development and clinical application of medicine to be used in a personalized therapy setting; in addition, the journal also publishes original research and commentary-style articles. In an era where medicine is recognizing that a one-size-fits-all approach is not always appropriate, it has become necessary to identify patients responsive to treatments and treat patient populations using a tailored approach. Areas covered include: Development and application of drugs targeted to specific genotypes and populations, as well as advanced diagnostic technologies and significant biomarkers that aid in this. Clinical trials and case studies within personalized therapy and drug development. Screening, prediction and prevention of disease, prediction of adverse events, treatment monitoring, effects of metabolomics and microbiomics on treatment. Secondary population research, genome-wide association studies, disease–gene association studies, personal genome technologies. Ethical and cost–benefit issues, the impact to healthcare and business infrastructure, and regulatory issues.
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