长期HDV-RNA抑制后停用布列韦肽治疗患者的长期随访
Long-term follow-up of patients discontinuing bulevirtide treatment upon long-term HDV-RNA suppression.
作者信息
Jachs Mathias, Panzer Marlene, Hartl Lukas, Schwarz Michael, Balcar Lorenz, Camp Jeremy V, Munda Petra, Mandorfer Mattias, Trauner Michael, Aberle Stephan W, Zoller Heinz, Reiberger Thomas, Ferenci Peter
机构信息
Division of Gastroenterology and Hepatology, Department of Internal Medicine III, Medical University of Vienna, Vienna, Austria.
Rare Liver Disease (RALID) Center of the European Reference Network for Rare Hepatological Diseases (ERN RARE-LIVER), Medical University Vienna, Vienna, Austria.
出版信息
JHEP Rep. 2023 Apr 7;5(8):100751. doi: 10.1016/j.jhepr.2023.100751. eCollection 2023 Aug.
BACKGROUND & AIMS: Bulevirtide (BLV) is a novel antiviral drug licensed for the treatment of chronic hepatitis D. Data on the safety and efficacy of stopping BLV therapy upon long-term HDV-RNA suppression are scarce.
METHODS
A total of seven patients (age, 31-68 years, four with cirrhosis) included in a prospective Austrian HDV registry discontinued BLV treatment (duration, 46-141 weeks) upon long-term HDV suppression (HDV-RNA negativity, 12-69 weeks). Pegylated interferon-ɑ2a was used in combination with BLV in two patients. HDV-RNA, alanine aminotransferase, and quantitative HBsAg levels were closely monitored during treatment-free follow-up.
RESULTS
The seven patients were followed up for 14 to 112 weeks. Six patients completed ≥24 weeks of follow-up. HDV-RNA became detectable again in three patients within 24 weeks, whereas one additional patient showed an HDV-RNA relapse after almost 1 year. All patients who relapsed at any point had undergone BLV monotherapy. Meanwhile, HDV-RNA remained undetectable in two patients who were treated with BLV + pegylated interferon-ɑ2a. Only one patient showed significant alanine aminotransferase increases within 24 weeks of follow-up. BLV was reintroduced in three patients after 13-62 BLV-free weeks and was well tolerated, and all patients achieved virologic response again.
CONCLUSIONS
BLV discontinuation upon long-term HDV-RNA suppression seems safe. Retreatment with BLV was effective in case of virologic relapse. These findings are within a limited number of patients, and future studies are needed to define stopping rules and further investigate the safety of stopping BLV.
IMPACT AND IMPLICATIONS
Limited data exist on stopping bulevirtide (BLV) treatment in patients who achieve long-term HDV-RNA suppression. In a small cohort of seven Austrian patients discontinuing BLV therapy, HDV-RNA relapses were observed in four patients during long-term follow-up, whereas significant alanine aminotransferase increases were recorded in only one. Retreatment with BLV was effective in relapsers. The safety and efficacy of stopping BLV needs to be further studied in larger cohorts.
背景与目的
布列韦替(BLV)是一种获批用于治疗慢性丁型肝炎的新型抗病毒药物。关于在长期HDV - RNA抑制后停止BLV治疗的安全性和有效性的数据较少。
方法
纳入奥地利一项前瞻性丁型肝炎登记研究的7名患者(年龄31 - 68岁,4名患有肝硬化)在长期HDV抑制(HDV - RNA阴性,持续12 - 69周)后停止BLV治疗(疗程46 - 141周)。2名患者在使用BLV的同时联合使用了聚乙二醇化干扰素 - α2a。在停药随访期间密切监测HDV - RNA、丙氨酸氨基转移酶和定量HBsAg水平。
结果
7名患者随访了14至112周。6名患者完成了≥24周的随访。3名患者在24周内HDV - RNA再次可检测到,而另外1名患者在近1年后出现HDV - RNA复发。所有在任何时间点复发的患者均接受过BLV单药治疗。同时,在接受BLV + 聚乙二醇化干扰素 - α2a治疗的2名患者中,HDV - RNA仍未检测到。仅1名患者在随访24周内丙氨酸氨基转移酶显著升高。在无BLV治疗13 - 62周后,3名患者重新使用BLV,耐受性良好,所有患者再次获得病毒学应答。
结论
在长期HDV - RNA抑制后停用BLV似乎是安全的。病毒学复发时重新使用BLV治疗有效。这些发现基于有限数量的患者,未来需要开展研究以确定停药规则并进一步研究停用BLV的安全性。
影响与意义
关于在实现长期HDV - RNA抑制的患者中停止布列韦替(BLV)治疗的数据有限。在一小群7名停止BLV治疗的奥地利患者中,4名患者在长期随访期间出现HDV - RNA复发,而仅1名患者丙氨酸氨基转移酶显著升高。重新使用BLV治疗对复发患者有效。需要在更大队列中进一步研究停用BLV的安全性和有效性。
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