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OP-02建立高效HBeAg功能治疗 REP 2139-Mg基慢性HBV感染的慢性HBV感 [复制链接]

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发表于 2019-2-23 03:44 |只看该作者 |倒序浏览 |打印
OP-02 Establishment of High Rates of Functional Cure of HBeAg
Negative Chronic HBV Infection with REP 2139-Mg Based
Combination Therapy: Ongoing Follow-up Results from the REP
401 Study
Michel Bazinet1, Victor Pantea2, Gheorghe Placinta2, Iurie Moscalu3, Valentin Cebotarescu2, Lilia
Cojuhari2, Pavlina Jimbei4, Liviu Iarovoi2, Valentina Smesnoi4, Tatiana Musteata4, Alina Jucov2 3,
Adalbert Krawczyk5, Andrew Vaillant1
1Replicor Inc., ., Montreal, Canada; 2Nicolae Testemiţanu State University of Medicine and Pharmacy,
Department of Infectious Diseases, Chișinău, Moldova; 3Arensia Exploratory Medicine, Republican
Clinical Hospital, Chișinău, Moldova; 4Toma Ciorbǎ Infectious Clinical Hospital, ., Chișinău, Moldova;
5Universitätsklinikum Essen, Institute for Virology, Essen, Germany
Email: [email protected]
Background and aims: The REP 401 study (NCT02565719) is assessing the safety and efficacy of
REP 2139-Mg (clinical lead) or REP 2165-Mg combined with tenofovir disoproxil fumarate (TDF) and
pegylated interferon α-2a (pegIFN) in Caucasian patients with HBeAg negative chronic HBV infection.
Method: Lead-in TDF therapy in 40 patients was followed by randomization into an experimental group
(48 weeks of TDF, pegIFN and REP 2139-Mg or REP 2165-Mg) or an adaptive control group (24 weeks
of TDF + pegIFN followed by cross over to 48 weeks of experimental therapy). All patients were
subsequently entered into a treatment-free follow-up scheduled for 48 weeks. Viremia is monitored on
the Abbott Architect and Realtime platforms.
Results: Baseline HBsAg was >1000 IU/ml in all patients and 14775.7 ± 9302 and 9018 ± 8743 IU/ml
in adaptive control and experimental groups. Therapy was well tolerated except for one withdrawal due
to pegIFN-related depression. Two additional participants withdrew where therapy was well tolerated.
Antiviral responses between REP 2139-Mg and REP 2165-Mg were indistinguishable and not related
to HBV genotype or HBsAg, ALT or fibrosis (Fibroscan) at baseline. Following the introduction of TDF,
HBV DNA was well controlled in all patients during therapy. Following the introduction of NAPs, HBsAg
reduction was >1 log in 36/40 patients and became <1 IU/ml in 28/40 and <0.05 IU/ml in 24/40
participants. Transaminase flares occurred in 38/40 patients and were correlated with reductions in
HBsAg, were self-resolving during therapy and not accompanied by any evidence of liver dysfunction.
Transaminase flares were especially pronounced (400-1748 U/L) in patients where HBsAg became <1
IU/ml and were accompanied by profound elevations in anti-HBs (up to 255, 055 mIU/ml).
As of the date of submission, treatment-free follow-up has been extended to 24 or 48 weeks in 34/40
patients completing treatment. Persistent and stable inactive chronic HBV (HBV DNA <2000 IU/ml with
normal ALT) is present in 15/34 (44%) of participants. An additional 14/34 (41%) participants have
functional cure (HBsAg and HBV DNA target not detected). Liver function has normalized in 94% of
patients (versus 47% at baseline) and median hepatic stiffness consistent with F0 ( ≤7kPa) is present
in 81% of patients (versus 52% at baseline).
Conclusion: A finite REP 2139-Mg based combination therapy with TDF and pegIFN is well tolerated
and results in a high proportion of patients achieving control of infection not requiring further therapy
under current guidelines. Transaminase flares appear therapeutic in nature and may reflect an immune
mediated clearance of infected hepatocytes essential in establishing persistent control of chronic HBV
infection

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才高八斗

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发表于 2019-2-23 03:44 |只看该作者
OP-02建立高效HBeAg功能治疗
REP 2139-Mg基慢性HBV感染的慢性HBV感染
联合治疗:REP正在进行的随访结果
401研究
Michel Bazinet1,Victor Pantea2,Gheorghe Placinta2,Iurie Moscalu3,Valentin Cebotarescu2,Lilia
Cojuhari2,Pavlina Jimbei4,Liviu Iarovoi2,Valentina Smesnoi4,Tatiana Musteata4,Alina Jucov2 3,
Adalbert Krawczyk5,Andrew Vaillant1
1Replicor Inc. ,,加拿大蒙特利尔; 2NicolaeTestemiţanu州立医药大学,
摩尔多瓦基希讷乌传染病科;共和党人3Arensia Exploratory Medicine
摩尔多瓦基希讷乌临床医院; 4TomaCiorbǎInfectiousClinical Hospital,。,基希讷乌,摩尔多瓦;
5UniversitätsklinikumEssen,德国埃森病毒学研究所
电子邮件:[email protected]
背景和目的:REP 401研究(NCT02565719)正在评估安全性和疗效
REP 2139-Mg(临床铅)或REP 2165-Mg联合替诺福韦地索普西富马酸盐(TDF)和
聚乙二醇化干扰素α-2a(pegIFN)在白种人HBeAg阴性慢性HBV感染患者中。
方法:对40例患者进行TDF治疗,随机分为实验组
(TDF 48周,pegIFN和REP 2139-Mg或REP 2165-Mg)或适应性对照组(24周)
TDF + pegIFN,然后交叉至48周的实验治疗)。所有患者都是
随后进行了为期48周的无治疗随访。监测病毒血症
雅培建筑师和实时平台。
结果:所有患者的基线HBsAg> 1000 IU / ml,14775.7±9302和9018±8743 IU / ml
在自适应控制和实验组。除一次停药外,治疗耐受性良好
与pegIFN相关的抑郁症。另外两名参与者退出治疗耐受良好的地方。
REP 2139-Mg和REP 2165-Mg之间的抗病毒反应难以区分且无相关性
基线时HBV基因型或HBsAg,ALT或纤维化(Fibroscan)。随着TDF的推出,
治疗期间所有患者均能很好地控制HBV DNA。随着NAPs的出台,HBsAg
在36/40患者中减少> 1 log,在28/40时变为<1 IU / ml,在24/40中变为<0.05 IU / ml
参与者。转氨酶发作在38/40例患者中发生,并与其减少相关
HBsAg在治疗期间自行消退,并未伴有任何肝功能障碍的证据。
在HBsAg <1的患者中,转氨酶突发特别明显(400-1748 U / L)
IU / ml并伴有抗-HBs的显着升高(高达255,055mIU / ml)。
截至提交日期,无治疗随访已延长至34/40周期的24或48周
患者完成治疗。持续稳定的慢性乙型肝炎病毒(HBV DNA <2000 IU / ml)
正常ALT)存在于15/34(44%)的参与者中。另有14/34(41%)参与者
功能性治愈(未检测到HBsAg和HBV DNA靶标)。肝功能已恢复正常,占94%
患者(基线时为47%)和中位肝硬度与F0(≤7kPa)一致
81%的患者(基线时为52%)。
结论:基于有限REP 2139-Mg的TDF和pegIFN联合治疗具有良好的耐受性
并且导致高比例的患者实现感染控制而不需要进一步治疗
根据现行准则。转氨酶耀斑在自然界中显得具有治疗作用,可能反映免疫
介导清除感染的肝细胞,对建立慢性HBV持续控制至关重要
感染
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