A Phase 2, Randomized, Open-Label Study to Evaluate the Safety and Efficacy of GS-4774 for the Treatment of Virally-Suppressed Subjects With Chronic Hepatitis B

The primary objectives of this study are to evaluate the safety and efficacy of GS-4774 in adults with chronic hepatitis B (CHB) viral infection who have been virally suppressed with an oral antiviral (OAV) medication.

开始日期2013-09-13

申办/合作机构

Gilead Sciences, Inc.

ChiCTR-ONRC-12002315 / Completed临床4期IIT

Contrast study of Entecavir monotherapy and the de novo combining Lamivudine with Adefovir therapy on HBeAg-positive CHB patients with high viral load

开始日期2011-09-02

申办/合作机构

南方医院

NCT01804387 / Unknown status临床4期IIT

Comparison of Telbivudine Plus Adefovir With Lamivudine Plus Adefovir for the Treatment of Lamivudine-resistant Chronic Hepatitis B at 52 Weeks: A Pilot Study

Lamivudine had been widely used for treatment-naïve chronic hepatitis B patients. However, development of antiviral resistance has been known as the major drawback: Incidence of lamivudine resistance was reported to be approximately 70% after 5 years (Lok AS et al, 2003). For the treatment of lamivudine resistance, adefovir has been widely used (Lok AS and McMahon B, 2009). However, switching to adefovir monotherapy was also reported to be at high risk of resistance, 25% at year 2 (Yeon JE et al, 2006). Recently, adding adefovir on lamivudine was shown to be superior to switching to adefovir monotherapy by decreasing the adefovir resistance (Rapti I et al, 2007, Lampertico P et al, 2007). However, combination of adefovir and lamivudine does not increase antiviral activity compared with adefovir monotherapy in patients with lamivudine resistance (Peters MG et al, 2004). As many patients are still viremic with the treatment of lamivudine and adefovir over 1 year, the investigators need more potent combination of the drugs. Telbivudine is a new nucleoside analogue with potent antiviral activity. The previous phase III study has shown the superiority of telbivudine over lamivudine in HBeAg positive and negative subjects (Lai CL et al, 2007). Therefore, telbivudine plus adefovir may be a better treatment option than lamivudine plus adefovir for the lamivudine-resistant chronic hepatitis B patients. No study assessing the efficacy of telbivudine plus adefovir has been conducted for these patients. The aim of this study is to evaluate the safety and efficacy of telbivudine plus adefovir compared with lamivudine plus adefovir in lamivudine resistant chronic hepatitis B patients at the end of 1 year follow-up,

开始日期2011-05-01

申办/合作机构

Korea University

100 项与阿德福韦相关的临床结果

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100 项与阿德福韦相关的转化医学

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100 项与阿德福韦相关的专利（医药）

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1,851

项与阿德福韦相关的文献（医药）

2024-08-07·Journal of the American Chemical Society

Regioselective Homolytic C²–H Borylation of Unprotected Adenosine and Adenine Derivatives via Minisci Reaction

Article

作者: Jiang, Yujie ; Zhou, Dazhi ; Que, Yingchuan ; Li, Zhiming ; Chen, Gang ; Zhou, Yutong ; Li, Yangyan ; Yang, Hui ; Butt, Madiha

A Minisci-type borylation of unprotected adenosine, adenine nucleotide, and adenosine analogues was successfully achieved through photocatalysis or thermal activation. Despite the challenges posed by the presence of two potential reactive sites (C² and C⁸) in the purine motif, the unique nucleophilic amine-ligated boryl radicals effortlessly achieved excellent C² site selectivity and simultaneously avoided the formation of multifunctionalized products. This protocol proved effective for the late-stage borylation of some important biomolecules as well as a few antiviral and antitumor drug molecules, such as AMP, cAMP, Vidarabine, Cordycepin, Tenofovir, Adefovir, GS-441524, etc. Theoretical calculations shed light on the site selectivity, revealing that the free energy barriers for the C²-Minisci addition are further lowered through the chelation of additive Mg²⁺ to N³ and furyl oxygen. This phenomenon has been confirmed by an IGMH analysis. Preliminary antitumor evaluation, derivation of the C²-borylated adenosine to other analogues with high-value functionalities, along with the CuAAC click reactions, suggest the potential application of this methodology in drug molecular optimization studies and chemical biology.

2024-07-01·Naunyn-Schmiedeberg's Archives of Pharmacology

Intravitreal ranibizumab injection is associated with an increased risk of chronic kidney disease: a population-based study in Taiwan

Article

作者: Chen, Chuan-Mu ; Lim, Paik Seong ; Yu, Teng-Shun ; Chuang, Wu-Lung ; Wu, Tsai-Kun ; Chang, Kuang-Hsi ; Chen, Chang-Hsu ; Tsai, Fuu-Jen

AbstractSystemic vascular endothelial growth factor (VEGF) blockade has been the top adjunctive chemotherapy since 1990. Anti-VEGF therapy has also been associated with worsened renal function in some patients. However, the association between patient outcomes and use of intravitreal VEGF inhibitors remains controversial. Thus, it is necessary to determine the action mechanism and long-term renal effects of ranibizumab. The National Health Insurance Research Database (NHIRD) is one of the largest global databases that are extensively used for epidemiological research. NHIRD contains the medical information of all insureds, such as inpatient, outpatient, emergency, and traditional Chinese medicine records. We selected subjects aged ≥ 20 years who recently administered ranibizumab for the ranibizumab cohort. Non-ranibizumab cohort consisted of subjects who did not receive ranibizumab, and the index date was a random date between 2008 and 2018. We excluded subjects with missing sex and age records and those in which the date of primary outcome was before the index date. The two cohorts were matched via 1:1 propensity score matching based on sex, age, index year, hypertension, diabetes mellitus, hyperlipidemia, stroke, coronary artery disease, alcoholism, chronic obstructive pulmonary disease, and age-related macular degeneration, retinal vein occlusion, and diabetic macular edema. Medical confounders were angiotensin I-converting enzyme inhibitors, statins, corticosteroids, VEGF inhibitors including bevacizumab and aflibercept, lithium, amphotericin B, adefovir, NSAIDS, cisplatin, and calcineurin inhibitors. Among 48,248 participants aged ≥ 20 years, 24,136 (50%) received ranibizumab (13,565 male [56.20%] and 10,571 female [43.80%]). Moreover, 24,136 participants who did not receive ranibizumab were matched by age, sex, comorbidities, and medications. Subjects who received ranibizumab exhibited a significantly higher risk of CKD than those who did not receive ranibizumab (adjusted hazard ratio = 1.88, 95% CI = 1.79–1.96). Our findings revealed that exposure to intravitreal ranibizumab is an independent risk factor for CKD. Therefore, physicians and ophthalmologists should make the patients aware of such a correlation to increase patient safety and decrease the CKD burden.

2024-07-01·European Journal of Clinical Pharmacology

Understanding adefovir pharmacokinetics as a component of a transporter phenotyping cocktail

Article

作者: Taubert, Max ; Bilal, Muhammad ; Fuhr, Uwe ; Dong, Qian ; Kinzig, Martina ; Dokos, Charalambos ; Scherf-Clavel, Oliver ; Sörgel, Fritz ; Chen, Chunli

AbstractPurposeAdefovir (as dipivoxil) was selected as a probe drug in a previous transporter cocktail phenotyping study to assess renal organic anion transporter 1 (OAT1), with renal clearance (CLR) as the primary parameter describing renal elimination. An approximately 20% higher systemic exposure of adefovir was observed when combined with other cocktail components (metformin, sitagliptin, pitavastatin, and digoxin) compared to sole administration. The present evaluation applied a population pharmacokinetic (popPK) modeling approach to describe adefovir pharmacokinetics as a cocktail component in more detail.MethodsData from 24 healthy subjects were reanalyzed. After establishing a base model, covariate effects, including the impact of co-administered drugs, were assessed using forward inclusion then backward elimination.ResultsA one-compartment model with first-order absorption (including lag time) and a combination of nonlinear renal and linear nonrenal elimination best described the data. A significantly higher apparent bioavailability (73.6% vs. 59.0%) and a lower apparent absorption rate constant (2.29 h−1 vs. 5.18 h−1) were identified in the combined period compared to the sole administration period, while no difference was seen in renal elimination. The population estimate for the Michaelis-Menten constant (Km) of the nonlinear renal elimination was 170 nmol/L, exceeding the observed range of adefovir plasma maximum concentration, while the maximum rate (Vmax) of nonlinear renal elimination was 2.40 µmol/h at the median absolute estimated glomerular filtration rate of 105 mL/min.ConclusionThe popPK modeling approach indicated that the co-administration primarily affected the apparent absorption and/or prodrug conversion of adefovir dipivoxil, resulting in the minor drug-drug interaction observed for adefovir as a victim. However, renal elimination remained unaffected. The high Km value suggests that assessing renal OAT1 activity by CLR has no relevant misspecification error with the cocktail doses used.

项与阿德福韦相关的新闻（医药）

2024-10-29

·医药观澜

抗乙肝1类新药获中国国家药监局批准上市

10月28日，中国国家药监局（NMPA）宣布批准新通药物全资子公司葛蓝新通制药申报的1类创新药甲磺酸普雷福韦片（曾用名：甲磺酸帕拉德福韦片）上市申请，用于治疗成人慢性乙型肝炎。根据新通药物公开资料，这是一种治疗慢性乙肝的肝靶向核苷类药物。慢性乙型病毒性肝炎是由乙型肝炎病毒（HBV）引起的、以肝脏炎症为主要表现的传染病。HBV是一个双链DNA病毒，其复制转录过程在人体肝细胞内完成。病毒复制的逆转录过程需要病毒基因整合到人体肝细胞核中，形成病毒核心颗粒，成熟的病毒核心颗粒在细胞质中进一步组装成为成熟病毒释放至肝细胞外，引发肝脏炎性病变。核苷（酸）类药物通过抑制病毒DNA聚合酶以阻止病毒持续复制。据新通药物此前招股书介绍，普雷福韦基于肝靶向创新药物研发平台开发，在阿德福韦结构基础上引入芳基磷酸环二酯结构，形成肝靶向阿德福韦前药。该产品在血液和胃肠道中稳定，只有药物进入肝脏后，被肝脏中特异性高表达的CYP3A4酶氧化后开环，再经β消除，才会释放出活性产物单磷酸化阿德福韦。后者是一种单磷酸腺苷的无环核苷（酸）类似物，其在体内细胞激酶作用下进一步磷酸化生成活性代谢产物阿德福韦二磷酸，它与天然底物脱氧腺苷三磷酸竞争，抑制HBV的DNA聚合酶（逆转录酶），且可以通过整合到病毒DNA链使得DNA复制终止，从而抑制乙肝病毒复制。在已完成的1期、2期和3期临床试验的核心临床阶段中的数据显示，普雷福韦片抑制乙肝病毒DNA复制率、乙肝e抗原（HBeAg）转阴率及肝功复常率等疗效指标与当前一线用药对比的疗效相当。在临床试验中，未观察到核苷（酸）类药物常见的对肾脏、骨骼的不良影响。相比于对照药，甲磺酸帕拉德福韦片在肾脏和骨骼等方面的安全性更佳，对血脂影响更低，长期用药心脑血管疾病隐患小。慢性乙型肝炎病毒（HBV）感染有着显著的发病率和死亡率，是全球公共卫生面临的紧迫挑战。希望普雷福韦在中国的获批，能为患者带来新的治疗选择。参考资料： [1]国家药监局批准甲磺酸普雷福韦片上市. Retrieved Oct 28, 2024. From https://www.nmpa.gov.cn/zhuanti/cxylqx/cxylqxlm/20241028144038195.html [2]新通药物招股书. Retrieved Apr 13, 2023. From http://listing.sse.com.cn/renewal/xmxq/index.shtml?auditId=1062&anchor_type=0 内容来源于网络，如有侵权，请联系删除。

上市批准寡核苷酸核酸药物

2024-09-30

·仁度生物

前沿速递 | 9月HBV RNA研究新进展

9月，有关HBV RNA的研究取得了一些新的进展，主要是有关HBV RNA在HBV-HIV合并感染人群中的诊断价值，这些崭新的研究成果为开发、研究HBV治疗新策略注入了新鲜的血液。大刊新文 Diagnostic Utility of Pre-Genomic Hepatitis B RNA in the Evaluation of HBV/HIV Coinfection [HBV RNA在HBV-HIV合并感染人群中的诊断价值] 发表期刊：Pathogens and Immunity 研究机构：University of Cincinnati College of Medicine 文章作者：Kenneth E Sherman , Susan D Rouster , Heidi Meeds , Marion G Peters , Jason T Blackard , Paul S Horn , Timothy Archampong , Awewura Kwara , Mark Anderson , Michael Stec , Gavin A Cloherty 背景乙肝新标志物HBV RNA在HBV-HIV合并感染人群中的应用价值有待探索。方法本研究共纳入283名患者。分为两个独立的组， 236名HBV/HIV合并感染者（ACTG队列），47名HBV感染者（Ghana队列），接受核苷类似物治疗（替诺福韦与阿德福韦）。结果在这两个队列中，HBe抗原血症（antigenmia）与pgRNA和HBV DNA水平高度相关。在治疗队列中，治疗前pgRNA血清浓度为7.0 log10 U/mL，平均 qHBsAg为 201,297 IU/mL。治疗12周及48周后，接受TDF治疗的个体，比接受ADV治疗的个体pgRNA下降更多（12w 0.24U/mL log10; 48w 0.30 log10U/mL）（图1）。图1. HBV治疗后不同用药方案pgRNA下降曲线（ACTG队列）图2：HBV RNA与HBV DNA及ALT相关性（Ghana队列） HBV RNA与HBV DNA中等相关，与ALT相关性弱（HBV DNA and pgRNA, (r=0.44; P=0.0001); ALT and pgRNA (r=0.23; P<0.05) 结论 pgRNA和qHBsAg是乙肝领域新标志物，有助于监测治疗结果，还可预测闭合环状DNA（cccDNA）模板的转录活性以及肝损伤情况。撰写：Brigette 审核：Jessica Candy 排版：六六往期回顾前沿速递 | 8月HBV RNA研究新进展前沿速递 | 7月HBV RNA研究新进展关于仁度上海仁度生物科技股份有限公司（股票代码：688193）成立于2007年，是国内最早一批专注于RNA分子诊断技术和产品的生命科学企业之一，致力于开发临床需求尚未满足的创新诊断技术和产品。公司拥有RNA实时荧光恒温扩增（SAT）的独家专利技术平台，以该技术平台为基础自主研发了一系列分子诊断试剂和设备一体化产品，专注于为生殖、呼吸、消化、血液、食品、环境安全等领域病原体的精准诊断、有效防控和个性化诊疗提供解决方案。仁爱生命度衡健康专注病原体RNA临床检测

临床研究

2023-06-08

·药智网

5月CDE药审报告：1442个药品获受理，贝达药业、百济神州…

看点 • 5月药审中心受理总量为1442个• 5月3个化药1类创新药申请上市• 5月新增62个按仿制药质量和疗效一致性评价申报的受理号• 奥磷布韦片、甲磺酸贝福替尼胶囊、贝妥单抗注射液等1类创新药获批上市据药智数据企业版——药品注册与受理数据库最新统计，2023年5月份CDE共承办新的药品注册申请以受理号计有1442个，其中化药受理955个，中药受理305个，生物制品受181个；2023年1-5月各类药品注册申请受理情况详见图1。PS：药智网公众号【ID:yaozh008】后台回复【5月CDE药审】，即可获取本文表格excel格式文档图1 2023年1-5月CDE药品受理情况2023年5月份（注：状态开始时间（药智）从2023年5月1日至2023年5月30日）完成审评的受理号共1449个，其中化药受理983个，中药受理269个，生物制品受理196个；2023年1-5月各类药品完成审评情况详见图2。图2 2023年1-5月CDE药品完成审评情况以下且看化药、中药、生物制品的注册受理及审评情况详细分析。一、化药申报与审评情况（一）化药受理情况5月份CDE承办新的化药注册申请955个（以受理号计），其中新药申请受理号127个，进口受理号46个，仿制申请受理号283个，补充申请429个，进口再注册45个；以审评任务类别统计（以受理号计），IND申请153个，ANDA申请288个，NDA申请12个；2023年1-5月CDE化药各审评任务类别申请受理情况详见图3。图3 2023年1-5月CDE化药各审评任务类别申请受理情况1.化药1类国产申报情况5月CDE受理化药国产1类新药共计109个（按受理号计），其中IND申请106个，涉及46个品种（按药品+企业维度统计），NDA申请3个，涉及3个品种（按药品+企业维度统计），目前均已进入相应序列排队待审；下表为5月新承办的1类国产新药。表1 2023年5月新承办的化药1类国产新药注：排队序号截止至2023年06月06日。2.化药1类进口药品申报情况5月共22个进口化药1类受理号获得承办，其中全是IND申请，共9个品种，目前均已进入相应序列排队待审；下表为5月新承办的1类进口新药。表2 2023年5月新承办的化药1类进口新药注：排队序号截止至2023年06月06日ISM3091胶囊ISM3091是英矽智能自主研发的USP1小分子抑制剂，已获得FDA新药临床试验申请批件，用于在实体瘤患者中开展I期临床试验。目前，国内新药临床试验申请已获CDE受理。HZ012注射液HZ012是和泽医药主导研发的GLP-1R/GIPR激动剂药物，GLP-1是能单独应用于临床的肠促胰素，具有高度脏器选择性、副作用少的特点，是近年来降糖药物的研发热点。目前国内布局GLP-1R/GIPR激动剂的药企已有博瑞医药、鸿运华宁、豪森药业、和泽医药等，豪森药业等。IPG11406片IPG11406是艾美斐自主研发的全球性创新药，是一款针对包括IBD（炎症性肠病）在内的自身免疫性疾病开发的新型GPCR小分子拮抗剂，具有理化性质优异、活性高、靶点特异性好、安全窗口大等特点，在多种自身免疫性疾病临床前研究中皆呈现剂量依赖性的显著药效。甲磺酸帕拉德福韦片甲磺酸帕拉德福韦是利用HepDirectTM前药技术开发的一款阿德福韦酯中间体阿德福韦（PMEA）的前药，用于治疗慢性乙型肝炎。该药为新通药物子公司凯华公司于2011年1月从LGND授权引进而来，目前，国内新药上市申请已获受理。3.化药改良型新药申报情况5月新增化药2类改良型新药25个（按受理号计），其中全为IND申请，共涉及16个品种；2023年1-5月CDE化药改良型新药申请受理情况详见图4。图4 2023年1-5月CDE化药改良型新药申请受理情况5月，改良型新药无新承办上市申请。（二）化药完成审评情况5月份CDE完成审评的化药注册申请983个（以受理号计），其中新药申请受理号138个，进口受理号77个，仿制申请受理号276个，补充申请446个；以审评任务类别统计（以受理号计），IND申请155个，ANDA申请280个，NDA申请32个，进口再注册申请27个，一致性评价79个；2023年5月CDE化药各审评任务类别完成审评情况详见图5；图5 2023年5月CDE化药各审评任务类别完成审评情况以受理号审评结论来看（结论数据统计截止2023年06月06日），其中批准临床168个，批准生产125个，批准进口24个，未被批准54个；2023年5月CDE化药化药完成审评结论情况详见图6；图6 2023年5月CDE化药化药完成审评结论情况1.化药新药和进口原研获批情况5月批准的新药和进口原研共13个，包括：2个1类新药、2个2类新药和9个进口原研批准上市；下表为5月化药获批新药和进口原研信息。表3 2023年5月化药获批新药和进口原研信息奥磷布韦片奥磷布韦片是南京圣和药业自主研发并拥有自主知识产权的1类创新药，是国内首个拥有自主知识产权的NS5B抑制剂，适用于与盐酸达拉他韦联用，治疗初治或干扰素经治的泛基因型成人慢性丙型肝炎病毒（HCV）感染，可合并或不合并代偿性肝硬化。该药品的上市为成人慢性丙型肝炎病毒患者提供了新的治疗选择。甲磺酸贝福替尼胶囊甲磺酸贝福替尼胶囊是贝达药业申报的1类创新药，是第三代表皮生长因子受体酪氨酸激酶抑制剂，能够选择性地抑制EGFR敏感突变和EGFR T790M耐药突变激酶，该药适用于既往经表皮生长因子受体（EGFR）酪氨酸激酶抑制剂治疗出现疾病进展，并且伴随EGFR T790M突变阳性的局部晚期或转移性非小细胞肺癌患者的治疗。该药品的上市为非小细胞肺癌患者提供了新的治疗选择。2.化药仿制药获批情况5月共98个化药仿制药批准上市（按药品名+企业维度统计，排除了“氧”的数据统计），其中包括3类仿制药的14个，4类仿制药的77个，进口5.2类7个；ATC分类包括：心血管系统、神经系统等（仿制药获批具体信息请关注药智数据企业版——药品注册与受理数据库）。二、中药申报与审评情况（一）中药受理情况5月份CDE承办的中药注册申请受理号共计305个，其中新药7个，补充申请297个，进口再注册1个；2023年1-5月CDE中药各申请类型受理情况详见图7。图7 2023年1-5月CDE中药各申请类型受理情况1.中药新药申报情况5月共承办申请类型为新药的受理号共7个，其中，5个中药1类创新药，共涉及5个品种，均为IND申请；1个2类改良型新药申请，为IND申请；1个3类经典名方制剂，为NDA申请；下表为5月新承办的中药新药。表4 2023年5月新承办的中药新药注：排队序号截止至2023年06月06日（二）中药完成审评情况5月份CDE完成审评的中药注册申请269个（以受理号计），其中新药受理号9个包含：8个IND申请和1个NDA申请，补充申请260个；在受理号审评结论方面（结论数据统计截止2023年06月06日），5月中药无新药获批上市，结论包括：批准补充253个，批准临床4个，未被批准7个。三、生物制品审评情况（一）生物制品受理情况5月份CDE承办新的生物制品注册申请受理号共计181个，新药94个，补充申请62个，进口21个，进口再注册1个，一次性进口3个；2023年1-5月CDE生物制品各申请类型受理情况详见图8。图8 2023年1-5月CDE生物制品各申请类型受理情况1.生物制品1类新药申报情况5月共77个生物制品1类新药受理号获得承办，其中，临床试验申请72个，上市申请5个，目前均已进入相应序列排队待审；下表为5月新承办的生物制品1类创新药。表5 2023年5月新承办的生物制品1类新药注：排队序号截止至2023年06月06日（二）生物制品完成审评情况5月份CDE完成审评的生物制品注册申请196个（以受理号计），其中新药申请受理号98个，进口受理号26个，补充申请61个；以审评任务类别统计（以受理号计），临床试验申请104个，上市申请20个；2023年5月CDE生物制品各审评任务类别完成审评情况详见图9；图9 2023年5月CDE生物制品各审评任务类别完成审评情况在受理号审评结论方面（结论数据统计截止2023年06月06日）：批准临床90个，批准生产14个，批准进口3个，批准再注册5个，未被批准3个；下表为5月生物制品批准上市信息。表6 2023年5月生物制品获批信息四、按一致性评价申报品种情况5月新增62个按一致性评价要求进行申报的受理号和285个视同受理号。（篇幅限制仅展示一致性信息，视同及具体信息请关注药智数据企业版——药品注册与受理数据库）；下表为5月新增一致性评价受理号信息。表7 2023年5月新增一致性评价受理数据数据来源：药智数据企业版——药品注册与受理数据库注：本文以上文章刊载内容知识产权归药智网所有，如需转载，请注明出处和本文链接。声明：本内容为作者独立观点，不代表药智网立场。如需转载，请务必注明文章作者和来源。对本文有异议或投诉，请联系maxuelian@yaozh.com。责任编辑 | 八角转载开白 | 马老师 18996384680（同微信）商务合作 | 王存星 19922864877（同微信）阅读原文，是昨天最受欢迎的文章哦

临床申请一致性评价申请上市

100 项与阿德福韦相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
D02768	阿德福韦	-	DB13868

研发状态

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适应症	最高研发状态	国家/地区	公司	日期
乙型肝炎	临床2期	-	Rega Institute for Medical Research	-
HIV感染	临床2期	美国	Gilead Sciences, Inc.	-

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临床结果

适应症

分期

评价

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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


NCT01943799 (CTgov)	临床2期	慢性乙型肝炎	178	OAV+telbivudine+tenofovir disoproxil fumarate+lamivudine+adefovir+entecavir (OAV Alone (Group A))	淵餘襯構廠襯積窪網窪(範齋齋淵壓繭範構壓鑰) = 繭餘壓鏇齋蓋夢網廠顧網網製淵鹹繭構鬱糧鏇 (製糧鏇範願積壓構窪築, 鬱獵糧蓋築鏇糧鹽衊艱 ~ 糧衊製糧廠餘齋範艱餘) 更多	-	2019-11-01
				OAV+GS-4774 (OAV + GS-4774 2 YU (Group B))	淵餘襯構廠襯積窪網窪(範齋齋淵壓繭範構壓鑰) = 觸顧淵鏇觸選遞衊夢遞網網製淵鹹繭構鬱糧鏇 (製糧鏇範願積壓構窪築, 襯膚窪願範膚積衊醖遞 ~ 觸鹽淵餘鏇獵齋願齋鬱) 更多
NCT00023309 (CTgov)	临床2期	慢性乙型肝炎	41	Lamivudine+adefovir (Lamivudine and Adefovir)	襯觸鬱窪鹹蓋鹹夢鑰襯(淵範鏇衊廠鹽糧顧鬱襯) = 繭艱壓願鹽艱構範廠鹹襯鑰淵廠簾衊鑰淵構遞 (窪積繭選齋鑰醖鹽網糧, 鹹齋醖鏇齋醖顧壓繭願 ~ 遞憲餘夢齋廠醖襯鏇網) 更多	-	2013-04-04
				Adefovir alone (Adefovir)	襯觸鬱窪鹹蓋鹹夢鑰襯(淵範鏇衊廠鹽糧顧鬱襯) = 鏇鬱範繭夢遞壓鹹衊鹹襯鑰淵廠簾衊鑰淵構遞 (窪積繭選齋鑰醖鹽網糧, 網獵願遞襯觸憲鹽鹽鹹 ~ 製網淵淵構鏇衊範獵窪) 更多