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FDA批准抗艾药Viread用于治疗乙型肝炎 [复制链接]

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发表于 2008-12-3 07:09
抗爱滋病毒处方药可抑制乙型肝炎病毒增长--美国联邦食品药物管理局批准Viread专家强调是抗乙肝病毒的重要进展--

DWNEWS.COM-- 2008年10月1日6:16:26(京港台时间) --多维新闻网

加州福斯特市2008年9月2日讯? Gilead Sciences (Nasdaq: GILD)今天宣布,美国联邦食品药物管理局(FDA)已经批准该公司的慢性乙肝治疗药Viread®(tenofovir disoproxil fumarate)的上市。慢性乙型肝炎是由乙型肝炎病毒(HBV)造成的严重肝病,也是全球各地造成肝癌的首要原因,在美国估计有二百万名患者。

Viread目前也被指示可以治疗成年人慢性乙肝病,每日口服一次药片,可以阻断乙肝病毒的DNA聚合?,也就是病毒在肝细胞里增殖所需的酵素。Viread从2001年起已经在美国用於治疗成人爱滋病。

Weill Cornell医学院肠胃肝学系主任Ira Jacobso表示:「Viread将是治疗乙型肝炎的一项重要选择,联邦食品药物管理局的批准代表着医学界研发抗慢性乙肝药物的重要进展。」

关键的临床试验

联邦当局的批准主要是根据两项一直在进行的随机双重盲检第三期临床试验,102和103号研究的数据,在48周治疗期间比较Viread和 Gilead’s Hepsera®(adefovir dipivoxil)的治疗反应。两项研究结果显示,接受Viread治疗的乙肝病人对治疗的完全应答比例,要比接受Hepsera治疗的高出很多。所谓完全应答是指乙肝病毒血清DNA水平低於400拷贝/mL而且组织明显改善,在Knodell肝炎活动指数方面至少降低两点(一种衡量细胞坏死导致肝脏发炎的方式,包括或导致肝细胞死亡的过程)没有肝组织硬化同时恶化的现象。参加试验的人士包括新接受乙肝治疗(n=375)的病人以及以前已经接受核甘治疗的病人(n=51)。截至目前,在这些研究中已经有400多名慢性乙肝病人接受Viread治疗试验。

Gilead Sciences公司商务部执行副总裁Kevin Young表示:「乙肝药Viread的批准代表了我们在爱滋病和肝炎两个研究领域十多年来开发药品的努力,希望能研究出一种每天只需服用一次既安全又能强力抑制病毒的疗法。我们感谢参加临床试验的研究员和病人,才能取得今天药品通过批准的成就。我们期待与社区人士合作,一起宣导对乙肝的认识和治疗。」

由於慢性乙型肝炎感染后可能持续多年而没有明显症状,很多病人不知道自己已经感染,也不知道早日寻求治疗。亚裔美国人罹患乙肝的比例偏高,几乎每10个出生国外的亚裔美国人曾感染乙肝,比非亚裔人士多出100倍,反映出许多乙肝在亚洲国家的盛行。

纽约社区医院医生Danny Chu表示:「虽然我们在降低美国境内乙型肝炎患者的病发率有很大进展,但是大众对於肝炎和如何选择有效新治疗的认识还有待提高。」

Viread获得批准扩展了Gilead在治肝炎健康药物方面的制造及经销权利。该公司第一个慢性乙肝治疗药Hepsera,目前是美国使用最广泛的乙肝口服处方药。该公司也在研发治疗丙型即C型肝炎的微分子复合药以及与肝炎有关的肝纤维症的治疗药,包括非酒精性脂肪变性肝炎nonalcoholic steatohepatitis (简称NASH)。

今年稍早Viread也获得欧盟、土耳其、奥地利和纽西兰等国家批准作为乙肝治疗药,在加拿大的上市申请目前正等待批准中。

慢性乙肝治疗药Viread

Viread (tenofovir disoproxil fumarate)用於治疗成年人慢性乙型肝炎。

在开始使用治疗时必须考虑以下几点:

· 本治疗是根据一年的治疗数据,主要是有失偿性肝硬化、呈HBeAg阳性和HBeAg阴性的成年人慢性乙肝病人。

· 曾经历核甘或干安能治疗突变的基线临床试验病人的数字太小而无法达到有效的结论。

· Viread对失偿性肝病病人还没有进行评估。

慢性乙肝的建议治疗剂量是每天口服300 mg毫克,可单独或与食物并服,有肾脏问题的病人服用剂量必须间歇性调整。

乳酸中毒/皮脂腺肝肿大以及治疗后的肝炎恶化

病人在单单使用核甘类似物或与其他抗逆转病毒的混合治疗后,有过乳酸中毒和严重的皮脂腺肝肿大,包括致命病例的报告。

乙肝病人在停用包括Viread在内的抗乙肝病毒治疗之后,有过肝炎可能严重恶化的报告。停止治疗的病人应利用临床和实验室追踪,密切观察肝功能至少数月。如果适当,可恢复抗乙肝治疗。

在使用Viread之后有过新出现或恶化的肾脏病例,包括急性肾衰竭和Fanconi症的报告。在开始使用Viread之前,最好评估容易出现风险的病人的肌酸酐清除试验creatinine clearance (CrCl)并检测CrCl和磷血清。使用Viread时应避免同时使用肾中毒的药物,包括Hepsera。

使用Viread治疗之前,应对乙肝病人提供爱滋病毒抗体检测。对於有或没有乙型肝炎的爱滋病人,Viread只能用作合适的抗逆转病毒混合疗程的一部份。

Viread对爱滋病人有骨骼矿物质疏松(BMD)的报告。有骨折病例或骨质疏松症的病人最好考虑骨骼矿物质疏松检测。Viread对慢性乙肝病人的骨质影响尚无研究。

在慢性乙肝病人控制临床试验中,最常见的负面反应是(all grades)恶心。在Viread治疗中出现多於5%的其他反应,包括:腹痛、腹泻、头痛、头晕、疲惫、鼻咽炎、背痛和皮肤疹。

慢性乙肝

乙型肝炎病毒(HBV)比爱滋病毒传染高出100倍。虽然原本健康的成人的新病例大部分会在几个月内因本身的免疫系统自行痊愈,很多人会演变成慢性的终身感染,特别是新生儿和儿童感染。慢性乙肝长期下来会破坏肝脏,导致肝硬化或肝癌等严重病症。

80 %的全球肝癌据信是乙型肝炎病毒引起,高居致癌危险因子的第二位,仅次於烟草。

乙型肝炎会藉由血液接触和人体体液的方式传染,包括性接触和使用污染的针筒吸毒,也会经由母体传染给新生婴儿,这是亚裔美国人主要的传染途径。亚裔是美国人口成长最快的族裔之一,2007年约有一千五百万人。最近的研究显示,三分之二的亚裔乙肝带菌者不知道自己已经感染。

慢性肝炎虽然没有简单的治愈方法,不过抗毒疗法可以延缓病毒的蔓延,减少肝脏受损。

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Gilead Sciences简介 (同是生产研制阿德福韦的公司)

Gilead Sciences是一家专门研发及商业推广创新医学疗法的生物制药公司。公司理念是提升对全球患有生命威胁疾病的病人的照顾。Gilead公司总部在加州福斯特市,在北美、欧洲和澳洲设有分公司。

本新闻稿包括免责声明forward-looking statements,依据1995年Private Securities Litigation诉讼改革法案,可能有风险、不确定和其他因素,包括医生在现有的乙肝治疗中不能开本产品处方药以及管理机构和保险付款人可能不愿核准或补偿本产品的付费等风险。这些风险、不确定和其他因素可能造成与免责声明不同的结果。读者必须谨慎,不能完全依赖这些声明。这些因素和其他风险在 2007年12月31日结束的公司年度报告10-K表格以及2008年第二季的季报告10-Q表格有详细叙述,一如呈交联邦证券交易委员会的报告。所有的免责声明是根据Gilead目前取得的资讯,Gilead不用负责更新这类声明。

[ 本帖最后由 liver411 于 2008-12-3 07:19 编辑 ]
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发表于 2008-12-3 07:15
Rescue Therapy with Entecavir (Baraclude) plus Tenofovir (Viread) Is Safe and Effective for Cirrhotic Hepatitis B Patients with Prior Treatment Failures

By Liz Highleyman



Several nucleoside/nucleotide analogs have potent activity against hepatitis B virus (HBV), but resistance mutations can emerge when these agents are used as monotherapy. Drug resistance is particularly a concern for patients who have experienced multiple prior treatment failures, which can lead to dangerous hepatic flares (worsening liver inflammation) in those with advanced disease.

In an open-label study presented at the recent 59th Annual Meeting of the American Association for the Study of Liver Diseases (AASLD 2008) in San Francisco, German researchers assessed the safety and efficacy of combination tenofovir (Viread) plus entecavir (Baraclude) initiated as rescue therapy in 12 treatment-experienced chronic hepatitis B patients with cirrhosis.

All participants were men, the median age was 49 years, all were HIV negative, and 9 were hepatitis B "e" antigen (HBeAg) positive. Patients had multidrug-resistant HBV or only partial response to previous treatment (median 3 regimens). At baseline, the median ALT level was 1.6 x the upper limit of normal (ULN) and the median HBV DNA level was 5 x 106 copies/mL.

Results

    • The median treatment duration after initiating tenofovir + entecavir was 6 months (range 3-15 months).

    • 9 of 12 patients (75%) achieved undetectable HBV DNA (< 400 copies/mL).

    • The median HBV DNA level decreased by 4.6 logs (range 1.7-7.8 log) (P < 0.0001).

    • ALT also decreased significantly (P = 0.001).

    • No significant clinical side effects were reported.

    • No patients experienced liver decompensation due to complications of cirrhosis or development of hepatocellular carcinoma (HCC).

    • 6 patients became HBV DNA negative for the first time, demonstrating the high antiviral efficacy of this combination despite pre-existing resistance mutations or only partial response to prior therapies.

    • However, no patients experienced HBeAg or hepatitis B surface antigen (HBsAg) loss.

Based on these findings, the researchers concluded that, "rescue therapy with entecavir and tenofovir in cirrhotic HBV monoinfected patients harboring complex viral resistance patterns or showing only partial antiviral responses earlier was highly efficient, safe, and well tolerated."

However, they added, "More data are certainly needed to judge about the long-term safety, long-term antiviral efficacy and prevention of emergence of new viral mutations and prevention of clinical decompensation or HCC using this therapeutical approach in HBV patients with advanced liver disease."

Department of Medicine, University Hospital Hamburg-Eppendorf, Hamburg, Germany; Department of Microbiology and Virology, University Hospital Hamburg-Eppendorf, Hamburg, Germany.

11/18/08

Reference
J Schollmeyer, M Lutgehetmann, T Volz, and others. Combination of entecavir and tenofovir as a rescue therapy is safe and highly efficient in cirrhotic HBV mono-infected patients with the history of multiple previous treatment failures. 59th Annual Meeting of the American Association for the Study of Liver Diseases (AASLD 2008). San Francisco. October 31-November 4, 2008. Abstract 985.
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发表于 2008-12-3 07:20
Tenofovir (Viread) Produces Continued HBV Suppression through 96 Weeks in HBeAg Positive and Negative Patients: Studies 102 and 103

By Liz Highleyman

Several antiviral agents have potent activity against hepatitis B virus (HBV), but the emergence of drug-resistance mutations is a barrier to long-term treatment effectiveness.

At the 59th Annual Meeting of the American Association for the Study of Liver Diseases (AASLD 2008) this week in San Francisco, researchers presented 96-week results from 2 Gilead clinical trials assessing tenofovir (Viread) in patients with hepatitis B "e" antigen (HBeAg) negative and HBeAg positive chronic hepatitis B.

Tenofovir is widely used to treat HIV, and was approved in August as a therapy for chronic hepatitis B.

Studies 102 and 103 were multicenter, randomized, double-blind Phase 3 trials comparing tenofovir versus adefovir (Hepsera) in chronic hepatitis B patients with compensated liver disease. Study 102 included 375 HBeAg negative patients, while Study 103 included 266 HBeAg positive participants. About 68% were men and the mean age was 43 years. In Study 102 about two-thirds were Caucasian and one-quarter were Asian; in Study 103, about half were Caucasian, and about one-third were Asian. Most were treatment-naive, though about 15% had previously used lamivudine (Epivir-HBV). The studies did not include patients with HIV-HBV coinfection.

As previously reported, tenofovir produced higher rates of HBV DNA clearance < 400 copies/mL compared with adefovir at 48 weeks (93% vs 63% in Study 102; 76% vs 13% in Study 203..

After the initial 48-week treatment period, patients originally randomized to receive adefovir in both studies switched to open-label tenofovir for another 48 weeks, while those originally assigned to tenofovir continued to take it for the same duration.

After 72 weeks, patients with continued HBV DNA > 400 copies/mL (confirmed on 2 consecutive visits) had the option of adding emtricitabine (Emtriva, also combined with tenofovir in the Truvada fixed-dose coformulation). Emtricitabine is approved for treatment of HIV and is under study for hepatitis B.

96-week data from both studies was presented at the Liver Meeting. The study is scheduled to continue through 384 weeks (more than 7 years).

Combined Results:

    • Patients who received tenofovir for up to 96 weeks experienced sustained HBV DNA suppression.

    • All patients who had undetectable HBV DNA while on adefovir maintained virological suppression after switching to tenofovir at week 48.

    • Patients generally had achieved ALT normalization by week 48, and this was maintained through week 96.

    • Tenofovir continued to be well-tolerated, and no new safety issues were identified.

    • No mutations associated with tenofovir resistance were identified in either study.

Study 102 Results

    • In an intent-to-treat analysis at 96 weeks, 91% of HBeAg negative patients originally randomized to the tenofovir arm and 89% of those who switched from adefovir to tenofovir achieved sustained HBV DNA suppression < 400 copies/mL.

    • In an as treated analysis, 96% of patients in the continuous tenofovir arm and all patients in the switch arm achieved undetectable HBV DNA.

    • Of the 2 patients who added emtricitabine after 72 weeks, 1 achieved full virological suppression by week 96.

    • None of the patients experienced hepatitis B surface antigen (HBsAg) loss.

    • 10% of patients in both the continuous tenofovir arm and the adefovir-to-tenofovir switch arm had grade 3-4 laboratory abnormalities.

    • No patients experienced a confirmed 0.5 mg/dL increase in serum creatinine or creatinine clearance less than 50 ml/min (markers of kidney damage, a potential side effect of adefovir and tenofovir in susceptible patients).
    The investigators concluded that tenofovir "produced potent, continuous viral suppression and was well tolerated through week 96."

"Patients switching to tenofovir after 48 weeks of adefovir treatment benefited with significant additional viral suppression and had a similar response to patients treated with tenofovir for 96 weeks," they added.

"In this study, Viread [tenofovir] produced a significant and sustained effect over two years of treatment with no evidence of resistance, which is a substantial clinical finding," said principle investigator Patrick Marcellin, MD, in a press release issued by Gilead. "Additionally, patients in this study taking Hepsera [adefovir] were rolled over to Viread without new safety signals and without compromising the efficacy of anti-HBV treatment."

Hopital Beaujon, University of Paris, Clichy, France; Hospital Valle Hebron, Barcelona, Spain; University Hospital St Ivan Rilsky, Sofia, Bulgaria; University of Uludag, Bursa, Turkey; Tokuda Hospital, Sofia, Bulgaria; Royal Free Hospital, London, UK; University of Calgary, Calgary, Alberta, Canada; Toronto Western Hospital, University of Toronto, Toronto, Ontario, Canada; Gilead Sciences, Durham, NC.

Study 103 Results

    • In a 96-week intent-to-treat analysis, 78% of HBeAg positive patients achieved HBV DNA suppression < 400 copies/mL in both the continuous tenofovir arm and the adefovir-to-tenofovir switch arm.

    • In an as-treated analysis, 89% and 85%, respectively, had undetectable HBV DNA at 96 weeks.

    • 82% of patients with detectable viremia at week 48 on adefovir experienced full viral suppression at 96 weeks after switching to tenofovir.

    • 28 patients added emtricitabine after 72 weeks due to continued viremia, 5 of whom achieved viral suppression by week 96.

    • 30% of patients in the continuous tenofovir arm and 28% in the switch arm experienced HBeAg loss, while 26% and 24%, respectively, experienced HBeAg seroconversion (appearance of anti-HBe antibodies).

    • 6% of patients in both groups experienced HBsAg loss; 4% who received continuous tenofovir and 5% who switched experienced HBsAg seroconversion (considered an indicator of resolved infection).

    • 7% of patients in the continuous tenofovir arm and 10% in the switch arm experienced grade 3-4 laboratory abnormalities.

    • No patients experienced creatinine clearance less than 50 ml/min, but 2 in the adefovir-to-tenofovir switch arm had a confirmed 0.5 mg/dL increase in serum creatinine.

As with Study 102, the investigators concluded that tenofovir produced potent, continuous viral suppression and was well tolerated through week 96 in HBeAg positive patients, and that switching from adefovir to tenofovir led to significant additional viral suppression.

Toronto Western Hospital, University of Toronto, Toronto, Ontario, Canada; Middlemore Hospital, Auckland, New Zealand; Erasmus MC, University Medical Center Rotterdam, Rotterdam, Netherlands; Dreamwork Medical Group, Flushing, NY; Monash University, Melbourne, Victoria, Australia; Center for HIV and Gastroenterology, Dusseldorf, Germany; Hopital Beaujon, University of Paris, Clichy, France; Gilead Sciences, Durham, NC.

11/07/08

References

P Marcellin, M Buti, Z Krastev, and others. Two Year Tenofovir Disoproxil Fumarate (TDF) Treatment and Adefovir Dipivoxil (ADV) Switch Data in HBeAg-Negative Patients with Chronic Hepatitis B (Study 102), Preliminary Analysis. 59th Annual Meeting of the American Association for the Study of Liver Diseases (AASLD 2008). San Francisco. October 31-November 4, 2008. Abstract 146.

E Heathcote, EJ Gane, RA deMan, and others. Two Year Tenofovir Disoproxil Fumarate (TDF) Treatment and Adefovir Dipivoxil (ADV) Switch Data in HBeAg-Positive Patients With Chronic Hepatitis B (Study 103), Preliminary Analysis. 59th Annual Meeting of the American Association for the Study of Liver Diseases (AASLD 2008). San Francisco. October 31-November 4, 2008. Abstract 158.

Other source
Gilead Sciences. Gilead Announces Two-Year Data from Pivotal Phase III Studies Evaluating Viread(R) for Chronic Hepatitis B. Press release. November 1, 2008.
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发表于 2008-12-3 14:00
又是一个好消息,这药的中文名应该叫什么呢,我国会引进吗?谢谢411在最前沿为我们提供最新资讯。
1987年初查感染,1990年再查大三,2007年9月硬化腹水。始服拉米,后加阿德。与病毒共舞,与灵魂同眠。
我的病历:http://www.hbvhbv.com/forum/index.php

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发表于 2008-12-3 14:21
是替诺福韦

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发表于 2008-12-3 20:37
不知道有多贵?据说要一百多一颗
快乐不是因为获得多,而是因为计较少。快乐来自于以感激的心珍惜拥有。...............

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发表于 2008-12-4 14:02
在国外替诺福韦(TDF),目前它比阿德(ADV),恩替(ETV)都便宜,仅比拉米(LAM)贵。

HBV Treatments  Cost Unit:
TDF $18.41 per day
ADV $21.46 per day
ETV $22.73 per day
LAM $9.44 per day

这是以美金计算的,不过提出主要是说明TDF虽然是新通过的但是并不是最贵的除非中国药物届市场想牟利。 价钱应该和中国市场和收入有区别。
God Made Everything That Has Life. Rest Everything Is Made In China

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发表于 2008-12-4 21:43
好呀好呀!比阿德(ADV),恩替(ETV)都便宜我用得起
快乐不是因为获得多,而是因为计较少。快乐来自于以感激的心珍惜拥有。...............

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发表于 2008-12-5 14:12
三毛用得起的,我就只能勉强了。
1987年初查感染,1990年再查大三,2007年9月硬化腹水。始服拉米,后加阿德。与病毒共舞,与灵魂同眠。
我的病历:http://www.hbvhbv.com/forum/index.php

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发表于 2008-12-5 15:23
快乐不是因为获得多,而是因为计较少。快乐来自于以感激的心珍惜拥有。...............
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