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Direct-acting antivirals:daclastasvir and asunaprevir [复制链接]

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发表于 2012-1-24 23:26 |只看该作者 |倒序浏览 |打印
本帖最后由 风雨不动 于 2012-4-14 15:41 编辑

Combination of Oral Drugs Suppresses Common Type of Hepatitis C, According to University of Michigan-led Research
       
                From the PharmaLive.com News Archive - Jan. 19, 2012                                                                                                       

Researchers targeted the type of hepatitis C most common in the United States, results reported in New England Journal of Medicine


ANN ARBOR, Mich., January 19, 2012, 2012 /PRNewswire-USNewswire/ -- A new combination of investigational drugs successfully suppressed hepatitis C genotype 1 infection in a high percent of patients who had not responded to previous treatment in a study led by a University of Michigan hepatologist.

The study, published Jan. 19 in the New England Journal of Medicine, focused on hepatitis C genotype 1, which is predominant in the United States and the most difficult to treat. Hepatitis C is a virus that infects the liver and can cause liver cancer and liver cirrhosis. It is transmitted through direct contact with infected blood and blood products.

In this pilot study, patients with hepatitis C genotype 1 infection, who had not responded to previous treatment with PEG-interferon alfa and ribavirin, were given a combination of two investigational direct-acting antiviral agents (daclatasvir and asunaprevir) alone, or were given these two antiviral agents along with PEG-interferon alfa-2a and ribavirin. All the patients saw their hepatitis C viral load drop rapidly, says Anna S. Lok, M.D., professor of Internal Medicine, Division of Gastroenterology at the University of Michigan Medical School and lead author of the study.

All 10 patients given the four drug treatment -- two direct-acting antiviral agents (daclastasvir and asunaprevir) that block the NS3 and NS5A regions of the hepatitis C virus plus PEG-interferon alfa and ribavirin -- had sustained virologic response with undetectable virus at the end of treatment and at 12 weeks after stopping treatment. Four of the 11 patients given the two direct-acting antiviral agents only also achieved sustained virologic response.

A sustained virologic response or SVR means there is no detectable Hepatitis C virus in a patient's blood after treatment is stopped. Achieving sustained virologic response is important, because research has shown that late relapse is rare.

"The two recently approved hepatitis C drugs - telaprevir or boceprevir -- combined with PEG-interferon alfa and ribavirin have limited success in patients who have not responded to previous treatment with PEG-interferon alfa and ribavirin. Because of this high unmet medical need, there is a necessity for new combination regimens that can increase response rates in that population," says Lok, who also is Director of Clinical Hepatology at U-M. "The high rate of sustained virologic response in patients who received the four drug regimen is very exciting. Although only four of 11 patients given the two direct-acting antiviral agents only achieved sustained virologic response, this is the first study to show that sustained virologic response can be achieved without the use of interferon or ribavirin. These data are very encouraging because PEG-interferon alfa and ribavirin are associated with many side effects and many patients with hepatitis C choose not to receive treatment for fear that they cannot tolerate those drugs."

An estimated 170 million people worldwide are infected with hepatitis C, with genotype 1 being the most prevalent genotype. Up to 80 percent of those infected with hepatitis C will become chronically infected. Twenty percent of people with chronic hepatitis C will develop cirrhosis and, of those, up to 25 percent may progress to liver cancer. Although there is no vaccine to prevent hepatitis C, it is a potentially curable disease. In the Phase II clinical trial, Lok, along with a team of researchers including scientists from Bristol-Myers Squibb, studied patients with Hepatitis C genotype 1, who had not responded to prior therapy with PEG-interferon alfa and ribavirin. The study was funded by Bristol-Myers Squibb.

"Overall, these results suggest that further research into combinations of direct-acting antiviral agents, with or without PEG-interferon and ribavirin, should be encouraged," Lok says. "Caution must be exercised in selecting the right combination of direct-acting antiviral agents in studies of interferon-free regimens because in this study, all 7 patients who received only two direct-acting antiviral agents that did not achieve sustained virologic response had emergence of drug resistance variants to both drugs."

In this study there were no serious adverse events on treatment or discontinuations due to adverse events. Diarrhea was the most common adverse event in both groups, but it was mild or moderate in all cases.

Journal citation: N Engl J Med 2012;366:216-24

Funding: Bristol Myers Squibb.

Additional authors: David F. Gardiner, M.D., Kurt Zhu, Ph.D., Dessislava I. Dimitrova, M.D., Timothy Eley, Ph.D., Dennis M. Grasela, Pharm.D., Ph.D., Claudio Pasquinelli, M.D., Ph.D., Fiona McPhee, Ph.D., Tong Guo, Ph.D., Megan Wind-Rotolo, Ph.D., Anna Persson, Ph.D., all of Bristol Myers Squibb; Eric Lawitz, M.D., of Alamo Medical Research, San Antonio, Texas; Claudia Martorell, M.D., of The Research Institute, Springfield, Mass.; Gregory T. Everson, M.D., of the University of Colorado-Denver; Reem Ghalib, M.D., of the Texas Clinical Research Institute; Robert Reindollar, M.D., of the Carolinas Center for Liver Disease; and Vinod Rustgi, M.D., of Metropolitan Research, Fairfax, Va.

About U-M's Division of Gastroenterology: U-M is one of the largest gastroenterology practices in the country and is a leader in the prevention, diagnosis, and treatment of diseases of the gastrointestinal tract and liver. Our 50-plus physicians are experts in the diagnosis and treatment of all diseases of the gastrointestinal system, from simple to complex, including those of the esophagus, stomach, small intestine, colon, rectum, liver, gallbladder, pancreas and biliary tract.

Web site: http://www.med.umich.edu/





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发表于 2012-1-24 23:28 |只看该作者
结合口服药物抑制丙型肝炎常见的类型,据密歇根大学领导的研究

从PharmaLive.com新闻档案 - 2012年1月19日





研究人员针对C型肝炎在美国最常见的类型,在新英格兰医学杂志报道的结果



安阿伯,密歇根州,1月19日,2012年,2012年/新华美通/ - 一个新研究的药物组合成功抑制高%的患者没有回应领导的一个研究以前的治疗丙型肝炎基因型1感染密歇根大学的肝病。

这项研究发表在新英格兰医学杂志“1月19日,C型肝炎基因型1,这是在美国,最难以治疗的主要重点。丙型肝炎是一种病毒感染的肝脏,并可能导致肝癌和肝硬化。它是通过直接接触感染的血液和血液制品传播。

在这项试验研究,丙型肝炎基因型1感染,没有回应与聚乙二醇干扰素和利巴韦林以前治疗,患者分别给予两个研究直接作用的抗病毒药物(daclatasvir和asunaprevir)单独的组合,或给予这两个一起聚乙二醇干扰素α- 2a和利巴韦林的抗病毒药物。所有患者看到他们的丙型肝炎病毒载量下降迅速,在密歇根大学医学院的大学和研究的主要作者,胃肠病科,内科教授安娜S.乐博士说。

两个直接作用的抗病毒药物(daclastasvir和asunaprevir)块C型肝炎病毒加聚乙二醇干扰素和利巴韦林的NS3和NS5A的地区 -  - 所有10给出的四个药物治疗的患者检测不到病毒持续病毒学应答在停止治疗后12周的治疗和结束。对11例患者中有四个给定的两个直接作用抗病毒药物,也取得了持续病毒学应答。

一个持续病毒学应答或SVR是指有没有检测到C型肝炎病人的血液中的病毒治疗后停止。实现持续病毒学应答是重要的,因为有研究表明,晚期复发是罕见的。

“最近批准的两个C型肝炎的药物 - telaprevir或boceprevir - 聚乙二醇干扰素和利巴韦林联合有限的成功,正因为如此高的满足医疗需求,在没有回应与聚乙二醇干扰素和利巴韦林以前治疗的患者。有一个新的组合方案,可以提高反应率,人口的必要性,说:“乐,谁也就是在澳主任临床肝胆病。他说:“病人谁收到的药物治疗是非常令人兴奋的持续病毒学应答率很高,虽然只有四个11例患者的两个直接作用只实现了持续病毒学应答的抗病毒药物,这是首次有研究显示,持续病毒学响应可以是实现不使用干扰素或利巴韦林,这些数据是非常令人鼓舞的,因为聚乙二醇干扰素阿尔法和利巴韦林是许多方的影响和丙型肝炎许多患者选择不向接收担心,他们可以不容忍这些药物治疗相关的。 “

全世界估计有1.7亿人感染丙型肝炎,基因1型是最流行的基因型。与C型肝炎感染者的80%将成为慢性感染。 20%的慢性丙型肝炎的人会发展为肝硬化,这些,可能高达25%进展到肝癌。虽然目前还没有疫苗来预防丙型肝炎,这是一个潜在的可治愈的疾病。在II期临床试验,乐,包括百时美施贵宝公司的科学家们的研究团队,研究与丙型肝炎基因型1,没有回应之前的治疗与聚乙二醇干扰素和利巴韦林患者。资助这项研究是由百时美施贵宝公司。

“总的来说,这些结果表明成直接作用的抗病毒药物的组合,进一步研究PEG -干扰素和利巴韦林有或没有,应鼓励,”乐说。 “小心,必须选择正确的组合直接作用的抗病毒药物干扰素治疗的研究行使,因为在这项研究中,所有7名患者只有两个直接作用的抗病毒药物,没有达到持续病毒学应答的出现这两种药物的耐药性变异。“

在这项研究中,有没有治疗或因不良反应停药的严重不良事件。腹泻是这两个群体中最常见的不良事件,但它是在所有情况下轻度或中度。
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