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意见:改进FDA评估,而不危及安全性和功效 [复制链接]

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发表于 2017-2-4 07:33 |只看该作者 |倒序浏览 |打印
                        Opinion: Improving FDA Evaluations Without Jeopardizing Safety and Efficacy        

What can be done to lower development costs and drug prices?

      

                                By John D. Loike and Jennifer Miller  | February 1, 2017                       

                                       
                                       
                                                                                                                   THE SCIENTIST STAFF; DATA FROM FDA AND CMSDrug approvals by the US Food and Drug Administration (FDA) dropped dramatically in 2016—down by 57 percent over the year before. While some of this decline was due to a record number of approvals in 2015, only 22 novel drugs were approved last year—fewer than in each of the previous five years. Striving to make returns on their investments—to gain FDA approval for a novel therapy averages around $2.6 billion and 10 years—pharmaceutical companies sometimes hike drug prices to offset low productivity. Prescription drugs are the fastest growing health-care cost, with costs increasing by 9 percent from 2014 to 2015, according to the latest report from the Centers for Medicare & Medicaid Services (CMS).
        In addition to translating to high medication prices for patients, the exorbitant cost of drug development can result in many other unwanted outcomes. First, it can financially strain small biotechs to the point that the companies can’t fund their own Phase 2 or 3 clinical trials and are forced to go to pharmaceutical giants for financial help. High costs can also deter companies, big and small, from innovating and researching therapeutics for small or low-income patient populations.
        Although the FDA has made efforts to reduce drug development costs and offers incentives for pharma to develop less-profitable drugs, such as those for orphan diseases, many in the industry believe these steps have not made a significant financial impact. Among other candidates, President Donald Trump is considering appointing Jim O’Neill as the new head of the FDA. As managing director of Peter Thiel’s Mithril Capital, O’Neill has publicly proposed eliminating the FDA’s requirement for Phase 2 and 3 trials, in an effort to lower drug development costs.
        Among other things, O’Neill favors “progressive approval” of drugs, similar to the methods employed by Japan, where medicines can be approved following proof of safety. Once a drug is in use, companies in Japan move to a Phase 4, post-market assessment to monitor their patients and regularly disclose efficacy data.
        We argue that eliminating Phase 2 and 3 clinical trials would be unwise for a number of reasons. Chief among them, testing drugs in fewer than 100 healthy volunteers—as is done in a typical Phase 1 trial—is not sufficient for identifying health risks in a target patient population. Moreover, Phase 2 trials, for conditions other than oncology, are not that expensive because they involve a limited number of patients. The costs of Phase 3 randomized control trials, in contrast, are high, in part because they require the recruitment of hundreds or thousands of patients, often across multiple states and countries, and require a lot of time in assessing a drug’s efficacy.
        The FDA could explore using adaptive licensing, whereby a drug is provisionally approved based on Phase 1 and 2 data for a defined short period of time. During the provisional approval period, efficacy data are collected directly from clinical use, accruing real-world data capable of overcoming the generalizability limitations of traditional trials. After a year or two, the drug is either fully approved or loses its marketing license.
        In lieu of eliminating late-stage trials, there may be other steps that the government can take to address the current regulatory challenges. First, pragmatic and adaptive trial designs could help reduce numbers of research subjects needed to test a drug and increase the likelihood trial data are generalizable to the patient population that will use a drug following FDA approval. Currently, many trials are conducted on highly specialized patient populations—for example, healthier and younger than typical patients—causing concerns about the quality of our medical evidence at the time a new drug is introduced to market.
        Second, the FDA could explore reducing the use of animal models in preclinical research. Currently, the FDA requires extensive and sometimes expensive animal trials before entering human studies. While such experiments often detect unwanted side effects, many animal models of diseases are poorly translated into successful human trials. As human organoid technology continues to be developed and improved, these mini human organs may prove to be a better and cheaper model system to test the effects of drugs instead of using expensive and often inaccurate animal models.
        Third, academic institutions and pharmaceutical companies should be required to publish the results of all clinical trials within one year of a trial’s primary completion date and to make their patient-level data available to all researchers and physicians. Currently, only 57 percent of trials for new drugs are registered and only 65 percent have publicly disclosed results. Fostering more open science is likely to save money and spur innovation, as researchers learn from the lessons of others and avoid duplicating costly trials.
        Fourth, greater adoption and integration of electronic health records with research protocols could help identify new uses for existing drugs, by enabling researchers to collate data on off-label use, for example, and expedite approvals for these indications. The savings that come with repurposing existing drugs can be dramatic: thalidomide, originally approved in Europe in the 1950s as a sedative and in the U.S. in 1998 to treat leprosy, gained FDA approval for the treatment of multiple myeloma in 2006 for less than $80 million.
        Last, Congress could explore creating or partnering with an offshoot-pricing agency for new drugs, separate from the FDA and similar to the U.K.’s National Institute for Health and Care Excellence. This agency could monitor drug prices and help assess their overall value, comparative effectiveness, and cost-effectiveness. The Institute for Clinical and Economic Review may be a potential partner. The organization is creating value-based price benchmarks based on the benefits a new drug brings to patients. Last year, PhRMA, the US pharmaceutical trade association, developed principles to guide value assessment frameworks.
        There is no doubt that, in general, the FDA has been successful in providing a reliable method for companies to bring new drugs to market. As expensive biotechnology begins to introduce new drug therapies, the agency should consider innovative ways to lower the costs without jeopardizing the safety of patients.
        John D. Loike is a faculty member at Columbia University College of Physicians and Surgeons. Jennifer Miller is a faculty member at New York University School of Medicine and the President of Bioethics International.
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                                                                        Tags                                regulation,                                 food and drug administration,                                 FDA,                                 drug testing,                                 drug pricing,                                 drug development,                                 drug approval,                                 clinical trials and                                 clinical trial design                       

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发表于 2017-2-4 07:35 |只看该作者
本帖最后由 StephenW 于 2017-2-4 07:37 编辑

意见:改进FDA评估,而不危及安全性和功效

可以做些什么来降低开发成本和药物价格?

作者:John D. Loike和Jennifer Miller | 2017年2月1日

科学工作人员;来自FDA和CMS的数据美国食品和药物管理局(FDA)的批准在2016年大幅下降,与前一年相比下降了57%。虽然一些下降是由于2015年批准的记录数量,去年只批准了22种新药 - 比前五年每年少。努力为他们的投资获得回报 - 获得FDA批准的新型治疗平均约26亿美元和10年 - 制药公司有时会提高药品价格以抵消低生产力。根据医疗保险和医疗补助服务中心(CMS)的最新报告,处方药是增长最快的医疗保健成本,从2014年到2015年,成本增加了9%。

除了将患者转化为高药物价格之外,药物开发的高昂成本还可能导致许多其他不必要的结果。首先,它可能对小型生物技术造成经济压力,使公司不能为自己的第二阶段或第三阶段临床试验提供资金,并被迫向制药巨头提供财务帮助。高成本还可以阻止大,小公司从小型或低收入患者群体的创新和研究治疗方法。

虽然FDA已经努力降低药物开发成本,并且鼓励药品开发低利润的药物,例如孤儿疾病药物,但许多业内人士认为这些步骤没有产生重大的财务影响。在其他候选人中,唐纳德·特朗普总统正在考虑任命吉姆·奥尼尔作为FDA的新主管。作为Peter Thiel的Mithril Capital的董事总经理,O'Neill公开提议取消FDA对第2阶段和第3阶段试验的要求,以降低药物开发成本。

除了其他事情,O'Neill赞成“逐步批准”药物,类似于日本采用的方法,其中药物可以在安全证明后批准。一旦使用药物,日本公司将进入第四阶段,进行上市后评估以监测其患者,并定期公布疗效数据。

我们认为,消除阶段2和3的临床试验是不明智的,原因有很多。其中主要是在少于100名健康志愿者中进行药物测试,如在典型的1期试验中所做的那样,不足以识别目标患者群体中的健康风险。此外,除了肿瘤学以外的其他疾病的2期试验不是那么昂贵,因为它们涉及有限数量的患者。相比之下,3期随机对照试验的成本较高,部分原因是它们需要招募数百或数千名患者,通常跨越多个州和国家,并且需要大量时间评估药物的疗效。

FDA可以探索使用自适应许可,从而根据第1阶段和第2阶段数据,在确定的短时间内暂时批准药物。在临时批准期间,效能数据直接从临床使用收集,累积真实数据,能够克服传统试验的一般化限制。一两年后,该药物或者完全批准或者失去营销许可证。

为了代替消除后期试验,政府可能采取其他措施来应对当前的监管挑战。首先,务实和适应性试验设计可以帮助减少测试药物所需的研究对象的数量,并增加可能的试验数据可推广给在FDA批准后使用药物的患者群体。目前,许多试验是针对高度专业化的患者群体进行的,例如,比典型患者更健康和更​​年轻,引起对新药物引入市场时我们的医学证据的质量的担忧。

第二,FDA可以探讨在临床前研究中减少动物模型的使用。目前,FDA在进入人类研究之前需要大量且有时是昂贵的动物试验。虽然这些实验经常检测不需要的副作用,但许多疾病的动物模型很少被翻译成成功的人体试验。随着人体类器官技术的继续发展和改进,这些微型人体器官可能被证明是一个更好和更便宜的模型系统,以测试药物的效果,而不是使用昂贵的,通常不准确的动物模型。

第三,学术机构和制药公司应该在试验的主要完成日期的一年内公布所有临床试验的结果,并向所有研究人员和医生提供他们的患者水平数据。目前,只有57%的新药物试验注册,只有65%的公开披露结果。培养更开放的科学可能节省资金并刺激创新,研究人员从他人的经验教训中学习,避免重复昂贵的试验。

第四,更多地采用和整合电子健康记录与研究协议可以帮助确定现有药物的新用途,例如,使研究人员能够整理关于标签外使用的数据,并加快对这些适应症的批准。重新利用现有药物可节省大量的成本:沙利度胺,最初在欧洲于1950年代作为镇静剂批准,并于1998年在美国治疗麻风病,在2006年获得FDA批准用于治疗多发性骨髓瘤,价格低于80美元百万。

最后,国会可以探索与新药分开的定价机构建立或合作,与FDA分开,类似于英国国家卫生和关怀卓越研究所。该机构可以监测药物价格并帮助评估其总体价值。临床和经济评价研究可能是潜在的合作伙伴。该组织正在根据新药给患者带来的好处创造基于价值的价格基准。去年,美国药物贸易协会PhRMA制定了指导价值评估框架的原则。

FDA已经成功地为公司提供一种可靠的方法将新药物推向市场。由于昂贵的生物技术开始引入新的药物治疗,该机构应考虑创新的方法降低成本,而不危及患者的安全。

John D. Loike是哥伦比亚大学内科医生和外科学院的教师。 Jennifer Miller是纽约大学医学院的教授和生物伦理国际的总裁。

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3
发表于 2017-2-4 10:03 |只看该作者
”除了肿瘤学...”那肿瘤病人怎么办?
日本是怎么处理的呢?
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发表于 2017-2-4 11:01 |只看该作者
回复 MP4 的帖子

我不是专家, 我同意作者的建议:
1.减少动物研究;
2.修改3期临床试验.

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发表于 2017-2-21 20:14 |只看该作者
欢迎收看肝胆卫士大型生活服务类节目《乙肝勿扰》,我们的目标是:普度众友,收获幸福。
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发表于 2017-2-21 20:51 |只看该作者
欢迎收看肝胆卫士大型生活服务类节目《乙肝勿扰》,我们的目标是:普度众友,收获幸福。
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