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开发心力衰竭的新疗法:聚焦于心脏。

Developing New Treatments for Heart Failure: Focus on the Heart.

作者信息

Gheorghiade Mihai, Larson Christopher J, Shah Sanjiv J, Greene Stephen J, Cleland John G F, Colucci Wilson S, Dunnmon Preston, Epstein Stephen E, Kim Raymond J, Parsey Ramin V, Stockbridge Norman, Carr James, Dinh Wilfried, Krahn Thomas, Kramer Frank, Wahlander Karin, Deckelbaum Lawrence I, Crandall David, Okada Shunichiro, Senni Michele, Sikora Sergey, Sabbah Hani N, Butler Javed

机构信息

From the Center for Cardiovascular Innovation (M.G.) and Division of Cardiology (S.J.S.), Northwestern Feinberg School of Medicine, Northwestern University, Chicago, IL; Cardiovascular & Metabolic Diseases Drug Discovery Unit, Takeda Pharmaceuticals, Chicago, IL (C.J.L., S.O.); Division of Cardiology, Duke University Medical Center, Durham, NC (S.J.G., R.J.K.); National Heart & Lung Institute, Imperial College, London, United Kingdom (J.G.F.C.); Cardiovascular Medicine Section, Boston University School of Medicine and Boston Medical Center, MA (W.S.C.); Division of Cardiovascular and Renal Products, the United States Food and Drug Administration, Silver Spring, MD (P.D., N.S.); MedStar Heart and Vascular Institute, MedStar Washington Hospital Center, Washington DC (S.E.E.); Psychiatry Department (R.V.P.) and Cardiology Division (J.B.), Stony Brook University, NY; Stealth Bio Therapeutics, Philadelphia, PA (J.C.); Global Drug Discovery, Bayer HealthCare AG, Wuppertal, Germany (W.D., T.K., F.K.); Department of Cardiology, Witten University, Witten, Germany (W.D.); Astra Zeneca Research and Development, Gothenburg, Sweden (K.W.); CSL Behring, Philadelphia, PA (L.I.D.); Sunovion Pharmaceuticals Inc, Marlborough, MA (D.C.); Dipartimento Cardiovascolare, Azienda Ospedaliera Papa Giovannni XXIII, Bergamo, Italy (M.S.); Cardiocell Inc, San Diego, CA (S.S.); and Cardiology Division, Henry Ford Hospital, Detroit, MI (H.N.S.).

出版信息

Circ Heart Fail. 2016 May;9(5). doi: 10.1161/CIRCHEARTFAILURE.115.002727.

Abstract

Compared with heart failure (HF) care 20 to 30 years ago, there has been tremendous advancement in therapy for ambulatory HF with reduced ejection fraction with the use of agents that block maladaptive neurohormonal pathways. However, during the past decade, with few notable exceptions, the frequency of successful drug development programs has fallen as most novel therapies have failed to offer incremental benefit or raised safety concerns (ie, hypotension). Moreover, no therapy has been approved specifically for HF with preserved ejection fraction or for worsening chronic HF (including acutely decompensated HF). Across the spectrum of HF, preliminary results from many phase II trials have been promising but are frequently followed by unsuccessful phase III studies, highlighting a disconnect in the translational process between basic science discovery, early drug development, and definitive clinical testing in pivotal trials. A major unmet need in HF drug development is the ability to identify homogeneous subsets of patients whose underlying disease is driven by a specific mechanism that can be targeted using a new therapeutic agent. Drug development strategies should increasingly consider therapies that facilitate reverse remodeling by directly targeting the heart itself rather than strictly focusing on agents that unload the heart or target systemic neurohormones. Advancements in cardiac imaging may allow for more focused and direct assessment of drug effects on the heart early in the drug development process. To better understand and address the array of challenges facing current HF drug development, so that future efforts may have a better chance for success, the Food and Drug Administration facilitated a meeting on February 17, 2015, which was attended by clinicians, researchers, regulators, and industry representatives. The following discussion summarizes the key takeaway dialogue from this meeting.

摘要

与20到30年前的心力衰竭(HF)治疗相比,通过使用阻断适应不良神经激素途径的药物,射血分数降低的门诊HF治疗取得了巨大进展。然而,在过去十年中,除了少数显著的例外情况,成功的药物研发项目频率下降,因为大多数新疗法未能带来额外益处或引发安全问题(如低血压)。此外,尚无专门针对射血分数保留的HF或慢性HF恶化(包括急性失代偿性HF)的疗法获批。在整个HF领域,许多II期试验的初步结果很有前景,但随后的III期研究却常常失败,这凸显了基础科学发现、早期药物研发与关键试验中的确定性临床试验之间转化过程的脱节。HF药物研发中一个尚未满足的主要需求是,能够识别出潜在疾病由特定机制驱动的患者同质亚组,而这种机制可以用新的治疗药物来靶向。药物研发策略应越来越多地考虑通过直接靶向心脏本身来促进逆向重塑的疗法,而不是严格专注于减轻心脏负荷或靶向全身神经激素的药物。心脏成像技术的进步可能使在药物研发过程早期更有针对性和直接地评估药物对心脏的作用成为可能。为了更好地理解和应对当前HF药物研发面临的一系列挑战,以便未来的努力有更大的成功机会,美国食品药品监督管理局于2015年2月17日促成了一次会议,临床医生、研究人员、监管人员和行业代表参加了此次会议。以下讨论总结了这次会议的关键要点对话。

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