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Drug Targets for Heart Failure with Preserved Ejection Fraction: A Mechanistic Approach and Review of Contemporary Clinical Trials

机译:保存射血分数的心力衰竭药物靶点:当代临床试验的机制方法和综述

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摘要

Heart failure with preserved ejection fraction (HFpEF) accounts for over half of prevalent heart failure (HF) worldwide, and prognosis after hospitalization for HFpEF remains poor. Due, at least in part, to the heterogeneous nature of HFpEF, drug development has proved immensely challenging. Currently, there are no universally accepted therapies that alter the clinical course of HFpEF. Despite these challenges, important mechanistic understandings of the disease have revealed that the pathophysiology of HFpEF is distinct from that of HF with reduced ejection fraction and have also highlighted potential new therapeutic targets for HFpEF. Of note, HFpEF is a systemic syndrome affecting multiple organ systems. Depending on the organ systems involved, certain novel therapies offer promise in reducing the morbidity of the HFpEF syndrome. In this review, we aim to discuss novel pharmacotherapies for HFpEF based on its unique pathophysiology and identify key research strategies to further elucidate mechanistic pathways to develop novel therapeutics in the future.
机译:与保存的射血分数(HFPEF)的心力衰竭占全球普遍存气(HF)的一半超过一半,并且HFPEF住院后的预后仍然很差。由于至少部分地,对​​于HFPEF的异质性质,药物开发已经证明了非常挑战性。目前,没有普遍接受的疗法改变了HFPEF的临床过程。尽管存在这些挑战,但对疾病的重要机制理解揭示了HFPEF的病理生理学与HF的病理生理学不同,射出分数降低,并且还强调了HFPEF的潜在的新治疗靶标。值得注意的是,HFPEF是影响多器官系统的全身综合症。根据所涉及的器官系统,某些新颖的疗法提供了降低HFPEF综合征的发病率的承诺。在这篇综述中,我们的目的是基于其独特的病理生理学讨论HFPEF的新型药物治疗,并确定了重点研究策略,以进一步阐明机械途径,在未来开发新的治疗性。

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