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New therapies for the treatment of heart failure: a summary of recent accomplishments

机译:心力衰竭的新疗法:近期成就的总结

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摘要

Despite continuous efforts to prevent cardiovascular diseases (CVDs), heart failure prevails as the number one cause of death in developed countries. To properly treat CVDs, scientists had to take a closer look at the factors that contribute to their pathogenesis and either modernize current pharmaceuticals or develop brand new treatments. Enhancement of current drugs, such as tolvaptan and omecamtiv mecarbil, sheds new light on already-known therapies. Tolvaptan, a vasopressin antagonist, could be adopted in heart failure therapy as it reduces pre- and afterload by decreasing systolic blood pressure and blood volume. Omecamtiv mecarbil, which is a myosin binding peptide, could aid cardiac contractility. The next generation vasodilators, serelaxin and ularitide, are based on naturally occurring peptides and they reduce peripheral vascular resistance and increase the cardiac index. In combination with their anti-inflammatory properties, they could turn out to be extremely potent drugs for heart failure treatment. Cardiotrophin has exceeded many researchers’ expectations, as evidence suggests that it could cause sarcomere hypertrophy without excessive proliferation of connective tissue. Rapid progress in gene therapy has caused it to finally be considered as one of the viable options for the treatment of CVDs. This novel therapeutic approach could restore stable heart function either by restoring depleted membrane proteins or by balancing the intracellular calcium concentration. Although it has been set back by problems concerning its long-term effects, it is still highly likely to succeed.
机译:尽管人们一直在努力预防心血管疾病(CVD),但在发达国家,心力衰竭仍然是导致死亡的第一大原因。为了正确治疗CVD,科学家们必须仔细研究导致其发病的因素,或者使当前的药物现代化或开发全新的治疗方法。当前药物的增强,例如托伐普坦和omecamtiv mecarbil,为已知的治疗方法提供了新的思路。血管加压素拮抗剂托伐普坦可用于心力衰竭治疗,因为它通过降低收缩压和血容量来减少前后负荷。 Omecamtiv mecarbil是一种肌球蛋白结合肽,可以帮助心脏收缩。下一代血管舒张药serelaxin和oliitide是基于天然存在的肽,它们可降低外周血管阻力并增加心脏指数。结合其抗炎特性,它们可能成为治疗心力衰竭的极有效药物。心肌营养素超出了许多研究人员的预期,因为有证据表明,它可以在不导致结缔组织过度增殖的情况下引起肌小节肥大。基因治疗的快速发展已使其最终被认为是治疗CVD的可行选择之一。这种新的治疗方法可以通过恢复耗尽的膜蛋白或平衡细胞内钙浓度来恢复稳定的心脏功能。尽管由于长期影响问题而受到挫折,但成功的可能性仍然很高。

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