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Alternatives to currently used antimalarial drugs: in search of a magic bullet

机译:当前使用的抗疟药物的替代品:寻找神奇的子弹

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Malaria is a major cause of morbidity and mortality in many African countries and parts of Asia and South America. Novel approaches to combating the disease have emerged in recent years and several drug candidates are now being tested clinically. However, it is long before these novel drugs can hit the market, especially due to a scarcity of safety and efficacy data.To reduce the malaria burden, the Medicines for Malaria Venture (MMV) was established in 1999 to develop novel medicines through industry and academic partners’ collaboration. However, no reviews were focused following various preclinical and clinical studies published since the MMV initiation (2000) to till date.We identify promising approaches in the global portfolio of antimalarial medicines, and highlight challenges and patient specific concerns of these novel molecules. We discuss different clinical studies focusing on the evaluation of novel drugs against malaria in different human trials over the past five years.The drugs KAE609 and DDD107498 are still being evaluated in Phase I trials and preclinical developmental studies. Both the safety and efficacy of novel compounds such as KAF156 and DSM265 need to be assessed further, especially for use in pregnant women. Synthetic non-artemisinin ozonides such as OZ277 raised concerns in terms of its insufficient efficacy against high parasitic loads. Aminoquinoline-based scaffolds such as ferroquine are promising but should be combined with good partner drugs for enhanced efficacy. AQ-13 induced electrocardiac events, which led to prolonged QTc intervals. Tafenoquine, the only new anti-relapse scaffold for patients with a glucose-6-phosphate dehydrogenase deficiency, has raised significant concerns due to its hemolytic activity. Other compounds, including methylene blue (potential transmission blocker) and fosmidomycin (DXP reductoisomerase inhibitor), are available but cannot be used in children.At this stage, we are unable to identify a single magic bullet against malaria. Future studies should focus on effective single-dose molecules that can act against all stages of malaria in order to prevent transmission. Newer medicines have also raised concerns in terms of efficacy and safety. Overall, more evidence is needed to effectively reduce the current malaria burden. Treatment strategies that target the blood stage with transmission-blocking properties are needed to prevent future drug resistance.Electronic supplementary materialThe online version of this article (doi:10.1186/s40249-016-0196-8) contains supplementary material, which is available to authorized users.
机译:在许多非洲国家以及亚洲和南美的部分地区,疟疾是发病和死亡的主要原因。近年来,已经出现了抗击这种疾病的新方法,目前正在对几种候选药物进行临床测试。但是,由于缺乏安全性和有效性数据,这些新药上市不久,为了减少疟疾负担,为了减少疟疾负担,成立于1999年的``Malaria for Malaria Venture(MMV)''通过行业和行业来开发新药。学术伙伴的合作。然而,自MMV发起(2000年)至今至今,尚未进行过各种临床前和临床研究的综述。我们在全球抗疟药物组合中确定了有希望的方法,并强调了这些新型分子的挑战和患者特定的关注。在过去的五年中,我们讨论了不同的临床研究,重点是在不同的人类试验中评估抗疟疾的新药.I期试验和临床前发展研究中仍在评估KAE609和DDD107498药物。新型化合物(例如KAF156和DSM265)的安全性和功效都需要进一步评估,尤其是用于孕妇中。合成的非青蒿素臭氧化物(如OZ277)因其对高寄生虫负载的功效不足而引起关注。基于氨基喹啉的支架(例如铁喹)是有前途的,但应与良好的伴侣药物联合使用以提高疗效。 AQ-13诱发了心电事件,导致QTc间隔延长。 Tafenoquine是唯一一种针对6磷酸葡萄糖脱氢酶缺乏症患者的新型抗复发支架,由于其溶血活性而引起了广泛关注。其他化合物,包括亚甲蓝(潜在的传播阻断剂)和fosmidomycin(DXP还原异构酶抑制剂)也可以使用,但不能在儿童中使用。在此阶段,我们无法确定出抗击疟疾的唯一灵丹妙药。未来的研究应该集中在有效的单剂量分子上,这些分子可以对抗疟疾的所有阶段,以防止传播。新型药物在功效和安全性方面也引起了人们的关注。总体而言,需要更多的证据来有效减轻当前的疟疾负担。为了防止将来出现耐药性,需要有针对性地针对具有输血阻滞特性的血液阶段的治疗策略。电子补充材料本文的在线版本(doi:10.1186 / s40249-016-0196-8)包含补充材料,可通过授权获得用户。

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