Kumar Sushil, Kumari Renu, Pandey Richa
SKA Institution for Research, Education and Development (SKAIRED), 4/11 SarvPriya Vihar, New Delhi, 110016, India,
Protoplasma. 2015 May;252(3):717-53. doi: 10.1007/s00709-014-0697-x. Epub 2014 Oct 17.
New challenges posed by the development of resistance against artemisinin-based combination therapies (ACTs) as well as previous first-line therapies, and the continuing absence of vaccine, have given impetus to research in all areas of malaria control. This review portrays the ongoing progress in several directions of malaria research. The variants of RTS,S and apical membrane antigen 1 (AMA1) are being developed and test adapted as multicomponent and multistage malaria control vaccines, while many other vaccine candidates and methodologies to produce antigens are under experimentation. To track and prevent the spread of artemisinin resistance from Southeast Asia to other parts of the world, rolling circle-enhanced enzyme activity detection (REEAD), a time- and cost-effective malaria diagnosis in field conditions, and a DNA marker associated with artemisinin resistance have become available. Novel mosquito repellents and mosquito trapping and killing techniques much more effective than the prevalent ones are undergoing field testing. Mosquito lines stably infected with their symbiotic wild-type or genetically engineered bacteria that kill sympatric malaria parasites are being constructed and field tested for stopping malaria transmission. A complementary approach being pursued is the addition of ivermectin-like drug molecules to ACTs to cure malaria and kill mosquitoes. Experiments are in progress to eradicate malaria mosquito by making it genetically male sterile. High-throughput screening procedures are being developed and used to discover molecules that possess long in vivo half life and are active against liver and blood stages for the fast cure of malaria symptoms caused by simple or relapsing and drug-sensitive and drug-resistant types of varied malaria parasites, can stop gametocytogenesis and sporogony and could be given in one dose. Target-based antimalarial drug designing has begun. Some of the putative next-generation antimalarials that possess in their scaffold structure several of the desired properties of malaria cure and control are exemplified by OZ439, NITD609, ELQ300 and tafenoquine that are already undergoing clinical trials, and decoquinate, usnic acid, torin-2, ferroquine, WEHI-916, MMV396749 and benzothiophene-type N-myristoyltransferase (NMT) inhibitors, which are candidates for future clinical usage. Among these, NITD609, ELQ300, decoquinate, usnic acid, torin-2 and NMT inhibitors not only cure simple malaria and are prophylactic against simple malaria, but they also cure relapsing malaria.
青蒿素联合疗法(ACTs)以及先前的一线疗法出现耐药性带来了新挑战,且疫苗仍未问世,这推动了疟疾防控各领域的研究。本综述描述了疟疾研究在几个方向上取得的进展。RTS,S和顶端膜抗原1(AMA1)的变体正在开发,并作为多组分、多阶段疟疾防控疫苗进行适应性测试,同时许多其他候选疫苗和生产抗原的方法也在试验中。为追踪并防止青蒿素耐药性从东南亚传播到世界其他地区,滚环增强酶活性检测(REEAD)这一在野外条件下省时且经济高效的疟疾诊断方法以及一种与青蒿素耐药性相关的DNA标记已可供使用。新型驱蚊剂以及比现有方法更有效的诱捕和杀灭蚊子技术正在进行野外测试。稳定感染共生野生型或基因工程改造细菌的蚊子品系正在构建并进行野外测试,这些细菌可杀死同域疟疾寄生虫,从而阻断疟疾传播。正在探索的一种补充方法是在ACTs中添加伊维菌素类药物分子以治疗疟疾并杀灭蚊子。通过使疟疾蚊子基因不育来根除疟疾的实验正在进行。正在开发并使用高通量筛选程序来发现具有长体内半衰期且对肝期和血期有活性的分子,以便快速治愈由单纯型、复发型以及药物敏感型和耐药型多种疟原虫引起的疟疾症状,能够阻止配子体形成和孢子增殖,并且可以一剂给药。基于靶点的抗疟药物设计已经开始。一些具有疟疾治疗和防控所需多种特性的下一代抗疟药物的雏形包括已在进行临床试验的OZ439、NITD609、ELQ300和tafenoquine,以及未来有望用于临床的癸氧喹酯、松萝酸、torin-2、铁喹啉、WEHI-916、MMV396749和苯并噻吩型N-肉豆蔻酰基转移酶(NMT)抑制剂。其中,NITD609、ELQ300、癸氧喹酯、松萝酸、torin-2和NMT抑制剂不仅能治愈单纯型疟疾并预防单纯型疟疾,还能治愈复发型疟疾。
