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malaria |
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malaria![]() The life cycle of the malaria parasite is split between mosquito and human hosts. The parasites are injected into the human bloodstream by an infected Anopheles mosquito and carried to the liver. Here they attack red blood cells, and multiply asexually. The infected blood cells burst, producing spores, or merozoites, which reinfect the bloodstream. After several generations, the parasite develops into a sexual form. If the human host is bitten at this stage, the sexual form of the parasite is sucked into the mosquito's stomach. Here fertilization takes place, the zygotes formed reproduce asexually and migrate to the salivary glands ready to be injected into another human host, completing the cycle. Infectious parasitic disease of the tropics transmitted by mosquitoes, marked by periodic fever and an enlarged spleen. When a female mosquito of the Anopheles genus bites a human who has malaria, it takes in with the human blood one of four malaria protozoa of the genus Plasmodium. This matures within the insect and is then transferred when the mosquito bites a new victim. As of 2007, the World Health Organization (WHO) estimated that malaria affects more than 500 million people each year, and more than 1 million children die of the disease, most of them in sub-Saharan Africa. In 1998, the Roll Back Malaria partnership was set up as a multi-agency programme for research and control of the disease. The agencies involved include the WHO, the World Bank, the United Nations Children's Fund, and the United Nations Development Programme. The Roll Back Malaria campaign aims to halve deaths from malaria by 2010. It has already saved many lives with measures such as the distribution of bed nets treated with long-lasting insecticides.
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3) The use of artemisinin-containing combinations increased on plantation 1 from 3% of all treatment courses in 2001 to 9% in 2002, whereas artemisinin combinations represented <2% of all anti-malarial drugs purchased at plantation 2 in 2002. Comment: If protease inhibitors that were never designed or optimized for malaria can be active, it should be possible to produce much better anti-malarial drugs in this class. The Africa Malaria Report also states that in most countries chloroquine--the most commonly available anti-malarial drug--has lost its clinical effectiveness. |
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