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首页> 外文期刊>Journal of vector borne diseases >Interrupting malaria transmission by genetic manipulation of anopheline mosquitoes.
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Interrupting malaria transmission by genetic manipulation of anopheline mosquitoes.

机译:通过对按蚊的遗传操纵来中断疟疾的传播。

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摘要

Malaria ranks among the deadliest infectious diseases that kills more than one million persons every year. The mosquito is an obligatory vector for malaria transmission. In the mosquito, Plasmodium undergoes a complex series of developmental events that includes transformation into several distinct morphological forms and the crossing of two different epithelia--midgut and salivary gland. Circumstantial evidence suggests that crossing of the epithelia requires specific interactions between Plasmodium and epithelial surface molecules. By use of a phage display library we have identified a small peptide-SM1--that binds to the surfaces of the mosquito midgut and salivary glands. Transgenic Anopheles stephensi mosquitoes expressing a SM1 tetramer from a blood-inducible and gut-specific promoter are substantially impaired in their ability to sustain parasite development and transmission. A second effector gene, phospholipase A2, also impairs parasite transmission in transgenic mosquitoes. These findings have important implications for the development of new strategies for malaria control.
机译:疟疾是最致命的传染病之一,每年造成超过100万人死亡。蚊子是疟疾传播的强制媒介。在蚊子中,疟原虫经历了一系列复杂的发育事件,包括转化成几种不同的形态学形式以及跨越两个不同的上皮细胞-中肠和唾液腺。间接证据表明,上皮细胞的杂交需要疟原虫和上皮表面分子之间的特定相互作用。通过使用噬菌体展示文库,我们已经鉴定出一种小肽SM1,该肽与蚊子中肠和唾液腺的表面结合。从血液诱导型和肠道特异性启动子表达SM1四聚体的转基因斯蒂芬按蚊蚊子维持寄生虫发育和传播的能力大大受损。第二个效应基因,磷脂酶A2,也损害了转基因蚊子中的寄生虫传播。这些发现对制定新的疟疾控制策略具有重要意义。

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