Team:EPF Lausanne
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We have discussed several ways of blocking the Plasmodium in the gut of the mosquito. We plan to test the following two approaches: | We have discussed several ways of blocking the Plasmodium in the gut of the mosquito. We plan to test the following two approaches: | ||
* Asaia produces an immunotoxin consisting of an antibody, which will bind to a specific site on the plasmodium and a toxin (a porin, which will perforate the cellular membrane of the parasite). | * Asaia produces an immunotoxin consisting of an antibody, which will bind to a specific site on the plasmodium and a toxin (a porin, which will perforate the cellular membrane of the parasite). | ||
+ | * p25 p28 are ookinete (a specific form of the plasmodium) surface proteins. It has been shown [2] that if these proteins are missing the formation of ookinetes and the transformation of plasmodium to the next stage are inhibited. We therefore want to engineer Asaia to inhibit these proteins. <br> | ||
+ | The next step is to achieve a release of the toxin or the receptors into the gut of the mosquito. This could be done by lysis of the cells or ideally by secretion. | ||
+ | As a last and very challenging step we consider the option of a blood sensor, which triggers lysis or secretion. This would greatly increase the probability that there is a sufficient amount of immunotoxin to stop the plasmodium from being able to travel to the salivary gland and hence being transmitted to the next victim. | ||
Revision as of 13:37, 15 July 2010
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The next step is to achieve a release of the toxin or the receptors into the gut of the mosquito. This could be done by lysis of the cells or ideally by secretion. As a last and very challenging step we consider the option of a blood sensor, which triggers lysis or secretion. This would greatly increase the probability that there is a sufficient amount of immunotoxin to stop the plasmodium from being able to travel to the salivary gland and hence being transmitted to the next victim.
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