Plasmo die uhmm? False-Ipa-room?
September 8, 2005 | 12:00am
When I was young, I should have answered the popular adult question, "Who would you like to be when you grow up?" with "I would want to be like the Plasmodium, sir." If P. falciparum were human, it would have obtained its Ph.D. and post-doctorate in two years time or less because of its intelligent niche and technique for propagation. P. falciparum completes its schizogony (asexual cycle) in the red blood cells of vertebrates (that include us) and sporogony (sexual cycle) in its carrier, the anopheline mosquito. Immediately after the Anopheles bites, the Plasmodium parasite enters our body and invades the immune system by sequestering the liver until it is mature for the next cycle. After pre-maturation, the parasite (now called a merozoite) invades the red blood cells, causing structural deformation and re-orientation of the cell membrane, and sequesters there until it matures into male and female gametocytes, upon which the red blood cells will rupture, releasing the gametocytes in the blood stream waiting to be ingested as blood meal by another Anopheles mosquito. What makes this parasite so clever is its ability to fool or deceive our immune system (that releases antibodies specific for an antigen due to an invasion of any foreign material). Not only is the infection "strain-specific," it is also "variant-specific." A single strain can produce different variants of antigenic proteins. In the erythrocytic stage, the merozoites infect the red blood cells and different parasitic proteins are formed in the RBC membrane to aid in survival, serve as a marker and assist other adhesion processes. One important protein antigen is the Plasmodium falciparum Erythrocytic Membrane Protein1 (PfEMP1). This protein is highly polymorphic and has evolved to have 60 copies of its gene in each genome, therefore enabling it to change! However, even if there is a change in DNA sequence, the activity or function of this PfEMP1 protein is still conserved! One example is its ability to bind to the human endothelium through its Cysteine Rich Interdomain Region1. This primitive property enables the PfEMP1 to anchor itself to endothelial CD36 and avoid spleen-dependent killing.
And yes, the acute, specific and polymorphic cleverness of this parasite is the primary reason why scientific researchers are having difficulty in developing a vaccine. To make things more complicated, each of the different maturity stages of the parasite is marked by different proteins. Examples of these proteins are the circumsporosite for the hepatic sporocyte stage, the PfEMP protein for the erythrocytic stage, and the Pfs25 protein for the oogenic stage.
Although the possibility of an anti-malarial vaccine seems difficult to see due to the nature of the parasite, there are clever ways to overcome the barriers imposed by the P. falciparum. How does an amateur such as myself propose to meet each challenge? Let us see. (To be concluded)
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