Parasite-host interaction in malaria: genetic clues and copy number variation
AUTOR(ES)
Faik, Imad
FONTE
BioMed Central
RESUMO
In humans, infections contribute highly to mortality and morbidity rates worldwide. Malaria tropica is one of the major infectious diseases globally and is caused by the protozoan parasite Plasmodium falciparum. Plasmodia have accompanied human beings since the emergence of humankind. Due to its pathogenicity, malaria is a powerful selective force on the human genome. Genetic epidemiology approaches such as family and twin studies, candidate gene studies, and disease-association studies have identified a number of genes that mediate relative protection against the severest forms of the disease. New molecular approaches, including genome-wide association studies, have recently been performed to expand our knowledge on the functional effect of human variation in malaria. For the future, a systematic determination of gene-dosage effects and expression profiles of protective genes might unveil the functional impact of structural alterations in these genes on either side of the host-parasite interaction.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=2768989Documentos Relacionados
- Plasmodium liver stage developmental arrest by depletion of a protein at the parasite–host interface
- etramps, a New Plasmodium falciparum Gene Family Coding for Developmentally Regulated and Highly Charged Membrane Proteins Located at the Parasite–Host Cell Interface
- Monitoring Malaria: Genomic Activity of the Parasite in Human Blood Cells
- Adaptive and genetic evolution of Toxoplasma gondii: a host-parasite interaction
- Periodic and chaotic host-parasite interactions in human malaria.
