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Exonuclease-mediated degradation of nascent RNA silences genes linked to severe malaria.

Nature.. 2014-06; 
Q Zhang, TN Siegel, RM Martins, F Wang, J Cao, Q Gao, X Cheng, L Jiang, CC Hon, CS Benatar, H Sakamoto, L Turner, ATR Jensen, A Claes, J Guizetti, NA Malmquist & A Scherf. Unite de Biologie des Interactions Hote-Parasite, Institut Pasteur, F-75724 Paris, France.
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摘要

Antigenic variation of the Plasmodium falciparum multicopy var gene family enables parasite evasion of immune destruction by host antibodies1, 2. Expression of a particular var subgroup, termed upsA, is linked to the obstruction of blood vessels in the brain and to the pathogenesis of human cerebral malaria3, 4, 5, 6. The mechanism determining upsA activation remains unknown. Here we show that an entirely new type of gene silencing mechanism involving an exonuclease-mediated degradation of nascent RNA controls the silencing of genes linked to severe malaria. We identify a novel chromatin-associated exoribonuclease, termed PfRNase II, that controls the silencing of upsA var genes by marking their transcription s... More

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