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   HIV integration targeting: A pathway involving transportin-3 and the nuclear pore protein RanBP2  
   
نویسنده ocwieja k.e. ,brady t.l. ,ronen k. ,huegel a. ,roth s.l. ,schaller t. ,james l.c. ,towers g.j. ,young j.a.t. ,chanda s.k. ,könig r. ,malani n. ,berry c.c. ,bushman f.d.
منبع plos pathogens - 2011 - دوره : 7 - شماره : 3
چکیده    Genome-wide sirna screens have identified host cell factors important for efficient hiv infection,among which are nuclear pore proteins such as ranbp2/nup358 and the karyopherin transportin-3/tnpo3. analysis of the roles of these proteins in the hiv replication cycle suggested that correct trafficking through the pore may facilitate the subsequent integration step. here we present data for coupling between these steps by demonstrating that depletion of transportin-3 or ranbp2 altered the terminal step in early hiv replication,the selection of chromosomal sites for integration. we found that depletion of transportin-3 and ranbp2 altered integration targeting for hiv. these knockdowns reduced hiv integration frequency in gene-dense regions and near gene-associated features,a pattern that differed from that reported for depletion of the hiv integrase binding cofactor psip1/ledgf/p75. mlv integration was not affected by the transportin-3 knockdown. using sirna knockdowns and integration targeting analysis,we also implicated several additional nuclear proteins in proper target site selection. to map viral determinants of integration targeting,we analyzed a chimeric hiv derivative containing mlv gag,and found that the gag replacement phenocopied the transportin-3 and ranbp2 knockdowns. thus,our data support a model in which gag-dependent engagement of the proper transport and nuclear pore machinery mediate trafficking of hiv complexes to sites of integration. © 2011 ocwieja et al.
آدرس department of microbiology,university of pennsylvania school of medicine,philadelphia,pa, United States, department of microbiology,university of pennsylvania school of medicine,philadelphia,pa, United States, department of microbiology,university of pennsylvania school of medicine,philadelphia,pa,united states,fred hutchinson cancer research center,seattle,wa, United States, department of microbiology,university of pennsylvania school of medicine,philadelphia,pa, United States, department of microbiology,university of pennsylvania school of medicine,philadelphia,pa, United States, medical research council centre for medical molecular virology,division of infection and immunity,university college london,london, United Kingdom, protein and nucleic acid chemistry division,medical research council laboratory of molecular biology,cambridge, United Kingdom, medical research council centre for medical molecular virology,division of infection and immunity,university college london,london, United Kingdom, infectious disease laboratory,the salk institute for biological studies,la jolla,ca, United States, infectious and inflammatory disease center,burnham institute for medical research,la jolla,ca, United States, infectious and inflammatory disease center,burnham institute for medical research,la jolla,ca, United States, department of microbiology,university of pennsylvania school of medicine,philadelphia,pa, United States, department of family/preventive medicine,university of california,san diego school of medicine,san diego,ca, United States, department of microbiology,university of pennsylvania school of medicine,philadelphia,pa, United States
 
     
   
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