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   HIV-1 Integrates Widely throughout the Genome of the Human Blood Fluke Schistosoma mansoni  
   
نویسنده suttiprapa s. ,rinaldi g. ,tsai i.j. ,mann v.h. ,dubrovsky l. ,yan h.-b. ,holroyd n. ,huckvale t. ,durrant c. ,protasio a.v. ,pushkarsky t. ,iordanskiy s. ,berriman m. ,bukrinsky m.i. ,brindley p.j.
منبع plos pathogens - 2016 - دوره : 12 - شماره : 10
چکیده    Schistosomiasis is the most important helminthic disease of humanity in terms of morbidity and mortality. facile manipulation of schistosomes using lentiviruses would enable advances in functional genomics in these and related neglected tropical diseases pathogens including tapeworms,and including their non-dividing cells. such approaches have hitherto been unavailable. blood stream forms of the human blood fluke,schistosoma mansoni,the causative agent of the hepatointestinal schistosomiasis,were infected with the human hiv-1 isolate nl4-3 pseudotyped with vesicular stomatitis virus glycoprotein. the appearance of strong stop and positive strand cdnas indicated that virions fused to schistosome cells,the nucleocapsid internalized and the rna genome reverse transcribed. anchored pcr analysis,sequencing hiv-1-specific anchored illumina libraries and whole genome sequencing (wgs) of schistosomes confirmed chromosomal integration; >8,000 integrations were mapped,distributed throughout the eight pairs of chromosomes including the sex chromosomes. the rate of integrations in the genome exceeded five per 1,000 kb and hiv-1 integrated into protein-encoding loci and elsewhere with integration bias dissimilar to that of human t cells. we estimated ~ 2,100 integrations per schistosomulum based on wgs,i.e. about two or three events per cell,comparable to integration rates in human cells. accomplishment in schistosomes of post-entry processes essential for hiv-1replication,including integrase-catalyzed integration,was remarkable given the phylogenetic distance between schistosomes and primates,the natural hosts of the genus lentivirus. these enigmatic findings revealed that hiv-1 was active within cells of s. mansoni,and provided the first demonstration that hiv-1 can integrate into the genome of an invertebrate. © 2016 suttiprapa et al.
آدرس department of microbiology,immunology & tropical medicine,research center for neglected diseases of poverty,school of medicine and health sciences,the george washington university,washington,dc,united states,department of microbiology,faculty of science,mahidol university,phyathai,rachthewee,bangkok,thailand,department of pathology,faculty of medicine,khon kaen university,muang khon kaen, Thailand, department of microbiology,immunology & tropical medicine,research center for neglected diseases of poverty,school of medicine and health sciences,the george washington university,washington,dc,united states,wellcome trust sanger institute,wellcome genome campus,hinxton,cambridge, United Kingdom, wellcome trust sanger institute,wellcome genome campus,hinxton,cambridge,united kingdom,biodiversity research center,academia sinica,taipei, Taiwan, department of microbiology,immunology & tropical medicine,research center for neglected diseases of poverty,school of medicine and health sciences,the george washington university,washington,dc, United States, department of microbiology,immunology & tropical medicine,research center for neglected diseases of poverty,school of medicine and health sciences,the george washington university,washington,dc, United States, department of microbiology,immunology & tropical medicine,research center for neglected diseases of poverty,school of medicine and health sciences,the george washington university,washington,dc,united states,veterinary research institute,chinese academy of agricultural sciences,xujiaping 1,lanzhou,gansu, Taiwan, wellcome trust sanger institute,wellcome genome campus,hinxton,cambridge, United Kingdom, wellcome trust sanger institute,wellcome genome campus,hinxton,cambridge, United Kingdom, wellcome trust sanger institute,wellcome genome campus,hinxton,cambridge, United Kingdom, wellcome trust sanger institute,wellcome genome campus,hinxton,cambridge, United Kingdom, department of microbiology,immunology & tropical medicine,research center for neglected diseases of poverty,school of medicine and health sciences,the george washington university,washington,dc, United States, department of microbiology,immunology & tropical medicine,research center for neglected diseases of poverty,school of medicine and health sciences,the george washington university,washington,dc,united states,national center for biodefense and infectious diseases,school of systems biology,george mason university,manassas,va, United States, wellcome trust sanger institute,wellcome genome campus,hinxton,cambridge, United Kingdom, department of microbiology,immunology & tropical medicine,research center for neglected diseases of poverty,school of medicine and health sciences,the george washington university,washington,dc, United States, department of microbiology,immunology & tropical medicine,research center for neglected diseases of poverty,school of medicine and health sciences,the george washington university,washington,dc, United States
 
     
   
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