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   Let-7 Represses Carcinogenesis and a Stem Cell Phenotype in the Intestine via Regulation of Hmga2  
   
نویسنده madison b.b. ,jeganathan a.n. ,mizuno r. ,winslow m.m. ,castells a. ,cuatrecasas m. ,rustgi a.k.
منبع plos genetics - 2015 - دوره : 11 - شماره : 8
چکیده    Let-7 mirnas comprise one of the largest and most highly expressed family of mirnas among vertebrates,and is critical for promoting differentiation,regulating metabolism,inhibiting cellular proliferation,and repressing carcinogenesis in a variety of tissues. the large size of the let-7 family of mirnas has complicated the development of mutant animal models. here we describe the comprehensive repression of all let-7 mirnas in the intestinal epithelium via low-level tissue-specific expression of the lin28b rna-binding protein and a conditional knockout of the mirlet7c-2/mirlet7b locus. this ablation of let-7 triggers the development of intestinal adenocarcinomas concomitant with reduced survival. analysis of both mouse and human intestinal cancer specimens reveals that stem cell markers were significantly associated with loss of let-7 mirna expression,and that a number of let-7 targets were elevated,including hmga1 and hmga2. functional studies in 3-d enteroids revealed that hmga2 is necessary and sufficient to mediate many characteristics of let-7 depletion,namely accelerating cell cycle progression and enhancing a stem cell phenotype. in addition,inactivation of a single hmga2 allele in the mouse intestine epithelium significantly represses tumorigenesis driven by lin28b. in aggregate,we conclude that let-7 depletion drives a stem cell phenotype and the development of intestinal cancer,primarily via hmga2. © 2015 madison et al.
آدرس division of gastroenterology,washington university school of medicine,saint louis,mo,united states,department of medicine,washington university school of medicine,saint louis,mo, United States, division of gastroenterology,university of pennsylvania perelman school of medicine,philadelphia,pa,united states,department of medicine,university of pennsylvania perelman school of medicine,philadelphia,pa,united states,department of surgery,university of pennsylvania perelman school of medicine,philadelphia,pa, United States, division of gastroenterology,university of pennsylvania perelman school of medicine,philadelphia,pa,united states,department of medicine,university of pennsylvania perelman school of medicine,philadelphia,pa, United States, department of genetics,stanford university school of medicine,stanford,ca, United States, gastroenterology department,hospital clínic,ciberehd,idibaps,barcelona,catalonia, Spain, department of pathology,pharmacology and microbiology,hospital clínic,cdb,university of barcelona,barcelona,catalonia, Spain, division of gastroenterology,university of pennsylvania perelman school of medicine,philadelphia,pa,united states,department of medicine,university of pennsylvania perelman school of medicine,philadelphia,pa,united states,department of genetics,university of pennsylvania perelman school of medicine,philadelphia,pa,united states,abramson cancer center,university of pennsylvania perelman school of medicine,philadelphia,pa, United States
 
     
   
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