Targeted deletion reveals essential and overlapping functions of the miR-17 through 92 family of miRNA clusters |
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Authors: | Ventura Andrea Young Amanda G Winslow Monte M Lintault Laura Meissner Alex Erkeland Stefan J Newman Jamie Bronson Roderick T Crowley Denise Stone James R Jaenisch Rudolf Sharp Phillip A Jacks Tyler |
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Affiliation: | Center for Cancer Research, Massachusetts Institute of Technology, Cambridge, MA 02139, USA. |
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Abstract: | miR-17 approximately 92, miR-106b approximately 25, and miR-106a approximately 363 belong to a family of highly conserved miRNA clusters. Amplification and overexpression of miR-1792 is observed in human cancers, and its oncogenic properties have been confirmed in a mouse model of B cell lymphoma. Here we show that mice deficient for miR-17 approximately 92 die shortly after birth with lung hypoplasia and a ventricular septal defect. The miR-17 approximately 92 cluster is also essential for B cell development. Absence of miR-17 approximately 92 leads to increased levels of the proapoptotic protein Bim and inhibits B cell development at the pro-B to pre-B transition. Furthermore, while ablation of miR-106b approximately 25 or miR-106a approximately 363 has no obvious phenotypic consequences, compound mutant embryos lacking both miR-106b approximately 25 and miR-17 approximately 92 die at midgestation. These results provide key insights into the physiologic functions of this family of microRNAs and suggest a link between the oncogenic properties of miR-17 approximately 92 and its functions during B lymphopoiesis and lung development. |
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