Aberrant overexpression and function of the miR-17-92 cluster in MLL -rearranged acute leukemia

Abstract: MicroRNA (miRNA)-17-92 cluster (miR-17-92), containing seven individual miRNAs, is frequently amplified and overexpressed in lymphomas and various solid tumors. We have found that it is also frequently amplified and the miRNAs are aberrantly overexpressed in mixed lineage leukemia (MLL)-rearranged acute leukemias. Furthermore, we show that MLL fusions exhibit a much stronger direct binding to the locus of this miRNA cluster than does wild-type MLL; these changes are associated with elevated levels of histone H… Show more

“…34 These potential target genes were all downregulated in MLL-rearranged ALL. 32,34,61 Two genes, that is, APP and RASSF2 were confirmed targets for miR-17-92 as shown by a luciferase 3 0 UTR-binding assay 34 and the expression of one gene (that is, TNFRSF21) inversely correlated with the expression of the miR-17-92 cluster. 32 The miR-17-92 cluster also has a oncogenic role in T-ALL.…”

“…Induced expression of the miRNA cluster enhanced the colony-forming capacity of mouse bone marrow progenitors especially when MLL fusion genes were co-expressed. 32,61 Increased expression of the miR-17-92 cluster was associated with a downregulation of p21 inhibitor of cell cycle progression. Complete knockdown of p21 mimicked the oncogenic effect of miR-17-92 in MLL-rearranged leukemia cells.…”

“…High expression of another set of miRNAs including miR-382 was unique for t(15;17)/PML-RARa-positive AML. 18,20 MLL-rearranged AML cases, the oncogenic miR-17-92 cluster was upregulated 21,34,32 whereas the tumor-suppressor miR-29 was downregulated (Table 2). 19,23 MiRNA expression levels are also associated with molecular subtypes of AML, the mutational status and associated gene expression pattern in AML (Table 2).…”

“…20,21,[32][33][34]61 Together with the fact that this polycistronic cluster cooperated with c-Myc to accelerate B-cell lymphoma formation in vivo 62 suggests that miR-17-92 acts as an oncogene in lymphoid tissue. Induced expression of the miRNA cluster enhanced the colony-forming capacity of mouse bone marrow progenitors especially when MLL fusion genes were co-expressed.…”

“…For example, amplification of the miR-17-92 gene cluster contributed to the high level of expression of this cluster in MLL-rearranged patients. 32 In addition, MLL-fusion proteins 32,61 and oncogene c-myc may be responsible for miR-17-92 cluster overexpression. 61 In T-ALL, the newly identified translocation t(13;14)(q32;q11) targeted the miR-17-92 gene cluster and possibly thereby facilitates its expression.…”

MicroRNAs in acute leukemia: from biological players to clinical contributors

“…34 These potential target genes were all downregulated in MLL-rearranged ALL. 32,34,61 Two genes, that is, APP and RASSF2 were confirmed targets for miR-17-92 as shown by a luciferase 3 0 UTR-binding assay 34 and the expression of one gene (that is, TNFRSF21) inversely correlated with the expression of the miR-17-92 cluster. 32 The miR-17-92 cluster also has a oncogenic role in T-ALL.…”

“…Induced expression of the miRNA cluster enhanced the colony-forming capacity of mouse bone marrow progenitors especially when MLL fusion genes were co-expressed. 32,61 Increased expression of the miR-17-92 cluster was associated with a downregulation of p21 inhibitor of cell cycle progression. Complete knockdown of p21 mimicked the oncogenic effect of miR-17-92 in MLL-rearranged leukemia cells.…”

“…High expression of another set of miRNAs including miR-382 was unique for t(15;17)/PML-RARa-positive AML. 18,20 MLL-rearranged AML cases, the oncogenic miR-17-92 cluster was upregulated 21,34,32 whereas the tumor-suppressor miR-29 was downregulated (Table 2). 19,23 MiRNA expression levels are also associated with molecular subtypes of AML, the mutational status and associated gene expression pattern in AML (Table 2).…”

“…20,21,[32][33][34]61 Together with the fact that this polycistronic cluster cooperated with c-Myc to accelerate B-cell lymphoma formation in vivo 62 suggests that miR-17-92 acts as an oncogene in lymphoid tissue. Induced expression of the miRNA cluster enhanced the colony-forming capacity of mouse bone marrow progenitors especially when MLL fusion genes were co-expressed.…”

“…For example, amplification of the miR-17-92 gene cluster contributed to the high level of expression of this cluster in MLL-rearranged patients. 32 In addition, MLL-fusion proteins 32,61 and oncogene c-myc may be responsible for miR-17-92 cluster overexpression. 61 In T-ALL, the newly identified translocation t(13;14)(q32;q11) targeted the miR-17-92 gene cluster and possibly thereby facilitates its expression.…”

MicroRNAs in acute leukemia: from biological players to clinical contributors

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