Consistent Deregulation of Gene Expression between Human and Murine <i>MLL</i> Rearrangement Leukemias

Li, Zejuan; Luo, Roger T.; Mi, Shuangli; Sun, Miao; Chen, Ping; Bao, Jingyue; Neilly, Mary Beth; Jayathilaka, Nimanthi; Johnson, Deborah; Wang, Lili; Lavau, Catherine; Zhang, Yanming; Tseng, Charles C.; Zhang, Xiuqing; Wang, Jian; Yu, Jun; Yang, Huanming; Wang, San Ming; Rowley, Janet D.; Chen, Jianjun; Thirman, Michael J.

doi:10.1158/0008-5472.can-08-3381

Cited by 78 publications

(76 citation statements)

References 51 publications

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“…Experimental data shows that MLL fusions inhibit hematopoietic differentiation in serial replating assays, a critical surrogate parameter for transformation activity (26,27). Although MLL-associated leukemias have been intensively studied, how miRNAs contribute to their development and how they can contribute or trigger the clonogenic capacity of MLLfusion dependent clones are largely unknown.We previously reported that the individual miRNAs of the miR-17-92 cluster were overexpressed in the majority of MLL-rearranged AML (16,28). In the present study, we demonstrate that the miR-17-92 cluster is highly expressed not only in MLL-associated AML, but also in MLL-associated ALL.…”

supporting

confidence: 73%

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

Mi¹,

Li²,

Chen³

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

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124

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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 H3 acetylation and H3K4 trimethylation and an up-regulation of these miRNAs. We further observe that forced expression of this miRNA cluster increases proliferation and inhibits apoptosis of human cells. More importantly, we show that this miRNA cluster can significantly increase colony-forming capacity of normal mouse bone marrow progenitor cells alone and, particularly, in cooperation with MLL fusions. Finally, through combinatorial analysis of miRNA and mRNA arrays of mouse bone marrow progenitor cells transfected with this miRNA cluster and/or MLL fusion gene, we identified 363 potential miR-17-92 target genes that exhibited a significant inverse correlation of expression with the miRNAs. Remarkably, these potential target genes are significantly enriched (P < 0.01; >2-fold) in cell differentiation, hematopoiesis, cell cycle, and apoptosis. Taken together, our studies suggest that overexpression of miR-17-92 cluster in MLL-rearranged leukemias is likely attributed to both DNA copy number amplification and direct up-regulation by MLL fusions, and that the miRNAs in this cluster may play an essential role in the development of MLL-associated leukemias through inhibiting cell differentiation and apoptosis, while promoting cell proliferation, by regulating relevant target genes.cell apoptosis and viability | colony-forming/replating assay | MLL binding | gene regulation | miRNA target M icroRNAs (miRNAs, miRs) are endogenous ≈22 nucleotides (nt) noncoding RNAs that play important regulatory roles in animals and plants by binding with the 3′ UTRs of messenger RNAs (mRNAs) of target genes, leading to mRNA cleavage/degradation or translational repression (1-4). Rapidly accumulating evidence has revealed that miRNAs are strongly associated with cancer (3, 5-7). Recent studies suggest that a cluster of miRNAs, the miR-17-92 polycistron located at 13q31 [containing seven individual miRNAs including miR-17-5p (now named miR-17), miR-17-3p (now named miR-17*), miR-18a, miR-19a, miR-20a, miR-19b-1, and miR-92a-1], may function as an oncogene (8-12). Particularly, He et al. (8) showed that enforced expression of the miR-17-92 cluster cooperated with Myc expression to accelerate tumor development in a mouse model of human B-cell lymphoma. Its oncogenic function is further supported by the finding that miRNAs from this cluster are overexpressed in lung, breast, colon, pancreas, prostate tumors, and chronic leukemias, and that overexpression of these miRNAs is usually correlated with the amplification of its genomic lo...

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supporting

confidence: 73%

“…We previously reported that the individual miRNAs of the miR-17-92 cluster were overexpressed in the majority of MLL-rearranged AML (16,28). In the present study, we demonstrate that the miR-17-92 cluster is highly expressed not only in MLL-associated AML, but also in MLL-associated ALL.…”

supporting

confidence: 73%

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

Mi¹,

Li²,

Chen³

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

138

124

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“…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.…”

Section: Oncogenic Mirnasmentioning

confidence: 96%

“…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.…”

Section: Oncogenic Mirnasmentioning

confidence: 99%

“…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).…”

Section: Aberrant Mirna Expression Characterizes Different Cytogenetimentioning

confidence: 99%

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MicroRNAs in acute leukemia: from biological players to clinical contributors

2011

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MicroRNAs (miRNAs) are involved in the management of hematopoiesis. As a consequence, miRNA dysregulation causes disruption of the hematopoietic system and leukemia may arise. We here comprehensively discuss miRNAs found discriminative for cytogenetic and molecular subtypes of acute leukemia. These miRNAs are either known miRNAs involved in leukemogenesis with proven tumor suppressor or oncogenic activities or are newly identified by high-throughput sequencing with yet unknown function. Furthermore, forces are outlined that drive aberrant miRNA function, which include genetic abnormalities (for example, deletions, translocations and mutations) and epigenetic aberrations (for example, aberrant DNA methylation or histone modifications). Interestingly, leukemia-silenced miRNAs can be re-expressed upon treatment with de-methylating agents. Targeting miRNA expression may serve a therapeutical role, albeit at present this way of targeted therapy is in its infancy. However, emerging knowledge about the biology of miRNAs in leukemia may result into a role for these miRNAs in the diagnosis and treatment of acute leukemia.

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2010

Data Mining for Genomics and Proteomics

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Consistent Deregulation of Gene Expression between Human and Murine MLL Rearrangement Leukemias

Cited by 78 publications

References 51 publications

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

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

MicroRNAs in acute leukemia: from biological players to clinical contributors

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