MicroRNA miR-29 Modulates Expression of Immunoinhibitory Molecule B7-H3: Potential Implications for Immune Based Therapy of Human Solid Tumors

Xu, Hong; Cheung, Irene Y.; Guo, Hong-Fen; Cheung, Nai‐Kong V.

doi:10.1158/0008-5472.can-08-4517

Cited by 232 publications

(188 citation statements)

References 29 publications

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“…In the present study, using the Src-specific small molecule inhibitors saracatinib and dasatinib, we identified miR-29b as an important mediator of the Src-ID1 pathway, controlling lung cancer cell invasion. Members of the miRNA-29 family (miR-29a, miR-29b and miR-29c) are known to be highly expressed in normal tissues and downregulated in different types of cancer, including neuroblastoma, sarcoma, glioma, high-risk chronic lymphatic leukemia, invasive breast cancer, cholangiocarcinoma and lung cancer (Calin et microRNA-29b in lung cancer SI Rothschild et al et al, 2006;Mott et al, 2007;Wu et al, 2009;Xu et al, 2009). The three miR-29 isoforms are arranged in two clusters: miR-29b1/miR-29a located on chromosome 7q32 and miR-29b2/miR-29c located on chromosome 1q32.…”

Section: Discussionmentioning

confidence: 99%

MicroRNA-29b is involved in the Src-ID1 signaling pathway and is dysregulated in human lung adenocarcinoma

et al. 2012

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Section: Discussionmentioning

confidence: 99%

MicroRNA-29b is involved in the Src-ID1 signaling pathway and is dysregulated in human lung adenocarcinoma

et al. 2012

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“…This is a mechanism that is distinct from H-Ras/MAPK regulation of C-myc, which is primarily through protein stabilization. Various microRNAs (mir-34a, mir-101, and let-7) have also been documented to regulate N-myc by targeting mRNA, resulting in reduced N-myc expression and decreased proliferation of MYCN-amplified neuroblastoma cells (75,76).…”

Section: Regulation Of N-mycmentioning

confidence: 99%

The N-myc Oncogene: Maximizing its Targets, Regulation, and Therapeutic Potential

Beltran

2014

Molecular Cancer Research

121

109

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N-myc (MYCN), a member of the Myc family of basic-helix-loop-helix-zipper (bHLHZ) transcription factors, is a central regulator of many vital cellular processes. As such, N-myc is well recognized for its classic oncogenic activity and association with human neuroblastoma. Amplification and overexpression of N-myc has been described in other tumor types, particularly those of neural origin and neuroendocrine tumors. This review outlines N-myc's contribution to normal development and oncogenic progression. In addition, it highlights relevant transcriptional targets and mechanisms of regulation. Finally, the clinical implications of N-Myc as a biomarker and potential as a target using novel therapeutic approaches are discussed. Mol Cancer Res; 12(6); 815-22. Ó2014 AACR. IntroductionThe N-myc gene was first reported in 1983, when Schwab and colleagues (1) and Kohl and colleagues (2) discovered that there were a subset of human neuroblastoma cell lines harboring multiple copies of a DNA sequence related to the C-myc oncogene (MYC), and this region was designated Nmyc (MYCN). Genomic amplification of N-myc resulted in overexpression of N-myc at the mRNA level, and rat embryo cells transfected with N-myc demonstrated oncogenic properties. These findings were first to bring attention to N-myc as a putative oncogene.

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“…Role of miR-29 family members expression in immune response was observed on B7-H3 and interferon γ (ref. 29,37 ). Currently a number of target genes affected by miR-29 family members in variety of cancers were identified.…”

Section: Target Genes Of Mir-29mentioning

confidence: 99%

The role of miR-29 family members in malignant hematopoiesis

Kollinerová¹,

Vassanelli²,

Modrianský³

2014

BIOMED PAP

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Aims. MicroRNAs of the miR-29 family members were one of the first microRNAs identified as possible therapeutic agents in malignant hematopoiesis. The aim of our review is to summarize the current state of knowledge on miR-29 family members. Methods. We performed literature searches involving miR-29 family members and their relationship to individual hematological malignancies, namely acute myeloid leukemia (AML), chronic lymphoblastic leukemia (CLL) and chronic myeloid leukemia (CML). We also searched for subgroups of hematological malignancies, e.g. multiple myeloma, that are regarded as members of the acute or chronic types of leukemias. Results. A number of genes appear to be regulated by miR-29 family members in various physiological and pathological situations. In our view regulation of Tcl-1, Mcl-1 and DNA methyltransferases is relevant in case of hematological malignancies, hence these are the focus of this review. miR-29 family members also function during normal T-cell and B-cell development. Conclusion. MiR-29 family members appear to govern some general features in commonly heterogenous hematological malignancies and therefore form a potential target for treatment.

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MicroRNA miR-29 Modulates Expression of Immunoinhibitory Molecule B7-H3: Potential Implications for Immune Based Therapy of Human Solid Tumors

Cited by 232 publications

References 29 publications

MicroRNA-29b is involved in the Src-ID1 signaling pathway and is dysregulated in human lung adenocarcinoma

MicroRNA-29b is involved in the Src-ID1 signaling pathway and is dysregulated in human lung adenocarcinoma

The N-myc Oncogene: Maximizing its Targets, Regulation, and Therapeutic Potential

The role of miR-29 family members in malignant hematopoiesis

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