Response of malignant B lymphocytes to ionizing radiation: Gene expression and genotype

Lyng, Heidi; Landsverk, Kirsti Solberg; Kristiansen, Eva; DeAngelis, Paula M.; Ree, Anne Hansen; Myklebost, Ola; Hovig, Eivind; Stokke, Trond

doi:10.1002/ijc.20962

Cited by 19 publications

(20 citation statements)

References 35 publications

(46 reference statements)

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“…Second, we focused on miRs that had been previously shown to be differentially expressed in other cancers and that had oncogenes or tumor suppressors as predicted targets. One example is miR‐Let‐7c, which had been previously published as a tumor suppressor miR and has predicted targets shown to be associated with cancer, such as CCNF (De Angelis et al., ; Lyng et al., ; Roy et al., ), E2F2 (Dong et al., ; Pusapati et al., ; Rempel et al., ; Shen et al., ), E2F6 (Lu et al., ; Sanchez‐Beato et al., ), and RAS (He et al., ; Khodayari et al., ; Oh et al., ). Finally, a number of miRs were chosen solely for their bio‐informatically predicted ability to regulate the expression of known oncogenic and tumor suppressor genes.…”

Section: Resultsmentioning

confidence: 99%

MicroRNA‐206 induces G1 arrest in melanoma by inhibition of CDK4 and Cyclin D

Georgantas¹,

Streicher²,

Luo³

et al. 2014

Pigment Cell Melanoma Res

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Expression profiling of microRNAs in melanoma lesional skin biopsies compared with normal donor skin biopsies, as well as melanoma cell lines compared with normal melanocytes, revealed that hsa-miR-206 was down-regulated in melanoma (-75.4-fold, P = 1.7 × 10(-4)). MiR-206 has been implicated in a large number of cancers, including breast, lung, colorectal, ovarian, and prostate cancers; however, its role in tumor development remains largely unknown, its biologic function is poorly characterized, and its targets affecting cancer cells are largely unknown. MiR-206 reduced growth and migration/invasion of multiple melanoma cell lines. Bioinformatics identified cell cycle genes CDK2, CDK4, Cyclin C, and Cyclin D1 as strong candidate targets. Western blots and 3'UTR reporter gene assays revealed that miR-206 inhibited translation of CDK4, Cyclin D1, and Cyclin C. Additionally, hsa-miR-206 transfection induced G1 arrest in multiple melanoma cell lines. These observations support hsa-miR-206 as a tumor suppressor in melanoma and identify Cyclin C, Cyclin D1, and CDK4 as miR-206 targets.

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Section: Resultsmentioning

confidence: 99%

MicroRNA‐206 induces G1 arrest in melanoma by inhibition of CDK4 and Cyclin D

Georgantas¹,

Streicher²,

Luo³

et al. 2014

Pigment Cell Melanoma Res

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“…Moreover, down-modulation of PLK1 expression was found to inhibit growth of bladder cancer in mice [29]. Expression of PLK1 and CCNF (cyclin F), which contributes to the G 2 to M phase transition, have been related to response to radio and chemotherapy [30, 31]. From the “invasion” gene set, secreted protein acidic and rich in cysteine ( SPARC ) (also known as osteonectin) is overexpressed in CRCs and induces proinvasive activity [32].…”

Section: Discussionmentioning

confidence: 99%

Identification of key genes for carcinogenic pathways associated with colorectal adenoma-to-carcinoma progression

et al. 2010

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Colorectal adenomas form a biologically and clinically distinct intermediate stage in development of colorectal cancer (CRC) from normal colon epithelium. Only 5% of adenomas progress into adenocarcinomas, indicating that malignant transformation requires other biological alterations than those involved in adenoma formation. The present study aimed to explore which cancer-related biological processes are affected during colorectal adenoma-to-carcinoma progression and to identify key genes within these pathways that can serve as tumor markers for malignant transformation. The activity of 12 cancer-related biological processes was compared between 37 colorectal adenomas and 31 adenocarcinomas, using the pathway analysis tool Gene Set Enrichment Analysis. Expression of six gene sets was significantly increased in CRCs compared to adenomas, representing chromosomal instability, proliferation, differentiation, invasion, stroma activation, and angiogenesis. In addition, 18 key genes were identified for these processes based on their significantly increased expression levels. For AURKA and PDGFRB, increased mRNA expression levels were verified at the protein level by immunohistochemical analysis of a series of adenomas and CRCs. This study revealed cancer-related biological processes whose activities are increased during malignant transformation and identified key genes which may be used as tumor markers to improve molecular characterization of colorectal tumors.Electronic supplementary materialThe online version of this article (doi:10.1007/s13277-009-0012-1) contains supplementary material, which is available to authorized users.

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“…Because dNTP production is critical for cell survival, additional mechanisms operate following genotoxic stress to regulate the cyclin F-RRM2 axis. For example, cyclin F mRNA levels decrease 6 hours after treatment of B lymphocytes with ionizing radiation [25]. Additionally, four RRM2 transcript variants have been found in zebrafish, and one of the four variants that is most highly expressed following the treatment of embryos with genotoxic stress lacks the first 52 amino acids, where the binding sites for cyclin F and Cdh1 reside.…”

Section: The Cyclin F-rrm2 Axismentioning

confidence: 99%

A cyclin without cyclin-dependent kinases: cyclin F controls genome stability through ubiquitin-mediated proteolysis

D’Angiolella

Esencay

Pagano

2013

Trends in Cell Biology

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Cell cycle transitions are driven by the periodic oscillations of cyclins, which bind and activate CDKs (cyclin-dependent kinases) to phosphorylate target substrates. Cyclin F uses a substrate recruitment strategy similar to that of the other cyclins, but its associated catalytic activity is substantially different. Indeed, cyclin F is the founding member of the F-box family of proteins, which are the substrate recognition subunits of SCF (Skp1-Cul1-F-box protein) ubiquitin ligase complexes. Here, we discuss cyclin F function and recently identified substrates of SCFcyclin F involved in dNTP production, centrosome duplication, and spindle formation. We highlight the relevance of cyclin F in controlling genome stability through ubiquitin-mediated proteolysis and the implications for cancer development.

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Response of malignant B lymphocytes to ionizing radiation: Gene expression and genotype

Cited by 19 publications

References 35 publications

MicroRNA‐206 induces G1 arrest in melanoma by inhibition of CDK4 and Cyclin D

MicroRNA‐206 induces G1 arrest in melanoma by inhibition of CDK4 and Cyclin D

Identification of key genes for carcinogenic pathways associated with colorectal adenoma-to-carcinoma progression

A cyclin without cyclin-dependent kinases: cyclin F controls genome stability through ubiquitin-mediated proteolysis

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