Promoter methylation study of the H37/RBM5 tumor suppressor gene from the 3p21.3 human lung cancer tumor suppressor locus

Oh, Juliana J.; Boctor, Baher; Jimenez, Cynthia A.; López, Roberto; Koegel, Ashley K.; Taschereau, Eileen; Phan, Diana T.; Jacobsen, Steven E.; Slamon, Dennis J.

doi:10.1007/s00439-007-0449-5

Cited by 48 publications

(95 citation statements)

References 29 publications

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“…Consistently, H37 triggers mitochondrial apoptotic pathways downstream of Bax, in a p53-independent manner, which include breakdown in the mitochondrial membrane potential, cytochrome c release into cytosol, and enhanced caspase-9 and caspase-3 activities [11]. Further, as compared with adjacent normal tissue, our findings show reduced expression in primary lung cancers of H37 transcript and protein in 9 of 11 (82%) and 46 of 62 (73%) samples, respectively [12], although the H37/3p21.3 LOH genomic status for these samples was unknown. The involvement of H37 in malignancy has been also reported by other investigators for a variety of cancer types.…”

Section: Introductionsupporting

confidence: 78%

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The two single nucleotide polymorphisms in the H37/RBM5 tumour suppressor gene at 3p21.3 correlated with different subtypes of non-small cell lung cancers

Koegel

Phan

et al. 2007

Lung Cancer

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SummaryAllele loss and genetic alteration in chromosome 3p, particularly in 3p21.3 region, are the most frequent and the earliest genomic abnormalities found in lung cancer. Multiple 3p21.3 genes exhibit various degrees of tumour suppression activity suggesting that 3p21.3 genes may function as an integrated tumour suppressor region through their diverse biological activities. We have previously demonstrated growth inhibitory effects and tumour suppression mechanism of the H37/RBM5 gene which is one of the 19 genes residing in the 370kb minimal overlap region at 3p21.3. In the current study, in an attempt to find, if any, mutations in the H37 coding region in lung cancer cells, we compared nucleotide sequences of the entire H37 gene in tumour vs. adjacent normal tissues from 17 non-small cell lung cancer (NSCLC) patients. No mutations were detected, instead, we found the two silent single nucleotide polymorphisms (SNPs), C1138T and C2185T, within the coding region of the H37 gene. In addition, we found that specific allele types at these SNP positions are correlated with different histological subtypes of NSCLC; tumours containing heterozygous alleles (C+T) at these SNP positions are more likely to be associated with adenocarcinoma (AC) whereas homozygous alleles (either C or T) are associated with squamous cell carcinoma (SCC) (p=0.0098). We postulate that, these two silent polymorphisms may be in linkage disequilibrium (LD) with a disease causative allele in the 3p21.3 tumour suppressor region which is packed with a large number of important genes affecting lung cancer development. In addition, because of prevalent loss of heterozygosity (LOH) detected at 3p21.3 which precedes lung cancer initiation, these SNPs may be developed into a marker screening for the high risk individuals. Keywords lung cancer; H37/RBM5/Luca15; single nucleotide polymorphism; 3p21.3; tumour suppressor gene; linkage disequilibrium; loss of heterozygosity

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Section: Introductionsupporting

confidence: 78%

“…Briefly, 5 μg of total RNA was primed with 500 ng of oligo(dT) [12][13][14][15][16][17][18] in a total of 12 μl reaction volume for 10 min. at 70°C followed by quick chill on ice.…”

Section: Rt-pcrmentioning

confidence: 99%

The two single nucleotide polymorphisms in the H37/RBM5 tumour suppressor gene at 3p21.3 correlated with different subtypes of non-small cell lung cancers

Koegel

Phan

et al. 2007

Lung Cancer

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“…Previous studies suggest that frequently reduced RBM5 levels exist in different types of tumors including breast cancer (25), schwannoma (26), and ~75% of primary lung cancers (27). We previously reported that the protein levels of RBM5 are lower in NSCLC compared with non-tumorous tissues (13).…”

Section: Discussionmentioning

confidence: 85%

RNA-binding motif protein 5 negatively regulates the activity of Wnt/β-catenin signaling in cigarette smoke-induced alveolar epithelial injury

Hao

et al. 2015

Oncology Reports

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Abstract. Cigarette smoking is closely associated with various respiratory diseases. Oxidants and carcinogens in cigarettes are reported to induce various airway epithelial injuries. However, the underlying mechanisms remain unclear. The aims of the present study were to determine the involvement of RNA-binding motif protein 5 (RBM5) and Wnt/β-catenin signaling in cigarette smoke-induced alveolar epithelial injury, as well as the interaction between both. A549 cells were treated with cigarette smoke extract (CSE). The MTT assay was used to assess the effects of CSE on cell viability. The levels of RBM5 and Wnt/β-catenin/GSK3β were detected by semi-quantitative reverse transcription-polymerase chain reaction (RT-PCR) and western blot analysis. A luciferase assay was used to assess the activity of β-catenin/T-cell factor (TCF) signaling. The results revealed that CSE inhibited A549 cell viability in both a dose-and time-dependent manner. Cytosolic and nuclear β-catenin levels were significantly increased following CSE treatment, compared with those in the control cells (P<0.05). The luciferase activity in CSE-exposed cells transfected with the TCF luciferase reporter wild-type plasmid (pGL3-OT) was significantly greater than that in cells without CSE exposure (33,167±3,085 vs. 19,978±1,916, respectively, P<0.05). Both the mRNA and protein levels of RBM5 in the CSE-treated cells were significantly reduced compared to the levels in the controls (all P<0.05). The overexpression of RBM5 inhibited Wnt/β-catenin signaling in the A549 cells, while silencing of RBM5 enhanced Wnt/β-catenin signaling. The β-catenin/TCF signaling inhibitor ICG-001 had no apparent effect on the RBM5 levels. Downregulation of RBM5 and activation of Wnt/β-catenin signaling are involved in CSE-induced alveolar epithelial injury. RBM5 acts as an upstream molecule that negatively regulates the activity of Wnt/β-catenin signaling.

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“…Loss of heterozygosity at this locus occurs in 95% of small-cell lung cancer (SCLC), as well as 70% of non-SCLC (Sutherland et al 2010). Consistent with a role as a tumor suppressor, RBM5 (also known as LUCA-15 and H37) was later shown to be down-regulated in a high proportion of lung cancers (Oh et al 2002). RBM5 was also one of nine genes down-regulated as part of a ''metastatic signature'' identified by microarray (Ramaswamy et al 2003).…”

Section: Rna-binding Motif 5 (Rbm5)mentioning

confidence: 96%

Alternative pre-mRNA splicing regulation in cancer: pathways and programs unhinged

David

Manley²

2010

Genes Dev.

721

667

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Alternative splicing of mRNA precursors is a nearly ubiquitous and extremely flexible point of gene control in humans. It provides cells with the opportunity to create protein isoforms of differing, even opposing, functions from a single gene. Cancer cells often take advantage of this flexibility to produce proteins that promote growth and survival. Many of the isoforms produced in this manner are developmentally regulated and are preferentially re-expressed in tumors. Emerging insights into this process indicate that pathways that are frequently deregulated in cancer often play important roles in promoting aberrant splicing, which in turn contributes to all aspects of tumor biology.

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Promoter methylation study of the H37/RBM5 tumor suppressor gene from the 3p21.3 human lung cancer tumor suppressor locus

Cited by 48 publications

References 29 publications

The two single nucleotide polymorphisms in the H37/RBM5 tumour suppressor gene at 3p21.3 correlated with different subtypes of non-small cell lung cancers

The two single nucleotide polymorphisms in the H37/RBM5 tumour suppressor gene at 3p21.3 correlated with different subtypes of non-small cell lung cancers

RNA-binding motif protein 5 negatively regulates the activity of Wnt/β-catenin signaling in cigarette smoke-induced alveolar epithelial injury

Alternative pre-mRNA splicing regulation in cancer: pathways and programs unhinged

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