Biallelic <i><scp>DICER1</scp></i> mutations occur in Wilms tumours

Wu, Mona; Sabbaghian, Nelly; Xu, Bin; Addidou-Kalucki, S.; Bernard, Chantal; Zou, Donghui; Reeve, Anthony E.; Eccles, Michael R.; Cole, Caroline; Choong, Catherine S.; Charles, Adrian; Tan, Tiong Yang; Iglesias, Diana M.; Goodyer, Paul; Foulkes, William D.

doi:10.1002/path.4196

Cited by 128 publications

(113 citation statements)

References 57 publications

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“…In sample D, the E1813G mutation was identified by initial genomic DNA (gDNA) sequencing, and subsequent cDNA sequencing of an amplicon spanning the RNase IIIb domain revealed two products, a long one containing the canonical DICER1 sequence and a shorter one with a 163 nt deletion missing exon 25 ( Figure 2B). This result agreed with a previous observation that the c.5438A > G (E1813G) mutation in DICER1 promotes inefficient exon 25 exclusion, producing both a full-length transcript with c.5438A > G and an exon-25-depleted transcript [13]. Interestingly, when the longer cDNA amplicon was sequenced, only c.5438A > G but no wild-type (WT) sequence was detected ( Figure 2B), suggesting that the expression of WT DICER1 is lost, probably due to either a cryptic genomic aberration or epigenetic silencing.…”

Section: Evaluation Of Biallelic Dicer1 Mutationssupporting

confidence: 93%

“…This is consistent across both the TCGA dataset (7/304) and our own local tumour bank (6/290; see supplementary material, Tables S1, S7). DICER1 hotspot mutations, although rare, were also identified in brain, colorectal and thyroid cancers (see supplementary material, TableDICER1 hotspot mutations in endometrial cancer 223 tumourigenesis beyond the spectrum of rare paediatric cancers [8][9][10][11][12][13][15][16][17][18]. DICER1 hotspot mutations and subsequent miRNA/mRNA dysregulation may therefore constitute a common oncogenic pathway in a small subset of endometrial tumours.…”

Section: Discussionmentioning

confidence: 99%

“…The two-hit hypothesis for DICER1 was initially proposed after identification of DICER1 hotspot mutations in tumours from PPB and PPB-FTDS patients with germline DICER1 mutations [11,13,29]. More recently, frequent biallelic DICER1 mutations were identified in sporadic (8/11) and germline PPB (12/12) from two independent studies [16,28].…”

Section: Discussionmentioning

confidence: 99%

“…Subsequent studies have shown that hotspot mutations at the four metal-binding sites in the RNase IIIb domain (E1705, D1709, D1810 and E1813) impair DICER1's ability to generate mature 5p miRNAs [4,11,12]. More recently, DICER1 hotspot mutations were identified in tumours from PPB and PPB-FTDS cases possessing germline DICER1 mutations, suggesting a two-hit hypothesis of tumourigenesis [11,[13][14][15][16].…”

Section: J Chen Et Almentioning

confidence: 99%

“…The mutational analyses of DICER1 have previously focused on rare paediatric cancers [6][7][8][9][10][11][13][14][15][16]. In this study, we investigated the prevalence of DICER1 mutations in a spectrum of more common malignancies.…”

Section: J Chen Et Almentioning

confidence: 99%

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Recurrent DICER1 hotspot mutations in endometrial tumours and their impact on microRNA biogenesis

Chen

Wang

McMonechy

et al. 2015

The Journal of Pathology

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DICER1 plays a critical role in microRNA (miRNA) biogenesis. Recurrent somatic 'hotspot' mutations at the four metal-binding sites within the RNase IIIb domain of DICER1 were identified in ovarian sex cord-stromal tumours and have since been described in other paediatric tumours. In this study, we screened the RNase IIIb domain of DICER1 in 290 endometrial tumours and identified six cases with hotspot mutations, including two cases affected by an atypical G1809R mutation directly adjacent to a metal-binding site. Using Illumina and Sanger targeted resequencing, we observed and validated biallelic DICER1 mutations in several cases with hotspot mutations. Through in vitro DICER1 cleavage assays, small RNA deep sequencing and real-time PCR, we demonstrated that mutations adding a positively charged side chain to residue 1809 have similar detrimental effects on 5p miRNA production to mutations at the metal-binding sites. As expected, 5p miRNAs were globally reduced in tumours and cell lines with hotspot mutations. Pathway analysis of gene expression profiles indicated that genes de-repressed due to loss of 5p miRNAs are strongly associated with pathways regulating the cell cycle. Using a Dicer1-null mouse cell line model, we found that expression of DICER1 hotspot mutants promoted cell proliferation, whereas wild-type (WT) DICER1 inhibited cell proliferation. Furthermore, targets of let-7 family miRNAs are enriched among the up-regulated genes, suggesting that loss of let-7 may be impacting downstream pathways. Our results reveal that DICER1 hotspot mutations are implicated in common malignancies and may constitute a unique oncogenic pathway.

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Section: Evaluation Of Biallelic Dicer1 Mutationssupporting

confidence: 93%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: J Chen Et Almentioning

confidence: 99%

Section: J Chen Et Almentioning

confidence: 99%

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Recurrent DICER1 hotspot mutations in endometrial tumours and their impact on microRNA biogenesis

Chen

Wang

McMonechy

et al. 2015

The Journal of Pathology

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The epithelial splicing regulator ESRP2 is epigenetically repressed by DNA hypermethylation in Wilms tumour and acts as a tumour suppressor

Legge

Moriarty

et al. 2021

Molecular Oncology

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Wilms tumour (WT), an embryonal kidney cancer, has been extensively characterised for genetic and epigenetic alterations, but a proportion of WTs still lack identifiable abnormalities. To uncover DNA methylation changes critical for WT pathogenesis, we compared the epigenome of foetal kidney with two WT cell lines, filtering our results to remove common cancer‐associated epigenetic changes and to enrich for genes involved in early kidney development. This identified four hypermethylated genes, of which ESRP2 (epithelial splicing regulatory protein 2) was the most promising for further study. ESRP2 was commonly repressed by DNA methylation in WT, and this occurred early in WT development (in nephrogenic rests). ESRP2 expression was reactivated by DNA methyltransferase inhibition in WT cell lines. When ESRP2 was overexpressed in WT cell lines, it inhibited cellular proliferation in vitro, and in vivo it suppressed tumour growth of orthotopic xenografts in nude mice. RNA‐seq of the ESRP2‐expressing WT cell lines identified several novel splicing targets. We propose a model in which epigenetic inactivation of ESRP2 disrupts the mesenchymal to epithelial transition in early kidney development to generate WT.

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Reduced DICER1 Expression Bestows Rheumatoid Arthritis Synoviocytes Proinflammatory Properties and Resistance to Apoptotic Stimuli

Alsaleh

Nehmar

Blüml

et al. 2016

Arthritis & Rheumatology

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Objective While the regulatory role of individual microRNAs (miRNAs) in rheumatoid arthritis (RA) is well established, the role of DICER1 in the pathogenesis of the disease has not yet been investigated. The purpose of this study was to analyze the expression of factors involved in miRNA biogenesis in fibroblast‐like synoviocytes (FLS) from RA patients and to monitor the arthritis triggered by K/BxN serum transfer in mice deficient in the Dicer gene (Dicerd/d). Methods The expression of genes and precursor miRNAs was quantified by quantitative reverse transcription–polymerase chain reaction (qRT‐PCR). MicroRNA macroarray profiling was monitored by qRT‐PCR. Cytokines were quantified by enzyme‐linked immunosorbent assay. Experimental arthritis in mice was achieved by the transfer of serum from K/BxN donors. Apoptosis was quantified using an enzyme‐linked immunosorbent assay. Results We found decreased DICER1 and mature miRNA expression in synovial fibroblasts from RA patients. These cells were hyperresponsive to lipopolysaccharide, as evidenced by their increased interleukin‐6 secretion upon stimulation. Experimental serum‐transfer arthritis in Dicerd/d mice confirmed that an unbalanced biogenesis of miRNAs correlated with an enhanced inflammatory response. Synoviocytes from both RA patients and Dicerd/d mice exhibited increased resistance to apoptotic stimuli. Conclusion The findings of this study further substantiate the important role of DICER1 in the maintenance of homeostasis and the regulation of inflammatory responses.

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Biallelic DICER1 mutations occur in Wilms tumours

Cited by 128 publications

References 57 publications

Recurrent DICER1 hotspot mutations in endometrial tumours and their impact on microRNA biogenesis

Recurrent DICER1 hotspot mutations in endometrial tumours and their impact on microRNA biogenesis

The epithelial splicing regulator ESRP2 is epigenetically repressed by DNA hypermethylation in Wilms tumour and acts as a tumour suppressor

Reduced DICER1 Expression Bestows Rheumatoid Arthritis Synoviocytes Proinflammatory Properties and Resistance to Apoptotic Stimuli

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