High-grade serous ovarian cancer arises from fallopian tube in a mouse model

Kim, Jaeyeon; Coffey, Donna; Creighton, Chad J.; Yu, Zhifeng; Hawkins, Shannon M.; Matzuk, Martin M.

doi:10.1073/pnas.1117135109

Cited by 342 publications

(328 citation statements)

References 41 publications

(47 reference statements)

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“…It is now believed that dissemination of serous cancers may occur by exfoliation of tumor cells originating from the distally located TICs (reviewed in [7]). Recent mouse models have shown transformation of human and mouse fallopian tube tissue into serous cancers through multiple genetic mutations [35,37]. These data suggest that serous cancers may arise from the fallopian tube.…”

Section: Discussionmentioning

confidence: 85%

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Stem‐Like Epithelial Cells Are Concentrated in the Distal End of the Fallopian Tube: A Site for Injury and Serous Cancer Initiation

et al. 2012

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Section: Discussionmentioning

confidence: 85%

“…The FTE is actively being explored as a site of initiation for serous cancers [35][36][37]. Dysplastic lesions identified typically in the distal end of the fallopian tube have been hypothesized to be precursor lesions for invasive serous cancers [38][39][40][41].…”

Section: Ftescs Are Expanded In the Fallopian Tube Epithelium Of Patimentioning

confidence: 99%

Stem‐Like Epithelial Cells Are Concentrated in the Distal End of the Fallopian Tube: A Site for Injury and Serous Cancer Initiation

et al. 2012

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“…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%

“…We identified an atypical hotspot mutation, G1809R, which is immediately adjacent to the metal-binding residue D1810, and characterized its functional impact on miRNAs and downstream signalling pathways. Using a Dicer1-null mouse fallopian tube carcinoma-derived cell line [17], we demonstrated that DICER1 hotspot mutations abolish the inhibitory effects of DICER1 on cell proliferation. Our data also suggested that loss of let-7 family miRNAs may contribute to the oncogenic properties of DICER1 hotspot mutations.…”

Section: J Chen Et Almentioning

confidence: 96%

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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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In Utero Exposure to Benzo[a]pyrene Induces Ovarian Mutations at Doses That Deplete Ovarian Follicles in Mice

Luderer

Meier

Lawson

et al. 2018

Environ and Mol Mutagen

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Polycyclic aromatic hydrocarbons like benzo[a]pyrene (BaP) are ubiquitous environmental contaminants formed during incomplete combustion of organic materials. Our prior work showed that transplacental exposure to BaP depletes ovarian follicles and increases prevalence of epithelial ovarian tumors later in life. We used the MutaMouse transgenic rodent model to address the hypothesis that ovarian mutations play a role in tumorigenesis caused by prenatal exposure to BaP. Pregnant MutaMouse females were treated with 0, 10, 20, or 40 mg/(kg day) BaP orally on gestational days 7–16, covering critical windows of ovarian development. Female offspring were euthanized at 10 weeks of age; some ovaries with oviducts were processed for follicle counting; other ovaries/oviducts and bone marrow were processed for determination of lacZ mutant frequency (MF). Mutant plaques were pooled within dose groups and sequenced to determine the mutation spectrum. BaP exposure caused highly significant dose‐related decreases in ovarian follicles and increases in ovarian/oviductal and bone marrow mutant frequencies at all doses. Absence of follicles, cell packets, and epithelial tubular structures were observed with 20 and 40 mg/(kg day) BaP. Depletion of ovarian germ cells was inversely associated with ovarian MF. BaP induced primarily G > T and G > C transversions and deletions in ovaries/oviducts and bone marrow cells and produced a mutation signature highly consistent with that of tobacco smoking in human cancers. Overall, our results show that prenatal BaP exposure significantly depletes ovarian germ cells, causes histopathological abnormalities, and increases the burden of ovarian/oviductal mutations, which may be involved in pathogenesis of epithelial ovarian tumors. Environ. Mol. Mutagen. 60:410–420, 2019. © 2018 Her Majesty the Queen in Right of Canada

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High-grade serous ovarian cancer arises from fallopian tube in a mouse model

Cited by 342 publications

References 41 publications

Stem‐Like Epithelial Cells Are Concentrated in the Distal End of the Fallopian Tube: A Site for Injury and Serous Cancer Initiation

Stem‐Like Epithelial Cells Are Concentrated in the Distal End of the Fallopian Tube: A Site for Injury and Serous Cancer Initiation

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

In Utero Exposure to Benzo[a]pyrene Induces Ovarian Mutations at Doses That Deplete Ovarian Follicles in Mice

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