A candidate precursor to serous carcinoma that originates in the distal fallopian tube (<b><i>J Pathol</i></b> 2007; 211: 26–35)

Lee, Y; Miron, Alexander; Drapkin, Ronny; Nucci,; Medeiros, Fabíola; Saleemuddin, Aasia; Garber, Judy E.; Birch, Christina M.; Mou, Haiwei; Gordon, R. J.; Dw, Cramer; McKeon, FD; Crum, CP

doi:10.1002/path.2212

Cited by 8 publications

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“…Not surprisingly, no marker in this group separated STINs or HGSCs from SCOUTs. This is in contrast to other published markers such as Ki67, cyclin E, p16, and others, which are significantly more commonly expressed in STINs and HGSCs relative to benign Fallopian tube mucosa .…”

Section: Resultscontrasting

confidence: 93%

“…The serous carcinogenic sequence involves not only frank malignancies with metastatic spread, but also serous cancer precursors, including latent precursors – the p53 signature – and serous tubal intraepithelial neoplasms (STINs). The latter include intramucosal carcinomas (STICs) and lesser but immunophenotypically similar atypias that are considered premalignant intraepithelial lesions (STILs) . Virtually all serous cancer precursors contain mutations in TP53 , evidence of a DNA damage response (γ‐H2AX p ), and predominate in the distal Fallopian tube .…”

Section: Introductionmentioning

confidence: 99%

“…The latter include intramucosal carcinomas (STICs) and lesser but immunophenotypically similar atypias that are considered premalignant intraepithelial lesions (STILs) . Virtually all serous cancer precursors contain mutations in TP53 , evidence of a DNA damage response (γ‐H2AX p ), and predominate in the distal Fallopian tube . Contiguous benign (p53 signatures) and malignant (STICs) epithelia have been documented with shared mutations in specific codons of TP53 .…”

Section: Introductionmentioning

confidence: 99%

“…Virtually all serous cancer precursors contain mutations in TP53 , evidence of a DNA damage response (γ‐H2AX p ), and predominate in the distal Fallopian tube . Contiguous benign (p53 signatures) and malignant (STICs) epithelia have been documented with shared mutations in specific codons of TP53 . In addition, further studies have unearthed other benign epithelial alterations, termed secretory cell outgrowths (SCOUTs), that do not contain TP53 mutations or evidence of a DNA damage response, yet share with precursors and carcinomas loss of PAX2 expression .…”

Section: Introductionmentioning

confidence: 99%

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The PAX2‐null immunophenotype defines multiple lineages with common expression signatures in benign and neoplastic oviductal epithelium

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Bijron

Yamamoto

et al. 2014

The Journal of Pathology

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The oviducts contain high grade serous cancer (HGSC) precursors (serous tubal intraepithelial neoplasia or STINs), which are γ-H2AXp- and TP53 mutation-positive. Although they express wild type p53, secretory cell outgrowths (SCOUTs) are associated with older age and serous cancer; moreover both STINs and SCOUTs share a loss of PAX2 expression (PAX2n). We evaluated PAX2 expression in proliferating adult and embryonic oviductal cells, normal mucosa, SCOUTs, Walthard cell nests (WCNs), STINs and HGSCs, and the expression of genes chosen empirically or from SCOUT expression arrays. Clones generated in vitro from embryonic gynecologic tract and adult fallopian tube were Krt7p/PAX2n/EZH2p and underwent ciliated (PAX2n/EZH2n/FOXJ1p) and basal (Krt7n/EZH2n/Krt5p) differentiation. Similarly non-ciliated cells in normal mucosa were PAX2p but became PAX2n in multilayered epithelium undergoing ciliated or basal (Walthard cell nests or WCN) cell differentiation. PAX2n SCOUTs fell into two groups; Type I were secretory or secretory/ciliated with a “tubal” phenotype and were ALDH1n and β-cateninmem (membraneous only). Type II displayed a columnar to pseudostratified (endometrioid) phenotype, with an EZH2p, ALDH1p, β-cateninnc (nuclear and cytoplasmic), stathminp, LEF1p, RCN1p and RUNX2p expression signature. STINs and HGSCs shared the Type I immunophenotype of PAX2n, ALDH1n, β-cateninmem, but highly expressed EZH2p, LEF1p, RCN1p, and stathminp. This study, for the first time, links PAX2n with proliferating fetal and adult oviductal cells undergoing basal and ciliated differentiation and shows that this expression state is maintained in SCOUTs, STINs and HGSCs. All three entities can demonstrate a consistent perturbation of genes involved in potential tumor suppressor gene silencing (EZH2), transcriptional regulation (LEF1), regulation of differentiation (RUNX2), calcium binding (RCN1) and oncogenesis (stathmin). This shared expression signature between benign and neoplastic entities links normal progenitor cell expansion to abnormal and neoplastic outgrowth in the oviduct and exposes a common pathway that could be a target for early prevention.

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Section: Resultscontrasting

confidence: 93%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The PAX2‐null immunophenotype defines multiple lineages with common expression signatures in benign and neoplastic oviductal epithelium

Ning

Bijron

Yamamoto

et al. 2014

The Journal of Pathology

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“…After removing the fallopian tubes during such surgery, pathologists typically gave them only a cursory look, so the significance of these STIC lesions wasn't clear at first. When Christopher Crum, a pathologist at Brigham and Women's Hospital in Boston, Massachusetts, decided to look at these structures more systematically in the mid-2000s, he and his team found that STIC lesions were widespread in the fallopian tubes of people with ovarian cancer risk genes, especially at the end nearest the ovary 5 . "That was really the 'flip the table' moment," says Ronny Drapkin, a gynaecological pathologist at the University of Pennsylvania in Philadelphia, who worked on Crum's study.…”

Section: Missing Linksmentioning

confidence: 99%

The origins of ovarian cancer

DeWeerdt¹

2021

Nature

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fter Ana Castillo underwent a double mastectomy two years ago, she had one question for her doctors: "What's the next step?"Castillo carries an altered form of a gene known as BRCA2 that makes her 3-5 times more likely than the general population to develop breast cancer, and between 9 and 14 times more likely to get ovarian Risk-reducing surgery to remove the fallopian tubes and ovaries is performed on people with ovarian cancer risk genes, such as BRCA2.

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High-grade fimbrial-ovarian carcinomas are unified by altered p53, PTEN and PAX2 expression

et al. 2010

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High-grade endometrioid and serous carcinomas of the ovary and fallopian tube are responsible for the majority of cancer deaths and comprise a spectrum that includes early or localized (tubal intraepithelial carcinoma) and advanced (invasive or metastatic) disease. We subdivided a series of these tumors into three groups, (1) classic serous, (2) mixed serous and endometrioid and (3) endometrioid carcinomas and determined: (1) the frequencies of coexisting tubal intraepithelial carcinoma, (2) frequency of a dominant ovarian mass suggesting an ovarian origin and (3) immuno-localization of WT-1, p53, PTEN, PAX2 and p16 ink4 . All tumors were analyzed for p53 mutations. Thirty six, 25 and 8% of groups 1-3 were associated with tubal intraepithelial carcinoma (P ¼ 0.09) and 34, 45 and 62% predominated in one ovary (P ¼ 0.028), respectively. Differences in frequencies of diffuse p53 immunostaining (85-93%), WT-1 (70-98%) and p16 ink4 positivity (69-75%) were not significant for all groups. Greater than 95% reduction in PAX2 and PTEN occurred in 67-75 and 5-12%, respectively; however, PAX2 and PTEN staining intensity, when present, was often heterogeneous, highlighting different tumor populations. PAX2 and PTEN expression were markedly reduced or absent in 12 of 12 and 4 of 12 tubal intraepithelial carcinomas. In summary, high-grade mü llerian carcinomas share identical frequencies of altered or reduced expression of p53, PTEN and PAX2, all of which can be appreciated in tubal intraepithelial carcinomas. Because only a subset of these tumors appears to arise in the fallopian tube, attention to expression of these biomarkers in the ovary and other mü llerian sites might facilitate the identification of other carcinogenic pathways. PAX2 and PTEN, in addition to p53 and p16 2-4 Type I tumors are felt to

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A candidate precursor to serous carcinoma that originates in the distal fallopian tube (J Pathol 2007; 211: 26–35)

Cited by 8 publications

References 0 publications

The PAX2‐null immunophenotype defines multiple lineages with common expression signatures in benign and neoplastic oviductal epithelium

The PAX2‐null immunophenotype defines multiple lineages with common expression signatures in benign and neoplastic oviductal epithelium

The origins of ovarian cancer

High-grade fimbrial-ovarian carcinomas are unified by altered p53, PTEN and PAX2 expression

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