Reliable Identification of Endometrial Precancers Through Combined Pax2, β-Catenin, and Pten Immunohistochemistry

Aguilar, Mitzi; Chen, Hao; Rivera-Colón, Glorimar; Niu, Shuang; Carrick, Kelley; Gwin, Katja; Cuevas, Ileana; Sahoo, Subhransu S.; Li, Hao-Dong; Zhang, Song; Zheng, Wenxin; Lucas, Elena; Castrillón, Diego H.

doi:10.1097/pas.0000000000001810

Cited by 30 publications

(56 citation statements)

References 51 publications

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“…However, Pten loss is a relatively poor driver of EMT, as evidenced by a lack of invasive phenotypes in Pten-alone contexts in this study, including live mice, cell lines, and organoids. This is also well-documented in aging human endometrium, where definitive Pten loss occurs in normal or hyperplastic endometrium (i.e., very early in EC progression, well before the acquisition of invasive phenotypes) ( 24 , 70 , 71 ). In contrast, in our studies, Foxa2 inhibited cell cycle progression via Myc, albeit modestly, confirming that it is a multitasking tumor suppressor with diverse biological roles, but with a much more potent effect as an EMT suppressor, as evidenced by upregulation of EMT factors and the striking pro-invasive/pro-metastatic phenotypes observed in the live animal and human/mouse cell line and organoid systems.…”

Section: Discussionmentioning

confidence: 73%

FOXA2 suppresses endometrial carcinogenesis and epithelial-mesenchymal transition by regulating enhancer activity

Sahoo¹,

Ramanand²,

Gao³

et al. 2022

Journal of Clinical Investigation

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FOXA2 encodes a transcription factor mutated in 10% of endometrial cancers (ECs), with a higher mutation rate in aggressive variants. FOXA2 has essential roles in embryonic and uterine development. However, FOXA2’s role in EC is incompletely understood. Functional investigations using human and mouse EC cell lines revealed that FOXA2 controls endometrial epithelial gene expression programs regulating cell proliferation, adhesion, and endometrial-epithelial transition. In live animals, conditional inactivation of Foxa2 or Pten alone in endometrial epithelium did not result in ECs, but simultaneous inactivation of both genes resulted in lethal ECs with complete penetrance, establishing potent synergism between Foxa2 and PI3K signaling. Studies in tumor-derived cell lines and organoids highlighted additional invasion and cell growth phenotypes associated with malignant transformation and identified key mediators, including Myc and Cdh1 . Transcriptome and cistrome analyses revealed that FOXA2 broadly controls gene expression programs through modification of enhancer activity in addition to regulating specific target genes, rationalizing its tumor suppressor functions. By integrating results from our cell lines, organoids, animal models, and patient data, our findings demonstrated that FOXA2 is an endometrial tumor suppressor associated with aggressive disease and with shared commonalities among its roles in endometrial function and carcinogenesis.

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Section: Discussionmentioning

confidence: 73%

FOXA2 suppresses endometrial carcinogenesis and epithelial-mesenchymal transition by regulating enhancer activity

Sahoo¹,

Ramanand²,

Gao³

et al. 2022

Journal of Clinical Investigation

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“…Briefly, when absence of staining was observed in ≥5% of lesional glands, PAX2 and PTEN were interpreted as lost. The cutoff is based on our previous observation that nonspecific PAX2 and PTEN loss in normal endometrium do not exceed 5% of the endometrial glands 29. The presence of strong, unequivocal nuclear staining with β-catenin in lesional glands, even when focal, was interpreted as positive/abnormal.…”

Section: Methodsmentioning

confidence: 99%

“…When tumor glands showed confluence, a diagnosis of EEC was rendered. Information regarding interpretation of β-catenin, PAX2 and PTEN was detailed and further reviewed in our recent publication 29,31. Briefly, when absence of staining was observed in ≥5% of lesional glands, PAX2 and PTEN were interpreted as lost.…”

Section: Methodsmentioning

confidence: 99%

“…IHC for PAX2, PTEN, and β-catenin was performed in the Parkland Hospital clinical laboratory on a DAKO Autostainer Link 48 instrument, following protocols previously validated for clinical testing. 29 The following primary antibodies were used: β-catenin (prediluted, clone β-catenin-1, #IR70261-2; Agilent), PAX2 (prediluted, clone EP235, #BSB2567; Cancer Diagnostics, Durham, NC), PTEN (prediluted, clone 6H2.1, #PM278AA; BioCare, Pacheco, CA), p40 (prediluted, clone Poly.Rb; BioCare, Pacheco, CA) and CD10 (prediluted, clone 56C6; Dako). High pH (50× Tris/ EDTA buffer, pH 9) solution was used for antigen retrieval.…”

Section: Immunohistochemistrymentioning

confidence: 99%

“…To investigate the relationship between the presence of morules and β-catenin status in AH/EIN, we divided all cases into groups with and without morules, and studied the expression pattern of β-catenin in the glandular component of AH/EIN and/or EEC in those 2 groups. The status of 2 other markers shown to often aberrant in AH/ EIN, PAX2, and PTEN, 29 were also examined in comparison. The normal and aberrant expression of the 3 markers is illustrated in Figure 2.…”

Section: Morules Are a Reliable Indicator Of β-Catenin Aberrant Expre...mentioning

confidence: 99%

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Morules But Not Squamous Differentiation are a Reliable Indicator of CTNNB1 (β-catenin) Mutations in Endometrial Carcinoma and Precancers

Niu

Lucas

Molberg

et al. 2022

American Journal of Surgical Pathology

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Although collectively regarded as "squamous differentiation (SD)" in endometrial endometrioid carcinoma (EEC) and atypical hyperplasia/endometrioid intraepithelial neoplasia (AH/EIN), morules (often referred to as "squamous morules") and true SD may represent two distinct phenomena. Here, we explored the distinction between morules versus SD and investigated the association of morules and SD with CTNNB1 mutations. A total of 270 cases of EEC and AH/EIN were studied, including EEC with (n = 36) or without (n = 36) morules and AH/ EIN with (n = 80) or without (n = 118) morules. Cases were analyzed by immunohistochemistry and selected cases (n = 20) by targeted next-generation sequencing panel. Near-perfect agreement was found between morules and glandular β-catenin nuclear staining in AH/EIN and EEC. A strong positive association was found between morules and glandular β-catenin nuclear staining (P < 0.0001, Φ = 0.59 in AH/EIN; P < 0.0001, Φ = 0.85 in EEC). There was no association between (1) morules and glandular PAX2 or PTEN aberrant expression or (2) SD and aberrant expression of β-catenin, PAX2 or PTEN (Φ = 0.09, β-catenin; Φ = 0.16, PAX2; Φ = 0.13, PTEN). CTNNB1 mutations were identified in all 20 selected morule-containing cases (100%). Next-generation sequencing was performed on 2 (preprogestin and postprogestin treatment) biopsies from 1 patient, revealing identical mutational profile in morules and glands. In conclusion, (1) SD and morules are distinct biological phenomena; (2) the presence of morules, but not SD, is a reliable indicator of CTNNB1 mutations in EEC and AH/EIN. Our findings demonstrate that SD and morules are distinct biological phenomena. Since morules but not SD are associated with β-catenin mutations, the distinction is clinically relevant and should be included in diagnostic reports.

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Mesonephric‐type adenocarcinomas of the ovary: prevalence, diagnostic reproducibility, outcome, and value of PAX2

Köbel,

Kang,

Lee

et al. 2024

The Journal of Pathology CR

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Mesonephric‐type (or ‐like) adenocarcinomas (MAs) of the ovary are an uncommon and aggressive histotype. They appear to arise through transdifferentiation from Müllerian lesions creating diagnostic challenges. Thus, we aimed to develop a histologic and immunohistochemical (IHC) approach to optimize the identification of MA over its histologic mimics, such as ovarian endometrioid carcinoma (EC). First, we screened 1,537 ovarian epithelial neoplasms with a four‐marker IHC panel of GATA3, TTF1, ER, and PR followed by a morphological review of EC to identify MA in retrospective cohorts. Interobserver reproducibility for the distinction of MA versus EC was assessed in 66 cases initially without and subsequently with IHC information (four‐marker panel). Expression of PAX2, CD10, and calretinin was evaluated separately, and survival analyses were performed. We identified 23 MAs from which 22 were among 385 cases initially reported as EC (5.7%) and 1 as clear cell carcinoma. The interobserver reproducibility increased from fair to substantial (κ = 0.376–0.727) with the integration of the four‐marker IHC panel. PAX2 was the single most sensitive and specific marker to distinguish MA from EC and could be used as a first‐line marker together with ER/PR and GATA3/TTF1. Patients with MA had significantly increased risk of earlier death from disease (hazard ratio = 3.08; 95% CI, 1.62–5.85; p < 0.0001) compared with patients with EC, when adjusted for age, stage, and p53 status. A diagnosis of MA has prognostic implications for stage I disease, and due to the subtlety of morphological features in some tumors, a low threshold for ancillary testing is recommended.

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Reliable Identification of Endometrial Precancers Through Combined Pax2, β-Catenin, and Pten Immunohistochemistry

Cited by 30 publications

References 51 publications

FOXA2 suppresses endometrial carcinogenesis and epithelial-mesenchymal transition by regulating enhancer activity

FOXA2 suppresses endometrial carcinogenesis and epithelial-mesenchymal transition by regulating enhancer activity

Morules But Not Squamous Differentiation are a Reliable Indicator of CTNNB1 (β-catenin) Mutations in Endometrial Carcinoma and Precancers

Mesonephric‐type adenocarcinomas of the ovary: prevalence, diagnostic reproducibility, outcome, and value of PAX2

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