Serial genomic analysis of endometrium supports the existence of histologically indistinct endometrial cancer precursors

Aguilar, Mitzi; Zhang, He; Zhang, Musi; Cantarell, Brandi; Sahoo, Subhransu S.; Li, Hao-Dong; Cuevas, Ileana; Lea, Jayanthi; Miller, David S.; Chen, Hao; Zheng, Wenxin; Gagan, Jeffrey; Lucas, Elena; Castrillón, Diego H.

doi:10.1002/path.5628

Cited by 13 publications

(36 citation statements)

References 64 publications

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“…This number is comparable to a recent serial genomic analysis of endometrial cancer progression, where next generation sequencing-directed immunohistochemistry found that 86% of endometrial cancers were aberrant for at least 1 of the 5 non-Pax2 markers, with persistence of AH/EIN marker patterns in samples from each patient. 37 Conversely, since 7.2% of bona fide AH/EIN were not aberrant for any of these markers, lack of aberrancy of all 3 should not dissuade from a diagnosis of AH/EIN when definitive histologic features are present.…”

Section: Discussionmentioning

confidence: 98%

“… 14 This likely reflects a sequential acquisition of mutations that characterize clonal outgrowth in early endometrial neoplasia. 19 , 37 …”

Section: Discussionmentioning

confidence: 99%

“… 53 β-Catenin patterns are also likely to be recapitulated following treatment. 37 Thus, in addition to facilitating the initial diagnosis of AH/EIN, establishment of baseline expression patterns should be useful diagnostically in follow-up biopsies in the setting of progestin treatment. Although this study provides critical information regarding patterns of marker aberrance and panel performance in definitive AH/EIN, additional investigations will be needed to determine the incidence and patterns of marker aberrance in mimics of AH/EIN, including endometrial polyps, disordered proliferative endometrium, or non-AH.…”

Section: Discussionmentioning

confidence: 99%

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

Aguilar¹,

Chen²,

Rivera-Colón³

et al. 2021

American Journal of Surgical Pathology

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The diagnosis of endometrial atypical hyperplasia/endometrioid intraepithelial neoplasia (AH/EIN) remains challenging and subjective in some cases, with variable histologic criteria and differences of opinion among gynecologic pathologists, potentially leading to under/overtreatment. There has been growing interest in the use of specific immunohistochemical markers as adjuncts in AH/EIN diagnosis. For example, the World Health Organization 2020 Classification specifies that loss of Pten, Pax2, or mismatch repair proteins are desirable diagnostic criteria. Other markers, most notably β-catenin and Ari-d1a, are also aberrantly expressed in some AH/EIN. However, the performance of some markers individually-and more importantly as a group-has not been rigorously explored, raising questions as to which marker(s) or combination(s) is the most effective in practice. Formalin-fixed paraffin-embedded tissue sections from AH/EIN cases (n = 111) were analyzed by immunohistochemistry for 6 markers: Pax2, Pten, Mlh1, β-catenin, Arid1a, and p53. Aberrant expression was tabulated for each case and marker. An additional set of normal endometria (n = 79) was also analyzed to define optimal diagnostic criteria for marker aberrance. The performance characteristics of each marker, the entire panel, and subsets thereof were quantitatively and statistically analyzed. In order of number of cases detected, the most frequently aberrant markers in AH/EIN were Pax2 (81.1% of cases), Pten (50.5%), β-catenin (47.7%), Arid1a (7.2%), Mlh1 (4.5%), and p53 (2.7%). The majority of cases showed aberrant expression of ≥ 2 markers. All 6 markers together identified 92.8% of cases. Arid1a, Mlh1, and p53 were robust and readily scored markers, but all cases showing aberrant expression of these 3 markers were also detected by Pax2, Pten, or β-catenin. A focused panel of only 3 markers (Pax2, Pten, and β-catenin) showed optimal performance characteristics as a diagnostic adjunct in the histopathologic diagnosis of AH/EIN. Use of this panel is practicable and robust, with at least 1 of the 3 markers being aberrant in 92.8% of AH/EIN.

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Section: Discussionmentioning

confidence: 98%

“… 14 This likely reflects a sequential acquisition of mutations that characterize clonal outgrowth in early endometrial neoplasia. 19 , 37 …”

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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

Aguilar¹,

Chen²,

Rivera-Colón³

et al. 2021

American Journal of Surgical Pathology

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“…In endometrial hyperplasia, PTEN and KRAS have been reported to have mutations frequently. [8][9][10][11][12][13] In addition, recent studies using next generation sequencer revealed many driver gene mutations in atypical hyperplasia and even in normal endometrial glands. [13][14][15][16] Li et al analyzed formalin-fixed paraffin embedded tissue with a diagnosis of atypical endometrial hyperplasia and found frequent mutations in driver genes, including PTEN, ARID1A, CTNNB1, KRAS, and PIK3CA.…”

Section: Molecular Profile Of Endometrial Lesionsmentioning

confidence: 99%

Diagnostic value of endometrial cytology and related technology

Munakata

2022

Diagnostic Cytopathology

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Background Endometrial cytology is not much popular in the world, but is commonly used in a few countries. Although cytomorphological evaluation of endometrial cytology is complicating, recent advance in technology helps improve diagnostic accuracy. In addition, new reporting system, The Yokohama System, has been introduced as a standard reporting system resembling The Bethesda System of the uterine cervical cytology. Although sample standardization is one of the causes in diagnostic problem, it was solved by liquid‐based cytology (LBC) technology. In addition, standardized diagnostic algorithm by cytomorphological assessment of LBC samples, the Osaki Study Group (OSG) method, was recently proposed as a reliable and reproducible method. LBC can be utilized for ancillary methods. Application of immunocytochemistry and molecular technology on endometrial cytology samples has been studied to improve diagnostic accuracy. Recent progress of molecular technology has revealed many driver gene mutations in endometrial cancer and its precursors. Surprisingly, many studies revealed that even normal endometrial tissue had driver gene mutations. Conclusion Based on the recent advance in knowledge of molecular profile of endometrial lesions and normal endometrial tissue, endometrial cytology will gain much power in clinical usefulness.

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“…It is important to note that these mutations were confirmed in the invasive cancer. This research provided unique insights into precancer initiation and progression and clearly demonstrated the existence of endometrial premalignant lesions with definitive mutations not readily identifiable by histology [ 100 ]. These findings are also supported by a case report in which tumor-specific mutations were identified in an asymptomatic individual without clinical or pathologic evidence of cancer nearly one year before symptoms developed, i.e., postmenopausal bleeding and a single microscopic focus of EC diagnosed at the time of hysteroscopy [ 101 ].…”

Section: Endometrial Precancerous Lesions and Early-stage Endometrial Cancermentioning

confidence: 99%

New Trends in the Detection of Gynecological Precancerous Lesions and Early-Stage Cancers

Holcakova

Bartošík

Anton

et al. 2021

Cancers

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The prevention and early diagnostics of precancerous stages are key aspects of contemporary oncology. In cervical cancer, well-organized screening and vaccination programs, especially in developed countries, are responsible for the dramatic decline of invasive cancer incidence and mortality. Cytological screening has a long and successful history, and the ongoing implementation of HPV triage with increased sensitivity can further decrease mortality. On the other hand, endometrial and ovarian cancers are characterized by a poor accessibility to specimen collection, which represents a major complication for early diagnostics. Therefore, despite relatively promising data from evaluating the combined effects of genetic variants, population screening does not exist, and the implementation of new biomarkers is, thus, necessary. The introduction of various circulating biomarkers is of potential interest due to the considerable heterogeneity of cancer, as highlighted in this review, which focuses exclusively on the most common tumors of the genital tract, namely, cervical, endometrial, and ovarian cancers. However, it is clearly shown that these malignancies represent different entities that evolve in different ways, and it is therefore necessary to use different methods for their diagnosis and treatment.

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Serial genomic analysis of endometrium supports the existence of histologically indistinct endometrial cancer precursors

Cited by 13 publications

References 64 publications

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

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

Diagnostic value of endometrial cytology and related technology

New Trends in the Detection of Gynecological Precancerous Lesions and Early-Stage Cancers

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