Molecular Analysis of Mixed Endometrial Carcinomas Shows Clonality in Most Cases

Köbel, Martin; Meng, Bo; Hoang, Lien; Almadani, Noorah; Li, Xiaodong; Soslow, Robert A.; Gilks, C. Blake; Lee, Cheng‐Han

doi:10.1097/pas.0000000000000536

Cited by 52 publications

(36 citation statements)

References 40 publications

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“…However, in our study we assigned those cases to either the endometrioid or the clear cell type, depending on the predominant morphology, assisted by IHC (see ). Similarly, we recently demonstrated that four of five ‘mixed’ endometrial clear cell–endometrioid carcinomas had dMMR . Regarding the question of which clear cell carcinomas may be selected for dMMR testing, we cannot present a reliable age cut‐off, but our patients were aged 48–55 years (perhaps <60 years).…”

Section: Discussionmentioning

confidence: 86%

Significant frequency of MSH2/MSH6 abnormality in ovarian endometrioid carcinoma supports histotype‐specific Lynch syndrome screening in ovarian carcinomas

et al. 2016

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Section: Discussionmentioning

confidence: 86%

Significant frequency of MSH2/MSH6 abnormality in ovarian endometrioid carcinoma supports histotype‐specific Lynch syndrome screening in ovarian carcinomas

et al. 2016

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“…In a single case there was failure to sample a dedifferentiated component of a tumor in the biopsy, a rare EC variant associated with mutations in chromatin remodelling genes and frequent MMR protein [34, 35]. In theory, mixed carcinomas may also pose a challenge to classify using ProMiSE, however, truly biologically mixed tumors are exceptionally rare [36] and most cases diagnosed as mixed carcinoma are actually due to morphologic ambiguity rather than admixtures of molecularly distinct clones [37]. …”

Section: Discussionmentioning

confidence: 99%

Molecular classification of endometrial carcinoma on diagnostic specimens is highly concordant with final hysterectomy: Earlier prognostic information to guide treatment

Talhouk

Hoang

McConechy

et al. 2016

Gynecologic Oncology

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Objective Categorization and risk stratification of endometrial carcinomas is inadequate; histomorphologic assessment shows considerable interobserver variability, and risk of metastases and recurrence can only be derived after surgical staging. We have developed a Proactive Molecular Risk classification tool for Endometrial cancers (ProMisE) that identifies four distinct prognostic subgroups. Our objective was to assess whether molecular classification could be performed on diagnostic endometrial specimens obtained prior to surgical staging and its concordance with molecular classification performed on the subsequent hysterectomy specimen. Methods Sequencing of tumors for exonuclease domain mutations (EDMs) in POLE and immunohistochemistry for mismatch repair (MMR) proteins and p53 were applied to both pre- and post-staging archival specimens from 60 individuals to identify four molecular subgroups: MMR-D, POLE EDM, p53 wild type, p53 abn(abnormal). Three gynecologic subspecialty pathologists assigned histotype and grade to a subset of samples. Concordance of molecular and clinicopathologic subgroup assignments were determined, comparing biopsy/curetting to hysterectomy specimens. Results Complete molecular and pathologic categorization was achieved in 57 cases. Concordance metrics for pre- vs. post-staging endometrial samples categorized by ProMisE were highly favorable; average per ProMisE class sensitivity(0.9), specificity(0.96), PPV(0.9), NPV(0.96) and kappa statistic 0.86(95%CI, 0.72-0.93), indicating excellent agreement. We observed the highest level of concordance for ‘p53 abn’ tumors, the group associated with the worst prognosis. In contrast, grade and histotype assignment from original pathology reports pre- vs. post-staging showed only moderate levels of agreement (kappa=0.55 and 0.44 respectively); even with subspecialty pathology review only moderate levels of agreement were observed. Conclusion Molecular classification can be achieved on diagnostic endometrial samples and accurately predicts the molecular features in the final hysterectomy specimens, demonstrating concordance superior to grade and histotype . This biologically relevant information, available at initial diagnosis, has the potential to inform management (surgery, adjuvant therapy) from the earliest time point in cancer care.

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“…Fundamental features of the immunophenotype for dedifferentiated, clear cell, and mixed carcinomas have been reported [50, 54, 109–111]. Assessment of mixed tumors show that despite morphologic differences/mimicry, the majority of molecular aberrations are shared across the tumor [112]. Thus the application of ProMisE or Leiden classification systems to these cancers may be of value.…”

Section: Rare Histotypes and Diversity Within Tumorsmentioning

confidence: 99%

New classification of endometrial cancers: the development and potential applications of genomic-based classification in research and clinical care

Talhouk

McAlpine

2016

gynaecol oncol res pract

159

157

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Endometrial carcinoma (EC) is the fourth most common cancer in women in the developed world. Classification of ECs by histomorphologic criteria has limited reproducibility and better tools are needed to distinguish these tumors and enable a subtype-specific approach to research and clinical care. Based on the Cancer Genome Atlas, two research teams have developed pragmatic molecular classifiers that identify four prognostically distinct molecular subgroups. These methods can be applied to diagnostic specimens (e.g., endometrial biopsy) with the potential to completely change the current risk stratification systems and enable earlier informed decision making. The evolution of genomic classification in ECs is shared herein, as well as potential applications and discussion of the essential research still needed in order to optimally integrate molecular classification in to current standard of care.

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Molecular Analysis of Mixed Endometrial Carcinomas Shows Clonality in Most Cases

Cited by 52 publications

References 40 publications

Significant frequency of MSH2/MSH6 abnormality in ovarian endometrioid carcinoma supports histotype‐specific Lynch syndrome screening in ovarian carcinomas

Significant frequency of MSH2/MSH6 abnormality in ovarian endometrioid carcinoma supports histotype‐specific Lynch syndrome screening in ovarian carcinomas

Molecular classification of endometrial carcinoma on diagnostic specimens is highly concordant with final hysterectomy: Earlier prognostic information to guide treatment

New classification of endometrial cancers: the development and potential applications of genomic-based classification in research and clinical care

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