Incorporation of molecular characteristics into endometrial cancer management

Vermij, Lisa; Smit, Vincent T.H.B.M.; Nout, Remi A.; Bosse, Tjalling

doi:10.1111/his.14015

Cited by 179 publications

(132 citation statements)

References 79 publications

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“…According to recent studies, MSI-H/hypermutated tumors which include Lynch syndrome cancers and are represented by loss of MMR (Mismatch Repair) through hypermethylation of one of MMR proteins, comprise 25-30% of endometrial carcinomas [15]. Our study revealed a significant percentage of MSI-H tumors (68%) diagnosed by evaluating loss of MSH6 and/or PMS2 expression, which contradicts various research performed on much larger cohorts [8,15,16]. Other parameters of our study correlated with this molecular subgroup similarly with other conducted studies: higher-grade ECs, endometrioid-type histology, moderate/marked TILs, substantial LVSI [8].…”

Section: Resultscontrasting

confidence: 88%

“…Our study revealed a significant percentage of MSI-H tumors (68%) diagnosed by evaluating loss of MSH6 and/or PMS2 expression, which contradicts various research performed on much larger cohorts [8,15,16]. Other parameters of our study correlated with this molecular subgroup similarly with other conducted studies: higher-grade ECs, endometrioid-type histology, moderate/marked TILs, substantial LVSI [8].…”

Section: Resultscontrasting

confidence: 79%

“…This particular molecular subgroup has no specific molecular incriminated driver [19]. Although this largely represented subclass is defined by a low mutational burden, there are numerous studies that show that these have an aggressive clinical behavior [8,18]. Studies show a 65% percentage of this group, but our cohort shows a much higher percentage (74%).…”

Section: Resultsmentioning

confidence: 67%

“…56% of cases presented with moderate TILs (tumor-infiltrating lymphocytes). Vermij et al [7,8] proved that LVSI in EC patients is connected with an increased risk of lymph node metastasis, locoregional as well as distant recurrences, regardless of stage and histotype. For that matter, LVSI will remain essential in risk stratification schemes, escalating adjuvant treatment regimens in those patients with substantial LVSI.…”

Section: Resultsmentioning

confidence: 99%

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Molecular Subgroups of Endometrial Carcinoma in Romanian Patients

Evsei¹,

Birceanu-Corobea²,

Csonka³

et al. 2020

Rev. Chim.

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Molecular classification of endometrial carcinoma (EC) has represented a breakthrough ever since the TCGA (The Cancer Genome Atlas) project published it in 2013. Four distinct molecular subgroups were recognized based on somatic copy number alterations and tumor mutational burden: POLE (polymerase-epsilon) ultramutated, MSI (microsatellite instability) hypermutated (MSI-H), copy number low (CNL) and copy number high (CNH). However, implementing a standardized algorithm in current practice is far from being definitive. Our purpose in this study was to determine different molecular subgroups in a cohort of Romanian patients using cost effective and available immuno-histochemistry markers and outline statistical associations with different parameters. Tissue microarrays encompassing 50 cases with previously diagnosed ECs were tested for ER, PR, HER2, p53, MSH6 and PMS2 and results showed 68% MSI-H cases with statistical correlation with tumor size ] 2 cm (p=0.028) and no association with overall survival. CNH ECs were reported in 26% of cases and showed important statistical significance with TILs (p=0.041) and no correlations with overall survival. The CNL subgroup was reported in 74% of ECs cases and showed statistical significance with the histopathological subtype (p=0.006), pT (removal of primary tumor according to AJCC/UICC convention) (p=0.033), risk category according to ESMO (European Society of Medical Oncology) criteria (p=0.022) and ER expression (p=0.002). Five-year overall survival was 84%. Molecular classification is an important additional tool in current pathology guidelines for reporting ECs, but it is not currently standardized or available in all laboratories. Its importance in evolving treatment strategies for this disease is well documented so we strongly recommend routine testing for molecular prognostic factors.

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Section: Resultscontrasting

confidence: 88%

Section: Resultscontrasting

confidence: 79%

Section: Resultsmentioning

confidence: 67%

Section: Resultsmentioning

confidence: 99%

See 2 more Smart Citations

Molecular Subgroups of Endometrial Carcinoma in Romanian Patients

Evsei¹,

Birceanu-Corobea²,

Csonka³

et al. 2020

Rev. Chim.

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“…Treatment of EC is usually surgical (hysterectomy and bilateral salpingo-oophorectomy), although a significant minority are offered conservative management in the form of hormonal manipulations, especially women of childbearing age who wish to preserve their fertility [9]. Decisions about adjuvant chemotherapy and radiotherapy are currently based on traditional pathological parameters that lack precision and therefore deny some women with biologically aggressive disease the opportunity to receive life-saving treatments whilst exposing others to unnecessary harms [5,22]. There is, at present, limited evidence to support the routine use of imaging or biochemical testing in the follow-up for EC due mainly to the lack of reliable monitoring tools [5].…”

Section: Introductionmentioning

confidence: 99%

Metabolomic Biomarkers for Detection, Prognosis and Identifying Recurrence in Endometrial Cancer

et al. 2020

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Metabolic reprogramming is increasingly recognised as one of the defining hallmarks of tumorigenesis. There is compelling evidence to suggest that endometrial cancer develops and progresses in the context of profound metabolic dysfunction. Whilst the incidence of endometrial cancer continues to rise in parallel with the global epidemic of obesity, there are, as yet, no validated biomarkers that can aid risk prediction, early detection, prognostic evaluation or surveillance. Advances in high-throughput technologies have, in recent times, shown promise for biomarker discovery based on genomic, transcriptomic, proteomic and metabolomic platforms. Metabolomics, the large-scale study of metabolites, deals with the downstream products of the other omics technologies and thus best reflects the human phenotype. This review aims to provide a summary and critical synthesis of the existing literature with the ultimate goal of identifying the most promising metabolite biomarkers that can augment current endometrial cancer diagnostic, prognostic and recurrence surveillance strategies. Identified metabolites and their biochemical pathways are discussed in the context of what we know about endometrial carcinogenesis and their potential clinical utility is evaluated. Finally, we underscore the challenges inherent in metabolomic biomarker discovery and validation and provide fresh perspectives and directions for future endometrial cancer biomarker research.

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Application of NGS molecular classification in the diagnosis of endometrial carcinoma: A supplement to traditional pathological diagnosis

Rao

Liao

et al. 2022

Cancer Medicine

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Objective: This study aims to demonstrate the advantages of NGS molecular classification in EC diagnosis and to assess whether molecular classification could be performed on curettage specimens and its concordance with subsequent hysterectomy specimens.Methods: 80 patients with hysterectomy specimens and 35/80 patients with paired curettage specimens were stratified as POLE mut, MSI-H, TP53 wt, or TP53 abn group by NGS panel. Histotype, tumor grade, IHC results, and other pathological details were taken from original pathological reports. Results:The correlation analysis of 80 patients with hysterectomy specimens between NGS molecular classification and clinicopathological characters displayed that the POLE mut group was associated with EEC (87.5%) and TP53 abn subtype was correlated to a later stage (Stage II-IV, 47.6%), G3 (76.2%), serous histology (61.9%) and myometrial invasion ≥50% (47.6%). A favorable concordance (31/32, 96.9%) was shown in MSI analysis and MMR IHC results, and the agreement rate of p53 IHC and TP53 mutation was 81.5% (53/65). Compared with the p53 IHC abnormal group, the TP53 mutation group had a higher correlation with highrisk factors. A high level of concordance (31/35, 88.0%) of NGS molecular classification was achieved between curettage specimens and hysterectomy specimens while grade and histotype (including unclassified group) from curettage specimens and hysterectomy specimens showed only moderate levels of agreement, 54.3% (19/35) and 68.6% (24/35), respectively. Conclusion: NGS molecular classification achieved on curettage samplesshowed high concordance with the final hysterectomy specimens, demonstrating superior to the conventional pathological assessment of grade and histotype and potential utilization in clinical practice. | METHODS | Patient cohort, sample collection, and pathological information collectionThe study consists of a retrospective cohort of patients with EC from Sun Yat-Sen Memorial Hospital, Sun Yat-Sun University treated for EC between 2018 and 2021.

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Incorporation of molecular characteristics into endometrial cancer management

Cited by 179 publications

References 79 publications

Molecular Subgroups of Endometrial Carcinoma in Romanian Patients

Molecular Subgroups of Endometrial Carcinoma in Romanian Patients

Metabolomic Biomarkers for Detection, Prognosis and Identifying Recurrence in Endometrial Cancer

Application of NGS molecular classification in the diagnosis of endometrial carcinoma: A supplement to traditional pathological diagnosis

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