A new perspective on Endometrial Carcinoma classification and management strategies in context of molecular subtypes

Pohľad na klasifi káciu a manažment endometriálneho karcinómu v kontexte molekulárnych subtypov

Karcinóm endometria je najčastejším gynekologickým karcinómom a druhým najčastejším ženským zhubným nádorom v rozvinutom svete. Zvyčajne sa diagnostikovaný u žien po menopauze s typickým klinickým obrazom abnormálneho krvácania z maternice. V minulosti sa na základe histologického hodnotenia zvažovali iba dva typy. Endometriálny karcinóm je však klinicky heterogénne ochorenie a je čoraz jasnejšie, že táto heterogenita môže byť hybnou silou pri určení rôznorodosti na základe molekulárnych zmien. The Cancer Genome Atlas klasifikačný systémy zlepšil diagnostiku, stratifikáciu rizika a manažment endometriálneho karcinómu popisom štyroch molekulárnych podskupín s rôznou mutačnou záťažou a zmenami v počte kópií.

Klíčová slova:

p53 – endometriálny karcinóm – molekulárna klasifikácia – POLE mutácia – The Cancer Genome Atlas Research Network – hysterektómia – cielená terapia – mismatch-repair

Authors: Z. Ballová ; P. Gašparová ; M. Sitáš ; E. Dosedla
Authors‘ workplace: Department of Gynaecology and Obstetrics, Faculty of Medicine, University P. J. Safarik in Košice, Hospital AGEL Košice-Šaca Inc., Slovak Republic
Published in: Ceska Gynekol 2024; 89(2): 128-132
Category:
doi: https://doi.org/10.48095/cccg2024128

Overview

Endometrial cancer is the most common gynecological cancer and the second most prevalent female malignancy in the developed world. It is typically diagnosed in postmenopausal women, presenting with the characteristic clinical symptom of uterine abnormal bleeding. In the past, only two histological types were considered. However, it has become increasingly evident that endometrial cancer is a clinically heterogeneous disease, and this heterogeneity is closely associated with the diversity of underlying molecular alterations. The Cancer Genome Atlas classification has significantly advanced the diagnosis, risk stratification, and management of endometrial cancer by categorizing it into four molecular subgroups, each characterized by distinct mutational burdens and copy number alterations.

Keywords:

p53 – endometrial cancer – Hysterectomy – targeted therapy – molecular classification – POLE mutation – The Cancer Genome Atlas Research Network – mismatch-repair

Introduction

Endometrial cancer (EC) is a malignancy that originates in the epithelial lining of the uterus [1]. It stands as the most prevalent gynecological cancer and ranks as the second most common malignancy affecting women in the developed world. Notably, EC incidence has shown a rapid and consistent increase worldwide in recent years [2], with disparities in its prevalence influenced by geographic, socioeconomic, and racial factors [1]. As projections anticipate a continued rise in EC incidence [2], the associated burden of this disease is poised to surge. This burden encompasses not only the sheer number of patients diagnosed annually, but it also encompasses their age, risk profiles, and concurrent medical conditions, all of which warrant significant attention in the pursuit of optimal prevention and therapeutic strategies [3].

Historically, EC was classified into two types primarily based on its association with estrogen stimulation [1,4]. However, this traditional classification now falls short in providing a comprehensive understanding of this complex disease. Recent molecular discoveries and novel histopathological parameters have ushered in a fresh perspective on risk stratification. The Cancer Genome Atlas Research Network (TCGA), through its comprehensive analysis of tumors, has shed new light on the management of endometrial cancer [5]. The identification of four distinct molecular subgroups holds significant prognostic value and offers a promising tool for guiding clinical decisions, particularly in the realm of adjuvant treatment [6].

In this review article, we aim to present an in-depth exploration of the evolving landscape of endometrial cancer classification and the therapeutic strategies, all within the context of these emerging molecular subtypes.

Features of the four molecular subtypes. Adapted and modifi ed from Alexa et al. [22]. </br>Tab. 1. Vlastnosti štyroch molekulárnych podtypov. Upravené podľa Alexa et al. [22]. — **1. Features of the four molecular subtypes. Adapted and modifi ed from Alexa et al. [22]. Tab. 1. Vlastnosti štyroch molekulárnych podtypov. Upravené podľa Alexa et al. [22].**

Endometrial cancer’s general characteristics

Endometrial cancer, also referred to as corpus uterine cancer, is a malignancy that originates in the inner lining of the uterine body [1,7]. It is characterized by the invasive and abnormal proliferation of the endometrial lining of the uterus [8]. EC holds a significant position in women’s health due to its associated mortality [7]. According to the GLOBOCAN database, in 2020, there were nearly half a million new cases detected and one hundred thousand deaths attributed to EC worldwide [9]. The 5-year survival rate in 2018 was estimated at 84% in the US Surveillance, Epidemiology, and End Results (SEER) database [4]. Data from the EUROCARE-5 study suggests a 5-year relative survival rate of approximately 76–80% for European women [10].

Endometrial cancer predominantly affects postmenopausal women, with the majority of cases occurring between the ages of 65 and 75. However, it’s estimated that up to 14–25% of cases are diagnosed before menopause [1,9,11]. The American Cancer Society recommends that all women over the age of 65 be informed of the risks [12]. Nearly three-quarters of patients present with early-stage disease, with postmenopausal bleeding being the dominant symptom [13].

Risk factors for EC include non-genetic factors such as increased age, lower parity, tamoxifen use, metabolic syndrome, family history, and notably, genetic predisposition [1,2]. Over 50% of cases are associated with a higher body mass index (BMI), including obesity, while lower risk is linked to normal BMI, higher parity, and oral contraception use [1]. The primary risk factors for EC development remain tied to excessive, unopposed exposure of the endometrium to estrogen [12]. Over 90% of EC cases are sporadic, with 5–10% being hereditary, typically as part of the hereditary non-polyposis colorectal cancer syndrome or Lynch syndrome [13]. Endometrial biopsy offers high sensitivity (90–100%) and specificity (98–100%) for detecting endometrial cancer and should be performed in primary care whenever possible [14].

Traditional classification system

Endometrial carcinomas are classified according to the World Health Organization (WHO) classification system. They are divided into several subgroups, including endometrioid (70%), serous, clear cell, mixed cell adenocarcinoma, and other relatively rare types such as mucinous adenocarcinoma, neuroendocrine tumors, dedifferentiated carcinoma, and undifferentiated carcinoma [11]. This classification has been in use since 1983, proposed by Bokhman, and is based on histological characteristics [11,13]. It relies on tumor morphology and grade, determined by glandular architecture and nuclear grade. Type I comprises of low-grade cells, is more common, has a favorable prognosis, and is estrogen-dependent, often consisting of grade I or grade II endometrioid adenocarcinomas histopathologically. Type II comprises of high-grade cells, is less common, and carries an unfavorable prognosis, including grade III endometrioid adenocarcinomas, and serous, clear cell, and undifferentiated carcinosarcomas [4,9].

Advanced molecular classification system

The WHO classification, while useful in determining surgical and adjuvant therapy, has limitations due to a lack of reproducibility and significant inter-observer variability [11,13]. Over the past decade, it has become evident that endometrial cancers are a diverse group of tumors, not only in terms of biology, histology, and clinical features, but also in terms of their genetic makeup [15]. Therefore, a more specific classification system was needed. Genomic analysis in 2013 and subsequent studies employing immunohistochemistry have led to the current molecular classification of EC. Initially, TCGA divided serous and endometrioid EC into four molecular subgroups based on mutational burden and copy number alterations. This approach resulted in molecular stratification of EC into four distinct molecular groups: MMR-deficient (MMR-d), p53 mutation (p53mut) -type, POLE mutation (POLEmut) -type, and cases with no specific molecular profile (NSMP) [9,16]. Next-generation sequencing (NGS) has become a standard procedure for cancer genomic analysis [13].

POLE ultramutated (POLE mut)

This subtype is characterized by ultramutation caused by POLE mutations [15]. These mutations typically occur in the exonuclease domain of the POLE gene, which encodes DNA polymerase epsilon involved in DNA replication and repair [6,17]. POLE encodes the catalytic subunit of DNA polymerase, responsible for leading strand DNA replication [18]. It recognizes and removes mispaired nucleotides through its exonuclease activity, ensuring high fidelity DNA replication [19,20]. ECs harboring POLE exonuclease domain mutations make up 5–15% of all EC cases and often affect young women with low BMI [21]. These tumors typically present at earlier stages and exhibit a high survival rate, around 96% at 5 years, despite their aggressive histological appearance (high-grade endometrioid histotype with intense tumor-infiltrating lymphocytes) [21]. The potential relationship between POLE mutations and the prognosis of endometrial cancer patients remains unclear [17].

p53 mutation (p53 mut/abn)

The tumor suppressor gene TP53, which encodes the p53 protein, is one of the most common mutations in human tumors. The p53 subgroup accounts for 8–24% of EC cases. This subgroup was initially defined by a high number of somatic copy-number alterations and a low mutational yield [22]. The p53 category is associated with older age and lower BMI, as well as more advanced stage and poorer prognosis, contributing to 50–70% of EC mortality [6]. p53--mutant ECs are typically high-grade and morphologically ambiguous [23]. Histologically, the proportion of p53 abnormalities is high in serous EC (93%), carcinosarcoma (85%), clear cell EC (38%), and grade 3 endometrioid EC (22%). Recent studies have consistently demonstrated a poor prognosis associated with p53 mutations in EC [22,23].

Mismatch repair deficient (MMRd)

Defective DNA mismatch repair (dMMR) leads to elevated tumor mutational burden (TMB) and microsatellite instability (MSI) in multiple cancer types [24]. The MMR-deficient molecular group represents 20–30% of EC cases [6,22]. Analysis of EC from the TCGA series revealed significant variation in proportions of tumor-infiltrating lymphocytes, CD8+, CD4+, NK cells, and immune checkpoint expression in MMR-deficient ECs [24]. MMR-deficient ECs show an intermediate prognosis and may benefit from immunotherapy [23]. Studies have evaluated the efficacy of immunotherapy, with pembrolizumab and avelumab being preferred due to their favorable toxicity profiles [25–27]. NCCN guidelines recommend pembrolizumab and nivolumab for treating patients with advanced or recurrent microsatellite instability-high/mismatch repair-deficient EC [28]. It is important to realize that mismatch repair-deficient cancers have varied responses to an immune-check--point blockade [29].

The „non-specific molecular profile“ (NSMP)

The category of EC that did not exhibit any of the previously described features was classified as “p53 wt” or “no specific molecular profile” (NSMP) [22]. The NSMP group is the most common in the TCGA dataset [23], accounting for approximately 40–50% of EC cases. This group primarily includes endometrioid ECs with estrogen and progesterone receptor positivity, and these tumors often exhibit high response rates to hormonal therapy [6]. Patients with “p53 wt” tumors tend to have a higher BMI [22]. The prognosis for this group is highly variable and influenced by clinicopathological and molecular factors, many of which are still under evaluation [23].

Discussion

Endometrial cancer ranks among the most prevalent female malignancies. Typically, primary treatment involves a combination of surgical procedures, vaginal brachytherapy, external beam radiation therapy, and adjuvant chemotherapy [22]. The surgical approach typically includes a hysterectomy, bilateral salpingo-oophorectomy, and pelvic lymph node dissection/biopsy, often extended to para-aortic lymph nodes [30,31]. Surgery may be the sole treatment option for early-stage, low--grade tumors, while advanced stages often necessitate a combination of adjuvant therapies, such as chemotherapy, radiotherapy, chemoradiotherapy, antiangiogenesis agents, immune checkpoint inhibitors, and multi-target agents [31]. Treatment decisions are primarily guided by the tumor stage and pathological findings. Historically, Bokhman’s 1983 classification system described two types of EC. The WHO has further categorized EC into four histological types: low-grade endometrioid, high-grade endometrioid, serous, and clear cell EC [22].

Endometrial cancer is a clinically heterogeneous disease, and it is increasingly evident that this heterogeneity arises from the diversity of underlying molecular alterations [32]. Understanding these molecular alterations offers the potential to enhance the current histologic classification system, improve diagnostic testing methods, and personalize treatments by incorporating targeted therapies [11,33].

Multiple studies have demonstrated discrepancies between pathologists in approximately 30% of cases. The Cancer Genome Atlas conducted a genome-wide analysis of 373 cases, encompassing exome sequencing, mRNA expression, protein expression, miRNA expression, and DNA methylation evaluation. This comprehensive analysis identified four distinct groups: Polymerase Epsilon ultra-mutated, microsatellite instability hypermutated, copy-number-low, and copy number high EC [22].

According to the recommendations for managing EC patients by the European Society of Gynecological Oncology (ESGO), the European Society for Radiotherapy and Oncology (ESTRO), and the European Society of Pathology (ESP), this classification holds strong prognostic value, particularly in high-risk endometrial cancer cases where adjuvant therapies are typically recommended. Additionally, the Proactive Molecular Risk Classifier for Endometrial Cancer (ProMisE) has been developed as an alternative classification system using immunohistochemical markers [6].

Epigenomics, genomics, transcriptomics, proteomics, and metabolomics have been subjects of extensive research. They provide valuable information on gene and protein expression, as well as the mechanisms involved in their regulation. These approaches offer the potential for a deeper understanding of the events occurring during cancer development, the molecular makeup of the tumor microenvironment, and the identification of new markers and therapeutic targets [6].

Conclusion

In conclusion, the TCGA classification has significantly improved the diagnosis, risk stratification, and management of EC. The utilization of next-generation sequencing techniques, including whole--genome sequencing, enables a comprehensive analysis of genetic material and uncovering critical genomic alterations that play a pivotal role in the understanding and treatment of this disease.

Sources

1. Makker V, MacKay H, Ray-Coquard I et al. Endometrial cancer. Nat Rev Dis Primers 2021; 7 (1): 88. doi: 10.1038/s41572-021-00324-8.

2. Raglan O, Kalliala I, Markozannes G et al. Risk factors for endometrial cancer: an umbrella review of the literature. Int J Cancer 2019; 145 (7): 1719–1730. doi: 10.1002/ijc.31961.

3. Clarke MA, Long BJ, Del Mar Morillo A et al. Association of endometrial cancer risk with postmenopausal bleeding in women: a systematic review and meta-analysis. JAMA Intern Med 2018; 178 (9): 1210–1222. doi: 10.1001/jmainternmed.2018.2820.

4. Brooks RA, Fleming GF, Lastra RR et al. Current recommendations and recent progress in endometrial cancer. CA Cancer J Clin 2019; 69 (4): 258–279. doi: 10.3322/caac.21561.

5. Bidzinski M, Danska-Bidzinska A, Rychlik A et al. Molecular classification of endometrial carcinoma, is it the new era of precision medicine? Ginekol Pol 2022; 93 (2): 163–167. doi: 10.5603/GP.a2021.0216.

6. Mitric C, Bernardini MQ. Endometrial cancer: transitioning from histology to genomics. Curr Oncol 2022; 29 (2): 741–757. doi: 10.3390/curroncol29020063.

7. Urick ME, Bell DW. Clinical actionability of molecular targets in endometrial cancer. Nat Rev Cancer 2019; 19 (9): 510–521. doi: 10.1038/s41568-019-0177-x.

8. Nees LK, Heublein S, Steinmacher S et al. Endometrial hyperplasia as a risk factor of endometrial cancer. Arch Gynecol Obstet 2022; 306 (2): 407–421. doi: 10.1007/s00404-021-06380-5.

9. Boroń D, Zmarzły N, Wierzbik-Strońska M et al. Recent multiomics approaches in endometrial cancer. Int J Mol Sci 2022; 23 (3): 1237. doi: 10.3390/ijms23031237.

10. Concin N, Matias-Guiu X, Vergote I et al. ESGO/ESTRO/ESP guidelines for the management of patients with endometrial carcinoma. Int J Gynecol Cancer 2021; 31 (1): 12–39. doi: 10.1136/ijgc-2020-002230.

11. Yen TT, Wang TL, Fader AN et al. Molecular classification and emerging targeted therapy in endometrial cancer. Int J Gynecol Pathol 2020; 39 (1): 26–35. doi: 10.1097/PGP.0000 00000 0000585.

12. Braun MM, Overbeek-Wager EA, Grumbo RJ. Diagnosis and management of endometrial cancer. Am Fam Physician 2016; 93 (6): 468–474.

13. Oaknin A, Bosse TJ, Creutzberg CL et al. ESMO Guidelines Committee. Endometrial cancer: ESMO Clinical Practice Guideline for diagnosis, treatment and follow-up. Ann Oncol 2022; 33 (9): 860–877. doi: 10.1016/j.annonc.2022.05.009.

14. Sobel M, Simpson AN, Ferguson SE. Endometrial cancer. CMAJ 2021; 193 (36): E1423. doi: 10.1503/cmaj.202731.

15. Murali R, Delair DF, Bean SM et al. Evolving roles of histologic evaluation and molecular/genomic profiling in the management of endometrial cancer. J Natl Compr Canc Netw 2018; 16 (2): 201–209. doi: 10.6004/jnccn.2017.7066.

16. Kobayashi Y, Kitazono I, Akahane T et al. Molecular evaluation of endometrial dedifferentiated carcinoma, endometrioid carcinoma, carcinosarcoma, and serous carcinoma using a custom-made small cancer panel. Pathol Oncol Res 2021; 27: 1610013. doi: 10.3389/pore.2021. 1610013.

17. Li Y, He Q, Li S et al. POLE mutation characteristics in a Chinese cohort with endometrial carcinoma. Onco Targets Ther 2020; 13: 7305–7316. doi: 10.2147/OTT.S258642.

18. León-Castillo A, Britton H, McConechy MK et al. Interpretation of somatic POLE mutations in endometrial carcinoma. J Pathol 2020; 250 (3): 323–335. doi: 10.1002/path.5372.

19. Jumaah AS, Salim MM, Al-Haddad HS et al. The frequency of POLE-mutation in endometrial carcinoma and prognostic implications: a systemic review and meta-analysis. J Pathol Transl Med 2020; 54 (6): 471–479. doi: 10.4132/jptm. 2020.07.23.

20. Yu S, Sun Z, Zong L et al. Clinicopathological and molecular characterization of high- -grade endometrial carcinoma with POLE mutation: a single center study. J Gynecol Oncol 2022; 33 (3): e38. doi: 10.3802/jgo.2022.33.e38.

21. Pasciuto MP, Felicioni L, Zampacorta C et al. POLE exonuclease domain mutations in endometrial carcinoma: a case report. Pathologica 2023; 1 (1): 181–185. doi: 10.32074/1591-951X- 872.

22. Alexa M, Hasenburg A, Battista MJ. The TCGA molecular classification of endometrial cancer and its possible impact on adjuvant treatment decisions. Cancers (Basel) 2021; 13 (6): 1478. doi: 10.3390/cancers13061478.

23. Arciuolo D, Travaglino A, Raffone A et al. TCGA molecular prognostic groups of endometrial carcinoma: current knowledge and future perspectives. Int J Mol Sci 2022; 23 (19): 11684. doi: 10.3390/ijms231911684.

24. Glaire MA, Ryan NA, Ijsselsteijn ME et al. Discordant prognosis of mismatch repair deficiency in colorectal and endometrial cancer reflects variation in antitumour immune response and immune escape. J Pathol 2022; 257 (3): 340–351. doi: 10.1002/path.5894.

25. O‘Malley DM, Bariani GM, Cassier PA et al. Pembrolizumab in patients with microsatellite instability-high advanced endometrial cancer: results from the KEYNOTE-158 study. J Clin Oncol 2022; 40 (7): 752–761. doi: 10.1200/JCO. 21.01874.

26. Konstantinopoulos PA, Gockley AA, Xiong N et al. Evaluation of treatment with talazoparib and avelumab in patients with recurrent mismatch repair proficient endometrial cancer. JAMA Oncol 2022; 8 (9): 1317–1322. doi: 10.1001/jamaoncol.2022.2181.

27. Maio M, Ascierto PA, Manzyuk L et al. Pembrolizumab in microsatellite instability high or mismatch repair deficient cancers: updated analysis from the phase II KEYNOTE-158 study. Ann Oncol 2022; 33 (9): 929–938. doi: 10.1016/ j.annonc.2022.05.519.

28. Zhao S, Chen L, Zang Y et al. Endometrial cancer in Lynch syndrome. Int J Cancer 2022; 150 (1): 7–17. doi: 10.1002/ijc.33763.

29. Chow RD, Michaels T, Bellone S et al. Distinct mechanisms of mismatch-repair deficiency delineate two modes of response to anti-PD-1 immunotherapy in endometrial carcinoma. Cancer Discov 2023; 13 (2): 312–331. doi: 10.1158/2159-8290.CD-22-0686.

30. Kovacevic N. Surgical treatment and fertility perservation in endometrial cancer. Radiol Oncol 2021; 55 (2): 144–149. doi: 10.2478/raon-2021-0009.

31. Tung HJ, Huang HJ, Lai CH. djuvant and post--surgical treatment in endometrial cancer. Best Pract Res Clin Obstet Gynaecol 2022; 78: 52–63. doi: 10.1016/j.bpobgyn.2021.06.002.

32. McAlpine J, Leon-Castillo A, Bosse T. The rise of a novel classification system for endometrial carcinoma; integration of molecular subclasses. J Pathol 2018; 244 (5): 538–549. doi: 10.1002/path.5034.

33. Imboden S, Nastic D, Ghaderi M et al. Phenotype of POLE-mutated endometrial cancer. PLoS One 2019; 14 (3): e0214318. doi: 10.1371/journal.pone.0214318.

ORCID authors

Z. Ballová 0000-0002-0605-948X

P. Gašparová 0000-0002-6354-6911

M. Sitáš 0000-0002-7273-1051

E. Dosedla 0000-0001-8319-9008

Submitted/Doručené: 18. 10. 2023

Accepted/Prijaté: 20. 10. 2023

Assoc. Prof. Erik Dosedla, MD, PhD, MBA

Department of Gynaecology and Obstetrics

Faculty of Medicine

University P. J. Safarik in Košice

Hospital AGEL Košice-Šaca Inc.