Polymerase ε (POLE) ultra-mutation in uterine tumors correlates with T lymphocyte infiltration and increased resistance to platinum-based chemotherapy in vitro

Bellone, Stefania; Bignotti, Eliana; Lonardi, Silvia; Ferrari, Francesca; Centritto, Floriana; Masserdotti, Alice; Pettinella, Francesca; Black, Jonathan; Menderes, Gulden; Altwerger, Gary; Hui, Pei; Lopez, Salvatore; Haydu, Christopher de; Bonazzoli, Elena; Predolini, Federica; Zammataro, Luca; Cocco, Emiliano; Ferrari, Federico; Ravaggi, Antonella; Romani, Chiara; Facchetti, Fabio; Sartori, Enrico; Odicino, Franco; Silasi, Dan‐Arin; Litkouhi, Babak; Ratner, Elena; Azodi, Masoud; Schwartz, Peter E.; Santin, Alessandro D.

doi:10.1016/j.ygyno.2016.11.023

Cited by 56 publications

(59 citation statements)

References 23 publications

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“…There is increasing appreciation of the importance of the tumor microenvironment in defining outcomes and therapeutic opportunities in cancer. In particular, TILs have been shown to be both prognostic and predictive in that their presence is generally associated with improved outcomes and favorable response to conventional chemotherapies and immune-targeting agents (1)(2)(3)(4)(45)(46)(47)(48)(49). We investigated the relationships between immune response, molecular subtype, and patient survival in endometrial cancer.…”

Section: Discussionmentioning

confidence: 99%

“…Thus, molecular subtype, not immune response, was the most significant prognostic factor in this series, suggesting that the molecular/genomic features of tumors influence outcome through mechanisms apart from the immune response. Immune markers have been assessed in endometrial cancer in both the pre-(2, 50) and post-TCGA eras (12,30,31,46,51). The latter have primarily focused on the newly recognized POLE ultramutated and MSI/MMRd-hypermutated subtypes.…”

Section: Discussionmentioning

confidence: 99%

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Molecular Subtype Not Immune Response Drives Outcomes in Endometrial Carcinoma

Talhouk

Derocher

Schmidt

et al. 2019

Clinical Cancer Research

100

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Purpose: Tumors with high mutation load are thought to engender stronger immune responses, which in turn promote prolonged patient survival. To investigate this, we assessed tumor-infiltrating lymphocytes (TILs) and immunosuppressive factors across the 4 molecular subtypes of endometrial cancer, which have characteristic mutation rates ranging from low to ultra-high.Experimental Design: A total of 460 endometrial cancers were stratified by ProMisE (Proactive Molecular Risk Classifier in Endometrial cancer) into 4 molecular subtypes: mismatch repair-deficient (MMRd), POLE mutant (POLE), p53 abnormal (p53abn), and p53 wild-type (p53wt). Immune markers (CD3, CD8, CD79a, CD138, PD-1, PD-L1, FoxP3, IDO-1) were quantified by multiplex IHC and tested for associations with ProM-isE subtype, survival, and other clinicopathologic parameters.Results: Two major TIL patterns were observed. TIL high tumors harbored dense T-and B-lineage infiltrates and multiple immunosuppressive features and were common in molecular subtypes associated with high mutation load (MMRd and POLE); however, equally strong responses were seen in significant numbers of p53abn and p53wt tumors, which have characteristically low mutation loads. TIL low tumors were generally devoid of immunologic features and were more prevalent in p53abn and p53wt endometrial cancers, yet were also seen in MMRd and POLE subtypes. In multivariable models involving ProMisE subtype, T-cell markers, and TIL clusters, only ProMisE showed independent prognostic significance.Conclusions: Immune response correlates with endometrial cancer molecular subtype but does not carry independent prognostic significance. Profound variation in immune response is seen across and within endometrial cancer molecular subtypes, suggesting that assessment of immune response rather than molecular subtype may better predict response to immunotherapy.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Molecular Subtype Not Immune Response Drives Outcomes in Endometrial Carcinoma

Talhouk

Derocher

Schmidt

et al. 2019

Clinical Cancer Research

100

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“…A review of the literature was undertaken, to the end of 2018, to identify ECs in which POLE had been sequenced and the mutations published [6,7,[9][10][11][12][13][14][15][17][18][19][20][21][22]24,25]. All literature contributing entries into the COSMIC database (POLE + endometrium) were reviewed; in addition, searches in PubMed and Web of Science were undertaken with the keywords 'POLE + Endometrial + Carcinoma' and 'POLE + Endometrial + Cancer', noting that 'POLε' is interpreted as 'POLE' in these resources.…”

Section: Somatic Pole Mutations Reported In Ecs and Not Detected In Tmentioning

confidence: 99%

“…'POLE ultramutated' EC (POLEmut EC) has therefore been proposed as a distinct clinical entity that can be diagnosed in the presence of a pathogenic POLE exonuclease domain mutation (EDM) [8]. For the five most common POLE mutations (P286R, V411L, S297F, A456P, and S459F), pathogenicity (in this sense meaning causal for tumour ultramutation) has been confirmed [4][5][6][9][10][11][12][13][14][15][16][17][18][19][20][21][22][23][24][25]; however, the classification of other, less frequent POLE variants is currently challenging. This is becoming an urgent problem, as POLE sequencing for molecular EC classification is rapidly entering clinical practice.…”

Section: Introductionmentioning

confidence: 99%

“…To define the extent of the problem of ascribing pathogenicity to POLE mutations in clinical practice, we identified 296/3840 (7.7%) tumours with a somatic POLE mutation from EC cohorts other than TCGA [6,7,[9][10][11][12][13][14][15][17][18][19][20][21][22]24,25] (Table 5 and supplementary material, Table S3). Of 296 non-TCGA POLE-mutant ECs reported in the literature, 15 had mutations outside the exonuclease domain, and 254 carried mutations in the exonuclease domain previously detected in the TCGA and classified by POLE-scores as pathogenic (249 cases), of uncertain pathogenicity (four cases), or non-pathogenic (one case).…”

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Interpretation of somatic POLE mutations in endometrial carcinoma

León‐Castillo

Britton

McConechy³

et al. 2020

The Journal of Pathology

223

207

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Pathogenic somatic missense mutations within the DNA polymerase epsilon (POLE) exonuclease domain define the important subtype of ultramutated tumours (‘POLE‐ultramutated’) within the novel molecular classification of endometrial carcinoma (EC). However, clinical implementation of this classifier requires systematic evaluation of the pathogenicity of POLE mutations. To address this, we examined base changes, tumour mutational burden (TMB), DNA microsatellite instability (MSI) status, POLE variant frequency, and the results from six in silico tools on 82 ECs with whole‐exome sequencing from The Cancer Genome Atlas (TCGA). Of these, 41 had one of five known pathogenic POLE exonuclease domain mutations (EDM) and showed characteristic genomic alterations: C>A substitution > 20%, T>G substitutions > 4%, C>G substitutions < 0.6%, indels < 5%, TMB > 100 mut/Mb. A scoring system to assess these alterations (POLE‐score) was developed; based on their scores, 7/18 (39%) additional tumours with EDM were classified as POLE‐ultramutated ECs, and the six POLE mutations present in these tumours were considered pathogenic. Only 1/23 (4%) tumours with non‐EDM showed these genomic alterations, indicating that a large majority of mutations outside the exonuclease domain are not pathogenic. The infrequent combination of MSI‐H with POLE EDM led us to investigate the clinical significance of this association. Tumours with pathogenic POLE EDM co‐existent with MSI‐H showed genomic alterations characteristic of POLE‐ultramutated ECs. In a pooled analysis of 3361 ECs, 13 ECs with DNA mismatch repair deficiency (MMRd)/MSI‐H and a pathogenic POLE EDM had a 5‐year recurrence‐free survival (RFS) of 92.3%, comparable to previously reported POLE‐ultramutated ECs. Additionally, 14 cases with non‐pathogenic POLE EDM and MMRd/MSI‐H had a 5‐year RFS of 76.2%, similar to MMRd/MSI‐H, POLE wild‐type ECs, suggesting that these should be categorised as MMRd, rather than POLE‐ultramutated ECs for prognostication. This work provides guidance on classification of ECs with POLE mutations, facilitating implementation of POLE testing in routine clinical care. © 2019 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland.

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Race, Prevalence of POLE and POLD1 Alterations, and Survival Among Patients With Endometrial Cancer

Zheng,

Donnelly,

Strauss

2024

JAMA Netw Open

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ImportanceBlack patients with endometrial cancer (EC) in the United States have higher mortality than patients of other races with EC. The prevalence of POLE and POLD1 pathogenic alterations in patients of different races with EC are not well studied.ObjectiveTo explore the prevalence of and outcomes associated with POLE and POLD1 alterations in differential racial groups.Design, Setting, and ParticipantsThis retrospective cohort study incorporated the largest available data set of patients with EC, including American Association for Cancer Research Project GENIE (Genomics Evidence Neoplasia Information Exchange; 5087 participants), Memorial Sloan Kettering–Metastatic Events and Tropisms (1315 participants), and the Cancer Genome Atlas Uterine Corpus Endometrial Carcinoma (517 participants), collected from 2015 to 2023, 2013 to 2021, and 2006 to 2012, respectively. The prevalence of and outcomes associated with POLE or POLD1 alterations in EC were evaluated across self-reported racial groups.ExposurePatients of different racial groups with EC and with or without POLE or POLD1 alterations.Main Outcomes and MeasuresThe main outcome was overall survival. Data on demographic characteristics, POLE and POLD1 alteration status, histologic subtype, tumor mutation burden, fraction of genome altered, and microsatellite instability score were collected.ResultsA total of 6919 EC cases were studied, of whom 444 (6.4%), 694 (10.0%), and 4869 (70.4%) patients were self-described as Asian, Black, and White, respectively. Within these large data sets, Black patients with EC exhibited a lower weighted average prevalence of pathogenic POLE alterations (0.5% [3 of 590 cases]) compared with Asian (6.1% [26 of 424]) or White (4.6% [204 of 4520]) patients. By contrast, the prevalence of POLD1 pathogenic alterations was 5.0% (21 cases), 3.2% (19 cases), and 5.6% (255 cases) in Asian, Black, and White patients with EC, respectively. Patients with POLD1 alterations had better outcomes regardless of race, histology, and TP53 alteration status. For a total of 241 clinically annotated Black patients with EC, a composite biomarker panel of either POLD1 or POLE alterations identified 7.1% (17 patients) with positive outcomes (1 event at 70 months follow up) in the small sample of available patients.Conclusions and RelevanceIn this retrospective clinicopathological study of patients of different racial groups with EC, a composite biomarker panel of either POLD1 or POLE alteration could potentially guide treatment de-escalation, which is especially relevant for Black patients.

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Polymerase ε (POLE) ultra-mutation in uterine tumors correlates with T lymphocyte infiltration and increased resistance to platinum-based chemotherapy in vitro

Cited by 56 publications

References 23 publications

Molecular Subtype Not Immune Response Drives Outcomes in Endometrial Carcinoma

Molecular Subtype Not Immune Response Drives Outcomes in Endometrial Carcinoma

Interpretation of somatic POLE mutations in endometrial carcinoma

Race, Prevalence of POLE and POLD1 Alterations, and Survival Among Patients With Endometrial Cancer

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