Refinement of high-risk endometrial cancer classification using DNA damage response biomarkers: a TransPORTEC initiative

被引:34
作者
Auguste, Aurelie [1 ]
Genestie, Catherine [1 ,2 ]
De Bruyn, Marco [3 ]
Adam, Julien [2 ]
Le Formal, Audrey [1 ]
Drusch, Francoise [4 ]
Pautier, Patricia [5 ]
Crosbie, Emma J. [6 ]
MacKay, Helen [7 ]
Kitchener, Henry C. [6 ]
Powell, Melanie [8 ]
Pollock, Pamela M. [9 ]
Mileshkin, Linda [10 ]
Edmondson, Richard J. [10 ,11 ]
Nout, Remi [12 ]
Nijman, Hans W. [13 ]
Creutzberg, Carien L. [12 ]
Bosse, Tjalling [14 ]
Leary, Alexandra [1 ,5 ]
机构
[1] Gustave Roussy, INSERM, Gynecol Unit, U981, Villejuif, France
[2] Gustave Roussy, Dept Med Oncol, Dept Pathol, Villejuif, France
[3] Univ Groningen, Univ Med Ctr Groningen, Dept Obstet & Gynecol, Groningen, Netherlands
[4] Gustave Roussy, Histocyto Pathol Platform, Villejuif, France
[5] Gustave Roussy, Dept Med Oncol, Villejuif, France
[6] Univ Manchester, St Marys Hosp, Inst Canc Sci, Manchester, Lancs, England
[7] Univ Toronto, Univ Hlth Network, Princess Margaret Hosp, Dept Obstet & Gynecol,Div Gynecol Oncol, Toronto, ON, Canada
[8] Arts Hlth NHS Trust, Dept Clin Oncol, London, England
[9] Queensland Univ Technol, Inst Hlth & Biomed Innovat, Brisbane, Qld, Australia
[10] Peter Mac Callum Canc Ctr, Div Canc Med, East Melbourne, Australia
[11] Univ Manchester, Inst Canc Sci, St Marys Hosp, Manchester, Lancs, England
[12] Eiden Univ, Dept Clin Oncol, Med Ctr, Leiden, Netherlands
[13] Univ Groningen, Univ Med Ctr Groningen, Dept Gynecol, Groningen, Netherlands
[14] Leiden Univ, Dept Pathol, Med Ctr, Leiden, Netherlands
来源
MODERN PATHOLOGY | 2018年 / 31卷 / 12期
关键词
REPAIR DEFECTS; RADIOTHERAPY; SENSITIVITY; GAMMA-H2AX; DEFICIENCY; BRCA1; 53BP1;
D O I
10.1038/s41379-018-0055-1
中图分类号
R36 [病理学];
学科分类号
100104 ;
摘要
The TransPORTEC consortium previouslclassified high-risk endometrial cancer including poor-risk histologies such as clear cells, into four molecular subtypes "POLE mutated," "microsatellite unstable," "TP53 mutated," and "no specific molecular profile." We evaluated whether DNA damage response biomarkers could further refine this high-risk tumors classification, in particular the heterogeneous "no specific molecular profile" and "TP53 mutated" subsets recently qualified as poor prognosis in high-risk endometrial cancer. DNA damage response biomarkers including proteins involved in DNA damage (delta-H2AX), homologous recombination (RAD51), regulators of error-prone Non Homologous End-Joining (DNA-pk, FANCD2), and PARP-1 were evaluated in 116 high-risk tumors by immunohistochemistry. CD8 and PD-1 expression by immunochemistry and mutation analyses were performed previously. Survival outcome were calculated using Kaplan-Meier and Log-rank test. None of the DNA damage response biomarkers alone were prognostic. However markers were informative within molecular subsets. Among the "no specific molecular profile" subset, delta-H2AX+ was significantly predictive of poor disease free survival (Hazard Ratio = 2.56; p = 0.026), and among "TP53 mutated," a DNA-pk+/FANCD2-profile (favouring error-prone Non Homologous End-Joining) predicted worst disease free survival (Hazard Ratio = 4.95; p = 0.009) resulting in five distinct prognostic subgroups from best to worst prognosis: group1 "POLE mutated/Microsatellite unstable" > group2 "no specific molecular profile with no DNA damage" > group3 "TP53 mutated/Non Homologous End-Joining negative" > group4 "no specific molecular profile with high DNA damage" > group5 "TP53 mutated/Non Homologous End-Joining positive"; p = 0.0002). Actionable targets were also different among subsets. Group3 had significantly higher infiltration of PD-1+ immune cells (p = 0.003), segregating with group1. Group2 had frequent PI3K pathway mutations and ER positivity. While group5, with the worst prognosis, had high DNA damage and PARP-1 expression providing a rationale for PARP inhibition. Our findings have refined the TransPORTEC prognostic classification of high-risk endometrial cancer into five distinct subgroups by integrating DNA damage response biomarkers and identified molecular subtype-specific therapeutic strategies.
引用
收藏
页码:1851 / 1861
页数:11
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