High prevalence of "non-pathogenic" POLE mutation with poor prognosis in a cohort of endometrial cancer from South India

被引:1
作者
Kuriakose, Santhosh [1 ,9 ]
Dhanasooraj, Dhananjayan [2 ]
Shiny, P. M. [3 ]
Shammy, S. [2 ]
Sona, V. P. [2 ]
Manjula, Anupama A. [3 ]
Ramachandran, Amrutha [1 ]
Vijaykumar, Bindu [4 ]
Susan, Nayana [4 ]
Dinesan, M. [5 ]
Sankar, Uma V. [6 ]
Ramachandran, Kavitha [7 ]
Sreedharan, P. S. [8 ]
机构
[1] Govt Med Coll, Dept Obstet & Gynecol, Gynecol Oncol Div, Kozhikode, Kerala, India
[2] Govt Med Coll, Multidisciplinary Res Unit, Kozhikode, Kerala, India
[3] Govt Med Coll, Dept Pathol, Kozhikode, Kerala, India
[4] Govt Med Coll, Dept Obstet & Gynecol, Kozhikode, Kerala, India
[5] Govt Med Coll, Tertiary Canc Care Ctr, Dept Radiat Oncol, Kozhikode, Kerala, India
[6] MVR Canc Ctr & Res Inst, Kozhikode, Kerala, India
[7] MVR Canc Ctr & Res Inst, Dept Pathol, Kozhikode, Kerala, India
[8] MVR Canc Ctr & Res Inst, Dept Med Oncol, Kozhikode, Kerala, India
[9] Govt Med Coll, Inst Maternal & Child Hlth IMCH, Med Coll, Kozhikode 673008, Kerala, India
来源
INTERNATIONAL JOURNAL OF GYNECOLOGY & OBSTETRICS | 2024年 / 166卷 / 03期
关键词
endometrial carcinoma; POLE mutation; polymerase epsilon (POLE) gene; prognosis; Sanger sequencing; EXONUCLEASE DOMAIN MUTATIONS; SURVIVAL; CLASSIFICATION; CARCINOMAS; POLYMERASE;
D O I
10.1002/ijgo.15486
中图分类号
R71 [妇产科学];
学科分类号
100211 ;
摘要
Objective: The Cancer Genome Atlas (TCGA) project identified favorable prognosis regarding the ultra-mutated endometrial cancer (EC) subtype linked to polymerase epsilon gene (POLE) mutations. This study investigated POLE mutations in EC of Indian patients. Methods: This retrospective analytical study was conducted between January 2016 and January 2023 at the Government Medical College, Kozhikode, and the MVR Cancer Center, Kozhikode, Kerala. Sanger sequencing of POLE gene exons 9 and 13 in 151 EC patients was carried out to analyze the relationship between mutations and epidemiological factors, clinicopathologic features, and treatment outcomes. Results: Among 151 cases enrolled, 39 were unique POLE-mutated cases. Significant associations were high-grade tumors, myometrial invasion >50%, and Lymph-vascular space invasion (LVSI). The median follow-up was 40 months (95% confidence interval [CI], 34-46). A lower mean disease-specific survival (DSS) of 51.7 months (95% CI, 43.7-59.6) was noted in the POLE-mutated group compared with 72.11 months (95% CI, 67.60-76.62) for the POLE wild-type. A statistically significant hazard ratio (HR) of 2.683 for DSS in the POLE-mutated group was noted. In advanced stages (FIGO stages II-IV), a nine-fold HR for DSS and overall survival (OS) compared with POLE wild-type was identified. After controlling for treatment effects using Cox proportional HR, advanced-stage POLE-mutated tumors had a significantly higher HR of 8.67 for DSS compared with POLE-wild-type tumors of the same stage. Conclusion: This study identified a unique set of POLE mutations in Indian EC patients associated with poor prognosis, which were particularly pronounced in advanced stages. Advanced stage of presentation, type of POLE mutations, and possibly ethnicity are predictors of adverse outcomes in POLE-mutated EC. The present study highlights ethnicity as a determinant of phenotypic expression of genetic change.
引用
收藏
页码:1263 / 1272
页数:10
相关论文
共 27 条
[1]   Polymerase ε (POLE) ultra-mutation in uterine tumors correlates with T lymphocyte infiltration and increased resistance to platinum-based chemotherapy in vitro [J].
Bellone, Stefania ;
Bignotti, Eliana ;
Lonardi, Silvia ;
Ferrari, Francesca ;
Centritto, Floriana ;
Masserdotti, Alice ;
Pettinella, Francesca ;
Black, Jonathan ;
Menderes, Gulden ;
Altwerger, Gary ;
Hui, Pei ;
Lopez, Salvatore ;
de Haydu, Christopher ;
Bonazzoli, Elena ;
Predolini, Federica ;
Zammataro, Luca ;
Cocco, Emiliano ;
Ferrari, Federico ;
Ravaggi, Antonella ;
Romani, Chiara ;
Facchetti, Fabio ;
Sartori, Enrico ;
Odicino, Franco E. ;
Silasi, Dan-Arin ;
Litkouhi, Babak ;
Ratner, Elena ;
Azodi, Masoud ;
Schwartz, Peter E. ;
Santin, Alessandro D. .
GYNECOLOGIC ONCOLOGY, 2017, 144 (01) :146-152
[2]   Prognostic Significance of POLE Exonuclease Domain Mutations in High-Grade Endometrioid Endometrial Cancer on Survival and Recurrence A Subanalysis [J].
Billingsley, Caroline C. ;
Cohn, David E. ;
Mutch, David G. ;
Hade, Erinn M. ;
Goodfellow, Paul J. .
INTERNATIONAL JOURNAL OF GYNECOLOGICAL CANCER, 2016, 26 (05) :933-938
[3]   Prognostic Significance of POLE Proofreading Mutations in Endometrial Cancer [J].
Church, David N. ;
Stelloo, Ellen ;
Nout, Remi A. ;
Valtcheva, Nadejda ;
Depreeuw, Jeroen ;
ter Haar, Natalja ;
Noske, Aurelia ;
Amant, Frederic ;
Tomlinson, Ian P. M. ;
Wild, Peter J. ;
Lambrechts, Diether ;
Jurgenliemk-Schulz, Ina M. ;
Jobsen, Jan J. ;
Smit, Vincent T. H. B. M. ;
Creutzberg, Carien L. ;
Bosse, Tjalling .
JNCI-JOURNAL OF THE NATIONAL CANCER INSTITUTE, 2015, 107 (01)
[4]   DNA polymerase ? and exonuclease domain mutations in endometrial cancer [J].
Church, David N. ;
Briggs, Sarah E. W. ;
Palles, Claire ;
Domingo, Enric ;
Kearsey, Stephen J. ;
Grimes, Jonathon M. ;
Gorman, Maggie ;
Martin, Lynn ;
Howarth, Kimberley M. ;
Hodgson, Shirley V. ;
Kaur, Kulvinder ;
Taylor, Jenny ;
Tomlinson, Ian P. M. .
HUMAN MOLECULAR GENETICS, 2013, 22 (14) :2820-2828
[5]   An NRG Oncology/GOG study of molecular classification for risk prediction in endometrioid endometrial cancer [J].
Cosgrove, Casey M. ;
Tritchler, David L. ;
Cohn, David E. ;
Mutch, David G. ;
Rush, Craig M. ;
Lankes, Heather A. ;
Creasman, William T. ;
Miller, David S. ;
Ramirez, Nilsa C. ;
Geller, Melissa A. ;
Powell, Matthew A. ;
Backes, Floor J. ;
Landrum, Lisa M. ;
Timmers, Cynthia ;
Suarez, Adrian A. ;
Zaino, Richard J. ;
Pearl, Michael L. ;
DiSilvestro, Paul A. ;
Lele, Shashikant B. ;
Goodfellow, Paul J. .
GYNECOLOGIC ONCOLOGY, 2018, 148 (01) :174-180
[6]   Analysis of patients with endometrial carcinoma using the ProMise classifier: a pilot study from India [J].
Dahiya, Alka ;
Rajadurai, Abarna ;
Daniel, Sherin ;
Sebastian, Ajit ;
Thomas, Dhanya Susan ;
Thomas, Vinotha ;
George, Rachel ;
Ram, Thomas Samuel ;
Sathyamurthy, Arvind ;
Rebekah, Grace ;
Peedicayil, Abraham ;
Pai, Rekha ;
Thomas, Anitha .
ARCHIVES OF GYNECOLOGY AND OBSTETRICS, 2024, 309 (04) :1499-1508
[7]   Integrated genomic characterization of endometrial carcinoma [J].
Getz, Gad ;
Gabriel, Stacey B. ;
Cibulskis, Kristian ;
Lander, Eric ;
Sivachenko, Andrey ;
Sougnez, Carrie ;
Lawrence, Mike ;
Kandoth, Cyriac ;
Dooling, David ;
Fulton, Robert ;
Fulton, Lucinda ;
Kalicki-Veizer, Joelle ;
McLellan, Michael D. ;
O'Laughlin, Michelle ;
Schmidt, Heather ;
Wilson, Richard K. ;
Ye, Kai ;
Ding, Li ;
Mardis, Elaine R. ;
Ally, Adrian ;
Balasundaram, Miruna ;
Birol, Inanc ;
Butterfield, Yaron S. N. ;
Carlsen, Rebecca ;
Carter, Candace ;
Chu, Andy ;
Chuah, Eric ;
Chun, Hye-Jung E. ;
Dhalla, Noreen ;
Guin, Ranabir ;
Hirst, Carrie ;
Holt, Robert A. ;
Jones, Steven J. M. ;
Lee, Darlene ;
Li, Haiyan I. ;
Marra, Marco A. ;
Mayo, Michael ;
Moore, Richard A. ;
Mungall, Andrew J. ;
Plettner, Patrick ;
Schein, Jacqueline E. ;
Sipahimalani, Payal ;
Tam, Angela ;
Varhol, Richard J. ;
Robertson, A. Gordon ;
Pashtan, Itai ;
Saksena, Gordon ;
Onofrio, Robert C. ;
Schumacher, Steven E. ;
Tabak, Barbara .
NATURE, 2013, 497 (7447) :67-73
[8]   POLE mutation combined with microcystic, elongated and fragmented (MELF) pattern invasion in endometrial carcinomas might be associated with poor survival in Chinese women [J].
He, Dan ;
Wang, Hui ;
Dong, Ying ;
Zhang, Yan ;
Zhao, Jian ;
Lv, Conghui ;
Zheng, Xianjing ;
Li, Dong ;
Li, Ting .
GYNECOLOGIC ONCOLOGY, 2020, 159 (01) :36-42
[9]   Phenotype of POLE-mutated endometrial cancer [J].
Imboden, Sara ;
Nastic, Denis ;
Ghaderi, Mehran ;
Rydberg, Filippa ;
Rau, Tilman T. ;
Mueller, Michael D. ;
Epstein, Elisabeth ;
Carlson, Joseph W. .
PLOS ONE, 2019, 14 (03)
[10]  
Jumaah AS, 2020, J PATHOL TRANSL MED, V54, P471
123