An NRG Oncology/GOG study of molecular classification for risk prediction in endometrioid endometrial cancer

Casey M. Cosgrove; David L. Tritchler; David E. Cohn; David G. Mutch; Craig M. Rush; Heather A. Lankes; William T. Creasman; David S. Miller; Nilsa C. Ramirez; Melissa A. Geller; Matthew A. Powell; Floor J. Backes; Lisa M. Landrum; Cynthia Timmers; Adrian A. Suarez; Richard J. Zaino; Michael L. Pearl; Paul A. DiSilvestro; Shashikant B. Lele; Paul J. Goodfellow

doi:10.1016/j.ygyno.2017.10.037

An NRG Oncology/GOG study of molecular classification for risk prediction in endometrioid endometrial cancer

Casey M. Cosgrove, David L. Tritchler, David E. Cohn, David G. Mutch, Craig M. Rush, Heather A. Lankes, William T. Creasman, David S. Miller, Nilsa C. Ramirez, Melissa A. Geller, Matthew A. Powell, Floor J. Backes, Lisa M. Landrum, Cynthia Timmers, Adrian A. Suarez, Richard J. Zaino, Michael L. Pearl, Paul A. DiSilvestro, Shashikant B. Lele, Paul J. Goodfellow

Obstetrics, Gynecology and Women's Health - Oncology

Research output: Contribution to journal › Article › peer-review

85 Scopus citations

Abstract

Objectives The purpose of this study was to assess the prognostic significance of a simplified, clinically accessible classification system for endometrioid endometrial cancers combining Lynch syndrome screening and molecular risk stratification. Methods Tumors from NRG/GOG GOG210 were evaluated for mismatch repair defects (MSI, MMR IHC, and MLH1 methylation), POLE mutations, and loss of heterozygosity. TP53 was evaluated in a subset of cases. Tumors were assigned to four molecular classes. Relationships between molecular classes and clinicopathologic variables were assessed using contingency tests and Cox proportional methods. Results Molecular classification was successful for 982 tumors. Based on the NCI consensus MSI panel assessing MSI and loss of heterozygosity combined with POLE testing, 49% of tumors were classified copy number stable (CNS), 39% MMR deficient, 8% copy number altered (CNA) and 4% POLE mutant. Cancer-specific mortality occurred in 5% of patients with CNS tumors; 2.6% with POLE tumors; 7.6% with MMR deficient tumors and 19% with CNA tumors. The CNA group had worse progression-free (HR 2.31, 95%CI 1.53–3.49) and cancer-specific survival (HR 3.95; 95%CI 2.10–7.44). The POLE group had improved outcomes, but the differences were not statistically significant. CNA class remained significant for cancer-specific survival (HR 2.11; 95%CI 1.04–4.26) in multivariable analysis. The CNA molecular class was associated with TP53 mutation and expression status. Conclusions A simple molecular classification for endometrioid endometrial cancers that can be easily combined with Lynch syndrome screening provides important prognostic information. These findings support prospective clinical validation and further studies on the predictive value of a simplified molecular classification system.

Original language	English (US)
Pages (from-to)	174-180
Number of pages	7
Journal	Gynecologic oncology
Volume	148
Issue number	1
DOIs	https://doi.org/10.1016/j.ygyno.2017.10.037
State	Published - Jan 2018

Bibliographical note

Funding Information:
The project described was supported by Award Number Grant UL1TR001070 from the National Center For Advancing Translational Sciences . The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Center For Advancing Translational Sciences or the National Institutes of Health.

Funding Information:
This work was supported by The Ohio State University (OSU) and James Comprehensive Cancer Center (CCC), James CCC Genomics , and Solid Tumor Translational Shared Resources ( P30CA016058 ), OSU Clinical & Translational Science Award ( UL1TR001070 ), SPORE in Endometrial Cancer ( P50CA134254 ), National Cancer Institute Grants U10CA27469 (Gynecologic Oncology Group [GOG] Administrative Office), U10 CA37517 (GOG Statistical Office), U10 CA180822 (NRG Oncology Group), U24 CA114793 (GOG Tissue Bank), and U10 CA180868 (NRG Operations).

Publisher Copyright:
© 2017 Elsevier Inc.

Keywords

Combined Lynch syndrome screening and molecular classification
Endometrioid endometrial cancer
Molecular classification
Prognosis

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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Cosgrove, C. M., Tritchler, D. L., Cohn, D. E., Mutch, D. G., Rush, C. M., Lankes, H. A., Creasman, W. T., Miller, D. S., Ramirez, N. C., Geller, M. A., Powell, M. A., Backes, F. J., Landrum, L. M., Timmers, C., Suarez, A. A., Zaino, R. J., Pearl, M. L., DiSilvestro, P. A., Lele, S. B., & Goodfellow, P. J. (2018). An NRG Oncology/GOG study of molecular classification for risk prediction in endometrioid endometrial cancer. Gynecologic oncology, 148(1), 174-180. https://doi.org/10.1016/j.ygyno.2017.10.037

Cosgrove, CM, Tritchler, DL, Cohn, DE, Mutch, DG, Rush, CM, Lankes, HA, Creasman, WT, Miller, DS, Ramirez, NC, Geller, MA, Powell, MA, Backes, FJ, Landrum, LM, Timmers, C, Suarez, AA, Zaino, RJ, Pearl, ML, DiSilvestro, PA, Lele, SB & Goodfellow, PJ 2018, 'An NRG Oncology/GOG study of molecular classification for risk prediction in endometrioid endometrial cancer', Gynecologic oncology, vol. 148, no. 1, pp. 174-180. https://doi.org/10.1016/j.ygyno.2017.10.037

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abstract = "Objectives The purpose of this study was to assess the prognostic significance of a simplified, clinically accessible classification system for endometrioid endometrial cancers combining Lynch syndrome screening and molecular risk stratification. Methods Tumors from NRG/GOG GOG210 were evaluated for mismatch repair defects (MSI, MMR IHC, and MLH1 methylation), POLE mutations, and loss of heterozygosity. TP53 was evaluated in a subset of cases. Tumors were assigned to four molecular classes. Relationships between molecular classes and clinicopathologic variables were assessed using contingency tests and Cox proportional methods. Results Molecular classification was successful for 982 tumors. Based on the NCI consensus MSI panel assessing MSI and loss of heterozygosity combined with POLE testing, 49% of tumors were classified copy number stable (CNS), 39% MMR deficient, 8% copy number altered (CNA) and 4% POLE mutant. Cancer-specific mortality occurred in 5% of patients with CNS tumors; 2.6% with POLE tumors; 7.6% with MMR deficient tumors and 19% with CNA tumors. The CNA group had worse progression-free (HR 2.31, 95%CI 1.53–3.49) and cancer-specific survival (HR 3.95; 95%CI 2.10–7.44). The POLE group had improved outcomes, but the differences were not statistically significant. CNA class remained significant for cancer-specific survival (HR 2.11; 95%CI 1.04–4.26) in multivariable analysis. The CNA molecular class was associated with TP53 mutation and expression status. Conclusions A simple molecular classification for endometrioid endometrial cancers that can be easily combined with Lynch syndrome screening provides important prognostic information. These findings support prospective clinical validation and further studies on the predictive value of a simplified molecular classification system.",

keywords = "Combined Lynch syndrome screening and molecular classification, Endometrioid endometrial cancer, Molecular classification, Prognosis",

author = "Cosgrove, {Casey M.} and Tritchler, {David L.} and Cohn, {David E.} and Mutch, {David G.} and Rush, {Craig M.} and Lankes, {Heather A.} and Creasman, {William T.} and Miller, {David S.} and Ramirez, {Nilsa C.} and Geller, {Melissa A.} and Powell, {Matthew A.} and Backes, {Floor J.} and Landrum, {Lisa M.} and Cynthia Timmers and Suarez, {Adrian A.} and Zaino, {Richard J.} and Pearl, {Michael L.} and DiSilvestro, {Paul A.} and Lele, {Shashikant B.} and Goodfellow, {Paul J.}",

note = "Funding Information: The project described was supported by Award Number Grant UL1TR001070 from the National Center For Advancing Translational Sciences . The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Center For Advancing Translational Sciences or the National Institutes of Health. Funding Information: This work was supported by The Ohio State University (OSU) and James Comprehensive Cancer Center (CCC), James CCC Genomics , and Solid Tumor Translational Shared Resources ( P30CA016058 ), OSU Clinical & Translational Science Award ( UL1TR001070 ), SPORE in Endometrial Cancer ( P50CA134254 ), National Cancer Institute Grants U10CA27469 (Gynecologic Oncology Group [GOG] Administrative Office), U10 CA37517 (GOG Statistical Office), U10 CA180822 (NRG Oncology Group), U24 CA114793 (GOG Tissue Bank), and U10 CA180868 (NRG Operations). Publisher Copyright: {\textcopyright} 2017 Elsevier Inc.",

year = "2018",

month = jan,

doi = "10.1016/j.ygyno.2017.10.037",

language = "English (US)",

volume = "148",

pages = "174--180",

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T1 - An NRG Oncology/GOG study of molecular classification for risk prediction in endometrioid endometrial cancer

AU - Cosgrove, Casey M.

AU - Tritchler, David L.

AU - Cohn, David E.

AU - Mutch, David G.

AU - Rush, Craig M.

AU - Lankes, Heather A.

AU - Creasman, William T.

AU - Miller, David S.

AU - Ramirez, Nilsa C.

AU - Geller, Melissa A.

AU - Powell, Matthew A.

AU - Backes, Floor J.

AU - Landrum, Lisa M.

AU - Timmers, Cynthia

AU - Suarez, Adrian A.

AU - Zaino, Richard J.

AU - Pearl, Michael L.

AU - DiSilvestro, Paul A.

AU - Lele, Shashikant B.

AU - Goodfellow, Paul J.

N1 - Funding Information: The project described was supported by Award Number Grant UL1TR001070 from the National Center For Advancing Translational Sciences . The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Center For Advancing Translational Sciences or the National Institutes of Health. Funding Information: This work was supported by The Ohio State University (OSU) and James Comprehensive Cancer Center (CCC), James CCC Genomics , and Solid Tumor Translational Shared Resources ( P30CA016058 ), OSU Clinical & Translational Science Award ( UL1TR001070 ), SPORE in Endometrial Cancer ( P50CA134254 ), National Cancer Institute Grants U10CA27469 (Gynecologic Oncology Group [GOG] Administrative Office), U10 CA37517 (GOG Statistical Office), U10 CA180822 (NRG Oncology Group), U24 CA114793 (GOG Tissue Bank), and U10 CA180868 (NRG Operations). Publisher Copyright: © 2017 Elsevier Inc.

PY - 2018/1

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N2 - Objectives The purpose of this study was to assess the prognostic significance of a simplified, clinically accessible classification system for endometrioid endometrial cancers combining Lynch syndrome screening and molecular risk stratification. Methods Tumors from NRG/GOG GOG210 were evaluated for mismatch repair defects (MSI, MMR IHC, and MLH1 methylation), POLE mutations, and loss of heterozygosity. TP53 was evaluated in a subset of cases. Tumors were assigned to four molecular classes. Relationships between molecular classes and clinicopathologic variables were assessed using contingency tests and Cox proportional methods. Results Molecular classification was successful for 982 tumors. Based on the NCI consensus MSI panel assessing MSI and loss of heterozygosity combined with POLE testing, 49% of tumors were classified copy number stable (CNS), 39% MMR deficient, 8% copy number altered (CNA) and 4% POLE mutant. Cancer-specific mortality occurred in 5% of patients with CNS tumors; 2.6% with POLE tumors; 7.6% with MMR deficient tumors and 19% with CNA tumors. The CNA group had worse progression-free (HR 2.31, 95%CI 1.53–3.49) and cancer-specific survival (HR 3.95; 95%CI 2.10–7.44). The POLE group had improved outcomes, but the differences were not statistically significant. CNA class remained significant for cancer-specific survival (HR 2.11; 95%CI 1.04–4.26) in multivariable analysis. The CNA molecular class was associated with TP53 mutation and expression status. Conclusions A simple molecular classification for endometrioid endometrial cancers that can be easily combined with Lynch syndrome screening provides important prognostic information. These findings support prospective clinical validation and further studies on the predictive value of a simplified molecular classification system.

AB - Objectives The purpose of this study was to assess the prognostic significance of a simplified, clinically accessible classification system for endometrioid endometrial cancers combining Lynch syndrome screening and molecular risk stratification. Methods Tumors from NRG/GOG GOG210 were evaluated for mismatch repair defects (MSI, MMR IHC, and MLH1 methylation), POLE mutations, and loss of heterozygosity. TP53 was evaluated in a subset of cases. Tumors were assigned to four molecular classes. Relationships between molecular classes and clinicopathologic variables were assessed using contingency tests and Cox proportional methods. Results Molecular classification was successful for 982 tumors. Based on the NCI consensus MSI panel assessing MSI and loss of heterozygosity combined with POLE testing, 49% of tumors were classified copy number stable (CNS), 39% MMR deficient, 8% copy number altered (CNA) and 4% POLE mutant. Cancer-specific mortality occurred in 5% of patients with CNS tumors; 2.6% with POLE tumors; 7.6% with MMR deficient tumors and 19% with CNA tumors. The CNA group had worse progression-free (HR 2.31, 95%CI 1.53–3.49) and cancer-specific survival (HR 3.95; 95%CI 2.10–7.44). The POLE group had improved outcomes, but the differences were not statistically significant. CNA class remained significant for cancer-specific survival (HR 2.11; 95%CI 1.04–4.26) in multivariable analysis. The CNA molecular class was associated with TP53 mutation and expression status. Conclusions A simple molecular classification for endometrioid endometrial cancers that can be easily combined with Lynch syndrome screening provides important prognostic information. These findings support prospective clinical validation and further studies on the predictive value of a simplified molecular classification system.

KW - Combined Lynch syndrome screening and molecular classification

KW - Endometrioid endometrial cancer

KW - Molecular classification

KW - Prognosis

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An NRG Oncology/GOG study of molecular classification for risk prediction in endometrioid endometrial cancer

Abstract

Bibliographical note

Keywords

UN SDGs

Access

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