DNA methylation profiling to predict recurrence risk in meningioma: development and validation of a nomogram to optimize clinical management

Authors

Farshad Nassiri
Yasin Mamatjan
Suganth Suppiah
Jetan H. Badhiwala
Sheila Mansouri
Shirin Karimi
Olli Saarela
Laila M. Poisson, Henry Ford Health Sciences CenterFollow
Irina Gepfner-Tuma
Jens Schittenhelm
Ho-Keung Ng
Houtan Noushmehr, Henry Ford HealthFollow
Patrick Harter
Peter Baumgarten
Michael Weller
Matthias Preusser
Christel Herold-Mende
Marcos Tatagiba
Ghazaleh Tabatabai
Felix Sahm
Andreas von Deimling
Gelareh Zadeh
Kenneth D. Aldape

Recommended Citation

Nassiri F, Mamatjan Y, Suppiah S, Badhiwala JH, Mansouri S, Karimi S, Saarela O, Poisson L, Gepfner-Tuma I, Schittenhelm J, Ng HK, Noushmehr H, Harter P, Baumgarten P, Weller M, Preusser M, Herold-Mende C, Tatagiba M, Tabatabai G, Sahm F, von Deimling A, Zadeh G, and Aldape KD. DNA methylation profiling to predict recurrence risk in meningioma: development and validation of a nomogram to optimize clinical management. Neuro Oncol 2019; Epub ahead of print.

Document Type

Article

Publication Date

6-3-2019

Publication Title

Neuro Oncol

Abstract

BACKGROUND: Variability in standard-of-care classifications precludes accurate predictions of early tumor recurrence for individual patients with meningioma, limiting the appropriate selection of patients who would benefit from adjuvant radiotherapy to delay recurrence. We aimed to develop an individualized prediction model of early recurrence risk combining clinical and molecular factors in meningioma.

METHODS: DNA methylation profiles of clinically annotated tumor samples across multiple institutions were used to develop a methylome model of 5-year recurrence-free survival (RFS). Subsequently, a 5-year meningioma recurrence score was generated using a nomogram that integrated the methylome model with established prognostic clinical factors. Performance of both models was evaluated and compared with standard-of-care models using multiple independent cohorts.

RESULTS: The methylome-based predictor of 5-year RFS performed favorably compared with a grade-based predictor when tested using the 3 validation cohorts (ΔAUC = 0.10, 95% CI: 0.03-0.018) and was independently associated with RFS after adjusting for histopathologic grade, extent of resection, and burden of copy number alterations (hazard ratio 3.6, 95% CI: 1.8-7.2, P < 0.001). A nomogram combining the methylome predictor with clinical factors demonstrated greater discrimination than a nomogram using clinical factors alone in 2 independent validation cohorts (ΔAUC = 0.25, 95% CI: 0.22-0.27) and resulted in 2 groups with distinct recurrence patterns (hazard ratio 7.7, 95% CI: 5.3-11.1, P < 0.001) with clinical implications.

CONCLUSIONS: The models developed and validated in this study provide important prognostic information not captured by previously established clinical and molecular factors which could be used to individualize decisions regarding postoperative therapeutic interventions, in particular whether to treat patients with adjuvant radiotherapy versus observation alone.

PubMed ID

31158293

ePublication

ePub ahead of print