The MIDA Mortality Risk Score: development and external validation of a prognostic model for early and late death in degenerative mitral regurgitation

Francesco Grigioni,Marie-Annick Clavel,Jean-Louis Vanoverschelde,Christophe Tribouilloy,Rodolfo Pizarro,Marianne Huebner,Jean-François Avierinos,Andrea Barbieri,Rakesh M. Suri,Agnes Pasquet,Dan Rusinaru,Gaetano Gargiulo,Pablo Oberti,Alexis Theron,Francesca Bursi,Hector I. Michelena,Siham Lazam,Catherine Szymanski,Vuyisile T. Nkomo,Martin Schumacher,Letizia Bacchi Reggiani,Maurice Enriquez-Sarano,C. Tribouilloy,F. Trojette,C. Szymanski,Dan Rusinaru,G. Touati,J P Remadi,F. Grigioni,A. Russo,E. Biagini,F. Pasquale,M Ferlito,C. Rapezzi,C. Savini,G. Marinelli,D. Pacini,G D Gargiulo,R. Di Bartolomeo,I. Corazza,P Oberti,R Pizarro,J Boulif,C. De Meester,G. El Khoury,B Gerber,S. Lazam,Agnès Pasquet,P. Noirhomme,D. Vancraeynest,J.-L. Vanoverschelde,J.F. Avierinos,F. Collard,A. Théron,G. Habib,A. Barbieri,F Bursi,F. Mantovani,R. Lugli,M. G. Modena,G. Boriani,M A Clavel,J. Maalouf,H. Michelena,M Enriquez Sarano,R. Suri,L. Bacchi-Reggiani,M. Schumacher,M. Huebner

The MIDA Mortality Risk Score: development and external validation of a prognostic model for early and late death in degenerative mitral regurgitation

2018

Aims: In degenerative mitral regurgitation (DMR), lack of mortality scores predicting death favours misperception of individual patients' risk and inappropriate decision-making. Methods and results: The Mitral Regurgitation International Database (MIDA) registries include 3666 patients (age 66 ± 14 years; 70% males; follow-up 7.8 ± 5.0 years) with pure, isolated, DMR consecutively diagnosed by echocardiography at tertiary (European/North/South-American) centres. The MIDA Score was derived from the MIDA-Flail-Registry (2472 patients with DMR and flail leaflet-Derivation Cohort) by weighting all guideline-provided prognostic markers, and externally validated in the MIDA-BNP-Registry (1194 patients with DMR and flail leaflet/prolapse-Validation Cohort). The MIDA Score ranged from 0 to 12 depending on accumulating risk factors. In predicting total mortality post-diagnosis, the MIDA Score showed excellent concordance both in Derivation Cohort (c = 0.78) and Validation Cohort (c = 0.81). In the whole MIDA population (n = 3666 patients), 1-year mortality with Scores 0, 7-8, and 11-12 was 0.4, 17, and 48% under medical management and 1, 7, and 14% after surgery, respectively (P < 0.001). Five-year survival with Scores 0, 7-8, and 11-12 was 98 ± 1, 57 ± 4, and 21 ± 10% under medical management and 99 ± 1, 82 ± 2, and 57 ± 9% after surgery (P < 0.001). In models including all guideline-provided prognostic markers and the EuroScoreII, the MIDA Score provided incremental prognostic information (P ≤ 0.002). Conclusion: The MIDA Score may represent an innovative tool for DMR management, being able to position a given patient within a continuous spectrum of short- and long-term mortality risk, either under medical or surgical management. This innovative prognostic indicator may provide a specific framework for future clinical trials aiming to compare new technologies for DMR treatment in homogeneous risk categories of patients.

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