The ability of three different models of frailty to predict all-cause mortality: Results from the European Male Aging Study (EMAS)

Rathi Ravindrarajah; David M. Lee; Stephen R. Pye; Evelien Gielen; Steven Boonen; Dirk Vanderschueren; Neil Pendleton; Joseph D. Finn; Abdelouahid Tajar; Matthew D.L. O'Connell; Kenneth Rockwood; György Bartfai; Felipe F. Casanueva; Gianni Forti; Aleksander Giwercman; Thang S. Han; Ilpo T. Huhtaniemi; Krzysztof Kula; Michael E.J. Lean; Margus Punab; Frederick C.W. Wu; Terence W. O'Neill; Luisa Petrone; Giovanni Corona; Herman Borghs; Jolanta Slowikowska-Hilczer; Renata Walczak-Jedrzejowska; Ilpo Huhtaniemi; Philip Steer; Ana I. Castro; Imre Földesi; Imre Fejes; Paul Korrovitz; Min Jiang

doi:10.1016/j.archger.2013.06.010

The ability of three different models of frailty to predict all-cause mortality: Results from the European Male Aging Study (EMAS)

Rathi Ravindrarajah, David M. Lee, Stephen R. Pye, Evelien Gielen, Steven Boonen, Dirk Vanderschueren, Neil Pendleton, Joseph D. Finn, Abdelouahid Tajar, Matthew D.L. O'Connell, Kenneth Rockwood, György Bartfai, Felipe F. Casanueva, Gianni Forti, Aleksander Giwercman, Thang S. Han, Ilpo T. Huhtaniemi, Krzysztof Kula, Michael E.J. Lean, Margus PunabFrederick C.W. Wu, Terence W. O'Neill, Luisa Petrone, Giovanni Corona, Herman Borghs, Jolanta Slowikowska-Hilczer, Renata Walczak-Jedrzejowska, Ilpo Huhtaniemi, Philip Steer, Ana I. Castro, Imre Földesi, Imre Fejes, Paul Korrovitz, Min Jiang

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124 Citas (Scopus)

Resumen

Few studies have directly compared the ability of the most commonly used models of frailty to predict mortality among community-dwelling individuals. Here, we used a frailty index (FI), frailty phenotype (FP), and FRAIL scale (FS) to predict mortality in the EMAS. Participants were aged 40-79 years (n=2929) at baseline and 6.6% (n=193) died over a median 4.3 years of follow-up. The FI was generated from 39 deficits, including self-reported health, morbidities, functional performance and psychological assessments. The FP and FS consisted of five phenotypic criteria and both categorized individuals as robust when they had 0 criteria, prefrail as 1-2 criteria and frail as 3+ criteria. The mean FI increased linearly with age (r²=0.21) and in Cox regression models adjusted for age, center, smoking and partner status the hazard ratio (HR) for death for each unit increase of the FI was 1.49. Men who were prefrail or frail by either the FP or FS definitions, had a significantly increased risk of death compared to their robust counterparts. Compared to robust men, those who were FP frail at baseline had a HR for death of 3.84, while those who were FS frail had a HR of 3.87. All three frailty models significantly predicted future mortality among community-dwelling, middle-aged and older European men after adjusting for potential confounders. Our data suggest that the choice of frailty model may not be of paramount importance when predicting future risk of death, enabling flexibility in the approach used.

Idioma original	English
Páginas (desde-hasta)	360-368
Número de páginas	9
Publicación	Archives of Gerontology and Geriatrics
Volumen	57
N.º	3
DOI	https://doi.org/10.1016/j.archger.2013.06.010
Estado	Published - nov. 2013

Nota bibliográfica

Funding Information:
The European Male Aging Study is funded by the Commission of the European Communities Fifth Framework Program “Quality of Life and Management of Living Resources” Grant QLK6-CT-2001-00258 . Non-financial support was also provided by Arthritis Research UK and the National Institute for Health Research Manchester Biomedical Research Center . The authors wish to thank the men who participated, the research/nursing staff in the eight centers: C. Pott (Manchester), E. Wouters (Leuven), M. Nilsson (Malmö), M. del Mar Fernandez (Santiago de Compostela), M. Jedrzejowska (Łódź), H.-M. Tabo (Tartu), A. Heredi (Szeged) for data collection, and C. Moseley (Manchester) for data entry and project co-ordination. S. Boonen is a senior clinical investigator of the Fund for Scientific Research, Flanders, Belgium (FWO – Vlaanderen); D. Vanderschueren is a senior clinical investigator supported by the Clinical Research Fund of the University Hospitals Leuven, Belgium .

ASJC Scopus Subject Areas

Health(social science)
Ageing
Gerontology
Geriatrics and Gerontology

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10.1016/j.archger.2013.06.010

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Ravindrarajah, R., Lee, D. M., Pye, S. R., Gielen, E., Boonen, S., Vanderschueren, D., Pendleton, N., Finn, J. D., Tajar, A., O'Connell, M. D. L., Rockwood, K., Bartfai, G., Casanueva, F. F., Forti, G., Giwercman, A., Han, T. S., Huhtaniemi, I. T., Kula, K., Lean, M. E. J., ... Jiang, M. (2013). The ability of three different models of frailty to predict all-cause mortality: Results from the European Male Aging Study (EMAS). Archives of Gerontology and Geriatrics, 57(3), 360-368. https://doi.org/10.1016/j.archger.2013.06.010

Ravindrarajah, R, Lee, DM, Pye, SR, Gielen, E, Boonen, S, Vanderschueren, D, Pendleton, N, Finn, JD, Tajar, A, O'Connell, MDL, Rockwood, K, Bartfai, G, Casanueva, FF, Forti, G, Giwercman, A, Han, TS, Huhtaniemi, IT, Kula, K, Lean, MEJ, Punab, M, Wu, FCW, O'Neill, TW, Petrone, L, Corona, G, Borghs, H, Slowikowska-Hilczer, J, Walczak-Jedrzejowska, R, Huhtaniemi, I, Steer, P, Castro, AI, Földesi, I, Fejes, I, Korrovitz, P & Jiang, M 2013, 'The ability of three different models of frailty to predict all-cause mortality: Results from the European Male Aging Study (EMAS)', Archives of Gerontology and Geriatrics, vol. 57, n.º 3, pp. 360-368. https://doi.org/10.1016/j.archger.2013.06.010

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title = "The ability of three different models of frailty to predict all-cause mortality: Results from the European Male Aging Study (EMAS)",

abstract = "Few studies have directly compared the ability of the most commonly used models of frailty to predict mortality among community-dwelling individuals. Here, we used a frailty index (FI), frailty phenotype (FP), and FRAIL scale (FS) to predict mortality in the EMAS. Participants were aged 40-79 years (n=2929) at baseline and 6.6% (n=193) died over a median 4.3 years of follow-up. The FI was generated from 39 deficits, including self-reported health, morbidities, functional performance and psychological assessments. The FP and FS consisted of five phenotypic criteria and both categorized individuals as robust when they had 0 criteria, prefrail as 1-2 criteria and frail as 3+ criteria. The mean FI increased linearly with age (r2=0.21) and in Cox regression models adjusted for age, center, smoking and partner status the hazard ratio (HR) for death for each unit increase of the FI was 1.49. Men who were prefrail or frail by either the FP or FS definitions, had a significantly increased risk of death compared to their robust counterparts. Compared to robust men, those who were FP frail at baseline had a HR for death of 3.84, while those who were FS frail had a HR of 3.87. All three frailty models significantly predicted future mortality among community-dwelling, middle-aged and older European men after adjusting for potential confounders. Our data suggest that the choice of frailty model may not be of paramount importance when predicting future risk of death, enabling flexibility in the approach used.",

author = "Rathi Ravindrarajah and Lee, {David M.} and Pye, {Stephen R.} and Evelien Gielen and Steven Boonen and Dirk Vanderschueren and Neil Pendleton and Finn, {Joseph D.} and Abdelouahid Tajar and O'Connell, {Matthew D.L.} and Kenneth Rockwood and Gy{\"o}rgy Bartfai and Casanueva, {Felipe F.} and Gianni Forti and Aleksander Giwercman and Han, {Thang S.} and Huhtaniemi, {Ilpo T.} and Krzysztof Kula and Lean, {Michael E.J.} and Margus Punab and Wu, {Frederick C.W.} and O'Neill, {Terence W.} and Luisa Petrone and Giovanni Corona and Herman Borghs and Jolanta Slowikowska-Hilczer and Renata Walczak-Jedrzejowska and Ilpo Huhtaniemi and Philip Steer and Castro, {Ana I.} and Imre F{\"o}ldesi and Imre Fejes and Paul Korrovitz and Min Jiang",

note = "Funding Information: The European Male Aging Study is funded by the Commission of the European Communities Fifth Framework Program “Quality of Life and Management of Living Resources” Grant QLK6-CT-2001-00258 . Non-financial support was also provided by Arthritis Research UK and the National Institute for Health Research Manchester Biomedical Research Center . The authors wish to thank the men who participated, the research/nursing staff in the eight centers: C. Pott (Manchester), E. Wouters (Leuven), M. Nilsson (Malm{\"o}), M. del Mar Fernandez (Santiago de Compostela), M. Jedrzejowska ({\L}{\'o}d{\'z}), H.-M. Tabo (Tartu), A. Heredi (Szeged) for data collection, and C. Moseley (Manchester) for data entry and project co-ordination. S. Boonen is a senior clinical investigator of the Fund for Scientific Research, Flanders, Belgium (FWO – Vlaanderen); D. Vanderschueren is a senior clinical investigator supported by the Clinical Research Fund of the University Hospitals Leuven, Belgium . ",

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doi = "10.1016/j.archger.2013.06.010",

language = "English",

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T1 - The ability of three different models of frailty to predict all-cause mortality

T2 - Results from the European Male Aging Study (EMAS)

AU - Ravindrarajah, Rathi

AU - Lee, David M.

AU - Pye, Stephen R.

AU - Gielen, Evelien

AU - Boonen, Steven

AU - Vanderschueren, Dirk

AU - Pendleton, Neil

AU - Finn, Joseph D.

AU - Tajar, Abdelouahid

AU - O'Connell, Matthew D.L.

AU - Rockwood, Kenneth

AU - Bartfai, György

AU - Casanueva, Felipe F.

AU - Forti, Gianni

AU - Giwercman, Aleksander

AU - Han, Thang S.

AU - Huhtaniemi, Ilpo T.

AU - Kula, Krzysztof

AU - Lean, Michael E.J.

AU - Punab, Margus

AU - Wu, Frederick C.W.

AU - O'Neill, Terence W.

AU - Petrone, Luisa

AU - Corona, Giovanni

AU - Borghs, Herman

AU - Slowikowska-Hilczer, Jolanta

AU - Walczak-Jedrzejowska, Renata

AU - Huhtaniemi, Ilpo

AU - Steer, Philip

AU - Castro, Ana I.

AU - Földesi, Imre

AU - Fejes, Imre

AU - Korrovitz, Paul

AU - Jiang, Min

N1 - Funding Information: The European Male Aging Study is funded by the Commission of the European Communities Fifth Framework Program “Quality of Life and Management of Living Resources” Grant QLK6-CT-2001-00258 . Non-financial support was also provided by Arthritis Research UK and the National Institute for Health Research Manchester Biomedical Research Center . The authors wish to thank the men who participated, the research/nursing staff in the eight centers: C. Pott (Manchester), E. Wouters (Leuven), M. Nilsson (Malmö), M. del Mar Fernandez (Santiago de Compostela), M. Jedrzejowska (Łódź), H.-M. Tabo (Tartu), A. Heredi (Szeged) for data collection, and C. Moseley (Manchester) for data entry and project co-ordination. S. Boonen is a senior clinical investigator of the Fund for Scientific Research, Flanders, Belgium (FWO – Vlaanderen); D. Vanderschueren is a senior clinical investigator supported by the Clinical Research Fund of the University Hospitals Leuven, Belgium .

PY - 2013/11

Y1 - 2013/11

N2 - Few studies have directly compared the ability of the most commonly used models of frailty to predict mortality among community-dwelling individuals. Here, we used a frailty index (FI), frailty phenotype (FP), and FRAIL scale (FS) to predict mortality in the EMAS. Participants were aged 40-79 years (n=2929) at baseline and 6.6% (n=193) died over a median 4.3 years of follow-up. The FI was generated from 39 deficits, including self-reported health, morbidities, functional performance and psychological assessments. The FP and FS consisted of five phenotypic criteria and both categorized individuals as robust when they had 0 criteria, prefrail as 1-2 criteria and frail as 3+ criteria. The mean FI increased linearly with age (r2=0.21) and in Cox regression models adjusted for age, center, smoking and partner status the hazard ratio (HR) for death for each unit increase of the FI was 1.49. Men who were prefrail or frail by either the FP or FS definitions, had a significantly increased risk of death compared to their robust counterparts. Compared to robust men, those who were FP frail at baseline had a HR for death of 3.84, while those who were FS frail had a HR of 3.87. All three frailty models significantly predicted future mortality among community-dwelling, middle-aged and older European men after adjusting for potential confounders. Our data suggest that the choice of frailty model may not be of paramount importance when predicting future risk of death, enabling flexibility in the approach used.

AB - Few studies have directly compared the ability of the most commonly used models of frailty to predict mortality among community-dwelling individuals. Here, we used a frailty index (FI), frailty phenotype (FP), and FRAIL scale (FS) to predict mortality in the EMAS. Participants were aged 40-79 years (n=2929) at baseline and 6.6% (n=193) died over a median 4.3 years of follow-up. The FI was generated from 39 deficits, including self-reported health, morbidities, functional performance and psychological assessments. The FP and FS consisted of five phenotypic criteria and both categorized individuals as robust when they had 0 criteria, prefrail as 1-2 criteria and frail as 3+ criteria. The mean FI increased linearly with age (r2=0.21) and in Cox regression models adjusted for age, center, smoking and partner status the hazard ratio (HR) for death for each unit increase of the FI was 1.49. Men who were prefrail or frail by either the FP or FS definitions, had a significantly increased risk of death compared to their robust counterparts. Compared to robust men, those who were FP frail at baseline had a HR for death of 3.84, while those who were FS frail had a HR of 3.87. All three frailty models significantly predicted future mortality among community-dwelling, middle-aged and older European men after adjusting for potential confounders. Our data suggest that the choice of frailty model may not be of paramount importance when predicting future risk of death, enabling flexibility in the approach used.

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The ability of three different models of frailty to predict all-cause mortality: Results from the European Male Aging Study (EMAS)

Resumen

Nota bibliográfica

ASJC Scopus Subject Areas

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