Inflammation as a risk factor for the development of frailty in the Lothian Birth Cohort 1936
Inflammation as a risk factor for the development of frailty in the Lothian Birth Cohort 1936
Background
Research suggests that frailty is associated with higher inflammation levels. We investigated the longitudinal association between chronic inflammation and frailty progression.
Methods
Participants of the Lothian Birth Cohort 1936, aged 70 at baseline were tested four times over 12 years (wave 1: n = 1091, wave 4: n = 550). Frailty was assessed by; the Frailty Index at waves 1–4 and Fried phenotype at waves 1, 3 and 4. Two blood-based inflammatory biomarkers were measured at wave 1: Fibrinogen and C-reactive protein (CRP).
Results
Fully-adjusted, linear mixed effects models showed higher Fibrinogen was significantly associated with higher wave 1 Frailty Index score (β = 0.011, 95% CI[0.002,0.020], p < .05). Over 12 year follow-up, higher wave 1 CRP (β = 0.001, 95% CI[0.000,0.002], p < .05) and Fibrinogen (β = 0.004, 95% CI[0.001,0.007], p < .05) were significantly associated with increased Frailty Index change. For the Fried phenotype, wave 1 Pre-frail and Frail participants had higher CRP and Fibrinogen than Non-frail participants (p < .001). Logistic regression models calculated risk of worsening frailty over follow-up and we observed no significant association of CRP or Fibrinogen in minimally-adjusted nor fully-adjusted models.
Conclusions
Findings showed a longitudinal association of higher wave 1 CRP and Fibrinogen on worsening frailty in the Frailty Index, but not Fried Phenotype. A possible explanation for this disparity may lie in the conceptual differences between frailty measures (a biopsychosocial vs physical approach). Future research, which further explores different domains of frailty, as well the associations between improving frailty and inflammation levels, may elucidate the pathway through which inflammation influences frailty progression. This may improve earlier identification of those at high frailty risk.
Welstead, M.
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Muniz-Terrera, G.
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Russ, Tom C.
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Corley, Janie
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Taylor, A. M.
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Gale, Catharine
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Luciano, M.
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1 October 2020
Welstead, M.
840f560f-c1a9-4eb7-9d06-486061fad9b7
Muniz-Terrera, G.
b1dd9234-1c31-4991-ad7a-94dbb67437af
Russ, Tom C.
e1750d17-78d5-444c-b5c2-4c680aeed263
Corley, Janie
1c668444-972e-4cc9-b1c2-8bc2eb83c870
Taylor, A. M.
2fbe4b3e-acbb-4f86-8024-8f234c4b366b
Gale, Catharine
5bb2abb3-7b53-42d6-8aa7-817e193140c8
Luciano, M.
a153a93b-bf45-4cae-8b9c-32779d8ec20c
Welstead, M., Muniz-Terrera, G., Russ, Tom C., Corley, Janie, Taylor, A. M., Gale, Catharine and Luciano, M.
(2020)
Inflammation as a risk factor for the development of frailty in the Lothian Birth Cohort 1936.
Experimental Gerontology, 139 (1), [111055].
(doi:10.1016/j.exger.2020.111055).
Abstract
Background
Research suggests that frailty is associated with higher inflammation levels. We investigated the longitudinal association between chronic inflammation and frailty progression.
Methods
Participants of the Lothian Birth Cohort 1936, aged 70 at baseline were tested four times over 12 years (wave 1: n = 1091, wave 4: n = 550). Frailty was assessed by; the Frailty Index at waves 1–4 and Fried phenotype at waves 1, 3 and 4. Two blood-based inflammatory biomarkers were measured at wave 1: Fibrinogen and C-reactive protein (CRP).
Results
Fully-adjusted, linear mixed effects models showed higher Fibrinogen was significantly associated with higher wave 1 Frailty Index score (β = 0.011, 95% CI[0.002,0.020], p < .05). Over 12 year follow-up, higher wave 1 CRP (β = 0.001, 95% CI[0.000,0.002], p < .05) and Fibrinogen (β = 0.004, 95% CI[0.001,0.007], p < .05) were significantly associated with increased Frailty Index change. For the Fried phenotype, wave 1 Pre-frail and Frail participants had higher CRP and Fibrinogen than Non-frail participants (p < .001). Logistic regression models calculated risk of worsening frailty over follow-up and we observed no significant association of CRP or Fibrinogen in minimally-adjusted nor fully-adjusted models.
Conclusions
Findings showed a longitudinal association of higher wave 1 CRP and Fibrinogen on worsening frailty in the Frailty Index, but not Fried Phenotype. A possible explanation for this disparity may lie in the conceptual differences between frailty measures (a biopsychosocial vs physical approach). Future research, which further explores different domains of frailty, as well the associations between improving frailty and inflammation levels, may elucidate the pathway through which inflammation influences frailty progression. This may improve earlier identification of those at high frailty risk.
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More information
Accepted/In Press date: 7 August 2020
e-pub ahead of print date: 11 August 2020
Published date: 1 October 2020
Identifiers
Local EPrints ID: 453742
URI: http://eprints.soton.ac.uk/id/eprint/453742
ISSN: 0531-5565
PURE UUID: e00de01a-5d22-4b49-8464-fd7bb634e94b
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Date deposited: 21 Jan 2022 17:48
Last modified: 17 Mar 2024 02:42
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Contributors
Author:
M. Welstead
Author:
G. Muniz-Terrera
Author:
Tom C. Russ
Author:
Janie Corley
Author:
A. M. Taylor
Author:
M. Luciano
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