Disclosure of Personalized Rheumatoid Arthritis Risk Using Genetics, Biomarkers, and Lifestyle Factors to Motivate Health Behavior Improvements: A Randomized Controlled Trial

Jeffrey A. Sparks; Maura D. Iversen; Zhi Yu; Nellie A. Triedman; Maria G. Prado; Rachel Miller Kroouze; Sarah S. Kalia; Michael L. Atkinson; Elinor A. Mody; Simon M. Helfgott; Derrick J. Todd; Paul F. Dellaripa; Bonnie L. Bermas; Karen H. Costenbader; Kevin D. Deane; Bing Lu; Robert C. Green; Elizabeth W. Karlson

doi:10.1002/acr.23411

Disclosure of Personalized Rheumatoid Arthritis Risk Using Genetics, Biomarkers, and Lifestyle Factors to Motivate Health Behavior Improvements: A Randomized Controlled Trial

Jeffrey A. Sparks, Maura D. Iversen, Zhi Yu, Nellie A. Triedman, Maria G. Prado, Rachel Miller Kroouze, Sarah S. Kalia, Michael L. Atkinson, Elinor A. Mody, Simon M. Helfgott, Derrick J. Todd, Paul F. Dellaripa, Bonnie L. Bermas, Karen H. Costenbader, Kevin D. Deane, Bing Lu, Robert C. Green, Elizabeth W. Karlson

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

47 Scopus citations

Abstract

Objective: To determine the effect of disclosure of rheumatoid arthritis (RA) risk personalized with genetics, biomarkers, and lifestyle factors on health behavior intentions. Methods: We performed a randomized controlled trial among first-degree relatives without RA. Subjects assigned to the Personalized Risk Estimator for Rheumatoid Arthritis (PRE-RA) group received the web-based PRE-RA tool for RA risk factor education and disclosure of personalized RA risk estimates, including genotype/autoantibody results and behaviors (n = 158). Subjects assigned to the comparison arm received standard RA education (n = 80). The primary outcome was readiness for change based on the trans-theoretical model, using validated contemplation ladder scales. Increased motivation to improve RA risk–related behaviors (smoking, diet, exercise, or dental hygiene) was defined as an increase in any ladder score compared to baseline, assessed immediately, 6 weeks, and 6 months post-intervention. Subjects reported behavior change at each visit. We performed intent-to-treat analyses using generalized estimating equations for the binary outcome. Results: Subjects randomized to PRE-RA were more likely to increase ladder scores over post-intervention assessments (relative risk 1.23, 95% confidence interval [95% CI] 1.01, 1.51) than those randomized to nonpersonalized education. At 6 months, 63.9% of PRE-RA subjects and 50.0% of comparison subjects increased motivation to improve behaviors (age-adjusted difference 15.8%; 95% CI 2.8%, 28.8%). Compared to nonpersonalized education, more PRE-RA subjects increased fish intake (45.0% versus 22.1%; P = 0.005), brushed more frequently (40.7% versus 22.9%; P = 0.01), flossed more frequently (55.7% versus 34.8%; P = 0.004), and quit smoking (62.5% versus 0.0% among 11 smokers; P = 0.18). Conclusion: Disclosure of RA risk personalized with genotype/biomarker results and behaviors increased motivation to improve RA risk–related behaviors. Personalized medicine approaches may motivate health behavior improvements for those at risk for RA and provide rationale for larger studies evaluating effects of behavior changes on clinical outcomes, such as RA-related autoantibody production or RA development.

Original language	English (US)
Pages (from-to)	823-833
Number of pages	11
Journal	Arthritis Care and Research
Volume	70
Issue number	6
DOIs	https://doi.org/10.1002/acr.23411
State	Published - Jun 2018

ASJC Scopus subject areas

Rheumatology

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10.1002/acr.23411

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Sparks, J. A., Iversen, M. D., Yu, Z., Triedman, N. A., Prado, M. G., Miller Kroouze, R., Kalia, S. S., Atkinson, M. L., Mody, E. A., Helfgott, S. M., Todd, D. J., Dellaripa, P. F., Bermas, B. L., Costenbader, K. H., Deane, K. D., Lu, B., Green, R. C., & Karlson, E. W. (2018). Disclosure of Personalized Rheumatoid Arthritis Risk Using Genetics, Biomarkers, and Lifestyle Factors to Motivate Health Behavior Improvements: A Randomized Controlled Trial. Arthritis Care and Research, 70(6), 823-833. https://doi.org/10.1002/acr.23411

Disclosure of Personalized Rheumatoid Arthritis Risk Using Genetics, Biomarkers, and Lifestyle Factors to Motivate Health Behavior Improvements : A Randomized Controlled Trial. / Sparks, Jeffrey A.; Iversen, Maura D.; Yu, Zhi et al.

In: Arthritis Care and Research, Vol. 70, No. 6, 06.2018, p. 823-833.

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

Sparks, JA, Iversen, MD, Yu, Z, Triedman, NA, Prado, MG, Miller Kroouze, R, Kalia, SS, Atkinson, ML, Mody, EA, Helfgott, SM, Todd, DJ, Dellaripa, PF, Bermas, BL, Costenbader, KH, Deane, KD, Lu, B, Green, RC & Karlson, EW 2018, 'Disclosure of Personalized Rheumatoid Arthritis Risk Using Genetics, Biomarkers, and Lifestyle Factors to Motivate Health Behavior Improvements: A Randomized Controlled Trial', Arthritis Care and Research, vol. 70, no. 6, pp. 823-833. https://doi.org/10.1002/acr.23411

@article{a8333179f8df4c809cb428981606c4ce,

title = "Disclosure of Personalized Rheumatoid Arthritis Risk Using Genetics, Biomarkers, and Lifestyle Factors to Motivate Health Behavior Improvements: A Randomized Controlled Trial",

abstract = "Objective: To determine the effect of disclosure of rheumatoid arthritis (RA) risk personalized with genetics, biomarkers, and lifestyle factors on health behavior intentions. Methods: We performed a randomized controlled trial among first-degree relatives without RA. Subjects assigned to the Personalized Risk Estimator for Rheumatoid Arthritis (PRE-RA) group received the web-based PRE-RA tool for RA risk factor education and disclosure of personalized RA risk estimates, including genotype/autoantibody results and behaviors (n = 158). Subjects assigned to the comparison arm received standard RA education (n = 80). The primary outcome was readiness for change based on the trans-theoretical model, using validated contemplation ladder scales. Increased motivation to improve RA risk–related behaviors (smoking, diet, exercise, or dental hygiene) was defined as an increase in any ladder score compared to baseline, assessed immediately, 6 weeks, and 6 months post-intervention. Subjects reported behavior change at each visit. We performed intent-to-treat analyses using generalized estimating equations for the binary outcome. Results: Subjects randomized to PRE-RA were more likely to increase ladder scores over post-intervention assessments (relative risk 1.23, 95% confidence interval [95% CI] 1.01, 1.51) than those randomized to nonpersonalized education. At 6 months, 63.9% of PRE-RA subjects and 50.0% of comparison subjects increased motivation to improve behaviors (age-adjusted difference 15.8%; 95% CI 2.8%, 28.8%). Compared to nonpersonalized education, more PRE-RA subjects increased fish intake (45.0% versus 22.1%; P = 0.005), brushed more frequently (40.7% versus 22.9%; P = 0.01), flossed more frequently (55.7% versus 34.8%; P = 0.004), and quit smoking (62.5% versus 0.0% among 11 smokers; P = 0.18). Conclusion: Disclosure of RA risk personalized with genotype/biomarker results and behaviors increased motivation to improve RA risk–related behaviors. Personalized medicine approaches may motivate health behavior improvements for those at risk for RA and provide rationale for larger studies evaluating effects of behavior changes on clinical outcomes, such as RA-related autoantibody production or RA development.",

author = "Sparks, {Jeffrey A.} and Iversen, {Maura D.} and Zhi Yu and Triedman, {Nellie A.} and Prado, {Maria G.} and {Miller Kroouze}, Rachel and Kalia, {Sarah S.} and Atkinson, {Michael L.} and Mody, {Elinor A.} and Helfgott, {Simon M.} and Todd, {Derrick J.} and Dellaripa, {Paul F.} and Bermas, {Bonnie L.} and Costenbader, {Karen H.} and Deane, {Kevin D.} and Bing Lu and Green, {Robert C.} and Karlson, {Elizabeth W.}",

note = "Funding Information: (grant R01-AR-059086). Dr. Costenbader{\textquoteright}s work was supported by the NIAMS (grants R01-AR-049880, K24-AR-066109, and R01-AR-059086). Dr. Deane{\textquoteright}s work was supported by the NIAMS (grant UM1-AI-110503). Dr. Green{\textquoteright}s work was supported by the NIH (grants U01-HG-006500, U19-HD-077671, R01-HG-005092, U01-HG008685, and U41-HG006834). Dr. Karlson{\textquoteright}s work was supported by the NIAMS (grants K24-AR-052403, R01-AR-049880, P30-AR-070253, and P30-AR-069625). Funding Information: Supported by the National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS; grant P60-AR-047782). Dr. Sparks{\textquoteright}s work was supported by the NIAMS (grants K23-AR-069688 and L30-AR-066953) and a Rheumatology Research Foundation Scientist Development Award. Dr. Iversen{\textquoteright}s work was supported by the NIAMS Funding Information: The authors thank Graham Colditz, MD, DrPH, and Hank Dart, MSc, for their assistance in creating the web-based PRE-RA tool, based on Your Disease Risk (http://www.yourdiseaserisk.wustl.edu/). They also thank Michelle L. Frits, BA, Christine K. Iannaccone, MPH, Taysir G. Mahmoud, BA, J. Adebukola Awosogba, MA, Jessica Brandano, BA, Jonathan C. Karlson, David J. Kreps, MS, and the Massachusetts Chapter of the Arthritis Foundation for assistance in recruitment and data collection. Finally, the authors thank the patients, families, staff, and physicians at the Brigham Orthopaedic and Arthritis Center at Brigham and Women's Hospital, the Arthritis and Orthopaedic Center at Brigham and Women's Faulkner Hospital, the 850 Boylston Arthritis Center, the Fish Center at 850 Boylston, and the Brigham and Women's Hospital Arthritis Center at Braintree. Publisher Copyright: {\textcopyright} 2017, American College of Rheumatology",

year = "2018",

month = jun,

doi = "10.1002/acr.23411",

language = "English (US)",

volume = "70",

pages = "823--833",

journal = "Arthritis Care and Research",

issn = "2151-464X",

number = "6",

}

TY - JOUR

T1 - Disclosure of Personalized Rheumatoid Arthritis Risk Using Genetics, Biomarkers, and Lifestyle Factors to Motivate Health Behavior Improvements

T2 - A Randomized Controlled Trial

AU - Sparks, Jeffrey A.

AU - Iversen, Maura D.

AU - Yu, Zhi

AU - Triedman, Nellie A.

AU - Prado, Maria G.

AU - Miller Kroouze, Rachel

AU - Kalia, Sarah S.

AU - Atkinson, Michael L.

AU - Mody, Elinor A.

AU - Helfgott, Simon M.

AU - Todd, Derrick J.

AU - Dellaripa, Paul F.

AU - Bermas, Bonnie L.

AU - Costenbader, Karen H.

AU - Deane, Kevin D.

AU - Lu, Bing

AU - Green, Robert C.

AU - Karlson, Elizabeth W.

N1 - Funding Information: (grant R01-AR-059086). Dr. Costenbader’s work was supported by the NIAMS (grants R01-AR-049880, K24-AR-066109, and R01-AR-059086). Dr. Deane’s work was supported by the NIAMS (grant UM1-AI-110503). Dr. Green’s work was supported by the NIH (grants U01-HG-006500, U19-HD-077671, R01-HG-005092, U01-HG008685, and U41-HG006834). Dr. Karlson’s work was supported by the NIAMS (grants K24-AR-052403, R01-AR-049880, P30-AR-070253, and P30-AR-069625). Funding Information: Supported by the National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS; grant P60-AR-047782). Dr. Sparks’s work was supported by the NIAMS (grants K23-AR-069688 and L30-AR-066953) and a Rheumatology Research Foundation Scientist Development Award. Dr. Iversen’s work was supported by the NIAMS Funding Information: The authors thank Graham Colditz, MD, DrPH, and Hank Dart, MSc, for their assistance in creating the web-based PRE-RA tool, based on Your Disease Risk (http://www.yourdiseaserisk.wustl.edu/). They also thank Michelle L. Frits, BA, Christine K. Iannaccone, MPH, Taysir G. Mahmoud, BA, J. Adebukola Awosogba, MA, Jessica Brandano, BA, Jonathan C. Karlson, David J. Kreps, MS, and the Massachusetts Chapter of the Arthritis Foundation for assistance in recruitment and data collection. Finally, the authors thank the patients, families, staff, and physicians at the Brigham Orthopaedic and Arthritis Center at Brigham and Women's Hospital, the Arthritis and Orthopaedic Center at Brigham and Women's Faulkner Hospital, the 850 Boylston Arthritis Center, the Fish Center at 850 Boylston, and the Brigham and Women's Hospital Arthritis Center at Braintree. Publisher Copyright: © 2017, American College of Rheumatology

PY - 2018/6

Y1 - 2018/6

N2 - Objective: To determine the effect of disclosure of rheumatoid arthritis (RA) risk personalized with genetics, biomarkers, and lifestyle factors on health behavior intentions. Methods: We performed a randomized controlled trial among first-degree relatives without RA. Subjects assigned to the Personalized Risk Estimator for Rheumatoid Arthritis (PRE-RA) group received the web-based PRE-RA tool for RA risk factor education and disclosure of personalized RA risk estimates, including genotype/autoantibody results and behaviors (n = 158). Subjects assigned to the comparison arm received standard RA education (n = 80). The primary outcome was readiness for change based on the trans-theoretical model, using validated contemplation ladder scales. Increased motivation to improve RA risk–related behaviors (smoking, diet, exercise, or dental hygiene) was defined as an increase in any ladder score compared to baseline, assessed immediately, 6 weeks, and 6 months post-intervention. Subjects reported behavior change at each visit. We performed intent-to-treat analyses using generalized estimating equations for the binary outcome. Results: Subjects randomized to PRE-RA were more likely to increase ladder scores over post-intervention assessments (relative risk 1.23, 95% confidence interval [95% CI] 1.01, 1.51) than those randomized to nonpersonalized education. At 6 months, 63.9% of PRE-RA subjects and 50.0% of comparison subjects increased motivation to improve behaviors (age-adjusted difference 15.8%; 95% CI 2.8%, 28.8%). Compared to nonpersonalized education, more PRE-RA subjects increased fish intake (45.0% versus 22.1%; P = 0.005), brushed more frequently (40.7% versus 22.9%; P = 0.01), flossed more frequently (55.7% versus 34.8%; P = 0.004), and quit smoking (62.5% versus 0.0% among 11 smokers; P = 0.18). Conclusion: Disclosure of RA risk personalized with genotype/biomarker results and behaviors increased motivation to improve RA risk–related behaviors. Personalized medicine approaches may motivate health behavior improvements for those at risk for RA and provide rationale for larger studies evaluating effects of behavior changes on clinical outcomes, such as RA-related autoantibody production or RA development.

AB - Objective: To determine the effect of disclosure of rheumatoid arthritis (RA) risk personalized with genetics, biomarkers, and lifestyle factors on health behavior intentions. Methods: We performed a randomized controlled trial among first-degree relatives without RA. Subjects assigned to the Personalized Risk Estimator for Rheumatoid Arthritis (PRE-RA) group received the web-based PRE-RA tool for RA risk factor education and disclosure of personalized RA risk estimates, including genotype/autoantibody results and behaviors (n = 158). Subjects assigned to the comparison arm received standard RA education (n = 80). The primary outcome was readiness for change based on the trans-theoretical model, using validated contemplation ladder scales. Increased motivation to improve RA risk–related behaviors (smoking, diet, exercise, or dental hygiene) was defined as an increase in any ladder score compared to baseline, assessed immediately, 6 weeks, and 6 months post-intervention. Subjects reported behavior change at each visit. We performed intent-to-treat analyses using generalized estimating equations for the binary outcome. Results: Subjects randomized to PRE-RA were more likely to increase ladder scores over post-intervention assessments (relative risk 1.23, 95% confidence interval [95% CI] 1.01, 1.51) than those randomized to nonpersonalized education. At 6 months, 63.9% of PRE-RA subjects and 50.0% of comparison subjects increased motivation to improve behaviors (age-adjusted difference 15.8%; 95% CI 2.8%, 28.8%). Compared to nonpersonalized education, more PRE-RA subjects increased fish intake (45.0% versus 22.1%; P = 0.005), brushed more frequently (40.7% versus 22.9%; P = 0.01), flossed more frequently (55.7% versus 34.8%; P = 0.004), and quit smoking (62.5% versus 0.0% among 11 smokers; P = 0.18). Conclusion: Disclosure of RA risk personalized with genotype/biomarker results and behaviors increased motivation to improve RA risk–related behaviors. Personalized medicine approaches may motivate health behavior improvements for those at risk for RA and provide rationale for larger studies evaluating effects of behavior changes on clinical outcomes, such as RA-related autoantibody production or RA development.

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DO - 10.1002/acr.23411

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IS - 6

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Disclosure of Personalized Rheumatoid Arthritis Risk Using Genetics, Biomarkers, and Lifestyle Factors to Motivate Health Behavior Improvements: A Randomized Controlled Trial

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