Improved Disease Course Associated With Early Initiation of Biologics in Polyarticular Juvenile Idiopathic Arthritis: Trajectory Analysis of a Childhood Arthritis and Rheumatology Research Alliance Consensus Treatment Plans Study

Mei Sing Ong; Sarah Ringold; Yukiko Kimura; Laura E Schanberg; George A Tomlinson; Marc D Natter; CARRA Registry Investigators

doi:10.1002/art.41892

Improved Disease Course Associated With Early Initiation of Biologics in Polyarticular Juvenile Idiopathic Arthritis: Trajectory Analysis of a Childhood Arthritis and Rheumatology Research Alliance Consensus Treatment Plans Study

Arthritis Rheumatol. 2021 Oct;73(10):1910-1920. doi: 10.1002/art.41892. Epub 2021 Aug 27.

Authors

Mei Sing Ong¹, Sarah Ringold², Yukiko Kimura³, Laura E Schanberg⁴, George A Tomlinson⁵, Marc D Natter⁶; CARRA Registry Investigators

Collaborators

CARRA Registry Investigators:
N Abel, K Abulaban, A Adams, M Adams, R Agbayani, J Aiello, S Akoghlanian, C Alejandro, E Allenspach, R Alperin, M Alpizar, G Amarilyo, W Ambler, E Anderson, S Ardoin, S Armendariz, E Baker, I Balboni, S Balevic, L Ballenger, S Ballinger, N Balmuri, F Barbar-Smiley, L Barillas-Arias, M Basiaga, K Baszis, M Becker, H Bell-Brunson, E Beltz, H Benham, S Benseler, W Bernal, T Beukelman, T Bigley, B Binstadt, C Black, M Blakley, J Bohnsack, J Boland, A Boneparth, S Bowman, C Bracaglia, E Brooks, M Brothers, A Brown, H Brunner, M Buckley, M Buckley, H Bukulmez, D Bullock, B Cameron, S Canna, L Cannon, P Carper, V Cartwright, E Cassidy, L Cerracchio, E Chalom, J Chang, A Chang-Hoftman, V Chauhan, P Chira, T Chinn, K Chundru, H Clairman, D Co, A Confair, H Conlon, R Connor, A Cooper, J Cooper, S Cooper, C Correll, R Corvalan, D Costanzo, R Cron, L Curiel-Duran, T Curington, M Curry, A Dalrymple, A Davis, C Davis, C Davis, T Davis, F De Benedetti, D De Ranieri, J Dean, F Dedeoglu, M DeGuzman, N Delnay, V Dempsey, E DeSantis, T Dickson, J Dingle, B Donaldson, E Dorsey, S Dover, J Dowling, J Drew, K Driest, Q Du, K Duarte, D Durkee, E Duverger, J Dvergsten, A Eberhard, M Eckert, K Ede, B Edelheit, C Edens, C Edens, Y Edgerly, M Elder, B Ervin, S Fadrhonc, C Failing, D Fair, M Falcon, L Favier, S Federici, B Feldman, J Fennell, I Ferguson, P Ferguson, B Ferreira, R Ferrucho, K Fields, T Finkel, M Fitzgerald, C Fleming, O Flynn, L Fogel, E Fox, M Fox, L Franco, M Freeman, K Fritz, S Froese, R Fuhlbrigge, J Fuller, N George, K Gerhold, D Gerstbacher, M Gilbert, M Gillispie-Taylor, E Giverc, C Godiwala, I Goh, H Goheer, D Goldsmith, E Gotschlich, A Gotte, B Gottlieb, C Gracia, T Graham, S Grevich, T Griffin, J Griswold, A Grom, M Guevara, P Guittar, M Guzman, M Hager, T Hahn, O Halyabar, E Hammelev, M Hance, A Hanson, L Harel, S Haro, J Harris, O Harry, E Hartigan, J Hausmann, A Hay, K Hayward, J Heiart, K Hekl, L Henderson, M Henrickson, A Hersh, K Hickey, P Hill, S Hillyer, L Hiraki, M Hiskey, P Hobday, C Hoffart, M Holland, M Hollander, S Hong, M Horwitz, J Hsu, A Huber, J Huggins, J Hui-Yuen, C Hung, J Huntington, A Huttenlocher, M Ibarra, L Imundo, C Inman, A Insalaco, A Jackson, S Jackson, K James, G Janow, J Jaquith, S Jared, N Johnson, J Jones, J Jones, J Jones, K Jones, S Jones, S Joshi, L Jung, C Justice, A Justiniano, N Karan, K Kaufman, A Kemp, E Kessler, U Khalsa, B Kienzle, S Kim, Y Kimura, D Kingsbury, M Kitcharoensakkul, T Klausmeier, K Klein, M Klein-Gitelman, B Kompelien, A Kosikowski, L Kovalick, J Kracker, S Kramer, C Kremer, J Lai, J Lam, B Lang, S Lapidus, B Lapin, A Lasky, D Latham, E Lawson, R Laxer, P Lee, P Lee, T Lee, L Lentini, M Lerman, D Levy, S Li, S Lieberman, L Lim, C Lin, N Ling, M Lingis, M Lo, D Lovell, D Lowman, N Luca, S Lvovich, C Madison, J Madison, S Magni Manzoni, B Malla, J Maller, M Malloy, M Mannion, C Manos, L Marques, A Martyniuk, T Mason, S Mathus, L McAllister, K McCarthy, K McConnell, E McCormick, D McCurdy, P McCurdy Stokes, S McGuire, I McHale, A McMonagle, C McMullen-Jackson, E Meidan, E Mellins, E Mendoza, R Mercado, A Merritt, L Michalowski, P Miettunen, M Miller, D Milojevic, E Mirizio, E Misajon, M Mitchell, R Modica, S Mohan, K Moore, L Moorthy, S Morgan, E Morgan Dewitt, C Moss, T Moussa, V Mruk, A Murphy, E Muscal, R Nadler, B Nahal, K Nanda, N Nasah, L Nassi, S Nativ, M Natter, J Neely, B Nelson, L Newhall, L Ng, J Nicholas, R Nicolai, P Nigrovic, J Nocton, B Nolan, E Oberle, B Obispo, B O'Brien, T O'Brien, O Okeke, M Oliver, J Olson, K O'Neil, K Onel, A Orandi, M Orlando, S Osei-Onomah, R Oz, E Pagano, A Paller, N Pan, S Panupattanapong, M Pardeo, J Paredes, A Parsons, J Patel, K Pentakota, P Pepmueller, T Pfeiffer, K Phillippi, D Pires Marafon, K Phillippi, L Ponder, R Pooni, S Prahalad, S Pratt, S Protopapas, B Puplava, J Quach, M Quinlan-Waters, C Rabinovich, S Radhakrishna, J Rafko, J Raisian, A Rakestraw, C Ramirez, E Ramsay, S Ramsey, R Randell, A Reed, A Reed, A Reed, H Reid, K Remmel, A Repp, A Reyes, A Richmond, M Riebschleger, S Ringold, M Riordan, M Riskalla, M Ritter, R Rivas-Chacon, A Robinson, E Rodela, M Rodriquez, K Rojas, T Ronis, M Rosenkranz, B Rosolowski, H Rothermel, D Rothman, E Roth-Wojcicki, K Rouster-Stevens, T Rubinstein, N Ruth, N Saad, S Sabbagh, E Sacco, R Sadun, C Sandborg, A Sanni, L Santiago, A Sarkissian, S Savani, L Scalzi, L Schanberg, S Scharnhorst, K Schikler, A Schlefman, H Schmeling, K Schmidt, E Schmitt, R Schneider, K Schollaert-Fitch, G Schulert, T Seay, C Seper, J Shalen, R Sheets, A Shelly, S Shenoi, K Shergill, J Shirley, M Shishov, C Shivers, E Silverman, N Singer, V Sivaraman, J Sletten, A Smith, C Smith, J Smith, J Smith, E Smitherman, J Soep, M Son, S Spence, L Spiegel, J Spitznagle, R Sran, H Srinivasalu, H Stapp, K Steigerwald, Y Sterba Rakovchik, S Stern, A Stevens, B Stevens, R Stevenson, K Stewart, C Stingl, J Stokes, M Stoll, E Stringer, S Sule, J Sumner, R Sundel, M Sutter, R Syed, G Syverson, A Szymanski, S Taber, R Tal, A Tambralli, A Taneja, T Tanner, S Tapani, G Tarshish, S Tarvin, L Tate, A Taxter, J Taylor, M Terry, M Tesher, A Thatayatikom, B Thomas, K Tiffany, T Ting, A Tipp, D Toib, K Torok, C Toruner, H Tory, M Toth, S Tse, V Tubwell, M Twilt, S Uriguen, T Valcarcel, H Van Mater, L Vannoy, C Varghese, N Vasquez, K Vazzana, R Vehe, K Veiga, J Velez, J Verbsky, G Vilar, N Volpe, S Vora, J Wagner, L Wagner-Weiner, D Wahezi, H Waite, J Walker, H Walters, T Wampler Muskardin, L Waqar, M Waterfield, M Watson, A Watts, P Weiser, J Weiss, P Weiss, E Wershba, A White, C Williams, A Wise, J Woo, L Woolnough, T Wright, E Wu, A Yalcindag, M Yee, E Yen, R Yeung, K Yomogida, Q Yu, R Zapata, A Zartoshti, A Zeft, R Zeft, Y Zhang, Y Zhao, A Zhu, C Zic

Affiliations

¹ Harvard Medical School and Harvard Pilgrim Health Care Institute, Boston, Massachusetts.
² Seattle Children's Hospital, Seattle, Washington.
³ Joseph M. Sanzari Children's Hospital and Hackensack Meridian School of Medicine, Hackensack, New Jersey.
⁴ Duke University Medical Center, Durham, North Carolina.
⁵ University of Toronto, Toronto, Ontario, Canada.
⁶ Boston Children's Hospital, Massachusetts General Hospital, and Harvard Medical School, Boston, Massachusetts.

PMID: 34105303
DOI: 10.1002/art.41892

Abstract

Objective: To investigate the effects of early introduction of biologic disease-modifying antirheumatic drugs (bDMARDs) on the disease course in untreated polyarticular juvenile idiopathic arthritis (JIA).

Methods: We analyzed data on patients with polyarticular JIA participating in the Start Time Optimization of Biologics in Polyarticular JIA (STOP-JIA) study (n = 400) and a comparator cohort (n = 248) from the Childhood Arthritis and Rheumatology Research Alliance Registry. Latent class trajectory modeling (LCTM) was applied to identify subgroups of patients with distinct disease courses based on disease activity (clinical Juvenile Arthritis Disease Activity Score in 10 joints) over 12 months from baseline.

Results: In the STOP-JIA study, 198 subjects (49.5%) received bDMARDs within 3 months of baseline assessment. LCTM analyses generated 3 latent classes representing 3 distinct disease trajectories, characterized by slow, moderate, or rapid disease activity improvement over time. Subjects in the rapid improvement trajectory attained inactive disease within 6 months from baseline. Odds of being in the rapid improvement trajectory versus the slow improvement trajectory were 3.6 times as high (95% confidence interval 1.32-10.0; P = 0.013) for those treated with bDMARDs ≤3 months from baseline compared with subjects who started bDMARDs >3 months after baseline, after adjusting for demographic characteristics, clinical attributes, and baseline disease activity. Shorter disease duration at first rheumatology visit approached statistical significance as a predictor of favorable trajectory without bDMARD treatment.

Conclusion: Starting bDMARDs within 3 months of baseline assessment is associated with more rapid achievement of inactive disease in subjects with untreated polyarticular JIA. These results demonstrate the utility of trajectory analysis of disease course as a method for determining treatment efficacy.

Trial registration: ClinicalTrials.gov NCT02593006.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Antirheumatic Agents / therapeutic use*
Arthritis, Juvenile / drug therapy*
Biological Products / therapeutic use*
Child
Consensus
Disease Progression
Female
Humans
Male
Treatment Outcome

Substances

Antirheumatic Agents
Biological Products

Associated data

ClinicalTrials.gov/NCT02593006

Grants and funding

CER-1408-20534/Patient-Centered Outcomes Research Institute® (PCORI®) Award