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Improving treatment decisions using personalized risk assessment from the International IgA Nephropathy Prediction Tool

免疫抑制 医学 蛋白尿 肾病 内科学 重症监护医学 糖尿病 内分泌学
作者
Sean J. Barbour,Mark Canney,Rosanna Coppo,Hong Zhang,Zhihong Liu,Yusuke Suzuki,Keiichi Matsuzaki,Ritsuko Katafuchi,Dilshani Induruwage,Lee Er,Heather N. Reich,John Feehally,Jonathan Barratt,Daniel C. Cattran,María Luisa Russo,Stéphan Troyanov,H. Terence Cook,Ian S. Roberts,Vladimı́r Tesař,Dita Maixnerová,Sigrid Lundberg,Loreto Gesualdo,Francesco Emma,Laura Fuiano,Giulietta Beltrame,Cristiana Rollino,Alfonso Amore,Roberta Camilla,Licia Peruzzi,Manuel Praga,Sandro Feriozzi,Rosaria Polci,Giuseppe Segoloni,Loredana Colla,Antonello Pani,Doloretta Piras,Andrea Angioi,Giovanni Cancarini,Sara Ravera,M. Durlik,Elisabetta Moggia,J. Ballarín,Salvatore Di Giulio,F. Pugliese,Ilaria Serriello,Yaşar Çalışkan,Mehmet Şükrü Sever,İşın Kiliçaslan,Francesco Locatelli,Lucia Del Vecchio,Jack F.M. Wetzels,Hilde P.E. Peters,Ulla Berg,Fernanda Carvalho,Alves Ferreira,Milena Maggio,Andrzej Wieçek,Mai Ots-Rosenberg,Riccardo Magistroni,Rezan Topaloğlu,Yelda Bilginer,Marco D’Amico,Μaria Stangou,F Giacchino,Dimitris Goumenos,Pantelitsa Kalliakmani,Miltiadis Gerolymos,Kres̆imir Gales̃ić,Colin C. Geddes,Kostas C. Siamopoulos,Olga Balafa,Marco Galliani,Piero Stratta,Marco Quaglia,R Bergia,Raffaella Cravero,Maurizio Salvadori,Lino Cirami,Bengt Fellström,Hilde Kloster Smerud,Franco Ferrario,Tiziana Stellato,Jesús Egido,Carina Aguilar Martín,Jürgen Floege,Frank Eitner,Antonio Lupo,Patrizia Bernich,Paolo Menè,Massimo Morosetti,Cees van Kooten,Ton J. Rabelink,Marlies E.J. Reinders,J.M. Grinyó,Stefano Cusinato,Luisa Benozzi,Silvana Savoldi,C. Licata,Małgorzata Mizerska-Wasiak,G Martina,Alessandra Messuerotti,Antonio Dal Canton,Ciro Esposito,C. Migotto,G Triolo,Filippo Mariano,Claudio Pozzi,R Boero,Shubha S. Bellur,Gianna Mazzucco,C. Giannakakis,E Honsová,Bo Sundelin,Anna Maria Di Palma,Eduardo Gutiérrez,A.M. Asunis,Regina Tardanico,Agnieszka Perkowska‐Ptasińska,J. Arce Terroba,M. Fortunato,Afroditi Pantzaki,Yasemin Özlük,Eric J. Steenbergen,Magnus Söderberg,Živile Riispere,Luciana Furci,Dıclehan Orhan,David Kipgen,Donatella Casartelli,Danica Galešić Ljubanović,Hariklia Gakiopoulou,E. Bertoni,Pablo Cannata Ortiz,Henryk Karkoszka,Hermann Josef Groene,Antonella Stoppacciaro,Ingeborg M. Bajema,Jan A. Bruijn,Xavier Fulladosa,Jadwiga Małdyk,Elli Ioachim,Nüket Bavbek,Terry Cook,Charles E. Alpers,F Berthoux,Stephen M. Bonsib,Vivette D. D’Agati,Giuseppe D’Amico,Steven N. Emancipator,F. Emmal,Fernando C. Fervenza,Sandrine Florquin,Agnes B. Fogo,Hermann Josef Groene,Mark Haas,Prue Hill,Ronald J. Hogg,Stephen I‐Hong Hsu,Tracy E. Hunley,Michelle A. Hladunewich,Caroline E. Jennette,Kensuke Joh,Bruce A. Julian,Tetsuya Kawamura,Fernand Mac‐Moune Lai,Chi Bon Leung,L. Li,P. Li,Z. Liu,Alfonso Eirin Massat,Bruce Mackinnon,Sergio Mezzano,Francesco Paolo Schena,Yasuhiko Tomino,Patrick D. Walker,H. Wang,Jj Weening,Caihong Zeng,Sufang Shi,Chieko Nogi,Hodaka Suzuki,Kentaro Koike,Keita Hirano,Takashi Yokoo,Mayuko Hanai,Kei Fukami,K. Takahashi,Yukio Yuzawa,Misao Niwa,Yoshinari Yasuda,Shoichi Maruyama,Daisuke Ichikawa,Takahide Suzuki,Sayuri Shirai,Akira Fukuda,Shota Fujimoto,Hernán Trimarchi
出处
期刊:Kidney International [Elsevier]
卷期号:98 (4): 1009-1019 被引量:33
标识
DOI:10.1016/j.kint.2020.04.042
摘要

Immunosuppression in IgA nephropathy (IgAN) should be reserved for patients at high-risk of disease progression, which KDIGO guidelines determine based solely on proteinuria 1g or more/day. To investigate if treatment decisions can be more accurately accomplished using individualized risk from the International IgAN Prediction Tool, we simulated allocation of a hypothetical immunosuppression therapy in an international cohort of adults with IgAN. Two decision rules for treatment were applied based on proteinuria of 1g or more/day or predicted risk from the Prediction Tool above a threshold probability. An appropriate decision was defined as immunosuppression allocated to patients experiencing the primary outcome (50% decline in eGFR or ESKD) and withheld otherwise. The net benefit and net reduction in treatment are the proportion of patients appropriately allocated to receive or withhold immunosuppression, adjusted for the harm from inappropriate decisions, calculated for all threshold probabilities from 0-100%. Of 3299 patients followed for 5.1 years, 522 (15.8%) experienced the primary outcome. Treatment allocation based solely on proteinuria of 1g or more/day had a negative net benefit (was harmful) because immunosuppression was increasingly allocated to patients without progressive disease. Compared to using proteinuria, treatment allocation using the Prediction Tool had a larger net benefit up to 23.4% (95% confidence interval 21.5-25.2%) and a larger net reduction in treatment up to 35.1% (32.3-37.8%). Thus, allocation of immunosuppression to high-risk patients with IgAN can be substantially improved using the Prediction Tool compared to using proteinuria. Immunosuppression in IgA nephropathy (IgAN) should be reserved for patients at high-risk of disease progression, which KDIGO guidelines determine based solely on proteinuria 1g or more/day. To investigate if treatment decisions can be more accurately accomplished using individualized risk from the International IgAN Prediction Tool, we simulated allocation of a hypothetical immunosuppression therapy in an international cohort of adults with IgAN. Two decision rules for treatment were applied based on proteinuria of 1g or more/day or predicted risk from the Prediction Tool above a threshold probability. An appropriate decision was defined as immunosuppression allocated to patients experiencing the primary outcome (50% decline in eGFR or ESKD) and withheld otherwise. The net benefit and net reduction in treatment are the proportion of patients appropriately allocated to receive or withhold immunosuppression, adjusted for the harm from inappropriate decisions, calculated for all threshold probabilities from 0-100%. Of 3299 patients followed for 5.1 years, 522 (15.8%) experienced the primary outcome. Treatment allocation based solely on proteinuria of 1g or more/day had a negative net benefit (was harmful) because immunosuppression was increasingly allocated to patients without progressive disease. Compared to using proteinuria, treatment allocation using the Prediction Tool had a larger net benefit up to 23.4% (95% confidence interval 21.5-25.2%) and a larger net reduction in treatment up to 35.1% (32.3-37.8%). Thus, allocation of immunosuppression to high-risk patients with IgAN can be substantially improved using the Prediction Tool compared to using proteinuria. In This IssueKidney InternationalVol. 98Issue 4PreviewInfections are a common complication after solid organ transplantation. Fernández-Ruiz et al. developed an easily applied method for risk stratifying a patient’s likelihood of developing any infection and a bacterial infection between months 1 and 6 after receiving a kidney allograft. They derived the Seeking for Immune Status on Peripheral Blood Lymphocytes, Immunoglobulins and Complement Activity (SIMPLICITY) score in an initial cohort of patients at a single center and then validated SIMPLICITY in an independent, multicenter cohort of kidney recipients. Full-Text PDF
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