Efficacy and Safety of Dapagliflozin in Patients With Inadequately Controlled Type 1 Diabetes (the DEPICT-2 Study): 24-Week Results From a Randomized Controlled Trial

Chantal Mathieu(KU Leuven), Paresh Dandona(University at Buffalo, State University of New York), Pieter Gillard(KU Leuven), Peter Senior(University of Alberta), Christoph Hasslacher(Diabetesinstitut Heidelberg), Eiichi Araki(Kumamoto University), Marcus Lind(NU Hospital Group), Stephen C. Bain(Swansea University), Serge Jabbour(Thomas Jefferson University), Niki Arya(AstraZeneca (Japan)), Lars Hansen, Fredrik Thorén(AstraZeneca (Sweden)), Anna Maria Langkilde(AstraZeneca (Sweden)), DEPICT-2 Investigators, Cecilia Luquez, Federico Pérez Manghi, María Rosa Ulla, Maria Alejandra Moisello, Virginia Visco, Silvia Gorban De Lapertoza, Silvana Ernestina Solís, Javier Farias, Georgina Sposetti(KU Leuven), Pieter Gillard(KU Leuven), Pascale Abrams, M. van Ypersele de Strihou, James R. W. Conway, Sue D. Pedersen(University of Alberta), Peter Senior(University of Alberta), Joanne Liutkus, Churn-Ern Yip, Zubin Punthakee, Frédéric Bernier, Heather Lochnan, Vincent Woo, Thomas G. Elliott, Juan Palma, C Merino, Alfredo Danin Vargas, Ulrich Wendisch, Andreas Reichel, Jochen Seufert, Bernd Becker, Hasan Alawi, Andreas L. Birkenfeld(Diabetesinstitut Heidelberg), Christoph Hasslacher(Diabetesinstitut Heidelberg), Joerg Luedemann, Thomas Schaum, Cornelia Marck, Joachim Sauter, Ulrich Aigner, Yukiko Onishi, Hiroaki Seino, Yuichi Sato, Kiyohide Nunoi, Akira Yamauchi, Eitaro Nakashima, Hiroki Ikeda, Toshihiko Shiraiwa, Yoshimitsu Yamasaki, Hiroki Yokoyama, Kunihiko Nakamura, Masayuki Noritake, Shozo Miyauchi, Tomomi Hakoda, Yoshihide Hirohata, Atsushi Hasegawa, Yoshihide Fukumoto, Hirotaka Nagashima, Masahiro Takihata, Tetsuro Kamada, Hideaki Jinnouchi, Yuri Ono, Takayuki Watanabe, Hiroshi Ohashi, Masahiko Takai, T Seguchi, Katsuya Yamazaki, Hajime Maeda, Shingo Iwasaki, Harold W. de Valk, Adriaan Kooy, S.A.N.T. Landewé-Cleuren, Katarzyna Madziarska, Andrzej Stankiewicz, Katarzyna Wasilewska, Gottfried Rudofsky, Maciej T. Małecki, Ewa Pańkowska, Ewa Szyprowska, Monika Łukaszewicz, Lidia Tokarska, Ирина Аркадьевна Бондарь, I. V. Karpova, Ludmila Ruyatkina, Alsu Gafurovna Zalevskaya, Ruslan Sardinov, Yury Khalimov, Folke Sjöberg, Pekka Koskinen(University at Buffalo, State University of New York), Dan Curiac(NU Hospital Group), Marcus Lind(NU Hospital Group), Birgit Bach-Kliegel, Bernd Schultes, Basil Issa, Anne Kilvert, Olívia R. Pereira(Swansea University), Stephen C. Bain(Swansea University), Biswa Ranjan Mishra, Deepak Bhatnagar, Leonard Chuck, David M. Gorson, David Robertson, Luis Casaubon, Louis Chaykin, Juan P. Frías, Stanley H. Hsia, Robert A. Jenders, Sam Lerman, Scott A. Segel(University of Alberta), Peter N. Weissman(AstraZeneca (Sweden)), Anna Chang, John H. Reed, Ivy-Joan Madu(University of Alberta), Peter Bressler, Lisa Abbott, Sumana Gangi, Kate Wheeler, Kenneth J. Cohen, William Biggs(Thomas Jefferson University), Serge Jabbour(Thomas Jefferson University), Dennis G. Karounos, Sajeev Menon, Wendell Miers, Grazia Aleppo, Gigi Lefebvre, Danny Sugimoto, R Ferraro, Richard Kelly, Marcel Twahirwa, Christopher Case, David C. Klonoff, Paul S. Denker, Priscilla Hollander, Michelle Welch, Matthew C. Leinung, Larry Kotek, Janet B. McGill, Yshay Shlesinger, Cynthia Huffman(Swansea University), Stephen Aronoff, Daniel Lorber, Antonio Terrelonge, Firas Akhrass, Cindy Bredefeld, Kenneth S. Hershon, James M. Lenhard, Daniel Donovan, Larry D. Stonesifer, Craig Greenberg, Eli Ipp, Anuj Bhargava, Shichun Bao
Diabetes Care
July 19, 2018
10.2337/dc18-0623
Cited by 251

Abstract

OBJECTIVE This 24-week, double-blinded, phase 3 clinical trial (DEPICT-2; ClinicalTrials.gov, NCT02460978) evaluated efficacy and safety of dapagliflozin as adjunct therapy to adjustable insulin in patients with inadequately controlled type 1 diabetes (HbA1c 7.5–10.5%). RESEARCH DESIGN AND METHODS Patients were randomized 1:1:1 to dapagliflozin 5 mg (n = 271), dapagliflozin 10 mg (n = 270), or placebo (n = 272) plus insulin. Insulin dose was adjusted by investigators according to self-monitored glucose readings, local guidance, and individual circumstances. RESULTS Baseline characteristics were balanced between treatment groups. At week 24, dapagliflozin significantly decreased HbA1c (primary outcome; difference vs. placebo: dapagliflozin 5 mg −0.37% [95% CI −0.49, −0.26], dapagliflozin 10 mg –0.42% [−0.53, −0.30]), total daily insulin dose (−10.78% [−13.73, −7.72] and −11.08% [−14.04, −8.02], respectively), and body weight (−3.21% [−3.96, −2.45] and −3.74% [−4.49, −2.99], respectively) (P < 0.0001 for all). Mean interstitial glucose, amplitude of glucose excursion, and percent of readings within target glycemic range (>70 to ≤180 mg/dL) versus placebo were significantly improved. More patients receiving dapagliflozin achieved a reduction in HbA1c ≥0.5% without severe hypoglycemia compared with placebo. Adverse events were reported for 72.7%, 67.0%, and 63.2% of patients receiving dapagliflozin 5 mg, dapagliflozin 10 mg, and placebo, respectively. Hypoglycemia, including severe hypoglycemia, was balanced between groups. There were more adjudicated definite diabetic ketoacidosis (DKA) events with dapagliflozin: 2.6%, 2.2%, and 0% for dapagliflozin 5 mg, dapagliflozin 10 mg, and placebo, respectively. CONCLUSIONS Dapagliflozin as adjunct therapy to adjustable insulin in patients with type 1 diabetes was well tolerated and improved glycemic control with no increase in hypoglycemia versus placebo but with more DKA events.

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