Glycemia Reduction in Type 2 Diabetes - Microvascular and Cardiovascular Outcomes

GRADE Study Research Group; David M Nathan; John M Lachin; Ionut Bebu; Henry B Burch; John B Buse; Andrea L Cherrington; Stephen P Fortmann; Jennifer B Green; Steven E Kahn; M Sue Kirkman; Heidi Krause-Steinrauf; Mary E Larkin; Lawrence S Phillips; Rodica Pop-Busui; Michael Steffes; Margaret Tiktin; Mark Tripputi; Deborah J Wexler; Naji Younes

doi:10.1056/NEJMoa2200436

Glycemia Reduction in Type 2 Diabetes - Microvascular and Cardiovascular Outcomes

N Engl J Med. 2022 Sep 22;387(12):1075-1088. doi: 10.1056/NEJMoa2200436.

Authors

GRADE Study Research Group; David M Nathan¹, John M Lachin¹, Ionut Bebu¹, Henry B Burch¹, John B Buse¹, Andrea L Cherrington¹, Stephen P Fortmann¹, Jennifer B Green¹, Steven E Kahn¹, M Sue Kirkman¹, Heidi Krause-Steinrauf¹, Mary E Larkin¹, Lawrence S Phillips¹, Rodica Pop-Busui¹, Michael Steffes¹, Margaret Tiktin¹, Mark Tripputi¹, Deborah J Wexler¹, Naji Younes¹

Collaborators

GRADE Study Research Group:
J P Crandall, M D McKee, S Behringer-Massera, J Brown-Friday, E Xhori, K Ballentine-Cargill, S Duran, H Estrella, S Gonzalez de la Torre, J Lukin, L S Phillips, E Burgess, D Olson, M Rhee, P Wilson, T S Raines, J Boers, J Costello, M Maher-Albertelli, R Mungara, L Savoye, C A White, C Gullett, L Holloway, F Morehead, S Person, M Sibymon, S Tanukonda, C Adams, A Ross, A Balasubramanyam, R Gaba, E Gonzalez Hattery, A Ideozu, J Jimenez, G Montes, C Wright, P Hollander, E Roe, A Jackson, A Smiley, P Burt, L Estrada, K Chionh, F Ismail-Beigi, C Falck-Ytter, L Sayyed Kassem, A Sood, M Tiktin, T Kulow, C Newman, K A Stancil, B Cramer, J Iacoboni, M V Kononets, C Sanders, L Tucker, A Werner, A Maxwell, G McPhee, C Patel, L Colosimo, A Krol, R Goland, J Pring, L Alfano, P Kringas, C Hausheer, J Tejada, K Gumpel, A Kirpitch, H Schneier, J B Green, H AbouAssi, R Chatterjee, M N Feinglos, J English Jones, S A Khan, J B Kimpel, R P Zimmer, M Furst, B M Satterwhite, C R Thacker, K Evans Kreider, C N Mariash, K J Mather, H M Ismail, A Lteif, M Mullen, T Hamilton, N Patel, G Riera, M Jackson, V Pirics, D Aguillar, D Howard, S Hurt, R Bergenstal, A Carlson, T Martens, M Johnson, R Hill, J Hyatt, C Jensen, M Madden, D Martin, H Willis, W Konerza, S Yang, K Kleeberger, R Passi, S Fortmann, M Herson, K Mularski, H Glauber, J Prihoda, B Ash, C Carlson, P A Ramey, E Schield, B Torgrimson-Ojerio, K Arnold, B Kauffman, E Panos, S Sahnow, K Bays, K Berame, J Cook, D Ghioni, J Gluth, K Schell, J Criscola, C Friason, S Jones, S Nazarov, J Barzilay, N Rassouli, R Puttnam, B Ojoawo, R Nelson, M Curtis, B Hollis, C Sanders-Jones, K Stokes, Z El-Haqq, A Kolli, T Tran, D Wexler, M E Larkin, J Meigs, B Chambers, A Dushkin, G Rocchio, M Yepes, B Steiner, H Dulin, M Cayford, K Chu, A DeManbey, M Hillard, K Martin, N Thangthaeng, L Gurry, R Kochis, E Raymond, V Ripley, C Stevens, J Park, V Aroda, A Ghazi, M Magee, A Ressing, A Loveland, M Hamm, M Hurtado, A Kuhn, J Leger, L Manandhar, F Mwicigi, O Sanchez, T Young, R Garg, V Lagari-Libhaber, H J Florez, W M Valencia, J Marks, S Casula, L Oropesa-Gonzalez, L Hue, A Cuadot, R Nieto-Martinez, A Riccio Veliz, M KGutt, Y J Kendal, B Veciana, A Ahmann, D Aby-Daniel, F Joarder, V Morimoto, C Sprague, D Yamashita, N Cady, N Rivera-Eschright, P Kirchhoff, B Morales Gomez, A Goncharova, S H Hox, H Petrovitch, M Matwichyna, V Jenkins, L Broadwater, R R Ishii, N O Bermudez, D S Hsia, W T Cefalu, F L Greenway, C Waguespack, E King, G Fry, A Dragg, B Gildersleeve, J Arceneaux, N Haynes, A Thomassie, M Pavlionis, B Bourgeois, C Hazlett, S Mudaliar, R Henry, S Boeder, J Pettus, E Diaz, D Garcia-Acosta, S Maggs, C DeLue, A Stallings, E Castro, S Hernandez, J Krakoff, J M Curtis, T Killean, M Khalid, E Joshevama, E Diaz, D Martin, K Tsingine, T Karshner, J Albu, F X Pi-Sunyer, S Frances, C Maggio, E Ellis, J Bastawrose, X Gong, M A Banerji, P August, M Lee, D Lorber, N M Brown, D H Josephson, L L Thomas, M Tsovian, A Cherian, M H Jacobson, M M Mishko, M S Kirkman, J B Buse, J Dostou, S Machineni, L Young, K Bergamo, A Goley, J Kerr, J F Largay, S Guarda, J Cuffee, D Culmer, R Fraser, H Almeida, S Coffer, E Debnam, L Kiker, S Morton, K Josey, G Fuller, W T Garvey, A L Cherrington, D Dyer, McR Lawson, O Griffith, A Agne, S McCullars, R M Cohen, J Craig, M C Rogge, K Burton, K Kersey, C Wilson, S Lipp, M B Vonder Meulen, C Adkins, T Onadeko, N Rasouli, C Baker, E Schroeder, M Razzaghi, C Lyon, R Penaloza, C Underkofler, R Lorch, S Douglass, S Steiner, W I Sivitz, E Cline, L K Knosp, J McConnell, T Lowe, W H Herman, R Pop-Busui, M H Tan, C Martin, A Waltje, A Katona, L Goodhall, R Eggleston, S Kuo, S Bojescu, S Bule, N Kessler, E LaSalle, K Whitley, E R Seaquist, A Bantle, T Harindhanavudhi, A Kumar, B Redmon, J Bantle, M Coe, M Mech, A Taddese, L Lesne, S Smith, C Desouza, L Kuechenmeister, V Shivaswamy, S Burbach, M G Rodriguez, K Seipel, A Alfred, A L Morales, J Eggert, G Lord, W Taylor, R Tillson, D S Schade, A Adolphe, M Burge, E Duran-Valdez, J Martinez, A Bancroft, S Kunkel, F Ali Jamaleddin Ahmad, D Hernandez McGinnis, B Pucchetti, E Scripsick, A Zamorano, R A DeFronzo, E Cersosimo, M Abdul-Ghani, C Triplitt, D Juarez, M Mullen, R I Garza, H Verastiqui, K Wright, C Puckett, P Raskin, C Rhee, S Abraham, L F Jordan, S Sao, L Morton, O Smith, L Osornio Walker, L Schnurr-Breen, R Ayala, R B Kreymer, D Sturgess, K M Utzschneider, S E Kahn, L Alarcon-Casas Wright, E J Boyko, E C Tsai, D L Trence, S Trikudanathan, B N Fattaleh, B K Montgomery, K M Atkinson, A Kozedub, T Concepcion, C Moak, N Prikhodko, S Rhothisen, T A Elasy, S Martin, L Shackelford, R Goidel, N Hinkle, C Lovell, J Myers, J Lipps Hogan, J B McGill, M Salam, T Schweiger, S Kissel, C Recklein, M J Clifton, W Tamborlane, A Camp, B Gulanski, S E Inzucchi, K Pham, M Alguard, P Gatcomb, K Lessard, M Perez, L Iannone, E Magenheimer, A Montosa, W T Cefalu, J Fradkin, H B Burch, A A Bremer, D M Nathan, J M Lachin, J B Buse, S E Kahn, H Krause-Steinrauf, M E Larkin, M Tiktin, D Wexler, H B Burch, A A Bremer, J M Lachin, H Krause-Steinrauf, N Younes, I Bebu, N Butera, C J Buys, A Fagan, Y Gao, A Ghosh, M R Gramzinski, S D Hall, E Kazemi, E Legowski, H Liu, C Suratt, M Tripputi, A Arey, M Backman, J Bethepu, C Lund, P Mangat Dhaliwal, P McGee, E Mesimer, L Ngo, M Steffes, J Seegmiller, A Saenger, V Arends, D Gabrielson, T Conner, S Warren, J Day, J Huminik, A Scrymgeour, E Z Soliman, Y Pokharel, Z M Zhang, C Campbell, J Hu, L Keasler, S Hensley, Y Li, W H Herman, S Kuo, C Martin, A Waltje, R Mihalcea, D J Min, V Perez-Rosas, L Prosser, K Resnicow, W Ye, H Shao, P Zhang, J Luchsinger, D Sanchez, S Assuras, E Groessl, F Sakha, H Chong, N Hillery, B M Everett, I Abdouch, G Bahtiyar, P Brantley, F E Broyles, G Canaris, P Copeland, J J Craine, W L Fein, A Gliwa, L Hope, M S Lee, R Meiners, V Meiners, H O'Neal, J E Park, A Sacerdote, E Sledge Jr, L Soni, J Steppel-Reznik, A Turchin, B Brooks-Worrell, C S Hampe, J P Palmer, A Shojaie, J Higgins, L Fischer, S Golden, J Gonzalez, A Naik, E Walker, L Doner Lotenberg, H Sharp, J M Gallivan, J Lim, D M Tuncer, S Behringer-Massera

Affiliation

¹ From the Massachusetts General Hospital Diabetes Center, Harvard Medical School, Boston (D.M.N., M.E.L., D.J.W.); the Biostatistics Center, Department of Biostatistics and Bioinformatics, Milken Institute School of Public Health, George Washington University, Rockville (J.M.L., I.B., H.K.-S., M. Tripputi, N.Y.), and the National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda (H.B.B.) - both in Maryland; the Division of Endocrinology and Metabolism, Department of Medicine, University of North Carolina School of Medicine, Chapel Hill (J.B.B., M.S.K.), and the Department of Medicine, Duke Division of Endocrinology, Metabolism, and Nutrition, Duke University Medical Center, Durham (J.B.G.) - both in North Carolina; the University of Alabama, Birmingham (A.L.C.); Kaiser Permanente Center for Health Research, Portland, OR (S.P.F.); the Division of Metabolism, Endocrinology, and Nutrition, Department of Medicine, Veterans Affairs (VA) Puget Sound Health Care System, University of Washington, Seattle (S.E.K.); the Atlanta VA Medical Center, Decatur, GA (L.S.P.); the Division of Metabolism, Endocrinology and Diabetes, Department of Internal Medicine, University of Michigan, Ann Arbor (R.P.-B.); the Advanced Research and Diagnostic Laboratory, Department of Laboratory Medicine and Pathology, University of Minnesota, Minneapolis (M.S.); and the Louis Stokes Cleveland VA Medical Center, Case Western Reserve University, Cleveland (M. Tiktin).

Abstract

Background: Data are lacking on the comparative effectiveness of commonly used glucose-lowering medications, when added to metformin, with respect to microvascular and cardiovascular disease outcomes in persons with type 2 diabetes.

Methods: We assessed the comparative effectiveness of four commonly used glucose-lowering medications, added to metformin, in achieving and maintaining a glycated hemoglobin level of less than 7.0% in participants with type 2 diabetes. The randomly assigned therapies were insulin glargine U-100 (hereafter, glargine), glimepiride, liraglutide, and sitagliptin. Prespecified secondary outcomes with respect to microvascular and cardiovascular disease included hypertension and dyslipidemia, confirmed moderately or severely increased albuminuria or an estimated glomerular filtration rate of less than 60 ml per minute per 1.73 m² of body-surface area, diabetic peripheral neuropathy assessed with the Michigan Neuropathy Screening Instrument, cardiovascular events (major adverse cardiovascular events [MACE], hospitalization for heart failure, or an aggregate outcome of any cardiovascular event), and death. Hazard ratios are presented with 95% confidence limits that are not adjusted for multiple comparisons.

Results: During a mean 5.0 years of follow-up in 5047 participants, there were no material differences among the interventions with respect to the development of hypertension or dyslipidemia or with respect to microvascular outcomes; the mean overall rate (i.e., events per 100 participant-years) of moderately increased albuminuria levels was 2.6, of severely increased albuminuria levels 1.1, of renal impairment 2.9, and of diabetic peripheral neuropathy 16.7. The treatment groups did not differ with respect to MACE (overall rate, 1.0), hospitalization for heart failure (0.4), death from cardiovascular causes (0.3), or all deaths (0.6). There were small differences with respect to rates of any cardiovascular disease, with 1.9, 1.9, 1.4, and 2.0 in the glargine, glimepiride, liraglutide, and sitagliptin groups, respectively. When one treatment was compared with the combined results of the other three treatments, the hazard ratios for any cardiovascular disease were 1.1 (95% confidence interval [CI], 0.9 to 1.3) in the glargine group, 1.1 (95% CI, 0.9 to 1.4) in the glimepiride group, 0.7 (95% CI, 0.6 to 0.9) in the liraglutide group, and 1.2 (95% CI, 1.0 to 1.5) in the sitagliptin group.

Conclusions: In participants with type 2 diabetes, the incidences of microvascular complications and death were not materially different among the four treatment groups. The findings indicated possible differences among the groups in the incidence of any cardiovascular disease. (Funded by the National Institute of Diabetes and Digestive and Kidney Diseases and others; GRADE ClinicalTrials.gov number, NCT01794143.).

Publication types

Comparative Study
Randomized Controlled Trial
Research Support, N.I.H., Extramural

MeSH terms

Albuminuria / etiology
Albuminuria / prevention & control
Blood Glucose / analysis
Cardiovascular Diseases* / etiology
Cardiovascular Diseases* / prevention & control
Comparative Effectiveness Research
Diabetes Complications* / etiology
Diabetes Complications* / prevention & control
Diabetes Mellitus, Type 2* / complications
Diabetes Mellitus, Type 2* / drug therapy
Diabetic Neuropathies / diagnosis
Diabetic Neuropathies / etiology
Diabetic Neuropathies / prevention & control
Drug Therapy, Combination
Dyslipidemias / etiology
Dyslipidemias / prevention & control
Glomerular Filtration Rate
Glycated Hemoglobin* / analysis
Heart Failure / etiology
Heart Failure / prevention & control
Humans
Hypertension / etiology
Hypertension / prevention & control
Hypoglycemic Agents* / adverse effects
Hypoglycemic Agents* / therapeutic use
Insulin Glargine / adverse effects
Insulin Glargine / therapeutic use
Liraglutide / adverse effects
Liraglutide / therapeutic use
Metformin* / adverse effects
Metformin* / therapeutic use
Microvessels / drug effects
Sitagliptin Phosphate / adverse effects
Sitagliptin Phosphate / therapeutic use
Sulfonylurea Compounds / adverse effects
Sulfonylurea Compounds / therapeutic use

Substances

Blood Glucose
Glycated Hemoglobin A
Hypoglycemic Agents
Sulfonylurea Compounds
Insulin Glargine
glimepiride
Liraglutide
Metformin
Sitagliptin Phosphate

Associated data

ClinicalTrials.gov/NCT01794143

Abstract

Publication types

MeSH terms

Substances

Associated data

Grants and funding