Albiglutide and cardiovascular outcomes in patients with type 2 diabetes and cardiovascular disease (Harmony Outcomes): a double-blind, randomised placebo-controlled trial

Hernandez, Adrian F.; Green, Jennifer B.; Janmohamed, Sherief R.; D’Agostino, Ralph B.; Granger, Christopher B.; Jones, Nigel C.; Leiter, Lawrence A.; Rosenberg, Anne E; Sigmon, Kristina N.; Somerville, Matthew C.; Thorpe, Karl M.; McMurray, John J.V.; Prato, Stefano Del; Califf, Robert M.; Holman, Rury R.; DeMets, David L.; Riddle, Matthew C.; Goodman, Shaun G.; McGuire, Darren K.; Alexander, Karen P.; DeVore, Adam D.; Melloni, Chiara; Patel, Chetan K.; Kong, David F.; Bloomfield, Gerald S.; Roe, Matthew T.; Tricoci, Pierluigi; Harrison, Rob; Lópes, Renato D.; Mathews, Robin; Mehta, Rajendra; Jones, W. Schuyler; Vemulapalli, Sreekanth; Povsic, Thomas J.; Eapen, Zubin J.; Dombrowski, Keith; Kolls, Brad J.; Jordan, J. Dedrick; Ambrosy, Andrew P.; Greene, Stephen J.; Mandawat, Aditya; Shavadia, Jay; Cooper, Lauren B.; Sharma, Abhinav; Guimarães, Patrícia O.; Friedman, Daniel J.; Wilson, Matt; Endsley, Patricia; Gentry, Tracy; Collier, Jeannie; Perez, Kathleen; James, Kourtnei; Roush, Jennifer E.; Pope, Connie; Howell, Christina Neiger; Johnson, Megan; Bailey, Matt; Cole, Joanna; Akers, Teresa; Vandyne, Beth; Thomas, Betsy; Rich, Jenny; Bartone, Susan; Beaulieu, Gail; Brown, Kim; Chau, Tuan; Christian, Tamra; Coker, Rebecca; Greene, Deb; Haddock, Trevorlyn; Jenkins, Wendy; Haque, Ghazala; Marquess, Marsha L.; Pesarchick, Jean; Rethaford, Renee; Stone, Allegra; Kawas, Firas Al; Anderson, Michelle A.; Enns, Robert; Sinay, Isaac; Mathieu, Chantal; Yordanov, Victor; Hramiak, Irene; Haluzı́k, Martin; Galatius, Søren; Guerci, Bruno; Nauck, Michael A.; Migdalis, Ilias; Tan, Choon Beng Kathryn; Kocsis, Győző; Giaccari, Andrea; Lee, Moon Kyu; Muñoz, Ernesto; Cornel, Jan H.; Birkeland, Kåre I.; Pinto, Miguel E.; Tirador, Louie; Olesińska-Mader, Martyna; Shestakova, Marina V.; Distiller, Larry A.; López‐Sendón, José; Eliasson, Björn; Chiang, Chern‐En; Srimahachota, Suphot; Mankovsky, Boris; Bethel, M. Angelyn; Dungan, Kathleen; Kosiborod, Mikhail; Alvarisqueta, Andres; Baldovino, Jorge; Besada, Diego; Calella, Pedro; Cantero, Maria Cecilia; Castaño, Patricia; Chertkoff, Alejandro; Cuadrado, Jesus; Loredo, Luis De; Domínguez, Andrea; Español, Maria Vanesa; Finkelstein, Hernan; Frechtel, Gustavo Daniel; Fretes, Jose; Santos, Natalia Garrido; Gonzalez, Joaquin; Litvak, Marcos; Loureyro, Juan; Maffei, Laura; Maldonado, Natacha; Gasparini, Diego Mohr; Orio, Silvia; Manghi, Federico Pérez; Papini, Nelson; Sala, Jorgelina; Schygiel, Pablo; Sposetti, Georgina; Ulla, María Rosa; Verra, F.; Zabalua, Silvina; Zaidman, Cesar J.; Crenier, Laurent; Debroye, Corinne; Duyck, Francis; Scheen, André; Gaal, Luc Van; Vercammen, Chris; Damyanova, Velichka; Dimitrov, Stefan; Kovacheva, Snezhina; Lozanov, L; Margaritov, Viktor; Mihaylova-Shumkova, Rositsa; Николаева, А. Г.; Stoyanova, Zhasmina; Akhras, Ronald; Beaudry, Yves; Bedard, Jacques; Berlingieri, Joseph; Chehayeb, R; Cheung, Stephen C.W.; Conway, James; Cusson, Jean R.; Siega, Anthony Della; Dumas, R; Dzongowski, Peter; Ferguson, Murdo; Gaudet, Daniel; Grondin, François; Gupta, Anil; Gupta, Milan; Halperin, Frank; Houle, Pierre-Alain; Jones, Michael A.; Kouz, Simon; Kovacs, Christopher; Landry, Daniel; Lonn, Eva; O’Mahony, William; Peterson, Sean; Reich, Dennis; Rosenbloom, Alan J.; St-Maurice, François; Tugwell, Barna; Vizel, Saul; Woo, Vincent; Brychta, Tomáš; Cech, Vladimir; Dvořáková, Eva; Edelsberger, Tomáš; Halčiaková, Katarina; Křížová, Jarmila; Laštůvka, Jiří; Piperek, Martin; Prymkova, Vera; Raclavska, Lea; Šilhová, Elena; Urbánek, R; Vrkoč, Jan; Andersen, Ulla; Brønnum-Schou, Jens; Hove, Jens D.; Jensen, Jan Skov; Køber, Lars; Kristiansen, Ole Peter; Lund, Per; Melchior, Thomas; Nyvad, Ole; Schou, Morten; Boye, Alain; Cadinot, Didier; Gouet, D.; Henry, Patrick; Kessler, L.; Lalau, Jean–Daniel; Petit, Catherine; Thuan, Jean-Francois; Voinot, C.; Vouillarmet, Julien; Axthelm, Christoph; Berger, Dirk; Bieler, Tasso; Birkenfeld, Andreas L.; Bott, Jochen; Busch, Klaus; Caca, Karel; Chevts, Julia; Donaubauer, Torsten; Erlinger, Rudolf; Funke, Klaus; Großkopf, Josef; Hagenow, Andreas; Hamann, Mónika Inés; Hartard, Manfred; Heymer, Peter; Huppertz, Wolfgang; Illies, Gabriele; Jacob, Stephan; Jung, Thomas; Kahrmann, Gerd; Kast, Petra; Kellerer, Monika; Kempe, Hans‐Peter; Khariouzov, Andrei; Klausmann, Gerhard; Klein, Christiane; Kleinecke-Pohl, Uwe; Kleinertz, Klaus; Koch, Thorsten; Kosch, Christine; Lorra, Babette; Luedemann, Joerg; Luttermann, Matthias; Maxeiner, Stephan; Milek, K; Moelle, Andrea; Neumann, Gerhard; Nischik, Ruth; Oehrig-Pohl, Edith; Plaßmann, Georg; Pohlmeier, Lars; Proepper, Felix; Regner, Stefan; Rieker, Werner; Rose, Ludger; Samer, Holger; Sauter, Joachim; Schäper, Frank; Schiffer, C; Schmidt, J.; Scholz, B.; Schulze, J; Segner, Alexander; Seufert, Jochen; Sigal, Helena; Steindorf, Joerg; Juergen, Stockhausen; Stuebler, Petra; Taeschner, Heidrun; Tews, Dietrich; Tschöepe, Diethelm; Wilhelm, Karl; Zeller-Stefan, Helga; Avramidis, Iakovos; Bousboulas, Stavros; Bristianou, Magdalini; Dimitriadis, Georgios; Elisaf, Moses; Kotsa, Kalliopi; Μelidonis, Αndreas; Mitrakou, Asimina; Pagkalos, Emmanouil; Παπάνας, Νικόλαος; Pappas, Angelos; Sampanis, Christos; Tentolouris, Nikolaοs; Τσάπας, Απόστολος; Tzatzagou, Glykeria; Ozaki, Risa; Hajdú, Csaba; Harcsa, Eleonóra; Könyves, L.; Mucsi, János; Pauker, Zsolt; Petró, Gizella; Plés, Zsolt; Révész, Katalin; Vangel, Sandor; Vass, Viktor; Avogaro, Angelo; Boemi, Massimo; Bonadonna, Riccardo C.; Consoli, Agostino; Cosmo, Salvatore De; Bartolo, Paolo Di; Dotta, Francesco; Frontoni, Simona; Galetta, Marianna; Gambineri, Alessandra; Gazzaruso, Carmine; Giorgino, Francesco; Lauro, Davide; Orsi, Emanuela; Paolisso, Giuseppe; Perriello, G.; Piatti, PierMarco; Pontiroli, Antonio E.; Ponzani, Paola; Rivellese, Angela Albarosa; Sesti, Giorgio; Tonolo, Giancarlo; Trevisan, Roberto; Ahn, Chul Woo; Baik, Sei-Hyun; Cha, Bong‐Soo; Chung, Choon Hee; Jang, Hak Chul; Kim, Chong‐Jin; Kim, Hye Soon; Kim, In Joo; Lee, Eun Young; Lee, Hyoung Woo; Lee, Kwan‐Woo; Moon, Keon-Woong; Namgung, June; Park, Kyong Soo; Yoo, Soon Jib; Yu, Jaemyung; Llamas, Edmundo-Alfredo Bayram; Cervantes-Escárcega, Jose-Luis; Flota-Cervera, Luis Fernando; González-González, José Gerardo; Pascoe-González, Sara; Pelayo-Orozco, Emilia Susana; Ramirez-Diaz, Santiago-Paulino; Saldana-Mendoza, Arturo; Jerjes-Díaz, Carlos Sánchez; Torres-Colores, Jose Juan; Vidrio-Velázquez, Maricela; Villagordoa-Mesa, Juan; Beijerbacht, Hugo Peter; Groutars, Reginald G.E.J.; Hoek, Boudewijn A; Hoogslag, Pieter A.M.; Kooy, Adriaan; Kragten, Johannes A.; Lieverse, Aloysius G.; Swart, Hendrik P.; Viergever, Eric P.; Ahlqvist, Jørn; Cooper, John G.; Gulseth, Hanne Løvdal; Guttormsen, Gaute; Wium, Cecilie; Arbañil, Hugo; Calderón, Jorge; Camacho, L. 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doi:10.1016/s0140-6736(18)32261-x

Cited by 1,219 publications

(929 citation statements)

References 22 publications

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“…The emergence of new approaches to glucose lowering with proven cardiovascular and renal benefits (ie, sodium‐glucose co‐transporter‐2 [SGLT‐2] inhibitors and glucagon‐like peptide‐1 [GLP‐1] agonists) has created further uncertainty as to the value of aiming for near normal glycaemic targets without consideration of the agents used. Indeed, the growing body of trial evidence would suggest that the agents used, at least over the short term (2‐5 years), may be even more important (especially in high‐risk patients with clinically apparent cardiovascular or renal disease) . The EMPA‐Reg, CANVAS, DECLARE‐TIMI and CREDENCE trials all reported the superiority of the introduction of SGLT‐2 inhibitors compared with placebo and standard care among patients with type 2 diabetes .…”

Section: Discussionmentioning

confidence: 99%

ADVANCE in context: The benefits, risks and feasibility of providing intensive glycaemic control based on gliclazide modified release

Zoungas

2020

Diabetes Obesity Metabolism

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In the last 3 decades, four large multicentre, randomized clinical trials of patients with type 2 diabetes (UKPDS, ADVANCE, ACCORD and VADT) have studied different approaches to achieving near normal glycaemic targets. Each was designed against a background of international and national guidelines recommending glycaemic targets of 6.5% or less to prevent diabetic complications. Collectively, these clinical trials provide the most robust evidence of the potential vascular benefits and risks of more versus less glucose control and provide critical insights into how therapies are used. In this review, the glucose‐lowering approach used by the ADVANCE trial is considered and compared with those used by the other trials.

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Section: Discussionmentioning

confidence: 99%

ADVANCE in context: The benefits, risks and feasibility of providing intensive glycaemic control based on gliclazide modified release

Zoungas

2020

Diabetes Obesity Metabolism

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“…All the test drugs showed their noninferiority to placebo with regard to their primary endpoint. In five of the twelve CVOTs, the Albiglutide and Cardiovascular Outcomes in Patients with Type 2 Diabetes and Cardiovascular Disease (HARMONY), the Liraglutide Effect and Action in Diabetes: Evaluation of Cardiovascular Outcome Results (LEADER), the Semaglutide and Cardiovascular Outcomes in Patients with Type 2 Diabetes (SUSTAIN‐6), the Canagliflozin Cardiovascular Assessment Study (CANVAS), and the Empagliflozin Cardiovascular Outcome Event Trial in Type 2 Diabetes Mellitus Patients (EMPA‐REG OUTCOME), the primary CV endpoint was significantly lower in the test drug than the placebo group. The CV efficacy shown in the five CVOTs was achieved alongside moderate glycemic control, with HbA1c values not less than 6.8% (Table ), as recommended by the ACP guidance …”

Section: Hba1c Targets and CV Risk Reduction Associated With Newer Glmentioning

confidence: 99%

Challenges to hemoglobin A1c as a therapeutic target for type 2 diabetes mellitus

Ikeda

Shimazawa

2019

J of Gen and Family Med

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Glycated hemoglobin (HbA1c) is widely accepted as the most reliable measure of long‐term glycemia. However, there is disagreement among professional medical societies on a proper glycemic target for long‐term benefits in type 2 diabetes (T2D). The use of some glucose‐lowering drugs was associated with heart failure despite substantial lowering of HbA1c. The failure of intensive glycemic control to reduce cardiovascular risk in some trials again brought into question the usefulness of HbA1c as a therapeutic target in T2D. In large cardiovascular outcome trials, some newer glucose‐lowering drugs were associated with higher risks of heart failure or amputation despite comparable glycemic control between the test and placebo groups. Here, we provide evidence that variation in hemoglobin glycation between individuals is responsible for these inconsistencies. We suggest that further research be conducted in this area and that the findings be applied to clinical trials and practice.

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“…nary syndrome, the rate of HAHF was 4.0% with lixisenatide and 4.2% with placebo (HR 0.96, 95% CI 0.75-1.23; P = 0.75) 160. HAHF combined with cardiac death was 4% in the albiglutide group and 5% in the placebo group (HR 0.85, 95% CI 0.7-1.04; P = 0.113) 161. HAHF combined with cardiac death was 4% in the albiglutide group and 5% in the placebo group (HR 0.85, 95% CI 0.7-1.04; P = 0.113) 161.…”

mentioning

confidence: 98%

Heart failure in the patient with diabetes: Epidemiology, aetiology, prognosis, therapy and the effect of glucose‐lowering medications

Bell¹,

Goncalves

2019

Diabetes Obesity Metabolism

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In people with type 2 diabetes the frequency of heart failure (HF) is increased and mortality from HF is higher than with non-diabetic HF. The increased frequency of HF is attributable to the cardiotoxic tetrad of ischaemic heart disease, left ventricular hypertrophy, diabetic cardiomyopathy and an extracellular volume expansion resistant to atrial natriuretic peptides. Activation of the renin-angiotensin-aldosterone system and sympathetic nervous systems results in cardiac remodelling, which worsens cardiac function. Reversal of remodelling can be achieved, and cardiac function improved in people with HF with reduced ejection fraction (HFrEF) by treatment with angiotensin-converting enzyme inhibitors and β-blockers. However, with HF with preserved ejection fraction (HFpEF), only therapy for the underlying risk factors helps.Blockers of mineralocorticoid receptors may be beneficial in both HFrEF and HFpEF. Glucoselowering drugs can have a negative effect (insulin, sulphonylureas, dipeptidyl peptidase-4 inhibitors and thiazolidinediones), a neutral effect (α-glucosidase inhibitors and glucagon-like peptide-1 receptor agonists) or a positive effect (sodium-glucose co-transporter-2 inhibitors and metformin).antidiabetic drug, GLP-1 analogue, heart failure, insulin therapy, SGLT2 inhibitor, thiazolidinediones 1 | INTRODUCTION Heart failure (HF) results from structural and/or functional impairment of ventricular filling and/or ejection 1 and it is a common and serious comorbidity of type 2 diabetes. 2 In the present review we document the increased incidence of HF, and the reasons for this increase, as well as its poor prognosis in patients with diabetes.The potential therapies to both prevent and treat HF are discussed, in addition to the positive and negative effects of glucoselowering medications.Several reviews on this important subject have been recently published 3-7 ; however, this is a rapidly evolving field. An important limitation has been that HF was not a primary endpoint in most cardiovascular (CV) outcome trials, and it has been the most heterogeneously distributed outcome. | EPIDEMIOLOGYAs long ago as the Framingham Heart Study, HF was shown to be twice as common in men with diabetes and five times more common in women with diabetes between the ages of 45 and 74 years when compared with age-matched non-diabetic controls, and, in those aged ≤65 years, there was a fourfold increase in the prevalence of HF in men with diabetes and an eightfold increase in women with diabetes. 8In almost 10 000 patients with type 2 diabetes enrolled in a Health Maintenance Organization, 12% had HF at entry. Independent risk factors for the presence of HF were older age, longer duration of diabetes, use of insulin and lower body mass index (BMI). 9 In addition, those with type 2 diabetes who did not have HF at entry developed HF at a rate of 3.3% per year. The Reykjavik Study reported a 12% prevalence of HF in people with diabetes compared with 3% in people

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Albiglutide and cardiovascular outcomes in patients with type 2 diabetes and cardiovascular disease (Harmony Outcomes): a double-blind, randomised placebo-controlled trial

Cited by 1,219 publications

References 22 publications

ADVANCE in context: The benefits, risks and feasibility of providing intensive glycaemic control based on gliclazide modified release

ADVANCE in context: The benefits, risks and feasibility of providing intensive glycaemic control based on gliclazide modified release

Challenges to hemoglobin A1c as a therapeutic target for type 2 diabetes mellitus

Heart failure in the patient with diabetes: Epidemiology, aetiology, prognosis, therapy and the effect of glucose‐lowering medications

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