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Journal Club E.S. Mearns*1,2,W. J. Saulsberry 1,2, C. M. White 1,2, C. G. Kohn3 , S. Lemieux1 , A. Sihabout1 , I. Salamucha1 and C. I. Coleman *1,2 Efficacy and safety of antihyperglycaemic drug regimens added to metformin and sulphonylurea therapy in Type 2 diabetes: a network meta-analysis Diabetic Medicine. 2015 June. doi: 10.1111/dme.12837. 2015年7月30日 8:30-8:55 8階 医局 埼玉医科大学 総合医療センター 内分泌・糖尿病内科 Department of Endocrinology and Diabetes, Saitama Medical Center, Saitama Medical University Sellami Mnif Houda ADA EASD Treatment Algorithm Type 2 Diabetes | NDEI •This slide reviews recommendations for antihyperglycemic therapy for type 2 diabetes from the updated position statement of the American Diabetes Association and the European Association for the Study of Diabetes (ADA/EASD). Abbreviations: DPP-4 inhibitor=dipeptidyl peptidase-4 inhibitor; GLP-1 RA=glucagon-like peptide-1 receptor agonist; MET=metformin; SGLT2 inhibitor=sodium glucose cotransporter 2 inhibitor; SU=sulfonylurea; TZD=thiazolidinedione Refer to source document for full recommendations. •Received Date : 20-Dec-2014 •Revised Date : 01-Apr-2015 •Accepted Date : 19-Jun-2015 •Article type : Systematic Review or Meta-analysis •Title: Diabetic Medicine •Created by: Maria Davie •Email proofs to: [email protected] •Article no.: DME-2014-01019 Article type: Review Article Review Article Efficacy and safety of antihyperglycaemic drug regimens added to metformin and sulphonylurea therapy in Type 2 diabetes: a network meta-analysis E. S. Mearns*1,2,W. J. Saulsberry 1,2, C. M. White1,2, C. G. Kohn3 , S. Lemieux1 , A. Sihabout1 , I. Salamucha1 and C. I. Coleman *1,2 1 University of Connecticut School of Pharmacy, Department of Pharmacy Practice, Storrs, 2 University of Connecticut/Hartford Hospital Evidence-Based Practice Center, Hartford, and 3 University of Saint Joseph School of Pharmacy, Hartford, CT, USA *These authors contributed equally to this meta-analysis. Ann Neurol. 2015 May 14. doi: 10.1002/ana.24439. Objective To assess the efficacy and safety of thirdline adjuvant antihyperglycaemic agents in people with Type 2 diabetes mellitus failing metformin and sulphonylurea combination therapy. - To help clinicians to choose the optimum therapy (reduction of HbA1C with less side effects) Methods Performed a systematic literature search from the earliest possible date–2014 Study selection 1- Published in English 2- Parallel RCT study 3- Comparing US/UE approved T2 Diabetes therapy (including non insulin and/or long acting Basal insulin) with another T2D drug therapy/ placebo 4- Only patients who showed inadequate response to Metformin-SU therapy combination at randomization. 5- study (treatment) duration: 12-52 week And report change in HbA1c, 6- Patients should be on Met+Su for at least 3 weeks Data synthesis - traditional meta-analyses: changes in HbA1c, body weight and SBP - P value < 0.05 - Pairwise meta-analyses were performed for each AHA - network meta-analysis were performed: analyze direct within-trial comparisons between two treatments + enables incorporation of indirect comparisons constructed from two trials that have one treatment in common FIGURE 1 Results of the literature search. CCTR, Cochrane Controlled Trials Register; EU, European Union; FDA, US Food and Drug Administration; SU, sulphonylurea. FIGURE 2 Network diagram of randomized controlled trials evaluating antihyperglycaemic agents in addition to metformin and a sulphonylurea in Type 2 diabetes. All therapies are in combination with metformin and a sulphonylurea. Lines represent the presence of direct comparison trial(s). All direct comparisons were based upon a single study; except where otherwise indicated. RESULTS: Characteristics of the included trials: 1. - The trial duration range : 16–52 weeks 2. - Mean age: 41–67 years 3. BMI 24–35 kg/m2 4. Weight 65–99 kg 5. SBP 127–146 mmHg 6. Baseline HbA1c: 64–80 mmol/mol (8.0–9.5%). Main ending points: 1-Change in HbA1c All AHAs significantly lowered HbA1c from baseline but by different magnitudes 2- Body weight Only SGLT2 inhibitors showed statistically significant weight loss compared with placebo/control (1.43–2.07 kg) TZDs, glargine and sitagliptin : significant weight gain compared with placebo/control 3- Systolic blood pressure •Rosiglitazone, liraglutide and all SGLT2 inhibitors: significantly decreased SBP compared with placebo/control (2.93–6.83 mmHg). •Pioglitazone, sitagliptin and insulin glargine : neutral effect In active drug comparisons: •Rosiglitazone significantly reduced SBP compared with all other therapies analyzed (3.43–9.38 mmHg) except dapagliflozin ( similar reduction). •All SLGT2 inhibitors and liraglutide were associated with a significant decrease in SBP compared with pioglitazone, insulin glargine and sitagliptin •No data were available for acarbose, exenatide, linagliptin, saxagliptin or vildagliptin 4-Confirmed hypoGlycemia •TZDs, glargine, sitagliptin, liraglutide, and canagliflozin : significantly higher rates of confirmed hypoglycaemia compared with placebo/control •Empagliflozin, exenatide and DPP-4 inhibitors (with the exception of sitagliptin) were not. •In active drug comparisons: Glargine and Rosiglitazone significant higher rate of confirmed hypoglycaemia compared with the SGLT-2 In, exenatide, linagliptin and sitagliptin 5- Urinary and genital tract infections •No data evaluating (acarbose, pioglitazone and rosiglitazone) for the UTI •Only four of the 13 agents (all SGLT2 inhibitors and sitagliptin) reported on GTI. No evaluable therapy was associated with an increased risk of UTI when compared with placebo/control and •only canagliflozin was associated with a greater risk of GTI compared with placebo/control (relative risk 3.9, 95% CI 1.58--9.6) and sitagliptin (relative risk 5.64, 95% CI 2.68–11.88) Direct and indirect meta-analysis coherence Comparing the results of the 36 possible direct and indirect effect estimates across all six endpoints Evidence of incoherence for only two comparisons; both for the body weight endpoint (canagliflozin–sitagliptin–placebo) and (pioglitazone–sitagliptin–placebo). INTERPRETATION - For peoples with strong apprehension about needles and self injections oral agents, such as SGLT2 inhibitors, maybe a better choice for them This meta-analysis suggests patients can be prescribed many oral agents with minimal sacrifice of glycaemic efficacy. -T2D high risk of albuminuria (Diabetes+Obesity+HBP) SGLT2 inhibitors,rosiglitazone and liraglutide have better BP reduction. SGLT2 inhibitors+++, GLP-1 analogues and acarbose Weight reduction -T2D (mostly women): high risk of UTI and GTI, however we did not find a greater risk of UTIs for SGLT2 Inh class (despite its Urine Tract action) or any other evaluable agent compared with placebo/control LIMITATIONS -Don’t assess other endpoints: CV events, Pancreatitis, GI effects.. - Some AHA were compared on only 1-2 trials - Most trials followed patients for 24 Weeks - Can not exclude the presence of incoherence in the network - The quality of trial reporting and conduct varied between studies, Message