879-P: Cardiorenal Outcomes Associated with the Use of Dapagliflozin Compared with DPP-4 Inhibitors as Add-on Treatment in Uncontrolled DM2 Patients with Failure to Previous Treatment—A Retrospective, Real-Life Evaluation in México

879-P: Cardiorenal Outcomes Associated with the Use of Dapagliflozin Compared with DPP-4 Inhibitors as Add-on Treatment in Uncontrolled DM2 Patients with Failure to Previous Treatment—A Retrospective, Real-Life Evaluation in México

Mexico is one of the three countries in Region of Americas with the highest prevalence (14.4%) of DM. We conducted a retrospective study in Mexico and compare Dapagliflozin effect in cardio-renal outcomes and metabolic control compared to DPP4-inhibitors (DPP4i) as added-on therapy in T2DM patients...

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Published in:Diabetes (New York, N.Y.) Vol. 72; no. Supplement_1; p. 1
Main Authors: ESPINOZA-PERALTA, DIEGO, HERNANDEZ-ALARCON, JIMENA, LOPEZ, IRLANDA N., CETINA-CANTO, JOSE, BÚRQUEZ-GONZÁLEZ, MARIA E., PAUL, PEDRO V., BUSTAMANTE, GUADALUPE A., CARLOS GARNICA CUELLAR, JUAN, MIRELES-ZAVALA, LEONOR G., JUAREZ-COMBONI, SONIA C., RODRÍGUEZ, ARELI M.
Format: Journal Article
Language:English
Published: New York American Diabetes Association 20-06-2023
Subjects:
Antidiabetics
Congestive heart failure
Creatinine
Diabetes mellitus
Renal failure
Statistical analysis
Statistics
Mexico
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Summary:Mexico is one of the three countries in Region of Americas with the highest prevalence (14.4%) of DM. We conducted a retrospective study in Mexico and compare Dapagliflozin effect in cardio-renal outcomes and metabolic control compared to DPP4-inhibitors (DPP4i) as added-on therapy in T2DM patients with failure to previous medications. Objectives: Compare proportion of patients achieving HbA1c below 7%, first appearance of eGFR below 60 ml/min, renal replacement therapy, heart failure hospitalization and death by the end of the 156-week observation period from index date. Inclusion Criteria: T2DM subjects ≥18 years old with failure to any previous antidiabetic medication and HbA1c% ≥7 that started Dapa or DPP4i as add-on to other antidiabetic drugs from August 2014 to December 2019. Statistical Methods and Analysis: A propensity score matching model (nearest neighbor algorithm) was used. Results: Of 1800 subjects, 267 met statistical matching criteria. There were no differences in basal characteristics of age, SBP, Creatinine Clearance, but DAPA group had higher basal HbA1c (8.54±1.45 vs 8.16±1.43, p<0.01). Patients in Dapa compared to DPP4i achieved A1c ≤7% in 49.8% vs 20% (p<0.01) by week 156. Creatinine clearance between groups favored DAPA after week 52 (76.07±18.52 vs 86.40±21.27, p<0.01), and persisted through week 156 (68.19±19.4 vs 88.45±19.73, p<0.01). By week 52, Incidental CKD was present in 5.8% of Dapa group and in 14.8% of DPP4i group, p=0.013 (OR 0.607, 95% IC 0.409-0.901), and by week 156 6.5% DAPA vs 27.6% DPP4i, p<0.01 (OR 0.275, 95% IC 0.191-396). There were no differences in HF hospitalizations. Conclusion: In patients with uncontrolled T2DM who have failed to previous antidiabetic therapies, the add-on of dapagliflozin significantly provides reductions of HbA1c, microalbuminuria and reduces the risk of CKD compared to DPP4i add-on.
ISSN:0012-1797
1939-327X
DOI:10.2337/db23-879-P