SGLT2-inhibition in patients with Alport syndrome /

Jan Boeckhaus; Daniel P Gale; James Simon; Jie Ding; Yanqin Zhang; Carsten Bergmann; A. Neil Turner; Matthew Hall; John A Sayer; Shalabh Srivastava; Hee Gyung Kang; Agnė Čerkauskaitė-Kerpauskienė; Valentine Gillion; Kathleen J Claes; Bastian Krueger; Jonathan de Fallois; Ulrike Walden; Mira Choi; Markus Schueler; Roman-Ulrich Mueller; Polina Todorova; Bernd Hohenstein; Michael Zeisberg; Tim Friede; Bertrand Knebelmann; Jan Halbritter; Oliver Gross

doi:10.1016/j.ekir.2024.09.014

Title	SGLT2-inhibition in patients with Alport syndrome /
Authors	Boeckhaus, Jan ; Gale, Daniel P ; Simon, James ; Ding, Jie ; Zhang, Yanqin ; Bergmann, Carsten ; Turner, A. Neil ; Hall, Matthew ; Sayer, John A ; Srivastava, Shalabh ; Kang, Hee Gyung ; Čerkauskaitė-Kerpauskienė, Agnė ; Gillion, Valentine ; Claes, Kathleen J ; Krueger, Bastian ; de Fallois, Jonathan ; Walden, Ulrike ; Choi, Mira ; Schueler, Markus ; Mueller, Roman-Ulrich ; Todorova, Polina ; Hohenstein, Bernd ; Zeisberg, Michael ; Friede, Tim ; Knebelmann, Bertrand ; Halbritter, Jan ; Gross, Oliver
DOI	10.1016/j.ekir.2024.09.014
Full Text
Is Part of	Kidney international reports.. New York : Elsevier Inc.. 2024, vol. 9, iss. 12, p. 3490-3500.. ISSN 2468-0249
Keywords [eng]	albuminuria ; Alport syndrome ; COL4 ; dapagliflozin ; empagliflozin ; kidney failure
Abstract [eng]	Introduction: Large-scale trials showed positive outcomes of sodium-glucose cotransporter-2 inhibitors (SGLT2i) in adults with chronic kidney disease (CKD). Whether the use of SGLT2i is safe and effective in patients with the common hereditary CKD Alport syndrome (AS) has not yet been investigated specifically in larger cohorts. Methods: This observational, multicenter, international study (NCT02378805) assessed 112 patients with AS after start of SGLT2i. The study's primary end point was change of albuminuria in albumin/g creatinine from the start of therapy. Results: Compared to randomized trials investigating the effect of SGLT2i in CKD, the adult patients in this study were younger (aged 38 ± 14 years) and had a better estimated glomerular filtration rate (eGFR, 63 ± 35 ml/min per 1.73 m2; n = 98). Maximum follow-up was 32 months. Compared to baseline, at the first 3 follow-up visits (months 1 to 3, 4 to 8, and 9 to 15) after initiation of SGLT2i therapy, a significant reduction of albuminuria in mg albumin/g creatinine (>30%) was observed. Mean loss of eGFR was 9 ± 12 ml/min per 1.73 m2 almost 1 year after initiation of SGLT2i therapy (n = 35). At a total of 71 patient-years at risk, 0.24 adverse events (AEs) per patient-year on SGLT2i were reported. Conclusion: This study indicates that, additive to renin-angiotensin system (RAS)-inhibition (RASi), SGLT2i have the potential to reduce the amount of albuminuria in patients with AS. Future studies are needed to investigate the long-term effects of SGLT2i on CKD progression in patients with AS to assess whether the observed reduction in albuminuria translates to a delay in kidney failure (KF).
Published	New York : Elsevier Inc
Type	Journal article
Language	English
Publication date	2024
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„SGLT2-inhibition in patients with Alport syndrome /“