Abstract
Background
Volume overload is common and associated with high mortality in patients on peritoneal dialysis (PD). Traditional strategies including diuretics, water/salt restriction, and icodextrin-based solutions cannot always fully correct this condition, necessitating novel alternative strategies. Recent studies confirmed the expression of sodium–glucose cotransporter 2 (SGLT2) in the human peritoneum. Experimental data suggest that SGLT2 inhibitors decrease glucose absorption from the PD solution, thereby increasing the ultrafiltration volume. This trial aims to assess whether SGLT2 inhibitors increase the ultrafiltration volume in patients on PD.
Methods
The EMPOWERED trial (trial registration: jRCTs051230081) is a multicenter, randomized, double-blind, placebo-controlled, crossover trial. Patients with clinically diagnosed chronic heart failure are eligible regardless of the presence of diabetes if they use at least 3 L/day glucose-based PD solutions. Participants will be randomly assigned (1:1) to receive empagliflozin 10 mg once daily and then placebo or vice versa. Each treatment period will last 8 weeks with a 4-week washout period. This study will recruit at least 36 randomized participants. The primary endpoint is the change in the daily ultrafiltration volume from baseline to week 8 in each intervention period. The key secondary endpoints include changes in the biomarkers of drained PD solutions, renal residual function, and anemia-related parameters.
Conclusions
This trial aims to assess the benefit of SGLT2 inhibitors in fluid management with a novel mechanism of action in patients on PD. It will also provide insights into the effects of SGLT2 inhibitors on solute transport across the peritoneal membrane and residual renal function.
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Introduction
Peritoneal dialysis (PD) is an established renal replacement therapy, based on the exchange of water and solute between capillary blood and dialysate fluid across the peritoneal membrane, and 11% of patients undergoing dialysis worldwide are on PD [1]. Given the link between volume overload and poor outcomes, encompassing both technical survival and mortality in patients on PD [2], adequate ultrafiltration, relying on the osmotic gradient typically induced by the hypertonic glucose concentration, is a crucial element for successful PD therapy. Ultrafiltration and the volume status are closely interrelated, and in fact, several studies reported that higher ultrafiltration volume was associated with better prognosis in patients on PD [3, 4]. The glucose gradient peaks at the start of dialysis but diminishes as glucose diffuses into blood. In patients with greater peritoneal vascularity in particular, it is difficult to achieve adequate ultrafiltration because the glucose gradient diminishes more rapidly [5]. One typical strategy in this setting is to use a PD solution with higher glucose content to obtain a higher glucose gradient. However, this strategy might be ineffective because of enhanced fluid intake attributable to hyperglycemia, and it can lead to more rapid damage to the peritoneal membrane, resulting in the discontinuation of PD therapy [6].
Recent studies confirmed the expression of sodium–glucose cotransporter 2 (SGLT2) in the human peritoneum [7,8,9]. Animal studies demonstrated that SGLT2 inhibitors increased ultrafiltration potentially through the maintenance of the glucose gradient upon the inhibition of SGLT2 activity in the peritoneum, although conflicting results exist [7, 9, 10]. In addition, SGLT2 inhibitors were reported to mitigate peritoneal fibrosis and angiogenesis, both of which contribute to ultrafiltration failure, in a mouse model [8, 11]. Based on this information, we hypothesized that SGLT2 inhibitors might increase the ultrafiltration volume and improve long-term prognosis in patients on PD by correcting volume overload and mitigating peritoneal tissue damage. Because there is little information on the use of SGLT2 inhibitors in patients on PD, we decided to first evaluate the effect of SGLT2 inhibitors on the ultrafiltration volume in short-term interventions.
Methods
Study design
The EMPOWERED trial is a multicenter, randomized, double-blind, placebo-controlled, crossover trial evaluating the efficacy and safety of once-daily oral empagliflozin 10 mg in patients on PD. This trial has been registered at the Japan Registry of Clinical Trials (jRCTs051230081). The trial was approved by the Osaka University Clinical Research Review Committee (approval number: S23004), and it is being conducted according to the 1964 Declaration of Helsinki and its later amendments or comparable ethical standards. This trial will be conducted at four academic and community hospitals in Japan (i.e., Osaka University Hospital, National Cerebral and Cardiovascular Center, Osaka General Medical Center, and Matsuyama Red Cross Hospital). Written, informed consent will be obtained from all individual participants included in the study. The trial is being managed by the Academic Clinical Research Center of Osaka University Hospital with the cooperation of intellim Corporation, a Contract Research Organization, which is responsible for monitoring, data management, and statistical analysis. This trial received funds from Nippon Boehringer Ingelheim Co., Ltd. and Eli Lilly Japan K.K. under a research agreement with Osaka University. Boehringer Ingelheim Pharma GmbH & Co. KG is providing drugs for the study. This study was collaboratively designed with input from both academic members and representatives from Nippon Boehringer Ingelheim. Patient enrollment will be started in December 2023, and the scheduled completion date is October 2024.
Study participants
Enrolled participants must meet all inclusion criteria and none of the exclusion criteria listed in Table 1. Key inclusion criteria include an age of 18–90 years, PD vintage ≥ 3 months, use of ≥ 3 L/day glucose-based PD solution, and a diagnosis of and treatment for chronic heart failure. The Japanese Ministry of Health, Labor, and Welfare had approved empagliflozin for the treatment of type 2 diabetes and chronic heart failure at the time of manuscript submission. However, because of a lack of efficacy in the hypoglycemic effect, empagliflozin is not approved for type 2 diabetes in patients on dialysis in Japan. Therefore, inclusion criteria for chronic heart failure were established to conduct the study under the approved indications in Japan. These include elevated N-terminal pro-brain natriuretic peptide (NT-proBNP)/brain natriuretic peptide (BNP) levels, structural heart disease, elevated left ventricular filling pressure, or a history of hospitalization for heart failure. The definitions of structural heart disease and elevated filling pressure are presented in Supplementary Table 1. Key exclusion criteria include treatment with SGLT2 inhibitors within 3 months of enrollment, hybrid therapy with PD and hemodialysis, and peritonitis within 2 months of enrollment. These criteria were selected because rapid ultrafiltration by hemodialysis and peritonitis can alter peritoneal function.
Randomization
The participants will be randomized to the empagliflozin or placebo group at a 1:1 ratio. This allocation will be executed utilizing a computer-generated random sequence and will be stratified by study sites, using a permuted block randomization method. Because the study is double-blinded, patients, their families, the study team, and the sponsor will not have access to the randomization information until the trial database is locked.
Intervention periods
Figure 1 displays a scheme for this trial. The study includes a two-period crossover consisting of 8 weeks of treatment and a 4-week washout between treatment periods. Participants will visit every 4 weeks and continue on trial medication, namely empagliflozin 10 mg or placebo, once daily, in each period. The utilization of SGLT2 inhibitors, excluding empagliflozin, is strictly proscribed, and changes in PD prescriptions are fundamentally prohibited. Adherence to the study drugs will be monitored by interviewing the patients at every visit and counting tablets at the end of each period. Table 2 presents the observation and evaluation schedule during the study period.
Primary endpoint
The primary endpoint of the study is the change in the daily ultrafiltration volume from baseline to week 8 in each intervention period. The ultrafiltration volume from non-glucose-based PD solution (i.e., icodextrin-containing PD solution) will be excluded. The daily ultrafiltration volume will be calculated as the mean of all results for 5 of 7 consecutive days, after excluding the maximum and minimum values. The participants will record data for each session including the type of PD solution, dwell time, and instilled/drained volume of the PD solution.
Secondary endpoints
Secondary outcomes are changes from baseline to week 8 in each intervention period as follows: (1) NT-proBNP and BNP levels; (2) the levels of biomarkers related to frequently and short time peritoneal equilibration test (FAST PET) [12] (ultrafiltration volume, sodium, potassium, glucose, urea nitrogen, creatinine, uric acid, protein, interleukin-6, cancer antigen 125, and drained solution-to-serum creatinine ratio); (3) the levels of biomarkers related to 24-h urine collection (urine volume, sodium, potassium, glucose, urea nitrogen, creatinine, uric acid, urine protein, and urea and creatinine clearance); (4) the levels of anemia-related factors (hemoglobin, hematocrit, ferritin, and transferrin saturation); (5) body weight, blood pressure and, body composition (intracellular and extracellular fluid volume). Details of FAST PET are shown in Supplementary Table 2. Urine kidney injury molecule 1 (KIM-1) levels will be compared at week 8 in each intervention period. Adverse events will be also evaluated during the study period.
Sample size calculation
Our preliminary data revealed an average increase in the daily ultrafiltration volume from the glucose-based PD solution of 90 mL/day in five patients on PD who received 10 mg of empagliflozin and used at least 3 L/day glucose-based PD solution. An increase in the ultrafiltration volume of 90 mL/day is associated with an 18% reduction in the risk of death [4], which appears to be clinically significant. Based on the Osaka University cohort of patients on PD, the between-subject standard deviation (SD) of the change in the ultrafiltration volume was conservatively estimated at 150 mL (actual between-subject SD of the cohort was 114 mL), and the ratio of the between-subject SD to the within-subject SD was 1:1. We calculated that 30 patients completing the study would provide 90% power (at α = 0.05, two-sided) to detect a 90 mL difference in the ultrafiltration volume between empagliflozin and placebo. The sample size was set at 36 subjects to compensate for potential dropouts.
Statistical analysis
Two different analysis sets, namely the full and safety analysis sets (FAS and SAS, respectively), will be used in the study. The FAS will include all study participants who receive at least one dose of the study drug and complete at least one post-baseline examination or assessment. The SAS will include all the study participants who receive at least one dose of the study drug. Analyses of the primary and secondary endpoints excluding adverse events will be conducted in the FAS. Adverse events will be compared between the two groups in the SAS. To assess the effects of empagliflozin versus placebo on the primary outcome, we will use a mixed-effects model for repeated measures (MMRM). The model includes treatment, period, and treatment-by-period interaction as fixed effects and individual as random effects. An unstructured marginal covariance structure will be specified. Secondary endpoints for continuous variables will be estimated in the same manner as described for primary endpoints excluding urine KIM-1. In the case of urinary KIM-1, the analysis using MMRM will be conducted with the absolute value at the end of each period as the dependent variable. Skewed data will be log-transformed before analyses. A list of adverse events will be summarized by tables for each treatment. For sensitivity analyses, we will employ a similar analysis by excluding the data with catheter dysfunction (i.e., drainage volume < 80% of the instilled volume or taking ≥ 20 min to instill the PD solution). A subgroup analysis will be performed using the following factors: age (< 65 years/ ≥ 65 years), sex, presence or absence of diabetes, use of icodextrin-containing PD solution, 24-h urine volume (< 200 mL/ ≥ 200 mL), the glucose load from the peritoneal dialysate (concentration × volume per day, median), the glucose concentration of the drained PD solution on FAST PET (median), and the drained PD solution-to-serum creatinine ratio (median) on FAST PET. Missing data will not be imputed. Statistical analyses will be performed using SAS software (SAS Institute, Cary, NC, USA). Interim analysis will not be conducted.
Discussion
A large amount of evidence supports the use of SGLT2 inhibitors in individuals with heart failure or chronic kidney disease (CKD) [13, 14]. However, few studies have examined treatment with SGLT2 inhibitors in patients with advanced CKD, especially those requiring dialysis. Because SGLT2 is expressed somewhat specifically in renal tubules [15], it is theoretically possible that the effectiveness of SGLT2 inhibitors could diminish as renal function worsens. On the contrary, emerging data indicate that the cardiovascular and kidney benefits of SGLT2 inhibitors do not wane even as the estimated glomerular filtration rate (eGFR) declines at least in patients with eGFR ≥ 20 mL/min/1.73 m2 [16, 17]. Furthermore, in the DAPA-CKD study (trial registration: NCT03036150), in which patients continued taking the study drug after starting renal replacement therapy, dapagliflozin achieved a 21% relative risk reduction in mortality within the subset of patients who commenced dialysis therapy (unpublished data described in the rationale for the RENAL LIFECYCLE Trial [18]). These observations raise the possibility that SGLT2 inhibitors can exert their organ-protective effects through mechanisms distinct from merely blocking SGLT2 in renal tubules.
The current trial was prompted by a report in 2019 that SGLT2 is expressed in the human peritoneum [7]. If SGLT2 plays a role in glucose absorption from the PD solution, SGLT2 inhibitors might enhance the ultrafiltration volume by preserving the glucose gradient across the peritoneum membrane. Although animal studies have yielded inconsistent results [7, 9, 10], recent human case series reported the positive effects of SGLT2 inhibitors on the ultrafiltration volume [19, 20]. Therefore, we planned to conduct a clinical trial evaluating the impact of SGLT2 inhibitors on the ultrafiltration volume. To the best of our knowledge, only two other small randomized, controlled trials (RCT) are currently investigating the effects of SGLT2 inhibitors in patients on PD. One of these trials is an open-label RCT involving 36 patients with type 2 diabetes on PD assessing BNP as the primary endpoint (trial registration: jRCT1011210022). The other trial is a double-blind, placebo-controlled, crossover RCT with 30 patients on PD, and the primary endpoint is glucose absorption from the PD solution (trial registration: NCT05671991). Notably, our trial is particularly unique in that the primary endpoint is the daily ultrafiltration volume, which is an important indicator for patients on PD [3, 4], and the impact on residual renal function will be evaluated. These ongoing RCTs are expected to furnish robust evidence regarding the efficacy and safety of SGLT2 inhibitors in patients on PD.
Conclusion
The EMPOWERED trial will evaluate the efficacy and safety of empagliflozin in patients on PD. The results of this study could reveal the beneficial effect of SGLT2 inhibitors for fluid management in this specific population.
Data availability
Data from this study will be made available upon reasonable request after consultation with the chief investigator and the sponsor.
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Acknowledgements
The authors are grateful to Kento Asano, Shigeru Sakamoto, Makiko Kobayashi, and Hiroko Nomura at the Academic Clinical Research Center of Osaka University Hospital for their support with protocol development and study management.
Funding
Open Access funding provided by Osaka University. This study received research funds from Boehringer Ingelheim by means of providing financial support, study drug and outside scientific medical advisory. BI was not involved in the collection, analysis, and interpretation of any study data. Name and contact information for the trial sponsor: Sponsor: Name: Department of Nephrology, Osaka University Graduate School of Medicine. Address: 2-2-D11, Yamada-oka, Suita, Osaka, Japan. Email address: ydoi@kid.med.osaka-u.ac.jp. Investigational product provider: Name: Boehringer Ingelheim Pharma GmbH & Co. KG. Address: Birkendorfer Strasse 65 88397 Biberach an der Riss, Germany. Email address: wolfram.eisenreich@boehringer-ingelheim.com
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YD is the Chief Investigator; he conceived the study and led the study design, protocol development, grant preparation and application, manuscript preparation, and editing. MS, TA, HO, AM, HK, YN, YN, YU, and FY contributed to the conception of the study design and protocol development. TK, TH, FY, and YI contributed to manuscript preparation and editing. All authors read and approved the final manuscript.
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Employment: Yumi Nakazono, Yoichi Nishiya (Nippon Boehringer Ingelheim Co., Ltd.), Consultancies: Yoshitaka Isaka (Nippon Boehringer Ingelheim Co., Ltd.), Honoraria: Yoshitaka Isaka (Nippon Boehringer Ingelheim Co., Ltd.). Other authors have no conflict of interest to declare.
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Ethical approval to conduct this study has been granted by the Osaka University Clinical Research Review Committee (approved number: S23004). Written, informed consent to participate will be obtained from all participants.
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Doi, Y., Shinzawa, M., Arisato, T. et al. Effects of sodium-glucose co-transporter 2 inhibitors on ultrafiltration in patients with peritoneal dialysis: a protocol for a randomized, double-blind, placebo-controlled, crossover trial (EMPOWERED). Clin Exp Nephrol 28, 629–635 (2024). https://doi.org/10.1007/s10157-024-02467-w
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DOI: https://doi.org/10.1007/s10157-024-02467-w