ERTU-SODIUM: Study on the Effects of Ertugliflozin on Sodium Storage, Interstitial Volume, and Plasma Volume in HFrEF

Phase 4

Recruiting

• Conditions: Congestion; Heart Failure With Reduced Ejection Fraction
• Interventions: Drug: Ertugliflozin; Drug: Placebo

• Registration Number: NCT05152940
• Lead Sponsor: Icahn School of Medicine at Mount Sinai

Brief Summary

The overall hypothesis is that treatment with the SGLT2 inhibitor Ertugliflozin induces a differential regulation in interstitial fluid vs plasma volume, with more reduction of the volume from the interstitial fluid than from the circulating plasma volume, which results in Ertugliflozin inducing more potent congestion relief with minimal impact on blood volume and organ perfusion. Ertugliflozin reduces the levels of sodium and water from the skin and the interstitial tissue (which improves tissue congestion).

Detailed Description

The glucosaminoglycan (GAG) network in the subcutaneous interstitium can non-osmotically bind large amounts of sodium. Therefore, the GAG network creates a hypertonic sodium concentration without fluid accumulation. This means that the subcutaneous GAG act as a third compartment that is able to non-osmotically store sodium without inducing congestion, thus serving as buffer in the case of sodium overload.

The researchers hypothesize that the SGLT2 inhibitor Ertugliflozin enhances the functionality of the subcutaneous GAG network. The hypothesis is that Ertugliflozin-induced GAG functionality induces more potent congestion relief (reduction in sodium and water content in the interstitial tissue) with minimal impact on blood volume and organ perfusion.

The research team will perform a randomized clinical trial with a cross-over design. Patients with heart failure with reduced ejection fraction (HFrEF) will be randomized to the SGLT2 inhibitor Ertuglifozin or to placebo. Skin punch biopsy will be performed before treatment and after treatment (one month) to evaluate skin content of water and sodium. At each time point, an oral salt challenge will be performed to investigate the functionality of the GAG network, and whether Ertugliflozin mitigates the degree of tissue and vascular congestion after this oral salt challenge as compared with placebo.

The overall hypothesis is that treatment with the SGLT2 inhibitor Ertugliflozin induces a differential regulation in interstitial fluid vs plasma volume, with more reduction of the volume from the interstitial fluid than from the circulating plasma volume, which results in Ertugliflozin inducing more potent congestion relief with minimal impact on blood volume and organ perfusion. Ertugliflozin reduces the levels of sodium and water from the skin and the interstitial tissue (which improves tissue congestion). This overarching hypothesis causes:

1. in the baseline situation, chronic treatment with Ertugliflozin:

1.1. will reduce skin/tissue congestion as demonstrated by lower skin water content and lower volume of interstitial-extracellular fluid

1.2. will reduce skin sodium content due to a mobilization of sodium from the subcutaneous glucosaminoglycan (GAG) network

1.3. will create a differential regulation of interstitial vs plasmatic volume, with ertugliflozin decreasing tissue congestion (B-lines and dielectric resistance in lungs) better than placebo

1.4. will only cause a mild reduction in plasma volume with no neurohormonal activation

1.5. will ameliorate GAG structure: higher GAG levels, higher sulfated (functional) GAG, less expression of enzymes degrading GAG, less GAG degradation products in plasma

2. after an oral salt challenge (sodium overload), previous chronic treatment with Ertugliflozin:

2.1. will improve the sodium buffering capacity of the skin GAG network, meaning ertugliflozin will enhance non-osmotic sodium storage in the skin without causing tissue congestion (edema) or vascular congestion (increase in plasma volume and filling pressures).

2.2. will reduce skin/tissue congestion (as mentioned in 2.1): lower skin water content and interstitial-extracellular fluid volume

2.3. will not cause vascular congestion, will not raise plasma volume or LV filling pressures

In summary, Ertugliflozin will protect HFrEF patients from acute decompensations induced by dietary transgressions by enhancing the skin sodium buffering capacity

Study Timeline

• Study First Submitted: 2021-11-29
• Study First Submitted QC: 2021-11-29
• Study First Posted: 2021-12-10
• Study Start: 2023-03-20
• Status Verified: 2023-10
• Last Update Submitted: 2023-10-11
• Last Update Posted: 2023-10-13
• Primary Completion: 2024-12
• Study Completion: 2024-12

Recruitment & Eligibility

• Status: RECRUITING
• Sex: All
• Target Recruitment: 28

Inclusion Criteria

Not provided

Exclusion Criteria

Not provided

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: CROSSOVER

Arm && Interventions

Group	Intervention	Description
Placebo	Placebo	Treatment with matching placebo for one month, washout period for one month, and then Ertugliflozin for one month
Ertugliflozin then Placebo	Placebo	Treatment with Ertugliflozin for one month, washout period for one month, and then with Placebo for one month
Ertugliflozin then Placebo	Ertugliflozin	Treatment with Ertugliflozin for one month, washout period for one month, and then with Placebo for one month
Placebo	Ertugliflozin	Treatment with matching placebo for one month, washout period for one month, and then Ertugliflozin for one month

Primary Outcome Measures

Name	Time	Method
Change in the skin water content	Baseline and One month	Skin water content is measured as total (wet) weight - dry weight, determined after desiccation at 90°C for 24 hours to stable weight

Secondary Outcome Measures

Name	Time	Method
Change in skin sodium content	Baseline and One month	Skin sodium content will be measured by flame spectrophotometry after dry ashing
Change in the number of pulmonary Kerley's B-lines	Baseline and One month	The number of pulmonary Kerley's B-lines (aka "comets") to measure tissue congestion and will be quantified using lung ultrasound
Change in vascular congestion	Baseline and One month	Vascular congestion will be evaluated using VExUS (Volume Evaluation by UltraSound)
Change in plasma concentrations of catecholamines	Baseline and One month	Neurohormonal activation to measure vascular congestion and will be evaluated using plasma concentrations of catecholamines.
Change in interstitial Fluid	Baseline and One month	Interstitial Fluid to measure tissue congestion and will be calculated as Extracellular Volume minus Plasma Volume
Change in left ventricular filling pressures	Baseline and One month	Left ventricular filling pressures to measure vascular and will be evaluated using the echocardiographic parameter E/e' (surrogate of LV filling pressures)
Change in pulmonary fluid	Baseline and One month	Pulmonary fluid content to measure tissue congestion and is quantified using remote dielectric sensing with ReDS Vest
Change in the plasma volume	Baseline and One month	Plasma volume to measure vascular congestion.
Change in plasma concentrations of aldosterone	Baseline and One month	Neurohormonal activation to measure vascular congestion and will be evaluated using plasma concentrations of aldosterone.
Change in plasma concentrations of plasma renin activity	Baseline and One month	Neurohormonal activation to measure vascular congestion and will be evaluated using plasma concentrations of plasma renin activity

Trial Locations

Locations (1)

Icahn School of Medicine at Mount Sinai; 🇺🇸 New York, New York, United States