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Clinical Trial
. 2019 May;176(9):1251-1267.
doi: 10.1111/bph.14621. Epub 2019 Mar 31.

Neprilysin inhibition for pulmonary arterial hypertension: a randomized, double-blind, placebo-controlled, proof-of-concept trial

Adrian J Hobbs  1 Amie J Moyes  1 Reshma S Baliga  1 Dipa Ghedia  2 Rachel Ochiel  2 Yvonne Sylvestre  3 Caroline J Doré  3 Kashfia Chowdhury  3 Kate Maclagan  3 Harriet L Quartly  3 Reecha Sofat  4 Angelique Smit  2 Benjamin E Schreiber  2 Gerry J Coghlan  2 Raymond J MacAllister  5
Affiliations
Clinical Trial

Neprilysin inhibition for pulmonary arterial hypertension: a randomized, double-blind, placebo-controlled, proof-of-concept trial

Adrian J Hobbs et al. Br J Pharmacol. 2019 May.

Abstract

Background and purpose: Pulmonary arterial hypertension (PAH) is an incurable, incapacitating disorder resulting from increased pulmonary vascular resistance, pulmonary arterial remodelling, and right ventricular failure. In preclinical models, the combination of a PDE5 inhibitor (PDE5i) with a neprilysin inhibitor augments natriuretic peptide bioactivity, promotes cGMP signalling, and reverses the structural and haemodynamic deficits that characterize PAH. Herein, we conducted a randomized, double-blind, placebo-controlled trial to assess the efficacy and safety of repurposing the neprilysin inhibitor, racecadotril, in PAH.

Experimental approach: Twenty-one PAH patients stable on PDE5i therapy were recruited. Acute haemodynamic and biochemical changes following a single dose of racecadotril or matching placebo were determined; this was followed by a 14-day safety and efficacy evaluation. The primary endpoint in both steps was the maximum change in circulating atrial natriuretic peptide (ANP) concentration (Δmax ), with secondary outcomes including pulmonary and systemic haemodynamics plus mechanistic biomarkers.

Key results: Acute administration of racecadotril (100 mg) resulted in a 79% increase in the plasma ANP concentration and a 106% increase in plasma cGMP levels, with a concomitant 14% fall in pulmonary vascular resistance. Racecadotril (100 mg; t.i.d.) treatment for 14 days resulted in a 19% rise in plasma ANP concentration. Neither acute nor chronic administration of racecadotril resulted in a significant drop in mean arterial BP or any serious adverse effects.

Conclusions and implications: This Phase IIa evaluation provides proof-of-principle evidence that neprilysin inhibitors may have therapeutic utility in PAH and warrants a larger scale prospective trial.

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Conflict of interest statement

B.S. has been a consultant/advisory board member for GSK & Actelion. J.C. has been a consultant/advisory board member for Actelion, GSK, Bayer, United Therapeutics, Endotronic, and Pfizer. A.H. has been a consultant/advisory board member for Bayer AG, Serodus ASA, and Palatin Technologies Inc.

Figures

Figure 1
Figure 1
CONSORT flow chart for Step 1 (left panel) and Step 2 (right panel)
Figure 2
Figure 2
Time course (left panel), absolute change (middle panels), and maximum percentage change from baseline (right panel) in plasma atrial natriuretic peptide concentration ([ANP]); (a) or cGMP concentration; (b) in PAH patients receiving racecadotril (100 mg) or matching placebo. Data are represented as geometric mean ± 95% CI. n = 4 (placebo) and n = 9 (racecadotril). Data were analysed by paired t test for absolute intrapatient change (i.e., before and after treatment) and by unpaired t test for intergroup comparison (i.e., placebo vs. racecadotril) of Δmax (%). Correlation between maximum percentage change in PVR and maximum percentage change in plasma [ANP] or plasma [cGMP] (c). n = 4 (placebo) and n = 8 (racecadotril). Data were analysed by Pearson correlation. In all cases, P < 0.05 was considered statistically significant
Figure 3
Figure 3
Time course (left panel), absolute change (middle panels), and maximum percentage change from baseline (right panel) in pulmonary vascular resistance (PVR; (a) or pulmonary capillary wedge pressure (PCWP); (b) in PAH patients receiving racecadotril (100 mg) or matching placebo. Data are presented as geometric mean ± 95% CI. n = 4 (placebo) and n = 8 (racecadotril). Data were analysed by paired t test for absolute intrapatient change (i.e., before and after treatment) and by unpaired t test for intergroup comparison (i.e., placebo vs. racecadotril) of Δmax (%). P < 0.05 was considered statistically significant
Figure 4
Figure 4
Time course (left panel), absolute change (middle panels), and maximum percentage change from baseline (right panel) in mean pulmonary artery pressure (mPAP; (a) or mean arterial BP (MABP); (b) in PAH patients receiving racecadotril (100 mg) or matching placebo. Data are presented as geometric mean ± 95% CI. n = 4 (placebo) and n = 9 (racecadotril). Data were analysed by paired t test for absolute intrapatient change (i.e., before and after treatment) and by unpaired t test for intergroup comparison (i.e., placebo vs. racecadotril) of Δmax (%). P < 0.05 was considered statistically significant
Figure 5
Figure 5
Time course (left panel), absolute change (middle panels), and maximum percentage change from baseline (right panel) in plasma endothelin‐1 concentration ([ET‐1]; (a) or N‐terminal‐pro‐brain natriuretic peptide concentration [NT‐proBNP]; (b) in PAH patients receiving racecadotril (100 mg) or matching placebo. Data are presented as geometric mean ± 95% CI. n = 4 (placebo) and n = 9 (racecadotril). Data were analysed by paired t test for absolute intrapatient change (i.e., before and after treatment) and by unpaired t test for intergroup comparison (i.e., placebo vs. racecadotril) of Δmax (%). P < 0.05 was considered statistically significant
Figure 6
Figure 6
Absolute change (left and middle panels) and maximum percentage change from baseline (right panel) in mean arterial BP (MABP); (a) or plasma atrial natriuretic peptide concentration [ANP]; (b) in PAH patients receiving racecadotril (100 mg; t.i.d.; 14 days) or matching placebo. Data are presented as geometric mean ± 95% CI. n = 3 (placebo) and n = 5 (racecadotril). Data were analysed by paired t test for absolute intrapatient change (i.e., before and after treatment) and by unpaired t test for intergroup comparison (i.e., placebo vs. racecadotril) of Δmax (%). P < 0.05 was considered statistically significant
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