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Clinical Trial
. 2025 Aug 5;334(5):409-418.
doi: 10.1001/jama.2025.9413.

Lorundrostat in Participants With Uncontrolled Hypertension and Treatment-Resistant Hypertension: The Launch-HTN Randomized Clinical Trial

Manish Saxena  1 Luke Laffin  2 Claudio Borghi  3 Beatriz Fernandez Fernandez  4 Jalal K Ghali  5 Branko Kopjar  6 Krishna Polu  7 Simon D Roger  8 B T Slingsby  7 Frank Strutz  9 Liffert Vogt  10 Matthew R Weir  11 David Rodman  7 Launch-HTN Investigators
Collaborators, Affiliations
Clinical Trial

Lorundrostat in Participants With Uncontrolled Hypertension and Treatment-Resistant Hypertension: The Launch-HTN Randomized Clinical Trial

Manish Saxena et al. JAMA. .

Abstract

Importance: Uncontrolled hypertension remains a global health concern and dysregulated aldosterone production is a central mechanism. Lorundrostat, a novel aldosterone synthase inhibitor that reduces aldosterone production, demonstrated efficacy in participants with uncontrolled hypertension, including those with treatment-resistant hypertension.

Objective: To evaluate the efficacy and safety of lorundrostat for lowering blood pressure (BP) when added to a prescribed regimen of 2 to 5 antihypertensive medications in adults with uncontrolled hypertension and treatment-resistant hypertension.

Design, setting, and participants: In this phase 3, randomized clinical trial, adults with uncontrolled hypertension, including those with treatment-resistant hypertension, were enrolled between November 2023 and September 2024 at 159 clinic sites across 13 countries. The last date of follow-up was January 24, 2025.

Intervention: Randomization ratio of 1:2:1 to 50 mg/d of lorundrostat for 6 weeks followed by 100 mg/d of lorundrostat for 6 weeks (n = 270) if they met prespecified criteria, 50 mg/d of lorundrostat for 12 weeks (n = 541), or daily placebo for 12 weeks (n = 272). The prespecified criteria included systolic BP of 130 mm Hg or greater, potassium level of 4.8 mmol/L or less, sodium level of 135 mmol/L or greater, an estimated glomerular filtration rate (eGFR) of greater than 45 mL/min/1.73 m2, and less than a 25% reduction in eGFR.

Main outcome and measures: The primary outcome was change in automated office systolic BP at week 6 for participants randomized to 50 mg of lorundrostat vs placebo. Adverse events of special interest included dose reduction, interruption, or discontinuation due to events such as hyperkalemia, hyponatremia, and reduction in kidney function.

Results: Of the 1083 participants, the mean age was 61.6 years (SD, 10.3 years), 508 (46.9%) were female, 311 (28.7%) were Black or African American, 733 (67.7%) were White, and 685 (63.3%) had a body mass index of 30 or greater (obesity). At randomization, 432 participants (39.9%) were taking 2 prescribed antihypertensive medications and 651 (60.1%) were taking 3 or more. For the pooled 50 mg of lorundrostat group (n = 808), the least-squares mean change in automated office systolic BP at week 6 was -16.9 mm Hg (95% CI, -19.0 to -14.9 mm Hg) vs -7.9 mm Hg (95% CI, -11.5 to -4.2 mm Hg) for the placebo group (least-squares mean difference, -9.1 mm Hg [95% CI, -13.3 to -4.9 mm Hg]; P < .001). Hyponatremia, hyperkalemia, and reduction in kidney function were reported more often with lorundrostat vs placebo. In the 50 mg of lorundrostat group with possible escalation to 100 mg, treatment discontinuation occurred in 1 participant (0.37%) due to hyperkalemia, in 1 (0.37%) due to hyponatremia, and in 0 due to reduction in kidney function. In the 50 mg of lorundrostat group, treatment discontinuation occurred in 2 participants (0.37%) due to hyperkalemia, in 2 (0.37%) due to hyponatremia, and in 3 (0.56%) due to reduction in kidney function. Treatment-emergent adverse events occurred in 49.9% of participants (538/1078) and were mostly mild or moderate in severity.

Conclusions and relevance: The efficacy and safety of lorundrostat, an aldosterone synthase inhibitor, was demonstrated for lowering BP in adults with uncontrolled hypertension, including those with treatment-resistant hypertension.

Trial registration: ClinicalTrials.gov Identifier: NCT06153693.

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Conflict of interest statement

Conflict of Interest Disclosures: Dr Saxena reported receiving personal fees from Alnylam, Arrowhead, AstraZeneca, Boehringer Ingelheim, C4 Research, Daiichi Sankyo, Sanofi, IQVIA, Mineralys Therapeutics, the Menarini Group, Novartis, PPD, Recor Medical, and Vifor Pharma; receiving institutional grant support from Ablative Solutions, MSD, Recor Medical, and Applied Therapeutics; and serving on advisory boards for Alnylam, AstraZeneca, Boehringer Ingelheim, Daiichi Sankyo, and the Menarini Group. Dr Laffin reported receiving institutional grant support from Arrowhead, AstraZeneca, and Crispr Therapeutics and receiving personal fees from AstraZeneca, Eli Lilly, Idorsia, LucidAct Health, Medtronic, Novo Nordisk, Recor, Rippler Medical, Stability Health, and Veradermics. Dr Borghi reported receiving personal fees from Servier Pharma, EGIS Pharma, the Menarini Group, and Mineralys Therapeutics. Dr Fernandez Fernandez reported receiving personal fees from Mineralys Therapeutics, AstraZeneca, Novo Nordisk, Boehringer Ingelheim, Lilly, Amgen, the Menarini Group, and Bayer. Dr Kopjar reported receiving personal fees from Mineralys Therapeutics. Dr Polu reported being an employee, being a shareholder, and serving as a clinical advisory board member for Mineralys Therapeutics. Dr Roger reported receiving personal fees from Mineralys Therapeutics. Dr Slingsby reported being an employee, being a shareholder, and serving as a clinical advisory board member for Mineralys Therapeutics. Dr Vogt reported receiving personal fees from Mineralys Therapeutics and Boehringer Ingelheim and receiving grants from CSL Vifor, Bayer, and AstraZeneca. Dr Weir reported receiving personal fees from Mineralys Therapeutics, AstraZeneca, Bayer, Corcept, Novo Nordisk, and CSL Vifor. Dr Rodman reported being an employee of Mineralys Therapeutics. No other disclosures were reported.

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