Regulus Therapeutics (RGLS) Study Update summary
Event summary combining transcript, slides, and related documents.
Study Update summary
3 Feb, 2026Study design and objectives
Phase 1b multiple ascending-dose, double-blind, placebo-controlled trial of RGLS8429 in adults with ADPKD, evaluating three weight-based cohorts (1, 2, 3 mg/kg) and a fourth fixed-dose cohort (300 mg) underway.
Primary objectives: safety, tolerability, pharmacokinetics, and mechanistic activity via urinary polycystin; exploratory endpoints include kidney volume changes by MRI and novel imaging markers.
Patients enrolled had moderate to severe disease, with inclusion based on Mayo Imaging Classification, reduced eGFR (30–90 mL/min), and large kidney volumes.
Each cohort received seven subcutaneous doses over 12 weeks, with biomarker and imaging follow-up; third cohort received 3 mg/kg every two weeks.
The study is designed to support dose selection and design for pivotal Phase 2/3 trials targeting accelerated approval.
Key results and findings
RGLS8429 at 3 mg/kg was well tolerated, with no serious safety concerns; most adverse events were mild injection site reactions.
Statistically significant, dose-dependent increases in urinary polycystin (PC1 and PC2) observed at 3 mg/kg compared to placebo, with the most consistent response at this dose.
70% of patients at 3 mg/kg showed reductions in height-adjusted total kidney volume (htTKV) after three months, with reductions ranging from 2.5% to 6%.
Exploratory analyses suggest a correlation between increased polycystin and reductions in kidney and cyst volume, as well as potential improvements in eGFR.
No significant changes in eGFR were observed over the short treatment period, as expected.
Mechanism of action and disease context
RGLS8429 is an antisense oligonucleotide targeting miR-17, a microRNA upregulated in ADPKD that represses polycystin production and disrupts gene networks.
Blocking miR-17 restores gene expression balance, increases polycystin, and reduces cystogenesis in preclinical models.
ADPKD is a severe, hereditary kidney disease with high unmet need; current therapy (tolvaptan) slows but does not halt disease progression and has safety limitations.
RGLS8429 is a next-generation oligonucleotide designed to preferentially target the kidney and has shown favorable safety and PK in prior studies.
The mechanism is expected to be effective across genotypes due to miR-17's central role in disease biology.
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