Clinical Takeaway
In this phase 3 trial of 820 adults with chronic low back pain, VER-01, a full-spectrum cannabis extract, was evaluated over a 12-week double-blind treatment period with up to 12 additional months of follow-up. The trial was designed to assess both efficacy and safety compared to placebo, addressing a condition for which current medications provide limited relief and carry meaningful risks. Results from this rigorously structured study contribute directly to the growing clinical evidence base for cannabis-based medicines in managing persistent musculoskeletal pain.
#1 Full-spectrum extract from Cannabis sativa DKJ127 for chronic low back pain: a phase 3 randomized placebo-controlled trial.
Citation: Karst Matthias et al.. Full-spectrum extract from Cannabis sativa DKJ127 for chronic low back pain: a phase 3 randomized placebo-controlled trial.. Nature medicine. 2025. PMID: 41023483.
Design: 5 Journal: 4 N: 2 Recency: 2 Pop: 2 Human: 1 Risk: -2
Quality Gate Alerts:
- Preclinical only
Methodological Considerations:
- Open-label design โ placebo effect not excluded
Abstract: Chronic low back pain (CLBP) affects over half a billion people worldwide. Current pharmacologic treatments offer limited efficacy and carry substantial risks, warranting the development of safe and effective alternatives. This multicenter, randomized, placebo-controlled phase 3 trial evaluated the efficacy and safety of VER-01 in CLBP. It enrolled 820 adults with CLBP (VER-01, nโ=โ394; placebo, nโ=โ426) and included a double-blind 12-week treatment phase (phase A), a 6-month open-label extension (phase B), followed by either a 6-month continuation (phase C) or randomized withdrawal (phase D). The primary endpoint of phase A was a change in mean numeric rating scale (NRS) pain intensity, with a change in total neuropathic pain symptom inventory (NPSI) score as a key secondary endpoint in participants with a neuropathic pain component (PainDETECTโ>โ18). The primary endpoint for phase D was time to treatment failure. The study met its primary endpoint in phase A, with a mean pain reduction of -1.9 NRS points in the VER-01 group (mean difference (MD) versus placeboโ=โ-0.6, 95% confidence interval (CI)โ=โ-0.9 to -0.3; Pโ<โ0.001). Pain further decreased to -2.9 NRS points in phase B, with effects sustained through phase C. The study also met its key secondary endpoint of phase A, with a mean NPSI decrease of -14.4 (standard error, 3.3) points from baseline in the VER-01 arm (MD versus placeboโ=โ-7.3, 95% CIโ=โ-13.2 to -1.3; Pโ=โ0.017). Although phase D did not meet its primary endpoint (hazard ratioโ=โ0.75, 95% CIโ=โ0.44-1.27; Pโ=โ0.288), pain increased significantly more with placebo upon withdrawal (MDโ=โ0.5, 95% CIโ=โ0.0-1.0; Pโ=โ0.034). In phase A, the incidence of adverse events-mostly mild to moderate and transient-was higher with VER-01 than with placebo (83.3% versus 67.3%; Pโ<โ0.001). VER-01 was well-tolerated, with no signs of dependence or withdrawal. VER-01 shows potential as a new, safe and effective treatment for CLBP. ClinicalTrials.gov registration: NCT04
| |