A new clinical trial demonstrates that hepatocyte growth factor plasmid therapy with AMG0001 is a promising, nonsurgical treatment option for accelerating wound healing in patients with moderate chronic limb-threatening ischemia (CLTI). Patients with CLTI have no FDA-approved pharmacologic therapy specifically targeting ulcer healing; therefore, there is a large therapeutic need. The study was published in Circulation: Cardiovascular Interventions by David G. and colleagues.
LEGenD-1 was a randomized, double-blind, placebo-controlled phase II clinical trial conducted at 22 sites in the United States. A total of 75 subjects with neuroischemic ulcers and moderate CLTI were enrolled. Eligibility required toe pressure or TcPO₂ between 30 and 59 mm Hg. Participants were randomized to AMG0001 4 mg, AMG0001 8 mg, or placebo in a 1:1:1 ratio, and received intramuscular injections along a target arterial path at days 0, 28, 56, and 84, guided by angiography. Co-primary endpoints were:
Secondary endpoints included healing at 12 months, ulcer recurrence, and hemodynamic measures.
Results
Baseline characteristics were comparable between the treatment groups: participants had a mean age of 62.6 years, 80.0% were male, and 70.7% had diabetes.
The mean toe pressure was 46.1 mmHg, whereas TcPO₂ averaged 49.8 mmHg, reflecting moderate ischemia.
AMG0001 significantly reduced healing time.
The median time to complete healing was:
84 days for pooled AMG0001 versus 280 days for placebo (P = 0.007)
98 days for the 4 mg dose (P = 0.017)
84 days for the 8 mg dose (P = 0.022)
At 6 months, the healing occurred in:
At 12 months, healing rates increased to:
77.6% vs 46.2%, respectively, for AMG0001 and placebo; P = 0.010
Adverse events were similar across groups, showing an acceptable safety profile.
Anatomically targeted intramuscular administration of the HGF plasmid AMG0001 significantly accelerated healing and improved long-term ulcer outcomes in patients with moderate CLTI and neuroischemic ulcers. In the absence of FDA-approved therapies for ulcer healing in this population, these results establish AMG0001 as a promising nonsurgical therapeutic option. Larger controlled trials will be required to confirm long-term safety, establish efficacy, and justify further development toward regulatory approval.
Reference:
Armstrong DG, Conte MS, Mills JL, Menard MT, Orgill DP, Galiano RD, Kirsner RS, Farber A, Lantis JC, Zelen CM, Carter MJ, Hicks CW, Powell RJ. Anatomically Directed Lower Extremity Gene Therapy for Ulcer Healing: A Double-Blind, Randomized, Placebo-Controlled Study (LEGenD-1). Circ Cardiovasc Interv. 2025 Nov 4:e015648. doi: 10.1161/CIRCINTERVENTIONS.125.015648. Epub ahead of print. PMID: 41186002.
Disclaimer: This website is primarily for healthcare professionals. The content here does not replace medical advice and should not be used as medical, diagnostic, endorsement, treatment, or prescription advice. Medical science evolves rapidly, and we strive to keep our information current. If you find any discrepancies, please contact us at corrections@medicaldialogues.in. Read our Correction Policy here. Nothing here should be used as a substitute for medical advice, diagnosis, or treatment. We do not endorse any healthcare advice that contradicts a physician's guidance. Use of this site is subject to our Terms of Use, Privacy Policy, and Advertisement Policy. For more details, read our Full Disclaimer here.
NOTE: Join us in combating medical misinformation. If you encounter a questionable health, medical, or medical education claim, email us at factcheck@medicaldialogues.in for evaluation.