Efficacy and Safety of Subcutaneous Elegrobart in Active Thyroid Eye Disease: Topline Results from the Phase 3 REVEAL-1 Trial
Background and Clinical Context
Thyroid eye disease (TED), frequently associated with Gravesโ disease, is a progressive, debilitating autoimmune condition characterized by the activation of orbital fibroblasts. This activation leads to inflammation, expansion of extraocular muscles, and accumulation of hyaluronan within the orbital space. Clinically, this manifests as proptosis (ocular bulging), severe diplopia (double vision), periorbital edema, and in severe cases, compressive optic neuropathy.
Historically, the management of moderate-to-severe TED relied heavily on systemic corticosteroids and orbital radiotherapy, both of which possess significant adverse effect profiles and limited disease-modifying efficacy. The advent of targeted biologic therapies, specifically insulin-like growth factor 1 receptor (IGF-1R) inhibitors, has revolutionized TED management. However, existing therapies often require frequent, prolonged intravenous (IV) infusions, presenting a significant logistical burden for patients and healthcare systems.
Elegrobart (Viridian Therapeutics) represents a novel therapeutic approach. It is a half-life extended monoclonal antibody engineered to antagonize the IGF-1R, formulated specifically for subcutaneous administration. The phase 3 REVEAL-1 trial evaluated the efficacy and safety of this agent in patients with active TED, aiming to establish a more accessible, lower-burden treatment paradigm.
Study Design and Patient Population
The REVEAL-1 trial was a randomized, double-blind, placebo-controlled phase 3 investigation enrolling 132 adult patients diagnosed with active thyroid eye disease. Participants were randomized into one of three distinct study arms for a 24-week observation period:
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Elegrobart Q4W: Subcutaneous administration every 4 weeks.
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Elegrobart Q8W: Subcutaneous administration every 8 weeks.
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Placebo: Matched subcutaneous placebo injections.
The primary efficacy endpoint was the proptosis response rate at 24 weeks, conventionally defined as a reduction of at least 2 millimeters (mm) in proptosis from baseline in the study eye, without a corresponding $\ge$2 mm increase in the fellow eye.
Efficacy Outcomes: Proptosis and Diplopia
Topline results demonstrated robust, statistically significant reductions in proptosis and visual impairment across both active treatment arms compared to placebo.
Table 1. Proptosis Response and Mean Reduction at 24 Weeks
| Clinical Endpoint | Elegrobart Q4W | Elegrobart Q8W | Placebo | P Value (vs. Placebo) |
| Proptosis Response Rate (%) | 54% | 63% | 18% | < .0001 (for both arms) |
| Mean Proptosis Reduction (mm) | โ2.33 mm | โ2.50 mm | โ0.81 mm | < .0001 (for both arms) |
Note: Proptosis measurements were rigorously confirmed utilizing both standardized exophthalmometry and orbital magnetic resonance imaging (MRI).
Improvements in extraocular muscle function and subsequent reduction in diplopia were similarly pronounced, particularly in the highly frequent dosing cohort.
Table 2. Diplopia Outcomes at 24 Weeks
| Clinical Endpoint | Elegrobart Q4W | Elegrobart Q8W | Placebo | P Value (vs. Placebo) |
| Any Reduction in Diplopia (%) | 71% | 54% | 32% | Not specified in source |
| Complete Resolution of Diplopia (%) | 51% | Not significantly different | 16% | .0013 (Q4W only) |
Safety Profile and Tolerability
The safety profile of elegrobart was consistent with the established class effects of IGF-1R antagonism. The drug was generally well tolerated across both subcutaneous dosing regimens. A notable adverse event of interest for this pharmacological class is hearing impairment.
Table 3. Placebo-Adjusted Hearing Impairment Rates
| Adverse Event | Elegrobart Q4W (Placebo-Adjusted) | Elegrobart Q8W (Placebo-Adjusted) |
| Overall Hearing Impairment | 11.3% | 2.3% |
| Clinical Presentation | Exclusively attributed to tinnitus; zero reports of audiometric hearing loss. | Exclusively attributed to tinnitus; zero reports of audiometric hearing loss. |
Clinical Implications and Expert Perspectives
The REVEAL-1 data establish subcutaneous elegrobart as a highly efficacious, disease-modifying therapy for active TED, successfully matching the historical benchmarks of IV-administered biologics while offering a vastly superior patient experience.
Prem Subramanian, MD, PhD, professor of ophthalmology at the University of Colorado Anschutz School of Medicine and chief of neuro-ophthalmology at the Sue Anschutz-Rodgers Eye Center, provided essential clinical context regarding these findings:
โSubcutaneous elegrobart showed rapid and clinically meaningful reductions in proptosis and diplopia in REVEAL-1 with a highly convenient, well-tolerated dosing profile. Patients are seeking more treatment choices for thyroid eye disease, and there remains a clear need for a more conveniently administered therapy. I am very encouraged to see the data for elegrobart and believe it has the potential to reach more thyroid eye disease patients than an intravenous therapy and to provide them with an attractive treatment option.โ
Future Directions
The clinical development pipeline for elegrobart continues to expand. Viridian Therapeutics has announced that topline data from the parallel REVEAL-2 trialโwhich evaluates the agent in patients with chronic (inactive) thyroid eye diseaseโare anticipated in the second quarter of 2026. Based on these cumulative data, a Biologics License Application (BLA) submission to the FDA is planned for the first quarter of 2027.
REVEAL-1 Trial Data Explorer
Efficacy & Safety of Elegrobart in Active Thyroid Eye Disease (Week 24)
