Back/Gyre Therapeutics Explores VMAT2 Insights Amid Neurocrine's INGREZZA Breakthrough in Neuropsychiatric Treatments
pharma·January 18, 2026·gyre

Gyre Therapeutics Explores VMAT2 Insights Amid Neurocrine's INGREZZA Breakthrough in Neuropsychiatric Treatments

ED
Editorial
Cashu Markets·2 min read
TL;DR
  • Neurocrine Biosciences' INGREZZA achieves nearly double VMAT2 occupancy compared to AUSTEDO XR, enhancing treatment efficacy.
  • Elevated VMAT2 occupancy with INGREZZA may improve clinical outcomes for movement disorders like tardive dyskinesia.
  • The study underscores pharmacological differences in VMAT2 inhibitors, potentially transforming treatment strategies for hyperkinetic movement disorders.

Neurocrine Biosciences Reveals Key Insights on VMAT2 Target Occupancy in Neuropsychiatric Treatments

Recent findings from Neurocrine Biosciences, Inc. spotlight the importance of VMAT2 target occupancy in the treatment of hyperkinetic movement disorders. At the American College of Neuropsychopharmacology’s 64th Annual Meeting, the company presents a comparative study of its drug INGREZZA® (valbenazine) and AUSTEDO XR (deutetrabenazine). The results reveal that INGREZZA achieves nearly double the VMAT2 occupancy compared to AUSTEDO XR, with estimates showing approximately 76.5% versus 38.3% at therapeutic doses. This pivotal data is crucial for understanding the efficacy of these medications in treating disorders such as tardive dyskinesia and Huntington's disease chorea.

The methodology employed in this study involves positron emission tomography (PET) imaging to assess VMAT2 target occupancy following the administration of single doses of either INGREZZA or AUSTEDO XR. Eight participants received doses of 40 mg or 80 mg of INGREZZA, and 24 mg or 48 mg of AUSTEDO XR. The findings suggest that the heightened VMAT2 occupancy associated with INGREZZA may correlate with its proven clinical efficacy documented in various trials. Dr. Sanjay Keswani, Chief Medical Officer at Neurocrine Biosciences, emphasizes that these results underline the pharmacological distinctions between VMAT2 inhibitors, bolstering the potential benefits of INGREZZA in achieving sustained clinical outcomes.

The implications of these findings extend beyond mere statistics; they signal a shift in how treatment strategies for hyperkinetic movement disorders may be developed. The superior potency of INGREZZA in engaging VMAT2 presents a promising avenue for enhancing patient care. By effectively mitigating excessive dopamine transmission—known to cause involuntary movements—INGREZZA positions itself as a potentially more effective treatment alternative in the neuropsychiatric landscape.

In related developments, the recent presentation at the conference highlights a growing interest in the pharmacological mechanisms underlying movement disorders. As researchers and clinicians alike focus on the nuanced differences between therapeutic agents, the insights gained from this study may catalyze further investigation into optimizing treatment protocols. The findings contribute to a broader understanding of VMAT2's role in drug efficacy and patient outcomes, ultimately leading to improved management strategies for those affected by these challenging conditions.

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