BHV-8000, a Selective Brain-Penetrant TYK2/JAK1 Inhibitor in Development for Neuroinflammatory and Neurodegenerative Diseases, Demonstrates Favorable PK/PD and Safety Profile in Phase 1 Studies
Lindsey Lee Lair1, Peter Ackerman1, Raj Bhardwaj2, Bavani Shankar1, Bharat Awsare1, Randall Killingsworth1, Eric Ashbrenner1, Jo Ann Malatesta2, Janet Plummer1, Richard Bertz1, Bruce Car1, Irfan Qureshi1, Vlad Coric1
1Biohaven Pharmaceuticals, 2Certara
Objective:

To assess the safety, tolerability, pharmacokinetics and pharmacodynamics of an investigational TYK2/JAK1 inhibitor in healthy adults.

Background:

BHV-8000 is a novel, brain-penetrant, oral small molecule highly selective against the TYK2 and JAK1 enzymes within the JAK-STAT pathway, avoiding the safety liabilities of JAK2/3 inhibition. TYK2 and JAK1 signaling is essential to the mixed inflammatory response driving progression of many neuroinflammatory conditions. BHV-8000 is being explored as a disease-modifying therapy in PD, MS, and AD, and as a preventative strategy against ARIA.

Design/Methods:

BHV8000-101 is a Phase 1 single- and multiple-ascending dose (SAD/MAD) study that explored BHV-8000 between 6 and 30mg for ≤14 days. BHV8000-102 is a Phase 1 study in which BHV-8000 (20mg) was administered daily for 7 days. Across all cohorts, 8 participants were randomized 3:1 to receive blinded BHV-8000 (extended-release formulation) or placebo. Inflammatory biomarkers were measured in the -101 MAD phase and cerebrospinal fluid (CSF)-to-plasma ratio was estimated in the -102 study.


Results:

BHV-8000 geometric mean t1/2 ranged from 11-14 hours. Accumulation at steady state for AUC and Cmax was ~1.7-fold. Mean (CV%) CSF-to-plasma ratio at 6- and 24-hours post-dose was 0.43 (10.1) and 0.50 (13.3), respectively.  

Overall, comparable rates of adverse events (AEs) occurred between participants receiving BHV-8000 and placebo (~20%). All AEs were mild in intensity except one (moderate headache). There were no serious AEs. In the MAD phase, dose-associated lowering of platelets (limited to CTCAE Grade 1) was observed, consistent with JAK1 class effects. There were no adverse trends across other laboratory parameters. Reductions in inflammatory biomarkers (IP-10, hsCRP, and IFN-ß) were numerically greater for BHV-8000 versus placebo.


Conclusions:

In healthy adults, BHV-8000 was generally safe and well-tolerated, while demonstrating anti-inflammatory effects and a favorable PK profile in the periphery and CNS. These results support continued development of BHV-8000 for neurodegenerative conditions, including PD, MS, AD, and ARIA.

10.1212/WNL.0000000000211559
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