Selective GPR84 Antagonist

GPR84 is a pro-inflammatory target primarily expressed on cells associated with the immune system and its expression levels increase significantly during periods of inflammatory stress. Inhibition of GPR84 can inhibit neutrophil and macrophage migration and reduce cytokine release.

We believe that the GPR84 receptor could be an important biological target in metabolic disease. Our clinical and preclinical research, combined with published work from other groups, indicates a potential role for antagonism of GPR84 in metabolic diseases, including MASH.

Our lead compound is CBI-6511 is a selective, high-potency, small molecule antagonist of the medium-chain fatty acid receptor GPR84. CBI-6511 has a differentiated but complimentary mechanism of action compared to standard of care therapies.

In pre-clinical experiments, GPR84 antagonists are active in high fat diet models of MASH/MAFLD with significant reductions in LDL-c and liver steatosis. 

CBI-6511 has completed a Phase 1 SAD/MAD clinical study in healthy volunteers and was found to be generally safe and well-tolerated with pharmacokinetics suitable for once or twice daily oral dosing.  

We have also completed a 28-day dose-range finding Phase 1b/2a clinical trial in healthy volunteers with high Body Mass Index (“BMI”) to evaluate the effect of CBI-6511 on serum lipids and to evaluate the effect of CBI-6511 taken in combination with a statin. 

We are now planning to commence a 12-week Phase IIa study in MASH in early 2027.