Hoth Therapeutics' GDNF Shows Superior Liver Fat Reprogramming in Preclinical Study
Event summary
- Hoth Therapeutics reported positive HT-VA study data showing GDNF reprograms liver fat metabolism at the genetic level in a MAFLD model.
- GDNF significantly reduced Srebf1 (fat production gene) and increased Pparα (fat metabolism gene) more effectively than semaglutide.
- Study conducted under CRADA with U.S. Department of Veterans Affairs and Emory University.
- Results position GDNF as potential first-in-class therapy targeting root causes of fatty liver disease and obesity.
The big picture
Hoth's positive GDNF data represents a strategic pivot into high-value metabolic indications beyond its core dermatology and oncology pipeline. The results suggest a potential first-in-class approach to metabolic reprogramming, which could position the company as a competitor to existing weight-loss focused therapies. The metabolic disease market, including MAFLD and obesity, represents a significant expansion opportunity for Hoth's clinical-stage portfolio.
What we're watching
- Clinical Translation
- Whether preclinical gene expression results will translate to clinical efficacy in human MAFLD patients.
- Competitive Positioning
- How Hoth will differentiate GDNF against established GLP-1 agonists in the obesity and metabolic disease market.
- Development Pathway
- The pace at which Hoth advances GDNF through additional preclinical validation and potential clinical trials.