Aramchol in patients with nonalcoholic steatohepatitis: a randomized, double-blind, placebo-controlled phase 2b trial

Ratziu, V.; de Guevara, L.; Safadi, R.; Poordad, F.; Fuster, F.; Flores-Figueroa, J.; Arrese, M.; Fracanzani, A. L.; Ben Bashat, D.; Lackner, K.; Gorfine, T.; Kadosh, S.; Oren, R.; Halperin, M.; Hayardeny, L.; Loomba, R.; Friedman, S.; Abdelmalek, M.; Angelico, F.; Angelico, M.; Arancibia, J. P.; Bardou-Jacquet, E.; Barrera, F.; Barish, C. F.; Baruch, Y.; Ben-Ari, Z.; Berg, T.; Bourliere, M.; Boursier, J.; Broide, E.; Carmiel, M.; Denham, D. S.; Di Cesare, L.; Dumitrascu, D. L.; Francis, A.; Gawrieh, S.; González- Huezo, M. S.; Hillon, P.; Iracheta, A.; Kayali, Z.; Kupcinskas, L.; Lau, G.; Serfaty, L.; Le Cleach, A.; Loguercio, C.; Manns, M.; Martinez Saldivar, B. I.; Mena, E. A.; Morales Garza, L. A.; Neutel, J. M.; Nikoleishvili, L.; Noureddin, M.; Pais, R.; Paredes, A. H.; Paredes, M.; Peters Watkins, R.; Picardi, A.; Pirisi, M.; Jofre, G. P.; Preotescu, L.; Saadi, T.; Samuel, D.; Sánchez Avila, J. F.; Schiefke, I.; Shibolet, O.; Siddiqui, M. S.; Torres-Mendoza, G.; Trotter, J. F.; Tsai, E.; Verna, E. C.; Zuckerman, E.; Zur, D.; Sanyal, A. J.

doi:10.1038/s41591-021-01495-3

Y Nonalcoholic steatohepatitis (NASH), a chronic liver disease without an approved therapy, is associated with lipotoxicity and insulin resistance and is a major cause of cirrhosis and hepatocellular carcinoma. Aramchol, a partial inhibitor of hepatic stearoyl-CoA desaturase (SCD1) improved steatohepatitis and fibrosis in rodents and reduced steatosis in an early clinical trial. ARREST, a 52-week, double-blind, placebo-controlled, phase 2b trial randomized 247 patients with NASH (n = 101, n = 98 and n = 48 in the Aramchol 400 mg, 600 mg and placebo arms, respectively; NCT02279524). The primary end point was a decrease in hepatic triglycerides by magnetic resonance spectroscopy at 52 weeks with a dose of 600 mg of Aramchol. Key secondary end points included liver histology and alanine aminotransferase (ALT). Aramchol 600 mg produced a placebo-corrected decrease in liver triglycerides without meeting the prespecified significance (-3.1, 95% confidence interval (CI) -6.4 to 0.2, P = 0.066), precluding further formal statistical analysis. NASH resolution without worsening fibrosis was achieved in 16.7% (13 out of 78) of Aramchol 600 mg versus 5% (2 out of 40) of the placebo arm (odds ratio (OR) = 4.74, 95% CI = 0.99 to 22.7) and fibrosis improvement by >= 1 stage without worsening NASH in 29.5% versus 17.5% (OR = 1.88, 95% CI = 0.7 to 5.0), respectively. The placebo-corrected decrease in ALT for 600 mg was -29.1 IU l(-1) (95% CI = -41.6 to -16.5). Early termination due to adverse events (AEs) was <5%, and Aramchol 600 and 400 mg were safe, well tolerated and without imbalance in serious or severe AEs between arms. Although the primary end point of a reduction in liver fat did not meet the prespecified significance level with Aramchol 600 mg, the observed safety and changes in liver histology and enzymes provide a rationale for SCD1 modulation as a promising therapy for NASH and fibrosis and are being evaluated in an ongoing phase 3 program.