Clinical Trial to Assess the Safety and Tolerability of Anti-IL 23 Monoclonal Antibody Guselkumab in Patients With Alcohol-Associated Liver Disease
link https://doi.org/10.1111/apt.70026account_box Díaz Piga, Luis Antonioaccount_box Morris, Sheldonaccount_box Dave, Shravanaccount_box Kim, Susy M.account_box Sarik, Wathnitaaccount_box Richards, Lisaaccount_box Madamba, Egbertaccount_box Bettencourt, Rickiaccount_box Fulinara, Christianaccount_box Pham, Thuyaccount_box Miller, Grantaccount_box Carvalho-Gontijo Weber, Raquelaccount_box Momper, Jeremiah D.account_box He, Fengaccount_box Jain, Soniaaccount_box Jamieson, Catrionaaccount_box Kisseleva, Tatianaaccount_box Brenner, Davidaccount_box Loomba, Rohit
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BackgroundThere are no FDA-approved therapies for alcohol-associated liver disease (ALD). Preclinical studies indicate that blocking IL-23/IL-17 signalling may reverse liver injury. Guselkumab, an IL-23-specific antibody approved for psoriasis, may be beneficial for ALD. AimsWe aimed to assess the safety and tolerability of guselkumab in patients with ALD. MethodsThis phase-1 dose-escalation study included patients with >= 2 DSM-5 criteria for alcohol use disorder, significant steatosis (MRI-PDFF >= 8%) and MRE < 3.63 kPa (to exclude advanced disease). Guselkumab was given subcutaneously on Days 1 and 29 in 30, 70 or 100 mg dose cohorts. Primary endpoints were adverse events (AEs) and dose-limiting toxicity. ResultsWe enrolled 13 patients (three 30 mg, three 70 mg, and seven 100 mg). Eleven completed the study and two early discontinued in the 100 mg group. Of them, 77% were men, and the median age was 53 [IQR 49-61] years. The median MRI-PDFF and MRE were 18.4% [IQR 8.4%-34.0%] and 2.5 [2.2-2.6] kPa, respectively. The most frequent AEs were hyperuricemia (13%, mild only) and elevated lipase (11%, mild and moderate). There were no serious adverse events or significant variations in liver enzymes. There was a suppression of peripheral interleukin (IL)-17, IL-23, IL-1b and TNF-alpha in the 70 and 100 mg groups, and a significant decrease in alcohol consumption over time (AUDIT-C: 6 [3-7] vs. 5 [1-6], p = 0.023). Conclusions Guselkumab is safe in doses up to 100 mg and may reduce inflammation markers in ALD. These findings support further phase 2 studies to evaluate the efficacy of guselkumab in ALD, particularly in patients with severe phenotypes.
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| Autor | Díaz Piga, Luis Antonio Morris, Sheldon Dave, Shravan Kim, Susy M. Sarik, Wathnita Richards, Lisa Madamba, Egbert Bettencourt, Ricki Fulinara, Christian Pham, Thuy Miller, Grant Carvalho-Gontijo Weber, Raquel Momper, Jeremiah D. He, Feng Jain, Sonia Jamieson, Catriona Kisseleva, Tatiana Brenner, David Loomba, Rohit |
| Título | Clinical Trial to Assess the Safety and Tolerability of Anti-IL 23 Monoclonal Antibody Guselkumab in Patients With Alcohol-Associated Liver Disease |
| Revista | Alimentary Pharmacology & Therapeutics |
| ISSN | 0269-2813 |
| ISSN electrónico | 1365-2036 |
| Fecha de publicación | 2025 |
| Resumen | BackgroundThere are no FDA-approved therapies for alcohol-associated liver disease (ALD). Preclinical studies indicate that blocking IL-23/IL-17 signalling may reverse liver injury. Guselkumab, an IL-23-specific antibody approved for psoriasis, may be beneficial for ALD. AimsWe aimed to assess the safety and tolerability of guselkumab in patients with ALD. MethodsThis phase-1 dose-escalation study included patients with >= 2 DSM-5 criteria for alcohol use disorder, significant steatosis (MRI-PDFF >= 8%) and MRE < 3.63 kPa (to exclude advanced disease). Guselkumab was given subcutaneously on Days 1 and 29 in 30, 70 or 100 mg dose cohorts. Primary endpoints were adverse events (AEs) and dose-limiting toxicity. ResultsWe enrolled 13 patients (three 30 mg, three 70 mg, and seven 100 mg). Eleven completed the study and two early discontinued in the 100 mg group. Of them, 77% were men, and the median age was 53 [IQR 49-61] years. The median MRI-PDFF and MRE were 18.4% [IQR 8.4%-34.0%] and 2.5 [2.2-2.6] kPa, respectively. The most frequent AEs were hyperuricemia (13%, mild only) and elevated lipase (11%, mild and moderate). There were no serious adverse events or significant variations in liver enzymes. There was a suppression of peripheral interleukin (IL)-17, IL-23, IL-1b and TNF-alpha in the 70 and 100 mg groups, and a significant decrease in alcohol consumption over time (AUDIT-C: 6 [3-7] vs. 5 [1-6], p = 0.023). Conclusions Guselkumab is safe in doses up to 100 mg and may reduce inflammation markers in ALD. These findings support further phase 2 studies to evaluate the efficacy of guselkumab in ALD, particularly in patients with severe phenotypes. |
| Derechos | registro bibliográfico |
| DOI | 10.1111/apt.70026 |
| Enlace | |
| Id de publicación en WoS | WOS:001421560400001 |
| Palabra clave | Alcoholic cirrhosis Alcohol-related liver disease ALD Cirrhosis Liver disease Steatotic liver disease |
| Temática | Medicina y salud |
| Tipo de documento | preprint |