Safety, tolerability, pharmacokinetics, and pharmacodynamics of HBM9161, a novel FcRn inhibitor, in a phase I study for healthy Chinese volunteers

Autor:	Yu Zhang, Desmond Y H Yap, Xueying Zhou, Paul C.H. Lee, Xiaoxiang Chen, Jojo Hai, Meng Wang, Michael Lee
Jazyk:	angličtina
Rok vydání:	2021
Předmět:	Adult Male China medicine.medical_specialty Adolescent Cmax Receptors Fc RM1-950 Antibodies Monoclonal Humanized Placebo Gastroenterology Article General Biochemistry Genetics and Molecular Biology Young Adult Neonatal Fc receptor Pharmacokinetics Internal medicine Humans Medicine Dosing General Pharmacology Toxicology and Pharmaceutics Adverse effect Dose-Response Relationship Drug business.industry Research General Neuroscience Histocompatibility Antigens Class I Articles General Medicine Middle Aged Rash Healthy Volunteers Pharmacodynamics Female Therapeutics. Pharmacology medicine.symptom Public aspects of medicine RA1-1270 business
Zdroj:	Clinical and Translational Science, Vol 14, Iss 5, Pp 1769-1779 (2021) Clinical and Translational Science
ISSN:	1752-8054 1752-8062
Popis:	Blockade of the binding between neonatal Fc receptor and IgG‐Fc reduces circulating IgG, and thus emerges as a potential therapy for IgG‐mediated autoimmune conditions. This was a double blind, randomized, single ascending dose study to evaluate the safety, pharmacokinetics, and pharmacodynamics of HBM9161 (a fully humanized Fc receptor monoclonal antibody) in healthy Chinese volunteers. Subjects were randomized to receive a single s.c. dose of HBM9161 or placebo in a 3:1 ratio in 3 dosing cohorts (340 mg, 510 mg, or 680 mg, respectively), and then followed up for 85 days. Study end points included incidence of adverse event (AE), serum drug concentration, IgG and its subclasses, and anti‐drug antibodies (ADAs). Twenty‐four subjects were randomized. Dose‐dependent reduction of total IgG occurred rapidly from baseline to reach nadir at day 11, then recovered steadily from day 11 to day 85. The mean maximum percentage reductions from baseline total IgG were 21.0 ± 9.3%, 39.8 ± 5.13%, and 41.2 ± 10.4% for subjects receiving HBM9161 340 mg, 510 mg, and 680 mg, respectively. The exposure of HBM9161 (areas under the curve [AUCs] and peak plasma concentration [Cmax]) increased in a more than dose‐proportional manner at the dose examined. All reported AEs were mild in severity. The most reported AEs in the HBM9161 groups were influenza‐like illness and rash. Two subjects developed ADA during the study period. A single s.c. dose of HBM9161 results in sustained and dose‐dependent IgG reduction, and was well‐tolerated at a dose up to 680 mg in Chinese subjects. The data warrant further investigation of its effects in IgG‐mediated autoimmune disorders.
Databáze:	OpenAIRE
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