Enhanced antibody half-life improves in vivo activity
J Zalevsky, AK Chamberlain, HM Horton, S Karki… - Nature …, 2010 - nature.com
J Zalevsky, AK Chamberlain, HM Horton, S Karki, IWL Leung, TJ Sproule, GA Lazar…
Nature biotechnology, 2010•nature.comImproved affinity for the neonatal Fc receptor (FcRn) is known to extend antibody half-life in
vivo. However, this has never been linked with enhanced therapeutic efficacy. We tested
whether antibodies with half-lives extended up to fivefold in human (h) FcRn transgenic mice
and threefold in cynomolgus monkeys retain efficacy at longer dosing intervals. We
observed that prolonged exposure due to FcRn-mediated enhancement of half-life improved
antitumor activity of Fc-engineered antibodies in an hFcRn/Rag1−/− mouse model. This …
vivo. However, this has never been linked with enhanced therapeutic efficacy. We tested
whether antibodies with half-lives extended up to fivefold in human (h) FcRn transgenic mice
and threefold in cynomolgus monkeys retain efficacy at longer dosing intervals. We
observed that prolonged exposure due to FcRn-mediated enhancement of half-life improved
antitumor activity of Fc-engineered antibodies in an hFcRn/Rag1−/− mouse model. This …
Abstract
Improved affinity for the neonatal Fc receptor (FcRn) is known to extend antibody half-life in vivo. However, this has never been linked with enhanced therapeutic efficacy. We tested whether antibodies with half-lives extended up to fivefold in human (h)FcRn transgenic mice and threefold in cynomolgus monkeys retain efficacy at longer dosing intervals. We observed that prolonged exposure due to FcRn-mediated enhancement of half-life improved antitumor activity of Fc-engineered antibodies in an hFcRn/Rag1−/− mouse model. This bridges the demand for dosing convenience with the clinical necessity of maintaining efficacy.
nature.com
