Brain penetration, target engagement, and disposition of the blood-brain barrier-crossing bispecific antibody antagonist of metabotropic glutamate receptor type 1

Carl I Webster; Nadia Caram-Salas; Arsalan S Haqqani; George Thom; Lee Brown; Kerry Rennie; Alvaro Yogi; Willard Costain; Eric Brunette; Danica B Stanimirovic

doi:10.1096/fj.201500078

Brain penetration, target engagement, and disposition of the blood-brain barrier-crossing bispecific antibody antagonist of metabotropic glutamate receptor type 1

FASEB J. 2016 May;30(5):1927-40. doi: 10.1096/fj.201500078. Epub 2016 Feb 2.

Authors

Affiliations

¹ Antibody Discovery and Protein Engineering, MedImmune, Cambridge, United Kingdom; websterc@medimmune.com.
² Human Health Therapeutics Portfolio, National Research Council of Canada, Ottawa, Ontario, Canada.
³ Antibody Discovery and Protein Engineering, MedImmune, Cambridge, United Kingdom;
⁴ Translational Sciences, MedImmune, Cambridge, United Kingdom; and.

PMID: 26839377
DOI: 10.1096/fj.201500078

Abstract

Receptor mediated transcytosis harnessing the cellular uptake and transport of natural ligands across the blood-brain barrier (BBB) has been identified as a means for antibody delivery to the CNS. In this study, we characterized bispecific antibodies in which a BBB-crossing antibody fragment FC5 was used as a BBB carrier. Cargo antibodies were either a high-affinity, selective antibody antagonist of the metabotropic glutamate receptor-1 (BBB-mGluR1), a widely abundant CNS target, or an IgG that does not bind the CNS target (BBB-NiP). Both BBB-NiP and BBB-mGluR1 demonstrated a similar 20-fold enhanced rate of transcytosis across an in vitro BBB model compared with mGluR1 IgG fused to a control antibody fragment. All 3 bispecific antibodies exhibited identical pharmacokinetics in vivo Comparative assessment of BBB-NiP and BBB-mGluR1 revealed that, whereas their serum pharmacokinetics and BBB penetration were identical, their central disposition (brain levels) and elimination (cerebrospinal fluid levels) were widely different, due to central target-mediated removal of the mGluR1-engaging antibody. Central mGluR1 target engagement after systemic administration was demonstrated by a dose-dependent inhibition of mGluR-1-mediated thermal hyperalgesia and by colocalization of the antibody with thalamic neurons involved in mGluR1-mediated pain processing. We demonstrate the feasibility of targeting central G-protein-coupled receptors using a BBB-crossing bispecific antibody approach and emerging principles that govern brain distribution and disposition of these antibodies. These data will be important for designing safe and selective CNS antibody therapeutics.-Webster, C. I., Caram-Salas, N., Haqqani, A. S., Thom, G., Brown, L., Rennie, K., Yogi, A., Costain, W., Brunette, E., Stanimirovic, D. B. Brain penetration, target engagement, and disposition of the blood-brain barrier-crossing bispecific antibody antagonist of metabotropic glutamate receptor type 1.

Keywords: brain endothelial cells; mass spectrometry; pain; receptor-mediated transcytosis.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Analgesics
Animals
Antibodies, Bispecific / pharmacology*
Biological Products / metabolism
Biological Transport
Blood-Brain Barrier / metabolism
Brain / drug effects
Brain / metabolism*
Camelidae
Cell Membrane
HEK293 Cells
Hot Temperature / adverse effects
Humans
Immunoconjugates / metabolism
Immunoglobulin G / immunology
Pain / drug therapy*
Pain / etiology
Protein Engineering / methods
Rats
Receptors, Metabotropic Glutamate / antagonists & inhibitors*
Receptors, Metabotropic Glutamate / metabolism

Substances

Analgesics
Antibodies, Bispecific
Biological Products
Immunoconjugates
Immunoglobulin G
Receptors, Metabotropic Glutamate
metabotropic glutamate receptor type 1