CD98hc is a target for brain delivery of biotherapeutics

Kylie S Chew ,Lakshman Annamalai ,Raymond K Tong ,Dojin Kim ,Hoang Nguyen ,Man Tong ,Meredith Calvert ,Hai L Tran ,David A Joy ,Yinhan Zhou ,Diana Lac ,Robert G Thorne ,Elisa Lozano ,Cathal Mahon ,Elysia Roche ,David Huynh ,René Meisner ,Kapil Gadkar ,Kristen N Knight ,Arash Moshkforoush ,Robert C Wells ,Kaitlin Xa ,Kendra J Lechtenberg ,Alexander Yang ,Joseph W Lewcock ,Joseph Mcinnes ,Padma Akkapeddi ,Yaneth Robles-Colmenares ,Marie Blanchette ,Mark S Dennis ,Richard Daneman ,Audrey Gill ,Joseph Duque ,Amy Wing-Sze Leung ,Patricia Sacayon ,Katrina W Lexa ,Ryan J Watts ,Timothy Earr ,Gerald Maxwell Cherf ,Kaja Bajc ,Divya Srivastava ,Nicholas P D Liau ,Johann Chow ,Isabel Becerra ,Hilda Solanoy ,Y Joy Yu Zuchero ,Mario Malfavon ,Darren Chan ,Michelle E Pizzo ,Mihalis S Kariolis

doi:10.1038/s41467-023-40681-4

Abstract

Brain exposure of systemically administered biotherapeutics is highly restricted by the blood-brain barrier (BBB). Here, we report the engineering and characterization of a BBB transport vehicle targeting the CD98 heavy chain (CD98hc or SLC3A2) of heterodimeric amino acid transporters (TVCD98hc). The pharmacokinetic and biodistribution properties of a CD98hc antibody transport vehicle (ATVCD98hc) are assessed in humanized CD98hc knock-in mice and cynomolgus monkeys. Compared to most existing BBB platforms targeting the transferrin receptor, peripherally administered ATVCD98hc demonstrates differentiated brain delivery with markedly slower and more prolonged kinetic properties. Specific biodistribution profiles within the brain parenchyma can be modulated by introducing Fc mutations on ATVCD98hc that impact FcγR engagement, changing the valency of CD98hc binding, and by altering the extent of target engagement with Fabs. Our study establishes TVCD98hc as a modular brain delivery platform with favorable kinetic, biodistribution, and safety properties distinct from previously reported BBB platforms.

Full Text