Targeting Transferrin Receptor to Transport Antisense Oligonucleotides Across the Blood-Brain Barrier

Scarlett J. Barker; Mai B. Thayer; Chaeyoung Kim; David Tatarakis; Matthew Simon; Rebekah Dial; Christian Nilewski; Robert C. Wells; Yinhan Zhou; Megan Afetian; Alfred E. Chappell; Kylie S. Chew; Johann Chow; Allisa Clemens; Claire B. Discenza; Jason C. Dugas; Chrissa A. Dwyer; Timothy Earr; Connie Ha; David Huynh; Srini Jayaraman; Wanda Kwan; Cathal Mahon; Michelle E. Pizzo; Elysia Roche; Laura Sanders; Alexander Stergioulis; Raymond K. Tong; Hai L. Tran; Joy Yu Zuchero; Anthony A. Estrada; Kapil Gadkar; Christopher MM Koth; Pascal E. Sanchez; Robert G. Thorne; Ryan J. Watts; Thomas Sandmann; Lesley A. Kane; Frank Rigo; Mark S. Dennis; Joseph W. Lewcock; Sarah L. DeVos

doi:10.1101/2023.04.25.538145

Targeting Transferrin Receptor to Transport Antisense Oligonucleotides Across the Blood-Brain Barrier

Scarlett J. Barker(Denali Therapeutics (United States)), Mai B. Thayer(Denali Therapeutics (United States)), Chaeyoung Kim(Denali Therapeutics (United States)), David Tatarakis(Denali Therapeutics (United States)), Matthew Simon(Denali Therapeutics (United States)), Rebekah Dial(Denali Therapeutics (United States)), Christian Nilewski(Denali Therapeutics (United States)), Robert C. Wells(Denali Therapeutics (United States)), Yinhan Zhou(Denali Therapeutics (United States)), Megan Afetian(Ionis Pharmaceuticals (United States)), Alfred E. Chappell(Ionis Pharmaceuticals (United States)), Kylie S. Chew(Denali Therapeutics (United States)), Johann Chow(Denali Therapeutics (United States)), Allisa Clemens(Denali Therapeutics (United States)), Claire B. Discenza(Denali Therapeutics (United States)), Jason C. Dugas(Denali Therapeutics (United States)), Chrissa A. Dwyer(Ionis Pharmaceuticals (United States)), Timothy Earr(Denali Therapeutics (United States)), Connie Ha(Denali Therapeutics (United States)), David Huynh(Denali Therapeutics (United States)), Srini Jayaraman(Denali Therapeutics (United States)), Wanda Kwan(Denali Therapeutics (United States)), Cathal Mahon(Denali Therapeutics (United States)), Michelle E. Pizzo(Denali Therapeutics (United States)), Elysia Roche(Denali Therapeutics (United States)), Laura Sanders(Denali Therapeutics (United States)), Alexander Stergioulis(Denali Therapeutics (United States)), Raymond K. Tong(Denali Therapeutics (United States)), Hai L. Tran(Denali Therapeutics (United States)), Joy Yu Zuchero(Denali Therapeutics (United States)), Anthony A. Estrada(Denali Therapeutics (United States)), Kapil Gadkar(Denali Therapeutics (United States)), Christopher MM Koth(Denali Therapeutics (United States)), Pascal E. Sanchez(Denali Therapeutics (United States)), Robert G. Thorne(Denali Therapeutics (United States)), Ryan J. Watts(Denali Therapeutics (United States)), Thomas Sandmann(Denali Therapeutics (United States)), Lesley A. Kane(Denali Therapeutics (United States)), Frank Rigo(Ionis Pharmaceuticals (United States)), Mark S. Dennis(Denali Therapeutics (United States)), Joseph W. Lewcock(Denali Therapeutics (United States)), Sarah L. DeVos(Denali Therapeutics (United States))

bioRxiv (Cold Spring Harbor Laboratory)

April 28, 2023

10.1101/2023.04.25.538145

Cited by 24Open Access

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Abstract

Abstract Antisense oligonucleotides (ASO) are promising therapies for neurological disorders, though they are unable to cross the blood-brain barrier (BBB) and must be delivered directly to the central nervous system (CNS). Here, we use a human transferrin receptor (TfR)-binding molecule to transport ASO across the BBB in mice and non-human primates, termed oligonucleotide transport vehicle (OTV). Systemically delivered OTV drives significant, cumulative, and sustained knockdown of the ASO target across multiple CNS regions and all major cell types. Further, systemic OTV delivery enables more uniform ASO biodistribution and knockdown compared to two other clinically relevant ASO delivery routes: a standard, high affinity TfR antibody, or direct ASO delivery to the CSF. Together, our data support systemically delivered OTV as a potential therapeutic platform for neurological disorders. One-Sentence Summary Systemically dosed OTV delivered via TfR1 targeting shows widespread and cumulative target knockdown in the mouse and NHP CNS.

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