Antibody-oligonucleotide conjugate achieves CNS delivery in animal models for spinal muscular atrophy
Suzan M. Hammond, … , Matthew J.A. Wood, Carl I. Webster
Suzan M. Hammond, … , Matthew J.A. Wood, Carl I. Webster
Published November 8, 2022
Citation Information: JCI Insight. 2022;7(24):e154142. https://doi.org/10.1172/jci.insight.154142.
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Research Article Neuroscience

Antibody-oligonucleotide conjugate achieves CNS delivery in animal models for spinal muscular atrophy

Abstract

Antisense oligonucleotides (ASOs) have emerged as one of the most innovative new genetic drug modalities. However, their high molecular weight limits their bioavailability for otherwise-treatable neurological disorders. We investigated conjugation of ASOs to an antibody against the murine transferrin receptor, 8D3130, and evaluated it via systemic administration in mouse models of the neurodegenerative disease spinal muscular atrophy (SMA). SMA, like several other neurological and neuromuscular diseases, is treatable with single-stranded ASOs that modulate splicing of the survival motor neuron 2 (SMN2) gene. Administration of 8D3130-ASO conjugate resulted in elevated levels of bioavailability to the brain. Additionally, 8D3130-ASO yielded therapeutic levels of SMN2 splicing in the central nervous system of adult human SMN2–transgenic (hSMN2-transgenic) mice, which resulted in extended survival of a severely affected SMA mouse model. Systemic delivery of nucleic acid therapies with brain-targeting antibodies offers powerful translational potential for future treatments of neuromuscular and neurodegenerative diseases.

Authors

Suzan M. Hammond, Frank Abendroth, Larissa Goli, Jessica Stoodley, Matthew Burrell, George Thom, Ian Gurrell, Nina Ahlskog, Michael J. Gait, Matthew J.A. Wood, Carl I. Webster

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Figure 2

PK of antibody and antibody-PMO conjugates in mice.

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PK of antibody and antibody-PMO conjugates in mice. Plasma, brain, and s...
Plasma, brain, and spinal cord exposure following 20 mg/kg dose of 8D3130 (±PMO) and NIP228 (±PMO), unconjugated and conjugated to the PMO. (A) Plasma PK of antibodies with or without PMO over a 1-week period. High statistical significance (****) shown for 8D3130 20 mg/kg versus 8D3130-PMO 20 mg/kg for the first 3 time points and a lower significance (*) for 24- and 96- hour time points. No statistical significance shown for NIP228-PMO 20 mg/kg versus 8D3130-PMO 20 mg/kg at any time point. (B) Brain exposure as a measure of μg compound/g brain. Statistical significance (****) shown for 8D3130 20 mg/kg versus 8D3130-PMO 20 mg/kg for first 3 time points. Statistical significance (####) shown for NIP228-PMO 20 mg/kg versus 8D3130-PMO 20 mg/kg at all time points. (C) Spinal cord exposure as a measure of μg compound/g spinal cord. Statistical significance (***) shown for 8D3130 20 mg/kg versus 8D3130-PMO 20 mg/kg at 96-hour time point. Statistical significance (####) shown for NIP228-PMO 20 mg/kg versus 8D3130-PMO 20 mg/kg at first 2 time points and a lower statistical significance (#) at the last 2 time points. Statistical significance (representative P values) for exposure in brain, spinal cord, and plasma between 8D3130 20 mg/kg versus 8D3130-PMO 20 mg/kg (*) and NIP228-PMO 20 mg/kg versus 8D3130-PMO 20 mg/kg (#) at all time points evaluated. Statistical analysis was performed in GraphPad Prism. Data shown as the mean ± SEM, n = 3–4 per group. Statistical significance shown using 2-way ANOVA, where appropriate, made using Tukey test. *P, < 0.05; ***P, < 0.001; ****P, < 0.0001; #P, < 0.05; ####P, < 0.0001.