Immune-evasive gene switch enables regulated delivery of chondroitinase after spinal cord injury.

Emily R Burnside,Elizabeth J Bradbury,Hugo Layard-Horsfall,Elizabeth M Muir,Elena-Cristina Andreica,Fred De Winter,Joost Verhaagen,Nicholas D James,Athanasios Didangelos

doi:10.1093/brain/awy158

Emily R Burnside, Elizabeth J Bradbury + Show 7 more

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https://doi.org/10.1093/brain/awy158

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Abstract

Chondroitinase ABC is a promising preclinical therapy that promotes functional neuroplasticity after CNS injury by degrading extracellular matrix inhibitors. Efficient delivery of chondroitinase ABC to the injured mammalian spinal cord can be achieved by viral vector transgene delivery. This approach dramatically modulates injury pathology and restores sensorimotor functions. However, clinical development of this therapy is limited by a lack of ability to exert control over chondroitinase gene expression. Prior experimental gene regulation platforms are likely to be incompatible with the non-resolving adaptive immune response known to occur following spinal cord injury. Therefore, here we apply a novel immune-evasive dual vector system, in which the chondroitinase gene is under a doxycycline inducible regulatory switch, utilizing a chimeric transactivator designed to evade T cell recognition. Using this novel vector system, we demonstrate tight temporal control of chondroitinase ABC gene expression, effectively removing treatment upon removal of doxycycline. This enables a comparison of short and long-term gene therapy paradigms in the treatment of clinically-relevant cervical level contusion injuries in adult rats. We reveal that transient treatment (2.5 weeks) is sufficient to promote improvement in sensory axon conduction and ladder walking performance. However, in tasks requiring skilled reaching and grasping, only long term treatment (8 weeks) leads to significantly improved function, with rats able to accurately grasp and retrieve sugar pellets. The late emergence of skilled hand function indicates enhanced neuroplasticity and connectivity and correlates with increased density of vGlut1+ innervation in spinal cord grey matter, particularly in lamina III-IV above and below the injury. Thus, our novel gene therapy system provides an experimental tool to study temporal effects of extracellular matrix digestion as well as an encouraging step towards generating a safer chondroitinase gene therapy strategy, longer term administration of which increases neuroplasticity and recovery of descending motor control. This preclinical study could have a significant impact for tetraplegic individuals, for whom recovery of hand function is an important determinant of independence, and supports the ongoing development of chondroitinase gene therapy towards clinical application for the treatment of spinal cord injury.

Highlights

Spinal cord injury results in permanent disruption to nervous system function, for which there is no current regenerative or pathology-modifying treatment (Ramer et al, 2014)
Since the majority of spinal injured individuals are injured at the cervical level (National Spinal Cord Statistical Centre, 2017) and a top priority for improving independence and quality of life is recovery of hand and digit function (Anderson, 2004), we investigate the effect of dox-i-chondroitinase ABC (ChABC) treatment following a clinically relevant cervical spinal contusion injury model in adult rats
The gene contains codons optimized for expression in mammalian cells, an optimized 50 Kozak sequence, and a mouse matrix metalloproteinase-2 signal sequence for secretion. It is modified by removal of specific post-translational N-glycosylation sites, which impede passage of the prokaryotic enzyme through the eukaryotic secretory machinery (Muir et al, 2010). This transgene was cloned into a lentiviral transfer vector where gene expression is under control of a tetracycline response element (TRE) comprising eight TetO repeats (p8teto-36ÁI) and a cytomegalovirus minimal promoter (Agha-Mohammadi et al, 2004; Hoyng et al, 2014)

Summary

Introduction

Spinal cord injury results in permanent disruption to nervous system function, for which there is no current regenerative or pathology-modifying treatment (Ramer et al, 2014). We have previously reported a gene therapy strategy whereby optimization of the prokaryotic ChABC gene to render it compatible with translation and secretion from mammalian cells (Muir et al, 2010) and incorporation of this gene into viral vectors (Zhao et al, 2011), leads to high levels of ChABC gene expression and active enzyme release in vivo. This results in extensive CSGAG digestion across many segments of the mammalian spinal cord (Bartus et al, 2014). ChABC gene therapy is a promising therapeutic strategy for the treatment of spinal cord injury

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