Canine olfactory ensheathing cells from the olfactory mucosa can be engineered to produce active chondroitinase ABC

Carwardine, Darren; Wong, Liang‐Fong; Fawcett, James W.; Muir, Elizabeth M.; Granger, Nicolas

doi:10.1016/j.jns.2016.06.011

Cited by 12 publications

(20 citation statements)

References 77 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Compared with previous reports, the transfection levels we have obtained for cOMCs appear to be within ranges reported for viral methods: Carwardine et al 17 reported a maximum transduction efficiency of 34% at a multiplicity of infection (MOI) of 10, using chondroitinase ABC encoding lentiviral vectors and Ruitenberg et al 31 reported 100% transduction of rodent olfactory bulb-derived OECs with a reporter plasmid at an MOI of 50 and 100 using lentiviral and adenoviral vectors, respectively. Wu et al 32 transfected purified rodent olfactory bulb-derived OECs with a plasmid encoding NT-3 using a commercial lipofection agent, reporting a maximum transfection efficiency of 30% showing our techniques also compare favourably with other non-viral methods.…”

Section: Discussionsupporting

confidence: 76%

“…This means that the additional benefits provided by the MP platform, such as the use of bimodal nanoparticles for simultaneous gene delivery and imaging 27 could be safely exploited. Future work will deploy this therapy in vivo in clinical spinal injuries (including in canine trials), and explore the ability of this technical approach to deliver other genes involved in repair such as additional neurotherapeutic factors to promote growth, chondroitinase ABC to degrade the glial scar, 17,46 and VEGF to promote local angiogenesis. 47…”

Section: Conclusion/future Directionsmentioning

confidence: 99%

“…Genetic engineering of OECs for release of neurotrophic factors at injury sites offers a potential strategy for improved regenerative outcomes; 13,14 for example, OECs genetically modified to secrete neurotrophin-3 (NT-3) and glial cell line-derived neurotrophic factor (GDNF) show improved functionality post-transplantation versus non-engineered OECs. [15][16][17] Whilst work is ongoing to improve the safety of viral vector mediated bioengineering approaches, they can be associated with significant oncogenic 18 and inflammatory 19 risks to recipients.…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

A fusion of minicircle DNA and nanoparticle delivery technologies facilitates therapeutic genetic engineering of autologous canine olfactory mucosal cells

et al. 2017

Self Cite

View full text Add to dashboard Cite

Olfactory ensheathing cells (OECs) promote axonal regeneration and improve locomotor function when transplanted into the injured spinal cord. A recent clinical trial demonstrated improved motor function in domestic dogs with spinal injury following autologous OEC transplantation. Their utility in canines offers promise for human translation, as dogs are comparable to humans in terms of clinical management and genetic/environmental variation. Moreover, the autologous, minimally invasive derivation of OECs makes them viable for human spinal injury investigation. Genetic engineering of transplant populations may augment their therapeutic potential, but relies heavily on viral methods which have several drawbacks for clinical translation. We present here the first proof that magnetic particles deployed with applied magnetic fields and advanced DNA minicircle vectors can safely bioengineer OECs to secrete a key neurotrophic factor, with an efficiency approaching that of viral vectors. We suggest that our alternative approach offers high translational potential for the delivery of augmented clinical cell therapies.

show abstract

Section: Discussionsupporting

confidence: 76%

Section: Conclusion/future Directionsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

A fusion of minicircle DNA and nanoparticle delivery technologies facilitates therapeutic genetic engineering of autologous canine olfactory mucosal cells

et al. 2017

Self Cite

View full text Add to dashboard Cite

show abstract

“…The lentiviral transfer vector used to deliver the mammalian-compatible Proteus vulgaris ChABC gene [ 22 ] and the GFP gene to canine OECs was identical to the pRRL-CMV-ChABC-SFFV-GFP vector previously reported [ 37 ]. The control transfer vector pRRL-CMV-GFP expressed solely GFP.…”

Section: Methodsmentioning

confidence: 99%

“…Canine OECs can be safely collected from the nasal mucosa, cultured in vitro and autologously transplanted into spinal cord lesions [ 30 ]. We have previously demonstrated that these canine OECs can be genetically modified to produce the mammalian-modified form of ChABC in vitro [ 37 ]. We further show here that canine OECs can act as a vehicle for delivering active ChABC to the site of SCI in rats.…”

Section: Introductionmentioning

confidence: 99%

Transplantation of canine olfactory ensheathing cells producing chondroitinase ABC promotes chondroitin sulphate proteoglycan digestion and axonal sprouting following spinal cord injury

et al. 2017

Self Cite

View full text Add to dashboard Cite

Olfactory ensheathing cell (OEC) transplantation is a promising strategy for treating spinal cord injury (SCI), as has been demonstrated in experimental SCI models and naturally occurring SCI in dogs. However, the presence of chondroitin sulphate proteoglycans within the extracellular matrix of the glial scar can inhibit efficient axonal repair and limit the therapeutic potential of OECs. Here we have used lentiviral vectors to genetically modify canine OECs to continuously deliver mammalian chondroitinase ABC at the lesion site in order to degrade the inhibitory chondroitin sulphate proteoglycans in a rodent model of spinal cord injury. We demonstrate that these chondroitinase producing canine OECs survived at 4 weeks following transplantation into the spinal cord lesion and effectively digested chondroitin sulphate proteoglycans at the site of injury. There was evidence of sprouting within the corticospinal tract rostral to the lesion and an increase in the number of corticospinal axons caudal to the lesion, suggestive of axonal regeneration. Our results indicate that delivery of the chondroitinase enzyme can be achieved with the genetically modified OECs to increase axon growth following SCI. The combination of these two promising approaches is a potential strategy for promoting neural regeneration following SCI in veterinary practice and human patients.

show abstract

Transplantation of encapsulated autologous olfactory ensheathing cell populations expressing chondroitinase for spinal cord injury: A safety and feasibility study in companion dogs

Prager

Fenn

Plested

et al. 2022

J Tissue Eng Regen Med

Self Cite

View full text Add to dashboard Cite

Spinal cord injury (SCI) can cause irreversible paralysis, with no regenerative treatment clinically available. Dogs with natural SCI present an established model and can facilitate translation of experimental findings in rodents to people. We conducted a prospective, single arm clinical safety study in companion dogs with chronic SCI to characterize the feasibility of intraspinal transplantation of hydrogel‐encapsulated autologous mucosal olfactory ensheathing cell (mOEC) populations expressing chondroitinase ABC (chABC). mOECs and chABC are both promising therapies for SCI, and mOECs expressing chABC drive greater voluntary motor recovery than mOECs alone after SCI in rats. Canine mOECs encapsulated in collagen hydrogel can be matched in stiffness to canine SCI. Four dogs with complete and chronic loss of function caudal to a thoraco‐lumbar lesion were recruited. After baseline measures, olfactory mucosal biopsy was performed and autologous mOECs cultured and transduced to express chABC, then hydrogel‐encapsulated and percutaneously injected into the spinal cord. Dogs were monitored for 6 months with repeat clinical examinations, spinal MRI, kinematic gait and von Frey assessment. No adverse effects or significant changes on neurological examination were detected. MRI revealed large and variable lesions, with no spinal cord compression or ischemia visible after hydrogel transplantation. Owners reported increased pelvic‐limb reflexes with one dog able to take 2–3 unsupported steps, but gait‐scoring and kinematic analysis showed no significant improvements. This novel combination approach to regeneration after SCI is therefore feasible and safe in paraplegic dogs in a clinical setting. A randomised‐controlled trial in this translational model is proposed to test efficacy.

show abstract

Canine olfactory ensheathing cells from the olfactory mucosa can be engineered to produce active chondroitinase ABC

Cited by 12 publications

References 77 publications

A fusion of minicircle DNA and nanoparticle delivery technologies facilitates therapeutic genetic engineering of autologous canine olfactory mucosal cells

A fusion of minicircle DNA and nanoparticle delivery technologies facilitates therapeutic genetic engineering of autologous canine olfactory mucosal cells

Transplantation of canine olfactory ensheathing cells producing chondroitinase ABC promotes chondroitin sulphate proteoglycan digestion and axonal sprouting following spinal cord injury

Transplantation of encapsulated autologous olfactory ensheathing cell populations expressing chondroitinase for spinal cord injury: A safety and feasibility study in companion dogs

Contact Info

Product

Resources

About