Copyright
©The Author(s) 2024.
World J Stem Cells. May 26, 2024; 16(5): 467-478
Published online May 26, 2024. doi: 10.4252/wjsc.v16.i5.467
Published online May 26, 2024. doi: 10.4252/wjsc.v16.i5.467
Table 1 Recently reported peripheral nerve injury repair in the experimental animal models
| Ref. | Experimental model (in vitro or animal) | Therapeutic modalities | Main findings |
| MSCs-based therapy | |||
| Zhang et al[4], 2024 | SCs from injured sciatic nerves and HUVECs | MSCs treated with PRP-derived exosomes | Treatment with PRP-exosome improved MSC survival. Exosome-treated MSCs, co-cultured with SCs, reduced their apoptosis and enhanced SC proliferation after PNI. Similarly, exosome-treated MSCs also had pro-migratory and angiogenic effects. Cytokine array analysis and ELISA showed upregulation of 155 proteins and downregulation of six proteins, with many pro-angiogenic and neurotrophic factors. Western blot revealed the activation of the PI3K/Akt signaling pathway in exosomes-treated MSCs |
| Sivanarayanan et al[5], 2023 | Sciatic nerve crush injury in rabbit | Allogenic BM-MSCs and their CM | BM-MSCs and BM-MSCS-CM treatment improved the regenerative capacity in acute and subacute injury groups, with slightly better improvements in the subacute groups. BM-MSCs supported the healing process of PNI, whereas CM increased the healing process |
| Yalçın et al[6], 2023 | Sciatic nerve injury in rat | ADSCs | The study documented the role of syndecan-1 and heat shock protein 70 in the regenerative effects of ADSCs on PNI. Histology and EMG showed that treatment with ADSCs significantly improved nerve regeneration and its functionality via the release of nerve growth factor |
| Liu et al[7], 2020 | Sprague-Dawley rats | SC-like ADSCs are placed on an acellular scaffold after treatment with nerve leachate | Sprague-Dawley rats were divided into four groups: Scaffold only, untreated ADSCs + scaffold, nerve leachate-treated ADSCs + scaffold, and autograft. Four months after treatment, the average area, density, and thickness of regenerated nerve fibers in the nerve leachate-treated ADSCs + scaffold group significantly increased compared to the untreated ADSCs + scaffold group. These data show the superiority of nerve leachate-treated ADSCs for treating PNI |
| Kizilay et al[8], 2017 | Wistar rat model of sciatica nerve injury by clip compression | BM-MSCs | The proximal, distal, and mean latency values were higher in MSC treatment groups vs without MSC-treated animals. The nerve conduction velocity, compound action potential, and the number of axons in MSC-treated animals are higher than in non-MSC-treated animals. Also, myelin damage decreased in MSC-treated animals |
| Cell-free therapy | |||
| Growth factor-based approach for PNI | |||
| Shi et al[9], 2022 | Rat sciatic nerve transection model | In vitro experimental studies show that BDNF/PLGA sustained-release microsphere treatment improved migration and neural differentiation of ADSCs. In vivo studies indicated that BDNF microsphere treatment significantly reduced the nerve conduction velocity compound amplitude compared to the untreated animals. Moreover, the BDNF microsphere group had more closely arranged and uniformly distributed nerve fibers than the control animals | |
| Li et al[10], 2021 | Rat sciatic nerve transection model | Leision site injection of a lentivirus expressing FGF13 | FGF13 treatment successfully recovered motor and sensory functions via axon elongation and remyelination. FGF13 pretreatment enhanced SCs survival and increased cellular microtubule-associated proteins in vitro PNI model. The data supported the role of FGF13 in stabilizing cellular microtubules, which is essential for promoting PNI repair following PNI |
| Su et al[11], 2020 | Rat sciatic nerve transection model | Composite nerve conduit with slow-release BDNF | The study used fabricated composite nerve conduits with slow-release BDNF to treat PNI and compare the regeneration potentials of autologous nerve grafts. The BDNF composite conduits remained bioactive for at least three months and successfully regenerated a 10-mm sciatic nerve gap |
| Lu et al[12], 2019 | Rat model of sciatic crush injury | Intramuscular delivery of FGF21 once daily for seven days | FGF21 treatment led to functional and morphologic recovery with improved motor and sensory function, enhanced axonal remyelination and re-growth, and increased SC proliferation. Local FGF21 treatment reduced oxidative stress via activation of Nrf-2 and ERK. FGF21 also reduced autophagic cell death in SCs |
| Exosome-based approach for PNI | |||
| Zhu et al[13], 2023 | Mouse model of spared nerve injury | Exosomes from UC-MSCs under hypoxia | After 48 h of culture under 3% oxygen in a serum-free culture system, UC-MSCs secreted higher EVs than the control cells. SCs could uptake EVs in vitro and increase their growth and migration. The treatment of animals with EVs accelerated the recruitment of SCs at the PNI site and supported PN repair and regeneration |
| Hu et al[14], 2023 | Rat model of the injured sciatic nerve | SCs-like cells derived from hA-MSCs. Exosomes from hA-MSCs or SC-like cells from hA-MSCs | SC-like cells were successfully differentiated from hA-MSCs and used for exosome collection. Treatment with exosomes from SC-like cells significantly enhanced (vs hA-MSCs-derived exosomes) motor function recovery, reduced gastrocnemius muscle atrophy, and supported axonal regrowth, myelin formation, and angiogenesis in the rat model. They were also more efficiently absorbed by SCs and promoted the proliferation and migration of SCs |
| Yin et al[15], 2021 | In vitro model and a rat model of sciatic nerve injury | ADSCs | Exosome treatment inhibited autophagy and karyopherin-α2 levels, which were significantly increased in SCs in the injured sciatic nerve, both in vivo and in vitro. Abrogation of karyopherin-α2 reduced SCs autophagy, with the role of miRNA-26b. Treatment with exosomes supported myelin sheath regeneration in rats with a sciatic NI |
| Liu et al[16], 2020 | PNI model rats supported by in vitro studies | ADSCs and their derivative exosomes | Treatment with ADSC-derived exosomes significantly reduced SC apoptosis after PNI via increased Bcl-2 and decreased Bax mRNA expression, in addition to increasing SC proliferation. Histological data in PNI model rats also observed these effects |
| Chen et al[17], 2019 | In vitro model and rat sciatic nerve transection model with a 10-mm gap | Human ADSCs-derived exosomes and in vitro | In vitro studies showed that SCs internalized human ASCs-derived exosomes to enhance their proliferation, migration, myelination, and secretion of neurotrophic factors. Treatment with ASC-exosomes supported axon regeneration in a rat sciatic nerve transection model with a 10-mm gap and supported myelination and restoration of denervation muscle atrophy. This data showed the efficacy of exosomes in promoting PN regeneration by restoring SC function |
| Masgutov et al[18], 2019 | Wistar rat sciatic nerve injury model | ADSCs | ADSCs-derived MSCs were delivered using fibrin glue to the traumatic injury, helped to fix the cells at the graft site, and gave extracellular matrix support to the provided cells. The transplanted cells were neuroprotective on DRG L5 sensory neurons and stimulated axon growth and myelination. Also, MSCs promoted nerve angiogenesis and motor function recovery |
Table 2 Clinical studies for peripheral nerve injury repair using Schwan cells, stem cells, and their derived exosomes
| NCT# | Study title | Conditions | Interventions | Primary outcome | Sponsor | Collaborators |
| NCT04346680 | Intraoperative ADSC administration during nerve release | Neurotmesis of peripheral nerve disorder | ADSC administration | Electrophysiological improvement, improvement in EMG - the appearance of activities in denervated muscles, one year | Mossakowski MRC Polish Academy of Sciences | Centre of Postgraduate Medical Education |
| NCT03964129 | BMAC nerve allograft study | PNI upper limb | Avance nerve graft with autologous BMAC | Comparison of AEs between patients treated with ANG with BMAC and the historical data of nerve repairs with the ANG only. Long-term study - AEs, such as infection, wound dehiscence, neuropathy, carpal tunnel syndrome, bleeding, seroma, and lymphocele, will be recorded and analyzed. AEs will be mapped to a MedDRA-preferred term and system organ classification | Brooke Army Medical Center | Walter Reed National Military Medical Center; Cleveland Clinic Lerner Research Institute |
| NCT03359330; PKUPH-PNI | Mid-term effect observation of biodegradable conduit small gap tublization repairing PNI | PNIs | Degradable conduit small gap tublization | To observe the mid-term clinical effect of biodegradable conduit small gap tublization on the repair of PNI in multi-center patients and fresh PNIs in the upper extremities | Peking University People’s Hospital | - |
| NCT05541250 | Safety and efficacy of autologous human SCs augmentation in severe peripheral nerve injury | PNIs | Autologous human SC | The primary purpose of this phase I study is to evaluate the safety of injecting one’s SCs along with nerve auto-graft after a severe nerve injury, such as a sciatic nerve or brachial plexus injury | University of Miami, Florida, United States (Recruiting) | - |
| NCT04654286 | Clinical outcomes of HAM and allogeneic MSCs composite augmentation for nerve transfer procedure in brachial plexus injury patients | Brachial plexus neuropathies | Nerve transfer or nerve transfer with HAM-MSC composite wrapping | AROM pre-surgery and 12-month follow-up for shoulder flexion, extension, abduction, adduction, external rotation, and internal rotation using the MRC scale (ranging from 0-5) | Dr. Soetomo General Hospital, Jakarta | |
| Huang et al[19], 2016 | A clinical study on the treatment of peripheral nerve injury growth factor of mecobalamin combined with nerve | 150 PNI patients | Mecobalamin (0.5 mg, I.V, once a day) combined with NGF (30 mg, I.M injection, once a day) for 3-6 wk | Treatment with mecobalamin combined with NGF improved the sensorimotor evaluation of the curative effect made by the British Medical Research Institute of Neurotrauma Society | Guangxi Basic Science and Technology Plan Project PR China (No.: 20111209) | |
| Civelek et al[20], 2024 | Effects of exosomes from mesenchymal stem cells on functional recovery of a patient with total radial nerve injury: A pilot study | One patient with total radial nerve injury | WJ-MSCs derived exosomes | The six-month follow-up based on the BMRC and Mackinnon-Dellon scales showed improved motor (M5, excellent), and sensory functions also showed improvement (S3+, good). These results were achieved without physical therapy. Substantial axonal damage was observed at a ten-week follow-up, but nerve re-innervation was observed by EMG, which also improved significantly during the six-month follow-up | Department of Neurosurgery, University of Health Sciences |
Table 3 List some commonly studied growth factors for peripheral nerve injury treatment
| Ref. | Growth factor |
| Sandoval-Castellanos et al[43], 2020 | Brain-derived neurotrophic factor |
| Xu et al[44], 2023 | Ciliary neurotrophic factor |
| Gu et al[45], 2024 | Chemokine platelet factor-4 |
| Romano and Bucci[46], 2020 | Epidermal growth factor |
| Cintron-Colon et al[47], 2022 | Glial cell line-derived neurotrophic factor |
| Ye et al[48], 2022 | Hepatocyte growth factor |
| Slavin et al[49], 2021 | Insulin-like growth factor-1 |
| Alastra et al[50], 2021 | Nerve growth factor |
| Li et al[51], 2023 | NGF+ basic fibroblast growth factor |
| Golzadeh and Mohammadi[52], 2016 | Platelet-derived growth factor |
| Ding et al[53], 2024 | Transforming growth factor |
| Xu et al[44], 2023 | Vascular endothelial growth factor |
- Citation: Mushtaq M, Zineldeen DH, Mateen MA, Haider KH. Mesenchymal stem cells’ “garbage bags” at work: Treating radial nerve injury with mesenchymal stem cell-derived exosomes. World J Stem Cells 2024; 16(5): 467-478
- URL: https://www.wjgnet.com/1948-0210/full/v16/i5/467.htm
- DOI: https://dx.doi.org/10.4252/wjsc.v16.i5.467