Stem Cells: Recent Developments Redefining Epilepsy Therapy

Abstract

The field of stem cell therapy is growing rapidly and hopes to offer an alternative solution to diseases that are historically treated medically or surgically. One such focus of research is the treatment of medically refractory epilepsy, which is traditionally approached from a surgical or interventional standpoint. Research shows that stem cell transplantation has potential to offer significant benefits to the epilepsy patient by reducing seizure frequency, intensity, and neurological deficits that often result from the condition. This review explores the basic science progress made on the topic of stem cells and epilepsy by focusing on experiments using animal models and highlighting the most recent developments from the last 4 years.

Keywords

stem cell therapy epilepsy neurological disease

Introduction

Epilepsy, defined by high occurrence of seizures secondary to aberrant electoral neural signaling, affects 50 to 60 million people around the world¹. There are several described seizure types, including generalized, focal, and epileptic spasms. Generalized seizures can be further broken down into tonic-clonic, absence, myoclonic, and atonic seizures². Furthermore, epilepsy can be categorized as idiopathic, acquired (through changes in brain structure, infection, or metabolic disorders), and immunological³. Despite these multiple classifications, seizures can often be related to a common underlying pathophysiology: neuronal hyperactivation. Thus, most therapeutic interventions aim to remove the aberrant signaling area, via surgery, or reduce neuronal action potentials, using pharmacological interventions². Unfortunately, only two of three patients obtain complete remittance from their seizures³. Initial treatment approaches for epilepsy are usually conservative. The availability of anti-epileptic drugs, costs, and insurance coverage for pharmaceutical treatments appear generally addressed by health care systems around the world although there are patients whose insurance does not cover anti-epileptic drugs. However, the clinical outcomes of pharmaceutical treatments remain variable, indicating the need for novel and more effective therapeutic approaches. To this end, while first-line treatments for epilepsy include pharmaceutical management, surgical interventions stand as an alternative treatment option when medical management fails. Unfortunately, cell-based therapy represents an experimental surgical intervention, which probably may pose as a challenge for uninsured patients warranting case management resolution. Even surgical interventions only result in complete absence of seizures in 58% of patients with medically refractory temporal lobe epilepsy (TLE)^4,5. Over time, repeated epileptic episodes can result in cell death, activation of astrocytes, reactive oxidative species production, and changes to mitochondria function³. This aberrant functioning at the cellular level, alongside a plethora of patients with refractory epilepsy, implores researchers to consider novel treatment strategies, such as cell-based therapies³. This review will discuss current methods of surgical and pharmacological approaches for treating epilepsy while also delving into the less developed concept of using stem cells to reprogram and remodel neuronal networks to reduce epileptic burden.

Pharmaceutical Treatments for Epilepsy

The primary goal of anti-seizure drugs (ASDs) is to eliminate seizures while minimizing adverse side effects⁶. Medication is considered after two documented cases of unprovoked seizures or one seizure that occurred during sleep or in the presence of the electrocardiogram (ECG) or magnetic resonance imaging (MRI)⁶. The best practice is to wait for reoccurrence before starting treatment, as treatment after the first seizure will not alter prognosis⁷. However, those with a higher risk of occurrence, including individuals with an identified structural abnormality, an abnormal electroencephalograph (EEG), or pre-existing neurological deficit, should start sooner. Considerations when choosing a medication include factors such as age, sex, existing comorbidities, seizure type, and tolerability⁷. The two main types of seizures, focal and generalized, are neurologically different, and specific medications may work better for one type over the other. Furthermore, new-generation drugs are often better tolerated and have similar efficacy as previous generation drugs⁸. Previous work demonstrated that up to 47% of patients become seizure free on the first appropriately selected ASD⁹. It is therefore crucial that physicians understand the classes and mechanisms of ASDs to choose the right option for their patient. Monotherapy (single drug) is the best option as polytherapy (multiple drugs) may increase the risk of poor adherence, adverse drug interactions, and the potential for long-term toxicity. If polytherapy is required, the physician must make sure to not prescribe drugs in the same class to avoid cross sensitivity; use combinations that have synergistic effects; combine drugs with different mechanisms of action; and anticipate drug doses appropriately based on potential side effects⁹. Each drug should be introduced slowly with the dosage gradually raised to the maximum tolerated dose. If the patient does not receive benefit at the maximally tolerated dose, an alternative first-line drug should then be tried⁷. Drug-resistant epilepsy is defined as the failure of adequate trials of two appropriately chosen ASDs⁷. Surgical intervention is the next likely choice for these individuals (Figure 1).

Figure 1.

The primary underlying pathophysiology of epilepsy: aberrant excitatory and inhibitory signaling at the neural level. Stem cells may ameliorate this imbalance in signaling pathways, while also promoting brain repair secondary to epileptic episodes.

There are currently 26 US Food and Drug Administration (FDA) approved ASDs which fall into four main categories. Eight (benzodiazepines, lamotrigine, levetiracetam, perampanel, phenobarbital, topiramate, sodium valproate, and zonisamide) are used for focal and most generalized epileptic conditions. An additional 10 (brivaracetam, carbamazepine, eslicarbazepine acetate, gabapentin, lacosamide, oxcarbazepine, phenytoin, pregabalin, tiagabine, and vigabatrin) are used in focal conditions only. Ethosuximide is used in absence seizures only, and the additional five (cannabidiol, everolimus, felbamate, rufinamide, and stiripentol) are used in special encephalopathies⁷. These drugs are classified into four main types of mechanisms⁹. Ion channel modulators include those that exert their effects on sodium, calcium, and potassium channels. The sodium channel modulators are phenytoin, carbamazepine, and lacosamide. The calcium channel modulators are lamotrigine and ethosuximide⁹. A second class of drugs enhances the effect of inhibitory neurotransmission. For example, phenobarbital and benzodiazepines bind to the GABA-A complex at distinct sites, felbamate and topiramate activate the GABA-A receptor, and vigabatrin irreversibly inhibits GABA-transaminase⁹. Perampanel is the sole ASD that acts on glutamate to attenuate excitatory neurotransmission while others such as felbamate and topiramate have multiple mechanisms that include the attenuation of excitatory neurotransmission. Finally, the new generation of ASDs have novel mechanisms such as the ability of levetiracetam and brivaracetam to bind to synaptic vesicle 2A (SV2A) on presynaptic vesicles. This is believed to regulate vesicle shape and neurotransmitter trafficking⁹.

As with all medications, potential side effects and drug–drug interactions must be considered when choosing which ASD to prescribe. In all, 20% to 50% of users experience neurologic, psychiatric, cognitive, or mental disorders such as mood, anxiety, attention deficit, and migraines⁶. Additional side effects such as fatigue, dizziness, unsteadiness, and irritability may also occur⁷. Furthermore, Cytochrome P450 ASDs such as carbamazepine and phenytoin may worsen comorbid coronary and cerebrovascular disease due to hyperlipidemia⁶. Also, women with childbearing potential should avoid valproate due to the potential side effect of teratogenicity⁸. Additional research is needed to develop new ASDs to increase their success rate while decreasing the potential side effects.

Surgical Treatments of Epilepsy

Three different randomized control trials have shown that surgery for epileptic patients is effective, but this treatment option is often underutilized^5,10,11. These studies show that surgical treatment is safe, but less than 1% of epilepsy patients are referred for surgery¹². Misconceptions or fears about surgery may cause this underutilization, but results have shown that the seizure-free rate of individuals after surgery ranges from 50% to 80%⁷. With the development of advanced imaging techniques such as functional magnetic resonance imaging (fMRI), surgeons can locate the epileptic region and determine any post-surgical deficits that may result from surgery in that area of the brain. The prototypical surgical patient is one with TLE due to unilateral hippocampal sclerosis; but recent advances have widened the range of patients who may benefit from surgical intervention⁷. Of the roughly 60% of patients with focal epilepsy, 15% do not receive the relief they need from medications alone¹³. Individual cases which may benefit from surgery include TLE with focal lesions, lesional extratemporal epilepsies, hemispherical epilepsies, and gelastic epilepsy with hypothalamic hamartoma. Furthermore, corpus callosotomy and vagal nerve stimulation may be beneficial for children with diffuse and multifocal epilepsies¹³. Those with an electro-clinically concordant structural lesion on MRI have the best outcomes with seizure reduction in 60% to 70% of cases, whereas those with extratemporal lobe foci, focal-to-bilateral tonic-clonic seizures, normal imaging, psychiatric comorbidities, and learning disabilities often have lower success rates⁴. The future of epilepsy surgery includes techniques such as stereotactic radiosurgery, radiofrequency thermocoagulation, and laser interstitial thermal therapy⁷. More research is required in these fields, but they have the potential to improve surgical outcomes while lessening the chance of unintended brain damage. Surgical treatments for epilepsy are underused but should seriously be considered for patients with focal epilepsy where two to three medications have failed.

Neurostimulative Interventions for Epilepsy

A variety of interventional treatments for epilepsy exist, including deep brain stimulation (DBS), responsive neurostimulation (RNS), vagus nerve stimulation therapy (VNS), and trigeminal nerve stimulation (TNS). In the 2010 SANTE trial, DBS of the anterior nuclei of the thalamus (ANT) reduced seizures by 29% more compared with the control group¹⁴. When a follow-up was performed 2 years later, the researchers found a median 56% reduction in seizure frequency. These results led to FDA approval for DBS in epilepsy patients¹⁵. Further work in the field of DBS agreed that stimulation of the ANT reduced seizures between 46% and 90%. Furthermore, stimulation of the hippocampus resulted in a 48% to 95% reduction in seizures¹⁶. The ANT connects to the hippocampus via the mammillothalamic tract and fornix before projecting to the cingulate cortex and neocortex. This area is involved in emotional processing and seizure propagation¹⁶. However, stimulation of this area is associated with higher rates of self-reported depression and subjective memory impairment; thus, more work is needed to elucidate these causes to help prevent them in the future¹⁷. Furthermore, the hippocampus is a target for DBS due to its role in the Papez circuit, as hippocampal stimulation may attenuate epileptic activity originating in the medial temporal region¹⁶. Other areas of possible DBS such as the centromedian nucleus of the thalamus, the cerebellum, and the nucleus accumbens have yet to show significant beneficial results¹⁷.

RNS was approved in 2013 as a potential therapy for adults with uncontrolled focal seizures that are limited to one or two foci. RNS works through an implantable neurostimulator connected to one or two cortical strip leads each containing four electrodes¹⁸. These leads are surgically placed at the seizure foci where they continually monitor electrical activity and provide responsive electrical stimulation when necessary. The measurement thresholds and response parameters are individually tailored to suit the needs of the patient¹⁸. Studies have shown a reduction in seizure frequency of 44% after 1 year, 53% after 2 years¹⁹, and 48% to 66% in years 3 to 6²⁰. The most common side effect after a 5.4-year follow-up was implant site infection which occurred in around 9% of patients²⁰.

VNS entails a pulse generator implanted below the clavicle with an attached lead that is wrapped around the vagus nerve in the carotid sheath^21,22. Complete seizure freedom is rare, but previous work revealed that 26% to 40% of patients see a 50% reduction in seizure frequency²³. External trigeminal nerve stimulation (ETNS), a new experimental treatment, demonstrated a benefit in small sample size studies²⁴. This therapy entails a non-invasive neurostimulation therapy that is delivered bilaterally with adhesive skin electrodes. Experimental results show a drop of 43.5% in seizure frequency in the treated group versus the control group. The same study shows that ETNS improved quality of life without an increase in anxiety or depression, and no relevant adverse events were observed. Additional research into this field is required to determine the efficacy and safety of this therapy as it relates to the larger population before widespread use.

Stem Cell Therapy in Epilepsy

The application of stem cells for neurological disorders is a rapidly growing field. Research has uncovered potential benefits for degenerative disorders such as Parkinson’s and Alzheimer’s disease, stroke recovery, and epilepsy among other diseases²⁵. Stem cells exist at various levels of differentiation such as pluripotent, multipotent, and oligopotent cells with varying potential to develop into target tissue. They can often proliferate much more often than target tissue, aiding in the recovery of damaged tissue²⁶. Stem cells are an attractive option for use in the treatment of epilepsy because of their potential to replace damaged cells, restore cognitive function, and stabilize focal electrical activity. Indeed, early animal models display potential for restricting the duration and frequency of focal seizures^27,28. This can be life-changing for patients with medically refractory epilepsy because it provides an alternative to invasive or stimulatory techniques. In fact, the use of stem cells has a distinct advantage over certain stimulatory control techniques because stem cells do not require real-time detection of seizures to deliver a therapeutic inhibitory signal.

Grafting embryonic striatal precursor cells collected from the lateral ganglionic eminence into adult rats with induced status epilepticus (SE) reduced the frequency of spontaneous recurrent major motor seizures by up to 89%, at 12 months post-SE²⁷. This is likely due to the presence of inhibitory GABA-ergic neurons in the graft which could control the frequency and intensity of subsequent seizures. These findings only looked at the improvements on major motor seizures, but the grafting of GABA progenitors was later found to also decrease the frequency of electrographic seizures, with the added benefit of restoring behavioral deficits such as aggression and hyperactivity²⁹. Evidence shows that the benefits of stem cell therapy also extend to absence seizures seen in stargazer mouse models. The transplantation of medial ganglion eminence (MGE) cells into the primary visual cortex of mice produces a significant post-synaptic inhibitory current which holds promise for the treatment of absence seizures. In fact, stargazer mouse models grafted with MGE cells experienced significant rescue from absence seizures and experienced significantly lower excitability in the primary visual cortex during potassium-induced excitability challenges when compared with control stargazer mice³⁰.

The findings discussed so far have been restricted to mouse models and mouse-derived cell grafts, but use of human cells, although much less studied, yields similar results. For example, human fetal fibroblast cells can be converted into induced neuronal cells in vitro and subsequently matured, with robust survival in the short term after being transplanted into adult rats³¹. Promisingly, fetal human fibroblast-derived induced neurons transplanted into rat hippocampi progressively matured and displayed robust functionality and integration into their transplant sites³². This highlights the feasibility of using induced neuron cell grafts as a potential human source of stem cells for cell replacement therapy. Interestingly, human adipose stem cell extract administered to mouse models prior to pilocarpine-induced SE seems to reduce abnormal behavior induced by SE³³. This is likely due to the cytokines and growth factors contained within these cells which have been shown to protect against neuroinflammation and rescue damaged neurons³⁴.

Human umbilical mesenchymal stem cells (HUMSCs) can also display positive effects on epileptic rat models. These cells can be obtained from Wharton’s jelly of fetal umbilical cords, which can raise ethical concerns although certain ethically secure techniques can be used, such as obtaining them from medical waste after delivery. These cells have displayed neuroprotective properties in other applications such as stroke³⁵, with possible use in epilepsy. Pilocarpine-treated rats transplanted with HUMSCs experienced lower frequencies of recurrent motor seizures and experienced less tissue damage than control rats, showing that this neuroprotective effect extends to damage caused by recurrent seizures³⁶. HUMSC implantation also corrected the dysregulated adenosine receptor expression seen in rat models of chronic epilepsy, showing potential for the treatment of medically refractory epilepsy³⁷. Recently, autologous mesenchymal stem cells (MSCs) were tested in human patients with medically refractory epilepsy and caused most patients in the treatment group to either experience remission or begin responding to ASDs^38–40.

Mechanisms of Stem Cell Therapy for Epilepsy

Stem cells may provide therapeutic and neuroprotective benefits to epileptic patients in various ways. Endogenous neural stem cells (NSCs) are activated as a result of seizure activity^41,42. Following a seizure, the brain undergoes many pathological changes, including excitotoxicity, neuroinflammation, oxidative damage, and ultimately neurodegeneration⁴³. These changes may contribute to the initial increase in adult hippocampal neurogenesis, causing an activation of endogenous NSC that normally remains quiescent in the dentate gyrus⁴¹. These endogenous stem cells offer insufficient neuroprotection, as persistently elevated adult hippocampal neurogenesis eventually depletes the NSC pool, resulting in a diminished neuroregenerative capacity⁴¹.

Both exogenous and endogenous stem cells exert much of their effects by redefining the aberrant neuronal circuitry characteristic of epilepsy. Specifically, stem cells function to restore inhibitory GABA-ergic neurons and provide a counter to the hyperexcitability that characterizes seizures^44,45. MSCs may attenuate glutamate excitotoxicity following seizures, as they have been shown to migrate to rat hippocampi and protect neurons by downregulating N-methyl D-aspartate (NMDA) receptor expression and glutamate-induced calcium activity⁴⁴. This is a significant therapeutic effect, as excitotoxicity leads to neuronal death and an inflammatory environment incompatible with neuroregeneration⁴⁶. Furthermore, NSCs, human embryonic stem cells (hESCs), and MGE-derived interneuron precursors can replenish hippocampal GABA-ergic interneurons in the epileptic rats^47–49. Specifically, these cells can integrate into pre-existing neuronal networks^47,49 and provide nearby excitatory cells with inhibitory post-synaptic signals⁵⁰, reducing epileptogenic processes. Given the loss of GABA-ergic interneurons in the epileptic brain⁴⁸, protecting and replenishing them may serve as a significant mechanism in ameliorating epilepsy-induced damage. Stem cells may also exert their effects via astrocytes⁴⁴. NSCs can differentiate into astrocytes, which play a key role in regulating neuronal homeostasis, neuroinflammation, and synaptic activity⁵¹. Astrocytes may also directly decrease seizure activity, as they secrete anti-convulsant protective proteins, such as glial-derived neurotrophic factor (GDNF)⁴⁴. In addition, MSCs inhibit astrogliosis, a response to pathological conditions that is associated with neuroinflammation⁵¹.

The ability of stem cells to attenuate neuroinflammation and oxidative damage is key to their therapeutic effects. Seizures cause increased reactive oxygen species (ROS), which cause neuronal apoptosis, cell loss, and mitochondrial damage⁵². Given the susceptibility of hippocampal CA1 pyramidal neurons to oxidative stress⁵², reducing such stress may preserve hippocampal architecture and function. Transplanted MSCs can reduce oxidative stress and neuroinflammation in SE mice. Specifically, MSC-derived exosomes (MSC-Exo) protect against neuroinflammation and oxidative stress via nuclear factor erythroid 2–related factor 2 (Nrf2) signaling^51,52. Nrf-2, an antioxidant transcription factor, regulates redox homeostasis by inducing the expression of antioxidant proteins⁵³. By inducing Nrf-2 signaling, MSC exosomes diminish neuroinflammation and promote antioxidant activity, creating an environment conducive to tissue repair^51,52.

Recent Developments in Stem Cell Therapy

Outlined in the following text and Table 1 are pertinent preclinical studies that focus on stem cell treatment in epilepsy models from 2018 to 2022. These papers were identified via a PubMed search using the terms “stem cell and seizure” and “stem cell and epilepsy.” A subsequent review of the resulting 873 studies to include only those that relate to translational models of stem cell therapy results in the studies described below and in Table 1. A variety of different types of stem cells are used in experiments from different sources, most often murine or human. Epilepsy models typically use pilocarpine, pentylenetetrazol, or kainate to induce SE. As stated below, stem cells and related cell products (such as extracellular vesicles and exosomes) provide therapeutic benefits in epilepsy models, often reducing seizure frequency and duration, and improving neurobehavioral outcomes.

Table 1.

In Vivo Stem Cell Studies Targeting Epileptic Disease Models.

Citation	Sample	Cell type	Route	Dosage	Results	Mechanism
Fukumura et al.⁵⁴	Pilocarpine-induced SE rats	MSCs	Intravenous	1 × 10⁶ cells	Epileptogenesis is inhibited with preservation of cognitive function. Abnormal mossy fiber sprouting is suppressed.	Paracrine neuroprotective effect
Backofen-Wehrhahn et al.⁴⁷	PTZ-induced seizure rats with or without pilocarpine-induced SE	Human/rat/porcine MGE-derived and VM-derived NPCs	Intracranial	8 × 10⁴ or 1.5 × 10⁵ (STN); 8 × 10⁴ or 5 × 10⁵ (aSNr)	MGE-derived and VM-derived NPCs migrate and differentiate into inhibitory interneurons. Anti-convulsant effects are produced with human and porcine VM-derived NPCs in the STN.	Direct GABA-ergic activity
Anderson et al.⁴⁹	Pilocarpine-induced TLE mice	hESC-derived interneuron progenitors	Intrahippocampal	2 × 10⁵ cells	Transplanted progenitors differentiate into GABA-ergic interneurons. Cognitive function improves without suppression of seizures.	Direct GABA-ergic activity
Upadhya et al.²⁸	KA-induced SE	hiPSC-derived MGE-like interneuron precursors	Intrahippocampal	3 × 10⁵ cells	Transplantation ameliorates spontaneous recurrent seizures, and improves cognition, memory, and mood. Interneuron loss in the hippocampus and aberrant neurogenesis is decreased.	Direct integration as GABA-ergic interneurons as well as a paracrine neuroprotective effect
Xu et al.⁵⁵	Pilocarpine-induced epileptic rats	NSCs	Intrahippocampal	3 × 10⁶ cells	NSCs decrease the frequency of electroencephalography in addition to the frequency and duration of spontaneous recurrent seizures.	Direct GABA-ergic activity
Ali et al.⁴⁶	PTZ-induced epileptic rats	EPCs	Intravenous	2 × 10⁶ cells	EPCs migrate to the hippocampus to improve memory and motor deficits. BDNF is upregulated, neurotransmitter activity is stabilized, and autophagy is upregulated.	Paracrine neuroprotective effect
Xian et al.⁵⁶	Pilocarpine-induced SE rats	MSC-derived exosomes	Intraventricular	3.2 × 10⁹ particles	MSC-derived exosomes ameliorate learning and memory deficits.	Paracrine/exosomal neuroprotective effect
Kodali et al.⁵⁷	KA-induced SE rats	MSC-derived EVs	Intranasal	1 × 10¹⁰ particles	Unilateral intranasal injections of MSC-derived EVs leads to bilateral incorporation in all regions of the forebrain, with favorable migration to the hippocampal CA subfield and entorhinal cortex.	Paracrine/exosomal neuroprotective effect
Hattiangady et al.⁴⁸	KA-induced SE rats	NSCs	Intrahippocampal	3.2 × 10⁵ cells	NSCs differentiate into GABA-ergic interneurons, astrocytes, and oligodendrocytes and express FGF-2, BDNF, IGF-1, and GDNF. This reduces abnormal neuronal migration, maintains normal neurogenesis, and diminishes progression of epileptogenic processes.	Direct integration as GABA-ergic interneurons as well as a paracrine neuroprotective effect
Liu et al.⁵¹	Pilocarpine-induced SE mice	IL-1β-treated MSC exosomes	Intraventricular	1.5 μL particles	IL-1β-treated MSC exosomes reduce neuroinflammation and improve cognitive function.	Paracrine/exosomal neuroprotective effect
Luo et al.⁵²	Pilocarpine-induced SE mice	MSC-derived EVs	Intravenous	50 μg particles	MSC-EVs upregulate the Nrf2 pathway to promote neurorestoration against oxidative damage from seizure-induced hippocampal injury.	Paracrine/exosomal neuroprotective effect
Wang et al.⁵⁸	KA-induced TLE rats	ADSCs	Intrahippocampal	5 × 10⁴ cells	ADSCs inhibit seizure activity and restore learning capacity, associated with a release of BDNF, NT3, NT4, and anti-apoptotic factors.	Paracrine neuroprotective effect
Waloschková et al.⁵⁰	KA-induced SE rats	hESC-derived GABA-ergic interneuron precursors	Intrahippocampal	1 × 10⁵ cells	GABA-ergic precursors promoted inhibitory synaptic connections between host neurons, reduced the rate of epileptiform discharges, and decreased both the frequency and length of spontaneously recurring seizures.	Direct GABA-ergic activity
Venugopal et al.⁵⁹	KA-induced SE mice	Dental pulp stem cells or BM-MSCs	Intrahippocampal	1 × 10⁵ cells	Dental pulp stem cells are more effective than BM-MSCs in preventing hippocampal neurodegeneration and neuroinflammation while promoting neurogenesis and cognitive function through downregulation of apoptosis.	Paracrine neuroprotective effect
Upadhya et al.⁶⁰	KA-induced TLE rats	hiPSC-derived MGE-like interneuron precursors	Intrahippocampal	3 × 10⁵ cells	Interneuron grafting reduces spontaneous recurrent seizures and ameliorates cognitive function.	Direct integration as GABA-ergic interneurons as well as a paracrine neuroprotective effect
Arshad et al.⁶¹	Pilocarpine-induced TLE mice	MGE-derived GABA-ergic progenitors	Intrahippocampal	1 × 10⁵ cells/μL	GABA-ergic progenitors reduce aberrant neurogenesis patterns, as evidenced through reductions in inverted type 1, type 2, and hilar ectopic type 3 cells.	Direct integration as GABA-ergic interneurons as well as a paracrine neuroprotective effect

This table outlines cell-based preclinical trials finding improved functional outcomes in epileptic disease from 2018 to 2022.

SE: status epilepticus; STN: subthalamic nucleus; PTZ: pentylenetetrazol; KA: kainic acid; GABA: γ-aminobutyric acid; NSC: neural stem cell; BDNF: brain-derived neurotrophic factor; FGF-2: fibroblast growth factor 2; IGF-1: insulin-like growth factor 1; GDNF: glial cell–derived neurotrophic factor; NT: neurotrophin; TLE: temporal lobe epilepsy; MSC: mesenchymal stem cell; BM-MSC: bone marrow–derived mesenchymal stem cell; NPC: neural progenitor cell; EPC: endothelial progenitor cell; hESC: human embryonic stem cell; hiPSC: human-induced pluripotent stem cell; ADSC: adipose-derived stem cell; MGE: medial ganglionic eminence; VM: ventral mesencephalon; EV: extracellular vesicle; Nrf2: nuclear factor erythroid 2–related factor 2; CA: cornu ammonis.

Fukumura et al.⁵⁴ sought to understand whether the systemic infusion of MSCs could attenuate epileptogenesis in a lithium-pilocarpine rat model of SE. Seizure frequency was quantified using a video-monitoring system, and a Morris water maze test was used to assess cognitive function of animals. The findings showed that MSC therapy reduced seizures and improved cognitive function of SE rats. Green flourescent protein staining also confirmed that the MSCs localized to the rat hippocampus, and thus promoted neuronal survival. The exact mechanism for this neuroprotective effect is unclear, but it may involve the direct preservation of GABA-ergic interneurons by the infused MSCs. Manganese-enhanced MRI and Timm staining also confirmed that MSC treatment decreased aberrant mossy fiber sprouting in the dentate gyrus of SE rats. Therefore, MSCs may have attenuated epileptogenesis by controlling neuronal death and preventing aberrant mossy fiber sprouting.

Seeing that various partial seizure types can be remotely controlled via inhibition of the subthalamic nucleus or substantia nigra pars reticulata, Backofen-Wehrhahn and others⁴⁷ investigated whether the transplantation of neural precursor cells (NPCs) into the above-mentioned brain sites could ameliorate seizures in pentylenetetrazol-injected rats. The group used NPCs harvested from the ventral mesencephalon and MGE of humans, pigs, and rats. The findings of their study showed that transplanted NPCs migrated as expected, transformed into GABA-ergic inhibitory interneuron phenotypes, and survived ≥4 months post-transplantation. Temporary anti-epileptic effects were also observed in rats that received bilateral grafting of NPCs derived from human and pig ventral mesencephalon into their subthalamic nucleus, but not into the substantia nigra. Unfortunately, NPCs derived from the MGE did not produce significant effects in either injection site, despite pretreatment of these cells with retinoic acid and potassium chloride to promote their differentiation into GABA-ergic neurons.

Anderson et al.⁴⁹ investigated whether hESC-derived interneuron progenitors could appropriately differentiate into GABA-ergic cells, correct hippocampus-dependent spatial memory deficits, and attenuate seizures in pilocarpine-treated mice. In their study, they used hESC-derived interneuron progenitors and transplanted them into the hippocampi of animals. The findings showed that the transplanted cells differentiated into GABA-ergic interneurons. Mice that received these cells showed improvement in Morris water maze performance, but not attenuation of seizures, contrary to the findings of most preclinical studies. The lack of effect of the transplant on seizures was attributed to cell type heterogeneity of the transplants.

In another study, Upadhya et al.²⁸ investigated the effects of human-induced pluripotent stem cell (hiPSC)–derived MGE-like interneurons in a TLE model. The hiPSC-derived MGE-like interneuron precursors were grafted into rat hippocampi following SE. They reported that grafted cells survived well, migrated into the different areas of the hippocampus, and differentiated into various types of inhibitory interneurons that express calcium-binding proteins and neuropeptides. Behaviorally, grafting of the cells also controlled spontaneous recurrent seizures (SRSs), and improved cognitive and memory deficits of SE animals. In addition, it reduced interneuron death and aberrant mossy fiber sprouting in the dentate gyrus, displaying a paracrine neuroprotective effect via the release of neurotrophic factors. Furthermore, efficient graft–host synaptic integration was observed as evidenced by axons from graft-derived interneurons forming synapses with dendrites of host excitatory neurons in the dentate gyrus and CA1 regions of the hippocampus. A recent study by the group further confirmed the grafted cells’ direct regulation of SRS and improvement of cognitive functions of rat models of TLE⁶⁰. Using hiPSC-derived MGE-like GABA-ergic progenitors that were engineered to express inhibitory designer receptors exclusively activated by designer drugs (DREADDs), they showed that activation of these DREADDs-expressing cells transplanted into the hippocampi reduced SRS and memory impairment. Deactivating them through the use of a designer drug produced the opposite effect, that is, it increased SRS and impaired memory functions of TLE rats.

Waloschkova and others⁵⁰ examined effects of hESC-derived GABA-ergic interneuron precursors grafted into rat hippocampi following kainate-induced SE. They observed that grafted cells were forming inhibitory GABA-ergic synaptic connections onto host neurons. This treatment reduced SRS frequency and duration compared with non-transplanted controls.

Xu and colleagues⁵⁵ examined whether GABA-ergic neurons generated in vitro from NSCs reduces SRS frequency and duration and compared their effects with those of intrahippocampal transplantation of NSCs. Using a pilocarpine-injection TLE model, they showed that transplantation of the differentiated cells decreased the seizure frequency and duration of SRS and achieved the highest number of GABA interneurons expression in the hippocampus compared with NSC transplantation and phosphate-buffered saline treatment (control). Moreover, GABA levels were also increased in the hippocampus of GABA interneuron-transplanted rats. Thus, the differentiated cells successfully grafted into the hippocampi of epileptic rats and produced anti-epileptic effects by enhancing GABA-mediated inhibition.

Ali et al.⁴⁶ explored the effects of intravenously administered endothelial progenitor cells (EPCs) in a pentylenetetrazol-induced epilepsy model in rats. They reported that EPCs migrated into the hippocampus and improved the memory and motor deficits of rats. There was a neuroprotective paracrine effect leading to an increase in brain-derived neurotrophic factor (BDNF) expression as well as autophagy-related proteins: light chain protein-3, beclin-1, and autophagy-related gene-7. Increasing autophagy activity is beneficial, allowing neurons to properly ensure equilibrium between synthesis and degradation of intracellular substances.

MSC-Exo exert substantial anti-inflammatory effects in the treatment of neurological disorders, including epilepsy. Xian et al.⁵⁶ investigated the mechanism behind MSC-Exo’s robust anti-inflammatory effects in in vitro and in vivo epilepsy models. They showed that MSC-Exo integrated well into hippocampal astrocytes and decreased reactive astrogliosis and inflammatory responses. Importantly, MSC-Exo improved learning and memory impairments of mice subjected to pilocarpine-induced SE. Inhibiting the Nrf2 pathway via ML385 injection in SE rats decreased the putative therapeutic effects of MSC-Exo. They proposed that the Nrf2 signaling pathway mediates the anti-inflammatory effects of MSC-Exo, and the therapeutic value of MSC-Exo in controlling seizures. In a different study, Liu et al.⁵¹ explored the mechanism underlying the therapeutic effects of exosomes derived from Interleukin-1β treated MSCs (IL-1-Exo) on SE mice. The IL-1-Exo reduced the inflammatory response and enhanced cognitive functions of SE mice. Moreover, they also showed that the Nrf2 pathway is involved in the anti-inflammatory effects of IL-1 Exo.

MSC-derived extracellular vesicles (MSC-EVs) attenuate oxidative stress-induced neuronal damage and show promise as neurological disorders treatment. Luo et al.⁵² further showed that MSC-EVs restored oxidative stress-induced dendritic spine alterations, electrophysiological changes, mitochondrial changes, and other functional and structural impairments in hippocampal neurons. Using mouse seizure models, they also showed that MSC-EVs improved cognitive functions of rats. Moreover, their studies showed that the antioxidant activity of MSC-EVs was exerted through the Nrf2 signaling pathway. This study further demonstrates the value of MSC-derived nanotherapeutics as epilepsy treatments.

In view of these outcomes, Kodali et al.⁵⁷ examined the impact of intranasally administered MSC-EVs in SE rats. Intranasal administration is non-invasive and allows repetitive administration and rapid delivery of EVs into multiple forebrain regions. The group administered 10 billion EVs via the left nares of control rats and those that underwent 2 h of kainate-induced SE. Six hours post administration, EVs were observed bilaterally in nearly all regions of the forebrain in both SE mice and controls. The percentage of neurons that incorporated EVs was comparable between groups for most forebrain regions, except in the hippocampal CA1 region and the entorhinal cortex, in which the percentage was higher in the SE group. Notably, these brain regions are most vulnerable to neurodegeneration after experimental SE. Therefore, unilateral intranasal administration of EVs is an effective method to deliver EVs to forebrain regions. That the integration of EVs was higher in injured neurons indicates that injury-related signals help in the penetration and incorporation of EVs in neurons. Moreover, the findings further demonstrate the therapeutic potential of MSC-EVs in epilepsy.

Hattiangady et al.⁴⁸ performed bilateral hippocampal grafting of neural progenitor cells 6 days after SE in animals to examine the effect of the transplant on the chronic phase of epilepsy. They showed that 8 months post-SE, the transplantation attenuated frequency and severity of SRS and improved memory. The grafted cells migrated into the hippocampus and differentiated into GABA-ergic interneurons, astrocytes, and oligodendrocytes, and also exhibited a neuroprotective paracrine effect. There was an increase in BDNF, fibroblast growth factor-2, insulin-like growth factor-1, and glial cell line–derived neurotrophic factor. The graft also improved host neurogenesis and reduced aberrant mossy fiber sprouting in the dentate gyrus.

Wang et al.⁵⁸ investigated the efficacy of adipose-derived stem cells in kainate-induced epilepsy rat models. They showed that the transplanted cells inhibited EEG seizure activity and restored learning capacity and memory of rats as measured by the Morris water maze conducted 2 weeks and 2 months post-transplantation. The proposed mechanism points to a neuroprotective effect due to the release of BDNF, NT3, and NT4 to reduce apoptosis within the hippocampus. Proapoptotic BAX was reduced, whereas anti-apoptotic Bcl-2 and Bcl-xL were increased.

Knowing that transplanted GABA-ergic interneurons form synaptic contacts with host cell, and help control seizures, Arshad et al.⁶¹ investigated whether grafted GABA-ergic progenitors into the dentate gyrus ameliorated existing abnormalities in adult neurogenesis due to TLE. Accordingly, TLE alters neurogenesis by increasing neuronal proliferation and abnormal inversion of Type 1 progenitors, leading to the ectopic migration of Type 3 progenitors into the hilus of the dentate gyrus. Upon their maturation into granule cells, they become hyperexcitable and thus contribute to SRS. Arshad et al. showed that GABA-ergic progenitors transplanted into intact mice increased GABA-ergic interneurons in the dentate gyrus and significantly reduced type 2 progenitors. Type 3 progenitors were also increased. However, in epileptic mice, the transplantation resulted in reductions of inverted type 1, type 2, and hilar ectopic type 3 cells. It also resulted in increased radial migration of type 3 cells into the granule cell layer of the hippocampus. These effects are presumed to be due to paracrine signaling changes caused by the implanted progenitors. Therefore, hilar transplantation of GABA-ergic interneurons may correct aberrant adult neurogenesis due to TLE and prevent seizures.

The recent research on stem cell therapy has elucidated new target pathways, methods of administration, and increased our knowledge on the integration of transplanted stem cells in translational epilepsy models. Other areas of neurological disease, such as stroke, have expert consensus and recommendations that direct future research in the field. For example, stem cell therapy as an emerging paradigm for stroke (STEPS) is a report generated to guide translational research on cell-based restorative therapy in stroke^62,63. This was later expanded via the RIGOR guidelines in 2013⁶⁴. A similar consensus and set of guidelines are missing in epilepsy stem cell research and could be beneficial for the structured development of the field. One of the important future directions of research will be to assess the safety and efficacy of stem cell therapy when combined with current established pharmaceutical and surgical interventions. Most patients who will qualify for stem cell therapy will have undergone several prior lines of therapy, and it is important to ensure their safety. Combining different treatments with stem cells may also result in a better outcome, so it is important to identify the most efficacious combination therapies for different epilepsy models.

Conclusion

Stem cell therapy is an emerging field with a promising future. Epilepsy has long been treated with medical, surgical, or interventional techniques, but among the emerging therapies lies the potential for stem cells to offer a potent and effective new way to treat the condition. Experiments with animal models display a striking capacity for stem cell grafts to inhibit major motor, electrographic, and absence seizures while also exhibiting neuroprotective and regenerative properties. Cells can be administered both before and after the onset of SE for varying neuroprotective effects. More recently, focus has shifted from animal-derived cell lines to the usage of human-derived cells such as mesenchymal and fibroblast cells. Limited human trials have taken place but as the body of evidence matures, it will become critical to apply the accumulated knowledge to humans in clinical trials to assess the safety of this therapy in humans and how well these results can translate to real-world applications.

Footnotes

Acknowledgements

We acknowledge the work of brgfx who designed the vectors used in Figure 1. The vectors were downloaded from .

Author Contributions

Conceptualization, A.A. and C.V.B.; investigation, A.A., G.L., J.G., J.C., M.M., S.S., and I.P.; writing—original draft preparation, A.A., G.L., J.G., J.C., M.M., S.S., and I.P.; writing—review and editing, A.A., G.L., J.G., J.C., M.M., S.S., I.P., and C.V.B.; visualization, A.A., G.L., J.G., J.C., M.M., S.S., and I.P.; supervision, C.V.B. All authors have read and agreed to the published version of the manuscript.

Ethical Approval

This study was approved by our institutional review board.

Statement of Human and Animal Rights

This article does not contain any studies with human or animal subjects.

Statement of Informed Consent

There are no human subjects in this article and informed consent is not applicable.

Declaration of Conflicting Interest

The author(s) declared the following potential conflicts of interest with respect to the research, authorship, and/or publication of this article: C.V.B. declared leadership position with University of South Florida, patents holder and patent applications on stem cell biology and its therapeutic applications, consultant to a number of stem cell–based companies, and research funding from the NIH. All of the other authors declared no potential conflicts of interest.

Funding

The author(s) received no financial support for the research, authorship, and/or publication of this article.

ORCID iDs

Adam Alayli

Jonah Gordon

Ike Dela Peña

Cesar V. Borlongan

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