Introduction
Despite available antiseizure medications (ASMs), drug resistant epilepsy (DRE) remains poorly controlled in approximately one-third of patients [1, 2].
The seizure-free rate after resective surgery for DRE is estimated at 59% [3]. This rate usually diminishes with a longer follow-up [3]. The seizure-free rates for temporal lobe epilepsy at 5 and 10 years after surgery are estimated at 61% and 45%, respectively [3]. However, up to 50% of patients suffering from DRE are deemed to be not suitable candidates for resective surgery [4]. For this group of patients, neuromodulation therapies may constitute the last resort in the treatment of DRE.
If resective surgery cannot be offered because of the involvement of the eloquent areas or the multifocal nature of the ictal epilepsy onset, the thalamic nuclei are an attractive region for neuromodulation. The stimulation of thalamic nuclei involves the stereotactic placement of deep brain stimulation (DBS) leads connected thereafter through connection cables to an implantable pulse generator (IPG) placed in the chest wall.
This review article will discuss the clinical application of anterior nucleus of the thalamus (ANT) and centromedian nucleus of the thalamus DBS. ANT DBS is CE marked and FDA-approved target for DBS as adjunctive therapy for patients 18 years of age or older affected by partial-onset seizures with or without secondary generalisation. The CMN DBS is not a CE marked or FDA-approved procedure. It is used for primary generalised seizures in the treatment of Lennox-Gastaut syndrome (LGS).
Another neuromodulatory technique is responsive neurostimulation (RNS). This technique has recently emerged as a safe and effective treatment for some patients with medically refractory focal epilepsy who are not candidates for surgical resection. RNS was approved in the United States in 2013 and to date c.1,800 patients have been treated worldwide [5]. RNS involves an implanted neurostimulator and intracranial leads that detect incipient seizures and respond with electrical counterstimulation [5]. Unlike thalamic DBS, which involves prespecified electrode locations within ANT or CMN, RNS involves intracranial strip and/or depth electrodes that can be flexibly configured based on knowledge of the seizure onset zone [5, 6]. Clinical studies have shown that RNS is a well-tolerated treatment option for patients especially with mesial temporal lobe epilepsy who are not candidates for a temporal lobe resection [5, 6].
ANT or CMN DBS can influence a widespread region of the cerebral cortex and limbic system. Thalamic stimulation is aimed to preserve brain tissue, and is adjustable and reversible [7, 8].
The purpose of this literature review was to present up-to-date knowledge regarding the clinical efficacy and safety of ANT and CMN DBS for DRE.
Paper selection
We conducted a systematic literature search for publications regarding DBS for DRE including the following thalamic nuclei: ANT and CMN, spanning the period from January 1980 to July 2023. The search algorithm included the following key words: deep brain stimulation, thalamic stimulation for drug-resistant epilepsy, stimulation of the anterior nucleus for epilepsy, stimulation of the centromedian nucleus for epilepsy, and thalamic stimulation. The following electronic databases were consulted: the Medical Literature, Analysis, and Retrieval System on-line (MEDLINE) and the Cochrane Central Register of Controlled Trials (CEN-TRAL). The search algorithm followed the PRISMA guidelines [9]. There were considered only research articles published in English. The research articles were restricted to the clinical studies involving only humans. No limitations were made regarding the study design. Clinical studies with at least three individuals with a minimum postoperative follow-up of 6 months DBS were included in our analysis.
The exclusion criteria included: animal studies, studies that included treatment of DRE without DBS, preclinical studies, review articles, letters to the editor, as well as clinical studies with fewer than three patients. The exclusion criteria also included articles describing patient populations other than those with DRE, and reports that mainly dealt with aspects related to surgical technique.
In relation to the fact that two thalamic nuclei constituted the separated targets, the flowchart showing the search strategy for both thalamic nuclei is presented separately in Figure 1. The search using these two databases and the above-mentioned key words yielded 43 articles presented in Figure 1. Among these, 30 articles were related to ANT DBS for DRE reporting cumulative number of approximately 635 patients. Thirteen articles were related to CMN DBS for DRE reporting cumulative number of 147 patients.
Indications and contraindications for ANT DBS
ANT is an FDA-approved and best-studied thalamic target for DBS to treat DRE [7, 8, 10, 11]. The ANT plays pivotal role in the circuit of Papez [12]. This nucleus connects to mesial, frontal and temporal regions. These brain regions are most often involved in focal epilepsy [8]. The efficacy of ANT DBS has been best documented in focal onset seizures originating from temporal or frontal lobes with or without secondary generalisation. Other predictors for ANT DBS efficacy are: age at seizure onset, normal MRI without structural abnormalities, lateralised EEG abnormality, and positive performance in executive functions [7, 9, 13–18]. Patients with DRE in whom a VNS or prior resective epilepsy surgery have failed, have also shown seizure reductions comparable to those individuals without these prior therapies [7, 19, 20].
The main contraindication for ANT DBS is a progressive neurological aetiology, usually defined as a brain tumour, Rasmussen encephalitis or dementia. Other contraindications include a history of psychogenic seizures, depression or memory deficit, suicide attempts, and psychosis unrelated to epilepsy [7, 11, 13, 16, 17]. Cognitively impaired patients who are unable to complete a neuropsychological assessment, or with an IQ of less than 70, are usually excluded from ANT DBS [7, 19].
Clinical efficacy of ANT DBS for treatment of DRE
Upton et al. in 1985 were the first to report the outcomes of ANT DBS in 6 patients with intractable epilepsy [10]. Four of the 6 patients showed a marked seizure frequency reduction and also an improvement in psychiatric symptoms. In subsequent open-label studies, the seizure reduction ranged from 54% to 75.6% with a follow-up ranging from 10.6 to 43.8 months [11, 13, 15, 16, 22, 23]. An uncontrolled study by Andrade et al. reported a 60-month follow-up in 6 patients after ANT DBS who were all responders with at least 50% complex partial seizure reduction [17]. Based on this pilot trial, a multicentre, randomised, controlled trial was initiated [7]. The acronym of this trial was ‘SANTE’ (Stimulation of the Anterior Nucleus of the Thalamus for Epilepsy) [7]. In this trial, over two years, there was a 56% median seizure frequency reduction, and 54% of patients were responders (defined as at least 50% seizure reduction) [7]. Five years after ANT DBS, the mean seizure frequency reduction was 69%, and the responder rate reached 68% [19]. In a 5-year follow-up, 16% of patients were seizure-free for at least 6 months [19]. Salanova et al. evaluated the efficacy and safety of ANT DBS after 7 and 10 years [20]. The most severe seizures, mainly focal to bilateral tonic clonic seizures (FBTCS), were reduced by 71% at 7 years, while focal impaired awareness seizures (FIAS) were reduced by 78%, and focal aware seizures (FAS) by 92%. At 7 years, the overall median seizure frequency reduction was 75%, with no outcome differences related to prior vagus nerve stimulation or resective surgery [20].
In the studies which followed the SANTE trial, the median seizure frequency reduction ranged from 50% to as much as 80.3%, with a responder rate exceeding 70–80% of patients [18, 21, 22, 24–42]. The outcomes of ANT DBS studies are set out in Table 1. In 2023, Peltola et al. reported the outcomes of the MORE Multicentre Patient Registry Study of ANT DBS [39]. Of the 191 patients recruited, 170 were implanted. The median monthly seizure frequency reduction at 2 years was 33.1%, and in 47 patients who completed 5 years follow-up, the median monthly seizure frequency reduction was 53.2% [39]. There were two factors which influenced strongly the outcomes: the centres recognized as high volume centres with more than 10 ANT DBS surgeries, and the presence of preoperative cognitive impairment. High-volume centres had a 42.5% monthly seizure frequency reduction, compared to 25.8% in low volume centres at 2 years. The absence of cognitive impairment resulted in a 36.1% monthly seizure reduction compared to a 26% reduction in patients with cognitive impairment [39].
Other factors (seizure origin, previous VNS therapy, resective surgery) affecting outcome of ANT DBS
Clinical long-term follow-up studies of ANT DBS have revealed that seizures originating in one or both temporal lobes, as well in frontal lobes, have a clearly better prognosis than seizures with their origin in parietal or occipital lobes [7, 19, 20].
The origin of the seizure focus may even have a stronger correlation with a long-term follow-up after ANT DBS [19, 20]. After 7 years of ANT DBS, the mean seizures frequency reductions for seizures originating in the frontal, temporal, and parietal/occipital lobes were 86%, 78% and 39% respectively [20]. Patients with multiple epileptic foci coexisted with structural brain abnormalities do not respond so favourably to ANT DBS [7, 16, 17–18]. As mentioned above, previous VNS therapy did not affect the final outcome [20]. At 7 years, patients who had previous VNS achieved a 75% mean seizure reduction compared to a 78% reduction in patients who had no prior VNS [20]. Subjects who had previous resective surgery had a median seizure frequency reduction of 69% at 7 years versus 75% without a history of resective surgery [20].
Although the evidence for the clinical effectiveness of VNS and DBS exists, the exact mechanisms of action remain unexplained [37]. PET studies during VNS have shown increased cerebral bloodflow in the thalamus [44]. This increased synaptic thalamic activity may mediate the anticonvulsant effects of VNS therapy. ANT DBS directly modulates thalamocortical activity through anterior thalamic radiation affecting the frontal lobes and limbic seizure network. Further work is needed to fully understand the effects of VNS and ANT DBS on epilepsy [20].
The predictors of clinical outcome of ANT DBS remain to be defined. A newer approach to predict the outcome to ANT DBS is the implantation of functional connectivity between the ANT and the seizure foci [45]. Xu et al. examined 18 patients with two or more seizure foci using normative human connectome data derived from 1,000 healthy participants. The authors performed functional connectivity between the seizure foci and the ANT. The degree of functional connectivity between ANT DBS and seizures foci were strongly correlated with seizure reduction [45]. The authors concluded that functional connectomic profile is a potentially reliable non-invasive biomarker to predict ANT-DBS outcomes [45]. Accordingly, the identification of ANT responders could decrease the surgical risk for patients who may not benefit and optimise the cost-effective allocation of healthcare resources.
Targeting and trajectory planning during ANT DBS surgery
One of the predictors for successful ANT DBS is the accurate placement of a DBS electrode within ANT, which ensures the optimal therapeutic effect [46, 47]. An indirect targeting method (in reference to the anterior commissure/posterior commissure line) for stereotactic determination of the ANT may not be applicable in epilepsy surgery [46, 47].
It has been shown that patients with long-standing intractable epilepsy have disturbed brain architecture, not only in the epileptic focus (foci) but also in the distinct brain areas, including the ANT. ANT atrophy is recognizable in patients with longstanding mesial temporal lobe epilepsy [48]. Most authors point out that indirect stereotactic coordinates should be used cautiously and corrections should be made following the individual patient’s anatomy [46, 48]. Direct visualization of the ANT and surrounding white matter tracts such as mammillothalamic tract (MTT), external and internal medullary laminae may be accomplished by following MRI sequences such as short tau inversion recovery (STIR) or T1-weighted magnetisation prepared gradient echo (MPRAGE) [48, 49]. Fast grey matter acquisition T1 inversion recovery (FGATIR) is another 3 Tesla MRI sequence that provides thin, high-resolution images with significantly better visualisation of ANT compared to standard 3 Tesla T1 and T2-weighted images [49].
In epilepsy surgery, it is not only the ANT targeting that is challenging but also the planning of stereotactic trajectories. Most authors have used a transventricular rather than an extraventricular approach [7, 19, 20]. An alternative novel extraventricular approach with entry points (burr holes) placed in parietal regions has been recently proposed [50]. Using this parietal extraventricular approach, a successful ANT targeting rate of 90% electrode placed bilaterally within ANT was achieved. Two or more contacts within the ANT were presented in 75% of all leads [50]. In the MORE study, the success rate of placing contacts within the ANT was strictly associated with the selection of a transventricular rather than an extraventricular trajectory [51]. The transventricular approach is thus regarded as the standard and best established approach for ANT DBS [19, 20, 51].
Search for ideal target in ANT DBS for DRE
The exact best location for stimulation within ANT remains a matter of controversy. According to the experience of Lehtimäki et al., stimulation of the ANT complex has a powerful anti-seizure effect [46, 47, 51]. Stimulation at the anterior aspects of ANT reaches anteromedial (AM) and anterior principal (Apr) subnuclei [47]. AM has well established connections to the frontal cortex, anterior cingulum, retrosplenial cortex, amygdala and hippocampus [12, 14]. Guo et al. found that active contacts located more adjacent to the centre of gravity of the anterior half of the ANT volume defined as anterior centre (AC) have the best effects on seizure reduction [33].
Krishna et al. have suggested that a basolateral part of the ANT that corresponds to the anteroventral (AV) subdivision of the ANT is the most efficacious site to be stimulated [22]. This site correlates to a region posterior and superior to mtt. The search for the optimal ANT target requires further detailed studies that will correlate the exact anatomical location of active contact(s) within ANT with a clinical outcome [12, 14–18, 22, 32]. The recent study by Schaper et al. suggested that stimulation of ANT-mtt junction was associated with increased seizure control, suggesting that co-stimulation of white matter of mtt may play a pivotal role in seizure control [32].
The effects of the ANT DBS on the efferents of mammillary bodies (nuclei), mainly the white matter tracts including mammillothalamic (mtt) and mammillotegmental (mtgt) tracts, may regulate the memory function. Recent studies in animals have provided evidence that mammillary body efferents are involved in regulating memory independently from the hippocampus, but the importance of these individual components in human brain functional anatomy associated with memory remains unexplained [52]. Mtgt takes part in controlling visceral functions and transforming spatial data by influencing the brainstem’s autonomic nuclei. Moreover, anatomical findings suggest that tegmental afferent fibres play a crucial role in modifying transport information from hippocampal formation to the anterior thalamus [52]. Postoperative MR imaging in different sequences with implanted ANT DBS leads is set out in Figure 2.
Stimulation parameters, polarity, and mode of ANT stimulation
There are no guidelines regarding setting the initial stimulation parameters in patients undergoing ANT DBS, and various authors have used different stimulation parameters, modes, and polarities (Tab. 1). The image-verified localisation of implanted DBS leads may be of great importance for choosing appropriate contacts, stimulation polarity, and mode [7, 19, 20, 53]. It has been shown that improperly placed DBS leads have a suboptimal effect on the seizure frequency reduction, and replacements have been warranted [7, 19, 53]. Moreover, stimulation of contacts outside the ANT can elicit unwanted psychiatric adverse events or cause subjective mood and memory problems [54].
|
Authors |
Country of study’s origin |
Number of |
Follow-up, |
Responder rate, number |
Seizure |
Stimulation parameters |
Mode |
Stim. |
|
Upton et al. 1987 [10] |
United States |
6 |
42 |
4 |
NR |
60–70 Hz 300 us 3.5–3.8 V |
C |
NA |
|
Hodaie et al. 2002 [13] |
Canada |
5 |
15 |
3 |
54% |
100 Hz 90 us 10 V |
I |
B/M |
|
Kerrigan et al. 2004 [11] |
United States |
5 |
6-36 |
4 |
48% |
100 Hz 90 us 1–10 V |
I |
B |
|
Lee et al. 2006 [23] |
South Korea |
3 |
11.2 |
3 |
75.4% |
130 Hz 90 us 10 V |
I |
M |
|
Andrade et al. 2006 [17] +1 patient, 5 previously reported by Hodaie |
Canada |
6 |
60 |
5 |
more than 50% |
10–185 Hz 90–120 us 1–10 |
I |
B/M |
|
Lim et al. 2007 [15] |
Taiwan |
4 |
43.8 |
1 |
51% |
90–180 Hz 60–120 us 4–7 V |
C/I |
B |
|
Osorio et al. 2007 [16] |
United States March 2000 to July 2004 |
4 |
36 |
4 |
75.6% |
175 Hz 90 us 4.1 V |
I |
M |
|
Fisher et al. 2010 [7] |
United States Trial registration 18 January, 2005 |
110 |
25 |
54% |
56% |
145 Hz 90 us 5 V |
I |
M |
|
Salanova et al 2015 [19] |
United States Trial registration 18 January, 2005 |
83 |
61 |
68% |
69% |
145 Hz 90 us 5 V |
I |
M |
|
Lee et al. 2012 [18] |
South Korea From 2005 |
15 |
27 |
12 |
70.4% |
100–185 Hz 90–150 us 1.5–3.1 V |
C |
M |
|
Piacentino et al. 2015 [25] |
Italy 2007 to 2011 |
6 |
12 |
2 |
50% |
140 Hz 90 us 4 V |
I |
B |
|
Krishna et al. 2016 [22] 5 pts previously published |
Toronto, Canada Early cohort 5 pts + 11 new pts |
16 |
52 |
11 |
NR |
> 100 Hz 90 us 2.4–4.7 V |
C |
M |
|
Kim et al. 2017 [21] |
South Korea From 2005 Early cohort 15 pts |
30 |
74.9 |
NR |
70% |
130 Hz 90 us 1.5–3.1 V |
C |
M |
|
Sitnikov et al. 2018 [24] |
Russia Time period NR |
12 |
7 months to 5.2 years |
NR |
80.3% |
130 Hz 90 us 1.5–4 V |
C |
M/B |
|
Hermann et al. 2018 [26] |
Norway April 2010 to March 2015 |
18 |
12 |
4 |
NR |
145 90 Hz 5 V |
I |
NR |
|
Park et al. 2019 [27] |
South Korea 2016 to 2017 |
7 |
12–18 |
5 |
58.4% |
133 Hz 184 us 1.9–2.1 V |
C |
M |
|
Koeppen et al. 2019 [28] |
Hamburg, Germany, August 2011 to February 2014 |
10 |
21.5 |
NR |
70% |
145 Hz 90 us up to 5 V |
I |
M |
|
Herrera et al. 2020 [29] |
Canada 2013 to 2020 |
6 |
4.9 years |
2 |
NR |
145 Hz 90 us up to 8.5 V |
I |
M/B |
|
Jarvenpaa et al. 2020 [30] |
Finland Time period NR |
27 |
24 |
19 |
65% [FIAS] |
140 Hz 90 us 5–6 V |
I |
M/B |
|
Salanova et al. 2020 [20] |
United States Trial registration 18 January, 2005 |
73 62 |
7 years 10 years |
74% |
75% [7 years] |
161 Hz 103.1 us 6.6 V |
I |
M/B |
|
Tassigny et al. 2020 [31] |
Belgium March to October 2016 |
5 |
15 |
NR |
24.5% |
140 Hz 90 us 5 V |
I |
NR |
|
Schaper et al. 2020 [32] |
Netherlands Time period NR |
20 |
12 |
14 |
46% |
145 Hz 90 us 5.6 V |
I |
M/B |
|
Guo et al. 2021 [33] |
South Korea Between 2016 and 2018 |
25 studied 19 |
12 |
15 |
64 .3% |
130 Hz 90 us 1.5–3.1 V |
C |
M |
|
Kaufmann et al. 2021 [34] |
Munich, Germany, August 2011 to June 2019 |
23 pts [unilateral DBS 2 pts] |
46.6 |
17 |
NR |
140–145 Hz 90 us 1.5–3.5 V |
I |
M/B |
|
Tong et al. 2022 [35] |
Beijing, China Between 2015 and 2019 |
20 studied 11 |
12 |
6 |
51.4% |
NR |
NR |
NR |
|
Miron et al. 2022 [36] |
Israel January 2017 to January 2021 |
11 |
28.5 |
8 |
54.8 ± 34.2% |
140–145 Hz 90 us 5 V |
I |
M/B |
|
Costa-Gerdrudes et al. 2022 [37] |
Lisbon, Portugal Between 2011 and 2019 |
16 studied 14 |
11 |
9 |
NR |
140–145 Hz 90 us 5 V |
I |
M |
|
Yan et al. 2023 [38] |
Beijing, China January 2012 to December 2021 |
45 |
44.2 |
29 |
82.2% |
NR |
NR |
NR |
|
Peltola et al. 2023 [39] |
Europe registration 31 January 2012 Patient enrollment 21 February 2012 to 19 June 2019 |
170 |
2 years 5 years |
2 years 32.3% 5 years 53.2% |
2 years 33.1% 5 years 55.1% |
145 Hz 90 us 5 V |
I |
M/B |
|
Dague et al. 2023 [40] |
Bonn, Germany 2012 to 2124 |
11 |
51.5 |
54.5% |
73.6% |
NR |
NR |
M/B |
|
Parisi et al. 2023 [41] |
United States, January 2011 to February 2021 |
31 |
27.6 |
26 |
65% |
Low/high frequency |
I/C |
M/B |
|
Sobstyl et al.2023 [42] |
Poland May 2020 to October 2022 |
10 |
13.6 |
9 |
73.3% |
Mean 132 Hz 84 us 3.2 V |
I |
M |
The antiepileptic effect of ANT DBS is based on animal studies and human data [7–22, 55, 56]. In animal models, thalamic stimulation at low frequencies drives synchronisation activity in distant brain regions, whereas stimulation at high frequencies desynchronises intrinsic cortical activity. High-frequency thalamic stimulation can block epileptiform activity in the cortex. A so called ‘driving response’ elicited by low-frequency ANT DBS is demonstrated on scalp EEG with synchronisation of brain activity. As mentioned above, high-frequency stimulation above 100–130 Hz is used to desynchronise the EEG activity. Frequencies as high as 185 Hz have also been reported, but higher frequencies can induce unwanted adverse events, and reduce battery life significantly [27].
Most older studies, including the SANTE trial, used relatively high initial voltage (around 5 Volts) [7]. An example of the volume of tissue activated (VTA) resembling the SANTE study voltage and presently applied voltage is depicted in Figure 3 (A, B, C). This may suggest that the initial stimulation parameters mentioned above could not only stimulate the ANT, but also the surrounding brain tissue. Moreover, in most studies, the intermittent stimulation mode consisting of 1 minute on stimulation followed by 5 minutes off stimula- tion was used [7, 11, 13, 19, 20, 25]. Today, the initial stimulation voltage is usually set in the range of 2 or 3 Volts [27, 34]. The pulse width in most studies is set above 90 microseconds [7, 19, 20, 22, 25]. Most studies have used an intermittent mode of stimulation, but a few have implemented a continuous stimulation mode [10, 15, 22–24, 33]. Clinical studies, where a continuous stimulation mode has been used, report higher scores for mean seizure frequency reduction [22–24, 33, 41].
Adverse events related to ANT DBS procedures
Adverse events related to the ANT DBS procedure can be divided into three categories, (i) intraoperative-related complications (bleeding, venous infarction, improper intraoperative placement of DBS lead/s); (ii) hardware-related complications (infection, erosions, fracture or migration of a DBS lead); and (iii) stimulation-induced complications (aggravation of seizure frequency or inducing de novo psychiatric/behavioural symptoms or aggravation of pre-existing comorbid psychiatric/behavioural symptoms).
Special attention should be paid to possible cognitive and emotional sequelae of ANT DBS as well as outcomes assessing quality of life. The ANT is a relay structure of the circuit of Papez and cognitive as well as emotional sequelae can be elicited by stimulation of a limbic system [57]. There is a possibility of de novo induction or aggravation of pre-existing psychiatric symptoms [58]. A relatively large number of patients with longstanding DRE are handicapped by memory and psychiatric side effects related to uncontrolled seizures before undergoing ANT DBS. Psychiatric and neuropsychological assessments play a major role in selecting patients for DBS for DRE [7, 19].
The SANTE trial has revealed gradual improvement in the cognitive domains of attention and executive functions [19]. Tröster et al. followed patients for 7 years after ANT DBS from the previously reported prospective randomised SANTE trial, and found no significant cognitive declines or worsening of depression [59].
Mood disturbances or memory problems seen only in a blinded phase of the SANTE trial may be related to the overstimulation of the ANT as well as to a lesional (microthalamotomy) effect [7]. Monopolar stimulation using relatively high stimulation parameters (especially voltage) in an early postoperative phase may explain this transient subjective mood and memory problems [7]. Nevertheless, the long-term neuropsychological outcomes have shown improvements in memory, verbal fluency, and mood in patients after ANT DBS [59]. Other authors who used ANT DBS have noticed objective improvements in alertness and communicative behaviour [60]. ANT DBS improves some cognitive domains without causing major mood and memory disturbances [59, 60]. Adverse events including procedural, hardware and stimulation- -related complications, as well as cognitive/emotional outcomes following ANT DBS, are set out in Table 2.
|
Authors |
Procedural- |
Hardware-related adverse events or other complications |
Stimulation-related adverse events |
Behavioural/cognitive changes |
Activities of daily living |
|
Upton et al. 1987 [10] |
NR |
NR |
Some pts experienced euphoric and ecstatic feelings |
Improvement in behaviour and emotional responses |
Improvement in activities of daily living |
|
Hodaie et al. 2002 [13] |
NR |
1 pt had skin erosion with wound revision |
NR |
Subjective improvements in cognitive status noted by family members |
Subjective improvements noted by family members |
|
Kerrigan et al. 2004 [11] |
NR |
1 pt required replacement of leads due to incorrect placement |
NR |
NR |
NR |
|
Lee et al. 2006 [23] |
NR |
1 pt had infection around IPG, removal of DBS system in a patient implanted in STN |
NR |
Subjective improvement of cognitive and behavioural status noted by family members |
Subjective improvements in quality of life noted by family members |
|
Andrade et al. 2006 [17] |
NR |
NR |
1 pt experienced lethargy due to continuous stimulation |
NR |
NR |
|
Lim et al. 2007 [15] |
1 pt had small frontal haemorrhage – mild hand weakness |
1 pt had erosion over extension; resulted in removal of whole system |
NR |
Behavioural changes occurred |
Subjective improvements in quality of life |
|
Osorio et al. 2007 [16] |
NR |
NR |
NR |
Verbal fluency, mental flexibility declined significantly in some patients |
Quality of life improvement in all patients – objective assessment |
|
No symptomatic haemorrhage 5 asymptomatic haemorrhages [4.5%] |
Adverse events provided for long term follow-up implant side pain 20.9% implant side paresthesias 22.7% 14 pts developed [12.7%] infection. DBS leads not in target in 8.2% Extension fracture 4.5% IPG migration 5.5% |
2 pts had acute, transient stimulation-associated seizures. 7 episodes of status epilepticus, 3 pts with status epilepticus were not stimulated |
Long-term objective improvements in all domains of attention, executive functions, depression, tension/ /anxiety, subjective cognitive functioning. SUDEP: 1 baseline phase, 2 definitive and 1 possible. |
Objective improvements in quality of life [Quality of Life in Epilepsy-QoLI-31] |
|
|
Lee et al. 2012 [18] |
NR |
1 pt had infection resulted in DBS explantation |
NR |
NR |
NR |
|
Piacentino et al. 2015 [25] |
NR |
NR |
NR |
Objective improvements in behaviour |
Objective improvements in quality of life [Quality of Life in Epilepsy-QoLIE-31] |
|
Krishna et al. 2016 [22] |
NR |
1 pt had a system explanted due to infection. 1 pt with infection required wound revision. 1 system explantation due to cosmetic reasons |
1 pt postoperative episode of psychosis. 2 pts developed an increase in seizure frequency in early postoperative period |
1 pt developed severe postoperative agitation causing switching off of stimulation |
NR |
|
Kim et al. 2017 [21] |
1 symptomatic haemorrhage left hemiparesis disappeared after 3 months |
1 infection with antibiotic treatment alone. 1 pt had system explantation that was not reimplanted. Lead disconnection in 2 pts [6.9%] Revision due to suboptimal lead placement in 3 pts out of 58 DBS leads [5.2%] |
2 pts had DBS hardware removals due to lack of efficacy |
Improvement in word fluency task. No significant changes in general abilities, information processing, and executive functions. 1 pt complained of agitation resulting in switching off of stimulation. One [3.4%] probable SUDEP occurred 5 years after implantation |
NR |
|
Sitnikov et al. 2018 [24] |
1 frontal haematoma – asymptomatic 1 haematoma in anterior lesion group |
1 system explantation due to ineffectiveness. 1 infection along extension cable and IPG–preservation of DBS electrodes |
2 pts experienced a current leak at the IPG site |
No side effects regarding mental and emotional status |
NR |
|
Hermann et al. 2018 [26] |
NR |
1 transient episode of dysarthria and left central facial nerve palsy 1 pt with stimulation-induced facial twitches – reimplantation of the electrode 2 pts increased of preoperative seizures |
NR |
Subjective reports of more energy, better sleep, shorter and less intense seizures, better cognitive functioning |
NR |
|
Park et al. 2019 [27] |
NR |
NR |
NR |
Objective behavioural improvements |
Objective quality of life improvements [Quality of Life in Epilepsy-QoLIE-31] |
|
Koeppen et al. 2019 [28] |
NR |
NR |
NR |
NR |
NR |
|
Herrera et al. 2020 [29] |
NR |
NR |
2 pts mild and transient headaches |
1 pt had SUDEP |
NR |
|
Jarvenpaa et al. 2020 [30] includes pts from 2016 |
NR |
NR |
NR |
2 pts had SUDEP |
NR |
|
Salonova et al. 2020 [20] |
Reported in previous studies by Fisher and Salanova |
Implant site infection from implant to 10 years — 12.7% of pts [1 year rate of 7.3%] Leads not in target 8.2% |
NR |
At 7 years 37.3% had depression 2/3 No deterioration in psychosocial functioning |
QOLIE-31 stable improved, meaningful improvement on QOLIE-31 in 43% of patients. Satisfied or greatly satisfied 84% [54/64]. |
|
Tassigny et al. 2020 [31] |
NR |
NR |
NR |
1 pt sleep disorder, 2 pts had mild memory impairment, 2 pts sleep disturbances, 2 pts had transient depression |
Objective quality of life improvements [Quality of Life in Epilepsy-QOLIE-31] improved in 4 pts |
|
Schapper et al. 2020 [32] |
NR |
NR |
NR |
2 pts irritability and sleep problems |
NR |
|
Guo at al. 2021 [33] |
NR |
1 pt hardware removal due to infection |
NR |
NR |
NR |
|
Kaufman et al. 2021 [34] |
NR |
2 pts had hardware removal due to bacterial meningitis and postauricular dermal defects |
Mild stimulation induced side effects |
NR |
Assessed in 9 pts depression [BDI] and [QOLIE-31] improved |
|
Tong et al. 2022 [35] |
NA |
NR |
NR |
NR |
NR |
|
Miron et al. 2022 [36] |
NR |
Trauma necessitating hardware removal and reimplantation |
NR |
2 pts subjective memory deterioration, 2 pts depressive symptoms |
NR |
|
Costa-Gerdrudes et al. [37] |
NR |
NR |
NR |
3 pts suffered depression, 1 pt had psychosis |
NR |
|
Yan et al. 2023 [38] |
NR |
NR |
NR |
NR |
NR |
|
Peltola et al. 2023 [39] |
DBS-related AEs were connected to procedure [n = 24] no intracranial haemorrhages, and no deaths related to DBS |
Total of 11 pts [6.1%] had lead modifications, of which most frequent being explant with replacement. 2 explants due to infection [1%], 1 explant due to suicidal ideation in 1 pt |
Increased frequency/ /severity] of seizure [16%], memory impairment [patient-reported complaint, 15%] |
1 pt had died with definite sudden unexpected death in epilepsy [SUDEP] depressive mood [patient-reported complaint, 13%], and epilepsy [12%], headache [7%], head injury [5%], irritability [5%], anxiety [5%], cognitive impairment [5%] |
2-point improvement in QOLIE-31, one third of pts improved by more than 5 points in QOLIE-31 assessment available for 78 pts |
|
Dague et al. 2023 [40] |
NR |
5 pts had DBS hardware removal due to psychiatric AE or insufficient seizure reduction |
Psychiatric AE noted in 5 pts |
Significant deterioration in executive functions reported in 1 pt. Long-term neuropsychological effects included significant intraindividual changes in verbal learning and memory. Figural memory, attention and executive functions, confrontative naming and mental rotation were mostly unchanged, and improved |
NR |
|
Parisi et al. 2023 [41] |
NR |
NR |
NR |
1 pt subjective memory impairment, 4 pts self-reported improved memory function, 4 pts major depression episodes |
NR |
|
Sobstyl et al. 2023 [42] |
Pneumothorax with urgent pleural drainage |
Head injury [10%] requiring surgery for chronic subdural haematoma |
NR |
Cognitive functioning preserved, deterioration in mental well-being [depressed mood] of operated pts |
NR |
Indications and contraindications for CMN DBS
The second most common thalamic nucleus targeted for DRE is CMN [6]. CMN represents a thalamic relay structure of a reticulocortical system that participates in wakefulness, affective processes and in widespread regulation of cortical excitability [59, 60]. It has been shown that CM DBS is an effective treatment for primary generalised tonic-clonic or multifocal (multilobar) seizures, atonic seizures, and myoclonic seizures. Good clinical results of CMN DBS have been obtained for DRE in patients with a diagnosis of LGS [63]. Intellectual disability does not constitute a contraindication for CMN DBS, because most patients with LGS exhibit intellectual disability, ranging from moderate to profound [63].
The exclusion criteria for CMN DBS constitute individuals with an increased risk of bleeding, anatomical brain abnormalities precluding safe CMN DBS surgery, focal seizure type, and previous or current psychogenic non-epileptic seizures.
Clinical efficacy of CMN DBS for treatment of DRE
The pioneers of CMN DBS were the Velasco brothers, publishing in 1987 their first study including 5 patients with DRE [65]. Stimulation was applied through percutaneous wires resulting in focal seizures reduction by 60–100%, and generalised seizure reduction by 80–100% [65]. Thereafter, Fisher published a crossover study in 7 patients [66]. The mean seizure frequency reduction was only 30% which was not statistically significant, versus 8% when stimulation was discontinued. Among Fisher’s 7 patients, three had temporal lobe epilepsy, which may explain the apparent lack of efficacy [66].
Additional studies published by Velasco’s group totalling nearly 100 patients pointed out that the best results were obtained in patients suffering from generalised onset seizures and multifocal seizures [64, 65, 67]. In Velasco’s experience, CMN DBS for focal seizures was limited. A two-centre, single-blind, controlled trial of CMN DBS in 11 patients with generalised and frontal lobe DRE demonstrated that CMN DBS was effective in generalised epilepsy, but not in frontal lobe epilepsy [68]. In 2020, Cukiert et al. published the results of a prospective open label study including 20 patients diagnosed with LGS [69]. CMN DBS produced significant reduction of tonic seizures by 66%, atypical absence seizures by 78%, atonic seizures by 83%, and generalised tonic-clonic seizures by 89% [69].
Recently, Dalic et al. published the results of a prospective double-blind, placebo-controlled clinical trial of CMN DBS for LGS [70]. The baseline seizure frequency reduction versus study exit was 46.7% [69]. Apart from the abovementioned clinical studies, other studies have reported mean seizure reduction for different generalised seizures ranging from 51% to 83% [71, 72–76]. The clinical outcomes of CMN DBS for DRE are set out in Table 3.
|
Authors |
Country of study’s origin, Time of patient recruitment |
Number of patients |
Follow-up in months, mean |
Responder rate, |
Seizure reduction |
Stimulation |
Stimulation mode |
Stimulation |
|
Velasco et al. 1987 [65] |
Mexico City, Mexico |
5 |
6 to 37 months |
5 |
80–100% reduction in BTCS, 60–100% reduction in partial complex seizures 100% reduction of myoclonic seizures in one patient. Astatic seizures not reduced |
60–100 Hz 100 us 0.8 to 2.0 mA |
I |
B |
|
Fisher et al. 1992 [66] |
United States |
7 |
3 to 13 months |
3 out of 6 patients in open label phase were responders |
30% in placebo-controlled phase |
65 Hz 90 us 0.5 to 10 V |
I |
B |
|
Velasco et al. 2000 [67] |
Mexico City, Mexico from 1990 to 1993 |
13 2 diagnosed with TSC |
Mean 41.2 12–94 months |
12 |
Significant improvement and atypical absences, better results for LGS patients |
60 Hz 90 us 4 to 6 V |
I. |
B/M |
|
Velasco et al. 2006 [64] |
Mexico City, Mexico |
13 with LGS |
46 from 23 to 132 months |
12 |
Significant reduction in severe BTCS [GTS] and atypical absence seizures [AA] 80% |
130 Hz 450 400–600 uA |
I |
B |
|
Cukiert et al. 2009 [71] |
Sao Paulo, Brazil |
4 with GTS after callosotomy |
18 from 12 to 24 months |
4 |
78% |
130 Hz 300 us 2 V |
C |
B |
|
Valentin et al. 2013 [68] |
London, United Kingdom, Madrid, Spain |
11 |
24 |
2 out of 5 pts with frontal lobe epilepsy responders, 5 out of 6 pts with generalised epilepsy responders |
81% in GTS, 10% in frontal seizures |
130 Hz 90 microseconds up to 5 V, in non-responders 60 Hz was used |
C |
M |
|
Son et al. 2016 [72] |
Seoul, SouthKorea |
14 |
Mean 18.2 ± 5.6 from 9 to 25 months |
11 [78.6%] |
68 ± 22.4% [25–100%] |
Mean 129.3 ± 2.7 Hz 124.4 ± 23 us 2.2 ± 0.41 V |
C |
M |
|
Kim et al. 2017 [73] |
Seoul, South Korea |
10 [3 GTS and 7 MFE] |
21 |
9 |
72% LGS patients showed 52% SR, whereas frontal epilepsy pts 80.3% |
130 Hz 90 us from 1.5 to 2 V |
C |
M |
|
Cukiert et al. 2020 [69] |
Sao Paulo, Brazil |
20 LGS or LGS like |
At least 12 months follow-up, mean 30 months |
90% |
90% of patients responders. Significant reduction of tonic seizures 66%, atypical absence 78%, atonic 83%, and generalised tonic-clonic seizures 89% |
130 Hz 300 us up to 4.5 V |
C |
B |
|
Dalic et al 2021 [70] |
Melbourne, Australia |
20 LGS randomised 19 |
6 |
Blinded phase 50% in stimulation group versus 22% of controls. [Primary outcome measure] |
46.7% |
145 Hz 90 us up to 2.5 V |
C |
M |
|
Alcala-Zermano et al. 2021 [74] |
Rochester, United States |
5 |
Mean 80 months–6.6 years Range [37–97] months] |
3 pts [60%] |
56% |
2–100 Hz 60–150 us 1.0 to 6.3 V |
I |
B |
|
Diaz et al. 2021 [75] |
Madrid, Spain |
10 |
Mean 92.4 months [42–129 months] |
8 |
51–% |
60 Hz 90 us up to 5 V |
NR |
NR |
|
Yang et al 2022 [76] |
Atlanta, United States |
14 including 5 with GLS |
Mean 19 ± 5 months [4.1–33 months] |
12 pts [68%] were responders |
91% |
60–130 Hz 90–300 us 1.0–5.5 V |
I [4 pts] C [10 pts] |
M [4 pts] B [10 pts] |
Other factors affecting outcome of CMN DBS for DRE
The most common predictor of a good clinical outcome of CMN is the recruiting response elicited by macrostimulation. Macrostimulation is carried out for proper target confirmation. Low-frequency stimulation (3–6 Hz) generates time-locked recruiting responses that are recorded bilaterally, even after unilateral CMN stimulation; the recruiting response amplitude is usually slightly smaller over the non-stimulated hemisphere. High-frequency stimulation does not generate recruiting responses, but rather a direct current shift, noted almost exclusively over the stimulated hemisphere [77]. This recruiting response correlates with a good clinical outcome [64, 67, 69]. Another possible predictor of a good clinical outcome of CMN DBS is the involvement of reticular system network by VTA generated by stimulation settings of implanted CMN DBS leads [75]. VTAs interconnected with a reticular system network encompassing sensorimotor and supplementary cortices with cerebellum and brainstem have produced significant seizure frequency reduction [75]. The clinical data demonstrate that CM DBS outcome in DRE is highly dependent on the individual connectivity profile involving the cerebello-thalamo-cortical circuits [75].
Targeting and trajectory planning during CMN DBS surgery
CMN is a difficult nucleus to target, lacking clear boundaries on the standard T1- and T2-weighted MRI, which hinder it as a direct DBS target for clinical applications [78]. This direct targeting of CMN without clear visualisation of this nucleus becomes more challenging when the structure is smaller than 10 mm in most dimensions. Even with two-dimensional high-resolution proton attenuation-weighted images at 3T, or by optimised 3D MPRAGE protocol, clear discrimination of all thalamic substructures is not achievable [78]. The direct targeting became possible with quantitative susceptibility mapping MRI which can assist localisation of CM with clear delineation from the surrounding subthalamic nuclei [79].
CMN is located at the level of the posterior commissure 10 mm away from the midline. CMN has an oval shape [78]. The trajectory to CMN is intraparenchymal without the need to transverse the ventricles as in the case of ANT targeting. In the absence of the abovementioned direct visualisation techniques, indirect targeting is usually performed [80].
Search for ideal target in CMN DBS for DRE
The CM is an intralaminar nucleus of the thalamus and is part of the reticulo-thalamo-cortical system that mediates cortical excitability and participates crucially in the modulation of conscious state [61, 62, 65, 69]. High frequency stimulation of CMN blocks diffuse cortical recruitment and augmenting responses [77]. CMN neurons project mainly to striatum and cerebral cortex, and ipsilateral central and precentral motor areas [72]. CMN neurons projecting to the cortical motor areas are located in the lateral part of CMN within the ventrolateral CM (CMpc). Consequently, CMN DBS would be expected to be most effective in generalised and frontal epilepsies and less in temporal epilepsies [72].
In Velasco’s experience, the optimal target within CMN associated with the greatest seizure frequency reduction was located in the ventrolateral part of CM (CMpc) [64, 67]. DBS leads located in this position were associated with a more than 80% reduction in seizure frequency [64]. More dorsal, posterior or medial DBS lead location was related to weaker seizure suppression. The effectiveness of DBS lead placement in this target has been proven by several reports of CMN DBS [68, 71, 72].
Modern neuromodulation software with visualisation of implanted DBS leads and simultaneous estimation of VTA has enabled interesting insights into thalamic nuclei being stimulated for DRE [75]. VTA of DBS leads implanted at the ventrolateral part of CM incorporate in the stimulation field the surrounding thalamic subnuclei such as posterior ventral part of the mediodorsal nucleus (parvocellular MD, MDpc), central lateral nucleus (CL), and posterior part of the ventrolateral nucleus (VLp) [81]. Using a relatively high stimulation setting in most reported studies, the antiseizure effect is related to the summation of neuronal activation of complex areas as CMpc, MDpc, CI, and VLp, not merely to the modulatory effect of CMN alone [72]. More focused stimulation restricted to ventrolateral CM may be more effective for generalised epilepsy, and a wider field of stimulation for multifocal, multilobar epilepsies [64, 67].
Stimulation parameters, polarity, and mode of CMN stimulation
As in the case of ANT DBS, there are no guidelines related to setting the initial stimulation parameters in patients undergoing CMN DBS. Different authors have used various stimulation parameters, modes, and polarities [64, 65, 68–70, 72]. The image-verified localisation of implanted DBS leads with visualisation of VTAs may be of great value for choosing appropriate contacts, stimulation polarity and settings [75].
Most studies have used 130 Hz stimulation, although in three studies 60 Hz stimulation was used [67, 75, 76]. In the context of neurostimulation, the application of electrical stimuli at frequencies of 80–200 Hz is considered to be ‘high frequency stimulation’.
The initial stimulation voltage for CM DBS is relatively high at up to 5 V, although most recent studies of CMN DBS report a range of stimulation voltage of 1–5 Volts, indicating that lower stimulation voltage may be associated with good clinical results [70, 72–74]. The pulse width for CMN DBS shows the widest range from 60, 90 microseconds to even 300 or 450 in older publications [69, 70–74].
The intermittent mode of stimulation was used up to 2006 [65, 66]. Continuous mode of stimulation was initiated by Cukiert in 2009 and most authors upward perform continuous stimulation of CMN for DRE [68, 69, 71–73].
The continuous mode of stimulation may be related to higher scores for mean seizure frequency reduction [70–73]. The stimulation settings, polarity as well stimulation mode in historical and present clinical trials of CMN stimulation are set out in Table 3.
Adverse events related to CMN DBS procedures
Intracranial haemorrhagic complications related to CMN DBS procedures have been encountered only in three patients [66, 74, 76]. In 2 patients the intracerebral hemorrhages were clinically silent [66, 76]. The third was a haemorrhage related to the DBS procedure which resulted in transient hemiparesis that resolved within one month [74]. Another intraoperative-related event due to pneumocephalus resulted in the misplacement of both DBS electrodes [72]. During revision surgery, both DBS electrodes were correctly implanted [72]. Patients with primary generalised seizures and with a diagnosis of LGS may be more prone to the development of skin erosions and subsequent infections. The targeted population for CMN DBS includes children and young adults where skin-related complications due to the implanted hardware pose a greater challenge compared to the adult patient population. Skin-related complications in children with LGS have been the main reason for DBS hardware explantation [64, 67, 68, 70]. Mechanical damage to the DBS hardware has also been reported in patients after CMN DBS, but less frequently than erosions and infections [64, 65].
Although the patient population for CMN DBS (LGS patients) has mild to profound mental retardation, interestingly, most studies have reported improvements in behaviour and emotional responses with better psychological functioning [64, 65, 68]. These behavioural, cognitive effects are directly related to the seizure reduction after CMN DBS [64, 65, 68]. One study reported stable psychological functioning after CMN DBS [66]. Some studies have not mentioned cognitive, behavioural changes after CMN DBS [67, 72, 73]. In general, most studies have reported improvements in activities of daily living or life satisfaction using objective clinical scales [64, 65, 68, 69, 74]. The above mentioned cognitive and emotional outcomes following CMN DBS are set out in Table 4.
|
Authors and year published |
Procedural- |
Hardware-related adverse events |
Stimulation-related adverse events |
Behavioural/cognitive changes |
Activities of daily living |
|
Velasco et al. 1987 [65] |
NR |
NR |
NR |
Improvement in behaviour and emotional responses. Better psychosocial functioning |
Improvement in activities of daily living |
|
Fisher et al. 1992 [66] |
1 patient asymptomatic bleeding |
1 pt revision due to breakage of connecting cable |
NR |
Psychosocial functioning stable |
NR |
|
Velasco et al. 2000 [67] |
NR |
2 pts [children aged 5 and 6] developed skin erosions. Removal of DBS systems in both children |
NR |
NR |
NR |
|
Velasco et al. 2006 [64] |
NR |
2 pts were explanted due to repeated skin erosions that could not be controlled by plastic surgery 1 pt had rupture of extracranial lead and connection cable, uncomplicated hardware replacement |
NR [patients were unaware of stimulation] |
Pts were in non-convulsive status, and former neuropsychological testing was difficult |
Improvements in education in most patients; 2 patients lead normal lives; 8 patients are independent or partially independent |
|
Cukiert et al. 2009 [71] |
NR |
NR |
Short-lasting [15–20 mins] parasthesia after each voltage increase beyond 1.0 V |
Improved psychosocial functioning |
Clinically relevant increase in attention level [SNAP- questionnaire]. IQ slight increase |
|
Valentin et al. 2013 [68] |
NR |
1 pt had infection resulted in DBS system explanation |
NR |
Improvements in psychosocial functioning |
Improvements in quality of life performed objectively in 7 pts, 6 months after stimulation |
|
Son et al. 2016 [72] |
Misplacement of both electrodes due to pneumocephalus requiring replacement |
NR |
NR |
NR |
NR |
|
Kim et al. 2017 [73] |
NR |
NR |
NR |
NR |
NR |
|
Cukiert et al. 2020 [69] |
NR |
2 pts had developed infections at IPG location. Treatment with antibiotics |
Persistent paresthesia which limited 4.5 Voltage |
Before surgery, patients were unable to undergo formal neuropsychological evaluation and quantitative attention protocols |
Improvement in attention, no worsening related to items of SNAP-IV questionnaire |
|
Dalic et al. 2021 [70] |
NR |
All adverse events included 7 pts [35%] 1 pt had infection and mega oedema requiring removal of DBS hardware, 1 patient had trauma and emergency surgery, 2 pts had mega oedema along course of electrodes in prestimulation period |
2 pts prolonged seizure status epilepticus, 1 patient with facial seizure related injury, 12 pts postoperative drowsiness with 3 pts profound drowsiness |
No noticeable behavioural or cognitive adverse events, no deterioration in cognitive function |
Parents/carers 18 of 19 pts reported improved alertness |
|
Alcala-Zermano et al. 2021 [74] |
1 pt had experienced postprocedural hemiparesis resolved within one month |
2 pts developed hardware complications; IPG rotation requiring revision DBS hardware infection resulted in removal |
NR |
NR |
Life satisfaction improved in 56% of pts |
|
Diaz et al. . 2021 [75] |
NR |
NR |
NR |
NR |
NR |
|
Yang et al. 2022 [76] |
1 pt with clinically silent intraventricular haemorrhage |
1 pt with hardware breakage, 1 pt with postoperative aspiration event |
2 pts developed subjective mood changes |
2 pts developed behavioural changes [behavioural outbursts], 1 patient memory difficulties |
NR |
Conclusions and future directions
The ANT and CMN represent the most common targeted thalamic nuclei of network brain hubs involved in the widespread propagation of epileptic seizures. The clinical experience of thalamic DBS for DRE is still limited compared to the high number of patients with multifocal DRE who are not amenable to resective surgery. The ANT DBS has shown clinical efficacy for focal to secondary generalised tonic-clonic seizures when epileptic foci involved the mesial/temporal or frontal brain regions. Epileptic foci restricted to parietal or occipital lobes do not respond so favourably to ANT DBS. The CMN DBS showed good clinical efficacy for primary generalised tonic-clonic seizures with multiple epileptic foci located in precentral motor areas, and primary somatosensory cortex.
Both thalamic nuclei are relatively small targets with different subnuclei. They both represent the relay structures of the Papez circuit (ANT), and the cerebello-thalamic-cortical circuit with afferents from reticular formation (CMN). Both thalamic targets have widespread cerebral connections through the appropriate brain networks. Compared to the anecdotal historical reports in the 20th century of ANT or CM DBS for DRE, today’s image-guided targeting prevails in the proper placement of DBS leads. The postoperative confirmation of implanted DBS leads by CT/MRI done after surgery, and merging with preoperative MRI, enables the selection of implanted contacts. Moreover, the visualisation of VTAs based on individual settings can avoid the overstimulation of the targeted nucleus, reducing the possible stimulation-induced adverse events.
The novel connectomic approach in selecting appropriate patients based on connectome of the targeted nucleus with epileptogenic focus/foci may have a great value in selecting patients for thalamic DBS for DRE. Functional imaging and diffusion imaging may direct stimulation settings optimisation by estimation of VTA which incorporate the brain networks involved in epilepsy propagation.
All of these factors may bring about in future better seizure frequency reduction after ANT or CMN DBS therapy for DRE.
