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Article

Meningioma-Related Epilepsy: A Happy Ending?

by
Giada Pauletto
1,
Annacarmen Nilo
2,*,
Sara Pez
3,
Maria Elisa Zonta
3,
Daniele Bagatto
4,
Miriam Isola
5,
Lorenzo Verriello
1,
Mariarosaria Valente
2,3,
Miran Skrap
6 and
Tamara Ius
6
1
Neurology Unit, Head-Neck and Neurosciences Department, Santa Maria della Misericordia University Hospital, 33100 Udine, Italy
2
Clinical Neurology Unit, Head-Neck and Neurosciences Department, Santa Maria della Misericordia University Hospital, 33100 Udine, Italy
3
Department of Medicine, University of Udine, 33100 Udine, Italy
4
Neuroradiology Unit, Department of Diagnostic Imaging, Santa Maria della Misericordia University Hospital, 33100 Udine, Italy
5
Division of Medical Statistics, Department of Medicine, University of Udine, 33100 Udine, Italy
6
Neurosurgery Unit, Head-Neck and Neurosciences Department, Santa Maria della Misericordia University Hospital, 33100 Udine, Italy
*
Author to whom correspondence should be addressed.
J. Pers. Med. 2023, 13(7), 1124; https://doi.org/10.3390/jpm13071124
Submission received: 14 April 2023 / Revised: 21 May 2023 / Accepted: 9 July 2023 / Published: 11 July 2023
(This article belongs to the Section Methodology, Drug and Device Discovery)
Browse Figures
Versions Notes

Abstract

:
(1) Background: More than one-third of patients with meningiomas experience at least one seizure during the course of their disease, and in the 20–50% of cases, seizure represents the onset symptom. After surgery, up to 30% of patients continue to have seizures, while others may experience them later; (2) Methods: The study analyzed retrospectively the risk factors for pre-operative seizures in a large cohort of 358 patients who underwent surgery for newly diagnosed brain meningioma; (3) Results: We identified age, peritumor edema, and location as risk factors for seizure at the onset. Patients with seizures differed from patients without seizures for the following characteristics: younger average age, lower pre-operative Karnofsky Performance Status (KPS), location on the convexity, lower Simpson Grade, lower incidence of pre-operative neurological deficits, and higher incidence of pre-operative peritumor edema. After 24 months, 88.2% of patients were classified as Engel class Ia, and no correlation with disease progression was observed; (4) Conclusions: Meningioma-related epilepsy has generally a positive outcome following surgery and it seems not to be linked to disease progression, even if further studies are needed.

Graphical Abstract

1. Introduction

Meningiomas account for 16–38% of all intracranial tumors in adults [1]. Approximately one-third of patients with meningiomas experience at least one seizure during their disease, and in 20–50% of cases, seizure is the first symptom [2,3]. Although surgical resection can offer seizure freedom in 60–90% of meningiomas, seizures continue to persist after surgery in up to 30% of patients [4].
Patients with meningiomas have a seizure incidence of over 33% during the course of their disease. However, meningioma-related epilepsy has received insufficient research attention, with the majority of studies focusing on tumor growth, resection size, and survival rates. It is essential to determine predictors of pre-operative seizures and post-operative seizure freedom, since epilepsy significantly impacts the patient’s quality of life [5]. Thus, achieving seizure freedom is a crucial goal after surgery for meningiomas, which can often be surgically removed and have a favorable long-term prognosis [5].
Recent studies have investigated the link between meningiomas and seizures. In this clinical setting, a wide range of seizure outcomes has been reported, mainly for different classification schemes adopted [6]. In addition, different uncertainties persist concerning the risk factors and the techniques for managing seizures in meningioma patients.
Studying the population of patients with seizures prior to meningioma resection is crucial in comprehending this intricate disease process, since they seem to have poorer outcomes than those without pre-operative seizures [2,7,8,9].
The aims of the present work were threefold: firstly, determining the frequency of seizures among individuals who underwent surgery for supratentorial meningiomas; secondly, exploring the risk factors linked to pre-operative seizures; and finally, assessing long-term seizure outcome in patients with meningioma-related epilepsy.

2. Materials and Methods

2.1. Study Population

We performed a retrospective analysis of a consecutive series of patients who underwent surgical treatment for newly diagnosed intracranial meningioma at the Neurosurgical Unit of Udine University Hospital, between January 2016 and November 2020.
Patients were enrolled according to the following inclusion criteria:
  • age ≥ 18 years;
  • newly diagnosed meningioma cases and non-previous treatments;
  • confirmed histological diagnosis of meningioma according to the updated 2016 World Health Organization (WHO) guidelines [10];
  • pre- and post-operative brain Magnetic Resonance Imaging (MRI) that were either performed at our Institution or available on the picture archiving and communication system (PACS) for review.
Additionally, patients were included if they were able to undergo a standard clinical and radiological follow-up starting from the 30th day after surgery. For those cases with seizure as onset symptom, diagnosis of tumor-related epilepsy was performed according to the International League Against Epilepsy (ILAE) definition [11]. Engel Class at 12- and 24-month follow-up was used to compute post-operative seizure outcome [12].
Patients were excluded in case of incomplete or inaccurate data in clinical, radiological, and surgical records, or if they were lost to follow-up. We only included patients who underwent a surgical procedure aimed at total or subtotal resection of the lesions. We excluded those who underwent biopsies.

2.2. Clinical Data

Clinical information was retrieved from medical records.
We collected the following data: gender, age, onset symptom, tumor localization and side, seizure type and frequency, type and number of anti-seizure medications (ASMs), pre-operative electroencephalogram (EEG), extent of resection (EOR), and post-operative seizure outcome.
We considered as focal neurological deficits: disorders affecting body movement and sensitivity, and cranial nerves. Regarding onset symptoms, we took into account, beyond seizures, other symptoms like dizziness, altered mental status, memory loss, intractable headaches, and incidental findings.
Tumor locations were categorized as skull base (sphenoid ridge, suprasellar, posterior fossa, olfactory groove, middle fossa/Meckel cave, and tentorial meningioma) or non-skull base (parasagittal, falcine, convexity, and lateral ventricular meningioma).
Extent of resection was considered as gross-total for Simpson I–III resection (or with no signs of tumor remnant on post-operative MRI) and sub-total for Simpson IV–V (or with obvious tumor remnant on post-operative MRI) [13]. Surgical complications such as hemorrhage, central nervous system (CNS) or wound infection, and cerebrospinal fluid (CSF) leakage were recorded.
The 2017 ILAE classification [14] was applied to classify seizures. Seizure frequency was assessed before surgery and after surgery every 6 months for 2 years.
Engel Class [12] at last follow-up was retrospectively assigned on the basis of self-completed seizure diaries and further grouped into favorable (class Ia) and unfavorable (class > Ia) outcomes.
Patients without reliable seizure outcome data and a minimum of 6-month postoperative follow-up were excluded.

2.3. Imaging Analysis and Region of Interest (ROI)-Drawing Process

All enrolled patients underwent a pre-operative brain MRI scan (Achieva 3 Tesla Scanner, Philips Medical Systems, Best, The Netherlands or Aera 1.5 Tesla Scanner, Siemens, Erlangen, Germany). The radiological evaluation included identifying the location of lesion, the presence of multiple meningiomas and/or meningiomatosis, the involvement of the subtentorial location, tumor diameter (measured in centimeters), and tumoral volume (measured in cubic centimeters). This was accomplished using isotropic volumetric T1-weighted sequences before and after intravenous administration of a paramagnetic contrast agent (gadolinium). Additionally, turbo spin echo (TSE) T2-weighted and fluid-attenuated inversion recovery (FLAIR) T2-weighted sequences were used to determine the edema volumes (measured in cubic centimeters) prior to anti-edema therapy.
To calculate the volume of the contrast-enhanced lesion and edema, a region of interest (ROI) was drawn in a volumetric enhancing postcontrast T1-weighted sequence (Mprage sequence) and in a T2-weighted TSE or FLAIR axial sequences using the software Horos. In 3D T1-weighted contrast-enhanced sequences, a pencil-draw semi-automatic tool was used to outline the lesion on all subsequent slices with a minimum thickness of 1.00 mm, conforming to the margins of the contrast-enhanced lesion with the software Horos. The same method was applied using T2-weighted images to outline the hyperintensity area, which is defined as “the high signal on T2-weighted imaging of brain sequences”, referring to the entire volume including the tumor lesion and associated tumor mass to obtain a new ROI.
Figure 1 summarizes one exemplificative case of meningioma with edema.

2.4. Surgery

The patients underwent several transcranial and skull base approaches according to the site of the meningioma. For lesions located in the olfactory groove and anterior floor different approaches were used, including supraorbital, cranio-orbital, and bi-frontal approaches. Meningiomas situated in the spheno-orbital and temporal floor were removed using the cranio-orbital zygomatic approach, while spheno-petroclival meningiomas were eliminated through retro-sigmoid one. Tentorial meningiomas were removed using the suboccipital and/or retro-sigmoid approaches [15].
The surgical resections of large meningiomas, especially when encasing nerves and/or the main cerebral vascular trunks and/or their perforating vessels skull base, were planned with the assistance of intra-operative neurophysiological monitoring.
For challenging cases, to determine whether adjunctive embolization of feeders was feasible [16,17], all patients underwent evaluation by a neuroradiologist.

2.5. Statistical Analysis

Categorical variables were reported as percentages, continuous variables were reported as mean ± standard deviation or median and range as appropriate, according to the data distribution. Normality of the continuous variables was tested using the Shapiro–Wilk test. The t-test or Mann–Whitney U-test, as appropriate, was used to compare continuous variables between groups (patients with pre-operative seizures versus patients without pre-operative seizures). Comparisons between nominal and categorical variables were made with a Chi-square test or Fisher’s exact test. For the outcome analysis, Engel classification was dichotomized as Engel Class Ia versus Engel Class > Ia (Ib-IV) (patients were either completely seizure free or not completely seizure free). A uni- and multi-variate ANOVA analysis along with contrast analysis and post hoc tests was performed to identify risk factors influencing pre-operative seizure onset and post-operative seizure outcome.
Continuous variable correlations were investigated with Pearson’s bi-variate correlation. All two-tailed statistical significance levels were set at p < 0.05.
All analyses were conducted using Stata/SE (StataCorp. 2015. Stata Statistical Software: Release 14. College Station, TX, USA: StataCorp LP) for Mac.

3. Results

3.1. Study Population and Characteristics of Meningioma-Related Epilepsy

Among 422 patients who underwent surgery for meningioma in the study period, 358 were enrolled. The neuroradiological diagnosis was consistently reached within a timeframe of two months from the initial onset of symptoms. The median time between diagnosis and surgery was 4 months (range 2–7 months). Only twelve patients (3.3%) underwent post-operative radiotherapy.
Demographic, clinical, histological, molecular, and radiological data of patients included in the study are summarized in Table 1.
Seizure was the onset symptom in 73 cases (20.4%). In detail, 45 subjects (61.6%) presented a single seizure, while the remaining 28 (38.4%) had more seizures before diagnosis. Focal seizures were detected in 28 cases (38.4%), while those with focal onset evolving into bilateral tonic-clonic seizures were 45 (61.6%). Seizures semiology was as follows: motor seizures in 79.5% of patients and non-motor in the remaining 20.5% (13.7% somato-sensitive, 2.7% cognitive, 2.7% autonomic, and 1.4% affective, respectively).
All patients were under ASMs: particularly, 67 (91.7%) were in monotherapy, while only six (8.3%) were in polytherapy. Levetiracetam was the most common ASM used in monotherapy (82.1%, n = 55), followed by Carbamazepine (10.4%, n = 7) and Valproic Acid (7.5%, n = 5). In polytherapy schemes, Perampanel was prescribed as first add-on drug in all patients.
Table 2 reports the main characteristics of patients with meningioma-related epilepsy.
A comparative analysis between the subgroup of patients with seizure onset (20.4%) and the one without seizure onset (79.6%) was performed to investigate the pre-operative differences influencing the clinical onset (see Table 3).
Age (OR 0.97, 95% CI 0.95–0.99, p = 0.003), pre-operative neurological deficit (OR 0.51, 95% CI 0.30–0.87, p = 0.014), tumor location (OR 0.06, 95% CI 0.01–0.48, p = 0.007), the presence of peritumoral edema (OR 4.56, 95% CI 2.46–8.46, p < 0.001) and tumoral grade (OR 2.17, 95% CI 1.12–4.22, p = 0.022) resulted, at univariate analysis, risk factors for clinical onset with seizures.
Regarding tumoral grade, patients with WHO grade II meningiomas had a higher risk than those with WHO grade I meningiomas of developing pre-operative seizures (p = 0.022).
With regard to tumor site, an increased risk was demonstrated for convexity meningiomas (p < 0.007). Among non-convexity meningiomas, there was a higher risk of pre-operative seizures for middle cranial fossa (MCF) meningiomas compared with meningiomas of posterior cranial fossa (PCF) (OR 29.57, 95% CI 3.44–254.08, p = 0.002).
Multivariate analysis confirmed age (p < 0.001), peritumoral edema (p < 0.001), and meningioma location (p = 0.016) as independent risk factors for pre-operative seizures (Table 4).
Pre-operative seizures were not risk factors, either for post-operative deficits (p = 0.91) or for disease progression (p = 0.97) (Table 3).

3.2. Post-Surgery Seizure Outcome

Among patients with meningioma-related epilepsy, eight developed early onset seizures after surgical treatment.
Seizure outcome was assessed every six months after surgery. All patients had 12-months follow-up; at 24 months, five patients were lost, and we could retrieve data from 68 subjects.
At 12 months, 87.6% (64/73) of patients were in Engel class Ia; at 24 months, 60 patients were still seizure-free (88.2%).
Non-seizure-free patients (Engel Class > Ia) had frequently meningiomas involving midline (33.3% vs. 6.2%, p = 0.04) or medial temporal fossa (33.3% vs. 9.5%, p = 0.05). Subjects under ASM polytherapy had a higher risk of seizure persistence after surgery (22.2% vs. 1.6%, p = 0.03). Evaluation at 24 months confirmed the association between seizure persistence and tumor location (midline lesions, p = 0.04) and polytherapy (p = 0.04) (Table 5).
No correlations were identified between seizure outcome and: histological grade (p = 0.06), tumor volume (p = 0.35) and EOR (p = 0.06).
Among patients without pre-operative seizures (n = 285), six (2.1%) had early-onset seizures after surgery and they were not treated with ASMs. Only one patient developed focal sensory seizures, six months after surgery and, consequently, he was put under treatment.

4. Discussion

Predictors and outcomes of meningioma-related epilepsy remain understudied, probably because most investigations have been dealing mainly with surgical aspects and prevention of neurological deficits. However, regardless of whether or not seizures may respond to ASMs, they represent a significant cause of morbidity and poor quality of life [9,18,19]. Therefore, proper understanding of these features is imperative to preventing seizure occurrence and guiding treatment strategies for patients with intracranial meningiomas. This is especially important considering the increase in meningioma detection due to the widespread availability of various neuroimaging modalities.
In our study, frequency of pre-operative meningioma-related seizures does not differ from data reported in the literature, affecting 20.4% of the entire population. Large previous and recent studies observed a percentage between 12.9% and 31.3% [3,9,19,20,21]. Demographic, clinical and radiological characteristics of patients are also in line with the literature [2,18,19,22,23,24,25,26] (Table 6).
Younger patients seem to more frequently develop pre-operative seizures. One could speculate that it may be due to cerebral plasticity, which influences active epileptogenic processes. Harward et al. suggest that a greater incidence of aggressive meningiomas in younger subjects may be the cause of frequent pre-operative meningioma-related seizures [24]. However, this observation is mainly related to the pediatric population, who are not represented in our study. Since younger patients in our sample had an age between 30 and 50 years, another possible factor influencing the occurrence of pre-operative seizures may be the effect of peritumoral edema. A certain level of cerebral atrophy, which is present in older patients, is protective against early symptoms of edema, such as seizures.
Gender does not appear to influence seizure occurrence in our study. There are controversial data regarding gender as a risk factor for pre-operative meningioma-related seizures; in fact, some authors observed a prevalence of seizures in females [27], while others reported a prevalence in males [8,28]. Furthermore, there are also studies that did not find any association between gender and meningioma-related seizures, as in our population [19,21,27]. Our results may depend on sample size, which presents a globally equal distribution in gender. Furthermore, the majority of women in our population were in peri- and post-menopausal age, thus with a possible reduction in sex-hormone-related epileptogenic mechanisms.
Tumor location is one of the main risk factors for meningioma-related epilepsy; in fact, meningiomas nested on cerebral convexity and in the temporal lobe are more prone to ignite seizures. This correlation depends on the involvement of larger cortical surface and the intrinsic predisposition to generate seizures of central and temporal brain areas [7,29,30,31]. Tumor side does not seem to influence seizure occurrence as reported by Howard et al. [24].
Our data confirm also that peritumoral edema represents the most significant risk factor for pre-operative seizures [31]. Chaichana et al. [28] reported that the presence of peritumoral edema at pre-surgical imaging increased the possibility to develop pre-operative seizures by a factor of three. Li et al. [9] identified peritumoral edema >/= 1 cm as one of the risk factors for pre-operative seizures, as well as in Bogdanovic’s recent work [19]. Edema may enhance seizures, determining neuronal death and excitotoxicity, by mean of mass effect on cerebral cortex. Furthermore, the breakdown of the blood–brain barrier, due to neo-angiogenesis and impaired vessel permeability, may determine local inflammatory responses and glutamate release that facilitate epileptogenic firing [32].
Besides the presence of edema, meningiomas are slow-growing tumors, thus they can induce changes in peritumoral brain areas that drives epileptogenesis. Among morphologic and functional changes happening in the brain tissue adjacent to meningiomas, there are alterations in synaptic vesicles trafficking and in glial gap-junction coupling, higher concentration of voltage-dependent Na+ channel, Ca++, and glutamate receptors and loss of inhibitory GABAergic synapses [24,33]. Changes in ion and neurotransmitter concentration as well as alterations of extracellular matrix are also advocated. These mechanisms, however, are common to different brain injuries and they have been extensively investigated, especially in glioma-related epilepsy [34]. Moreover, in meningioma-related epilepsy, NF2 mutation was shown to be predictive marker for seizures, via an indirect mediation effect with atypical histology and edema [35].
In contrast with the literature [19,24,36], we observed a significant statistical correlation between the occurrence of pre-operative seizures and histological grading. Particularly, patients with WHO grade II meningiomas are at higher risk of developing seizures, maybe due to invasion of cerebral cortex and the consequent cascade of local events leading to epileptic network building up [37], in addition to the increased development of peritumoral edema [24,28].
Patients with meningioma-related epilepsy are less associated with concomitant focal neurological deficits. These findings are consistent with the work of Seyedi et al. [26] and Hwang et al. [20]. Focal neurological deficits are usually expressions of rapidly destructive pathological processes, thus limiting the organization of epileptic foci and networks. Moreover, patients with seizures at clinical onset, especially in case of motor ones, may receive earlier diagnosis and surgery, preventing the occurrence of structural damages.
Surprisingly, mean pre-operative KPS value appears to be lower among patients with meningioma-related epilepsy; however, this apparently contrasting result can be explained by the impact of seizures on quality of life and by ASMs side effects.
Long-term seizure freedom after surgery occurred in 87.5% of cases in our population. In the literature, seizure freedom rate ranges between 60 and 90%, even if follow-up periods may vary [19,35].
Predictive factors for post-operative seizure outcome, at 12 months, are tumor location and side, and medical therapy. Lesion side and medical therapy have been confirmed also at long-term follow-up. Seyedi et al. [26] reported a relation between poor seizure outcome and meningioma location in the left hemisphere. In our population, instead, midline cortical involvement is related with worse post-operative seizure control, maybe due to the development of multiple epileptic foci or easier and faster spreading of ictal discharges. Convexity meningiomas, on the contrary, are associated with a better seizure outcome, as observed in previous studies [19,27]. Surgical approach for convexity meningiomas permits, in fact, an increased probability of gross total resection, with less manipulation and minor risk of vascular accidents.
In our study, EOR does not influence post-operative seizure outcome, in contrast with the literature [24,25,35]. Also, tumoral volume, histology, pre-operative seizure type, and frequency do not appear to be related with Engel class. It is possible that these data depend mainly on sample size.
Finally, patients treated with only one ASM have a better seizure outcome than those on polytherapy. This result is expected, since a pre-surgical pharmaco-resistance indicates more complex epileptogenic phenomena and diffuse epileptic network that may persist despite surgery.
To prevent the development of pharmaco-resistance, a prompt pre-surgical treatment with a carefully chosen ASM should be established, taking into consideration side effects, especially in the case of elderly patients. ASMs with a broad spectrum of efficacy, little or no interactions and easier titration scheme should be preferred. In our population, we chose Perampanel as add-on therapy, when needed, because it is generally well tolerated and presents an easy therapeutic scheme, being administered only once a day, before sleep [38,39]. Prophylaxis with ASMs, instead, should be avoided because it does not have any proven role in preventing post-operative seizures and it may cause useless side effects [7,9,19,38,40].
Furthermore, ASMs withdrawal is often troublesome and post-resection seizures may arise from a fast pharmacological tapering [5].
Table
Table 6. Literature review of studies about patients with meningioma and seizures.
Table 6. Literature review of studies about patients with meningioma and seizures.
Author (year)Gadot et al.
(2021) [35]		Baumgarten et al.
(2021) [41]		Schneider et al. (2019) [25]Hwang et al.
(2019) [20]		Seyedi et al.
(2018) [26]		Wirsching et al. (2016) [21] Zheng et al.
(2013) [42]
Number of patients57420187303295661 *97
Female
(n, %)		29/57 (51%)282 (67%)121 (65%)215 (71%)197 (66.8%)532 (80.5%)59 (60.8%)
Location- Non-Skull Base: 42/57 (73.7%)
- Skull Base:
15/57 (26.3%)		- Non-Skull Base: 273/420 (65%)
- Skull Base: 147/420 (35%)		- Non-Skull Base: 134/187 (71.6%)
- Skull Base:
53/187 (28.4%)		- Non-Skull Base: 199/303 (65.7%)
- Skull Base:
104/303 (34.3%)		- Non-Skull Base: 208/295 (70.5%)
- Skull Base:
87/295 (29.5%)		- Non-Skull Base: 320/661 (48.4%)
- Skull Base:
341/661 (51.6%)		- Non-Skull Base:
81/97 (83.5%)
- Skull Base:
16/97 (16.5%)
Pathology- WHO I: 40/57 (70.2%)
- WHO II: 14/57 (24.6%)
- WHO III: 3/57 (5.2%)		- WHO I: 244/420 (58%)
- WHO II: 164/420 (39%)
- WHO III 7/420 (1.7%)
- Unknown: 5/420 (1.3%)		- WHO I: 140/187 (75%)
- WHO II–III: 47/187 (25%)		- WHO I: 251/303 (82.8%)
- WHO II: 44/303 (14.5%)
- WHO III: 8 (2.6%)		- WHO I: 268/295 (90.8%)
- WHO II-III: 27/295 (9.2%)		- WHO I: 638/779 (81.9%)
- WHO II: 119/779 (15.3%)
- WHO III: 22/779 (2.8%)		- WHO I: 90/97 (92.8%)
- WHO II: 6 (6.2%)
- WHO III: 1 (1.0%)
Pre-operative seizure (n, %)57/57 (100%)87/420 (20.7%)187 (100%)49 (16.2%)72/295 (24.4%)244/779 (31.3%)97/97 (100%)
Seizure type- Focal: 30/57 (52.6%)
- Focal to bilateral tonic-clonic evolution: 25/57 (43.9%)
- Unknown: 2/57
(3.5%)		Unknown- Focal: 63/187 (34%)
- Focal to bilateral tonic-clonic evolution: 124/187 (66%)		UnknownUnknownAvailable in 237 patients
- Focal: 114/237 (48.1%)
- Focal to bilateral tonic-clonic evolution: 123/237 (51.9%)		- Focal: 45/97 (46.4%)
- Focal to bilateral tonic-clonic evolution: 52/97 (53.6%)
Seizure OutcomeSeizure-free: 42/57 (73.7%)Pre-operative seizures (n = 87):
seizure-free 24/87 (72.4%)		Seizure-free: 169/187 (90%)Pre-operative seizures (n = 49):
seizure-free 33/49 (67.3%)		Pre-operative seizures (n = 72):
seizure-free 46/72 (63.8%)		Pre-operative seizures (n = 244): seizure-free 144/244 (59%)Seizure-free: 50/97
(51.5%)
ASM prophylaxis54/57 (94.7%)UnknownUnknown294/303 (97%)57/72 (79.2%)Unknown58/97 (60%)
Tumor recurrence/progression (n, %)- Residual disease:
13/57 (22.8%)
- Recurrent disease:
10/57 (17.5%)		Tumor recurrence:
44/420 (10.5%)		Tumor progression: 18/187 (9.6%)48 (15.84)- Tumor progression:
70/295 (23.7%)
- Unknown:
22/295 (7.5%)		203/779 (26.1%)2/97 (2.1%)
Prognostic factors related to pre-operative seizures/- Temporal location
- Pre-operative edema		/- Vasogenic edema
- Falx/parasagittal tumor location
- Absence of pre-operative neurologic deficit		- Peritumoral edema//
Prognostic factors related to epileptological outcome- Postresection ischemia and recurrent disease: independent predictors of worse seizure outcome.
- WHO grade I tumor status: independent categorical predictor of improved Engel class outcome.
- MIB-1 index: independent linear predictor of Engel class outcome.		- Tumor volume, sensomotory deficit and sphenoid wing location: independently associated with the occurrence of post-operative seizures.
- Post-operative status epilepticus: independently associated with pre-operative seizures, sphenoid wing location and tumor volume.		- Peritumoral edema, high WHO grade, lower EOR: independent predictors of worse epileptological outcome.- Pre-operative seizures, larger tumor size and continuation of ASMs: significantly associated with late post-operative seizures.- Tumors located on left: predictor of post-operative seizures,
- no post-operative complications and tumor location in the convexity/parasagittal/falx: lower risks of developing post-operative seizures.		- Younger age, tumor progression, and pre-operative epilepsy: predictors of post-operative epilepsy.
- Risk factors for acute symptomatic seizures were radiographic gross total resection and surgical complications.		- Tumor progression and new permanent post-operative neurological deficit: significantly associated with late post-operative seizure.
* excluded 118 patients with multiple meningiomatosis.

5. Conclusions

Meningiomas are the most common non-malignant primary brain tumor and often associated with seizures. Seizure control is an important treatment goal because of the significant impact on patients’ quality of life. We identified age, convexity location, and peritumoral edema as the predictive risk factors of pre-operative seizures. In our experience, meningioma-related epilepsy appears to have generally a positive outcome following surgery and does not seem to be linked to oncological progression, even if further studies are needed.
Understanding seizure rates, risk factors, and possible mechanisms associated with meningioma-related epilepsy is crucial to better stratify and predict surgical outcome and optimally treat patients with the most effective treatment strategies.

Author Contributions

Conceptualization, G.P., A.N. and T.I.; methodology, G.P., A.N., S.P., D.B. and T.I.; validation, G.P. and T.I.; formal analysis, M.I.; investigation, A.N., G.P., S.P., M.E.Z. and T.I.; data curation, M.E.Z. and S.P.; writing—original draft preparation, G.P., A.N. and T.I.; writing—review and editing, M.S., M.V., L.V. and T.I.; supervision, M.S. and M.V. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

The study was conducted in accordance with the Declaration of Helsinki and approved by the Institutional Review Board of the University of Udine (Prot. IRB: 53/2023, Tit III cl 13 fasc. 5/2023).

Informed Consent Statement

Written informed consent was not provided considering the retrospective nature of the study. All the procedures performed were part of the routine care; written informed consent was obtained for surgery.

Data Availability Statement

All authors had full access to all the data in the study and take responsibility for the integrity of the data and the accuracy of the data analysis.

Conflicts of Interest

The authors declare no conflict of interest.

References

  1. Ostrom, Q.T.; Cioffi, G.; Waite, K.; Kruchko, C. CBTRUS Statistical Report: Primary Brain and Other Central Nervous System Tumors Diagnosed in the United States in 2014–2018. Neuro-Oncology 2021, 23, iii1–iii105. [Google Scholar] [CrossRef]
  2. Xue, H.; Svenisson, O.; Tomson, T.; Mathiesen, T. Intracranial meningiomas and seizures: A review of the literature. Acta Neurochir. 2015, 157, 1542–1548. [Google Scholar] [CrossRef]
  3. Xue, H.; Svenisson, O.; Bartek, J., Jr.; Forander, P.; Skyrman, S.; Kihlstrom, L.; Shafiei, R.; Mathiesen, T.; Tomson, T. Long-term control and predictors of seizures in intracranial meningioma surgery: A population-based study. Acta Neurochir. 2018, 160, 589–596. [Google Scholar] [CrossRef] [PubMed]
  4. Van Breemen, M.S.M.; Wilms, E.B.; Vecht, C.J. Seizure Control in Brain Tumors. Handb. Clin. Neurol. 2012, 104, 381–389. [Google Scholar] [CrossRef]
  5. Maschio, M.; Aguglia, U.; Avanzini, G.; Banfi, P.; Buttinelli, C.; Capovilla, G.; Casazza, M.M.L.; Colicchio, G.; Coppola, A.; Costa, C.; et al. Management of epilepsy in brain tumors. Neurol. Sci. 2019, 40, 2217–2234. [Google Scholar] [CrossRef]
  6. Sheth, R.D. Epilepsy surgery. Presurgical evaluation. Neurol. Clin. 2002, 20, 1195–1215. [Google Scholar] [CrossRef]
  7. Chen, W.C.; Magill, S.T.; Englot, D.J.; Baal, J.D.; Wagle, S.; Rick, J.W.; McDermott, M.W. Factors associated with pre- and post-operative seizures in 1033 patients undergoing supratentorial meningioma resection. Neurosurgery 2017, 81, 297–306. [Google Scholar] [CrossRef] [PubMed]
  8. Skardelly, M.; Rother, C.; Noell, S.; Behling, F.; Wuttke, T.V.; Schittenhelm, J.; Bisdas, S.; Meisner, C.; Rona, S.; Tabatabai, G. Risk Factors of Preoperative and Early Postoperative Seizures in Patients with Meningioma: A Retrospective Single-Center Cohort Study. World Neurosurg. 2017, 97, 538–546. [Google Scholar] [CrossRef]
  9. Li, X.; Wang, C.; Lin, Z.; Zhao, M.; Ren, X.; Zhang, X.; Jiang, Z. Risk factors and control of seizures in 778 Chinese patients undergoing initial resection of supratentorial meningiomas. Neurosurg. Rev. 2020, 43, 597–608. [Google Scholar] [CrossRef]
  10. Louis, D.N.; Perry, A.; Reifenberger, G.; von Deimling, A.; Figarella-Branger, D.; Cavenee, W.K.; Ohgaki, H.; Wiesterl, O.D.; Kleihues, P.; Ellison, D.W. The 2016 World Health Organization Classification of Tumors of the Central Nervous System: A summary. Acta Neuropathol. 2016, 131, 803–820. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  11. Fisher, R.S.; Acevedo, C.; Arzimanoglou, A.; Bogacz, A.; Cross, J.H.; Elger, C.E.; Engel, J., Jr.; Forsgren, L.; French, J.A.; Glynn, M.; et al. ILAE Officila Report: A Practical, Clinical Definition of Epilepsy. Epilepsia 2014, 55, 475–482. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  12. Engel, J., Jr.; Burchfiel, J.; Ebersole, J.; Gates, J.; Gotman, J.; Homan, R.; Ives, J.; King, D.; Lieb, J.; Sato, S.; et al. Long-term monitoring for epilepsy. Report of an IFCN committee. Electroencephalogr. Clin. Neurophysiol. 1993, 87, 437–458. [Google Scholar] [CrossRef]
  13. Simpson, D. The recurrence of intracranial meningiomas after surgical treatment. J. Neurol. Neurosurg. Psychiatry 1957, 20, 22–39. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  14. Fisher, R.S.; Cross, J.H.; French, J.A.; Higurashi, N.; Hirsch, E.; Jansen, F.E.; Lagae, L.; Moshé, S.L.; Peltola, J.; Roulet, P.E.; et al. Operational classification of seizure types by the International League Against Epilepsy: Position Paper of the ILAE Commission for Classification and Terminology. Epilepsia 2017, 58, 522–530. [Google Scholar] [CrossRef] [Green Version]
  15. Ius, T.; Tel, A.; Minniti, G.; Somma, T.; Solari, D.; Longhi, M.; De Bonis, P.; Scerrati, A.; Caccese, M.; Barresi, V.; et al. Advances in Multidisciplinary Management of Skull Base Meningiomas. Cancers 2021, 13, 2664. [Google Scholar] [CrossRef] [PubMed]
  16. Oyama, H.; Noda, S.; Negoro, M.; Kinomoto, T.; Miyachi, S.; Kuwayama, N.; Kajita, Y. Giant meningioma fed by the anterior choroidal artery: Successful removal following embolization—Case report. Neurol. Med.-Chir. 1992, 32, 839–841. [Google Scholar] [CrossRef] [Green Version]
  17. Gajbhiye, S.; Gosal, J.S.; Pandey, S.; Das, K.K. Apoplexy Inside a Giant Medial Sphenoid Wing Meningothelial (Grade I) Meningioma: An Extremely Rare but a Potentially Dangerous Complication. Asian. J. Neurosurg. 2019, 14, 961–963. [Google Scholar] [CrossRef]
  18. Englot, D.J.; Magill, S.T.; Han, S.J.; Chang, E.F.; Berger, M.S.; McDermott, M.W. Seizures in supratentorial meningioma: A systematic review and meta-analysis. J. Neurosurg. 2016, 124, 1552–1561. [Google Scholar] [CrossRef] [Green Version]
  19. Bogdanovic, I.; Ristic, A.; Ilic, R.; Bascarevic, V.; Bukumiric, Z.; Miljkovic, A.; Milisavljevic, F.; Stepanovic, A.; Lazic, I.; Grujicic, D. Factors associated with preoperative and early and late postoperative seizures in patients with supratentorial meningiomas. Epileptic Disord. 2023, 25, 244–254. [Google Scholar] [CrossRef]
  20. Hwang, K.; Joo, J.D.; Kim, Y.H.; Han, J.H.; Oh, C.W.; Yun, C.H.; Park, S.H.; Kim, C.Y. Risk factors for preoperative and late postoperative seizures in primary supratentorial meningiomas. Clin. Neurol. Neurosurg. 2019, 180, 34–39. [Google Scholar] [CrossRef]
  21. Wirsching, H.G.; Morel, C.; Gmür, C.; Neidert, M.C.; Baumann, C.R.; Valavanis, A.; Rushing, E.J.; Krayenbuhl, N.; Weller, M. Predicting outcome of epilepsy after meningioma resection. Neuro-Oncology 2016, 18, 1002–1010. [Google Scholar] [CrossRef] [Green Version]
  22. Chamberlain, M.C.; Blumenthal, D.T. Intracranial meningiomas: Diagnosis and treatment. Expert. Rev. Neurother. 2004, 4, 641–648. [Google Scholar] [CrossRef]
  23. Fathi, A.R.; Roelcke, U. Meningioma. Curr. Neurol. Neurosci. Rep. 2013, 13, 337. [Google Scholar] [CrossRef] [PubMed]
  24. Harward, S.C.; Rolston, J.D.; Englot, D.J. Seizures in meningioma. Handb. Clin. Neurol. 2020, 170, 187–200. [Google Scholar] [CrossRef] [PubMed]
  25. Schneider, M.; Güresir, A.; Borger, V.; Hamed, M.; Rácz, A.; Vatter, H.; Güresir, E.; Schuss, P. Preoperative tumor-associated epilepsy in patients with supratentorial meningioma: Factors influencing seizure outcome after meningioma surgery. J. Neurosurg. 2019, 11, 1–7. [Google Scholar] [CrossRef]
  26. Seyedi, J.F.; Pedersen, C.B.; Poulsen, F.R. Risk of seizures before and after neurosurgical treatment of intracranial meningiomas. Clin. Neurol. Neurosurg. 2018, 165, 60–66. [Google Scholar] [CrossRef]
  27. Baumgarten, P.; Sarlak, M.; Baumgarten, G.; Marquardt, G.; Seifert, V.; Strzelczyk, A.; Rosenow, F.; Freiman, T.M. Focused review on seizures caused by meningiomas. Epilepsy Behav. 2018, 88, 146–151. [Google Scholar] [CrossRef]
  28. Chaichana, K.L.; Pendleton, C.; Zaidi, H.; Olivi, A.; Weingart, J.D.; Gallia, G.L.; Lim, M.; Brem, H.; Quiñones-Hinojosa, A. Seizure control for patients undergoing meningioma surgery. World. Neurosurg. 2013, 79, 515–524. [Google Scholar] [CrossRef]
  29. Lee, J.W.; Wen, P.Y.; Hurwitz, S.; Black, P.; Kesari, S.; Drappatz, J.; Golby, A.J.; Wells, W.M., 3rd; Warfield, S.K.; Kikinis, R.; et al. Morphological characteristics of brain tumors causing seizures. Arch. Neurol. 2010, 67, 336–342. [Google Scholar] [CrossRef] [Green Version]
  30. Lieu, A.S.; Howing, S.L. Intracranial meningiomas and epilepsy: Incidence, prognosis and influencing factors. Epilepsy Res. 2000, 38, 45–52. [Google Scholar] [CrossRef] [PubMed]
  31. Rohringer, M.; Sutherland, G.R.; Louw, D.F.; Sima, A.A. Incidence and clinicopathological features of meningioma. J. Neurosurg. 1989, 71, 665–672. [Google Scholar] [CrossRef] [PubMed]
  32. Pistolesi, S.; Fontanini, G.; Camacci, T.; De Ieso, K.; Boldrini, L.; Lupi, G.; Padolecchia, R.; Pingitore, R.; Parenti, G. Meningioma-associated brain oedema: The role of angiogenic factors and pial blood supply. J. Neurooncol. 2002, 60, 159–164. [Google Scholar] [CrossRef]
  33. Ahmed, R.E.; Tang, H.; Asemota, A.; Huang, L.; Boling, W.; Bannout, F. Meningioma Related Epilepsy- Pathophysiology, Pre/postoperative Seizures Predicators and Treatment. Front. Oncol. 2022, 12, 905976. [Google Scholar] [CrossRef]
  34. Schaller, B. Brain Tumor and Seizures: Pathophysiology and its Implications for Treatment Revisited (Epilepsia, 2003; 44: 1223–1232). Epilepsia 2006, 47, 661–664. [Google Scholar] [CrossRef] [PubMed]
  35. Gadot, R.; Khan, A.B.; Patel, R.; Goethe, E.; Shetty, A.; Hadley, C.C.; Bayley, J.C.V.; Harmanci, A.S.; Klisch, T.J.; Yoshor, D.; et al. Predictors of postoperative seizure outcome in supratentorial meningioma. J. Neurosurg. 2021, 10, 515–524. [Google Scholar] [CrossRef] [PubMed]
  36. Brokinkel, B.; Hinrichs, F.L.; Schipmann, S.; Grauer, O.; Sporns, P.B.; Adeli, A.; Brokinkel, C.; Hess, K.; Paulus, W.; Stummer, W.; et al. Predicting postoperative seizure development in meningiomas—Analyses of clinical, histological and radiological risk factors. Clin. Neurol. Neurosurg. 2021, 200, 106315. [Google Scholar] [CrossRef]
  37. Hess, K.; Spille, D.C.; Adeli, A.; Sporns, P.B.; Brokinkel, C.; Grauer, O.; Mawrin, C.; Stummer, W.; Paulus, W.; Brokinkel, B. Brain invasion and the risk of seizures in patients with meningioma. J. Neurosurg. 2018, 130, 789–796. [Google Scholar] [CrossRef] [Green Version]
  38. Maschio, M.; Pauletto, G.; Zarabla, A.; Maialetti, A.; Ius, T.; Villani, V.; Fabi, A.; Koudriavtseva, T.; Giannarelli, D. Perampanel in patients with brain tumor-related epilepsy in real-life clinical practice: A retrospective analysis. Int. J. Neurosci. 2019, 129, 593–597. [Google Scholar] [CrossRef]
  39. Nilo, A.; Pauletto, G.; Gigli, G.L.; Vogrig, A.; Dolso, P.; Valente, M. Perampanel as add-on therapy in epilepsies with known etiology: A single center experience with long-term follow-up. Epilepsy Behav. Rep. 2020, 15, 100393. [Google Scholar] [CrossRef]
  40. Glantz, M.J.; Cole, B.F.; Forsyth, P.A.; Recht, L.D.; Wen, P.Y.; Chamberlain, M.C.; Grossman, S.A.; Cairncross, J.G. Practice parameter: Anticonvulsant prophylaxis in patients with newly diagnosed brain tumors. Report of the Quality Standards Subcommittee of the American Academy of Neurology. Neurology 2000, 54, 1886–1893. [Google Scholar] [CrossRef] [Green Version]
  41. Baumgarten, P.; Sarlak, M.; Monden, D.; Spyrantis, A.; Bernatz, S.; Gessler, F.; Dubinski, D.; Hattingen, E.; Marquardt, G.; Strzelczyk, A.; et al. Early and Late Postoperative Seizures in Meningioma Patients and Prediction by a Recent Scoring System. Cancers 2021, 13, 450. [Google Scholar] [CrossRef] [PubMed]
  42. Zheng, Z.; Chen, P.; Fu, W.; Zhu, J.; Zhang, H.; Shi, J.; Zhang, J. Early and late postoperative seizure outcome in 97 patients with supratentorial meningioma and preoperative seizures: A retrospective study. J. Neurooncol. 2013, 114, 101–109. [Google Scholar] [CrossRef] [PubMed]
Jpm 13 01124 g001 550
Figure 1. A brain MRI of a patient with left frontal meningioma. (A,B) show pre-operative postcontrast T1-weighted (A) and T2-weighted TSE MRI sequences, demonstrating ROI segmentation of lesion and peritumor edema, circumferentially outlined, using Horos software. (C,D) display postcontrast T1-weighted and T2-weighted TSE MRI sequences after surgical resection.
Figure 1. A brain MRI of a patient with left frontal meningioma. (A,B) show pre-operative postcontrast T1-weighted (A) and T2-weighted TSE MRI sequences, demonstrating ROI segmentation of lesion and peritumor edema, circumferentially outlined, using Horos software. (C,D) display postcontrast T1-weighted and T2-weighted TSE MRI sequences after surgical resection.
Jpm 13 01124 g001
Table
Table 1. Demographic, clinical, radiological, histological and molecular data of all study patients.
Table 1. Demographic, clinical, radiological, histological and molecular data of all study patients.
Variables
No. of patients358
Gender, n (%)
    Male
    Female
115 (32.1)
243 (67.9)
Age, (years)
    Mean (±SD)
    Range
Age subclasses, n (%)
    20–29 y
    30–39 y
    40–49 y
    50–59 y
    60–69 y
    70–79 y
    ≥80 y
62.1 (±13.1)
23–90

2 (0.5)
16 (4.5)
46 (12.8)
82 (22.9)
96 (26.8)
92 (25.7)
24 (6.8)
Pre-operative KPS, Mean (±SD)92.8 (20–100)
Onset symptoms, n (%)
    Seizures
    Other neurological symptoms
    No symptoms (incidental meningiomas)
73 (20.4)
226 (63.1)
59 (16.5)
Tumor Side, n (%)
    Right
    Left
    Midline
159 (44.4)
160 (44.7)
39 (10.9)
Tumor Location, n (%)
    Skull base
    Non-skull base (convexity)
148 (41.3)
210 (58.7)
Pre-operative tumor volume (T1-weighted MRI images–cm3)
    Mean
    Range
20.7
1–128
Pre-operative peritumoral edema volume (T2-weighted MRI images–cm3)
    Mean
    Range
22.9
1–227
Type of Resection, n (%)
    Gross Total Resection (I, II)
    Subtotal Resection (III, IV)
283 (79.1)
75 (20.9)
Histological Grade, n (%)
    WHO grade I
    WHO grade II
    WHO grade III
302 (84.4)
50 (13.9)
6 (1.7)
Molecular aspects
    Ki67, mean (±SD)
    Mitotic index, mean (±SD)
    Brain Invasion, n (%)
4.7 (±6.2)
1.81 (±4.8)
23 (6.5)
Post-operative radiotherapy, n (%)
    Yes
    No
12 (3.3)
346 (96.7)
Post-operative neurological deficit 1 week after surgery, n (%)
    Yes
    No
113 (32)
245 (68)
Post-operative neurological deficit at 6 months, n (%)
    Yes
    No
41 (11.9)
317 (88.1)
Legend: KPS, Karnofsky Performance Status; MRI, Magnetic Resonance Imaging; SD, Standard Deviation; WHO, World Health Organization.
Table
Table 2. Characteristics of patients with meningioma-related epilepsy.
Table 2. Characteristics of patients with meningioma-related epilepsy.
Variables
No. of patients73
Gender, n (%)
   Male
   Female
30 (41.1)
43 (58.9)
Age, (years)
   Mean (±SD)
   Range
Age subclasses, n (%)
   20–29 y
   30–39 y
   40–49 y
   50–59 y
   60–69 y
   70–79 y
   >80 y
56 (±10.1)
39–87

0 (0)
6 (8.2)
13 (17.8)
22 (30.1)
19 (26.1)
10 (13.7)
3 (4.1)
Seizure frequency, n (%)
   Single
   Multiple
45 (61.6)
28 (38.4)
Seizure onset, n (%)
   Focal seizures
   Focal to bilateral tonic–clonic seizures
28 (38.4)
45 (61.6)
Seizure type, n (%)
   Motor
   Non-motor
        Somato-sensitive
        Cognitive
        Autonomic
        Affective
58 (79.5)
15 (20.5)
    10 (13.7)
    2 (2.7)
    2 (2.7)
    1 (1.4)
Pre-operative EEG features, n (%)
   Normal activity
   Slow activity
   Epileptiform activity
36 (49.4)
21 (28.7)
16 (21.9)
ASMs regimen, n (%)
   Monotherapy
   Polytherapy
67 (91.7)
6 (8.3)
ASMs, n (%)
   Levetiracetam
   Carbamazepine
   Valproic acid
   Perampanel
55 (82.1)
7 (10.4)
5 (7.5)
6 (8.3)
Legend: ASM, anti-seizure medication; EEG, electroencephalogram.
Table
Table 3. Comparative analysis between patients with seizures and those without seizures at onset.
Table 3. Comparative analysis between patients with seizures and those without seizures at onset.
VariablesOnset without SeizuresOnset with Seizuresp-Value
n = 285n = 73
Age, median (IQR)66 (53–74)56 (49–67)0.001
Female, n (%)
Male, n (%)		200 (70.2)
85 (29.8)		43 (58.9)
30 (41.1)		0.07
Pre-operative KPS, median (IQR)100 (90–100)90 (90–100)0.002
Post-operative KPS at 6 months, median (IQR)100 (90–100)100 (90–100)0.89
Tumor Side, n (%)
   Right
   Left
   Midline
123 (43.5)
129 (45.6)
31 (10.9)
36 (49.3)
31 (42.5)
6 (8.2)		0.61
Tumor Location, n (%)
   Non-skull base (convexity)
   Skull base		157 (55.1)
128 (44.9)		53 (72.6)
20 (27.4)
<0.001
Simpson Grade, n (%)
   Grade 1–2
   Grade 3–4
218 (76.5)
67 (23.5)
65 (89.0)
8 (11.0)		0.02
Pre-operative neurological deficit, n (%)152 (53.3)27 (37.0)0.01
Post-operative neurological deficit (6 months), n (%)83 (32.1)21 (28.7)0.91
Histological grade, n (%)
   WHO grade I
   WHO grade II
   WHO grade III
246 (86.3)
33 (11.6)
6 (2.1)
56 (76.7)
16 (21.9)
1 (1.4)		0.06
Molecular aspects
   Ki67, median (IQR)
   Mitotic index, median (IQR)
   Brain invasion, n (%)
3 (2–5)
1 (0–2)
17 (6.0)
3 (2–5)
1 (0–2)
6 (8.2)
0.82
0.59
0.43
Pre-operative tumor volume, median (T1) (IQR)20.6 (9.1–39.7)20.8 (9.1–45.3)0.70
Peri-tumoral Edema (T2), n (%)122/271 (42.8)56/71 (76.7)<0.001
Disease progression, n (%)23 (8.1)6 (8.2)0.97
Legend: KPS, Karnofsky Performance Status; IQR, interquartile range; WHO, World Health Organization. Bold values are statistically significant.
Table
Table 4. Risk factors associated with pre-operative seizures.
Table 4. Risk factors associated with pre-operative seizures.
VariableUnivariate AnalysisMultivariate Analysis
OR95% CIp-ValueOR95% CIp-Value
Female0.610.36–1.04 0.067
Age0.970.95–0.990.0030.950.93–0.97<0.001
Pre-operative KPS0.980.96–1.000.109
Tumor Side
   Left vs. Right
0.82
0.48, 1.41
0.474
Tumor Location
   Skull-base vs. convexity
   MCF vs. PCF
0.06
29.57
0.01–0.48
3.44–254.08
0.007
0.002
0.08
17.05
0.01–0.62
1.86–155.94
0.016
0.012
Simpson Grade
   3 + 4 vs. 1 + 2		0.400.18–0.880.022
WHO Grade
   Grade II vs. Grade I
2.17
1.12–4.22
0.022
Pre-operative tumor volume1.000.99–1.010.814
Pre-operative peritumoral Edema4.562.46–8.46<0.0015.282.62–10.61<0.001
Pre-operative neurological deficit0.510.30–0.870.0140.750.42–1.370.352
Legend: CI, confidential interval; KPS, Karnofsky Performance Status; MCF, middle cranial fossa; OR, odds ratio; PCF, posterior cranial fossa; WHO, World Health Organization. Bold values are statistically significant.
Table
Table 5. Seizure outcome in patients with pre-operative meningioma-related epilepsy at 12- and 24-months follow-up.
Table 5. Seizure outcome in patients with pre-operative meningioma-related epilepsy at 12- and 24-months follow-up.
VariablesAt 12 MonthsAt 24 Months
Engel Class Ia
(n = 64)		Engel Class > Ia
(n = 9)		p-ValueEngel Class Ia
(n = 60)		Engel Class > Ia
(n = 8)		p-Value
Female, n (%)
Male, n (%)		38 (59.3)
26 (40.7)		5 (55.5)
4 (44.5)		0.9636 (60.0)
24 (40.0)		5 (62.5)
3 (37.5)		0.98
Age, median (IQR)57 (48–68)56 (50–66)0.7756 (47.5–66.5)56 (50–69)0.79
Tumor Side, n (%)
   Right
   Left
   Midline
33 (51.5)
27 (42.3)
4 (6.2)
4 (44.4)
2 (22.2)
3 (33.3)
0.05
30 (50.0)
27 (45.0)
3 (5.0)
4 (50.0)
2 (25.0)
2 (25.0)
0.05
Tumor Location
   Non-skull base (Convexity)
   Skull base
48 (75.0)
16 (25.0)
4 (44.4)
5 (55.6)

0.04
 
45 (75.0)
15 (25.0)
4 (50.0)
4 (50.0)

0.04
 
Simpson Grade
   Grade 1–2
   Grade 3–4
59 (92.2)
5 (7.8)
6 (66.7)
3 (33.3)
0.06
55 (91.7)
5 (8.3)
6 (75.0)
2 (25.0)
0.06
Pre-operative tumor volume, median (IQR)
21.4 (9.1–34.9)
25.1 (10.2–63.3)
0.66
20.8 (9.0–44.8)
33.5 (15.0–45.4)
0.35
Seizure type, n (%)
   Focal seizures
   Focal to bilateral tonic-clonic seizures		25 (39.1)
39 (60.9)		4 (44.4)
5 (55.6)		1.0023 (38.3)
37 (61.7)		3 (37.5)
5 (62.5)
1.00
 
Seizure frequency, n (%)
   Single seizure
   Multiple seizures
40 (62.5)
24 (37.5)
4 (44.4)
5 (55.6)
0.30
37 (61.7)
23 (38.3)
5 (62.5)
3 (37.5)
1.00
Motor seizures, n (%)52 (81.2)6 (66.7)0.3948 (80.0)5 (62.5)0.36
ASMs regimen, n (%)
   Monotherapy
   Polytherapy
63 (98.4)
1 (1.6%)
7 (77.8)
2 (22.2)
0.03
59 (98.3)
1 (1.7)
1 (12.5)
7 (87.5)
0.04
Legend: ASM, anti-seizure medication; IQR, interquartile range. Bold values are statistically significant.
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Pauletto, G.; Nilo, A.; Pez, S.; Zonta, M.E.; Bagatto, D.; Isola, M.; Verriello, L.; Valente, M.; Skrap, M.; Ius, T. Meningioma-Related Epilepsy: A Happy Ending? J. Pers. Med. 2023, 13, 1124. https://doi.org/10.3390/jpm13071124

AMA Style

Pauletto G, Nilo A, Pez S, Zonta ME, Bagatto D, Isola M, Verriello L, Valente M, Skrap M, Ius T. Meningioma-Related Epilepsy: A Happy Ending? Journal of Personalized Medicine. 2023; 13(7):1124. https://doi.org/10.3390/jpm13071124

Chicago/Turabian Style

Pauletto, Giada, Annacarmen Nilo, Sara Pez, Maria Elisa Zonta, Daniele Bagatto, Miriam Isola, Lorenzo Verriello, Mariarosaria Valente, Miran Skrap, and Tamara Ius. 2023. "Meningioma-Related Epilepsy: A Happy Ending?" Journal of Personalized Medicine 13, no. 7: 1124. https://doi.org/10.3390/jpm13071124

APA Style

Pauletto, G., Nilo, A., Pez, S., Zonta, M. E., Bagatto, D., Isola, M., Verriello, L., Valente, M., Skrap, M., & Ius, T. (2023). Meningioma-Related Epilepsy: A Happy Ending? Journal of Personalized Medicine, 13(7), 1124. https://doi.org/10.3390/jpm13071124

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