Exploring Correlation of PSEN1 E280A Mutation with Clinical Features in Patients with Glioma Related Seizures
Exploring Correlation of PSEN1 E280A Mutation with Clinical Features in Patients with Glioma Related Seizures
Zhi Qiang Gao*, Dan Dan Zhang, Qin Gmei Qin, Xiu Xiu Li, Li Li,
Yan Zhong Xue and Shifeng Guo
Department of Neurology, Linyi Central Hospital, Linyi City, Shandong Province, 276400, China
ABSTRACT
The correlation between Presenilin-1 (PSEN1) E280A mutation and clinical characteristics of glioma-related seizures (GRS) was explored. For this purpose, brain tissue samples were collected from 40 patients diagnosed with glioneuronal tumors (GNTs), including 25 cases of gangliogliomas (GGs) and 15 cases of dysembryoplastic neuroepithelial tumors (DNTs). Then, the DNA of GNTs tissues was extracted, and the PSEN1 E280A mutation was detected by sequencing. Finally, the correlation of PSEN1 E280A mutation with clinical characteristics was analyzed. PSEN1 E280A mutation was detected in 16 GNTs patients (44% in GGs (11/25) and 33.3% in DNTs (5/15)). PSEN1 E280A mutation was obviously elevated in females (10/16, 62.5%) versus in males (6/24, 25%) (P = 0.025). Meanwhile, more extensive seizure types were present in GNTs with PSEN1 mutations versus wilds (P = 0.001), but there was no clear correlation between PSEN1 and clinical manifestations like age of seizure, operative age, duration and absence of seizures after surgery. To conclude, PSEN1 E280A mutation is present in GNTs seizures patients, and greatly associated with multiple types of seizures and gender. The requirement of larger sample studies and long-term follow-up is implemented for further confirmation.
Article Information
Received 21 January 2022
Revised 18 March 2022
Accepted 08 April 2022
Available online 02 November 2022
(early access)
Published 13 December 2023
Authors’ Contribution
ZQG conceived the idea and designed the study. DDZ and QGQ analyzed the data. XXL, LL, YZX and SG contributed to literature review. ZQG wrote the manuscript. All authors read and approved the final manuscript.
Key words
Presenilin-1 E280A, Dysembryoplastic neuroepithelial tumors, Glioneuronal tumors, Gangliogliomas, Seizures
DOI: https://dx.doi.org/10.17582/journal.pjz/20220121100106
* Corresponding author: [email protected]
0030-9923/2024/0001-0193 $ 9.00/0
Copyright 2024 by the authors. Licensee Zoological Society of Pakistan.
This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
INTRODUCTION
In line with the European Epileptic Brain Bank’s data, a quarter of patients undergoing epilepsy surgery suffer from brain tumors (Blumcke et al., 2014). Glioneuronal tumor (GNTs), consisting of gangliogliomas (GGs) and dysembryoplastic neuroepithelial tumors (DNTs) are extremely familiar histological kind. The location of slow growing tumors is the neocortex, and the linked symptoms will be manifested at a young age, among which, epilepsy is a greatly salient, and frequently the only neurological symptom. Under the microscope, the symptoms manifest as the differentiation of neurons and glial cells, revealing as the hybrid neural epithelium cell types, including malformed neurons and glial elements (Delev et al., 2020). Cortical dysplasia frequently coexist, suggesting an advanced mechanism of these lesions (Prabowo et al., 2014). As epilepsy surgery is advancing, GNTs are gaining much more attention.
Presenilin-1 (PSEN1) is believed to mediate amyloid precursor protein (APP) processing through its influence on gamma-secretase (an enzyme cutting APP). Abnormal PSEN1 has been observed in various cancers (Ma et al., 2018; Gou et al., 2020). In the meantime, studies have clarified that PSEN1 mutations occupy 95% of familial autosomal dominant early-onset alzheimer’s disease (AD) cases (Hunter and Brayne, 2018), whereas PARK-DJ1 mutations, PARK-Parkin or PARK PINK1 are extremely familiar single-gene reasons of early-onset Parkinson’s disease (Niemann and Jankovic, 2019). Up to now, over 280 pathogenic mutations of PSEN1 have appeared (Shen et al., 2019), characterized by ataxia, globular symptoms, spastic paraplegia and extrapyramidal symptoms (dystonia, myo clonus, Parkinson’s disease and tremors), and been associated with neuropsychiatric and neurobehavioral disorders, neurocognition and rapid cognitive decline of varying degrees of severity (Carecchio et al., 2017). Studies have affirmed that point mutations in codon 280 of PSEN1 cause the change of glutamate to alanine (Alzheimer’s Disease Collaborative Group, 1995), which has been characterized in antioquia, colombia (Lalli et al., 2014; Ochoa et al., 2017; Fleisher et al., 2012). Moreover, PSEN1 E280A has been demonstrated to change the proteolytic process of Aβ C-terminal AβPP through prosenectin/γ-secretase, thereby augmenting the deposition mechanism (Sisodia, 2001; Sisodia and George-Hyslop, 2002) of amyloid β (Aβ(1-42/43)) (Lemere et al., 1996). Nevertheless, the correlation between PSEN1 E280A mutation and clinicopathological features in patients with seizures was hardly explored.
In this study, clinical and pathological data were gained from 40 patients with epileptic GNTs. The purpose was verification of the presence of PSEN1 E280A mutation in epileptic GNTs and explore its association with clinical features.
MATERIALS AND METHODS
Subjects
From September 2014 to March 2018, brain tissue samples were collected from patients undergoing epileptic surgery in Linyi Central Hospital, of which 40 cases were diagnosed as GNTs (including 25 GGs and 15 DNTs) in line with the tumor classification in central nervous system revised by WHO in 2007. A detailed history manifested clinical features like demographic data, age of seizures, duration of seizures, and type of seizures, previous history (i.e., head trauma, hypoxic-ischemic brain injury, encephalitis), epilepsy, and family history of brain tumor, etc. All patients (n = 40) were received with noninvasive long-term Video-Electroencephalography (VEEG), postoperative seizure time, medication, seizure and magnetic resonance imaging (MRI) results. Multiple seizure kinds were regarded as two or over two kinds, consisting of partial seizure evolving into secondary systemic seizure, simple partial seizure, complex partial seizure, etc. Follow-up was over 3 months. The approvement of this study was via the Ethics Committee of Linyi Central Hospital.
Tissue immunofluorescence
The brain tumor specimens were fixed with 10% buffered formalin and embedded in paraffin, and 4 μm sections were cut for immunostaining. Incubation of the sections was with primary anti-PSEN1 antibody (1: 1000, Abcam) and second antibody. Immunofluorescence images were obtained with a Zeiss LSM 710 confocal microscope. Staining of the nucleus was via 4’, 6-diamidino-2-phenylindole.
DNA extraction and PSEN1 E280A mutation analysis
DNA was extracted from tissues with the QIAamp DNA FFPE Tissue Kit (QIAGNE Cat No: 56404, Germany) under manufacturer’s instructions. PCR amplification and sequencing of PSEN1 E280A was done accourding to Fleisher et al. (2015). The purified PCR products were sequenced vis an ABI3730xl sequencer (Applied Biosystems, Foster City, CA).
Statistical analysis
All analyses were done via Prism software. Description of continuous variables was via means and ranges. Categorical variables having proportions and percentages were manifested. The Student’s t test was employed for assessment of differences of groups (duration of epilepsy, age of seizure, and age at surgery), but two-tailed chi-square or Fisher’s exact tests for evaluation of the correlation between PSEN1 E280A mutation and other clinical manifestations (multiple seizure type, site, drug-resistant epilepsy, tumor location, post-operation seizure-free, etc.). P < 0.05 was considered statistically significant.
RESULTS
Study characteristics
Forty patients (24 males, 16 females) with mean duration of seizures 5.4 years, and the mean age of seizures 21.0 years. Approximately 75% of the patients were under age of 35, and the mean age of surgery was 25.4 years (Table I). In 40 patients, 28 (70%) owned a drug-resistant seizures history. Partial seizures were an extremely familiar kind of seizures, accounting for 85% of the sample. Presence of two or more seizure types was in seventeen patients (42.5%). GNTs patients were with complex partial seizures (plant-based or affective aura, psychosensory aura, autosomia and epileptic seizure) and partial seizures evolving into secondary systemic seizures. Only 3 patients were affirmed with a prior history of febrile seizures. The patients had no previous encephalitis, cerebral trauma, hypoxic-ischemic brain injury, and none of the patients reported a family history of brain tumors. Among the 32 patients diagnosed by non-invasive long-term VEEG examination, 26 patients presented with slow wave, and 30 patients presented with epileptic discharge. The lesions could be clearly displayed in the 40 patients implemented with MRI examination, and the extremely familiar sites of GNTs were the temporal and the frontal lobes (Table I). In GGs, major of the lesions were cystic or solid in nature, with full-bottomed T1 and T2 signals. MRI of DNTs manifested as clear edges of the lesions, with long T1 and T2 signals. Most were concomitant with one or more cysts or septations, with occasional triangular or gyrus appearance. Moreover, MRI features of PSEN1 E280A mutant and wild-type (WT) patients were similar. Surgical treatment was implemented in all patients, containing lesionectomy and resection of epileptogenic focus, and 25 GGs and 15 DNTs were present. The performance of focal cortical dysplasia (FCD), also known as FCD IIIb, was detected in 9 GGs. Follow-up must be for at least 3 months. Luckily, 80% (32/40) of the patients were seizure-free, and the other 10 patients assured a clear decline in seizure frequency (Table I).
Table I. Summary of clinical manifestations of patients.
Feature |
GNTs (n = 40) |
GGs (n = 25) |
DNTs (n = 15) |
Male/female |
24/16 |
15/10 |
9/6 |
Mean age of seizures years (range) |
21.0 (0.5-54) |
19.6 (0.5-55) |
23.2 (3-52) |
Duration of epilepsy years (range) |
5.4 (0.4-32) |
5.6 (0.2-34) |
3.9 (0.3-15) |
Mean age at surgery years (range) |
25.4 (3.5-50) |
23.6 (2.5-52) |
24.3 (4-51) |
Febrile convulsion (positive/ negative) |
3/37 |
2/23 |
1/14 |
Past history (positive/negative) |
0/40 |
0/25 |
0/15 |
Family history (positive/negative) |
0/40 |
0/25 |
0/15 |
Multiple seizure types (yes/no) |
17/23 |
12/13 |
5/10 |
VEEG at diagnosis |
|||
Negative |
0 |
0 |
0 |
Slow wave |
26 |
18 |
8 |
Epileptiform discharge |
30 |
20 |
10 |
NA |
10 |
7 |
3 |
Drug-resistant seizures (yes/no) |
28/12 |
18/7 |
10/5 |
Location |
|||
Temporal lobe |
28 |
20 |
8 |
Frontal lobe |
8 |
5 |
3 |
Parietal lobe |
4 |
3 |
1 |
Coexisting with FCD (yes/no) |
9/31 |
9/16 |
0/15 |
Postoperative seizure-free (yes/no) |
32/8 |
20/5 |
12/3 |
PSEN1 E280A mutation is found in GNTs
DNA sequencing revealed PSEN1 E280A mutation in 16 patients (Fig. 1A-D), including 11 GGs (44% mutation frequency), 5 DNTs (33.3% mutation frequency), and 6 males and 10 females. In the mutant, there were the mean age of seizures 20.0 years; the mean duration of seizures 5.3 years; the mean surgical age 24.2 years; 75% (12/16) was drug-resistant epilepsy, which was one of multiple seizure types. Location of major of the GNTs of PSEN1 E280A mutations was in the temporal lobe (Fig. 2). Among them, 3 cases were related to FCD and 75% of patients were with PSEN1 E280A mutation had no seizures after surgery, lasting over 3 months (Table II).
Correlation between PSEN1 E280A mutation and clinical characteristics in GNTs
The possibility of PSEN1 E280A mutation in females (10/16, 62.5%) was greatly elevated versus that in males (6/24, 25%) (P = 0.025). Meanwhile, more extensive seizure types were in GNTs with PSEN1 mutations versus WT (P= 0.001). Nevertheless, PSEN1 status was not greatly linked with a number of clinical features, like seizure age, duration of seizures, surgical age, febrile convulsion, drug-resistant seizures, tumor location and seizure-free time after surgery (Table II). Moreover, 28 patients with drug-resistant epilepsy (12 with PSEN1 E280A mutation) were chosen for further evaluation. Within this subgroup, consistence of the results of PSEN1 mutation and WT was with the above analysis (gender P = 0.020; multiple seizure kinds P = 0.019) (Table III).
Table II. Correlation between PSEN1 E280A mutation and clinical characteristics in GNTs.
Parameter |
PSEN1 E280A mutation |
PSEN1 wild type |
P |
Gender (male/female) |
6/10 |
18/6 |
0.025 |
Age of seizures years (range) |
20.0 (2-51) |
20.6 (1.5-54) |
0.758 |
Duration of seizures years (range) |
5.3 (0.2-20) |
5.0 (0.5-30) |
0.866 |
Age at surgery years (range) |
24.2 (5-52) |
27.5 (2.5-50) |
0.673 |
Febrile convulsion (positive/negative) |
1/15 |
2/22 |
1.000 |
Multiple seizure kinds (yes/no) |
12/4 |
5/19 |
0.001 |
Drug-resistant seizures (yes/no) |
12/4 |
16/8 |
0.729 |
Location (temporal/other) |
13/3 |
15/9 |
0.297 |
Coexist with FCD (yes/no) |
4/12 |
5/19 |
1.000 |
Postoperative seizure free (yes/no) |
12/4 |
20/4 |
0.691 |
Table III. Correlation of PSEN1 E280A mutation with clinical characteristics in drug-resistant epilepsy.
Parameters |
PSEN1 E280A mutation |
PSEN1 wild type |
P |
Gender (male/female) |
3/9 |
12/4 |
0.020 |
Age of seizures years (range) |
21.2 (1.4-51) |
22.6 (0.6-54) |
0.668 |
Duration of seizures years (range) |
5.1 (0.3-18) |
5.0 (0.4-32) |
0.769 |
Age at surgery years (range) |
25.6 (4-50) |
26.5 (2.7-53) |
0.578 |
Febrile convulsion (positive/ negative) |
1/11 |
1/15 |
1.000 |
Multiple seizure types (yes/no) |
8/4 |
3/13 |
0.019 |
Drug-resistant seizures (yes/no) |
9/3 |
12/4 |
1.000 |
Location (temporal/other) |
10/2 |
11/5 |
0.662 |
Coexisting with FCD (yes/no) |
3/9 |
4/12 |
1.000 |
Postoperative seizure free (yes/no) |
8/4 |
11/5 |
1.000 |
The correlation of PSEN1 E280A mutation and clinical features in DNTs and GGs
GGs subgroup analysis manifested that PSEN1 state with various epilepsy types had apparent correlation (P < 0.001), but no statistical significance (P = 0.116) exhibited in gender differences (Table IV). Similar results were indicated in the DNTs subgroup (Table V).
Table IV. Correlation between PSEN1 E280A mutation and clinical characteristics in GGs.
Parameter |
PSEN1 E280A mutation |
PSEN1 wild type |
P |
Gender (male/female) |
4/7 |
10/4 |
0.116 |
Age of seizures years (range) |
24.0 (3-54) |
22.1 (1.5-55) |
0.534 |
Duration of seizures years (range) |
5.5 (0.4-19) |
5.3 (0.2-33) |
0.476 |
Age at surgery years (range) |
24.0 (5.5-53) |
25.4 (2.8-54) |
0.603 |
Febrile convulsion (positive/ negative) |
0/11 |
2/12 |
0.487 |
Multiple seizure kinds (yes/no) |
10/1 |
2/12 |
< 0.001 |
Drug-resistant seizures (yes/no) |
7/4 |
10/4 |
1.000 |
Location (temporal/other) |
9/2 |
11/3 |
1.000 |
Coexisting with FCD (yes/no) |
3/8 |
5/9 |
1.000 |
Postoperative seizure free (yes/no) |
8/3 |
12/2 |
0.623 |
Table V. Correlation between PSEN1 E280A mutation and clinical characteristics in DNTs.
Parameter |
PSEN1 E280A mutation |
PSEN1 wild type |
P |
Gender (male/female) |
2/3 |
8/2 |
0.251 |
Age of seizures years (range) |
20.5 (1-52) |
21.8 (0.5-53) |
0.322 |
Duration of seizures years (range) |
5.2 (0.3-21) |
5.4 (0.6-31) |
0.549 |
Age at surgery years (range) |
25.8 (4.7-50) |
22.5 (2.5-51) |
0.428 |
Febrile convulsion (positive/negative) |
0/5 |
1/9 |
1.000 |
Multiple seizure kinds (yes/no) |
5/0 |
0/10 |
< 0.001 |
Drug-resistant seizures (yes/no) |
3/2 |
7/3 |
1.000 |
Location (temporal/other) |
3/2 |
5/5 |
1.000 |
Coexisting with FCD (yes/no) |
0/5 |
0/10 |
1.000 |
Postoperative seizure free (yes/no) |
4/1 |
8/2 |
1.000 |
DIsCUSSION
GNTs are frequently defined as a low-grade glioma with mixed neuron-glioma. The seizure frequency of DNTs is up to 100%, and that of GGs is up to 80%-90% (van Breemen et al., 2007). Seizures linked with GNTs are usually not mediated via antiepileptic drugs, so GNTs are also grouped as long-term seizures related tumors, but additionally, highly responsive to surgical treatment (Luyken et al., 2003).
In this study, 40 epileptic patients with GNTs were collected. Additionally, its clinical and pathological characteristics are greatly coincident with former studies (Bonney et al., 2015, 2016; Chassoux et al., 2013). The study manifested that GNTs were widespread in men (male: female = 3: 2) and consistently presented as early occurrence but long duration seizures, coincident with plenty of former studies (Blümcke, 2009; Thom et al., 2011). Meanwhile, in line with this study, most frequent location of GNTs is the temporal lobe (Thom et al., 2012; Martinoni et al., 2015). Moreover, partial seizures (chiefly complex) were the extremely familiar kind of seizures, with about 50% patients having two or more seizures kinds.
At present, PSEN1 E280A mutation is widely present in various central nervous system diseases, particularly in AD, stimulating wide attention (Lanoiselée et al., 2017; Qiu, 2020; Jiang, 2020; Raut et al., 2021). Here, it was demonstrated PSEN1 E280A mutation in 16 of 40 patients (40%), with 44% mutation rate in GGs and 33.3% in DNTs. It was acknowledged that this study is the first case in patients with GRS.
PSEN1 E280A mutation and its clinical relevance were evaluated in GNTs in the study, which has rarely been previously reported. In this study, the frequency of PSEN1 E280A mutation in female patients was greatly elevated versus male, particularly in patients with drug-resistant seizures. This result might be directly or indirectly implicated with sex hormones with ambiguous mechanism. This association with gender is interesting and deserves further confirmation.
In the meantime, clear association of PSEN1 E280A mutation was manifested with multiple seizure types. The semiotic characteristics of epileptic seizure are associated with epileptogenic area and transmission network (Chauvel and McGonigal, 2014). It was hypothesized that there was a complex interaction between PSEN1 E280A mutation and seizures, and the mutation may be influential in neural networks, resulting in ictal discharge of different kinds of neurons in various parts, further leading to different types of seizures. Nevertheless, further research is required to confirm this. Noticeably, drug-resistance was present in nearly all patients with multiple seizure kinds. Thus, this could mean that PSEN1 E280A mutation could induce multiple kinds of seizures, which could make drug therapy difficult in these patients. No association was found between PSEN1 E280A mutation and age of seizure or clinical variables like age at surgery, tumor location, duration of epilepsy, etc. Unlike previous Alzheimer’s studies, the subjects in this study were patients with seizures. Therefore, postoperative seizures were focused. However, a surprising result was obtained that the incidence of postoperative seizures was not linked with PSEN1 E280A mutation. Owing to the limited follow-up time, further confirmation of the connection of PSEN1 E280A mutation together with postoperative prognosis of seizures is required.
Some limitations are present in the study. Owing to limited follow-up time of some cases, changes of the seizure-free findings with time advancing, and not large sample size, the ability to further subgroup analysis and providing for more accurate results was limited. Large sample explorations and long-term follow-up are needed to testify the validity of the findings.
Statement of conflict of interest
The authors have declared no conflict of interest.
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