Your search keyword '"Cacna1a"' showing total 517 results

1. N-Acetyl-leucine in progressive CACNA1A ataxia: A case series

Author

Martakis, K., Giorgi, M., Spanou, M., Neubauer, B.A., Dinopoulos, A., and Hahn, A.

Published

2025

2. "Living with" CACNA1A -related hemiplegic migraine, a disease concept model.

Author

Schaare, Donna, Allison, Kendra, Skorge, Kara, Fox, Pangkong, Lusk, Laina, Sarasua, Sara M., Helbig, Ingo, and Boccuto, Luigi

Subjects

NEUROLOGICAL disorders, PATIENT experience, CAREGIVERS, PATIENTS' attitudes, LOSS of consciousness

Abstract

Introduction: CACNA1A -related Hemiplegic Migraine (HM) is a rare neurological disorder distinguished by paroxysmal episodes of hemiparesis/hemiplegia with and without headache. Clinical features have been widely characterized, yet the impacts of the paroxysmal events on the patient and caregiver have not been thoroughly explored. Disease concept models are formal frameworks used to describe the lived experiences of patients and their families, offering a source for surrogate endpoints for clinical trials. Methods: We completed 13 semi-structured interviews with caregivers of 12 individuals diagnosed with CACNA1A -related HM. We methodically coded themes, grouping concepts into three domains. We measured the occurrence of concepts throughout all interviews and subgroups stratified by age categories. Results: Over 11 h of interviews yielded 2,018 references to 27 distinct concepts. Established symptoms such as seizures (87 references; including status epilepticus 27 references), hemiparesis/hemiplegia (24 references), and unconsciousness (17 references) were referenced, as well as previously underreported symptoms such as apneic episodes (32 references), lost ability to eat (13 references), and vascular access challenges (10 references). The symptom impacts were largely medical (294 references), followed by health (101 references), emotional (36 references), daily living (28 references), and social (26 references). Caregiver impacts were the most referenced domain (995 references), with the pivotal effects seen in caregiver requirements (355 references), emotional (245 references), HM treatments (179 references), daily living (148 references), and health support (135 references). Discussion: CACNA1A -related HM is a complex disorder defined by serious paroxysmal events that affects a broad range of social and clinical domains. We systematically classified symptoms and impacts from HM episodes, creating a disease concept model to help develop surrogate endpoints for future clinical trials, and identified two opportunities to improve patient management, including a written emergency protocol and a transition plan for adolescents approaching adulthood. [ABSTRACT FROM AUTHOR]

Published

2024

3. A patient presenting downbeat positioning nystagmus with 19/11 CAG repeats in the CACNA1A gene: A case report.

Author

Yaguchi, Hiroaki, Abe, Megumi, Fujiwara, Keishi, Kudo, Akihiko, Naganuma, Ryoji, Uwatoko, Hisashi, Shirai, Shinichi, Takahashi‐Iwata, Ikuko, Matsushima, Masaaki, and Yabe, Ichiro

Subjects

*CEREBELLAR ataxia, *CALCIUM channels, *SPINOCEREBELLAR ataxia, *POLYGLUTAMINE, *ATAXIA, *NYSTAGMUS

Abstract

Spinocerebellar ataxia type 6 (SCA6) is a polyglutamine disorder caused by the expansion of CAG repeats in the gene encoding voltage‐gated calcium channel subunit alpha1 A (CACNA1A). The clinical features of SCA6 include slowly progressive cerebellar ataxia and downbeat positioning nystagmus. The clinical significance of 19 CAG repeats is unclear. We report a case with 19/11 CAG repeats in CACNA1A determined by direct sequencing. The case presented with DPN, which is one of the most important symptoms of SCA6, but did not present with ataxia. [ABSTRACT FROM AUTHOR]

Published

2024

4. Progressive Ataxia due to de novo Missense Variants in the CACNA1A Gene.

Author

Zhu, Chen-Hao, Yu, Jin-Yang, Ma, Yin, Dong, Yi, and Wu, Zhi-Ying

Subjects

*MISSENSE mutation, *CALCIUM channels, *CHINESE people, *ATAXIA, *GENETIC variation

Abstract

The CACNA1A gene encodes the alpha-1A subunit of P/Q type voltage-gated calcium channel Cav2.1, which is associated with a broad clinical spectrum and variable symptomatology. While few patients with progressive ataxia caused by CACNA1A missense variants have been reported, here we report three unrelated Chinese patients with progressive ataxia due to de novo missense variants in the CACNA1A gene, including a novel pathogenic variant (c.4999C > G) and a previously reported pathogenic variant (c.4037G > A). Our findings and a systematic literature review show the unique phenotype of progressive ataxia caused by missense variants and enlarge the genetic and clinical spectrum of CACNA1A. This suggests that in addition to routine screening for dynamic mutations, screening for CACNA1A variants is important for clinicians facing patients with progressive ataxia. [ABSTRACT FROM AUTHOR]

Published

2024

5. Natural history of non-polyglutamine CACNA1A disease in Austria.

Author

Indelicato, Elisabetta, Nachbauer, Wolfgang, Amprosi, Matthias S., Maier, Sarah, Unterberger, Iris, Delazer, Margarete, Kaltseis, Katharina, Kiechl, Stefan, Broessner, Gregor, Baumann, Matthias, and Boesch, Sylvia

Subjects

*MONTREAL Cognitive Assessment, *DEVELOPMENTAL delay, *NATURAL history, *SYMPTOM burden, *MOVEMENT disorders

Abstract

Background and objectives: Non-polyglutamine CACNA1A variants underlie an extremely variable phenotypic spectrum encompassing developmental delay, hemiplegic migraine, epilepsy, psychiatric symptoms, episodic and chronic cerebellar signs. We provide our experience with the long-term follow-up of CACNA1A patients and their response to interval therapy. Methods: Patients with genetically confirmed non-polyglutamine CACNA1A disease were prospectively followed at the Center for Rare Movement Disorders of the Medical University of Innsbruck from 2004 to 2024. Results: We recruited 41 subjects with non-polyglutamine CACNA1A disease, of which 38 (93%) familial cases. The mean age at the first examination was 35 ± 22 years. Disease onset was in the childhood/adolescence in 31/41 patients (76%). Developmental delay and episodic symptoms were the first disease manifestation in 9/41 (22%) and 32/41 (78%) patients respectively. Chronic neurological signs encompassed a cerebellar syndrome in 35/41 (85%), which showed almost no progression during the observation period, as well as cognitive deficits in 9/20 (45%, MOCA test score < 26), psychiatric and behavioral symptoms in 11/41(27%). Seizures occurred in two patients concomitant to severe hemiplegic migraine. At the last visit, 27/41 patients (66%) required an interval prophylaxis (including acetazolamide, flunarizine, 4-aminopyridine, topiramate), which was efficacious in reducing the frequency and severity of episodic symptoms in all cases. In one patient in his 70ies with progressively therapy resistant hemiplegic migraine, treatment with the anti-CGRP antibody galcanezumab successfully reduced the frequency of migraine days from 4 to 1/month. Conclusions: Non-polyglutamine CACNA1A disease show an evolving age-dependent presentation. Interval prophylaxis is effective in reducing the burden of episodic symptoms. [ABSTRACT FROM AUTHOR]

Published

2024

6. CACNA1A variant associated with generalized dystonia.

Author

Rinaldi, Domiziana, Tangari, Marta Maria, Ledda, Claudia, Dematteis, Francesca, Rizzone, Mario Giorgio, Lopiano, Leonardo, and Artusi, Carlo Alberto

Subjects

*MIGRAINE aura, *DEEP brain stimulation, *BOTULINUM toxin, *CEREBRAL atrophy, *MISSENSE mutation

Abstract

Introduction: CACNA1A gene variants are correlated with different disorders, including episodic ataxia type 2, spinocerebellar ataxia type 6, and familial hemiplegic migraine type 1. Despite dystonia not being a typical manifestation of CACNA1A variants, there are reports indicating a link between this gene mutation and dystonic features. Methods: We report the case of a patient with a novel missense variant of the CACNA1A gene presenting headache, head and arm tremor, dystonia, episodic painful focal dystonic attacks, and unexplained falls. Results: A 57-year-old woman presented with a history of neck dystonia, head and arm tremor, and headaches since age 15. In 2017, she progressively developed dystonic tremor of the head and arms with an unremarkable brain MRI. In 2018 she experienced worsening of tremor and developed painful dystonic attacks, resistant to treatments including clonazepam, trihexyphenidyl, baclofen, and levodopa/benserazide. Botulinum toxin injections for neck dystonia provided limited benefit. The next-generation sequencing exam revealed a CACNA1A gene missense variant (NM_023035.2:c.1630C > T; p.Arg544Trp). In 2021 we observed a worsening of dystonia, accompanied by weight loss, mood changes, and unexplained falls. Deep brain stimulation was considered but ruled out due to cortical atrophy and mild cognitive deficits revealed by the neuropsychological examination. Discussion: Only a few studies reported dystonia as part of the clinical features in carriers of CACNA1A mutations. This case points out the relevance of a need to expand the literature on voltage-dependent P/Q-type Ca2 + channels' role in dystonia's pathogenesis and stresses the complex phenotype-genotype presentation of CACNA1A mutation. [ABSTRACT FROM AUTHOR]

Published

2024

7. 'Living with' CACNA1A-related hemiplegic migraine, a disease concept model

Author

Donna Schaare, Kendra Allison, Kara Skorge, Pangkong Fox, Laina Lusk, Sara M. Sarasua, Ingo Helbig, and Luigi Boccuto

Subjects

CACNA1A, hemiplegic migraine, disease concept model, impacts, symptoms, caregivers, Neurology. Diseases of the nervous system, RC346-429

Abstract

IntroductionCACNA1A-related Hemiplegic Migraine (HM) is a rare neurological disorder distinguished by paroxysmal episodes of hemiparesis/hemiplegia with and without headache. Clinical features have been widely characterized, yet the impacts of the paroxysmal events on the patient and caregiver have not been thoroughly explored. Disease concept models are formal frameworks used to describe the lived experiences of patients and their families, offering a source for surrogate endpoints for clinical trials.MethodsWe completed 13 semi-structured interviews with caregivers of 12 individuals diagnosed with CACNA1A-related HM. We methodically coded themes, grouping concepts into three domains. We measured the occurrence of concepts throughout all interviews and subgroups stratified by age categories.ResultsOver 11 h of interviews yielded 2,018 references to 27 distinct concepts. Established symptoms such as seizures (87 references; including status epilepticus 27 references), hemiparesis/hemiplegia (24 references), and unconsciousness (17 references) were referenced, as well as previously underreported symptoms such as apneic episodes (32 references), lost ability to eat (13 references), and vascular access challenges (10 references). The symptom impacts were largely medical (294 references), followed by health (101 references), emotional (36 references), daily living (28 references), and social (26 references). Caregiver impacts were the most referenced domain (995 references), with the pivotal effects seen in caregiver requirements (355 references), emotional (245 references), HM treatments (179 references), daily living (148 references), and health support (135 references).DiscussionCACNA1A-related HM is a complex disorder defined by serious paroxysmal events that affects a broad range of social and clinical domains. We systematically classified symptoms and impacts from HM episodes, creating a disease concept model to help develop surrogate endpoints for future clinical trials, and identified two opportunities to improve patient management, including a written emergency protocol and a transition plan for adolescents approaching adulthood.

Published

2024

8. Migraine with prolonged aphasic aura associated with a CACNA1A mutation: A case report and narrative review

Author

Jicha, Crystal J, Alex, Ashley, Herskovitz, Steven, Haut, Sheryl R, and Lipton, Richard

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Genetics, Neurosciences, Pain Research, Brain Disorders, Chronic Pain, Headaches, Rare Diseases, Migraines, Stroke, Aphasia, Clinical Research, 2.1 Biological and endogenous factors, Aetiology, Male, Humans, Migraine Disorders, Migraine with Aura, Mutation, Epilepsy, Paresis, Calcium Channels, aphasic aura, CACNA1A, familial hemiplegic migraine, migraine aura, Neurology & Neurosurgery, Clinical sciences

Abstract

ObjectiveTo demonstrate that a known CACNA1A variant is associated with a phenotype of prolonged aphasic aura without hemiparesis.BackgroundThe usual differential diagnosis of prolonged aphasia without hemiparesis includes vascular disease, seizure, metabolic derangements, and migraine. Genetic mutations in the CACNA1A gene can lead to a myriad of phenotypes, including familial hemiplegic migraine (FHM) type 1, an autosomal dominant disorder characterized by an aura of unilateral, sometimes prolonged weakness. Though aphasia is a common feature of migraine aura, with or without hemiparesis, aphasia without hemiparesis has not been reported with CACNA1A mutations.MethodsWe report the case of a 51-year-old male who presented with a history of recurrent episodes of aphasia without hemiparesis lasting days to weeks. His headache was left sided and was heralded by what his family described as "confusion." On examination, he had global aphasia without other focal findings. Family history revealed several relatives with a history of severe headaches with neurologic deficits including aphasia and/or weakness. Imaging revealed T2 hyperintensities in the left parietal/temporal/occipital regions on MRI scan with corresponding hyperperfusion on SPECT. Genetic testing revealed a missense mutation in the CACNA1A gene.ConclusionsThis case expands the phenotypic spectrum of the CACNA1A mutation and FHM to include prolonged aphasic aura without hemiparesis. Our patient's SPECT imaging demonstrated hyperperfusion in areas correlating with aura symptoms which can occur in prolonged aura.

Published

2023

9. AARS and CACNA1A mutations: diagnostic insights into a case report of uncommon epileptic encephalopathy phenotypes in two siblings.

Author

Romero, Vanessa I., Sáenz, Samantha, Arias-Almeida, Benjamín, DiCapua, Daniela, and Kazuyoshi Hosomichi

Subjects

EPILEPSY, PHENOTYPES, NEUROLOGICAL disorders, BRAIN diseases, PEOPLE with epilepsy, GENETIC variation

Abstract

Epilepsy, characterized by recurrent seizures, impacts 70–80% of patients, leading to cognitive deficits. The intricate relationship between seizure control and cognitive impairment remains complex. Epileptic encephalopathy (EE), an intensified form often rooted in genetic factors, is detectable through next-generation sequencing, aiding in precise diagnoses, family counseling, and potential treatment strategies. We present a case involving two sisters with refractory generalized seizures evolving into dysarthria, dysphagia, ataxia, and cognitive decline. Despite normal physical exams, abnormal electroencephalogram results consistent with epilepsy were noted. Whole Exome Sequencing identified heterozygous variants in the alanyl-tRNA synthetase (AARS) and Calcium Voltage-Gated Channel Subunit Alpha 1 (CACNA1A) genes. The AARS variant (c.C2083T, p.R695*) was maternal, while the CACNA1A variant (c.G7400C, p.R2467P) was paternal. Patients A and B exhibited a unique blend of neurological and psychiatric conditions, distinct from common disorders that begin adolescence, like Juvenile Myoclonic Epilepsy. Whole Exome Sequencing uncovered an AARS gene and CACNA1A gene, linked to various autosomal dominant phenotypes. Presence in both parents, coupled with familial reports of migraines and seizures, provides insight into accelerated symptom progression. This study underscores the importance of genetic testing in decoding complex phenotypes and emphasizes the value of documenting family history for anticipating related symptoms and future health risks. [ABSTRACT FROM AUTHOR]

Published

2024

10. AARS and CACNA1A mutations: diagnostic insights into a case report of uncommon epileptic encephalopathy phenotypes in two siblings

Author

Vanessa I. Romero, Samantha Sáenz, Benjamín Arias-Almeida, Daniela DiCapua, and Kazuyoshi Hosomichi

Subjects

AARS, CACNA1A, case review, epilepsy, progressive cognitive decline, epileptic encephalopathy, Neurology. Diseases of the nervous system, RC346-429

Abstract

Epilepsy, characterized by recurrent seizures, impacts 70–80% of patients, leading to cognitive deficits. The intricate relationship between seizure control and cognitive impairment remains complex. Epileptic encephalopathy (EE), an intensified form often rooted in genetic factors, is detectable through next-generation sequencing, aiding in precise diagnoses, family counseling, and potential treatment strategies. We present a case involving two sisters with refractory generalized seizures evolving into dysarthria, dysphagia, ataxia, and cognitive decline. Despite normal physical exams, abnormal electroencephalogram results consistent with epilepsy were noted. Whole Exome Sequencing identified heterozygous variants in the alanyl-tRNA synthetase (AARS) and Calcium Voltage-Gated Channel Subunit Alpha 1 (CACNA1A) genes. The AARS variant (c.C2083T, p.R695*) was maternal, while the CACNA1A variant (c.G7400C, p.R2467P) was paternal. Patients A and B exhibited a unique blend of neurological and psychiatric conditions, distinct from common disorders that begin adolescence, like Juvenile Myoclonic Epilepsy. Whole Exome Sequencing uncovered an AARS gene and CACNA1A gene, linked to various autosomal dominant phenotypes. Presence in both parents, coupled with familial reports of migraines and seizures, provides insight into accelerated symptom progression. This study underscores the importance of genetic testing in decoding complex phenotypes and emphasizes the value of documenting family history for anticipating related symptoms and future health risks.

Published

2024

11. CACNA1A-Related Channelopathies: Clinical Manifestations and Treatment Options

Author

Indelicato, Elisabetta, Boesch, Sylvia, Michel, Martin C., Editor-in-Chief, Barrett, James E., Editorial Board Member, Centurión, David, Editorial Board Member, Flockerzi, Veit, Editorial Board Member, Geppetti, Pierangelo, Editorial Board Member, Hofmann, Franz B., Editorial Board Member, Meier, Kathryn Elaine, Editorial Board Member, Page, Clive P., Editorial Board Member, Wang, KeWei, Editorial Board Member, and Striessnig, Jörg, editor

Published

2023

12. The Tottering Mouse

Author

Carter, Russell E., Ebner, Timothy J., Gruol, Donna L., editor, Koibuchi, Noriyuki, editor, Manto, Mario, editor, Molinari, Marco, editor, Schmahmann, Jeremy D., editor, and Shen, Ying, editor

Published

2023

13. The Rolling Nagoya Mouse

Author

Plomp, Jaap J., van den Maagdenberg, Arn M. J. M., Tolner, Else A., Gruol, Donna L., editor, Koibuchi, Noriyuki, editor, Manto, Mario, editor, Molinari, Marco, editor, Schmahmann, Jeremy D., editor, and Shen, Ying, editor

Published

2023

14. Genotype–phenotype relations for episodic ataxia genes: MDSGene systematic review.

Author

Olszewska, Diana Angelika, Shetty, Aakash, Rajalingam, Rajasumi, Rodriguez‐Antiguedad, Jon, Hamed, Moath, Huang, Jana, Breza, Marianthi, Rasheed, Ashar, Bahr, Natascha, Madoev, Harutyan, Westenberger, Ana, Trinh, Joanne, Lohmann, Katja, Klein, Christine, Marras, Connie, and Waln, Olga

Subjects

*ATAXIA, *MOVEMENT disorders, *GENETIC testing, *PHENOTYPIC plasticity, *GENETIC disorders

Abstract

Background: Most episodic ataxias (EA) are autosomal dominantly inherited and characterized by recurrent attacks of ataxia and other paroxysmal and non‐paroxysmal features. EA is often caused by pathogenic variants in the CACNA1A, KCNA1, PDHA1, and SLC1A3 genes, listed as paroxysmal movement disorders (PxMD) by the MDS Task Force on the Nomenclature of Genetic Movement Disorders. Little is known about the genotype–phenotype correlation of the different genetic EA forms. Methods: We performed a systematic review of the literature to identify individuals affected by an episodic movement disorder harboring pathogenic variants in one of the four genes. We applied the standardized MDSGene literature search and data extraction protocol to summarize the clinical and genetic features. All data are available via the MDSGene protocol and platform on the MDSGene website (https://www.mdsgene.org/). Results: Information on 717 patients (CACNA1A: 491, KCNA1: 125, PDHA1: 90, and SLC1A3: 11) carrying 287 different pathogenic variants from 229 papers was identified and summarized. We show the profound phenotypic variability and overlap leading to the absence of frank genotype–phenotype correlation aside from a few key 'red flags'. Conclusion: Given this overlap, a broad approach to genetic testing using a panel or whole exome or genome approach is most practical in most circumstances. [ABSTRACT FROM AUTHOR]

Published

2023

15. Characterization of novel CACNA1A splice variants by RNA‐sequencing in patients with episodic or congenital ataxia.

Author

Riant, Florence, Burglen, Lydie, Corpechot, Michaelle, Robert, Julien, Durr, Alexandra, Solé, Guilhem, Petit, Florence, Freihuber, Cécile, De Marco, Olivier, Sarret, Catherine, Castelnovo, Giovanni, Devillard, Françoise, Afenjar, Alexandra, Héron, Bénédicte, and Lasserve, Elisabeth Tournier

Subjects

*ATAXIA, *RNA sequencing, *DEVELOPMENTAL delay, *NEUROLOGICAL disorders, *RNA analysis

Abstract

Loss of function variants in CACNA1A cause a broad spectrum of neurological disorders, including episodic ataxia, congenital or progressive ataxias, epileptic manifestations or developmental delay. Variants located on the AG/GT consensus splice sites are usually considered as responsible of splicing defects, but exonic or intronic variants located outside of the consensus splice site can also lead to abnormal splicing. We investigated the putative consequences on splicing of 11 CACNA1A variants of unknown significance (VUS) identified in patients with episodic ataxia or congenital ataxia. In silico splice predictions were performed and RNA obtained from fibroblasts was analyzed by Sanger sequencing. The presence of abnormal transcripts was confirmed in 10/11 patients, nine of them were considered as deleterious and one remained of unknown significance. Targeted next‐generation RNA sequencing was done in a second step to compare the two methods. This method was successful to obtain the full cDNA sequence of CACNA1A. Despite the presence of several isoforms in the fibroblastic cells, it detected most of the abnormally spliced transcripts. In conclusion, RNA sequencing was efficient to confirm the pathogenicity of nine novel CACNA1A variants. Sanger or Next generation methods can be used depending on the facilities and organization of the laboratories. [ABSTRACT FROM AUTHOR]

Published

2023

16. A novel CACNA1A R2201W variant in a woman with hemiplegic migraine.

Author

Baso, Giacomo, Mele, Francesco, Del Giudice, Elda, Leon, Alberta, and Pantoni, Leonardo

Subjects

*MIGRAINE aura, *MIGRAINE, *LEUKOENCEPHALOPATHIES, *GENETIC variation, *MAGNETIC resonance imaging, *CEREBRAL small vessel diseases

Abstract

Introduction: Familial hemiplegic migraine type 1 (FHM1) is a monogenic rare disease that is characterized by migraine attacks accompanied by unilateral weakness and is caused by mutations in the CACNA1A gene. We report the case of a patient with a clinical history consistent with hemiplegic migraine who underwent genetic testing that revealed a variant in the CACNA1A gene. Case presentation: A 68-year-old woman was evaluated for progressive postural instability and subjective cognitive decline. She had suffered from recurrent migraine episodes accompanied by fully reversible unilateral weakness that had started around the age of thirty and had fully disappeared at the time of evaluation. Magnetic resonance imaging (MRI) showed an extensive leukoencephalopathy, with features suggestive of small vessel disease, significantly progressing over the years. Exome sequencing revealed the heterozygous variant c.6601C>T (p.Arg2201Trp) in the CACNA1A gene. This variant, located in a highly conserved region, causes the substitution of arginine with tryptophan at codon 2202 of exon 47, with a high likelihood of a damaging effect on protein activity and/or structure. Discussion: This is the first report describing the missense mutation c.6601C>T (p.Arg2201Trp) in heterozygosity in the CACNA1A gene in a patient with clinical features of hemiplegic migraine. The presence of a diffuse leukoencephalopathy on MRI is not typical of hemiplegic migraine and may suggest a phenotypic variant related to this mutation or result from the combined effect of the patient's comorbidities. [ABSTRACT FROM AUTHOR]

Published

2023

17. The genotype–phenotype correlations of the CACNA1A-related neurodevelopmental disorders: a small case series and literature reviews.

Author

Kessi, Miriam, Baiyu Chen, Nan Pang, Lifen Yang, Jing Peng, Fang He, and Fei Yin

Subjects

STATUS epilepticus, SEIZURES (Medicine), NEURAL development, AUTISM spectrum disorders, MYOCLONUS, PHENOTYPES

Abstract

Background: Genotype–phenotype correlations of the CACNA1A-related neurodevelopmental disorders such as global developmental delay (GDD)/ intellectual disability (ID), epileptic encephalopathy (EE), and autism spectrum disorder (ASD) are unknown. We aimed to summarize genotype–phenotype correlations and potential treatment for CACNA1A-related neurodevelopmental disorders. Methods: Six children diagnosed with CACNA1A-related neurodevelopmental disorders at Xiangya Hospital, Central South University from April 2018 to July 2021 were enrolled. The PubMed database was systematically searched for all reported patients with CACNA1A-related neurodevelopmental disorders until February 2023. Thereafter, we divided patients into several groups for comparison. Results: Six patients were recruited from our hospital. Three cases presented with epilepsy, five with GDD/ID, five with ataxia, and two with ASD. The variants included p.G701R, p.R279C, p.D1644N, p.Y62C, p.L1422Sfs*8, and p. R1664Q [two gain-of-function (GOF) and four loss-of-function (LOF) variants]. About 187 individuals with GDD/ID harboring 123 variants were found (case series plus data from literature). Of those 123 variants, p.A713T and p.R1664* were recurrent, 37 were LOF, and 7 were GOF. GOF variants were linked with severe-profound GDD/ ID while LOF variants were associated with mild–moderate GDD/ID (p =  0.001). The p.A713T variant correlated with severe-profound GDD/ID (p =  0.003). A total of 130 epileptic patients harboring 83 variants were identified. The epileptic manifestations included status epilepticus (n =  64), provoked seizures (n =  49), focal seizures (n =  37), EE (n =  29), absence seizures (n =  26), and myoclonic seizures (n =  10). About 49 (42.20%) patients had controlled seizures while 67 (57.80%) individuals remained with refractory seizures. Status epilepticus correlated with variants located on S4, S5, and S6 (p =  0.000). Among the 83 epilepsy-related variants, 23 were recurrent, 32 were LOF, and 11 were GOF. Status epilepticus was linked with GOF variants (p =  0.000). LOF variants were associated with absence seizures (p =  0.000). Six patients died at an early age (3  months to ≤5  years). We found 18 children with ASD. Thirteen variants including recurrent ones were identified in those 18 cases. GOF changes were more linked to ASD. Conclusion: The p.A713T variant is linked with severe-profound GDD/ID. More than half of CACNA1A-related epilepsy is refractory. The most common epileptic manifestation is status epilepticus, which correlates with variants located on S4, S5, and S6. [ABSTRACT FROM AUTHOR]

Published

2023

18. The Transcription Factor, α1ACT, Acts Through a MicroRNA Network to Regulate Neurogenesis and Cell Death During Neonatal Cerebellar Development.

Author

Wei, Cenfu, Benzow, Kellie, Koob, Michael D., Gomez, Christopher M., and Du, Xiaofei

Subjects

*CELL death, *TRANSCRIPTION factors, *GENE expression, *NEONATAL death, *NEURAL stem cells

Abstract

MicroRNAs, a class of small RNA regulators, function throughout neurodevelopment, from neural stem cell neurogenesis to neuronal maturation, synaptic formation, and plasticity. α1ACT, a transcription factor (TF), plays a critical role in neonatal cerebellar development by regulating an ensemble of genes. Of these, ChIP-seq analysis matched near 50% genes directly regulated by α1ACT. Yet, more than half the regulated transcripts lacked direct interaction with α1ACT. To investigate whether α1ACT acts through a microRNA network, we studied α1ACT-associated simultaneous miRNA:mRNA transcriptome profiles, using miRNA-seq paired with RNA-seq. Thirty-one differentially expressed miRNAs (DEMs) associated with α1ACT-regulated differentially expressed genes (DEGs) were profiled in α1ACT-overexpressing PC12 cells and were further validated in neonatal transgenic mouse cerebellum overexpressing α1ACT in a context-dependent manner. Here, we also demonstrated that α1ACT facilitates neurogenesis and development of dendritic synapses and is partially a result of the downregulation of the miR-99 cluster, miR-143, miR-23, miR-146, miR-363, and miR-484. On the other hand, the miR-181, miR-125, and miR-708 clusters were upregulated by α1ACT, which inhibit MAPK signaling and cell death pathways by targeting Ask1, Odc1, Atf4, and Nuf2 for decreased expression. MiR-181a-5p was verified as the most abundant DEM in neonatal cerebellum, which was further induced by α1ACT. Overall, under α1ACT modulation, up-/downregulated miRNA clusters with their paired target genes may form a regulatory network controlling the balance between the neuronal proliferation, differentiation, and cell death in the cerebellum to promote neonatal development. Our findings concerning the α1ACT-related miRNA/mRNA expression profiles in neonatal cerebellum may inform future investigations for cerebellar development. [ABSTRACT FROM AUTHOR]

Published

2023

19. A novel CACNA1A mutation in a neonate with severe encephalopathy at birth

Author

Ozdil, Mine, Eroglu, Arzu, and Gerik-Celebi, Hamide Betul

Published

2024

20. Hippocampus-related cognitive disorders develop in the absence of epilepsy and ataxia in the heterozygous Cacna1a mutant mice tottering

Author

Akito Nakao, Katsumi Hayashida, Hiroo Ogura, Yasuo Mori, and Keiji Imoto

Subjects

CACNA1A, tottering, behavior, synaptic plasticity, cognitive impairments, hippocampus, Therapeutics. Pharmacology, RM1-950, Physiology, QP1-981

Abstract

CACNA1A-associated epilepsy and ataxia frequently accompany cognitive impairments as devastating co-morbidities. However, it is unclear whether the cognitive deficits are consequences secondary to the neurological symptoms elicited by CACNA1A mutations. To address this issue, Cacna1a mutant mice tottering (tg), and in particular tg/+ heterozygotes, serve as a suitable model system, given that tg/+ heterozygotes fail to display spontaneous absence epilepsy and ataxia typically observed in tg/tg homozygotes. Here, we examined hippocampus-dependent behaviors and hippocampal learning-related synaptic plasticity in tg mice. In behavioral analyses of tg/+ and tg/tg, acquisition and retention of spatial reference memory were characteristically impaired in the Morris water maze task, while working memory was intact in the eight-arm radial maze and T-maze tasks. tg/+ heterozygotes showed normal motor function in contrast to tg/tg homozygotes. In electrophysiological analyses, Schaffer collateral–CA1 synapses showed a deficit in the maintenance of long-term potentiation in tg/+ and tg/tg mice and an increased paired-pulse facilitation induced by paired pulses with 100 ms in tg/tg mice. Our results indicate that the tg mutation causes a dominant disorder of the hippocampus-related memory and synaptic plasticity, raising the possibility that in CACNA1A-associated human diseases, functionally aberrant CaV2.1 Ca2+ channels actively induce the observed cognitive deficits independently of the neurological symptoms.

Published

2022

21. Prolonged neurologic deficits with brain MRI changes following ECT in an adolescent with a CACNA1a-related disorder; a case report

Author

Joseph Vithayathil, Colbey Freeman, Marin Jacobwitz, Erin Simon Schwartz, and Sonika Agarwal

Subjects

Electroconvulsive therapy (ECT), CACNA1a, Status epilepticus, Cerebral edema, Hemiplegic migraine, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Electroconvulsive therapy is used to treat depression and schizophrenia with infrequent use in pediatric patients. We report a case of an adolescent with autism spectrum disorder and acute catatonia that presented with status epilepticus (SE) and prolonged neurologic deficits with unilateral left cerebral edema on imaging following unilateral electroconvulsive therapy (ECT) on the right side, subsequently found to have a CACNA1a pathogenic variant. This case highlights a potential adverse effect of ECT in patients with CACNA1a related disorders. Case The patient received unilateral ECT to the right side and subsequently had an episode of SE with right-sided hemiplegia for 72 h prior to regaining some function with persistent mild right-hand weakness that persisted for at least 1–2 weeks. A brain MRI 2 days after ECT was unremarkable, but a repeat MRI on day four of admission showed left hemisphere cortical diffusion restriction, increased perfusion and T2 prolongation suggestive of cortical edema. They had whole exome genetic testing sent after discharge that showed a known pathogenic CACNA1a variant (p.I1709T). CACNA1a encodes the P/Q type calcium channels and deleterious variants in this gene result in a channelopathy associated with a spectrum of neurodevelopmental disorders that include autism spectrum disorder, hemiplegic migraine with unilateral cerebral edema, epileptic encephalopathies, or episodic ataxia syndromes. Conclusion A literature review of ECT and neurologic deficits showed that most neurologic deficits resolve within 30 min of ECT. Case reports of prolonged deficits are rare and there are no prior reports of acute MRI changes related to ECT. Thus, the acute deterioration and MRI findings in this patient are likely related to the underlying CACNA1a channelopathy disorder with ECT as a precipitating event. This case report suggests care should be taken when using ECT in patients with pathogenic variants in CACNA1a. Furthermore, it reinforces the utility and importance of expanded genetic testing in patients with neurodevelopmental disorders as findings can provide valuable information that can guide treatment decisions.

Published

2022

22. Familial hemiplegic migraine in pediatric patients: A genetic, clinical, and follow‐up study.

Author

Mangano, Giuseppe Donato, Capizzi, Maria Rita, Mantuano, Elide, Veneziano, Liana, Santangelo, Giuseppe, Quatrosi, Giuseppe, Nardello, Rosaria, and Raieli, Vincenzo

Subjects

*COGNITION disorders, *SCIENTIFIC observation, *NEUROLOGICAL disorders, *GENETIC mutation, *MIGRAINE, *PEDIATRICS, *RETROSPECTIVE studies, *MOLECULAR pathology, *ADENOSINE triphosphatase, *COMPARATIVE studies, *GENOTYPES, *DESCRIPTIVE statistics, *HEMIPLEGIA, *PHENOTYPES, *RARE diseases, *LONGITUDINAL method

Abstract

Objective: The aim of this study was to describe a cohort of pediatric patients with genetically confirmed familial hemiplegic migraine (FHM). The knowledge of genotype–phenotype correlations may suggest prognostic factors associated with severe phenotypes. Background: Hemiplegic migraine is a rare disease and data concerning the pediatric population are even more rare as they are often extrapolated from mixed cohorts. Methods: We selected patients who met International Classification of Headache Disorders, third edition criteria for FHM, who had a molecular diagnosis, and whose first attack occurred under the age of 18 years. Results: We enrolled nine patients (seven males and two females) first referred to our three centers. Three of the nine (33%) patients had calcium voltage‐gated channel subunit alpha1 A (CACNA1A) mutations, five (55%) had ATPase Na+/K+ transporting subunit alpha 2 (ATP1A2) mutations, and one had both genetic mutations. The patients experienced at least one aura feature other than hemiplegia during the first attack. The mean (SD) duration of HM attacks in the sample was 11.3 (17.1) h; 3.8 (6.1) h in the ATP1A2 group, and 24.3 (23.5) h in the CACNA1A group. The mean (SD, range) duration of follow‐up was 7.4 (2.2, 3–10) years. During the first year from the disorder's onset, only four patients had additional attacks. Over the course of follow‐up, the attack frequency overall was 0.4 attacks/year without a difference between the two groups (CACNA1A and ATP1A2). Conclusion: The study data show that most of our patients with early‐onset FHM experienced infrequent and non‐severe attacks, which improved over time. Furthermore, the clinical course revealed neither the appearance of novel neurological disorders or a deterioration of basic neurological or cognitive functioning. [ABSTRACT FROM AUTHOR]

Published

2023

23. Rolling Nagoya Mouse

Author

Tolner, Else A., van den Maagdenberg, Arn M. J. M., Plomp, Jaap J., Koibuchi, Noriyuki, Section editor, Manto, Mario U., editor, Gruol, Donna L., editor, Schmahmann, Jeremy D., editor, Koibuchi, Noriyuki, editor, and Sillitoe, Roy V., editor

Published

2022

24. Channelopathies and Cerebellar Disease

Author

Morino, Hiroyuki, Matsuda, Yukiko, Kawakami, Hideshi, Gruol, Donna L., Section editor, Manto, Mario U., editor, Gruol, Donna L., editor, Schmahmann, Jeremy D., editor, Koibuchi, Noriyuki, editor, and Sillitoe, Roy V., editor

Published

2022

25. The genotype–phenotype correlations of the CACNA1A-related neurodevelopmental disorders: a small case series and literature reviews

Author

Miriam Kessi, Baiyu Chen, Nan Pang, Lifen Yang, Jing Peng, Fang He, and Fei Yin

Subjects

CACNA1A, genotype–phenotype correlations, global developmental delay, intellectual disability, epilepsy, autism spectrum disorder, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

BackgroundGenotype–phenotype correlations of the CACNA1A-related neurodevelopmental disorders such as global developmental delay (GDD)/intellectual disability (ID), epileptic encephalopathy (EE), and autism spectrum disorder (ASD) are unknown. We aimed to summarize genotype–phenotype correlations and potential treatment for CACNA1A-related neurodevelopmental disorders.MethodsSix children diagnosed with CACNA1A-related neurodevelopmental disorders at Xiangya Hospital, Central South University from April 2018 to July 2021 were enrolled. The PubMed database was systematically searched for all reported patients with CACNA1A-related neurodevelopmental disorders until February 2023. Thereafter, we divided patients into several groups for comparison.ResultsSix patients were recruited from our hospital. Three cases presented with epilepsy, five with GDD/ID, five with ataxia, and two with ASD. The variants included p.G701R, p.R279C, p.D1644N, p.Y62C, p.L1422Sfs*8, and p. R1664Q [two gain-of-function (GOF) and four loss-of-function (LOF) variants]. About 187 individuals with GDD/ID harboring 123 variants were found (case series plus data from literature). Of those 123 variants, p.A713T and p.R1664* were recurrent, 37 were LOF, and 7 were GOF. GOF variants were linked with severe-profound GDD/ID while LOF variants were associated with mild–moderate GDD/ID (p = 0.001). The p.A713T variant correlated with severe-profound GDD/ID (p = 0.003). A total of 130 epileptic patients harboring 83 variants were identified. The epileptic manifestations included status epilepticus (n = 64), provoked seizures (n = 49), focal seizures (n = 37), EE (n = 29), absence seizures (n = 26), and myoclonic seizures (n = 10). About 49 (42.20%) patients had controlled seizures while 67 (57.80%) individuals remained with refractory seizures. Status epilepticus correlated with variants located on S4, S5, and S6 (p = 0.000). Among the 83 epilepsy-related variants, 23 were recurrent, 32 were LOF, and 11 were GOF. Status epilepticus was linked with GOF variants (p = 0.000). LOF variants were associated with absence seizures (p = 0.000). Six patients died at an early age (3 months to ≤5 years). We found 18 children with ASD. Thirteen variants including recurrent ones were identified in those 18 cases. GOF changes were more linked to ASD.ConclusionThe p.A713T variant is linked with severe-profound GDD/ID. More than half of CACNA1A-related epilepsy is refractory. The most common epileptic manifestation is status epilepticus, which correlates with variants located on S4, S5, and S6.

Published

2023

26. A neurodevelopmental disorder caused by a dysfunctional CACNA1A allele

Author

Audra A. Kramer, Daniel F. Bennett, Kristin W. Barañano, and Roger A. Bannister

Subjects

CACNA1A, CaV2.1, α1A, P/Q-type, ataxia, Developmental delay, Neurology. Diseases of the nervous system, RC346-429

Abstract

P/Q-type Ca2+ flux into nerve terminals via CaV2.1 channels is essential for neurotransmitter release at neuromuscular junctions and nearly all central synapses. Mutations in CACNA1A, the gene encoding CaV2.1, cause a spectrum of pediatric neurological disorders. We have identified a patient harboring an autosomal-dominant de novo frameshift-causing nucleotide duplication in CACNA1A (c.5018dupG). The duplicated guanine precipitated 43 residues of altered amino acid sequence beginning with a glutamine to serine substitution in CaV2.1 at position 1674 ending with a premature stop codon (CaV2.1 p.Gln1674Serfs*43). The patient presented with episodic downbeat vertical nystagmus, hypotonia, ataxia, developmental delay and febrile seizures. In patch-clamp experiments, no Ba2+ current was observed in tsA-201 cells expressing CaV2.1 p.Gln1674Serfs*43 with β4 and α2δ-1 auxiliary subunits. The ablation of divalent flux in response to depolarization was likely attributable to the inability of CaV2.1 p.Gln1674Serfs*43 to form a complete channel pore. Our results suggest that the pathology resulting from this frameshift-inducing nucleotide duplication is a consequence of an effective haploinsufficiency.

Published

2023

27. Concomitant Calcium Channelopathies Involving CACNA1A and CACNA1F: A Case Report and Review of the Literature.

Author

Schaare, Donna, Sarasua, Sara M., Lusk, Laina, Parthasarathy, Shridhar, Wang, Liangjiang, Helbig, Ingo, and Boccuto, Luigi

Subjects

*CALCIUM channels, *SUMATRIPTAN, *CEREBRAL edema, *CALCIUM, *CENTRAL nervous system, *CELL physiology

Abstract

Calcium channels are an integral component in maintaining cellular function. Alterations may lead to channelopathies, primarily manifested in the central nervous system. This study describes the clinical and genetic features of a unique 12-year-old boy harboring two congenital calcium channelopathies, involving the CACNA1A and CACNA1F genes, and provides an unadulterated view of the natural history of sporadic hemiplegic migraine type 1 (SHM1) due to the patient's inability to tolerate any preventative medication. The patient presents with episodes of vomiting, hemiplegia, cerebral edema, seizure, fever, transient blindness, and encephalopathy. He is nonverbal, nonambulatory, and forced to have a very limited diet due to abnormal immune responses. The SHM1 manifestations apparent in the subject are consistent with the phenotype described in the 48 patients identified as part of a systematic literature review. The ocular symptoms of CACNA1F align with the family history of the subject. The presence of multiple pathogenic variants make it difficult to identify a clear phenotype–genotype correlation in the present case. Moreover, the detailed case description and natural history along with the comprehensive review of the literature contribute to the understanding of this complex disorder and point to the need for comprehensive clinical assessments of SHM1. [ABSTRACT FROM AUTHOR]

Published

2023

28. Focal Dystonic Tremor as a Prominent Feature in a Child with a CACNA1A‐Related Disorder.

Author

Mercati, Marta, Graziola, Federica, Canafoglia, Laura, Caputo, Davide, Danti, Federica Rachele, Reale, Chiara, and Zorzi, Giovanna

Subjects

*MOVEMENT disorders, *CEREBELLUM degeneration, *TREMOR, *NUCLEOTIDE sequencing, *MIGRAINE aura, *WECHSLER Adult Intelligence Scale

Abstract

Next generation sequencing gene panel for movement disorders identified in the proband a de novo heterozygous c.1108delG variant in exon 8 of the I CACNA1A i gene (NM 001127222.2), causing a premature stop codon (p.Val370TrpTer7). Keywords: dystonic tremor; tremor; children; CACNA1A EN dystonic tremor tremor children CACNA1A 1554 1556 3 10/24/23 20231001 NES 231001 Pathogenic variants in the I CACNA1A i gene have been associated to a wide spectrum of neurological disorders including paroxysmal and persistent epileptic or non-epileptic symptoms.[1] Cerebellar phenotype is a relevant clinical features including autosomal-dominant spinocerebellar ataxias, several autosomal recessive ataxias and episodic ataxias.[2] Herein we describe a Caucasian 14-year-old female, fourth child of non-consanguineous healthy parents, born at term via scheduled caesarean section. Dystonia have been recently reported associated to I CACNA1A i by two independent group showing activity-induced dystonia[3] and cervical dystonia[4] with mild ataxia. [Extracted from the article]

Published

2023

29. Seizure response to carbamazepine in a patient with CACNA1A-associated epilepsy: A case report.

Author

Pinna, Francesca, Corda, Davide, Fois, Chiara, Maccabeo, Alessandra, Sechi, Gian Pietro, and Solla, Paolo

Published

2023

30. Paroxysmal Tonic Upward Gaze: A Clinical Clue for CACNA1A‐Related Disorders.

Author

Massuyama, Breno Kazuo, Tonholo Silva, Thiago Yoshinaga, Gambirasio, Bruna Gutierres, Pedroso, José Luiz, and Barsottini, Orlando Graziani Povoas

Subjects

*EPILEPSY, *GAZE, *NUCLEOTIDE sequencing, *MIGRAINE aura, *NEUROLOGICAL disorders, *SINGLE nucleotide polymorphisms

Abstract

CACNA1A, ataxias, DEE42, epilepsy, neurogenetics In contrast, cryptogenic PTU may have only coordination difficulties during its ictal phase.[10] In conclusion, CACNA1A sequencing should also be considered in the settings of early epilepsy and/or developmental delay when chronic cerebellar signs are present. Keywords: CACNA1A; ataxias; DEE42; epilepsy; neurogenetics EN CACNA1A ataxias DEE42 epilepsy neurogenetics 1225 1227 3 08/29/23 20230801 NES 230801 The gene CACNA1A encodes the a1A pore-forming subunit of the neuronal calcium channel P/Q.[1] CACNA1A-related disorders include the allelic episodic neurological disorders, familial hemiplegic migraine type 1 and episodic ataxia type 2, and the spinocerebellar ataxia type 6, which is a late-onset and progressive cerebellar ataxia. [Extracted from the article]

Published

2023

31. Prolonged neurologic deficits with brain MRI changes following ECT in an adolescent with a CACNA1a-related disorder; a case report.

Author

Vithayathil, Joseph, Freeman, Colbey, Jacobwitz, Marin, Schwartz, Erin Simon, and Agarwal, Sonika

Subjects

SPINOCEREBELLAR ataxia, ELECTROCONVULSIVE therapy, MAGNETIC resonance imaging, CEREBRAL edema, AUTISM spectrum disorders, CHILD patients

Abstract

Background: Electroconvulsive therapy is used to treat depression and schizophrenia with infrequent use in pediatric patients. We report a case of an adolescent with autism spectrum disorder and acute catatonia that presented with status epilepticus (SE) and prolonged neurologic deficits with unilateral left cerebral edema on imaging following unilateral electroconvulsive therapy (ECT) on the right side, subsequently found to have a CACNA1a pathogenic variant. This case highlights a potential adverse effect of ECT in patients with CACNA1a related disorders. Case: The patient received unilateral ECT to the right side and subsequently had an episode of SE with right-sided hemiplegia for 72 h prior to regaining some function with persistent mild right-hand weakness that persisted for at least 1–2 weeks. A brain MRI 2 days after ECT was unremarkable, but a repeat MRI on day four of admission showed left hemisphere cortical diffusion restriction, increased perfusion and T2 prolongation suggestive of cortical edema. They had whole exome genetic testing sent after discharge that showed a known pathogenic CACNA1a variant (p.I1709T). CACNA1a encodes the P/Q type calcium channels and deleterious variants in this gene result in a channelopathy associated with a spectrum of neurodevelopmental disorders that include autism spectrum disorder, hemiplegic migraine with unilateral cerebral edema, epileptic encephalopathies, or episodic ataxia syndromes. Conclusion: A literature review of ECT and neurologic deficits showed that most neurologic deficits resolve within 30 min of ECT. Case reports of prolonged deficits are rare and there are no prior reports of acute MRI changes related to ECT. Thus, the acute deterioration and MRI findings in this patient are likely related to the underlying CACNA1a channelopathy disorder with ECT as a precipitating event. This case report suggests care should be taken when using ECT in patients with pathogenic variants in CACNA1a. Furthermore, it reinforces the utility and importance of expanded genetic testing in patients with neurodevelopmental disorders as findings can provide valuable information that can guide treatment decisions. [ABSTRACT FROM AUTHOR]

Published

2022

32. Biallelic CACNA1A variants: Review of literature and report of a child with drug‐resistant epilepsy and developmental delay.

Author

Wong‐Spracklen, Vivien M. Y., Kolesnik, Anna, Eck, Josefine, Sabanathan, Saras, Spasic‐Boskovic, Olivera, Maw, Anna, and Baker, Kate

Abstract

Biallelic variants in CACNA1A have previously been reported in nine individuals (four families) presenting with epilepsy and cognitive impairments of variable severity and age‐of‐onset. Here, we describe a child who presented at 6 months of age with drug‐resistant epilepsy and developmental delay. At 10 years of age, she has profound impairments in motor function and communication. MRI was initially unremarkable, but progressed to severe cerebellar atrophy by age 3 years. Next Generation Sequencing and panel analysis identified a maternally inherited truncating variant c.2042_2043delAG, p.(Gln681ArgfsTer100) and paternally inherited missense variant c.1693G>A, p.(Glu565Lys). In contrast to previously reported biallelic cases, parents carrying these monoallelic variants did not display clear signs of a CACNA1A‐associated syndrome. In conclusion, we provide further evidence that biallelic CACNA1A variants can cause a severe epileptic and developmental encephalopathy with progressive cerebellar atrophy, and highlight complexities of genetic counseling in such situations. [ABSTRACT FROM AUTHOR]

Published

2022

33. Calcium Channel Splice Variants and Their Effects in Brain and Cardiovascular Function

Author

Yeow, Sean Qing Zhang, Loh, Kelvin Wei Zhern, Soong, Tuck Wah, Crusio, Wim E., Series Editor, Dong, Haidong, Series Editor, Radeke, Heinfried H., Series Editor, Rezaei, Nima, Series Editor, Steinlein, Ortrud, Series Editor, Xiao, Junjie, Series Editor, and Zhou, Lei, editor

Published

2021

34. Other Paroxysmal Movement Disorders

Author

Erro, Roberto, Sethi, Kapil D., Bhatia, Kailash P., Sethi, Kapil D., editor, Erro, Roberto, editor, and Bhatia, Kailash P., editor

Published

2021

35. Clinical and molecular spectrum of P/Q type calcium channel Cav2.1 in epileptic patients

Author

Elham Alehabib, Zahra Esmaeilizadeh, Sakineh Ranji-Burachaloo, Abbas Tafakhori, Hossein Darvish, and Abolfazl Movafagh

Subjects

CACNA1A, Epilepsy, Calcium channels, Intellectual disability, Neurodevelopmental disorder, Brain imaging abnormalities, Medicine

Abstract

Abstract Background Epilepsy is a neurological disorder characterized by the potential to induce seizure and accompanied by cognitive, psychological, and social consequences. CACNA1A gene is a voltage-gated P/Q-type Cav2.1 channel that is broadly expressed in the central nervous system, and the pathogenic variants within this gene may be associated with the epileptic phenotype. In the present study, we collected clinical and molecular data related to epileptic patients with CACNA1A pathogenic variants and investigated possible meaningful relationship between age at onset, neurodevelopmental disorders, type of seizures, brain imaging abnormalities, genotype, and protein domains. Results In our retrospective literature studies, from among 890 articles reviewed, a total of 90 individuals were related to epilepsy phenotype. Our findings showed that about 90 percent of patients have shown the first symptoms in childhood and teenage years and different types of neurodevelopmental disorders, such as intellectual disability, developmental arrest, and behavioral disorders, have been common findings for these patients. Further, a wide range of abnormalities have been observed in their brain imaging, and generalized seizures have been the most type of seizures in these patients. However, our data showed no specific genotype–phenotype correlation in epileptic patients with CACNA1A pathogenic alterations. Conclusions Our study focused on epileptic phenotype in patients with CACNA1A pathogenic variants and showed a wide range of clinical and molecular heterogeneity with no specific genotype–phenotype correlation. It seems that incomplete penetrance, de-novo variants, and modifier genes are obstacles in predicting the clinical outcome.

Published

2021

36. Clinical and genetic characterization of CACNA1A‐related disease.

Author

Lipman, Amy R., Fan, Xiao, Shen, Yufeng, and Chung, Wendy K.

Subjects

*MIGRAINE aura, *DEVELOPMENTAL delay, *AUTISM spectrum disorders, *NEUROBEHAVIORAL disorders, *SPINOCEREBELLAR ataxia, *CHILDREN with autism spectrum disorders, *CHILDREN with developmental disabilities

Abstract

Pathogenic variants in the CACNA1A gene have been associated with episodic ataxia type 2, familial hemiplegic migraine, and spinocerebellar ataxia 6. With increasing use of clinical genetic testing, associations have expanded to include developmental delay, epilepsy, paroxysmal dystonia, and neuropsychiatric disorders. We report 47 individuals with 33 unique likely pathogenic or pathogenic CACNA1A variants. A machine learning method, funNCion, was used to predict loss‐of‐function (LoF)/gain‐of‐function (GoF) impact of genetic variants, and a heuristic severity score was designed to analyze genotype/phenotype correlations. Commonly reported phenotypes include developmental delay/intellectual disability (96%), hemiplegic migraines (36%), episodic ataxia type 2 (32%), epilepsy (55%), autism spectrum disorder (23%), and paroxysmal tonic upward gaze (36%). Severity score was significantly higher for predicted GoF variants, variants in the S5/S6 helices, and the recurrent p.Val1392Met variant. Seizures/status epilepticus were correlated with GoF and were more frequent in those with the p.Val1392Met variant. Our findings demonstrate a breadth of disease severity in CACNA1A‐related disease and suggest that the clinical phenotypic heterogeneity likely reflects diverse molecular phenotypes. A better understanding of the natural history of CACNA1A‐related disease and genotype/phenotype correlations will help inform prognosis and prepare for future clinical trials. [ABSTRACT FROM AUTHOR]

Published

2022

37. EA2 and temporal lobe epilepsy associated with a novel variant in CACNA1A.

Author

Lu, Xi and Xie, Xufang

Published

2023

38. Longitudinal MRI brain findings in the R1349Q pathogenic variant of CACNA1A

Author

Chang Y. Ho, MD, Harrison L. Love, MSIV, Deborah K. Sokol, MD, and Laurence E. Walsh, MD

Subjects

CACNA1A, Hemiplegic Migraines, Episodic Ataxia, Medical physics. Medical radiology. Nuclear medicine, R895-920

Abstract

Pathogenic CACNA1A gene variants are associated with a spectrum of disorders including migraine with or without hemiplegia, ataxia, epilepsy, and developmental disability. We present a case of a pathogenic variant (c.4046G>A, p.R1349Q) in the CACNA1A gene associated with a clinical phenotype of global developmental delay, left hemiparesis, epilepsy, and stroke-like episodes. Longitudinal neuroimaging demonstrates hemispheric encephalomalacia with mismatched perfusion and angiographic imaging, in addition to progressive cerebellar atrophy.

Published

2021

39. Coincidental occurance of episodic ataxia and multiple sclerosis: a case report and review of the literature.

Author

Batum, Melike, Kısabay Ak, Ayşın, Çetin, Güldeniz, Çelebi, Hamide Betül Gerik, Çam, Sırrı, and Mavioğlu, Hatice

Subjects

*MULTIPLE sclerosis, *ATAXIA, *LITERATURE reviews, *INNER ear diseases, *SPINOCEREBELLAR ataxia, *CALCIUM channels

Abstract

Episodic ataxia is a clinical condition characterized by episodes of balance and coordination problems that last minutes to hours. It can be inherited or sporadic, and it can be seen sporadically in epilepsy, basilar migraine, multiple sclerosis, vertebrobasilar ischaemia, and labyrinth diseases. In this article, we present a case of a patient who had a coincidental occurrence of episodic ataxia type 2 (EA2) and multiple sclerosis (MS) Results: The patient who had a previously unidentified heterozygous mutation in the calcium voltage-gated channel subunit alpha 1 A gene (CACNA1A). There is no publication in the literature reporting the co-occurrence of MS and EA2. This combination may be coincidental in this patient, or it may be a relationship that has not yet been scientifically revealed. [ABSTRACT FROM AUTHOR]

Published

2022

40. Instrumented gait analysis defines the walking signature of CACNA1A disorders.

Author

Indelicato, Elisabetta, Raccagni, Cecilia, Runer, Sarah, Hannink, Julius, Nachbauer, Wolfgang, Eigentler, Andreas, Amprosi, Matthias, Wenning, Gregor, and Boesch, Sylvia

Subjects

*GAIT in humans, *RANGE of motion of joints, *WALKING speed, *MIGRAINE aura, *WEARABLE technology, *ANKLE injuries

Abstract

Background: Gait disturbances are a frequent symptom in CACNA1A disorders. Even though, data about their severity and progression are lacking and no CACNA1A-specific scale or assessment for gait is available. Methods: We applied a gait assessment protocol in 20 ambulatory patients with genetically confirmed CACNA1A disorders and 39 matched healthy controls. An instrumented gait analysis (IGA) was performed by means of wearable sensors in basal condition and after a treadmill/cycloergometer challenge in selected cases. Results: CACNA1A patients displayed lower gait speed, shorter steps with increased step length variability, a reduced landing acceleration as well as a reduced range of ankle motion compared to controls. Furthermore, gait-width in patients with episodic CACNA1A disorders was narrower as compared to controls. In one patient experiencing mild episodic symptoms after the treadmill challenge, the IGA was able to detect a deterioration over all gait parameters. Conclusions: In CACNA1A patients, the IGA with wearable sensors unravels specific gait signatures which are not detectable at naked eye. These features (narrow-based gait, lower landing acceleration) distinguish these patients from other ataxic disorders and may be target of focused rehabilitative interventions. IGA can potentially be applied to monitor the neurological fluctuations associated with CACNA1A disorders. [ABSTRACT FROM AUTHOR]

Published

2022

41. The complexities of CACNA1A in clinical neurogenetics.

Author

Hommersom, Marina P., van Prooije, Teije H., Pennings, Maartje, Schouten, Meyke I., van Bokhoven, Hans, Kamsteeg, Erik-Jan, and van de Warrenburg, Bart P. C.

Subjects

*MIGRAINE aura, *NEUROGENETICS, *SPINOCEREBELLAR ataxia, *PHENOTYPIC plasticity, *CEREBELLUM degeneration, *MOLECULAR diagnosis, *INTELLECTUAL disabilities

Abstract

Variants in CACNA1A are classically related to episodic ataxia type 2, familial hemiplegic migraine type 1, and spinocerebellar ataxia type 6. Over the years, CACNA1A has been associated with a broader spectrum of phenotypes. Targeted analysis and unbiased sequencing of CACNA1A result not only in clear molecular diagnoses, but also in large numbers of variants of uncertain significance (VUS), or likely pathogenic variants with a phenotype that does not directly match the CACNA1A spectrum. Over the last years, targeted and clinical exome sequencing in our center has identified 41 CACNA1A variants. Ultimately, variants were considered pathogenic or likely pathogenic in 23 cases, with most phenotypes ranging from episodic or progressive ataxia to more complex ataxia syndromes, as well as intellectual disability and epilepsy. In two cases, the causality of the variant was discarded based on non-segregation or an alternative diagnosis. In the remaining 16 cases, the variant was classified as uncertain, due to lack of opportunities for segregation analysis or uncertain association with a non-classic phenotype. Phenotypic variability and the large number of VUS make CACNA1A a challenging gene for neurogenetic diagnostics. Accessible functional read-outs are clearly needed, especially in cases with a non-classic phenotype. [ABSTRACT FROM AUTHOR]

Published

2022

42. Case Report: A Novel CACNA1A Mutation Caused Flunarizine-Responsive Type 2 Episodic Ataxia and Hemiplegic Migraine With Abnormal MRI of Cerebral White Matter.

Author

Yuan, Xiaoqiu, Zheng, Yiming, Gao, Feng, Sun, Wei, Wang, Zhaoxia, and Zhao, Guiping

Subjects

SPINOCEREBELLAR ataxia, WHITE matter (Nerve tissue), NEUROLOGICAL disorders, MAGNETIC resonance imaging, MIGRAINE, ATAXIA

Abstract

Episodic ataxia type 2 (EA2) is one autosomal-dominant neurological disorder characterized by debilitating attacks of ataxia. It is mainly caused by loss-of-function mutations of the CACNA1A gene, which encodes the pore-forming α1A subunit of Cav2.1 (P/Q type voltage-gated calcium channel). Sporadic hemiplegic migraine (SHM) is another rare disease involving CACNA1A variants, which seldom coexists with EA2. Here we report a novel pathogenic mutation in CACNA1A (c.3836dupA, exon 23, p.Y1279X) of a 16-year-old female, who complained about paroxysmal dizziness, headache, and unsteady gait. Her brain MRI revealed a slightly atrophic cerebellum and numerous asymptomatic hyperintense lesions of the cerebral white matter. The diagnosis of EA2 combined with SHM was made. Administration of 5-mg flunarizine once daily at night effectively reduced the attacks and attenuated her symptoms for a month. [ABSTRACT FROM AUTHOR]

Published

2022

43. CACNA1A Mutations Associated With Epilepsies and Their Molecular Sub-Regional Implications.

Author

Li, Xue-Lian, Li, Zong-Jun, Liang, Xiao-Yu, Liu, De-Tian, Jiang, Mi, Gao, Liang-Di, Li, Huan, Tang, Xue-Qing, Shi, Yi-Wu, Li, Bing-Mei, He, Na, Li, Bin, Bian, Wen-Jun, Yi, Yong-Hong, Cheng, Chuan-Fang, and Wang, Jie

Subjects

EPILEPSY, PARTIAL epilepsy, MEDICAL genetics, MEDICAL genomics, GENETIC mutation, PHENOTYPIC plasticity

Abstract

Purpose: Previously, mutations in the voltage-gated calcium channel subunit alpha1 A (CACNA1A) gene have been reported to be associated with paroxysmal disorders, typically as episodic ataxia type 2. To determine the relationship between CACNA1A and epilepsies and the role of molecular sub-regional on the phenotypic heterogeneity. Methods: Trio-based whole-exome sequencing was performed in 318 cases with partial epilepsy and 150 cases with generalized epilepsy. We then reviewed all previously reported CACNA1A mutations and analyzed the genotype-phenotype correlations with molecular sub-regional implications. Results: We identified 12 CACNA1A mutations in ten unrelated cases of epilepsy, including four de novo null mutations (c.2963_2964insG/p.Gly989Argfs*78, c.3089 + 1G > A, c.4755 + 1G > T, and c.6340-1G > A), four de novo missense mutations (c.203G > T/p.Arg68Leu, c.3965G > A/p.Gly1322Glu, c.5032C > T/p.Arg1678Cys, and c.5393C > T/p.Ser1798Leu), and two pairs of compound heterozygous missense mutations (c.4891A > G/p.Ile1631Val& c.5978C > T/p.Pro1993Leu and c.3233C > T/p.Ser1078Leu&c.6061G > A/p.Glu2021Lys). The eight de novo mutations were evaluated as pathogenic or likely pathogenic mutations according to the criteria of American College of Medical Genetics and Genomics (ACMG). The frequencies of the compound heterozygous CACNA1A mutations identified in this cohort were significantly higher than that in the controls of East Asian and all populations (P = 7.30 × 10–4, P = 2.53 × 10–4). All of the ten cases were ultimately seizure-free after antiepileptic treatment, although frequent epileptic seizures were observed in four cases. Further analysis revealed that episodic ataxia type 2 (EA2) had a tendency of higher frequency of null mutations than epilepsies. The missense mutations in severe epileptic phenotypes were more frequently located in the pore region than those in milder epileptic phenotypes (P = 1.67 × 10–4); de novo mutations in the epilepsy with intellectual disability (ID) had a higher percentage than those in the epilepsy without ID (P = 1.92 × 10–3). Conclusion: This study suggested that CACNA1A mutations were potentially associated with pure epilepsy and the spectrum of epileptic phenotypes potentially ranged from the mild form of epilepsies such as absence epilepsy or partial epilepsy, to the severe form of developmental epileptic encephalopathy. The clinical phenotypes variability is potentially associated with the molecular sub-regional of the mutations. [ABSTRACT FROM AUTHOR]

Published

2022

44. CACNA1A Mutations Associated With Epilepsies and Their Molecular Sub-Regional Implications

Author

Xue-Lian Li, Zong-Jun Li, Xiao-Yu Liang, De-Tian Liu, Mi Jiang, Liang-Di Gao, Huan Li, Xue-Qing Tang, Yi-Wu Shi, Bing-Mei Li, Na He, Bin Li, Wen-Jun Bian, Yong-Hong Yi, Chuan-Fang Cheng, and Jie Wang

Subjects

CACNA1A, partial epilepsy, childhood absence epilepsy, genotype-phenotype correlation, molecular sub-regional implication, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

PurposePreviously, mutations in the voltage-gated calcium channel subunit alpha1 A (CACNA1A) gene have been reported to be associated with paroxysmal disorders, typically as episodic ataxia type 2. To determine the relationship between CACNA1A and epilepsies and the role of molecular sub-regional on the phenotypic heterogeneity.MethodsTrio-based whole-exome sequencing was performed in 318 cases with partial epilepsy and 150 cases with generalized epilepsy. We then reviewed all previously reported CACNA1A mutations and analyzed the genotype-phenotype correlations with molecular sub-regional implications.ResultsWe identified 12 CACNA1A mutations in ten unrelated cases of epilepsy, including four de novo null mutations (c.2963_2964insG/p.Gly989Argfs*78, c.3089 + 1G > A, c.4755 + 1G > T, and c.6340-1G > A), four de novo missense mutations (c.203G > T/p.Arg68Leu, c.3965G > A/p.Gly1322Glu, c.5032C > T/p.Arg1678Cys, and c.5393C > T/p.Ser1798Leu), and two pairs of compound heterozygous missense mutations (c.4891A > G/p.Ile1631Val& c.5978C > T/p.Pro1993Leu and c.3233C > T/p.Ser1078Leu&c.6061G > A/p.Glu2021Lys). The eight de novo mutations were evaluated as pathogenic or likely pathogenic mutations according to the criteria of American College of Medical Genetics and Genomics (ACMG). The frequencies of the compound heterozygous CACNA1A mutations identified in this cohort were significantly higher than that in the controls of East Asian and all populations (P = 7.30 × 10–4, P = 2.53 × 10–4). All of the ten cases were ultimately seizure-free after antiepileptic treatment, although frequent epileptic seizures were observed in four cases. Further analysis revealed that episodic ataxia type 2 (EA2) had a tendency of higher frequency of null mutations than epilepsies. The missense mutations in severe epileptic phenotypes were more frequently located in the pore region than those in milder epileptic phenotypes (P = 1.67 × 10–4); de novo mutations in the epilepsy with intellectual disability (ID) had a higher percentage than those in the epilepsy without ID (P = 1.92 × 10–3).ConclusionThis study suggested that CACNA1A mutations were potentially associated with pure epilepsy and the spectrum of epileptic phenotypes potentially ranged from the mild form of epilepsies such as absence epilepsy or partial epilepsy, to the severe form of developmental epileptic encephalopathy. The clinical phenotypes variability is potentially associated with the molecular sub-regional of the mutations.

Published

2022

45. Generation of induced pluripotent stem cell lines carrying monoallelic (UCSFi001-A-60) or biallelic (UCSFi001-A-61; UCSFi001-A-62) frameshift variants in CACNA1A using CRISPR/Cas9

Author

Marina P. Hommersom, Chantal Bijnagte-Schoenmaker, Silvia Albert, Bart P.C. van de Warrenburg, Nael Nadif Kasri, and Hans van Bokhoven

Subjects

CACNA1A, ataxia, neuron, Biology (General), QH301-705.5

Abstract

CACNA1A encodes a P/Q-type voltage-gated calcium channel. Heterozygous loss-of-function variants in this gene have been associated with episodic ataxia type 2. In this study, we used CRISPR/Cas9 to generate isogenic human induced pluripotent stem cell lines with a gene-dosage dependent deficiency of CACNA1A. We obtained one clone with monoallelic (UCSFi001-A-60) and two clones with biallelic (UCSFi001-A-61; UCSFi001-A-62) frameshift variants in CACNA1A. All three lines showed expression of pluripotency markers and a normal karyotype.

Published

2022

46. Case Report: A Novel CACNA1A Mutation Caused Flunarizine-Responsive Type 2 Episodic Ataxia and Hemiplegic Migraine With Abnormal MRI of Cerebral White Matter

Author

Xiaoqiu Yuan, Yiming Zheng, Feng Gao, Wei Sun, Zhaoxia Wang, and Guiping Zhao

Subjects

episodic ataxia type 2, CACNA1A, MRI, flunarizine, case report, hemiplegic migraine, Neurology. Diseases of the nervous system, RC346-429

Abstract

Episodic ataxia type 2 (EA2) is one autosomal-dominant neurological disorder characterized by debilitating attacks of ataxia. It is mainly caused by loss-of-function mutations of the CACNA1A gene, which encodes the pore-forming α1A subunit of Cav2.1 (P/Q type voltage-gated calcium channel). Sporadic hemiplegic migraine (SHM) is another rare disease involving CACNA1A variants, which seldom coexists with EA2. Here we report a novel pathogenic mutation in CACNA1A (c.3836dupA, exon 23, p.Y1279X) of a 16-year-old female, who complained about paroxysmal dizziness, headache, and unsteady gait. Her brain MRI revealed a slightly atrophic cerebellum and numerous asymptomatic hyperintense lesions of the cerebral white matter. The diagnosis of EA2 combined with SHM was made. Administration of 5-mg flunarizine once daily at night effectively reduced the attacks and attenuated her symptoms for a month.

Published

2022

47. CACNA1A haploinsufficiency leads to reduced synaptic function and increased intrinsic excitability.

Author

Hommersom MP, Doorn N, Puvogel S, Lewerissa EI, Mordelt A, Ciptasari U, Kampshoff F, Dillen L, van Beusekom E, Oudakker A, Kogo N, Dolga AM, Frega M, Schubert D, van de Warrenburg BPC, Nadif Kasri N, and van Bokhoven H

Abstract

Haploinsufficiency of the CACNA1A gene, encoding the pore-forming α1 subunit of P/Q-type voltage-gated calcium channels, is associated with a clinically variable phenotype ranging from cerebellar ataxia, to neurodevelopmental syndromes with epilepsy and intellectual disability. To understand the pathological mechanisms of CACNA1A loss-of-function variants, we characterized a human neuronal model for CACNA1A haploinsufficiency, by differentiating isogenic induced pluripotent stem cell lines into glutamatergic neurons, and investigated the effect of CACNA1A haploinsufficiency on mature neuronal networks through a combination of electrophysiology, gene expression analysis, and in silico modeling. We observed an altered network synchronization in CACNA1A+/- networks alongside synaptic deficits, notably marked by an augmented contribution of GluA2-lacking AMPA receptors. Intriguingly, these synaptic perturbations coexisted with increased non-synaptically driven activity, as characterized by inhibition of NMDA and AMPA receptors on micro-electrode arrays. Single-cell electrophysiology and gene expression analysis corroborated this increased intrinsic excitability through reduced potassium channel function and expression. Moreover, we observed partial mitigation of the CACNA1A+/- network phenotype by 4-aminopyridine, a therapeutic intervention for episodic ataxia type 2. Positive modulation of KCa2 channels could reverse the CACNA1A+/- network electrophysiological phenotype. In summary, our study pioneers the characterization of a human induced pluripotent stem cell-derived neuronal model for CACNA1A haploinsufficiency, and has unveiled novel mechanistic insights. Beyond showcasing synaptic deficits, this neuronal model exhibited increased intrinsic excitability mediated by diminished potassium channel function, underscoring its potential as a therapeutic discovery platform with predictive validity., (© The Author(s) 2024. Published by Oxford University Press on behalf of the Guarantors of Brain.)

Published

2024

48. Treatment of CACNA1A Encephalopathy and Cerebral Edema with Magnesium and Dexamethasone.

Author

Turner C, Campbell L, Fung R, Desai S, Oyenubi A, Cayabyab F, and Huntsman RJ

Abstract

Pathogenic CACNA1A mutations can result in paroxysmal attacks of encephalopathy, hemiplegia and cerebral edema. We report two patients with CACNA1A-associated encephalopathy, hemiplegia and contralateral hemispheric cerebral edema treated successfully with intravenous magnesium sulfate and dexamethasone. One patient met the clinical criteria for familial hemiplegic migraine. There is a paucity of guidance in the literature on how to manage these patients. Despite some discrepancies in the treatment protocols in our two cases, they indicate that magnesium and dexamethasone could be part of the treatment algorithm for these patients. Further research to delineate appropriate dosing and duration of therapy is needed.

Published

2024

49. Voltage-gated Calcium Channels as Potential Therapeutic Targets in Migraine.

Author

Chichorro JG, Gambeta E, Baggio DF, and Zamponi GW

Subjects

Humans, Calcitonin Gene-Related Peptide metabolism, Calcitonin Gene-Related Peptide antagonists & inhibitors, Animals, Calcium Channel Blockers pharmacology, Calcium Channel Blockers therapeutic use, Migraine Disorders drug therapy, Migraine Disorders metabolism, Migraine Disorders physiopathology, Calcium Channels metabolism, Calcium Channels drug effects

Abstract

Migraine is a complex and highly incapacitating neurological disorder that affects around 15% of the general population with greater incidence in women, often at the most productive age of life. Migraine physiopathology is still not fully understood, but it involves multiple mediators and events in the trigeminovascular system and the central nervous system. The identification of calcitonin gene-related peptide as a key mediator in migraine physiopathology has led to the development of effective and highly selective antimigraine therapies. However, this treatment is neither accessible nor effective for all migraine sufferers. Thus, a better understanding of migraine mechanisms and the identification of potential targets are still clearly warranted. Voltage-gated calcium channels (VGCCs) are widely distributed in the trigeminovascular system, and there is accumulating evidence of their contribution to the mechanisms associated with headache pain. Several drugs used in migraine abortive or prophylactic treatment target VGCCs, which probably contributes to their analgesic effect. This review aims to summarize the current evidence of VGGC contribution to migraine physiopathology and to discuss how current pharmacological options for migraine treatment interfere with VGGC function. PERSPECTIVE: Calcitonin gene-related peptide (CGRP) represents a major migraine mediator, but few studies have investigated the relationship between CGRP and VGCCs. CGRP release is calcium channel-dependent and VGGCs are key players in familial migraine. Further studies are needed to determine whether VGCCs are suitable molecular targets for treating migraine., (Copyright © 2024 United States Association for the Study of Pain, Inc. Published by Elsevier Inc. All rights reserved.)

Published

2024

50. Clinical and molecular spectrum of P/Q type calcium channel Cav2.1 in epileptic patients.

Author

Alehabib, Elham, Esmaeilizadeh, Zahra, Ranji-Burachaloo, Sakineh, Tafakhori, Abbas, Darvish, Hossein, and Movafagh, Abolfazl

Subjects

PEOPLE with epilepsy, CALCIUM channels, MOLECULAR spectra, CHILDREN with epilepsy, NEUROLOGICAL disorders, GENETIC variation

Abstract

Background: Epilepsy is a neurological disorder characterized by the potential to induce seizure and accompanied by cognitive, psychological, and social consequences. CACNA1A gene is a voltage-gated P/Q-type Cav2.1 channel that is broadly expressed in the central nervous system, and the pathogenic variants within this gene may be associated with the epileptic phenotype. In the present study, we collected clinical and molecular data related to epileptic patients with CACNA1A pathogenic variants and investigated possible meaningful relationship between age at onset, neurodevelopmental disorders, type of seizures, brain imaging abnormalities, genotype, and protein domains.Results: In our retrospective literature studies, from among 890 articles reviewed, a total of 90 individuals were related to epilepsy phenotype. Our findings showed that about 90 percent of patients have shown the first symptoms in childhood and teenage years and different types of neurodevelopmental disorders, such as intellectual disability, developmental arrest, and behavioral disorders, have been common findings for these patients. Further, a wide range of abnormalities have been observed in their brain imaging, and generalized seizures have been the most type of seizures in these patients. However, our data showed no specific genotype-phenotype correlation in epileptic patients with CACNA1A pathogenic alterations.Conclusions: Our study focused on epileptic phenotype in patients with CACNA1A pathogenic variants and showed a wide range of clinical and molecular heterogeneity with no specific genotype-phenotype correlation. It seems that incomplete penetrance, de-novo variants, and modifier genes are obstacles in predicting the clinical outcome. [ABSTRACT FROM AUTHOR]

Published

2021