Your search keyword '"Baykan, Betül"' showing total 14 results

1. Effects of Transcranial Direct Current Stimulation on Clinical Outcomes, Calcitonin Gene-Related Peptide, and Pituitary Adenylate Cyclase-Activating Polypeptide-38 Levels in Menstrual Migraine

Author

Hasırcı Bayır, Buse Rahime, Aksu, Serkan, Gezegen, Haşim, Karaaslan, Zerrin, Yüceer, Hande, Cerrahoğlu Şirin, Tuba, Küçükali, Cem İsmail, Kurt, Adnan, Karamürsel, Sacit, Yılmaz, Vuslat, and Baykan, Betül

Published

2024

2. Long-term prognosis of patients with photosensitive idiopathic generalized epilepsy

Author

Yılmaz Erol, Tülay, Cerrahoğlu Şirin, Tuba, Görkem Şirin, Nermin, Bebek, Nerses, and Baykan, Betül

Published

2024

3. Acute effect of transcranial direct current stimulation on photoparoxysmal response

Author

Yılmaz Erol, Tülay, İlgezdi Kaya, İrem, Ur Özçelik, Emel, Aksu, Serkan, Şirin, Nermin Görkem, Bebek, Nerses, Kurt, Adnan, Karamürsel, Sacit, and Baykan, Betül

Published

2024

4. Clinical and epilepsy characteristics in Wolf-Hirschhorn syndrome (4p-): A review

Author

Paprocka, Justyna, Kaminiów, Konrad, Yetkin, Ozgun, Tekturk, Pınar, Baykan, Betül, Leiz, Steffen, Kluger, Gerhard, and Striano, Pasquale

Published

2024

5. Exploring shared triggers and potential etiopathogenesis between migraine and idiopathic/genetic epilepsy: Insights from a multicenter tertiary-based study

Author

Yapıcı, Zuhal, Midi, İpek, Saygı, Serap, Çelebi, Ulufer, Darol, Elif Sarıca, Ağan, Kadriye, Ayça, Senem, Gazioğlu, Sibel, Okudan, Zeynep Vildan, Şirin, Nermin Görkem, Bebek, Nerses, Dericioğlu, Neşe, Altun, İlknur Güçlü, Yalçın, Ayşe Destina, Sürmeli, Reyhan, Erdinç, Oğuz Osman, Erdal, Abidin, Algın, Demet İlhan, Kutlu, Gülnihal, Bek, Semai, Erdal, Yüksel, Özön, Akçay Övünç, Reyhani, Aylin, Güldiken, Babürhan, Baklan, Barış, Genç, Bülent Oğuz, Altındağ, Ebru Aykutlu, Karahan, Gökçen, Koç, Güray, Mısırlı, Handan, Öztura, İbrahim, Aslan-Kara, Kezban, Çakar, Merve Melodi, Türkmen, Nur, Bulut, Onur, Karadaş, Ömer, Şahin, Özlem Kesim, Ferik, Sevgi, Peköz, Mehmet Taylan, Topaloğlu, Pınar, Özek, Sibel Üstün, Düzgün, Ülkühan, Yayla, Vildan, Gömceli, Yasemin, Acar, Zeynep Ünlüsoy, Türk, Bengi Gül, Yeni, Seher Naz, Atalar, Arife Çimen, Ekizoğlu, Esme, Gök, Duygu Kurt, Baykan, Betül, Özge, Aynur, Ayta, Semih, Erdoğan, Füsun Ferda, Taşdelen, Bahar, and Velioğlu, Sibel K.

Published

2024

6. Diffusion tensor imaging in photosensitive and nonphotosensitive juvenile myoclonic epilepsy

Author

Acar, Dilan, Ozcelik, Emel Ur, Baykan, Betül, Bebek, Nerses, Demiralp, Tamer, and Bayram, Ali

Published

2024

7. Olfactory function assessment of migraine patients by using the Sniffin’ sticks test: A clinical study

Author

Efendioğlu, Merih Karbay, Orhan, Elif Kocasoy, Şen, Cömert, Sönmez, Said, Orhan, Kadir Serkan, and Baykan, Betül

Published

2024

8. Exploring shared triggers and potential etiopathogenesis between migraine and idiopathic/genetic epilepsy: Insights from a multicenter tertiary-based study

Author

Türk, Bengi Gül, primary, Yeni, Seher Naz, additional, Atalar, Arife Çimen, additional, Ekizoğlu, Esme, additional, Gök, Duygu Kurt, additional, Baykan, Betül, additional, Özge, Aynur, additional, Ayta, Semih, additional, Erdoğan, Füsun Ferda, additional, Taşdelen, Bahar, additional, Velioğlu, Sibel K., additional, Yapıcı, Zuhal, additional, Midi, İpek, additional, Saygı, Serap, additional, Çelebi, Ulufer, additional, Darol, Elif Sarıca, additional, Ağan, Kadriye, additional, Ayça, Senem, additional, Gazioğlu, Sibel, additional, Okudan, Zeynep Vildan, additional, Şirin, Nermin Görkem, additional, Bebek, Nerses, additional, Dericioğlu, Neşe, additional, Altun, İlknur Güçlü, additional, Yalçın, Ayşe Destina, additional, Sürmeli, Reyhan, additional, Erdinç, Oğuz Osman, additional, Erdal, Abidin, additional, Algın, Demet İlhan, additional, Kutlu, Gülnihal, additional, Bek, Semai, additional, Erdal, Yüksel, additional, Özön, Akçay Övünç, additional, Reyhani, Aylin, additional, Güldiken, Babürhan, additional, Baklan, Barış, additional, Genç, Bülent Oğuz, additional, Altındağ, Ebru Aykutlu, additional, Karahan, Gökçen, additional, Koç, Güray, additional, Mısırlı, Handan, additional, Öztura, İbrahim, additional, Aslan-Kara, Kezban, additional, Çakar, Merve Melodi, additional, Türkmen, Nur, additional, Bulut, Onur, additional, Karadaş, Ömer, additional, Şahin, Özlem Kesim, additional, Ferik, Sevgi, additional, Peköz, Mehmet Taylan, additional, Topaloğlu, Pınar, additional, Özek, Sibel Üstün, additional, Düzgün, Ülkühan, additional, Yayla, Vildan, additional, Gömceli, Yasemin, additional, and Acar, Zeynep Ünlüsoy, additional

Published

2024

9. Glycine Receptor β-Targeting Autoantibodies Contribute to the Pathology of Autoimmune Diseases.

Author

Wiessler, Anna-Lena, Talucci, Ivan, Piro, Inken, Seefried, Sabine, Hörlin, Verena, Baykan, Betül B., Tüzün, Erdem, Schaefer, Natascha, Maric, Hans M., Sommer, Claudia, and Villmann, Carmen

Published

2024

10. Seeing Clowns with a Ring 20 Chromosome.

Author

Gezegen, Haşim, Kaya, İrem İlgezdi, Kalaycı, Tuğba, Şirin, Nermin Görkem, Karaman, Birsen, Bebek, Nerses, and Baykan, Betül

Subjects

FANTASY (Psychology), ELECTROENCEPHALOGRAPHY, CHROMOSOME abnormalities, STATUS epilepticus, POSITRON emission tomography computed tomography, AMIDES, HALLUCINATIONS, SEIZURES (Medicine), COGNITION disorders, NEURORADIOLOGY, DRUG resistance

Abstract

Ring chromosome 20 syndrome is a rare genetic disorder characterized by non-convulsive status epilepticus (NCSE) attacks, leading to prolonged confusional states of varying intensity. It is often accompanied by electroencephalography (EEG) changes, such as long-lasting slow waves and occasional spikes, primarily over the frontal lobes, as well as focal seizures with visual hallucinations, cognitive impairment, and behavioral problems. Although clinical suspicion, typical EEG abnormalities, and network disorders revealed by functional neuroimaging method aid in diagnosis, karyotyping remains essential. Seizures are typically drug-resistant although some limited success has been reported with certain anti-seizure drugs. In this report, we present the case of a patient with previously frequent drug-resistant NCSE periods characterized by prolonged confusional states and frightening visual hallucinations. Treatment with lacosamide partially decreased the frequency of seizures. In addition, positron emission tomography/computed tomography (PET/CT) imaging revealed hypometabolism in the frontal and parietal regions of the brain. In patients with drug-resistant and early frightening hallucinations, consideration of the ring 20 chromosome anomaly is crucial. PET/CT imaging may demonstrate hypometabolism in the parietal and frontal lobes, potentially associated with the hallucinations and epileptogenesis of the syndrome. Lacosamide may be a viable option for reducing seizures in Ring chromosome 20 syndrome. [ABSTRACT FROM AUTHOR]

Published

2024

11. Epilepsy with generalized tonic–clonic seizures alone: Electroclinical features and prognostic patterns.

Author

Cerulli Irelli, Emanuele, Gesche, Joanna, Schlabitz, Sophie, Fortunato, Francesco, Catania, Cecilia, Morano, Alessandra, Labate, Angelo, Vorderwülbecke, Bernd J., Gambardella, Antonio, Baykan, Betül, Holtkamp, Martin, Di Bonaventura, Carlo, and Beier, Christoph P.

Subjects

EPILEPSY, SEIZURES (Medicine), TERMINATION of treatment, PATIENT experience, PROGNOSIS, PATIENTS' attitudes

Abstract

Objective: Epilepsy with generalized tonic–clonic seizures alone (GTCA) is a common but poorly characterized idiopathic generalized epilepsy (IGE) syndrome. Hence, we investigated electroclinical features, seizure outcome, and antiseizure medication (ASM) withdrawal in a large cohort of GTCA patients. Methods: In this multicenter retrospective study, GTCA patients defined according to the diagnostic criteria of the International League Against Epilepsy (2022) were included. We investigated prognostic patterns, drug resistance at the last visit, and ASM withdrawal, along with their prognostic factors. Results: We included 247 patients with a median (interquartile range [IQR]) age at onset of 17 years (13–22) and a median follow‐up duration of 10 years (IQR = 5–20). Drug resistance at the last visit was observed in 40 (16.3%) patients, whereas the median latency to achieve 2‐year remission was 24 months (IQR = 24–46.5) with a median number of 1 (IQR = 1–2) ASM. During the long‐term follow‐up (i.e., 202 patients followed ≥5‐years after the first ASM trial), 69 (34.3%) patients displayed an early remission pattern and 36 (17.9%) patients displayed a late remission pattern, whereas 16 (8%) and 73 (36.3%) individuals had no‐remission and relapsing–remitting patterns, respectively. Catamenial seizures and morning predominance of generalized tonic–clonic seizures (GTCS) independently predicted drug resistance at the last visit according to multivariable logistic regression. Treatment withdrawal was attempted in 63 (25.5%) patients, with 59 (93.7%) of them having at least a 12‐month follow‐up after ASM discontinuation. At the last visit, 49 (83%) of those patients had experienced GTCS recurrence. A longer duration of seizure freedom was the only factor predicting a higher chance of successful ASM withdrawal according to multivariable Cox regression. Significance: GTCA could be considered a relatively easily manageable IGE syndrome, with a low rate of drug resistance and a high prevalence of early response to treatment. Nevertheless, a considerable proportion of patients experience relapsing patterns of seizure control, highlighting the need for appropriate counseling and lifestyle recommendations. [ABSTRACT FROM AUTHOR]

Published

2024

12. Exome sequencing of 20,979 individuals with epilepsy reveals shared and distinct ultra-rare genetic risk across disorder subtypes.

Author

Chen S, Abou-Khalil BW, Afawi Z, Ali QZ, Amadori E, Anderson A, Anderson J, Andrade DM, Annesi G, Arslan M, Auce P, Bahlo M, Baker MD, Balagura G, Balestrini S, Banks E, Barba C, Barboza K, Bartolomei F, Bass N, Baum LW, Baumgartner TH, Baykan B, Bebek N, Becker F, Bennett CA, Beydoun A, Bianchini C, Bisulli F, Blackwood D, Blatt I, Borggräfe I, Bosselmann C, Braatz V, Brand H, Brockmann K, Buono RJ, Busch RM, Caglayan SH, Canafoglia L, Canavati C, Castellotti B, Cavalleri GL, Cerrato F, Chassoux F, Cherian C, Cherny SS, Cheung CL, Chou IJ, Chung SK, Churchhouse C, Ciullo V, Clark PO, Cole AJ, Cosico M, Cossette P, Cotsapas C, Cusick C, Daly MJ, Davis LK, Jonghe P, Delanty N, Dennig D, Depondt C, Derambure P, Devinsky O, Di Vito L, Dickerson F, Dlugos DJ, Doccini V, Doherty CP, El-Naggar H, Ellis CA, Epstein L, Evans M, Faucon A, Feng YA, Ferguson L, Ferraro TN, Da Silva IF, Ferri L, Feucht M, Fields MC, Fitzgerald M, Fonferko-Shadrach B, Fortunato F, Franceschetti S, French JA, Freri E, Fu JM, Gabriel S, Gagliardi M, Gambardella A, Gauthier L, Giangregorio T, Gili T, Glauser TA, Goldberg E, Goldman A, Goldstein DB, Granata T, Grant R, Greenberg DA, Guerrini R, Gundogdu-Eken A, Gupta N, Haas K, Hakonarson H, Haryanyan G, Häusler M, Hegde M, Heinzen EL, Helbig I, Hengsbach C, Heyne H, Hirose S, Hirsch E, Ho CJ, Hoeper O, Howrigan DP, Hucks D, Hung PC, Iacomino M, Inoue Y, Inuzuka LM, Ishii A, Jehi L, Johnson MR, Johnstone M, Kälviäinen R, Kanaan M, Kara B, Kariuki SM, Kegele J, Kesim Y, Khoueiry-Zgheib N, Khoury J, King C, Klein KM, Kluger G, Knake S, Kok F, Korczyn AD, Korinthenberg R, Koupparis A, Kousiappa I, Krause R, Krenn M, Krestel H, Krey I, Kunz WS, Kurlemann G, Kuzniecky RI, Kwan P, La Vega-Talbott M, Labate A, Lacey A, Lal D, Laššuthová P, Lauxmann S, Lawthom C, Leech SL, Lehesjoki AE, Lemke JR, Lerche H, Lesca G, Leu C, Lewin N, Lewis-Smith D, Li GH, Liao C, Licchetta L, Lin CH, Lin KL, Linnankivi T, Lo W, Lowenstein DH, Lowther C, Lubbers L, Lui CHT, Macedo-Souza LI, Madeleyn R, Madia F, Magri S, Maillard L, Marcuse L, Marques P, Marson AG, Matthews AG, May P, Mayer T, McArdle W, McCarroll SM, McGoldrick P, McGraw CM, McIntosh A, McQuillan A, Meador KJ, Mei D, Michel V, Millichap JJ, Minardi R, Montomoli M, Mostacci B, Muccioli L, Muhle H, Müller-Schlüter K, Najm IM, Nasreddine W, Neaves S, Neubauer BA, Newton CRJC, Noebels JL, Northstone K, Novod S, O'Brien TJ, Owusu-Agyei S, Özkara Ç, Palotie A, Papacostas SS, Parrini E, Pato C, Pato M, Pendziwiat M, Pennell PB, Petrovski S, Pickrell WO, Pinsky R, Pinto D, Pippucci T, Piras F, Piras F, Poduri A, Pondrelli F, Posthuma D, Powell RHW, Privitera M, Rademacher A, Ragona F, Ramirez-Hamouz B, Rau S, Raynes HR, Rees MI, Regan BM, Reif A, Reinthaler E, Rheims S, Ring SM, Riva A, Rojas E, Rosenow F, Ryvlin P, Saarela A, Sadleir LG, Salman B, Salmon A, Salpietro V, Sammarra I, Scala M, Schachter S, Schaller A, Schankin CJ, Scheffer IE, Schneider N, Schubert-Bast S, Schulze-Bonhage A, Scudieri P, Sedláčková L, Shain C, Sham PC, Shiedley BR, Siena SA, Sills GJ, Sisodiya SM, Smoller JW, Solomonson M, Spalletta G, Sparks KR, Sperling MR, Stamberger H, Steinhoff BJ, Stephani U, Štěrbová K, Stewart WC, Stipa C, Striano P, Strzelczyk A, Surges R, Suzuki T, Talarico M, Talkowski ME, Taneja RS, Tanteles GA, Timonen O, Timpson NJ, Tinuper P, Todaro M, Topaloglu P, Tsai MH, Tumiene B, Turkdogan D, Uğur-İşeri S, Utkus A, Vaidiswaran P, Valton L, van Baalen A, Vari MS, Vetro A, Vlčková M, von Brauchitsch S, von Spiczak S, Wagner RG, Watts N, Weber YG, Weckhuysen S, Widdess-Walsh P, Wiebe S, Wolf SM, Wolff M, Wolking S, Wong I, von Wrede R, Wu D, Yamakawa K, Yapıcı Z, Yis U, Yolken R, Yücesan E, Zagaglia S, Zahnert F, Zara F, Zimprich F, Zizovic M, Zsurka G, Neale BM, and Berkovic SF

Abstract

Identifying genetic risk factors for highly heterogeneous disorders like epilepsy remains challenging. Here, we present the largest whole-exome sequencing study of epilepsy to date, with >54,000 human exomes, comprising 20,979 deeply phenotyped patients from multiple genetic ancestry groups with diverse epilepsy subtypes and 33,444 controls, to investigate rare variants that confer disease risk. These analyses implicate seven individual genes, three gene sets, and four copy number variants at exome-wide significance. Genes encoding ion channels show strong association with multiple epilepsy subtypes, including epileptic encephalopathies, generalized and focal epilepsies, while most other gene discoveries are subtype-specific, highlighting distinct genetic contributions to different epilepsies. Combining results from rare single nucleotide/short indel-, copy number-, and common variants, we offer an expanded view of the genetic architecture of epilepsy, with growing evidence of convergence among different genetic risk loci on the same genes. Top candidate genes are enriched for roles in synaptic transmission and neuronal excitability, particularly postnatally and in the neocortex. We also identify shared rare variant risk between epilepsy and other neurodevelopmental disorders. Our data can be accessed via an interactive browser, hopefully facilitating diagnostic efforts and accelerating the development of follow-up studies., Competing Interests: Competing Interests B.M.N is a member of the scientific advisory board at Deep Genomics and Neumora. No other authors have competing interests to declare

Published

2024

13. Predictors of Seizure Recurrence in Women With Idiopathic Generalized Epilepsy Who Switch From Valproate to Another Medication.

Author

Cerulli Irelli E, Cocchi E, Morano A, Gesche J, Caraballo RH, Lattanzi S, Strigaro G, Rosati E, Catania C, Ferlazzo E, Casciato S, Di Gennaro G, Pizzanelli C, Giuliano L, Viola V, Mostacci B, Pignatta P, Fortunato F, Pulitano P, Panzini C, Gambardella A, Atalar AÇ, Labate A, Operto FF, Giallonardo AT, Baykan BB, Beier CP, and Di Bonaventura C

Subjects

Humans, Female, Retrospective Studies, Anticonvulsants therapeutic use, Seizures drug therapy, Levetiracetam therapeutic use, Lamotrigine therapeutic use, Immunoglobulin E therapeutic use, Valproic Acid therapeutic use, Epilepsy, Generalized drug therapy

Abstract

Background and Objectives: To investigate the predictors of seizure recurrence in women of childbearing age with idiopathic generalized epilepsy (IGE) who switched from valproate (VPA) to alternative antiseizure medications (ASMs) and compare the effectiveness of levetiracetam (LEV) and lamotrigine (LTG) as VPA alternatives after switch., Methods: This multicenter retrospective study included women of childbearing age diagnosed with IGE from 16 epilepsy centers. Study outcomes included worsening or recurrence of generalized tonic-clonic seizure (GTCS) at 12 months and 24 months after the switch from VPA to an alternative ASM. The comparative effectiveness of LEV and LTG as alternative ASM following VPA discontinuation was assessed through inverse probability treatment-weighted (IPTW) Cox regression analysis., Results: We included 426 women with IGE, with a median (interquartile range) age at VPA switch of 24 (19-30) years and a median VPA dosage of 750 (500-1,000) mg/d. The most common reason for VPA switch was teratogenicity concern in 249 women (58.6%), and the most common ASM used in place of VPA was LEV in 197 (46.2%) cases, followed by LTG in 140 (32.9%). GTCS worsening/recurrence occurred in 105 (24.6%) and 139 (32.6%) women at 12 and 24 months, respectively. Catamenial worsening of seizures, higher VPA dosage during switch, multiple seizure types, and shorter duration of GTCS freedom before switch were independent predictors of GTCS recurrence or worsening at 12 months according to mixed multivariable logistic regression analysis. After internal-external validation through 16 independent cohorts, the model showed an area under the curve of 0.71 (95% CI 0.64-0.77). In the subgroup of 337 women who switched to LEV or LTG, IPTW Cox regression analysis showed that LEV was associated with a reduced risk of GTCS worsening or recurrence compared with LTG (adjusted hazard ratio 0.59, 95% CI 0.40-0.87, p = 0.008) during the 24-month follow-up., Discussion: Our findings can have practical implications for optimizing counselling and treatment choices in women of childbearing age with IGE and may help clinicians in making informed treatment decisions in this special population of patients., Classification of Evidence: This study provides Class III evidence that for women with IGE switching from VPA, LEV was associated with a reduced risk of GTCS worsening or recurrence compared with LTG.

Published

2024

14. Glycine Receptor β-Targeting Autoantibodies Contribute to the Pathology of Autoimmune Diseases.

Author

Wiessler AL, Talucci I, Piro I, Seefried S, Hörlin V, Baykan BB, Tüzün E, Schaefer N, Maric HM, Sommer C, and Villmann C

Subjects

Humans, Autoantibodies, Glycine, Autoimmune Diseases, Receptors, Glycine immunology, Receptors, Glycine metabolism, Stiff-Person Syndrome immunology

Abstract

Background and Objectives: Stiff-person syndrome (SPS) and progressive encephalomyelitis with rigidity and myoclonus (PERM) are rare neurologic disorders of the CNS. Until now, exclusive GlyRα subunit-binding autoantibodies with subsequent changes in function and surface numbers were reported. GlyR autoantibodies have also been described in patients with focal epilepsy. Autoimmune reactivity against the GlyRβ subunits has not yet been shown. Autoantibodies against GlyRα1 target the large extracellular N-terminal domain. This domain shares a high degree of sequence homology with GlyRβ making it not unlikely that GlyRβ-specific autoantibody (aAb) exist and contribute to the disease pathology., Methods: In this study, we investigated serum samples from 58 patients for aAb specifically detecting GlyRβ. Studies in microarray format, cell-based assays, and primary spinal cord neurons and spinal cord tissue immunohistochemistry were performed to determine specific GlyRβ binding and define aAb binding to distinct protein regions. Preadsorption approaches of aAbs using living cells and the purified extracellular receptor domain were further used. Finally, functional consequences for inhibitory neurotransmission upon GlyRβ aAb binding were resolved by whole-cell patch-clamp recordings., Results: Among 58 samples investigated, cell-based assays, tissue analysis, and preadsorption approaches revealed 2 patients with high specificity for GlyRβ aAb. Quantitative protein cluster analysis demonstrated aAb binding to synaptic GlyRβ colocalized with the scaffold protein gephyrin independent of the presence of GlyRα1. At the functional level, binding of GlyRβ aAb from both patients to its target impair glycine efficacy., Discussion: Our study establishes GlyRβ as novel target of aAb in patients with SPS/PERM. In contrast to exclusively GlyRα1-positive sera, which alter glycine potency, aAbs against GlyRβ impair receptor efficacy for the neurotransmitter glycine. Imaging and functional analyses showed that GlyRβ aAbs antagonize inhibitory neurotransmission by affecting receptor function rather than localization.

Published

2024