Your search keyword '"Sodium Channel Blockers"' showing total 6,497 results

1. A New Type of Pain Pill.

Author

BROADFOOT, MARLA

Subjects

*SODIUM channel blockers, *ZINC-finger proteins, *CHRONIC pain, *SODIUM channels, *REWARD (Psychology)

Abstract

Vertex Pharmaceuticals has developed a new pain pill called VX-548 that shows promise in relieving acute pain without the risk of addiction. Clinical trials have demonstrated that the drug is as effective as Vicodin, a commonly prescribed opioid, in reducing pain levels. This drug is now being considered for FDA approval and could offer a safer alternative for patients who cannot tolerate or are allergic to other pain medications. Other companies are also researching pain drugs that target sodium channels, which are involved in pain signaling, inspired by Vertex's success. However, further research is needed to ensure the safety and effectiveness of these drugs for chronic pain. [Extracted from the article]

Published

2024

2. Mechanism of Human Cold Pain Perception - Involvement of TRPA1, TRPM8, Nav1.7 and Nav1.8

Author

Stefan Heber, Principal Investigator

Published

2024

3. Arbidol, an antiviral drug, identified as a sodium channel blocker with anticonvulsant activity.

Author

Li, Min, Jin, Yuchen, Wu, Jun, Zhao, Miao, Yu, Kexin, and Yu, Haibo

Subjects

*SODIUM channel blockers, *DRUG discovery, *EPILEPTIFORM discharges, *SODIUM channels, *MALE models

Abstract

Background and purpose: Sodium channel blockers (SCBs) have traditionally been utilized as anti‐seizure medications by primarily targeting the inactivation process. In a drug discovery project aiming at finding potential anticonvulsants, we have identified arbidol, originally an antiviral drug, as a potent SCB. In order to evaluate its anticonvulsant potential, we have thoroughly examined its biophysical properties as well as its effects on animal seizure models. Experimental approach: Patch clamp recording was used to investigate the electrophysiological properties of arbidol, as well as the binding and unbinding kinetics of arbidol, carbamazepine and lacosamide. Furthermore, we evaluated the anticonvulsant effects of arbidol using three different seizure models in male mice. Key results: Arbidol effectively suppressed neuronal epileptiform activity by blocking sodium channels. Arbidol demonstrated a distinct mode of action by interacting with both the fast and slow inactivation of Nav1.2 channels compared with carbamazepine and lacosamide. A kinetic study suggested that the binding and unbinding rates might be associated with the specific characteristics of these three drugs. Arbidol targeted the classical binding site of local anaesthetics, effectively inhibited the gain‐of‐function effects of Nav1.2 epileptic mutations and exhibited varying degrees of anticonvulsant effects in the maximal electroshock model and subcutaneous pentylenetetrazol model but had no effect in the pilocarpine‐induced status epilepticus model. Conclusions and implications: Arbidol shows promising potential as an anticonvulsant agent, providing a unique mode of action that sets it apart from existing SCBs. [ABSTRACT FROM AUTHOR]

Published

2024

4. Are SCN2A‐related BFNISs also responsible for seizures in adulthood? A case report opens new scenarios.

Author

Brunetti, Sara, Muda, Alice, Conti, Chiara, Gazzina, Stefano, Accorsi, Patrizia, and Giordano, Lucio

Abstract

Large cohort studies and variant‐specific electrophysiology have enabled the delineation of different SCN2A‐epilepsy phenotypes, phenotype–genotype correlations, prediction of pharmacosensitivity to sodium channel blockers, and long‐term prognostication for clinicians and families. One of the most common clinical presentations of SCN2A pathological variants is benign familial neonatal‐infantile seizures (BFNIS), which are characterized by seizure onset between the first day of life and 23 months of age and typically resolve, either spontaneously or with the aid of sodium channel blockers, within the first 2 years of life. In 2004, Berkovic et al. reported the case of a young boy affected by SCN2A‐related BFNIS whose mother, who carried the same pathological variant, had also presented with BFNIS in infancy. Our case report focuses on the aforementioned woman who, more than 40 years later, presented two additional seizures, therefore opening the possibility of a role for SCN2A‐related seizures in adulthood. [ABSTRACT FROM AUTHOR]

Published

2024

5. Development of new Kir2.1 channel openers from propafenone analogues.

Author

Li, Encan, Boujeddaine, Najla, Houtman, Marien J. C., Maas, Renee G. C., Sluijter, Joost P. G., Ecker, Gerhard F., Stary‐Weinzinger, Anna, Ham, Willem B., and Heyden, Marcel A. G.

Subjects

*ACTION potentials, *SODIUM channel blockers, *DRUG discovery, *WESTERN immunoblotting, *VENTRICULAR arrhythmia, *POTASSIUM channels

Abstract

Background and Purposes Experimental Approach Key Results Conclusion and Implications Reduced inward rectifier potassium channel (Kir2.1) functioning is associated with heart failure and may cause Andersen‐Tawil Syndrome, among others characterized by ventricular arrhythmias. Most heart failure or Andersen–Tawil Syndrome patients are treated with β‐adrenoceptor antagonists (β‐blockers) or sodium channel blockers; however, these do not specifically address the inward rectifier current (IK1) nor aim to improve resting membrane potential stability. Consequently, additional pharmacotherapy for heart failure and Andersen–Tawil Syndrome treatment would be highly desirable. Acute propafenone treatment at low concentrations enhances IK1 current, but it also exerts many off‐target effects. Therefore, discovering and exploring new IK1‐channel openers is necessary.Effects of propafenone and 10 additional propafenone analogues were analysed. Currents were measured by single‐cell patch‐clamp electrophysiology. Kir2.1 protein expression levels were determined by western blot analysis and action potential characteristics were further validated in human‐induced pluripotent stem cells–derived cardiomyocytes (hiPSC‐CMCs). Molecular docking was performed to obtain detailed information on drug‐channel interactions.Analogues GPV0019, GPV0057 and GPV0576 strongly increased the outward component of IK1 while not affecting the Kir2.1 channel expression levels. GPV0057 did not block IKr at concentrations below 0.5 μmol L−1 nor NaV1.5 current below 1 μmol L−1. Moreover, hiPSC‐CMC action potential duration was also not affected by GPV0057 at 0.5 and 1 μmol L−1. Structure analysis indicates a mechanism by which GPV0057 might enhance Kir2.1 channel activation.GPV0057 has a strong efficiency towards increasing IK1, which makes it a good candidate to address IK1 deficiency‐associated diseases. [ABSTRACT FROM AUTHOR]

Published

2024

6. V1848I Mutation in the Voltage-Gated Sodium Channel Confers High-Level Resistance to Indoxacarb and Metaflumizone in Spodoptera exigua.

Author

Liu, Xiangjie, Cao, Minhui, Mei, Wenjuan, Wang, Xingliang, and Wu, Yidong

Subjects

*BEET armyworm, *SODIUM channels, *SODIUM channel blockers, *INSECTICIDE resistance, *SPINOSAD

Abstract

Simple Summary: The role of the V1848I mutation in the voltage-gated sodium channel (VGSC) concerning SCBI resistance and inheritance patterns in Spodoptera exigua was investigated by developing and characterizing a near-isogenic resistant strain called WH-1848I. This mutation confers significant resistance to indoxacarb (146-fold) and metaflumizone (431-fold) in the WH-1848I strain. The SCBI resistance in this strain is autosomal, nonrecessive, and genetically linked to the V1848I mutation. Spodoptera exigua is one of the most serious lepidopteran pests of global importance. With the intensive use of insecticides, S. exigua has evolved resistance to many insecticides, including the sodium channel blocker insecticides (SCBIs) indoxacarb and metaflumizone. In this study, we investigated the role of the V1848I mutation in the voltage-gated sodium channel (VGSC) in SCBI resistance and its inheritance patterns in S. exigua through the development and characterization of a near-isogenic resistant strain. The AQ-23 strain of S. exigua, collected in 2023 from Anqing, Anhui province of China, shows 165-fold resistance to indoxacarb compared with the susceptible WH-S strain. A frequency of 44.6% for the V1848I mutation was detected in the SeVGSC of the AQ-23 strain, while no F1845Y mutation was found. Through repeated backcrossing and marker-assisted selection, the V1848I mutation in the AQ-23 strain was introgressed into the susceptible WH-S strain, creating a near-isogenic strain named WH-1848I. This WH-1848I strain exhibits high levels of resistance to indoxacarb (146-fold) and metaflumizone (431-fold) but remains susceptible to broflanilide and spinosad compared with the WH-S strain. Inheritance analysis revealed that SCBI resistance in the WH-1848I strain is autosomal, nonrecessive, and genetically linked to the V1848I mutation. These findings establish a clear link between the V1848I mutation and SCBI resistance in S. exigua, offering valuable insights for developing molecular detection tools and resistance management strategies. [ABSTRACT FROM AUTHOR]

Published

2024

7. Pharmacological management of prolonged seizures in Dravet syndrome including intravenous phenytoin.

Author

Abi Tayeh, Rana, Dozières‐Puyravel, Blandine, Arnaud, Lionel, Titomanlio, Luigi, Dauger, Stéphane, Höhn, Sophie, Le Guern, Eric, and Auvin, Stéphane

Subjects

*STATUS epilepticus, *SODIUM channel blockers, *DRUG repositioning, *EMERGENCY medical services, *SEIZURES (Medicine)

Abstract

Dravet syndrome (DS) is an infantile onset developmental and epileptic encephalopathy. Sodium channel blockers are known to exacerbate seizures in this syndrome. Due to its high incidence, the management of prolonged seizures is crucial for DS patients. There is still ambiguity regarding the use of intravenous phenytoin for prolonged seizure in DS patients mainly due to the lack of data, raising concern about the safety of it use. We conducted a retrospective study (from January 2009 to January 2020) aiming to assess the management of prolonged seizures in DS with a focus on the use of intravenous phenytoin. Data were collected for patients admitted to our hospital for seizures lasting >5 min. Among 52 identified patients in our database, 23 experienced 59 prolonged seizures managed in our hospital. Only four seizures ceased without rescue medication. Notably, the use of intravenous phenytoin was not associated with discernible adverse effects and was effective in stopping status epilepticus in 71% of cases. This study suggests the safety and efficacy of intravenous phenytoin for prolonged seizure in DS. There is a need for broader investigations of emergency treatments for evidence‐based recommendations for the emergency plan of each patient. [ABSTRACT FROM AUTHOR]

Published

2024

8. Adjunctive cenobamate in people with focal onset seizures: Insights from the Italian Expanded Access Program.

Author

Roberti, Roberta, Assenza, Giovanni, Bisulli, Francesca, Boero, Giovanni, Canafoglia, Laura, Chiesa, Valentina, Di Bonaventura, Carlo, Di Gennaro, Giancarlo, Elia, Maurizio, Ferlazzo, Edoardo, Giordano, Alfonso, La Neve, Angela, Liguori, Claudio, Meletti, Stefano, Operto, Francesca Felicia, Pietrafusa, Nicola, Puligheddu, Monica, Pulitano, Patrizia, Rosati, Eleonora, and Sammarra, Ilaria

Subjects

*SODIUM channel blockers, *SEIZURES (Medicine), *PARTIAL epilepsy, *DRUG interactions, *CLOBAZAM

Abstract

Objective: This study was undertaken to assess the effectiveness/tolerability of adjunctive cenobamate, variations in the load of concomitant antiseizure medications (ASMs) and predictors of clinical response in people with focal epilepsy. Methods: This was a retrospective study at 21 centers participating in the Italian Expanded Access Program. Effectiveness outcomes included retention and responder rates (≥50% and 100% reduction in baseline seizure frequency). Tolerability/safety outcomes included the rate of treatment discontinuation due to adverse events (AEs) and their incidence. Total drug load was quantified as the number of concomitant ASMs and total defined daily dose (DDD). Concomitant ASMs were also classified according to their mechanism of action and pharmacokinetic interactions to perform explorative subgroup analyses. Results: A total of 236 subjects with a median age of 38 (Q1–Q3 = 27–49) years were included. At 12 months, cenobamate retention rate was 78.8% and responders were 57.5%. The seizure freedom rates during the preceding 3 months were 9.8%, 12.2%, 16.3%, and 14.0% at 3, 6, 9, and 12 months. A higher percentage of responders was observed among subjects treated with clobazam, although the difference was not statistically significant. A total of 223 AEs were recorded in 133 of 236 participants, leading to cenobamate discontinuation in 8.5% cases. At 12 months, a reduction of one or two concomitant ASMs occurred in 42.6% and 4.3% of the subjects. The median total DDD of all concomitant ASMs decreased from 3.34 (Q1–Q3 = 2.50–4.47) at baseline to 2.50 (Q1–Q3 = 1.67–3.50) at 12 months (p <.001, median percentage reduction = 22.2%). The highest rates of cotreatment withdrawal and reductions in the DDD were observed for sodium channel blockers and γ‐aminobutyric acidergic modulators (above all for those linked to pharmacokinetic interactions), and perampanel. Significance: Adjunctive cenobamate was associated with a reduction in seizure frequency and in the burden of concomitant ASMs in adults with difficult‐to‐treat focal epilepsy. The type of ASM associated did not influence effectiveness except for a favorable trend with clobazam. [ABSTRACT FROM AUTHOR]

Published

2024

9. Persistent sodium currents in neurons: potential mechanisms and pharmacological blockers.

Author

Müller, Peter, Draguhn, Andreas, and Egorov, Alexei V.

Subjects

*SODIUM channel blockers, *AMYOTROPHIC lateral sclerosis, *CENTRAL nervous system, *CHRONIC pain, *TOPIRAMATE, *RILUZOLE, *AMIODARONE

Abstract

Persistent sodium current (INaP) is an important activity-dependent regulator of neuronal excitability. It is involved in a variety of physiological and pathological processes, including pacemaking, prolongation of sensory potentials, neuronal injury, chronic pain and diseases such as epilepsy and amyotrophic lateral sclerosis. Despite its importance, neither the molecular basis nor the regulation of INaP are sufficiently understood. Of particular significance is a solid knowledge and widely accepted consensus about pharmacological tools for analysing the function of INaP and for developing new therapeutic strategies. However, the literature on INaP is heterogeneous, with varying definitions and methodologies used across studies. To address these issues, we provide a systematic review of the current state of knowledge on INaP, with focus on mechanisms and effects of this current in the central nervous system. We provide an overview of the specificity and efficacy of the most widely used INaP blockers: amiodarone, cannabidiol, carbamazepine, cenobamate, eslicarbazepine, ethosuximide, gabapentin, GS967, lacosamide, lamotrigine, lidocaine, NBI-921352, oxcarbazepine, phenytoine, PRAX-562, propofol, ranolazine, riluzole, rufinamide, topiramate, valproaic acid and zonisamide. We conclude that there is strong variance in the pharmacological effects of these drugs, and in the available information. At present, GS967 and riluzole can be regarded bona fide INaP blockers, while phenytoin and lacosamide are blockers that only act on the slowly inactivating component of sodium currents. [ABSTRACT FROM AUTHOR]

Published

2024

10. Clinical and genetic analysis of 23 Chinese children with epilepsy associated with KCNQ2 gene mutations.

Author

Yu, Xixi, Che, Fengyuan, Zhang, Xin, Yang, Li, Zhu, Liping, Xu, Na, Qiu, Shiyan, and Li, Yufen

Subjects

CHILDREN with epilepsy, SODIUM channel blockers, CHILDHOOD epilepsy, GENETIC testing, CHINESE people, PHENOBARBITAL

Abstract

Objective: To summarize the clinical features and genetic mutation characteristics of Chinese children with KCNQ2‐related epilepsy. Methods: A cohort of children with genetically caused epilepsy was evaluated at Linyi People's Hospital from January 2017 to December 2023. After next‐generation sequencing and pathogenicity analysis, we summarized the medical records and genetic testing data of the children who had KCNQ2 gene mutations. Results: We identified 23 KCNQ2 gene mutations. 73.9% (n = 17) of the mutation sites were located in S5–S6 segments and the C‐terminal region. In addition to the common phenotypes, 2 new phenotypes were identified: infantile convulsion with paroxysmal choreoathetosis (ICCA) and febrile seizure plus (FS+). Of all the cases with abnormal video‐electro‐encephalography, three cases with self‐limited familial infantile epilepsy (SeLNE) exhibited a small number of multifocal discharges. Of the patients who have taken a particular antiepileptic drug, the statistics on the number of patients who have responded to the drug are as follows: oxcarbazepine (8/9, 88.9%), levetiracetam (5/7, 71.4%), phenobarbital (9/16, 56.3%), and topiramate (2/5, 40.0%). However, the efficacy of phenobarbital varied widely in treating SeLNE and KCNQ2‐DEE. At the final follow‐up, 1 case with SeLNE had a transient developmental regression and 7 cases with KCNQ2‐DEE had mild to severe developmental backwardness. Significance: Although clinically rare, we report 10 new KCNQ2 mutations and two new phenotypes: ICCA and FS+. This further expands genetic and phenotypic spectrum of KCNQ2‐related epilepsy. The gene mutation sites are mostly located in S5–S6 segments and the C‐terminal region, and the former is usually associated with KCNQ2‐DEE. Sodium channel blockers (including oxcarbazepine and topiramate) and levetiracetam should be prioritized over phenobarbital for KCNQ2‐DEE. Some cases with KCNQ2‐related epilepsy may have transient developmental regression during periods of frequent seizures. Early treatment and early seizure control may be beneficial for willing outcomes in children with KCNQ2‐DEE. Plain Language Summary: This article reports 23 cases of children with KCNQ2‐related epilepsy, including 10 new mutation sites and 2 new phenotypes. It further expands the genetic and phenotypic spectrum of KCNQ2‐related epilepsy. In addition, the article summarizes the gene mutation characteristics and clinical manifestations of children with KCNQ2‐related epilepsy, with the expectation of providing a certain theoretical basis for the diagnosis and treatment of such patients. [ABSTRACT FROM AUTHOR]

Published

2024

11. Navigating Dravet syndrome in Spain: A cross‐sectional study of diagnosis, management, and care coordination.

Author

Solaz, Sandra, Cardenal‐Muñoz, Elena, Muñoz, Alicia, Giorgi, Simona, Pallardó, Federico V., Romá‐Mateo, Carlos, and Aibar, José Ángel

Subjects

EMERGENCY room visits, DELAYED diagnosis, PATIENT satisfaction, SODIUM channel blockers, MEDICAL care

Abstract

Objectives: Dravet syndrome (DS) is a rare form of refractory epilepsy that begins in the first year of life. Approximately 85% of patients have a mutation in the SCN1A gene, which encodes a voltage‐gated sodium channel. The main objective of the present work was to assess the degree of knowledge of DS among Spanish primary care (PC) professionals, the communication flow between them and the pediatric neurologists (PNs), and the services available and resources offered to patients in Spain when searching for a diagnosis and adequate treatment. Methods: Two anonymized online surveys on DS diagnosis and patient management in PC were conducted with Spanish PC pediatricians (PCPs) and caregivers of DS patients in Spain. Results: Most PCPs are aware of genetic epilepsy but lack full knowledge of DS and patient advocacy groups (PAGs). Access to epilepsy treatments varies among regions, with many referrals to hospitals and pediatric neurologists. Diagnosis is often delayed, with misdiagnoses and frequent emergency room (ER) visits. Treatment involves multiple drugs, and sodium channel blockers are used, which are contraindicated in DS treatment. Improved training, resources, and communication are needed for early diagnosis. Significance: To improve the care and treatment of DS patients in Spain, early diagnosis is required and, possibly, specific efforts aimed at identifying patients in adulthood, generating socio‐sanitary structures that integrate social and health services to provide comprehensive care, taking into account the different features and comorbidities of the disease. Plain Language Summary: Dravet syndrome (DS) is a form of genetic epilepsy that starts within the first year of life. We present a study showing that, while family doctors are aware of genetic epilepsies, many don't have a complete understanding of DS. Unfortunately, getting the right diagnosis can take a long time, leading to unnecessary visits to the emergency room. Patients often need several medications, and sometimes they're given drugs that aren't recommended for DS. The takeaway is that training for doctors, more resources, and improved communication could help creating better healthcare systems and therefore give easier access to the right therapies. [ABSTRACT FROM AUTHOR]

Published

2024

12. CYP2C19 genotype and sodium channel blockers in lacosamide-treated children with epilepsy: two major determinants of trough lacosamide concentration or clinical response.

Author

Li, Yue, Guo, Hong-Li, Wang, Jie, Zhang, Yuan-Yuan, Wang, Wei-Jun, Huang, Jian, Fan, Lin, Hu, Ya-Hui, Lu, Xiao-Peng, and Chen, Feng

Subjects

SODIUM channel blockers, CHILDREN with epilepsy, HOSPITAL care of children, CHILD patients, DRUG monitoring

Abstract

Background: The widespread clinical use of lacosamide (LCM) has revealed significant individual differences in clinical response, with various reported influencing factors. However, it remains unclear how genetic factors related to the disposition and clinical response of LCM, as well as drug–drug interactions (DDIs), exert their influence on pediatric patients with epilepsy. Objectives: To evaluate the impact of genetic variations and DDIs on plasma LCM concentrations and clinical response. Design: Patients with epilepsy treated with LCM from June 2021 to March 2023 in the Children's Hospital of Nanjing Medical University were included in the analysis. Methods: The demographic information and laboratory examination data were obtained from the hospital information system. For the pharmacogenetic study, the left-over blood specimens, collected for routine plasma LCM concentration monitoring, were used to perform genotyping analysis for the selected 26 single nucleotide polymorphisms from 14 genes. The trough concentration/daily dose (C 0/D) ratio and efficacy outcomes were compared. Results: Patients achieved 90.1% and 68.9% responder rates in LCM mono- and add-on therapy, respectively. The genetic variant in the CYP2C19 *2 (rs4244285) was associated with a better responsive treatment outcome (odds ratio: 1.82; 95% confidence interval: 1.05–3.15; p = 0.031). In monotherapy, 36% of patients were CYP2C19 normal metabolizers (NMs), 49% were intermediate metabolizers (IMs), and 15% were poor metabolizers (PMs) carrying CYP2C19 *2 or *3. Of note, the C 0/D ratios of IMs and PMs were 9.1% and 39.6% higher than those of NMs, respectively. Similar results were in the add-on therapy group, and we also observed a substantial decrease in the C 0/D ratio when patients were concomitant with sodium channel blockers (SCBs). Conclusion: This study was the first to confirm that CYP2C19 *2 or *3 variants impact the disposition and treatment response of LCM in children with epilepsy. Moreover, concomitant with SCBs, particularly oxcarbazepine, also decreased plasma LCM concentration. Plain language summary: CYP2C19 genotype and sodium channel blockers in lacosamide-treated children with epilepsy: two major determinants of plasma lacosamide concentration or treatment efficacy This study examined the impact of genetic factors and drug combinations on the effectiveness and plasma concentrations of lacosamide, an antiseizure medication, in patients under 18. Analyzing blood samples from 316 patients at the Children's Hospital of Nanjing Medical University, researchers discovered that genetic variations in the CYP2C19 (i.e. *2 and *3), along with metabolic capacity, and co-medication with sodium channel blockers, all influence plasma lacosamide concentration. Understanding these genetic influences could inform personalized dosing strategies, improving the medication's management for pediatric epilepsy patients. [ABSTRACT FROM AUTHOR]

Published

2024

13. North American Congress of Clinical Toxicology (NACCT) 2024.

Author

Wong, Anselm, McNulty, Richard, Hodgson, Sarah, Gunja, Naren, Graudins, Andis, Wood, Hunter, Cao, Dazhe, Sydlik, Stefanie, Lajeunesse, Brooke, Choi, Jae Hyek, Sachs, Kaysie, Sundermann, Heang, Rodriguez, Dylan, Garcia, Ashley, Maddry, Joseph K., Ng, Patrick C., Paredes, R. Madelaine, Feldman, Ryan, Lyneis, John, and Hawi, Mark

Subjects

*DRUG side effects, *SODIUM channel blockers, *BOTULINUM toxin, *BUPRENORPHINE, *DRUG overdose, *ACETAMINOPHEN, *MEDICAL education, *FENTANYL, *ASPIRIN

Abstract

The given text is a compilation of case reports and studies related to toxicology and poisoning. It covers a range of topics, including medication overdoses, adverse effects of substances, and the management of toxic exposures. The document provides valuable insights into the complexities of toxicology and highlights the importance of prompt and individualized treatment approaches. It can be a useful resource for library patrons conducting research in this field. [Extracted from the article]

Published

2024

14. Preliminary Observations and Domestic Management of The Polyphagous Fall Armyworm, (Spodoptera frugiperda) in Sharqia Governorate, Egypt.

Author

Khedr, M. M. A., Amer, A. E. A., Nada, M. M., and El-Sayed, A. A. A.

Subjects

FALL armyworm, SODIUM channel blockers, POISONS, INSECTICIDE resistance, FIELD research, INSECTICIDES

Abstract

Purpose: In mid-2019, fall armyworm, Spodoptera frugiperda (FAW), a highly destructive and polyphagous pest was first discovered in Egypt. It is now a candidate to be a major economic threat to crop production. This study is the first report of this pest at Sharqia Governorate, northern-east Egypt. The available chemical control that is reviewed and reported which is mostly the first assessment in Egypt regarding the extreme shortage in any local data Research Method: Compare the morphological features and description of the detected insect stages with the ideal published data. Through leaf dip bioassay in second instar larvae; the lethal concentrations (LC values) of various conventional and newer insecticides were detected in FAW. Four different insecticides (indoxacarb, methomyl, chlorpyrifos, and metaflumizone were evaluated against both strains (laboratory and field) of FAW. Findings: Generally, the field strain showed resistance to the tested insecticides as compared to the laboratory one; however, indoxacarb (sodium channel blocker) was recorded as the most toxicant one, recording the lowest LC50 and LC90 values (48.79 and 208.47%) for field strain and (16.47 and 103.78%) for laboratory one, respectively. The field strain’s observed insecticide resistance was attributed to resistance mechanisms including a noteworthy rise in the activities of detoxification enzymes. indoxacarb showed the lowest resistance significant values in the field strain as compared to laboratory one. We can conclude that sodium channel blocker i.e. indoxicarb is a promising choice in IPM strategies of FAW in Egypt. Research Limitations: More field studies are required to examine the tested insecticides on different plant species to confirm their effectiveness under field circumstances and to make conclusive recommendations. Originality / Value: Findings can confirm the presence of the invasive FAW in this specific area, register it for the first time, and provide detailed descriptions, also the candidate insecticides proved to be promising control agents to combat FAW larvae under local efforts and domestic circumstances. [ABSTRACT FROM AUTHOR]

Published

2024

15. Gender-based Differences in the Outcome of Treatment With Aldosterone Antagonists in Patients With Heart Failure (GBDAL-HF)

Published

2024

16. Diagnosis of Brugada Syndrome With a Sodium- Channel-Blocker Test: Who Should Be Tested? Who Should Not?

Author

Viskin, Sami, Chorin, Ehud, Rosso, Raphael, Amin, Ahmad S., and Wilde, Arthur A.

Subjects

*SODIUM channel blockers, *VENTRICULAR fibrillation, *ASYMPTOMATIC patients, *INTRAVENOUS therapy, *CARDIAC arrest

Abstract

Intravenous infusion of sodium-channel blockers (SCB) with either ajmaline, flecainide, procainamide, or pilsicainide to unmask the ECG of Brugada syndrome is the drug challenge most commonly used for diagnostic purposes when investigating cases possibly related to inherited arrhythmia syndromes. For a patient undergoing an SCB challenge, the impact of a positive result goes well beyond its diagnostic implications. It is, therefore, appropriate to question who should undergo a SCB test to diagnose or exclude Brugada syndrome and, perhaps more importantly, who should not. We present a critical review of the benefits and drawbacks of the SCB challenge when performed in cardiac arrest survivors, patients presenting with syncope, family members of probands with confirmed Brugada syndrome, and asymptomatic patients with suspicious ECG. [ABSTRACT FROM AUTHOR]

Published

2024

17. Therapeutic Efficacy of Mexiletine for Long QT Syndrome Type 2: Evidence From Human Induced Pluripotent Stem Cell-Derived Cardiomyocytes, Transgenic Rabbits, and Patients.

Author

Crotti, Lia, Neves, Raquel, Dagradi, Federica, Musu, Giulia, Giannetti, Federica, Bos, J. Martijn, Barbieri, Miriam, Cerea, Paolo, Giovenzana, Fulvio L. F., Torchio, Margherita, Mura, Manuela, Gnecchi, Massimiliano, Conte, Giulio, Auricchio, Angelo, Sala, Luca, Odening, Katja E., Ackerman, Michael J., and Schwartz, Peter J.

Subjects

*INDUCED pluripotent stem cells, *PLURIPOTENT stem cells, *LONG QT syndrome, *ACTION potentials, *SODIUM channel blockers

Abstract

BACKGROUND: Despite major advances in the clinical management of long QT syndrome, some patients are not fully protected by beta-blocker therapy. Mexiletine is a well-known sodium channel blocker, with proven efficacy in patients with sodium channel-mediated long QT syndrome type 3. Our aim was to evaluate the efficacy of mexiletine in long QT syndrome type 2 (LQT2) using cardiomyocytes derived from patient-specific human induced pluripotent stem cells, a transgenic LQT2 rabbit model, and patients with LQT2. METHODS: Heart rate-corrected field potential duration, a surrogate for QTc, was measured in human induced pluripotent stem cells from 2 patients with LQT2 (KCNH2-p.A561V, KCNH2-p.R366X) before and after mexiletine using a multiwell multi-electrode array system. Action potential duration at 90% repolarization (APD90) was evaluated in cardiomyocytes isolated from transgenic LQT2 rabbits (KCNH2-p.G628S) at baseline and after mexiletine application. Mexiletine was given to 96 patients with LQT2. Patients were defined as responders in the presence of a QTc shortening ≥40 ms. Antiarrhythmic efficacy of mexiletine was evaluated by a Poisson regression model. RESULTS: After acute treatment with mexiletine, human induced pluripotent stem cells from both patients with LQT2 showed a significant shortening of heart rate-corrected field potential duration compared with dimethyl sulfoxide control. In cardiomyocytes isolated from LQT2 rabbits, acute mexiletine significantly shortened APD90 by 113 ms, indicating a strong mexiletine-mediated shortening across different LQT2 model systems. Mexiletine was given to 96 patients with LQT2 either chronically (n=60) or after the acute oral drug test (n=36): 65% of the patients taking mexiletine only chronically and 75% of the patients who performed the acute oral test were responders. There was a significant correlation between basal QTc and ΔQTc during the test (r= -0.8; P<0.001). The oral drug test correctly predicted long-term effect in 93% of the patients. Mexiletine reduced the mean yearly event rate from 0.10 (95% CI, 0.07-0.14) to 0.04 (95% CI, 0.02-0.08), with an incidence rate ratio of 0.40 (95% CI, 0.16-0.84), reflecting a 60% reduction in the event rate (P=0.01). CONCLUSIONS: Mexiletine significantly shortens cardiac repolarization in LQT2 human induced pluripotent stem cells, in the LQT2 rabbit model, and in the majority of patients with LQT2. Furthermore, mexiletine showed antiarrhythmic efficacy. Mexiletine should therefore be considered a valid therapeutic option to be added to conventional therapies in higher-risk patients with LQT2. [ABSTRACT FROM AUTHOR]

Published

2024

18. Basal release of 6-cyanodopamine from rat isolated vas deferens and its role on the tissue contractility.

Author

Pozzo, Caroline Fernanda Sanches Dal, Junior, Jose Eduardo Maldonado, Britto-Júnior, José, Badin, João Felipe Agostini, de Souza, Valéria Barbosa, Schenka, André Almeida, Peterson, Larryn W., Fregonesi, Adriano, Antunes, Edson, and De Nucci, Gilberto

Subjects

*VAS deferens, *TYROSINE hydroxylase, *SODIUM channel blockers, *RATS, *HIGH performance liquid chromatography

Abstract

6-Cyanodopamine is a novel catecholamine released from rabbit isolated heart. However, it is not known whether this catecholamine presents any biological activity. Here, it was evaluated whether 6-cyanodopamine (6-CYD) is released from rat vas deferens and its effect on this tissue contractility. Basal release of 6-CYD, 6-nitrodopamine (6-ND), 6-bromodopamine, 6-nitrodopa, and 6-nitroadrenaline from vas deferens were quantified by LC-MS/MS. Electric-field stimulation (EFS) and concentration-response curves to noradrenaline, adrenaline, and dopamine of the rat isolated epididymal vas deferens (RIEVD) were performed in the absence and presence of 6-CYD and /or 6-ND. Expression of tyrosine hydroxylase was assessed by immunohistochemistry. The rat isolated vas deferens released significant amounts of both 6-CYD and 6-ND. The voltage-gated sodium channel blocker tetrodotoxin had no effect on the release of 6-CYD, but it virtually abolished 6-ND release. 6-CYD alone exhibited a negligible RIEVD contractile activity; however, at 10 nM, 6-CYD significantly potentiated the noradrenaline- and EFS-induced RIEVD contractions, whereas at 10 and 100 nM, it also significantly potentiated the adrenaline- and dopamine-induced contractions. The potentiation of noradrenaline- and adrenaline-induced contractions by 6-CYD was unaffected by tetrodotoxin. Co-incubation of 6-CYD (100 pM) with 6-ND (10 pM) caused a significant leftward shift and increased the maximal contractile responses to noradrenaline, even in the presence of tetrodotoxin. Immunohistochemistry revealed the presence of tyrosine hydroxylase in both epithelial cell cytoplasm of the mucosae and nerve fibers of RIEVD. The identification of epithelium-derived 6-CYD and its remarkable synergism with catecholamines indicate that epithelial cells may regulate vas deferens smooth muscle contractility. [ABSTRACT FROM AUTHOR]

Published

2024

19. Global modified Delphi consensus on diagnosis, phenotypes, and treatment of SCN8A‐related epilepsy and/or neurodevelopmental disorders.

Author

Conecker, Gabrielle, Xia, Maya Y., Hecker, JayEtta, Achkar, Christelle, Cukiert, Cristine, Devries, Seth, Donner, Elizabeth, Fitzgerald, Mark P., Gardella, Elena, Hammer, Michael, Hegde, Anaita, Hu, Chunhui, Kato, Mitsuhiro, Luo, Tian, Schreiber, John M., Wang, Yi, Kooistra, Tammy, Oudin, Madeleine, Waldrop, Kayla, and Youngquist, J. Tyler

Subjects

*SODIUM channel blockers, *MAGNETIC resonance imaging, *DELPHI method, *LITERATURE reviews, *DEVELOPMENTAL delay, *EPILEPSY

Abstract

Objective: We aimed to develop consensus for diagnosis/management of SCN8A‐related disorders. Utilizing a modified Delphi process, a global cohort of experienced clinicians and caregivers provided input on diagnosis, phenotypes, treatment, and management of SCN8A‐related disorders. Methods: A Core Panel (13 clinicians, one researcher, six caregivers), divided into three subgroups (diagnosis/phenotypes, treatment, comorbidities/prognosis), performed a literature review and developed questions for the modified Delphi process. Twenty‐eight expert clinicians, one researcher, and 13 caregivers from 16 countries participated in the subsequent three survey rounds. We defined consensus as follows: strong consensus, ≥80% fully agree; moderate consensus, ≥80% fully/partially agree, <10% disagree; and modest consensus, 67%–79% fully/partially agree, <10% disagree. Results: Early diagnosis is important for long‐term clinical outcomes in SCN8A‐related disorders. There are five phenotypes: three with early seizure onset (severe developmental and epileptic encephalopathy [DEE], mild/moderate DEE, self‐limited (familial) infantile epilepsy [SeL(F)IE]) and two with later/no seizure onset (neurodevelopmental delay with generalized epilepsy [NDDwGE], NDD without epilepsy [NDDwoE]). Caregivers represented six patients with severe DEE, five mild/moderate DEE, one NDDwGE, and one NDDwoE. Phenotypes vary by age at seizures/developmental delay onset, seizure type, electroencephalographic/magnetic resonance imaging findings, and first‐line treatment. Gain of function (GOF) versus loss of function (LOF) is valuable for informing treatment. Sodium channel blockers are optimal first‐line treatment for GOF, severe DEE, mild/moderate DEE, and SeL(F)IE; levetiracetam is relatively contraindicated in GOF patients. First‐line treatment for NDDwGE is valproate, ethosuximide, or lamotrigine; sodium channel blockers are relatively contraindicated in LOF patients. Significance: This is the first‐ever global consensus for the diagnosis and treatment of SCN8A‐related disorders. This consensus will reduce knowledge gaps in disease recognition and inform preferred treatment across this heterogeneous disorder. Consensus of this type allows more clinicians to provide evidence‐based care and empowers SCN8A families to advocate for their children. [ABSTRACT FROM AUTHOR]

Published

2024

20. Effect of Obesity on the Use of Antiarrhythmics in Adults With Atrial Fibrillation: A Narrative Review.

Author

Shaikh, Fahad, Wynne, Rochelle, Castelino, Ronald L., Davidson, Patricia M., Inglis, Sally C., and Ferguson, Caleb

Subjects

ATRIAL fibrillation, SODIUM channel blockers, DRUG lipophilicity, OBESITY, BODY mass index, ARRHYTHMIA

Abstract

Background: Atrial fibrillation (AF) and obesity coexist in approximately 37.6 million and 650 million people globally, respectively. The anatomical and physiological changes in individuals with obesity may influence the pharmacokinetic properties of drugs. Aim: This review aimed to describe the evidence of the effect of obesity on the pharmacokinetics of antiarrhythmics in people with AF. Methods: Three databases were searched from inception to June 2023. Original studies that addressed the use of antiarrhythmics in adults with AF and concomitant obesity were included. Results: A total of 4549 de‐duplicated articles were screened, and 114 articles underwent full‐text review. Ten studies were included in this narrative synthesis: seven cohort studies, two pharmacokinetic studies, and a single case report. Samples ranged from 1 to 371 participants, predominately males (41%–85%), aged 59–75 years, with a body mass index (BMI) of 23–66 kg/m2. The two most frequently investigated antiarrhythmics were amiodarone and dofetilide. Other drugs investigated included diltiazem, flecainide, disopyramide, propafenone, dronedarone, sotalol, vernakalant, and ibutilide. Findings indicate that obesity may affect the pharmacokinetics of amiodarone and sodium channel blockers (e.g., flecainide, disopyramide, and propafenone). Factors such as drug lipophilicity may also influence the pharmacokinetics of the drug and the need for dose modification. Discussion: Antiarrhythmics are not uniformly affected by obesity. This observation is based on heterogeneous studies of participants with an average BMI and poorly controlled confounding factors such as multimorbidity, concomitant medications, varying routes of administration, and assessment of obesity. Controlled trials with stratification at the time of recruitment for obesity are necessary to determine the significance of these findings. [ABSTRACT FROM AUTHOR]

Published

2024

21. Treatment simplification to optimize cenobamate effectiveness and tolerability: A real‐world retrospective study in Spain.

Author

Rodríguez‐Uranga, Juan Jesús, Sánchez‐Caro, Juan María, and Hariramani Ramchandani, Roshan

Subjects

DRUG side effects, SODIUM channel blockers, PARTIAL epilepsy, PEOPLE with epilepsy, INDUSTRIAL efficiency

Abstract

Objective: This study aimed to explore the impact of co‐antiseizure medication (co‐ASM) optimization on the effectiveness and tolerability of adjunctive cenobamate (CNB) in patients with drug‐resistant epilepsy in a real‐world setting. Methods: This unicentric, retrospective, observational study included adults with focal‐onset seizures who had received ≥2 previous ASMs. The main effectiveness endpoints included responder rates and seizure frequency reduction at 3, 6, and 12‐month visits. The number of co‐ASMs and defined daily dose (DDD) were analyzed at every visit. Safety endpoints included adverse drug reactions (ADRs). Results: Thirty‐four patients with a median epilepsy duration of 22 years and a median of 15.5 seizures/month were analyzed. The median number of prior ASMs was 12, and the mean number of co‐ASMs was 2.9 (SD 1). There was a reduction in seizure frequency/month from baseline to the last visit (p < 0.0001). Between baseline and the end of the study, the mean number of co‐ASMs in the per‐protocol (PP) population was reduced from 2.9 to 1.6 (p < 0.0001), and DDD was reduced from 3.6 to 1.4 (p < 0.0001). Sodium channel blockers (carbamazepine and lacosamide) and GABAergic drugs (clobazam) were the agents with the most significant reductions in DDD after 12 months. The percentage of patients in the PP population with ≥3 co‐ASMs was reduced from 61.8% at baseline to 14.3% at 12 months; 1 patient was receiving CNB as monotherapy at the last visit. At the last visit, 85.7% of the PP population were ≥50% responders, and 33.3% were seizure‐free. The percentage of patients with ADRs in the PP population was 71.9% at 3 months and 52.3% at 12 months. Significance: Following rational polytherapy, optimization of co‐ASM management during CNB treatment allowed high seizure freedom rates despite meaningful reductions in co‐medication, while also achieving both good tolerability and patient satisfaction scores in a highly drug‐resistant population. Plain Language Summary: Many patients with epilepsy still have seizures, even after being treated with several different epilepsy drugs. In this study of 34 patients from a Spanish clinic, we show that the epilepsy drug cenobamate can reduce the number of seizures in these patients, even after many other epilepsy drugs have failed. We also show that patients treated with cenobamate can reduce the dose or even stop taking certain other epilepsy drugs. This allows them to simplify their treatment and reduce adverse effects while still keeping control of their epilepsy. [ABSTRACT FROM AUTHOR]

Published

2024

22. Prostaglandin E2 depolarises sensory axons in vitro in an ANO1 and Nav1.8 dependent manner.

Author

Kimourtzis, Georgios, Rangwani, Natasha, Jenkins, Bethan J., Jani, Siddharth, McNaughton, Peter A., and Raouf, Ramin

Subjects

*DORSAL root ganglia, *ACTION potentials, *CHLORIDE channels, *SODIUM channel blockers, *AXONS, *SODIUM channels

Abstract

Prostaglandin E2 (PGE2) is a major contributor to inflammatory pain hyperalgesia, however, the extent to which it modulates the activity of nociceptive axons is incompletely understood. We developed and characterized a microfluidic cell culture model to investigate sensitisation of the axons of dorsal root ganglia neurons. We show that application of PGE2 to fluidically isolated axons leads to sensitisation of their responses to depolarising stimuli. Interestingly the application of PGE2 to the DRG axons elicited a direct and persistent spiking activity propagated to the soma. Both the persistent activity and the membrane depolarisation in the axons are abolished by the EP4 receptor inhibitor and a blocker of cAMP synthesis. Further investigated into the mechanisms of the spiking activity showed that the PGE2 evoked depolarisation was inhibited by Nav1.8 sodium channel blockers but was refractory to the application of TTX or zatebradine. Interestingly, the depolarisation of axons was blocked by blocking ANO1 channels with T16Ainh-A01. We further show that PGE2-elicited axonal responses are altered by the changes in chloride gradient within the axons following treatment with bumetanide a Na-K-2Cl cotransporter NKCC1 inhibitor, but not by VU01240551 an inhibitor of potassium-chloride transporter KCC2. Our data demonstrate a novel role for PGE2/EP4/cAMP pathway which culminates in a sustained depolarisation of sensory axons mediated by a chloride current through ANO1 channels. Therefore, using a microfluidic culture model, we provide evidence for a potential dual function of PGE2 in inflammatory pain: it sensitises depolarisation-evoked responses in nociceptive axons and directly triggers action potentials by activating ANO1 and Nav1.8 channels. [ABSTRACT FROM AUTHOR]

Published

2024

23. Chronic Mexiletine Administration Increases Sodium Current in Non-Diseased Human Induced Pluripotent Stem Cell-Derived Cardiomyocytes.

Author

Nasilli, Giovanna, Verkerk, Arie O., O'Reilly, Molly, Yiangou, Loukia, Davis, Richard P., Casini, Simona, and Remme, Carol Ann

Subjects

MEXILETINE, ACTION potentials, SODIUM channels, SODIUM channel blockers, SODIUM

Abstract

A sodium current (INa) reduction occurs in the setting of many acquired and inherited conditions and is associated with cardiac conduction slowing and increased arrhythmia risks. The sodium channel blocker mexiletine has been shown to restore the trafficking of mutant sodium channels to the membrane. However, these studies were mostly performed in heterologous expression systems using high mexiletine concentrations. Moreover, the chronic effects on INa in a non-diseased cardiomyocyte environment remain unknown. In this paper, we investigated the chronic and acute effects of a therapeutic dose of mexiletine on INa and the action potential (AP) characteristics in human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs) of a healthy individual. Control hiPSC-CMs were incubated for 48 h with 10 µM mexiletine or vehicle. Following the wash-out of mexiletine, patch clamp analysis and immunocytochemistry experiments were performed. The incubation of hiPSC-CMs for 48 h with mexiletine (followed by wash-out) induced a significant increase in peak INa of ~75%, without any significant change in the voltage dependence of (in)activation. This was accompanied by a significant increase in AP upstroke velocity, without changes in other AP parameters. The immunocytochemistry experiments showed a significant increase in membrane Nav1.5 fluorescence following a 48 h incubation with mexiletine. The acute re-exposure of hiPSC-CMs to 10 µM mexiletine resulted in a small but significant increase in AP duration, without changes in AP upstroke velocity, peak INa density, or the INa voltage dependence of (in)activation. Importantly, the increase in the peak INa density and resulting AP upstroke velocity induced by chronic mexiletine incubation was not counteracted by the acute re-administration of the drug. In conclusion, the chronic administration of a clinically relevant concentration of mexiletine increases INa density in non-diseased hiPSC-CMs, likely by enhancing the membrane trafficking of sodium channels. Our findings identify mexiletine as a potential therapeutic strategy to enhance and/or restore INa and cardiac conduction. [ABSTRACT FROM AUTHOR]

Published

2024

24. Spanish consensus on the management of concomitant antiseizure medications when using cenobamate in adults with drug‐resistant focal seizures.

Author

Carreño, Mar, Gil‐Nagel, Antonio, Serratosa, José M., Toledo, Manuel, Rodriguez‐Uranga, Juan Jesus, and Villanueva, Vicente

Subjects

PHENOBARBITAL, SEIZURES (Medicine), SODIUM channel blockers, ADULTS, DELPHI method, PEOPLE with epilepsy

Abstract

Objective: Cenobamate is an antiseizure medication (ASM) associated with high rates of seizure freedom and acceptable tolerability in patients with focal seizures. To achieve the optimal cenobamate dose for maximal potential effectiveness while avoiding or minimizing drug‐related adverse events (AEs), the administration of cenobamate with other ASMs must be managed through concomitant ASM load reduction. A panel of Spanish epilepsy experts aimed to provide a Spanish consensus on how to adjust the dose of concomitant ASMs in patients with drug‐resistant epilepsy (DRE) in order to improve the effectiveness and tolerability of adjunctive cenobamate. Methods: A three‐stage modified Delphi consensus process was undertaken, including six Spanish epileptologists with extensive experience using cenobamate. Based on current literature and their own expert opinion, the expert panel reached a consensus on when and how to adjust the dosage of concomitant ASMs during cenobamate titration. Results: The expert panel agreed that tailored titration and close follow‐up are required to achieve the best efficacy and tolerability when initiating cenobamate in patients receiving concomitant ASMs. When concomitant clobazam, phenytoin, phenobarbital, and sodium channel blockers are taken at high dosages, or when the patient is receiving two or more sodium channel blockers, dosages should be proactively lowered during the cenobamate titration period. Other concomitant ASMs should be reduced only if the patient reports a moderate/severe AE at any stage of the titration period. Significance: Cenobamate is an effective ASM with a dose‐dependent effect. To maximize effectiveness while maintaining the best tolerability profile, co‐medication management is needed. The recommendations included herein provide practical guidance for proactive and reactive management of co‐medication in cenobamate‐treated patients with DRE and a high drug load. Plain Language Summary: Patients with epilepsy may continue to have seizures even after treatment with several different antiseizure medications (ASMs). Cenobamate is an ASM that can reduce seizures in these patients. In this study, six Spanish experts in epilepsy discussed the best way to use cenobamate in drug‐resistant epilepsy. They provide practical guidance on when and how the dose of other ASMs might be adjusted to reduce side effects and optimize the use of cenobamate. [ABSTRACT FROM AUTHOR]

Published

2024

25. Development of long-acting local anesthetics: a long way from basic research to clinical application.

Author

Oda, Yutaka

Subjects

*SODIUM channel blockers, *POSTOPERATIVE pain treatment, *AFFERENT pathways, *BIOPOLYMERS, *LOCAL anesthetics, *ANESTHESIA adjuvants, *CONDUCTION anesthesia, *NERVE block

Abstract

This article discusses the development of long-acting local anesthetics for postoperative pain management. The use of opioids for pain relief can lead to adverse effects, so researchers have been exploring alternative options. The article explores different strategies, including quaternary lidocaine derivatives, voltage-gated sodium channel antagonists, site-1 sodium channel blockers, and controlled-release local anesthetics. While some of these options have shown promise, there are still limitations and challenges to overcome before they can be widely used in clinical practice. [Extracted from the article]

Published

2024

26. How pharmacology can aid in the diagnosis of mental disorders

Author

Seifert, Roland, Schirmer, Bastian, and Seifert, Johanna

Published

2024

27. Gender difference in the pharmacokinetics and metabolism of VX‐548 in rats.

Author

Yu, Guilan and Zhou, Xueying

Subjects

*RATS, *ORAL drug administration, *PHARMACOKINETICS, *LIVER microsomes, *SODIUM channel blockers

Abstract

VX‐548 is a sodium channel blocker, which acts as an analgesic. This study aims to investigate the gender differences in the pharmacokinetics and metabolism of VX‐548 in rats. After intravenous administration, the area under the curve (AUC0−t) of VX‐548 was much higher in female rats (1505.8 ± 47.3 ng·h/mL) than in male rats (253.8 ± 6.3 ng·h/mL), and the clearance in female rats (12.5 ± 0.8 mL/min/kg) was much lower than in male rats (65.1 ± 1.7 mL/min/kg). After oral administration, the AUC0−t in female rats was about 50‐fold higher than that in male rats. The oral bioavailability in male rats was 11% while it was 96% in female rats. An in vitro metabolism study revealed that the metabolism of VX‐548 in female rat liver microsomes was much slower than in male rats. Further metabolite identification suggested that the significant gender difference in pharmacokinetics was attributed to demethylation. The female rat liver microsomes showed a limited ability to convert VX‐548 into desmethyl VX‐548. Phenotyping experiments indicated that the formation of desmethyl VX‐548 was mainly catalyzed by CYP3A2 and CYP2C11 using rat recombinant CYPs. Overall, we revealed that the pharmacokinetics and metabolism of VX‐548 in male and female rats showed significant gender differences. [ABSTRACT FROM AUTHOR]

Published

2024

28. Common pitfalls in the use of hypertonic sodium bicarbonate for cardiac toxic drug poisonings.

Author

Chan, Betty S. and Buckley, Nicholas A.

Subjects

*DRUG toxicity, *SODIUM bicarbonate, *CARDIOVASCULAR agents, *SODIUM channel blockers, *BUNDLE-branch block, *RODENTICIDES

Abstract

Hypertonic sodium bicarbonate is advocated for the treatment of sodium channel blocker poisoning, but its efficacy varies amongst different sodium channel blockers. This Commentary addresses common pitfalls and appropriate usage of hypertonic sodium bicarbonate therapy in cardiotoxic drug poisonings. Serum alkalinization is best achieved by the synergistic effect of hypertonic sodium bicarbonate and hyperventilation (PCO2 ∼ 30–35 mmHg [0.47–0.6 kPa]). This reduces the dose of sodium bicarbonate required to achieve serum alkalinization (pH ∼ 7.45–7.55) and avoids adverse effects from excessive doses of hypertonic sodium bicarbonate. Tricyclic antidepressant poisoning responds well to sodium bicarbonate therapy, but many other sodium channel blockers may not. For instance, drugs that block the intercellular gap junctions, such as bupropion, do not respond well to alkalinization. For sodium channel blocker poisonings in which the expected response is unknown, a bolus of 1–2 mmol/kg sodium bicarbonate can be used to assess the response to alkalinization. Hypertonic sodium bicarbonate can cause electrolyte abnormalities such as hypokalaemia and hypocalcaemia, leading to QT interval prolongation and torsade de pointes in poisonings with drugs that have mixed sodium and potassium cardiac channel properties, such as hydroxychloroquine and flecainide. Excessive doses of hypertonic sodium bicarbonate commonly occur if it is administered until the QRS complex duration is < 100 ms. A prolonged QRS complex duration is not specific for sodium channel blocker toxicity. Some sodium channel blockers do not respond, and even when there is a response, it takes a few hours for the QRS complex duration to return completely to normal. In addition, QRS complex prolongation can be due to a rate-dependent bundle branch block. So, no further doses should be given after achieving serum alkalinization (pH ∼ 7.45–7.55). A further strategy to avoid overdosing patients with hypertonic sodium bicarbonate is to set maximum doses. Exceeding 6 mmol/kg is likely to cause hypernatremia, fluid overload, metabolic alkalosis, and cerebral oedema in many patients and potentially be lethal. We propose that hypertonic sodium bicarbonate therapy be used in patients with sodium channel blocker poisoning who have clinically significant toxicities such as seizures, shock (systolic blood pressure < 90 mmHg, mean arterial pressure <65 mmHg) or ventricular dysrhythmia. We recommend initial bolus dosing of hypertonic sodium bicarbonate of 1–2 mmol/kg, which can be repeated if the patient remains unstable, up to a maximum dose of 6 mmol/kg. This is recommended to be administered in conjunction with mechanical ventilation and hyperventilation to achieve serum alkalinization (PCO2∼30–35 mmHg [4-4.7 kPa]) and a pH of ∼7.45–7.55. With repeated bolus doses of hypertonic sodium bicarbonate, it is imperative to monitor and correct potassium and sodium abnormalities and observe changes in serum pH and on the electrocardiogram. Hypertonic sodium bicarbonate is an effective antidote for certain sodium channel blocker poisonings, such as tricyclic antidepressants, and when used in appropriate dosing, it works synergistically with hyperventilation to achieve serum alkalinization and to reduce sodium channel blockade. However, there are many pitfalls that can lead to excessive sodium bicarbonate therapy and severe adverse effects. [ABSTRACT FROM AUTHOR]

Published

2024

29. Grundlagen der Pharmakologie von Lokalanästhetika.

Author

Bockholt, Rebecca and Mirus, Martin

Subjects

*LIPID metabolism, *PHARMACOLOGY, *LOCAL anesthetics, *CONTINUING education units, *SYNDROMES, *NEUROTOXICOLOGY, *NEURONS, *MOLECULAR structure, *CARDIOTOXICITY, *SODIUM channel blockers, *DRUG development, *PHARMACODYNAMICS

Abstract

The development of local anesthetics revolutionized the performance of painful interventions. Local anesthetics have an effect on voltage-gated sodium channels in nerve fibers and modulate the conduction of impulses. With respect to the chemical structure, local anesthetics can be divided into amide and ester types. The structural differences of local anesthetics have an influence on the duration of action, the degradation pathways and specific side effects. Severe adverse events include cardiotoxicity and neurotoxicity. In addition to basic measures, such as the monitoring and securing of vital parameters, lipid infusion represents a treatment option in cases of intoxication. The recent developments of local anesthetics are particularly concerned with the reduction of toxicity and prolonging the duration of action. [ABSTRACT FROM AUTHOR]

Published

2024

30. Safety and Efficacy of Cenobamate for the Treatment of Focal Seizures in Older Patients: Post Hoc Analysis of a Phase III, Multicenter, Open-Label Study.

Author

O'Dwyer, Rebecca, Stern, Sean, Wade, Clarence T., Guggilam, Anuradha, and Rosenfeld, William E.

Subjects

*PATIENT safety, *DRUG side effects, *DATA analysis, *RESPIRATORY infections, *RESEARCH funding, *DIZZINESS, *FATIGUE (Physiology), *CLINICAL trials, *TREATMENT effectiveness, *DESCRIPTIVE statistics, *HYPERSOMNIA, *EPILEPSY, *DRUG efficacy, *STATISTICS, *COMPARATIVE studies, *SODIUM channel blockers, *ANTICONVULSANTS, *ACCIDENTAL falls, *POSTURAL balance, *EVALUATION, *OLD age

Abstract

Background: Cenobamate is an antiseizure medication (ASM) approved in the US and Europe for the treatment of uncontrolled focal seizures. Objective: This post hoc analysis of a phase III, open-label safety study assessed the safety and efficacy of adjunctive cenobamate in older adults versus the overall study population. Methods: Adults aged 18–70 years with uncontrolled focal seizures taking stable doses of one to three ASMs were enrolled in the phase III, open-label safety study; adults aged 65–70 years from that study were included in our safety analysis. Discontinuations due to adverse events and treatment-emergent adverse events (TEAEs) were assessed throughout the study in all patients who received one or more doses of cenobamate (safety study population). Efficacy was assessed post hoc in patients who had adequate seizure data available (post hoc efficacy population); we assessed patients aged 65–70 years from that population. Overall, 100% responder rates were assessed in the post hoc efficacy maintenance-phase population in 3-month intervals. Concomitant ASM drug load changes were also measured. For each ASM, drug load was defined as the ratio of actual drug dose/day to the World Health Organization defined daily dose (DDD). Results: Of 1340 patients (mean age 39.7 years) in the safety study population, 42 were ≥ 65 years of age (mean age 67.0 years, 52.4% female). Median duration of exposure was 36.1 and 36.9 months for overall patients and older patients, respectively, and mean epilepsy duration was 22.9 and 38.5 years, respectively. At 1, 2, and 3 years, 80%, 72%, and 68% of patients overall, and 76%, 71%, and 69% of older patients, respectively, remained on cenobamate. Common TEAEs (≥ 20%) were somnolence and dizziness in overall patients, and somnolence, dizziness, fall, fatigue, balance disorder, and upper respiratory tract infection in older patients. Falls in older patients occurred after a mean 452.1 days of adjunctive cenobamate treatment (mean dose 262.5 mg/day; mean concomitant ASM drug load 2.46). Of 240 patients in the post hoc efficacy population, 18 were ≥ 65 years of age. Mean seizure frequency at baseline was 18.1 seizures/28 days for the efficacy population and 3.1 seizures/28 days for older patients. Rates of 100% seizure reduction within 3-month intervals during the maintenance phase increased over time for the overall population (n = 214) and older adults (n = 15), reaching 51.9% and 78.6%, respectively, by 24 months. Mean percentage change in concomitant ASM drug load, not including cenobamate, was reduced in the overall efficacy population (31.8%) and older patients (36.3%) after 24 months of treatment. Conclusions: Results from this post hoc analysis showed notable rates of efficacy in older patients taking adjunctive cenobamate. Rates of several individual TEAEs occurred more frequently in older patients. Further reductions in concomitant ASMs may be needed in older patients when starting cenobamate to avoid adverse effects such as somnolence, dizziness, and falls. Clinical Trials Registration: ClinicalTrials.gov NCT02535091. [ABSTRACT FROM AUTHOR]

Published

2024

31. EFFECTS OF SELECTIVE AND NON-SELECTIVE SODIUM CHANNEL BLOCKERS ON RAT PAIN SENSITIVITY.

Author

MÂRZA, AURELIA, CARĂTAŞU, CĂTALIN CEZAR, BILD, VERONICA, TAMBA, BOGDAN IONEL, and BILD, WALTHER

Subjects

SODIUM channel blockers, SODIUM channels, SENSORY neurons, MOLECULAR biology, PAIN measurement, BRUGADA syndrome

Abstract

Copyright of Farmacia is the property of Societatea de Stiinte Farmaceutice Romania and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2024

32. Update on Treating Painful Diabetic Peripheral Neuropathy: A Review of Current US Guidelines with a Focus on the Most Recently Approved Management Options.

Author

Mallick-Searle, Theresa and Adler, Jeremy A

Subjects

ANALGESIA, DIABETIC neuropathies, SODIUM channel blockers, ELECTRICAL injuries, QUALITY of life, ORAL medication, DIABETES complications, SEROTONIN syndrome

Abstract

Painful diabetic peripheral neuropathy (DPN) is a highly prevalent and disabling complication of diabetes that is often misdiagnosed and undertreated. The management of painful DPN involves treating its underlying cause via lifestyle modifications and intensive glucose control, targeting its pathogenesis, and providing symptomatic pain relief, thereby improving patient function and health-related quality of life. Four pharmacologic options are currently approved by the US Food and Drug Administration (FDA) to treat painful DPN. These include three oral medications (duloxetine, pregabalin, and tapentadol extended release) and one topical agent (capsaicin 8% topical system). More recently, the FDA approved several spinal cord stimulation (SCS) devices to treat refractory painful DPN. Although not FDA-approved specifically to treat painful DPN, tricyclic antidepressants, serotonin/norepinephrine reuptake inhibitors, gabapentinoids, and sodium channel blockers are common first-line oral options in clinical practice. Other strategies may be used as part of individualized comprehensive pain management plans. This article provides an overview of the most recent US guidelines for managing painful DPN, with a focus on the two most recently approved treatment options (SCS and capsaicin 8% topical system), as well as evidence for using FDA-approved and guideline-supported drugs and devices. Also discussed are unmet needs for this patient population, and evidence for potential future treatments for painful DPN, including drugs with novel mechanisms of action, electrical stimulation devices, and nutraceuticals. [ABSTRACT FROM AUTHOR]

Published

2024

33. Dapagliflozin and atrial fibrillation: elevated dosing to achieve class I antiarrhythmic effects?

Author

Christ, Torsten, Schwedhelm, Edzard, and Eschenhagen, Thomas

Subjects

*DAPAGLIFLOZIN, *MYOCARDIAL depressants, *ATRIAL fibrillation, *SODIUM channel blockers

Abstract

The article discusses the potential antiarrhythmic effects of sodium-glucose co-transporter-2 inhibitors (SGLT2i) in patients with atrial fibrillation (AF). The authors examine the pharmacodynamics of dapagliflozin, a specific SGLT2i, and question the validity of previous research suggesting that SGLT2i may block peak cardiac sodium currents. They argue that the concentrations of dapagliflozin required to achieve this effect are much higher than therapeutic doses, making it unlikely that sodium channel block is the mechanism behind the potential benefits of SGLT2i in AF. The authors also emphasize the safety of SGLT2i, as they have a wide safety margin in terms of their effects on sodium channels. [Extracted from the article]

Published

2024

34. Reversibilität einer kritischen intraventrikulären Leitungsverzögerung unter Flecainid und Lacosamid durch Natriumbicarbonat

Author

Gallinger, Anja, Osei-Davies, Rahman, and Hennersdorf, F.

Published

2024

35. Distinctive In Vitro Phenotypes in iPSC-Derived Neurons From Patients With Gain- and Loss-of-Function SCN2A Developmental and Epileptic Encephalopathy.

Author

Miaomiao Mao, Mattei, Cristiana, Rollo, Ben, Byars, Sean, Cuddy, Claire, Berecki, Geza, Heighway, Jacqueline, Pachernegg, Svenja, Menheniott, Trevelyan, Apted, Danielle, Linghan Jia, Dalby, Kelley, Nemiroff, Alex, Mullen, Saul, Reid, Christopher A., Maljevic, Snezana, and Petrou, Steven

Subjects

*SODIUM channels, *INDUCED pluripotent stem cells, *PHENOTYPES, *NEURONS, *NEURAL circuitry, *SODIUM channel blockers, *PEOPLE with epilepsy

Abstract

SCN2A encodes NaV1.2, an excitatory neuron voltage-gated sodium channel and a major monogenic cause of neurodevelopmental disorders, including developmental and epileptic encephalopathies (DEE) and autism. Clinical presentation and pharmocosensitivity vary with the nature of SCN2A variant dysfunction and can be divided into gain-of-function (GoF) cases with pre- or peri-natal seizures and loss-of-function (LoF) patients typically having infantile spasms after 6 months of age. We established and assessed patient induced pluripotent stem cell (iPSC) - derived neuronal models for two recurrent SCN2A DEE variants with GoF R1882Q and LoF R853Q associated with early- and late-onset DEE, respectively. Two male patient-derived iPSC isogenic pairs were differentiated using Neurogenin-2 overexpression yielding populations of cortical-like glutamatergic neurons. Functional properties were assessed using patch clamp and multielectrode array recordings and transcriptomic profiles obtained with total mRNA sequencing after 2-4 weeks in culture. At 3 weeks of differentiation, increased neuronal activity at cellular and network levels was observed for R1882Q iPSC-derived neurons. In contrast, R853Q neurons showed only subtle changes in excitability after 4 weeks and an overall reduced network activity after 7 weeks in vitro. Consistent with the reported efficacy in some GoF SCN2A patients, phe-nytoin (sodium channel blocker) reduced the excitability of neurons to the control levels in R1882Q neuronal cultures. Transcriptomic alterations in neurons were detected for each variant and convergent pathways suggested potential shared mechanisms underlying SCN2A DEE. In summary, patient iPSC-derived neuronal models of SCN2A GoF and LoF pathogenic variants causing DEE show specific functional and transcriptomic in vitro phenotypes. [ABSTRACT FROM AUTHOR]

Published

2024

36. Methylglyoxal activates transient receptor potential A1/V1 via reactive oxygen species in the spinal dorsal horn.

Author

Ueno, Takeru, Yamanaka, Manabu, Taniguchi, Wataru, Nishio, Naoko, Matsuyama, Yuki, Miyake, Ryo, Kaimochi, Yuta, Nakatsuka, Terumasa, and Yamada, Hiroshi

Subjects

*NEURAL transmission, *REACTIVE oxygen species, *ADVANCED glycation end-products, *PYRUVALDEHYDE, *SODIUM channel blockers

Abstract

Methylglyoxal (MGO), a highly reactive dicarbonyl metabolite of glucose primarily formed during the glycolytic pathway, is a precursor of advanced glycation end-products (AGEs). Recently, numerous studies have shown that MGO accumulation can cause pain and hyperalgesia. However, the mechanism through which MGO induces pain in the spinal dorsal horn remains unclear. The present study investigated the effect of MGO on spontaneous excitatory postsynaptic currents (sEPSC) in rat spinal dorsal horn neurons using blind whole-cell patch-clamp recording. Perfusion of MGO increased the frequency and amplitude of sEPSC in spinal horn neurons in a concentration-dependent manner. Additionally, MGO administration increased the number of miniature EPSC (mEPSC) in the presence of tetrodotoxin, a sodium channel blocker. However, 6-cyano-7-nitroqiunocaline-2,3-dione (CNQX), an AMPA/kainate receptor antagonist, blocked the enhancement of sEPSC by MGO. HC-030031, a TRP ankyrin-1 (TRPA1) antagonist, and capsazepine, a TRP vanilloid-1 (TRPV1) antagonist, inhibited the action of MGO. Notably, the effects of MGO were completely inhibited by HC-030031 and capsazepine. MGO generates reactive oxygen species (ROS) via AGEs. ROS also potentially induce pain via TRPA1 and TRPV1 in the spinal dorsal horn. Furthermore, we examined the effect of MGO in the presence of N-tert-butyl-α-phenylnitrone (PBN), a non-selective ROS scavenger, and found that the effect of MGO was completely inhibited. These results suggest that MGO increases spontaneous glutamate release from the presynaptic terminal to spinal dorsal horn neurons through TRPA1, TRPV1, and ROS and could enhance excitatory synaptic transmission. [ABSTRACT FROM AUTHOR]

Published

2024

37. First Full-Length Cloning of Human NaV1.7 in S. Cerevisiae-Based Novel D-Crypt™ Platform for its High-Scale Production.

Author

Arora, Kajal, Roy, Sourav Singha, Kumar, Sudhir, Rastogi, Ruchir, Prattipati, Mahesh, Gupta, Reeshu, Mehrotra, Nupur, and Kundu, Prabuddha

Subjects

*HUMAN cloning, *SODIUM channels, *FLUORESCENCE resonance energy transfer, *HOMOLOGOUS recombination, *MOLECULAR cloning, *MEMBRANE potential, *PYRETHROIDS

Abstract

NaV1.7, a voltage-gated sodium channel, induces chronic pain. Current research on the discovery of inhibitors against NaV1.7 is advancing with the hope of treating chronic pain conditions in patients suffering from various diseases. However, to characterize NaV1.7 and inhibitor interactions, a higher yield of expression is required to obtain sufficient protein. Molecular cloning of hNaV1.7 was done using the homologous recombination method in our novel S. cerevisiae-based D-crypt™ platform. The platform was designed for the high-yield production of 'difficult-to-express' proteins (DTE-Ps) up to 500 L. The changes in the cell membrane potential of hNaV1.7 were determined using a fluorescence resonance energy transfer (FRET) assay with tetracaine (hNaV1.7 inhibitor). Expression analysis of hNaV1.7 showed 2 bands of size 250 and 280 kDa that were absent in untransfected yeast cells. Immunofluorescence images revealed the presence of hNaV1.7 on the membrane of hNaV1.7-expressing yeast cells. Tetracaine exhibited concentration-dependent inhibition of the FRET ratio, with the order of potency (IC50 = 0.46 µM) being approximately the same as previously reported, suggesting the functionality of the channel protein expressed in the D-crypt™ platform. Cloning of NaV1.7 in the D-crypt™ platform will help to scale up the production of channel proteins, which will ultimately help in the structural and functional characterization of the binding interactions between toxins and the NaV1.7 channel to identify more specific NaV1.7 inhibitors. [ABSTRACT FROM AUTHOR]

Published

2024

38. Functional neuronal circuits emerge in the absence of developmental activity.

Author

Barabási, Dániel L., Schuhknecht, Gregor F. P., and Engert, Florian

Subjects

ACTION potentials, SODIUM channel blockers, GENETIC code, FISH locomotion

Abstract

The complex neuronal circuitry of the brain develops from limited information contained in the genome. After the genetic code instructs the birth of neurons, the emergence of brain regions, and the formation of axon tracts, it is believed that temporally structured spiking activity shapes circuits for behavior. Here, we challenge the learning-dominated assumption that spiking activity is required for circuit formation by quantifying its contribution to the development of visually-guided swimming in the larval zebrafish. We found that visual experience had no effect on the emergence of the optomotor response (OMR) in dark-reared zebrafish. We then raised animals while pharmacologically silencing action potentials with the sodium channel blocker tricaine. After washout of the anesthetic, fish could swim and performed with 75–90% accuracy in the OMR paradigm. Brain-wide imaging confirmed that neuronal circuits came 'online' fully tuned, without requiring activity-dependent plasticity. Thus, complex sensory-guided behaviors can emerge through activity-independent developmental mechanisms. How functional neuronal circuits are established during development is not fully understood. Here the authors show, by raising fish in the dark and under anesthesia, that brain activity is not needed for the development of complex, decision-making circuits. [ABSTRACT FROM AUTHOR]

Published

2024

39. Medication Pipeline Schizophrenia and PTSD.

Author

Miller, John

Subjects

*MENTAL illness drug therapy, *DRUG approval, *DRUG efficacy, *PSYCHIATRY, *PARASYMPATHOMIMETIC agents, *SODIUM channel blockers, *SEROTONIN antagonists, *POST-traumatic stress disorder, *MUSCARINIC agonists, *CELL receptors, *MEMBRANE proteins, *DRUG development, *ANTIPSYCHOTIC agents, *ASPARTIC acid, *CARRIER proteins, *PATIENT safety, *PSYCHOTHERAPY, *PHARMACODYNAMICS, *CHEMICAL inhibitors, DRUG therapy for schizophrenia

Abstract

The article discusses the novel agents and other treatments for psychiatric disorders, particularly schizophrenia and posttraumatic stress disorders (PTSD), that are under clinical trials. Also cited are the new drug application filed by Karuna Therapeutics with the U.S. Food and Drug Administration (FDA) for KarXT as schizophrenia treatment in adults and the other drugs like emraclidine from Cerevel Therapeutics and roluperidone from Minerva Neurosciences, Inc.

Published

2024

40. Safety and efficacy of the epithelial sodium channel blocker idrevloride in people with primary ciliary dyskinesia (CLEAN-PCD): a multinational, phase 2, randomised, double-blind, placebo-controlled crossover trial.

Author

Ringshausen, Felix C, Shapiro, Adam J, Nielsen, Kim G, Mazurek, Henryk, Pifferi, Massimo, Donn, Karl H, van der Eerden, Menno M, Loebinger, Michael R, Zariwala, Maimoona A, Leigh, Margaret W, Knowles, Michael R, and Ferkol, Thomas W

Subjects

CILIARY motility disorders, DYSKINESIAS, SODIUM channel blockers, CROSSOVER trials, HYPERTONIC saline solutions, MUCOCILIARY system

Abstract

Mucociliary clearance is dysfunctional in people with primary ciliary dyskinesia, resulting in the accumulation of dehydrated mucus in the airways that is difficult to clear. We undertook a study to assess the benefit on lung function of treatment with a nebulised epithelial sodium channel (ENaC) blocker, idrevloride, with or without hypertonic saline, in people with primary ciliary dyskinesia. The CLEAN-PCD trial was a phase 2, randomised, double-blind, placebo-controlled crossover trial conducted at 32 tertiary adult and paediatric care centres and university hospitals in Canada, Denmark, Germany, Italy, the Netherlands, Poland, the UK, and the USA. People with a confirmed diagnosis of primary ciliary dyskinesia, aged 12 years or older, with a percentage of predicted FEV 1 (ppFEV 1) in the range of 40% to <90%, were randomly assigned in a 2:2:1:1 ratio (block size=6), stratified by ppFEV 1 at screening, to one of four sequences: (1) idrevloride in hypertonic saline in treatment period 1 then hypertonic saline in treatment period 2; (2) hypertonic saline in treatment period 1 then idrevloride in hypertonic saline in treatment period 2; (3) idrevloride in treatment period 1 then placebo in treatment period 2; and (4) placebo in treatment period 1 then idrevloride in treatment period 2. The idrevloride dose was 85 μg and hypertonic saline was 4·2% NaCl. 3 mL of each study treatment was nebulised twice daily for 28 days in treatment periods 1 and 2; the two 28-day treatment periods were separated by a 28-day washout period. The primary endpoint was absolute change from baseline in ppFEV 1 after 28 days. Safety assessments and reports of adverse events were made at clinic visits during each treatment period and by a follow-up telephone call 28 days after the last dose of study drug. Additionally, adverse events could be reported at a follow-up telephone call 3 days after the start of dosing and as they arose. Participants who received at least one dose of study drug were included in the safety analyses (safety set), and those who also had spirometry data were included in the efficacy analyses (full analysis set). The completed study is registered (EudraCT 2015-004917-26; ClinicalTrials.gov NCT02871778). Between Sep 14, 2016, and May 31, 2018, 216 patients were screened and 123 were randomly assigned to one of four crossover sequences. Across the two treatment periods, treatment with idrevloride in hypertonic saline was initiated in 80 patients and completed in 78 patients (all 78 had data available and were included in the analysis); hypertonic saline initiated in 81 patients and completed in 76 patients (75 had data available and were included in the analysis); idrevloride initiated in 37 patients and completed in 35 patients (34 had data available and were included in the analysis); and placebo initiated in 36 patients and completed in 34 patients (all 34 had data available and were included in the analysis). Greater absolute increases in ppFEV 1 from baseline to 28 days of treatment were seen with idrevloride in hypertonic saline (least-squares mean absolute change from baseline 1·0 percentage points, 95% CI –0·4 to 2·4) than with hypertonic saline alone (least-squares mean absolute change from baseline of –0·5 percentage points, –2·0 to 0·9; difference 1·5 percentage points, 95% CI <0·1 to 3·0; p=0·044). There was no significant difference in ppFEV 1 for the parallel comparison of idrevloride in hypertonic saline compared with placebo or the crossover comparison of idrevloride with placebo. Adverse events were similar across treatments (57 to 65% of patients). Cough occurred in a greater proportion of participants during treatments that contained idrevloride or hypertonic saline compared with placebo, and oropharyngeal pain occurred in a greater proportion of participants during idrevloride treatments than during treatment with hypertonic saline alone or placebo, whereas chest discomfort was more common during treatments that included hypertonic saline. In this phase 2 crossover study, idrevloride in hypertonic saline was safe and associated with improved lung function over a 28-day period in people with primary ciliary dyskinesia compared with hypertonic saline alone. Larger, longer clinical studies are warranted to explore the potential benefits of idrevloride in combination with hypertonic saline in people with primary ciliary dyskinesia. Parion Sciences, under agreement with Vertex Pharmaceuticals. [ABSTRACT FROM AUTHOR]

Published

2024

41. The "Near"-Narrowed Internal Auditory Canal Syndrome in Adults: Clinical Aspects, Audio-Vestibular Findings, and Radiological Criteria for Diagnosis.

Author

Ionescu, Eugen C., Reynard, Pierre, Idriss, Samar A., Ltaief-Boudriga, Aicha, Joly, Charles-Alexandre, and Thai-Van, Hung

Subjects

*VERTIGO, *SYMPTOMS, *ANATOMICAL planes, *INNER ear, *DIAGNOSIS, *ADULTS

Abstract

Introduction: Vestibular Paroxysmia (VP) refers to short attacks of vertigo, spontaneous or triggered by head movements, and implies the presence of a compressive vascular loop in contact with the cochleovestibular nerve (CVN). Classically, a narrowed internal auditory canal (IAC) corresponds to a diameter of less than 2 mm on CT, usually associated with a hypoplastic CVN on MRI. The aim of this study was to discuss a distinct clinical entity mimicking VP in relation to a "near"-narrowed IAC (NNIAC) and to propose radiological criteria for its diagnosis. Methods: Radiological measurements of the IAC were compared between three groups: the study group (SG, subjects with a clinical presentation suggestive of VP, but whose MRI of the inner ear and pontocerebellar angle excluded a compressive vascular loop) and two control groups (adult and children) with normal vestibular evaluations and no history of vertigo. Results: 59 subjects (18 M and 41 F) were included in the SG. The main symptoms of NNIAC were positional vertigo, exercise- or rapid head movements-induced vertigo, and dizziness. The statistical analysis in the study group showed that the threshold values for diagnosis were 3.3 mm (in tomodensitometry) and 2.9 mm (in MRI) in coronal sections of IAC. Although a significantly lower mean value for axial IAC diameter was found in SG compared with controls, the statistics did not reveal a threshold due to the large inter-individual variations in IAC measurements in normal subjects. There was no significant difference in IAC diameter between the adult and pediatric controls. Conclusions: In the present study, we report a new anatomopathological condition that appears to be responsible for a clinical picture very similar—but not identical—to VP in association with the presence of an NNIAC. The diagnosis requires a careful analysis of the IAC's shape and diameters in both axial and coronal planes. [ABSTRACT FROM AUTHOR]

Published

2023

42. Use of Sodium Channel Blockers in the Thr226Met Pathologic Variant of SCN1A : A Case Report.

Author

Nájera-Chávez, Brenda Carolina, Seeber, Lea, Goldhahn, Klaus, and Panzer, Axel

Subjects

*SODIUM channel blockers, *EPILEPSY, *PSYCHOGENIC nonepileptic seizures, *FEBRILE seizures, *SODIUM channels, *DRUG therapy, *DEVELOPMENTAL delay

Abstract

The Thr226Met pathologic variant of the SCN1A gene has been associated with the clinical development of an early infantile developmental and epileptic encephalopathy (EIDEE) different from Dravet's syndrome. The electrophysiological mechanisms of the mutated channel lead to a paradoxical gain and loss of function. The use of sodium channel blockers (SCB) that counteract this gain of function has been described in previous studies and they can be safely administered to patients carrying mutations in other sodium channel subtypes without causing a worsening of seizures. We report the use of SCB in a child harboring the Thr226Met pathologic variant of SCN1A with early-onset pharmaco-resistant migrating seizures, as well as developmental delay. Lacosamide led to a dramatic reduction in seizure frequency; however, only a mild improvement in the epileptic activity depicted by electroencephalography (EEG) was achieved. The introduction of carbamazepine as an add-on therapy led to a notable reduction in epileptic activity via EEG and to an improvement in sensorimotor development. Despite the overall clinical improvement, the patient developed febrile seizures and a nonepileptic jerking of the right hand. In this case of EIDEE with the Thr226Met variant, we demonstrate a beneficial pharmacological intervention of SCB in contrast to findings described in current literature. Our report encourages the cautious use of SCB at early stages of the disease in patients carrying this pathologic variant. [ABSTRACT FROM AUTHOR]

Published

2023

43. Study of Amiloride Binding to Human Serum Albumin: Insights from Thermodynamic, Spectroscopic, and Molecular Docking Investigations.

Author

Rahman, Safikur, Iram, Sana, Rehman, Md Tabish, Hussain, Afzal, Jan, Arif Tasleem, and Kim, Jihoe

Subjects

*SERUM albumin, *MOLECULAR docking, *AMILORIDE, *SODIUM channels, *SODIUM channel blockers, *MOLECULAR dynamics, *MOLECULAR spectroscopy, *DICHROISM

Abstract

This study was undertaken to investigate the interaction between the sodium channel blocker amiloride (AML) and human serum albumin (HSA). A combination of multi-spectroscopic techniques and computational methods were employed to identify the AML binding site on HSA and the forces responsible for the formation of the HSA–AML complex. Our findings revealed that AML specifically binds to Sudlow's site II, located in subdomain IIIA of HSA, and that the complex formed is stabilized using van der Waals hydrogen-bonding and hydrophobic interactions. FRET analysis showed that the distance between AML and Trp214 was optimal for efficient quenching. UV-Vis spectroscopy and circular dichroism indicated minor changes in the structure of HSA after AML binding, and molecular dynamics simulations (MDS) conducted over 100 ns provided additional evidence of stable HSA–AML-complex formation. This study enhances understanding of the interaction between AML and HSA and the mechanism responsible. [ABSTRACT FROM AUTHOR]

Published

2023

44. General Anesthesia Blocks Pain-Induced Hemorrhage and Locomotor Deficits After Spinal Cord Injury in Rats.

Author

Davis, Jacob A., Bopp, Anne C., Henwood, Melissa K., Bean, Paris, and Grau, James W.

Subjects

*SPINAL cord injuries, *CONDUCTION anesthesia, *SODIUM channel blockers, *GENERAL anesthesia, *SYSTOLIC blood pressure

Abstract

Research has shown that engaging pain (nociceptive) pathways after spinal cord injury (SCI) aggravates secondary injury and undermines locomotor recovery. This is significant because SCI is commonly accompanied by additional tissue damage (polytrauma) that drives nociceptive activity. Cutting communication with the brain by means of a surgical transection, or pharmacologically transecting the cord by slowly infusing a sodium channel blocker (lidocaine) rostral to a thoracic contusion, blocks pain-induced hemorrhage. These observations suggest that the adverse effect of pain after SCI depends on supraspinal (brain) systems. We hypothesize that inhibiting brain activity using a general anesthetic (e.g., pentobarbital, isoflurane) should have a protective effect. The present study shows that placing rats in an anesthetic state with pentobarbital or isoflurane 24 h after a lower thoracic contusion injury blocks pain-induced intraspinal inflammation and hemorrhage when administered before pain. Pentobarbital also extends protective effects against locomotor deficits produced by noxious stimulation. Inducing anesthesia after noxious stimulation, however, has no effect. Similarly, subanesthetic dosages of pentobarbital were also ineffective at blocking pain-induced hemorrhage. Also examined were the hemodynamic impacts of both pain and anesthetic delivery after SCI. Peripheral pain-input induced an acute increase in systolic blood pressure; isoflurane and pentobarbital prevent this increase, which may contribute to the protective effect of anesthesia. The results suggest that placing patients with SCI in a state akin to a medically induced coma can have a protective effect that blocks the adverse effects of pain. [ABSTRACT FROM AUTHOR]

Published

2023

45. Sodium Channel Blockers

Author

Pant, AB

Published

2024

46. Tuning Sodium Channel Blockers to the Near-Atomic Level.

Author

Eyal, Sara

Subjects

*SODIUM channel blockers, *ANTICONVULSANTS, *INVESTIGATIONAL drugs, *STRUCTURE-activity relationships, *LOCAL anesthetics

Abstract

Dual-Pocket Inhibition of Nav Channels by the Antiepileptic Drug Lamotrigine Huang J, Fan X, Jin X, Teng L, Yan N. Proc Natl Acad Sci USA. 2023;120(41):e2309773120. doi:10.1073/pnas.2309773120 Voltage-gated sodium (Nav) channels govern membrane excitability, thus setting the foundation for various physiological and neuronal processes. Nav channels serve as the primary targets for several classes of widely used and investigational drugs, including local anesthetics, antiepileptic drugs, antiarrhythmics, and analgesics. In this study, we present cryogenic electron microscopy (cryo-EM) structures of human Nav1.7 bound to two clinical drugs, riluzole (RLZ) and lamotrigine (LTG), at resolutions of 2.9 Å and 2.7 Å, respectively. A 3D EM reconstruction of ligand-free Nav1.7 was also obtained at 2.1 Å resolution. RLZ resides in the central cavity of the pore domain and is coordinated by residues from repeats III and IV. Whereas one LTG molecule also binds to the central cavity, the other is found beneath the intracellular gate, known as site BIG. Therefore, LTG, similar to lacosamide and cannabidiol, blocks Nav channels via a dual-pocket mechanism. These structures, complemented with docking and mutational analyses, also explain the structure-activity relationships of the LTG-related linear 6,6 series that have been developed for improved efficacy and subtype specificity on different Nav channels. Our findings reveal the molecular basis for these drugs' mechanism of action and will aid the development of novel antiepileptic and pain-relieving drugs. [ABSTRACT FROM AUTHOR]

Published

2024

47. Therapeutic Use of Neuraxial Drugs in Veterinary Medicine

Author

Guedes, Alonso, Kennedy, Martin, Yaksh, Tony, editor, and Hayek, Salim, editor

Published

2023

48. A systemic review and PASS assisted prediction of phytoconstituents for epilepsy.

Author

Muduli, Sushanta Kumar, Sharma, Itika, Sharma, Neha, and Khurana, Navneet

Subjects

*CALCIUM antagonists, *GABA receptors, *NEUROTRANSMITTER uptake inhibitors, *SODIUM channel blockers, *EPILEPSY, *LITERATURE reviews, *THERAPEUTICS

Abstract

Epilepsy is one of the oldest known neurological illnesses with at least 3000 years of proven history. It is the most common neurological disorder, affecting 1-2 percent of the world's population and having a significant impact on many parts of one's quality of life. Other approaches, such as PASS prediction software, exist for determining the therapeutic use of phytochemicals. Various phytochemicals were chosen from the literature review and their action was examined in the PASS program. In the therapy or management of epilepsy, phytochemicals or medicinal plants are widely used. The main objective of this study is to predict the biological activities of the certain phytoconstituents which are interpreted to possesses some Antiseizures activity. A number of phytoconstituents were chosen for this study based on the available published literature. Using the sanctioned improved on sub-atomic information line-passage approach obtained from PubChem and PASS online programming, the various anti-seizure activities of the chosen phytoconstituents were deciphered. In the pharmacological intervention categories, several phytoconstituents were found to have better results than licensed drugs. PASS software was used to analyses the biological activities of the selected Thirty-one phytoconstituents in this investigation. Using the PASS programmed, the following activities were Anticonvulsant, GABA transport-3 inhibitor, Acute neurologic disorders treatment, Calcium regulator, GABA B receptor agonist, 5 Hydroxytryptamine uptake stimulant, Calcium channel blocker, Dementia treatment, Kainate receptor antagonist, Membrane integrity agonist, Nav1.8 sodium channel blocker, Neurotransmitter uptake inhibitor, neurodegenerative diseases treatment. PASS is a powerful online tool that was employed in this work to virtually screen compounds and phytoconstituents for biological activity. Selected phytoconstituents were discovered to be useful in the treatment of epilepsy in this investigation. The outcomes of this study can be used to guide future phytochemical research. [ABSTRACT FROM AUTHOR]

Published

2023

49. Genetic Background of Epilepsy and Antiepileptic Treatments.

Author

Borowicz-Reutt, Kinga, Czernia, Julia, and Krawczyk, Marlena

Subjects

*EPILEPSY, *SODIUM channel blockers, *GENETIC variation, *GABA receptors, *SODIUM channels, *CHROMOSOME duplication, *PHENOBARBITAL

Abstract

Advanced identification of the gene mutations causing epilepsy syndromes is expected to translate into faster diagnosis and more effective treatment of these conditions. Over the last 5 years, approximately 40 clinical trials on the treatment of genetic epilepsies have been conducted. As a result, some medications that are not regular antiseizure drugs (e.g., soticlestat, fenfluramine, or ganaxolone) have been introduced to the treatment of drug-resistant seizures in Dravet, Lennox-Gastaut, maternally inherited chromosome 15q11.2-q13.1 duplication (Dup 15q) syndromes, and protocadherin 19 (PCDH 19)-clusterig epilepsy. And although the effects of soticlestat, fenfluramine, and ganaxolone are described as promising, they do not significantly affect the course of the mentioned epilepsy syndromes. Importantly, each of these syndromes is related to mutations in several genes. On the other hand, several mutations can occur within one gene, and different gene variants may be manifested in different disease phenotypes. This complex pattern of inheritance contributes to rather poor genotype–phenotype correlations. Hence, the detection of a specific mutation is not synonymous with a precise diagnosis of a specific syndrome. Bearing in mind that seizures develop as a consequence of the predominance of excitatory over inhibitory processes, it seems reasonable that mutations in genes encoding sodium and potassium channels, as well as glutamatergic and gamma-aminobutyric (GABA) receptors, play a role in the pathogenesis of epilepsy. In some cases, different pathogenic variants of the same gene can result in opposite functional effects, determining the effectiveness of therapy with certain medications. For instance, seizures related to gain-of-function (GoF) mutations in genes encoding sodium channels can be successfully treated with sodium channel blockers. On the contrary, the same drugs may aggravate seizures related to loss-of-function (LoF) variants of the same genes. Hence, knowledge of gene mutation–treatment response relationships facilitates more favorable selection of drugs for anticonvulsant therapy. [ABSTRACT FROM AUTHOR]

Published

2023

50. Effects of aconitine on the respiratory activity of brainstem-spinal cord preparations isolated from newborn rats.

Author

Yoda, Shunya, Onimaru, Hiroshi, and Izumizaki, Masahiko

Subjects

*SODIUM channel blockers, *SODIUM channels, *MOTOR neurons, *NEWBORN infants, *BRAIN stem, *LOCAL anesthetics, *RESPIRATORY muscles

Abstract

Aconitine is a sodium channel opener, but its effects on the respiratory center are not well understood. We investigated the dose-dependent effects of aconitine on central respiratory activity in brainstem-spinal cord preparations isolated from newborn rats. Bath application of 0.5–5 μM aconitine caused an increase in respiratory rhythm and decrease in the inspiratory burst amplitude of the fourth cervical ventral root (C4). Separate application of aconitine revealed that medullary neurons were responsible for the respiratory rhythm increase, and neurons in both the medulla and spinal cord were involved in the decrease of C4 amplitude by aconitine. A local anesthetic, lidocaine (100 μM), or a voltage-dependent sodium channel blocker, tetrodotoxin (0.1 μM), partially antagonized the C4 amplitude decrease by aconitine. Tetrodotoxin treatment tentatively decreased the respiratory rhythm, but lidocaine tended to further increase the rhythm. Treatment with 100 μM riluzole or 100 μM flufenamic acid, which are known to inhibit respiratory pacemaker activity, did not reduce the respiratory rhythm enhanced by aconitine + lidocaine. The application of 1 μM aconitine depolarized the preinspiratory, expiratory, and inspiratory motor neurons. The facilitated burst rhythm of inspiratory neurons after aconitine disappeared in a low Ca2+/high Mg2+ synaptic blockade solution. We showed the dose-dependent effects of aconitine on respiratory activity. The antagonists reversed the depressive effects of aconitine in different manners, possibly due to their actions on different sites of sodium channels. The burst-generating pacemaker properties of neurons may not be involved in the generation of the facilitated rhythm after aconitine treatment. [ABSTRACT FROM AUTHOR]

Published

2023