17,667 results on '"LAMOTRIGINE"'
Search Results
2. Physiological-based Pharmacokinetics Approach to Medication Exposure During Pregnancy and Breastfeeding (PBPK)
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Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD) and Page B. Pennell, MD, Professor
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- 2024
3. Bioequivalence Study of 200 mg Lamotrigine Tablet Under Fasting Conditions
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- 2024
4. Bioequivalence Study of 200 mg Lamotrigine Tablet Under Non-Fasting Conditions
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- 2024
5. Lamotrigine 25 mg Chewable Tablets, Non-Fasting
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- 2024
6. Lamotrigine 25 mg Chewable Tablets, Fasting
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- 2024
7. Ketogenic Diet for New-Onset Absence Epilepsy
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- 2024
8. Effect of Adding Lamotrigine to Sodium Valproate in Childhood Epilepsy: Clinicolabratory Study
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Mona Mohammed Abdellatief, Principle investigator
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- 2024
9. Lithium Versus Lamotrigine in Bipolar Disorder, Type II (LiLa-Bipolar)
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Lars Vedel Kessing, professor, MD, DMSc.
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- 2024
10. Fasting Study of Lamotrigine Tablets 25 mg to Lamictal® Tablets 25 mg
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Will Sullvan, Global Head of Product Risk and Safety Management
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- 2024
11. A Pilot Study of Prophylactic Management of Lamotrigine in Pregnant Women
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National Institute on Aging (NIA)
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- 2024
12. Drug Concentrations in Breast Milk and Prediction of Blood Levels of the Breastfed Infants
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St. Justine's Hospital, University of Waterloo, and Shinya Ito, Senior Scientist
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- 2024
13. Precision Medicine in the Treatment of Epilepsy (BDE)
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Gitte Moos Knudsen, professor, MD neurology
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- 2024
14. Low vs. Standard Daily Doses of Antiepileptic Drugs in Newly Diagnosed, Previously Untreated Epilepsy(STANDLOW) (STANDLOW)
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Azienda Ospedaliera San Gerardo di Monza and Ministry of Health, Italy
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- 2024
15. Longitudinal Comparative Effectiveness of Bipolar Disorder Therapies
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Patient-Centered Outcomes Research Institute, Montana State University, National Alliance on Mental Illness Montana, CGStat LLC, Risk Benefit Statistics LLC, National Alliance on Mental Illness New Mexico, National Alliance on Mental Illness Westside Los Angeles, and Christophe Gerard Lambert, Associate Professor
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- 2024
16. Lamotrigine Emerging as a Driver of Stevens-Johnson Syndrome and Toxic Epidermal Necrolysis: An 8-Year Retrospective Study.
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Glahn, Joshua Zev, Almeida, Mariana N., Kochen, Alejandro, Noel, Olivier, Stogner, Viola, Hsia, Henry C., and Savetamal, Alisa
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TOXIC epidermal necrolysis , *OFF-label use (Drugs) , *BURN care units , *LAMOTRIGINE , *MUCOUS membranes , *STEVENS-Johnson Syndrome - Abstract
Stevens-Johnson syndrome (SJS) and toxic epidermal necrolysis (TEN) represent severe manifestations of a potentially life-threatening spectrum defined by a desquamating rash of the skin and mucous membranes. This study was prompted by the observed increase in the off-label use of lamotrigine as a causal agent in SJS/TEN in our regional burn center. A retrospective cohort of 48 patients presenting to the Connecticut Burn Center from 2015–2022 with suspicion for SJS/TEN were reviewed for age, sex, causative drug, presenting symptoms, hospital course, biopsy confirmation, length of stay, comorbidities, and 30-day mortality. Descriptive statistical analysis was conducted to identify trends in causative agent, clinical presentation, and mortality. Thirty patients in our cohort received a final diagnosis of SJS/TEN. While antibiotics remain the most frequent cause of SJS/TEN across the study period (33.3 %, n = 10), the incidence of cases attributable to lamotrigine increased from 1 case between 2015 and 2018 (6.7 %) to 6 cases between 2019 and 2022 (40 %). In 2020 alone, 50 % of all cases were attributable to lamotrigine (n = 4). Of the patients where lamotrigine was implicated, 71.4 % (n = 5) were prescribed lamotrigine for off-label use in the treatment of non-bipolar mood disorders. The average lamotrigine-associated SJS/TEN patient was younger (p < 0.001), had fewer comorbidities, and was more likely to be female than the general SJS/TEN population. Off-label use of lamotrigine is emerging as a major driver of SJS/TEN with notable changes in patient demographics. Further research is necessary to understand how changing trends in the patient population will impact clinical course and optimal management. • Lamotrigine is emerging as an increasing cause of Stevens-Johnson Syndrome (SJS) and Toxic Epidermal Necrolysis (TEN). • Increased lamotrigine prescription for depression and anxiety disorders may account for the changing demographics of SJS/TEN. • Patients with lamotrigine-attributed SJS/TEN tended to be younger, healthier, and female compared to previous SJS/TEN cohorts. • 62 % of patients admitted to the burn unit with concern for SJS/TEN will ultimately receive a corresponding diagnosis. • The observed mortality rate for SJS was 14.3 % as compared to 75 % for TEN. [ABSTRACT FROM AUTHOR]
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- 2024
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17. Amoxicillin and lamotrigine‐induced DRESS syndrome: A case report.
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Demas, Nicholas and Shaikh, Mohammad Baseem
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DRESS syndrome , *LAMOTRIGINE , *CLINICAL pathology , *DRUGS , *PATHOLOGICAL laboratories - Abstract
Key Clinical Message: This case demonstrated with importance of recognizing DRESS syndrome presenting without the typical eosinophilia due to possible cross‐reactivity between amoxicillin and the well‐documented inciting medication lamotrigine. Steroid tapering is an effective treatment, but medication avoidance should be stressed to avoid symptom recurrence. [ABSTRACT FROM AUTHOR]
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- 2024
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18. Lamotrigine vs levetiracetam in female patients of childbearing age with juvenile absence epilepsy: A Bayesian reanalysis.
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Cerulli Irelli, Emanuele, Cocchi, Enrico, Gesche, Joanna, Peña‐Ceballos, Javier, Caraballo, Roberto H., Lattanzi, Simona, Strigaro, Gionata, Orlando, Biagio, Moloney, Patrick B., Catania, Cecilia, Ferlazzo, Edoardo, Pascarella, Angelo, Casciato, Sara, Pizzanelli, Chiara, Milano, Chiara, Giuliano, Loretta, Viola, Veronica, Mostacci, Barbara, Fortunato, Francesco, and Pulitano, Patrizia
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PROPORTIONAL hazards models , *CHILDBEARING age , *MEDICAL research , *IDIOPATHIC diseases , *LAMOTRIGINE - Abstract
Objective: Women of childbearing age with juvenile absence epilepsy (JAE) face treatment challenges due to limited access to safe and effective anti‐seizure medications (ASMs). In a previous study we compared the effectiveness of levetiracetam (LEV) and lamotrigine (LTG) in women with idiopathic generalized epilepsy (IGE), highlighting a superiority of LEV in juvenile myoclonic epilepsy. In this study, we specifically reanalyzed, through a Bayesian approach and by expanding the previously published cohort, the comparative effectiveness of these ASMs as initial monotherapy in JAE. Methods: We conducted a multicenter, retrospective, comparative effectiveness study on women of childbearing age diagnosed with JAE and prescribed LEV or LTG as the initial ASM. Inverse probability treatment weighting (IPTW) Bayesian Cox proportional hazard models were employed to evaluate treatment failure (TF) due to ineffectiveness and ASM retention. The patients' center of provenance and year of prescription were considered as random effect factors. Posterior probabilities and relative log‐risk distribution were computed, and the distribution of posterior draws was analyzed to assess the evidence supporting LTG superiority over LEV. Results: Of 123 patients, those treated with LTG (n = 67) demonstrated lower TF and higher ASM retention than those treated with LEV (n = 56), with the IPTW‐weighted Bayesian Cox proportional hazards model showing a 99.2% posterior probability of LTG being superior on TF and a 99.5% probability on ASM retention. Additional analyses on ≥50% and ≥75% seizure reduction through IPTW‐weighted Bayesian logistic regression largely confirmed these findings, whereas the two ASMs did not show evident differences in terms of seizure freedom. The two ASMs showed comparable safety profiles, with only a minority of patients discontinuing treatment due to side effects. Significance: Bayesian reanalysis supports LTG as first‐line monotherapy for JAE in women of childbearing age, emphasizing the importance of individualized treatment strategies in women with IGE. This study underscores the value of Bayesian methods in refining clinical research and treatment decisions. [ABSTRACT FROM AUTHOR]
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- 2024
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19. Mexiletine versus lamotrigine in non-dystrophic myotonias: a randomised, double-blind, head-to-head, crossover, non-inferiority, phase 3 trial.
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Vivekanandam, Vinojini, Skorupinska, Iwona, Jayaseelan, Dipa L, Matthews, Emma, Barohn, Richard J, McDermott, Michael P, and Hanna, Michael G
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SCHEDULING software , *CLINICAL trials , *LAMOTRIGINE , *ION channels , *PUBLIC hospitals - Abstract
Non-dystrophic myotonias are skeletal muscle channelopathies caused by ion channel dysfunction. Symptom onset is frequently in the first decade of life, causing disability in a young cohort. Although there is no cure, symptomatic treatments exist. Previous trials provide evidence of the efficacy of mexiletine. More recently, lamotrigine has been shown to be effective. Both treatments have different profiles, including pharmacokinetics and adverse events. This trial aimed to investigate whether lamotrigine is non-inferior to mexiletine to directly inform clinical practice. We did a randomised, double-blind, crossover, non-inferiority, phase 3 trial at the National Hospital for Neurology and Neurosurgery (London, UK). Participants (aged ≥18 years) who had genetically confirmed symptomatic non-dystrophic myotonia were randomly assigned (1:1), by means of a block randomisation schedule created by a computer program, to receive either mexiletine for 8 weeks followed by lamotrigine for 8 weeks, or lamotrigine followed by mexiletine, with a 7-day washout period in between. Investigators and participants were masked to treatment allocation. The primary outcome measure was the mean interactive voice response (IVR) diary stiffness score (0–9 scale) over the participant's final 2 weeks of diary reporting in each treatment period. Non-inferiority was assessed using a mixed-effects model with a predefined margin of 0·5 and included all randomly assigned participants who contributed at least 7 days of IVR-diary data in either treatment period. The trial is registered at ClinicalTrials.gov , NCT05017155 , and EudraCT, 2020-003375-17. Between Aug 1, 2021, and Dec 12, 2022, of 60 participants were screened (24 females and 36 males) and randomly assigned between Aug 1, 2021 and Dec 12, 2022, to either the mexiletine–lamotrigine sequence (n=30) or the lamotrigine–mexiletine sequence (n=30). 53 participants contributed data to the primary analysis. The mean IVR stiffness score after treatment with mexiletine was 2·54 (95% CI 1·98 to 3·10) versus 2·77 (2·21 to 3·32) with lamotrigine (mean mexiletine–lamotrigine difference −0·23 [95% CI −0·63 to 0·17]). The most common adverse event with both treatments was indigestion–reflux (eight participants, 208 participant-days receiving mexiletine; seven participants, 130 participant-days receiving lamotrigine). No serious adverse events were reported. We were unable to conclude that lamotrigine is non-inferior to mexiletine; however, improvements in all outcome measures from baseline were similar between lamotrigine and mexiletine. Lamotrigine is an important treatment consideration in non-dystrophic myotonias alongside mexiletine; we propose a treatment algorithm to guide clinical practice. Neuromuscular Study Group, Jon Moulton Charity Trust, UCLH BRC Fast Track Grant. [ABSTRACT FROM AUTHOR]
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- 2024
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20. Pharmacokinetic interaction of quetiapine and lamotrigine – victim and perpetrator?
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Gilleßen, Florian, Gaebler, Arnim Johannes, Haen, Ekkehard, Schoretsanitis, Georgios, Wozniak, Justyna, Stingl, Julia C., and Paulzen, Michael
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DRUG monitoring ,DRUG interactions ,LAMOTRIGINE ,GLUCURONOSYLTRANSFERASE ,QUETIAPINE - Abstract
Objective: We aimed to investigate the ambiguous findings of earlier research regarding the reduction of quetiapine plasma levels when combined with lamotrigine, most likely via UDP-glucuronosyltransferase induction by lamotrigine. Methods: One thousand one hundred and fifty samples, divided into four groups of patients receiving either quetiapine immediate- (IR) or extended-release (XR) without or in combination with lamotrigine were compared regarding absolute and dose-adjusted plasma concentrations. Furthermore, samples of intra-individual controls were analyzed. Results: Patients receiving quetiapine IR in combination with lamotrigine showed 31% lower plasma (p = 0.002) and 23% lower dose-adjusted plasma concentrations (p = 0.004) compared to those receiving IR monotherapy. The proportion of patients with quetiapine plasma concentrations below the lower limit of the therapeutic reference range was 50% and 30% in the combination group and in patients receiving monotherapy, respectively (p = 0.03). However, no significant differences regarding plasma concentration (p = 0.13) and dose-adjusted plasma concentration (p = 0.42) were observed in patients with combination vs. monotherapy with the XR formulation of quetiapine. In the intra-individual controls, no trends could be identified, possibly due to insufficient number of samples (p > 0.05). Conclusions: The combination of quetiapine IR with lamotrigine is associated with significantly lower drug concentrations of quetiapine, potentially impacting quetiapine effectiveness. For quetiapine ER, a significant interaction is less likely. [ABSTRACT FROM AUTHOR]
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- 2024
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21. Breastfed infants exposed to lamotrigine faced a low risk of toxic effects.
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Alvarez, Ingrid, Tötterman, Katarina, Honkaniemi, Emma, Sarman, Ihsan, Bäck, Karin, Forsberg, Lisa, Heinonen, Essi Whaites, and Svedenkrans, Jenny
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POISONS , *LAMOTRIGINE , *BIRTH weight , *GESTATIONAL age , *INFANTS , *ANKYLOGLOSSIA - Abstract
Aim Methods Results Conclusion We aimed to investigate plasma lamotrigine concentrations and clinical effects in infants exposed to lamotrigine through breastfeeding.This was a retrospective study of mother–infant dyads in a clinical follow‐up programme in Stockholm, Sweden. Data were collected from medical records.We included 47 breastfed infants, born from 2011 to 2021, with a median gestational age of 39 + 6 weeks/days and a median birth weight of 3420 g. The median lamotrigine concentration in the infants' plasma was 2.5 (range 2.5–14.0) μmol/L. These concentrations correlated significantly with both the maternal plasma concentrations and the maternal doses (R = 0.79, p < 0.001 versus R = 0.54, p < 0.001). During the follow up, lamotrigine concentrations within the reference range for epilepsy treatment were detected in six (14%) infants and one had clinical symptoms that were probably related to lamotrigine exposure. Liver transaminases were elevated in three of 21 infants. All infants whose mothers had a dose of 150 mg or less had undetectable plasma concentrations and no symptoms during follow up.Infants exposed to lamotrigine through breastfeeding had a low risk of toxic effects. All infants whose mothers had low lamotrigine doses had unmeasurable plasma concentrations and no symptoms of lamotrigine exposure. These low‐risk infants might be offered a simplified follow up. [ABSTRACT FROM AUTHOR]
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- 2024
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22. Stevens-Johnson syndrome/toxic epidermal necrolysis: initial assessment.
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Creamer, Daniel, Lumb, Tatiana, Tibbles, Carrie D., and Haur Yueh Lee
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BLISTERS ,PHYSICAL diagnosis ,OXYGEN saturation ,STEVENS-Johnson Syndrome ,DRUG side effects ,DIFFERENTIAL diagnosis ,TOXIC epidermal necrolysis ,EXANTHEMA ,MUCOUS membranes ,DISEASE management ,FLUID therapy ,AMOXICILLIN ,SEVERITY of illness index ,LAMOTRIGINE ,ANALGESIA ,ALLOPURINOL ,INFLAMMATION ,PATIENTS' attitudes ,HEALTH care teams ,DISEASE complications ,SYMPTOMS - Published
- 2024
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23. Olanzapine vs. magnesium valproate vs. lamotrigine in anti-N-methyl-D-aspartic acid receptor encephalitis: a retrospective study.
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Yan, Yinhua, Yao, Chenxiao, Zhang, Bo, Yang, Zhenyu, Xie, Jiahui, Tang, Miao, Long, Qiong, Tu, Ewen, and Dong, Xuanqi
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MONTREAL Cognitive Assessment , *LAMOTRIGINE , *ANTI-NMDA receptor encephalitis , *OLANZAPINE , *VALPROIC acid , *DRUG therapy - Abstract
Background: This study aimed to compare the impact of olanzapine, magnesium valproate, and lamotrigine as adjunctive treatments for anti-N-methyl-D-aspartate receptor (NMDAR) encephalitis. And it is expected to add supporting points related to the rebalance of neurotransmitters in the brain through adjuvant therapy in the clinical management of anti-NMDAR encephalitis. Methods: This retrospective study included patients diagnosed with anti-NMDAR encephalitis who received standardized immunotherapy at Hunan Brain Hospital between January 2018 and December 2020. Results: Compared to the olanzapine group, both the magnesium valproate and lamotrigine groups showed lower scores on the positive and negative symptom scale (PANSS) total score after 3 weeks of treatment (all P < 0.05). The Montreal Cognitive Assessment Scale (MoCA) scores in the magnesium valproate and lamotrigine groups were significantly higher than in the olanzapine group after 3 weeks and 3 months of treatment (all P < 0.05). After 3 months of treatment, the proportions of patients with a modified Rankin scale score (mRS) of 0–1 in the magnesium valproate and lamotrigine groups were significantly higher than in the olanzapine group (all P < 0.05). The electroencephalogram (EEG) abnormality ranks at 3 months were significantly lower in the magnesium valproate and lamotrigine groups compared with the olanzapine group (all P < 0.05). Furthermore, the Glx/Cr ratio significantly decreased after 3 months of treatment (all P < 0.05) in the magnesium valproate and lamotrigine groups, while the Glx/Cr ratio in the olanzapine group showed no significant change (P > 0.05). Conclusion: Compared with olanzapine, the addition of magnesium valproate or lamotrigine to immunotherapy might be associated with a lower PANSS score, higher MoCA score, and lower mRS score. The improvement of neurological functions and cognitive function may be related to the decreased Glx/Cr ratio. [ABSTRACT FROM AUTHOR]
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- 2024
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24. Retrospective analysis of drug eruptions in 89 cases.
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ZHANG Yali, LI Jun, LIANG Su, WANG Xue, CAO Juanmei, and JIA Xuesong
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Objective To investigate the clinical features of drug eruptions and the most common causative drugs in inpatients in order to provide a reference for the diagnosis and the treatment of drug eruptions. Methods We retrospectively analyzed the clinical data of inpatients with drug eruptions at the First Affiliated Hospital of Shihezi University from April 2019 to December 2023. Results A total of 89 inpatients with drug eruptions, accounting for 2.90% of the total inpatients at the dermatology department during the same period, included 63 cases(70.79%) of mild drug eruptions(mainly the exanthematous eruptions) and 26 cases (29.21%) of severe drug eruptions (mainly SJS). The most common condition using allergenic drugs was infectious diseases (44 cases, 49.44%), while the majority of drug eruptions(63 cases, 70.79%) were caused by single drug. The top 3 allergenic drugs were antibiotics (33.33%), traditional Chinese medicine (26.98%) and antiepileptics (14.29%). The latency time of mild drug eruptions was shorter than that of severe drug eruptions (4.56 ± 6.14 days vs. 9.35 ± 11.33 days, t = 2.03, P = 0.025). High fever at the early stage was observed in 19.05% of patients with mild drug eruptions and 46.15% of patients with severe drug eruptions. The mean times of hospital stay were comparable between patients with mild drug eruptions and severe drug eruptions (9.02 ± 3.58 days). Systemic glucocorticoids were given to 46(51.69%) patients, including 4 cases of severe drug eruptions, two of each treated together with immunoglobulin and tumor necrosis factor (TNF) -α antagonist, respectively. No deaths were found during the follow-up. Conclusions Exanthematous eruption is the most common type of drug eruptions, while the common allergenic drugs are antibiotics, traditional Chinese medicines and antiepileptics. Large portion of patients with drug eruptions, especially severe cases, experience high fever at the early stage. However, hospitalization time does not diifer between patients with severe and mild drug eruptions. Early administration of sufficient glucocorticoids alone or in combination with other therapies can shorten the hospitalization time for severe drug eruptions. [ABSTRACT FROM AUTHOR]
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- 2024
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25. Physiologically based pharmacokinetic models for predicting lamotrigine exposure and dose optimization in pediatric patients receiving combination therapy with carbamazepine or valproic acid.
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Liu, Zhiwei, Shao, Wenxin, Wang, Xingwen, Geng, Kuo, Wang, Wenhui, Li, Yiming, Chen, Youjun, and Xie, Haitang
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VALPROIC acid , *PRESCHOOL children , *CHILD patients , *DRUG interactions , *PEOPLE with epilepsy - Abstract
Introduction: Lamotrigine (LTG) is an antiepileptic drug that has been used in pediatric epilepsy as a combination therapy or monotherapy after stabilization in recent years. However, there are significant drug–drug interactions (DDI) between LTG and combined drugs such as carbamazepine (CBZ) and valproic acid (VPA). It is particularly important to consider the risk of DDI in combination therapy for intractable epilepsy in pediatric patients. Therefore, it is necessary to adjust the dosage of LTG accordingly. The aim of this study was to establish and validate a pediatric physiologically based pharmacokinetic (PBPK) model for predicting LTG exposure. The model is designed to explore the potential for quantifying pharmacokinetic (PK) DDI of LTG when administered concurrently with CBZ or VPA in pediatric patients. Method: Adult and pediatric PBPK models for LTG and VPA were developed using PK‐Sim® software in combination with physiological information and drug‐specific parameters, and a DDI model was developed in combination with the published CBZ model. The models were validated against available PK data. Results: Predictive and observational results in adults, children, and the DDI model were in good agreement. The recommended doses of LTG for preschool children (2–6 years) and school‐aged children (6–12 years) in the absence of drug interactions were 1.47 and 1.2 times higher than those for adults, respectively; 3.1 and 2.6 times higher than those for adults in combination with CBZ; and 0.67 and 0.57 times lower than those for adults in combination with VPA. In addition, plasma exposures in adolescents (12–18 years) were similar to those in adults at the same doses. Conclusion: We have successfully developed PBPK models and DDI models for LTG in adults and children, which provide a reference for rational drug use in the pediatric population. [ABSTRACT FROM AUTHOR]
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- 2024
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26. PBPK Modeling of Lamotrigine and Efavirenz during Pregnancy: Implications for Personalized Dosing and Drug-Drug Interaction Management.
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Costa, Bárbara, Gouveia, Maria João, and Vale, Nuno
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PREGNANT women , *DRUG interactions , *GENETIC polymorphisms , *LAMOTRIGINE , *PREDICTION models - Abstract
This study aimed to model the pharmacokinetics of lamotrigine (LTG) and efavirenz (EFV) in pregnant women using physiologically based pharmacokinetic (PBPK) and pregnancy-specific PBPK (p-PBPK) models. For lamotrigine, the adult PBPK model demonstrated accurate predictions for pharmacokinetic parameters. Predictions for the area under the curve (AUC) and peak plasma concentration (Cmax) generally agreed well with observed values. During pregnancy, the PBPK model accurately predicted AUC and Cmax with a prediction error (%PE) of less than 25%. The evaluation of the EFV PBPK model revealed mixed results. While the model accurately predicted certain parameters for non-pregnant adults, significant discrepancies were observed in predictions for higher doses (600 vs. 400 mg) and pregnant individuals. The model's performance during pregnancy was poor, indicating the need for further refinement to account for genetic polymorphism. Gender differences also influenced EFV pharmacokinetics, with lower exposure levels in females compared to males. These findings highlight the complexity of modeling EFV, in general, but specifically in pregnant populations, and the importance of validating such models for accurate clinical application. The study highlights the importance of tailoring dosing regimens for pregnant individuals to ensure both safety and efficacy, particularly when using combination therapies with UGT substrate drugs. Although drug-drug interactions between LTG and EFV appear minimal, further research is needed to improve predictive models and enhance their accuracy. [ABSTRACT FROM AUTHOR]
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- 2024
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27. Development of a UPLC-MS/MS Method to Simultaneously Measure 13 Antiepileptic Drugs with Deuterated Internal Standards.
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Jae Hyun Cha, Hyebin Choi, Jisook Yim, Keun Ju Kim, Minjeong Nam, Myung Hyun Nam, Chang Kyu Lee, Dae Won Kim, Yunjung Cho, and Seung Gyu Yun
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ANTICONVULSANTS ,CARBAMAZEPINE ,PERAMPANEL ,DRUG monitoring ,TOPIRAMATE ,PREGABALIN ,LEVETIRACETAM - Abstract
Background: The goal of this study was to develop and validate a UPLC-MS/MS method for simultaneous measurement of 13 AEDs, including carbamazepine, oxcarbazepine, lamotrigine, levetiracetam, topiramate, primidone, zonisamide, gabapentin, lacosamide, perampanel, pregabalin, rufinamide, and vigabatrin, in whole blood samples. Methods: A UPLC-MS/MS method for simultaneous determination of 13 AEDs in whole blood was developed, and validation was conducted for accuracy, precision, limit of quantification (LOQ), matrix effect, and stability. Our method was compared to two different hospitals using UPLC-MS/MS. Results: All AEDs exhibited linearity across the AMR (analytical measurement range), with R² values ranging from 0.994 to 1.000. The imprecision and inaccuracy for low and high quality control (QC) levels were within an acceptable range, with the coefficient of variation (CV) < 15%. The LOQ was 0.62 μg/mL for carbamazepine, 1.61 μg/mL for oxcarbazepine, 1.30 μg/mL for lamotrigine, 13.20 μg/mL for levetiracetam, 1.26 μg/mL for topiramate, 1.01 μg/mL for primidone, 1.59 μg/mL for zonisamide, 1.09 μg/mL for lacosamide, 1.61 μg/mL for gabapentin, 0.50 μg/mL for pregabalin, 0.07 ng/mL for perampanel, 3.00 μg/mL for rufinamide, and 2.06 μg/mL for vigabatrin. All AEDs demonstrated acceptable assay parameters for carryover, stability, and matrix effects. Moreover, the assay showed satisfactory results compared to two different hospitals with a bias of less than 15%. Conclusions: We successfully developed and validated a fast and robust UPLC-MS/MS method for routine therapeutic drug monitoring of thirteen antiepileptic drugs simultaneously. [ABSTRACT FROM AUTHOR]
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- 2024
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28. What Is the Best First-Line Treatment for Young Women with Generalized Epilepsy?
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HETEROCYCLIC compounds , *WOMEN , *TREATMENT effectiveness , *LAMOTRIGINE , *EPILEPSY , *VALPROIC acid , *SEIZURES (Medicine) , *DRUG development , *ANTICONVULSANTS - Abstract
The article discusses a study comparing the effectiveness of levetiracetam and lamotrigine as first-line treatments for idiopathic generalized epilepsy (IGE) in women of childbearing age. Topics discussed include the teratogenic risks of valproate, the comparison of seizure control between levetiracetam and lamotrigine, and the study's focus on juvenile myoclonic epilepsy.
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- 2024
29. Single-dose, Two-way Crossover Bioequivalence of Lamotrigine in Healthy Male Volunteers Under Fasting Conditions
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BioPharma Services, Inc
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- 2023
30. UGT2B10 is the Major UDP-Glucuronosyltransferase 2B Isoform Involved in the Metabolism of Lamotrigine and is Implicated in the Drug-Drug Interaction with Valproic Acid.
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Tang, Lloyd Wei Tat, Lapham, Kimberly, and Goosen, Theunis C.
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Lamotrigine is a phenyltriazine anticonvulsant that is primarily metabolized by phase II UDP-glucuronosyltransferases (UGT) to a quaternary N2-glucuronide, which accounts for ~ 90% of the excreted dose in humans. While there is consensus that UGT1A4 plays a predominant role in the formation of the N2-glucuronide, there is compelling evidence in the literature to suggest that the metabolism of lamotrigine is catalyzed by another UGT isoform. However, the exact identity of the UGT isoform that contribute to the formation of this glucuronide remains uncertain. In this study, we harnessed a robust reaction phenotyping strategy to delineate the identities and its associated fraction metabolized (f
m ) of the UGTs involved in lamotrigine N2-glucuronidation. Foremost, human recombinant UGT mapping experiments revealed that the N2-glucuronide is catalyzed by multiple UGT isoforms. (i.e., UGT1A1, 1A3, 1A4, 1A9, 2B4, 2B7, and 2B10). Thereafter, scaling the apparent intrinsic clearances obtained from the enzyme kinetic experiments with our in-house liver-derived relative expression factors (REF) and relative activity factors (RAF) revealed that, in addition to UGT1A4, UGT2B10 was involved in the N2-glucuronidation of lamotrigine. This was further confirmed via chemical inhibition in human liver microsomes with the UGT1A4-selective inhibitor hecogenin and the UGT2B10-selective inhibitor desloratadine. By integrating various orthogonal approaches (i.e., REF- and RAF-scaling, and chemical inhibition), we quantitatively determined that the fm for UGT1A4 and UGT2B10 ranged from 0.42 – 0.64 and 0.32 – 0.57, respectively. Finally, we also provided nascent evidence that the pharmacokinetic interaction between lamotrigine and valproic acid likely arose from the in vivo inhibition of its UGT2B10-mediated pathway. [ABSTRACT FROM AUTHOR]- Published
- 2024
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31. Development of an HPLC method using relative molar sensitivity for the measurement of blood concentrations of nine pharmaceutical compounds
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Takashi Ohtsuki, Yi Huang, Ayane Kamiya, Yuki Nakayama, Miyuki Matsushita, Satoru Morikawa, and Hiroshi Matsufuji
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Relative molar sensitivity ,HPLC ,Carbamazepine ,Phenytoin ,Voriconazole ,Lamotrigine ,Therapeutics. Pharmacology ,RM1-950 ,Pharmacy and materia medica ,RS1-441 - Abstract
Abstract We developed a reliable high-performance liquid chromatographic analysis method using a relative molar sensitivity (RMS) technique that does not require an authentic, identical reference analyte material to quantify blood serum carbamazepine, phenytoin, voriconazole, lamotrigine, meropenem, mycophenolic acid, linezolid, vancomycin, and caffeine levels for routine blood concentration measurements. Carbamazepine and caffeine were also used as non-analyte reference materials to calculate the RMS of each analyte. The RMS was calculated from the ratio of the slope of the calibration equation (analyte/non-analyte reference material), then used to quantify analytes in control serum samples spiked with carbamazepine, phenytoin, voriconazole, meropenem, mycophenolic acid, linezolid or vancomycin. In addition, the concentrations of these six drugs in control serum samples determined by the proposed RMS method agreed well with that obtained using a conventional method. The proposed RMS method is a promising tool for the clinical determination of nine drugs, given the accuracy, precision, and efficiency of quantifying these analytes.
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- 2024
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32. Effects of co‐administration of lamotrigine on valproate transfer across the placenta and its brain entry in developing Genetic Absence Epilepsy Rats from Strasbourg (GAERS).
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Qiu, Fiona, Huang, Yifan, Dziegielewska, Katarzyna M., Habgood, Mark D., and Saunders, Norman R.
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FETAL development , *VALPROIC acid , *LAMOTRIGINE , *BLOOD proteins , *CEREBROSPINAL fluid , *FETAL brain - Abstract
During development, embryos and foetuses may be exposed to maternally ingested antiseizure medications (ASM), valproate and lamotrigine, essential in some patients to control their epilepsy symptoms. Often, the two drugs are co‐administered to reduce required doses of valproate, a known potential teratogen. This study used Genetic Absence Epilepsy Rat from Strasbourg to evaluate transfer of valproate and lamotrigine across late gestation placenta and their entry into cerebrospinal fluid (CSF) and brain of developing rats, in mono‐ and combination therapies. Animals at embryonic day (E) 19, postnatal day (P) 0, 4 and 21, and adults were administered valproate (30 mg/kg) or lamotrigine (6 mg/kg) with their respective [3H]‐tracers, either alone or in combination. In chronic experiments, females consumed valproate‐containing diet from 2 weeks prior to mating until offspring were used at E19 and P0. Drugs were injected 30 min before blood, CSF and brain samples were collected from terminally anaesthetised animals. Radioactivity in samples was measured. In acute monotherapy brain entry of valproate was higher in foetal than postnatal animals, correlating with its plasma protein binding. Brain entry of lamotrigine was not age‐dependent. Combination therapy enhanced entry of lamotrigine into the adult brain but had no effects on brain and CSF entry of valproate. Following chronic valproate exposure, placental transfer of valproate decreased in combination therapy; however, foetal brain entry increased. Results suggest that during pregnancy, the use of combination therapy of valproate and lamotrigine may mitigate overall foetal exposure to valproate but potential risks to foetal brain development are less clear. [ABSTRACT FROM AUTHOR]
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- 2024
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33. SCN8A self‐limited infantile epilepsy: Does epilepsy resolve?
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Young, Emma, Harris, Rebekah, Lieffering, Nico, de Valles‐Ibáñez, Guillem, Nyaga, Denis, Bennett, Mark F., Hildebrand, Michael S., Scheffer, Ingrid E., and Sadleir, Lynette G.
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PARTIAL epilepsy , *SEIZURES (Medicine) , *LAMOTRIGINE , *BRAIN diseases , *PEOPLE with epilepsy , *EPILEPSY - Abstract
SCN8A variants cause a spectrum of epilepsy phenotypes ranging from self‐limited infantile epilepsy (SeLIE) to developmental and epileptic encephalopathy. SeLIE is an infantile onset focal epilepsy, occurring in developmentally normal infants, which often resolves by 3 years. Our aim was to ascertain when epilepsy resolves in SCN8A‐SeLIE. We identified unpublished individuals with SCN8A‐SeLIE and performed detailed phenotyping. Literature was searched for published SCN8A‐SeLIE cases. Nine unpublished individuals from four families were identified (age at study = 3.5–66 years). Six had their last seizure after 3 years (range = 4–21 years); although drug‐responsive and despite multiple weaning attempts (1–5), five of six remain on antiseizure medications (carbamazepine, n = 3; lamotrigine, n = 2). We identified 29 published individuals with SCN8A‐SeLIE who had data on seizure progression. Of the 22 individuals aged at least 10 years, reported here or in the literature, nine of 22 (41%) had seizure offset prior to 3 years, five of 22 (23%) had seizure offset between 3 and 10 years, and eight of 22 (36%) had seizures after 10 years. Our data highlight that more than half of individuals with SCN8A‐SeLIE continue to have seizures into late childhood. In contrast to SeLIE due to other etiologies, many individuals have a more persistent, albeit drug‐responsive, form of epilepsy. [ABSTRACT FROM AUTHOR]
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- 2024
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34. The efficacy of lamotrigine in bipolar disorder: A systematic review and meta‐analysis.
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Haenen, N., Kamperman, A. M., Prodan, A., Nolen, W. A., Boks, M. P., and Wesseloo, R.
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LAMOTRIGINE , *RANDOMIZED controlled trials , *BIPOLAR disorder , *HOSPITAL admission & discharge , *COMPARATOR circuits - Abstract
Objective: To provide up‐to‐date clinical guidance on the efficacy of lamotrigine in bipolar disorder (BD). Methods: Eligible studies were identified during a systematic literature search according to PRISMA‐guidelines. We included randomized controlled trials (RCTs) and cohort studies that quantitatively assessed lamotrigine's efficacy in BD. We divided the included studies into three groups: 1. acute treatment of depression, 2. acute treatment of mania and hypomania, and 3. maintenance treatment. Analyses were stratified by control group (placebo vs active comparator) and treatment strategy (monotherapy vs add‐on treatment). Results: We included 20 RCTs (n = 1166 lamotrigine users) and 20 cohort studies (n = 11,141 lamotrigine users). Twenty‐four of these studies were included in meta‐analyses. During depressive episodes, greater decreases in depressive symptomatology were associated with initiation of lamotrigine as add‐on treatment than with placebo (SMD −0.30 [95% CI = −0.51, −0.10], df = 3, p = 0.004). Decreases in depressive symptomatology did not differ significantly between lamotrigine and the active comparator (SMD −0.28 [95% CI = −1.06, 0.50], df = 3, p = 0.488). As a maintenance treatment, lamotrigine was associated with a significantly lower relapse/recurrence rate than placebo (risk ratio (RR) 0.84 [95% CI = 0.71, 0.99], df = 2, p = 0.037). Relapse/recurrence rates did not differ significantly between lamotrigine and lithium (RR 1.06 [95% CI = 0.89, 1.25], df = 2, p = 0.513). A qualitative assessment of high‐quality register‐based studies found that lamotrigine was associated with lower hospital admission rates than other commonly used treatment regimes. Conclusions: There is substantial evidence for the efficacy of lamotrigine in BD, specifically as add‐on treatment during acute depressive episodes and as maintenance treatment for preventing relapse and recurrence. [ABSTRACT FROM AUTHOR]
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- 2024
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35. A toxikus epidermalis necrolysis szemészeti vonatkozásai.
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Killik, Petra, Kostyál, Erika, Tóth, Gábor, Szentmáry, Nóra, Nagy, Zoltán Zsolt, and Maneschg, Otto Alexander
- Abstract
Copyright of Hungarian Medical Journal / Orvosi Hetilap is the property of Akademiai Kiado 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.)
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- 2024
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36. An update on pharmacotherapy for trigeminal neuralgia.
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Pergolizzi Jr, Joseph V., LeQuang, Jo Ann, El-Tallawy, Salah N., Wagner, Morgan, Ahmed, Rania S., and Varrassi, Giustino
- Abstract
Trigeminal neuralgia is a rare condition that can be effectively treated by carbamazepine or oxcarbazepine but these older drugs are associated with dose-dependent and potentially treatment-limiting adverse effects. Third-generation anticonvulsants, new calcitonin gene-related peptide blockers for migraine, and older drugs such as ketamine and cannabinoids may be promising adjuvants or monotherapeutic options. The new drugs, their presumed mechanisms of action, safety and efficacy are discussed herein. There is a paucity of robust clinical evidence in support of these drugs for trigeminal neuralgia. New migraine agents are considered as well although migraines and trigeminal neuralgia are distinct, albeit similar, conditions. No new drugs have been released to market in recent years with the specific indication of trigeminal neuralgia. In real-world clinical practice, about half of trigeminal neuralgia patients take more than one agent for prevention and combination therapy may be the optimal approach. Combination therapy might allow for lower doses of carbamazepine or oxcarbazepine, thus reducing the number and severity of potential adverse events but the potential for pharmacokinetic drug-drug interactions must be considered. Drug therapy for trigeminal neuralgia involves acute or abortive treatments, often administered in hospital versus long-term preventive therapy, usually involving oral agents. Trigeminal neuralgia is a relatively rare condition that usually affects one side of the face below the eye around the cheekbone. The cause of trigeminal neuralgia is sometimes a damaged nerve or a nerve that has lost part of its outer protective sheath (myelin). However, trigeminal neuralgia may have other neurological causes as well. Pain can be triggered by touch, pressure, or chewing and it tends to occur in very painful brief attacks followed by pauses with little or no pain. There are two types of drug treatment for trigeminal neuralgia: drugs to stop an ongoing attack (which are often administered in an emergency room or hospital intravenously) and drugs that are taken orally over the long term to reduce or prevent attacks. The two most effective drugs for trigeminal neuralgia are carbamazepine and oxcarbazepine, which are actually drugs to prevent seizures. They are effective in reducing the pain intensity and number of attacks of trigeminal neuralgia but they have side effects. In fact, these side effects can be so severe that people stop taking the drugs. Many new drugs have come to market recently that may work for trigeminal neuralgia, although none was specifically developed for this use. The newest generation of anti-seizure medications including eslicarbazepine, lacosamide, levetiracetam, and retigabine, may be just as effective as the older carbamazepine and oxcarbazepine drugs with fewer side effects. Clinical studies are needed to test them in trigeminal neuralgia patients but their mechanisms of action suggest that they might work well. There are some new drugs developed for migraine headache that inhibit a substance in the body called CGRP. Migraine headaches and trigeminal neuralgia have some of the same symptoms but they are different conditions but both involve too much CGRP. Other new drugs include lasmiditan, pimozide (used for Tourette syndrome), tizanidine (muscle relaxant), lamotrigine and vixotrigine (anti-seizure drugs) may also be beneficial. It may be that people with trigeminal neuralgia will have to take combination therapy, the use of two or more drugs with different mechanisms of action. Older drugs like ketamine and cannabinoids are also being considered as possible add-on agents for therapy for trigeminal neuralgia. [ABSTRACT FROM AUTHOR]
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- 2024
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37. Development of an HPLC method using relative molar sensitivity for the measurement of blood concentrations of nine pharmaceutical compounds.
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Ohtsuki, Takashi, Huang, Yi, Kamiya, Ayane, Nakayama, Yuki, Matsushita, Miyuki, Morikawa, Satoru, and Matsufuji, Hiroshi
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MEROPENEM ,CAFFEINE ,VORICONAZOLE ,MYCOPHENOLIC acid ,HIGH performance liquid chromatography ,CHROMATOGRAPHIC analysis ,PHENYTOIN ,SERUM - Abstract
We developed a reliable high-performance liquid chromatographic analysis method using a relative molar sensitivity (RMS) technique that does not require an authentic, identical reference analyte material to quantify blood serum carbamazepine, phenytoin, voriconazole, lamotrigine, meropenem, mycophenolic acid, linezolid, vancomycin, and caffeine levels for routine blood concentration measurements. Carbamazepine and caffeine were also used as non-analyte reference materials to calculate the RMS of each analyte. The RMS was calculated from the ratio of the slope of the calibration equation (analyte/non-analyte reference material), then used to quantify analytes in control serum samples spiked with carbamazepine, phenytoin, voriconazole, meropenem, mycophenolic acid, linezolid or vancomycin. In addition, the concentrations of these six drugs in control serum samples determined by the proposed RMS method agreed well with that obtained using a conventional method. The proposed RMS method is a promising tool for the clinical determination of nine drugs, given the accuracy, precision, and efficiency of quantifying these analytes. [ABSTRACT FROM AUTHOR]
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- 2024
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38. Lithium versus anticonvulsants and the risk of physical disorders – Results from a comprehensive long-term nation-wide population-based study emulating a target trial.
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Kessing, Lars Vedel, Knudsen, Mark Bech, Rytgaard, Helene Charlotte Wiese, Torp-Pedersen, Christian, and Berk, Michael
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ANTICONVULSANTS , *LITHIUM carbonate , *PARKINSON'S disease , *CHRONIC kidney failure , *MYOCARDIAL infarction , *EMPAGLIFLOZIN , *PHENOBARBITAL - Abstract
Bipolar disorder is associated with increased rates of many physical disorders, but the effects of medication are unclear. We systematically investigated the associations between sustained use of first line maintenance agents, lithium versus lamotrigine and valproate, and the risk of physical disorders using a nation-wide population-based target trial emulation covering the entire 5.9 million inhabitants in Denmark. We identified two cohorts. Cohort 1: patients with a diagnosis of bipolar disorder prior to first purchase (N = 12.607). Cohort 2: all 156.678 adult patients who had their first ever purchase (since 1995) of either lithium, lamotrigine or valproate between 1997 and 2021 regardless of diagnosis. Main analyses investigated the effect of sustained exposure defined as exposure for all consecutive 6-months periods during a 10-year follow-up. Outcomes included a diagnosis of incident stroke, arteriosclerosis, angina pectoris, myocardial infarction, diabetes mellitus, myxedema, osteoporosis, dementia, Parkinson's disease, chronic kidney disease and cancer (including subtypes). In both Cohorts 1 and 2, there were no systematic statistically significant differences in associations between sustained use of lithium versus lamotrigine and valproate, respectively, and any physical disorder, including subtypes of disorders, except myxedema, for which exposure to lithium increased the absolute risk of myxedema with 7–10 % compared with lamotrigine or valproate. In conclusion, these analyses emulating a target trial of "real world" observational register-based data show that lithium does not increase the risk of developing any kind of physical disorders, except myxedema, which may be a result of detection bias. [ABSTRACT FROM AUTHOR]
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- 2024
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39. The use of psychotropic medication in the perinatal period.
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Petrosellini, Chiara, McAlpine, Lynsey, Protti, Olivia, and Siassakos, Dimitrios
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MENTAL illness drug therapy , *THERAPEUTIC use of lithium , *DRUG-induced abnormalities , *BREASTFEEDING , *MENTAL health , *PATIENT safety , *INFANT development , *SEROTONIN uptake inhibitors , *PREGNANCY outcomes , *ANTIDEPRESSANTS , *LAMOTRIGINE , *NORADRENALINE , *VALPROIC acid , *CARBAMAZEPINE , *H2 receptor antagonists , *PSYCHIATRIC drugs , *PERINATAL period - Abstract
Key content: The perinatal period confers an elevated risk of both relapses and new onset of mental illness. Suboptimal treatment can have a profound impact on maternal mortality and morbidity, neonatal outcomes and longer term child development.Most psychotropic medication can be used safely in pregnancy, with some notable exceptions.While decisions on the use of psychotropic medications in pregnancy are often complex and should be multidisciplinary, it is imperative that obstetricians and gynaecologists familiarise themselves with current literature to provide evidence‐based counselling and care.Existing guidelines on the use of psychotropic medication are largely aimed at psychiatrists, and to date there has been a lack of concise, digestible information with a focus on core knowledge for obstetricians and gynaecologists.We summarise existing evidence on the use of antidepressants, antipsychotics, mood stabilisers and sedatives in the perinatal period. For each drug class we describe the teratogenicity, impact on pregnancy, breastfeeding and the newborn. Learning objectives: To be familiar with common psychotropic medication used in pregnancy and the postpartum period.To understand key evidence on the safety profile of psychiatric medication in the perinatal period and apply this to individualised counselling. [ABSTRACT FROM AUTHOR]
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- 2024
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40. Higher autism risk with valproate than topiramate, lamotrigine.
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AUTISM risk factors , *TOPIRAMATE , *PRENATAL exposure delayed effects , *NEURAL development , *LAMOTRIGINE , *VALPROIC acid , *PREGNANCY - Abstract
A cohort study examining both publicly and commercially insured individuals has found that prenatal exposure to topiramate or lamotrigine is associated with lower risk of childhood autism compared with exposure to valproate. Study results were largely unchanged in analyses limited to women who received the medications late in pregnancy. Results were published March 21/28, 2024, in The New England Journal of Medicine. [ABSTRACT FROM AUTHOR]
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- 2024
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41. Harnessing the power of natural alkaloids: the emergent role in epilepsy therapy.
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Siyu Li, Xinyu Lin, and Lijuan Duan
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EPILEPSY ,METHYL aspartate receptors ,BLOOD-brain barrier ,LAMOTRIGINE ,NANOPARTICLES ,ISOQUINOLINE alkaloids ,INDOLE - Abstract
The quest for effective epilepsy treatments has spotlighted natural alkaloids due to their broad neuropharmacological effects. This review provides a comprehensive analysis of the antiseizure properties of various natural compounds, with an emphasis on their mechanisms of action and potential therapeutic benefits. Our findings reveal that bioactive substances such as indole, quinoline, terpenoid, and pyridine alkaloids confer medicinal benefits by modulating synaptic interactions, restoring neuronal balance, and mitigating neuroinflammation--key factors in managing epileptic seizures. Notably, these compounds enhance GABAergic neurotransmission, diminish excitatory glutamatergic activities, particularly at NMDA receptors, and suppress proinflammatory pathways. A significant focus is placed on the strategic use of nanoparticle delivery systems to improve the solubility, stability, and bioavailability of these alkaloids, which helps overcome the challenges associated with crossing the blood-brain barrier (BBB). The review concludes with a prospective outlook on integrating these bioactive substances into epilepsy treatment regimes, advocating for extensive research to confirm their efficacy and safety. Advancing the bioavailability of alkaloids and rigorously assessing their toxicological profiles are essential to fully leverage the therapeutic potential of these compounds in clinical settings. [ABSTRACT FROM AUTHOR]
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- 2024
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42. THERAPEUTIC DRUG MONITORING OF NEW-GENERATION ANTIEPILEPTICS IN PEDIATRIC PATIENTS: A FOCUS ON FACTORS INFLUENCING THE PLASMA CONCENTRATION.
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Damnjanović, Ivana, Stefanović, Nikola, Tošić, Tatjana, Catić-Djordjević, Aleksandra, Kundalić, Ana, Živanović, Slavoljub, and Veličković-Radovanović, Radmila
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DRUG monitoring , *CHILD patients , *VALPROIC acid , *LAMOTRIGINE , *ANTICONVULSANTS , *EPILEPSY - Abstract
Monitoring the concentrations of antiepileptic drugs (AEDs) in the pediatric population represents an important step in the vast variety of decisions related to the optimization of new-generation epilepsy therapy. The primary objective of this research was to determine the concentrations of lamotrigine (LTG) and levitiracetam (LEV) in the plasma of children and adolescents receiving combined antiepileptic therapy. Secondly, we examined the influence of demographic factors and co-therapy on the measured concentrations of AEDs. The prospective study included 71 subjects diagnosed with epilepsy, aged 2-18 years, receiving combined antiepileptic therapy, which included the following therapeutic regimens/modalities: valproic acid (VA)/LTG, VA/LEV and LTG/LEV. The results indicated that 86.27% of LTG concentrations and 68.97% of LEV concentrations were within the reference range. No statistically significant influence of comedication on the concentrations of the tested AEDs was recorded. Additionally, the obtained results confirmed that LTG dose was the most significant predictor for LTG concentrations. The results of the conducted research indicated that only LEV dose corrected by body weight could potentially affect LEV concentrations. Although the therapeutic monitoring of new-generation AEDs is not commonly imposed in daily clinical practice, the results of the conducted research indicate that monitoring the concentrations of LTG and LEV can be of great benefit in the pediatric population receiving combined antiepileptic therapy due to the very nature of the disease and the potential pharmacokinetic variability of the investigated antiepileptics. [ABSTRACT FROM AUTHOR]
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- 2024
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43. Dose-dependent effect of lamotrigine on quetiapine serum concentration in patients using instant release tablets.
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Hole, Kristine, Lorentsen, Silje K, Nordby, Karoline L, Slettvik, Marie, Sørum, Ida TG, Molden, Espen, and Haslemo, Tore
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COMBINATION drug therapy , *BIPOLAR disorder , *T-test (Statistics) , *RESEARCH funding , *RETROSPECTIVE studies , *DESCRIPTIVE statistics , *LAMOTRIGINE , *DRUG monitoring , *DRUG interactions , *ANALYSIS of variance , *COMPARATIVE studies , *QUETIAPINE , *DRUG dosage , *DRUG administration ,DRUG therapy for schizophrenia - Abstract
Purpose: Lamotrigine was previously reported to reduce serum concentration of quetiapine. The aim of this study was to investigate whether lamotrigine dose or quetiapine formulation was of importance for the drug interaction. Methods: Patients combining lamotrigine with quetiapine (cases) were included retrospectively from a routine therapeutic drug monitoring (TDM) service, as were a control group of patients using quetiapine without any interacting drugs. The case and control groups were divided into groups using immediate release (IR) and extended release (XR) quetiapine. The case group was further split into high-dose (> 200 mg/day) and low-dose (≤ 200 mg/day) lamotrigine users. Quetiapine concentration-to-dose (C/D) ratio and metabolite-to-parent ratio (MPR) were compared between the control group and dose-separated case groups using ANOVA test and t-tests. Results: In total, 406 patients were included. The mean C/D ratio of IR quetiapine was 46% lower in the high-dose lamotrigine group compared with the control group (P < 0.001), while no interaction effect was present in the low dose lamotrigine group (P = 0.7). Regardless of lamotrigine dose, there was no difference in quetiapine C/D ratio for patients using the XR formulation (P = 0.4). The quetiapine MPR was unaffected regardless of formulation and lamotrigine dose (P ≥ 0.06). Conclusion: The effect of lamotrigine in reducing quetiapine concentration is only significant for patients using quetiapine IR tablets who are treated with lamotrigine doses > 200 mg/day. Because of high variability in the interaction effect, TDM of quetiapine should be recommended during co-prescription of high-dose lamotrigine. [ABSTRACT FROM AUTHOR]
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- 2024
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44. Sexual dysfunction and commonly used drugs in neurology.
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Behn, Maya, Kielhofner, Jane, Panicker, Jalesh N., and Kaplan, Tamara B.
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CAFFEINE , *SEXUAL excitement , *ORGASM , *SEROTONIN uptake inhibitors , *LIBIDO , *CURARE-like agents , *NEUROLOGICAL disorders , *ANTIDEPRESSANTS , *PHENYTOIN , *LAMOTRIGINE , *QUALITY of life , *IMPOTENCE , *CARBAMAZEPINE , *ANTICONVULSANTS - Abstract
Sexual dysfunction is common in men and women with neurological diseases. Medications used in neurology can cause sexual dysfunction independently of the disease process and this may adversely affect patients' quality of life. This review focuses on medications commonly prescribed to neurological patients that may contribute to altered sexual function, and discusses how they may differ in men and women. [ABSTRACT FROM AUTHOR]
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- 2024
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45. Physiologically Based Pharmacokinetic Modelling of UGT Substrate Drugs Lamotrigine and Raltegravir during Pregnancy.
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Berezowska, Monika, Coppola, Paola, Pilla Reddy, Venkatesh, and Sharma, Pradeep
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PHARMACOKINETICS , *LAMOTRIGINE , *RALTEGRAVIR , *PREGNANCY , *ENZYMATIC analysis - Abstract
Pregnancy is associated with various physiological changes that can significantly impact the disposition of drugs. To further the insight into how pregnancy affects the pharmacokinetics of drugs at different stages, clinical studies can be simulated using Physiologically Based Pharmacokinetic modelling. PBPK modelling of drugs metabolised by Phase I enzymes (CYPs) in pregnant population models had been reported in the past, while its use in Phase II (UGTs) is not known. In this study, based on the results of a recent meta-analysis, lamotrigine (UGT1A4) and raltegravir (UGT1A1) were selected as candidate drugs, and pregnancy-specific models were developed for both using the Simcyp v.21 simulator. A middle-out strategy was used where previously published drug parameters were adapted from a minimal to a full PBPK model to allow their application for the pregnancy population models using Simcyp PBPK software. Adapted models were successfully validated against observed clinical data both qualitatively (visual overlay of plasma concentrations on graphs) and quantitatively (calculating the predicted/observed ratios for AUC, Cmax and CL as well as statistical analysis using model prediction power metrics). They were then applied to predict the PKs of both drugs in pregnancy population models. The temporal changes in maternal enzymatic activities during gestation were modelled based on in vitro data reported in literature and default relationships encoded in the Simcyp platform for UGT1A1 and UGT1A4, respectively. Our study demonstrates the successful development and validation of a PBPK model for LTG and RTG in pregnancy population models. Future work with additional UGT1A4 substrate drugs using the proposed changes in UGT1A4 activity may enable validating the pregnancy population model and its subsequent use for the prospective prediction of PK. [ABSTRACT FROM AUTHOR]
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- 2024
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46. Chemical Behavior and Bioactive Properties of Spinorphin Conjugated to 5,5′-Dimethyl- and 5,5′-Diphenylhydantoin Analogs.
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Georgieva, Stela, Todorov, Petar, Tchekalarova, Jana, Subaer, Subaer, Peneva, Petia, Chakarov, Kalin, Hartati, Hartati, and Faika, Sitti
- Subjects
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PHENOBARBITAL , *FOURIER transform infrared spectroscopy , *PEPTIDES , *PEPTIDE derivatives , *CIRCULAR dichroism , *LAMOTRIGINE - Abstract
The discovery of new peptides and their derivatives is an outcome of ongoing efforts to identify a peptide with significant biological activity for effective usage as a possible therapeutic agent. Spinorphin peptides have been documented to exhibit numerous applications and features. In this study, biologically active peptide derivatives based on novel peptide analogues of spinorphin conjugated with 5,5′-dimethyl (Dm) and 5,5′-diphenyl (Ph) hydantoin derivatives have been successfully synthesized and characterized. Scanning electron microscopy (SEM) and spectral methods such as UV-Vis, FT-IR (Fourier Transform Infrared Spectroscopy), CD (Circular Dichroism), and fluorimetry were used to characterize the microstructure of the resulting compounds. The results revealed changes in peptide morphology as a result of the restructuring of the aminoacidic sequences and aromatic bonds, which is related to the formation of intermolecular hydrogen bonds between tyrosyl groups and the hydantoin moiety. Electrochemical and fluorescence approaches were used to determine some physicochemical parameters related to the biological behavior of the compounds. The biological properties of the spinorphin derivatives were evaluated in vivo for anticonvulsant activity against the psychomotor seizures at different doses of the studied peptides. Both spinorphin analog peptides with Ph and Dm groups showed activity against all three phases of the seizure in the intravenous Pentylenetetrazole Seizure (ivPTZ) test. This suggests that hydantoin residues do not play a crucial role in the structure of spinorphin compounds and in determining the potency to raise the seizure threshold. On the other hand, analogs with a phenytoin residue are active against the drug-resistant epilepsy test (6-Hz test). In addition, bioactivity analyses revealed that the new peptide analogues have the potential to be used as antimicrobial and antioxidant compounds. These findings suggest promising avenues for further research that may lead to the development of alternative medicines or applications in various fields beyond epilepsy treatment. [ABSTRACT FROM AUTHOR]
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- 2024
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47. Stevens–Johnson Syndrome and Toxic Epidermal Necrolysis: Analysis of the Russian Database of Spontaneous Reports.
- Author
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Zyryanov, Sergey, Asetskaya, Irina, Butranova, Olga, Terekhina, Elizaveta, Polivanov, Vitaly, Yudin, Alexander, and Samsonova, Kristina
- Subjects
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TOXIC epidermal necrolysis , *DRUG side effects , *STEVENS-Johnson Syndrome , *AZITHROMYCIN , *DOPING in sports , *DATABASES , *CARBAMAZEPINE , *VALPROIC acid , *LACTAMS - Abstract
(1) Background: Stevens–Johnson syndrome (SJS) and toxic epidermal necrolysis (TEN) are extremely severe cutaneous adverse drug reactions which are relatively rare in routine clinical practice. An analysis of a national pharmacovigilance database may be the most effective method of obtaining information on SJS and TEN. (2) Methods: Design—a retrospective descriptive pharmacoepidemiologic study of spontaneous reports (SRs) with data on SJS and TEN retrieved from the Russian National Pharmacovigilance database for the period from 1 April 2019 to 31 December 2023. Descriptive statistics was used to assess the demographic data of patients and the structure of suspected drugs. (3) Results: A total of 170 SRs on SJS and TEN were identified, of which 32.9% were SJS and 67.1%—TEN. In total, 30% were pediatric SRs, 21.2%—SRs of the elderly. There were 12 lethal cases, and all cases were TEN. The leading culprit drugs were anti-infectives for systemic use and nervous system agents. The top 10 involved drugs are as follows: lamotrigine (23.5%), ibuprofen (12.9%), ceftriaxone (8.8%), amoxicillin and amoxicillin with beta-lactam inhibitors (8.8%), paracetamol (7.6%), carbamazepine (5.9%), azithromycin (4.1%), valproic acid (4.1%), omeprazole (3.5%), and levetiracetam (3.5%). (4) Conclusions: Our study was the first study in Russia aimed at the assessment of the structure of the drugs involved in SJS and TEN on the national level. [ABSTRACT FROM AUTHOR]
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- 2024
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48. Risk of Autism After Prenatal Topiramate, Valproate, or Lamotrigine Exposure.
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AUTISM risk factors , *RISK assessment , *TOPIRAMATE , *MENTAL health , *LAMOTRIGINE , *VALPROIC acid , *EPILEPSY , *SUBSTANCE abuse in pregnancy , *PUBLIC health , *CHILDREN - Abstract
The article examines the risk of autism spectrum disorder (ASD) following prenatal exposure to topiramate, valproate, or lamotrigine. Among children with maternal epilepsy, only valproate exposure showed a significantly increased risk of ASD, with no substantial risk observed for topiramate or lamotrigine exposure. Topics include the risk variation among the three medications and the methodology to adjust for confounders, reassuring about topiramate's association with ASD.
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- 2024
49. Ethosuximide lowers lamotrigine serum concentrations: Evidence for a clinically relevant interaction.
- Author
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Hagemann, Anne, Herting, Arne, Klimpel, Dennis, Bien, Christian G., and Polster, Tilman
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LAMOTRIGINE , *VALPROIC acid , *ADULTS , *TEENAGERS - Abstract
We investigated the effect of comedication with ethosuximide (ESM) on lamotrigine (LTG) blood levels. Based on observations from clinical practice, we hypothesized that ESM reduces the LTG serum concentration. We additionally evaluated this effect in the presence of concomitant valproic acid (VPA). We retrospectively analyzed samples of inpatients from our department who had been treated with a combination of ESM and LTG between 2017 and 2021. We additionally used data on LTG serum concentrations from a previously published cohort from our center. Generalized estimation equations (GEEs) were used for statistical analyses. We included 523 samples from 209 patients. GEE analyses showed that LTG trough serum concentrations were significantly lower in samples with ESM comedication and significantly higher in samples with concomitant VPA. The effect of ESM was moderated by patients' age; in children and adolescents, LTG serum concentrations were 37% lower than in samples without ESM, whereas in adults, LTG serum concentrations were 14% lower. The effect we found in our data is relevant to daily clinical practice, if patients are not seizure‐free despite typical daily LTG dosage, or if they develop side effects during ESM withdrawal. It should be considered especially in children and adolescents. [ABSTRACT FROM AUTHOR]
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- 2024
- Full Text
- View/download PDF
50. The Use of Compounds Derived from Cannabis sativa in the Treatment of Epilepsy, Painful Conditions, and Neuropsychiatric and Neurodegenerative Disorders.
- Author
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Stasiłowicz-Krzemień, Anna, Nogalska, Wiktoria, Maszewska, Zofia, Maleszka, Mateusz, Dobroń, Maria, Szary, Agnieszka, Kępa, Aleksandra, Żarowski, Marcin, Hojan, Katarzyna, Lukowicz, Malgorzata, and Cielecka-Piontek, Judyta
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NEUROBEHAVIORAL disorders , *NEURODEGENERATION , *NEUROLOGICAL disorders , *MEDICAL marijuana , *EPILEPSY , *CANNABIS (Genus) , *LAMOTRIGINE , *PLANT polyphenols - Abstract
Neurological disorders present a wide range of symptoms and challenges in diagnosis and treatment. Cannabis sativa, with its diverse chemical composition, offers potential therapeutic benefits due to its anticonvulsive, analgesic, anti-inflammatory, and neuroprotective properties. Beyond cannabinoids, cannabis contains terpenes and polyphenols, which synergistically enhance its pharmacological effects. Various administration routes, including vaporization, oral ingestion, sublingual, and rectal, provide flexibility in treatment delivery. This review shows the therapeutic efficacy of cannabis in managing neurological disorders such as epilepsy, neurodegenerative diseases, neurodevelopmental disorders, psychiatric disorders, and painful pathologies. Drawing from surveys, patient studies, and clinical trials, it highlights the potential of cannabis in alleviating symptoms, slowing disease progression, and improving overall quality of life for patients. Understanding the diverse therapeutic mechanisms of cannabis can open up possibilities for using this plant for individual patient needs. [ABSTRACT FROM AUTHOR]
- Published
- 2024
- Full Text
- View/download PDF
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