Pharmacokinetic‐Pharmacodynamic Modeling of Intravenous and Oral Topiramate and Its Effect on the Symbol‐Digit Modalities Test in Adult Healthy Volunteers

Lim, Chay Ngee; Brundage, Richard C.; Leppik, Ilo E.; Cloyd, James C.; Clark, Annie; Marino, Susan E.

doi:10.1002/jcph.646

Cited by 6 publications

(16 citation statements)

References 27 publications

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“…Most studies were conducted in epilepsy patients in various age groups including infants, 24 infants and children, 19 children and adults, 25,26 and children, adults and elderly 21 . Moreover, three were conducted solely in adults with epilepsy, 18,20,22 and two studies in healthy volunteers 23,27 . The number of subjects and the number of observations varied across studies, ranging from 22 to 1217 and 118 to 4640, respectively.…”

Section: Resultsmentioning

confidence: 99%

“…All studies used NONMEM software for model development, with various estimation methods (Table 3). For the structural model development, six studies used a linear one‐compartment structure, 18,19,22,24–26 while three studies reported a two‐compartment linear model 20,21,27 and the other one used an E max model to describe the effects of single‐dose TPM on working memory, attention and psychomotor speed 23 . This model is commonly used to explain the concentration–effect relationship, in which E max is the maximal effect when all the receptors are occupied by the drug.…”

Section: Resultsmentioning

confidence: 99%

“…Other significant covariates included age, 21,26 renal function 18,22 and TPM daily dose 18 . As for the V D , weight, 18,19,22,24–27 age 19 and a baseline Symbol Digit Modalities Test (SDMT) score of the E max model 23 were significant predictors. The SDMT is a tool used to assess neurological dysfunction by identifying nine different symbols corresponding to the numbers 1–9.…”

Section: Resultsmentioning

confidence: 99%

“…Nonetheless, this study was conducted in healthy volunteers with TPM concentrations ranging from 0.05–3 mg/L, therefore, the applicability of these results to patients with epilepsy should be further investigated. The effects of 100 or 200 mg single dose TPM on working memory, attention and psychomotor speed were also investigated using SDMT 23 . The relationship between TPM concentrations and SDMT score was well described using an inhibitory E max model.…”

Section: Discussionmentioning

confidence: 99%

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Significant predictors for topiramate pharmacokinetics: a systematic review of population pharmacokinetic studies

Tippayachai

Leelakanok

Methaneethorn

2022

Pharmacy Practice and Res

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Background: Topiramate (TPM) is a second-generation antiepileptic drug with a good pharmacokinetic profile; nonetheless, several factors such as age, renal function and concomitant medications have been reported to affect TPM clearance and dosage adjustments are necessary. Several population pharmacokinetic studies of TPM were developed and the results were partially inconsistent, with different predictors for TPM pharmacokinetic parameters and different structural models. Thus, we aimed to systematically summarise clinically significant covariates influencing TPM pharmacokinetics and clinical responses. Methods: PubMed, CINAHL Complete, Science Direct and SCOPUS databases were systematically searched from the date of their inception to May 2021. Studies conducted in humans employing a nonlinear mixed-effects approach were included in this review. Information from retrieved articles were independently extracted using the prespecified data abstraction form. Results: Ten studies were included and most of them characterised TPM pharmacokinetics with a linear one-compartment model. The estimated TPM clearance without covariate effects ranged from 1.15 to 2.25 L/h. Significant predictors for TPM clearance included concomitant medications, weight, age, creatinine clearance and TPM daily dose. Moreover, two studies reported the effect of TPM exposure on cognitive function, with limitations on the generalisability. Conclusions: Significant predictors for TPM clearance that are essential for individualising dosage regimens were concomitant medications, weight, age, creatinine clearance and TPM daily dose. High TPM levels had negative impacts on verbal fluency, working memory, attention and psychomotor speed; however, future studies with broader population characteristics are needed to increase generalisability.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

See 2 more Smart Citations

Significant predictors for topiramate pharmacokinetics: a systematic review of population pharmacokinetic studies

Tippayachai

Leelakanok

Methaneethorn

2022

Pharmacy Practice and Res

View full text Add to dashboard Cite

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“…vs IR topiramate b.i.d., but plasma concentration fluctuations may impact signature adverse cognitive effects such as word‐finding difficulty and psychomotor slowing. The occurrence and severity of these and other CNS AEs associated with topiramate are influenced by dose, rate of dose escalation, and plasma topiramate concentrations . Given this PK‐PD relationship, a bioequivalence study comparing an XR formulation (Trokendi XR q.d.)…”

Section: Extended‐release Topiramatementioning

confidence: 99%

Topiramate in Migraine Prevention: A 2016 Perspective

Silberstein

2016

Headache

103

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Topiramate has activity at multiple molecular targets, which may account for why it is effective in migraine and most other, more specific, anticonvulsants are not. Based on randomized controlled trials, topiramate reduces migraine frequency and acute medication use, improves quality of life, and reduces disability in patients with episodic migraine and in those with chronic migraine with or without medication overuse headache. Its efficacy in chronic migraine is not improved by the addition of propranolol. Topiramate's ability to prevent progression from high-frequency episodic migraine to chronic migraine remains unclear. Consistent with clinicians' perceptions, migraineurs are more sensitive to topiramate-associated side effects than patients with epilepsy. Paresthesia is a common occurrence early in treatment but is rarely cause for terminating topiramate treatment. Cognitive problems occur much less frequently than paresthesia but are more troublesome in terms of treatment discontinuation. Cognitive complaints can often be managed by slowly increasing the topiramate dose in small increments to allow habituation. As with other carbonic anhydrase inhibitors, topiramate has metabolic effects that favor the development of metabolic acidosis and possibly renal stones. Because migraineurs have an increased risk of renal stones independent of topiramate exposure, clinicians should counsel all migraine patients to maintain hydration. Abrupt onset of blurring, other visual disturbances, and/or ocular pain following topiramate's initiation should be evaluated promptly since this may indicate rare but potentially sight-threatening idiosyncratic events. Postmarketing evidence has shown that first-trimester exposure to topiramate monotherapy is associated with increased occurrence of cleft lip with or without cleft palate (Pregnancy Category D). Even though topiramate's long half-life would seemingly support q.d. dosing, randomized controlled migraine trials used b.i.d. administration of immediate-release (IR) topiramate, which has more favorable plasma concentration-time profile (ie, lower peak concentrations and higher trough concentrations) than q.d. IR dosing. Given the sensitivity of migraineurs to topiramate-related adverse events, particularly cognitive effects, pharmacokinetic profiles should be considered when optimizing migraine outcomes. The extended-release (XR) formulations Qudexy XR (Upsher-Smith Laboratories) and Trokendi XR (Supernus Pharmaceuticals) were specifically designed to achieve the adherence benefits of q.d. dosing but with more favorable (ie, more constant) steady-state plasma concentrations over the 24-hour dosing interval vs IR topiramate b.i.d. Intriguing results from a study in healthy volunteers showed consistently less impairment in neuropsychometric tests of verbal fluency and mental processing speed with an XR topiramate formulation (Trokendi XR) vs IR topiramate b.i.d. These findings suggest a pharmacodynamic effect associated with significantly reducing plasma concentration fluctuatio...

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Severity of Topiramate‐Related Working Memory Impairment Is Modulated by Plasma Concentration and Working Memory Capacity

Callisto

Illamola

Barkley

et al. 2020

The Journal of Clinical Pharma

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Drug side effects that impair cognition can lead to diminished quality of life and discontinuation of therapy. Topiramate is an antiepileptic drug that elicits cognitive deficits more frequently than other antiepileptic drugs, impairing multiple cognitive domains including language, attention, and memory. Although up to 40% of individuals taking topiramate may experience cognitive deficits, we are currently unable to predict which individuals will be most severely affected before administration. The objective of this study was to show the contributions of plasma concentration and working memory capacity in determining the severity of an individual's topiramate‐related cognitive impairment. Subjects were enrolled in a double‐blind, placebo‐controlled crossover study during which they received a single dose of either 100, 150, or 200 mg topiramate. Working memory function was assessed using a modified Sternberg working memory task with 3 memory loads administered 4 hours after dosing. After adjustment for differences in working memory capacity, each 1 μg/mL of topiramate plasma concentration was associated with a 3.6% decrease in accuracy for all memory loads. Placebo effects occurred as a function of working memory capacity, with individuals with high working memory capacity experiencing less severe placebo‐related impairment compared with those with low working memory capacity. Our results demonstrate that severity of topiramate‐related cognitive deficits occurs as a function of both drug exposure and baseline cognitive function. By identifying patient‐ and exposure‐related characteristics that modulate the severity of cognitive side effects, topiramate dosing strategies may be individually tailored in the future to prevent unwanted cognitive impairment.

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Pharmacokinetic‐Pharmacodynamic Modeling of Intravenous and Oral Topiramate and Its Effect on the Symbol‐Digit Modalities Test in Adult Healthy Volunteers

Cited by 6 publications

References 27 publications

Significant predictors for topiramate pharmacokinetics: a systematic review of population pharmacokinetic studies

Significant predictors for topiramate pharmacokinetics: a systematic review of population pharmacokinetic studies

Topiramate in Migraine Prevention: A 2016 Perspective

Severity of Topiramate‐Related Working Memory Impairment Is Modulated by Plasma Concentration and Working Memory Capacity

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