The pharmacokinetics of oral carbamazepine in rats dosed using an automated drug delivery system

Hill, A. Cameron; Rower, Joseph E.; White, H. Steve

doi:10.1111/epi.16293

Cited by 5 publications

(6 citation statements)

References 19 publications

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“…As Neuro-2a cells were exposed to CBZ, the amplitude of I Na(T) was also decreased in combination with a substantial decrease in the τ inact(S) value of the current evoked in response to the short depolarizing pulse. The previous pharmacokinetic studies have shown that following one hour of administration with CBZ, its plasma level could reach concentrations ranging between 2 and 14 μg/mL (or 8.5 and 59 μM) [ 69 , 70 ]. The observed and predicted CBZ concentrations were also found within therapeutic windows (4–12 μg/mL or 17–51 μM) [ 70 ].…”

Section: Discussionmentioning

confidence: 99%

“…The previous pharmacokinetic studies have shown that following one hour of administration with CBZ, its plasma level could reach concentrations ranging between 2 and 14 μg/mL (or 8.5 and 59 μM) [ 69 , 70 ]. The observed and predicted CBZ concentrations were also found within therapeutic windows (4–12 μg/mL or 17–51 μM) [ 70 ]. Moreover, the actions of CBZ on membrane excitability could be heavily dependent on various factors, including the CBZ concentration used, the pre-existing level of resting potential, different firing patterns of action potentials, and a combination of these three.…”

Section: Discussionmentioning

confidence: 99%

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Characterization in Inhibitory Effectiveness of Carbamazepine in Voltage-Gated Na+ and Erg-Mediated K+ Currents in a Mouse Neural Crest-Derived (Neuro-2a) Cell Line

Cho

Chiang

et al. 2022

IJMS

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Carbamazepine (CBZ, Tegretol®) is an anticonvulsant used in the treatment of epilepsy and neuropathic pain; however, several unwanted effects of this drug have been noticed. Therefore, the regulatory actions of CBZ on ionic currents in electrically excitable cells need to be reappraised, although its efficacy in suppressing voltage-gated Na+ current (INa) has been disclosed. This study was undertaken to explore the modifications produced by CBZ on ionic currents (e.g., INa and erg-mediated K+ current [IK(erg)]) measured from Neuro-2a (N2a) cells. In these cells, we found that this drug differentially suppressed the peak (transient, INa(T)) and sustained (late, INa(L)) components of INa in a concentration-dependent manner with effective IC50 of 56 and 18 μM, respectively. The overall current–voltage relationship of INa(T) with or without the addition of CBZ remained unchanged; however, the strength (i.e., ∆area) in the window component of INa (INa(W)) evoked by the short ascending ramp pulse (Vramp) was overly lessened in the CBZ presence. Tefluthrin (Tef), a synthetic pyrethroid, known to stimulate INa, augmented the strength of the voltage-dependent hysteresis (Hys(V)) of persistent INa (INa(P)) in response to the isosceles-triangular Vramp; moreover, further application of CBZ attenuated Tef-mediated accentuation of INa(P)’s Hys(V). With a two-step voltage protocol, the recovery of INa(T) inactivation seen in Neuro-2a cells became progressively slowed by adding CBZ; however, the cumulative inhibition of INa(T) evoked by pulse train stimulation was enhanced during exposure to this drug. Neuro-2a-cell exposure to CBZ (100 μM), the magnitude of erg-mediated K+ current measured throughout the entire voltage-clamp steps applied was mildly inhibited. The docking results regarding the interaction of CBZ and voltage-gate Na+ (NaV) channel predicted the ability of CBZ to bind to some amino-acid residues in NaV due to the existence of a hydrogen bond or hydrophobic contact. It is conceivable from the current investigations that the INa (INa(T), INa(L), INa(W), and INa(P)) residing in Neuro-2a cells are susceptible to being suppressed by CBZ, and that its block on INa(L) is larger than that on INa(T). Collectively, the magnitude and gating of NaV channels produced by the CBZ presence might have an impact on its anticonvulsant and analgesic effects occurring in vivo.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Characterization in Inhibitory Effectiveness of Carbamazepine in Voltage-Gated Na+ and Erg-Mediated K+ Currents in a Mouse Neural Crest-Derived (Neuro-2a) Cell Line

Cho

Chiang

et al. 2022

IJMS

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“…Blood levels at the end of each week were 5.5 ± 1.1, 11.5 ± 2.3, and 18.0 ± 5.3 μg/mL, respectively; n = 7 dose-response relationship and all required regular handling of the animals to administer the drugs (several times a day), which could have an impact on the seizures in addition to being stressful to the animals. One study placed the drug in the food, 16,17 but it is not clear whether this approach would work if the drug was unpalatable. These previous studies showed that using animals with higher seizure frequencies required fewer animals to show an effect.…”

Section: Discussionmentioning

confidence: 99%

“…Multiple doses must be provided to maintain therapeutic levels while avoiding toxicity, typically by intraperitoneal or gastric gavage administration, which can be very stressful to animals and staff. Inventive approaches to chronic self‐administration have been developed, 16 but unpleasant taste may result in inconsistent levels. There are other models used for drug screening, but it is controversial whether these models really have epilepsy 17 .…”

Section: Introductionmentioning

confidence: 99%

Chronic limbic epilepsy models for therapy discovery: Protocols to improve efficiency

Bertram

Edelbroek

2021

Epilepsia

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Objective There have been recommendations to improve therapy discovery for epilepsy by incorporating chronic epilepsy models into the preclinical process, but unpredictable seizures and difficulties in maintaining drug levels over prolonged periods have been obstacles to using these animals. We report new protocols in which drugs are administered through a new chronic gastric tube to rats with higher seizure frequencies to minimize these obstacles. Methods Adult rats with spontaneous limbic seizures following an episode of limbic status epilepticus induced by electrical hippocampal stimulation were monitored with long‐term video– electroencephalography (EEG). Animals with a predetermined baseline seizure frequency received an intragastric tube for drug administration. Carbamazepine, levetiracetam, phenobarbital, and phenytoin were tested with either an acute protocol (an increasing single dose every other day for a maximum of three doses) or with a chronic protocol (multiple administrations of one dose for a week). Drug levels were obtained to correlate the effect with the level. Results With the acute protocol, all four drugs induced a clear dose‐related response. Similar dose‐related responses were seen following the week‐long dosing protocol for carbamazepine, phenobarbital, and phenytoin, and these responses were associated with drug levels that were in the human therapeutic range. The response to chronic levetiracetam was much less robust. The gastric tube route of administration was well tolerated over a number of months. Significance Using rats with stable, higher seizure frequencies made it possible to identify the potential of a drug to suppress seizures in a realistic model of epilepsy with drug levels that are similar to those of human therapeutic levels. The acute protocol provided a full dose response in 1 week. The chronic administration protocol further differentiated drugs that may be effective long term. The gastric tube facilitates a less stressful, humane, and consistent administration of multiple doses.

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“…Human washed platelets were incubated with CBZ in a dose-dependent manner at 37°C for 70 H. In order to avoid lesion caused by extrusion and contamination, platelets were kept gently stirring under a sterile condition. For antiepilepsy purpose, it is the only method for CBZ to achieve the therapeutic dose range (4–12 μg/ml) in patients under steady-state conditions ( Hill et al, 2019 ). However, the peak serum concentration of CBZ can achieve more than 36 μg/ml ( Brahmi et al, 2006 ; Yang et al, 2018 ).…”

Section: Methodsmentioning

confidence: 99%

Carbamazepine Induces Platelet Apoptosis and Thrombocytopenia Through Protein Kinase A

et al. 2021

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Carbamazepine is extensively used worldwide to treat a wide range of disorders such as epilepsy, peripheral neuralgia and bipolar disorder. Thrombocytopenia and hemorrhage have been identified in multiple carbamazepine-treated patients. However, the underlying mechanism remains poorly understood. Here, we show that platelets undergo apoptosis after carbamazepine treatment. The apoptotic platelets induced by carbamazepine are rapidly removed in vivo, which accounts for thrombocytopenia. We found that carbamazepine treatment attenuates the phosphorylation level of bcl-xl/bcl-2-associated death promoter (BAD), vasodilator-associated stimulated phosphoprotein (VASP) and GPIbβ in platelets, indicating an inhibition effect on protein kinase A (PKA). We further demonstrated that carbamazepine reduced PKA activity through PI3K/Akt/PDE3A signaling pathway. Pharmacological activation of PKA or inhibition of PI3K/Akt/PDE3A protects platelets from apoptosis induced by carbamazepine. Importantly, PDE3A inhibitors or PKA activator ameliorates carbamazepine-mediated thrombocytopenia in vivo. These findings shed light on a possible mechanism of carbamazepine-induced thrombocytopenia, designating PDE3A/PKA as a potential therapeutic target in the treatment of carbamazepine-induced thrombocytopenia.

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The pharmacokinetics of oral carbamazepine in rats dosed using an automated drug delivery system

Cited by 5 publications

References 19 publications

Characterization in Inhibitory Effectiveness of Carbamazepine in Voltage-Gated Na+ and Erg-Mediated K+ Currents in a Mouse Neural Crest-Derived (Neuro-2a) Cell Line

Characterization in Inhibitory Effectiveness of Carbamazepine in Voltage-Gated Na+ and Erg-Mediated K+ Currents in a Mouse Neural Crest-Derived (Neuro-2a) Cell Line

Chronic limbic epilepsy models for therapy discovery: Protocols to improve efficiency

Carbamazepine Induces Platelet Apoptosis and Thrombocytopenia Through Protein Kinase A

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