Open‐label clinical trial of rectally administered levetiracetam as supplemental treatment in dogs with cluster seizures

Cagnotti, Giulia; Odore, R.; Bertone, Iride; Corona, Cristiano; Dappiano, Elena; Gardini, Giulia; Iulini, Barbara; Bellino, Claudio; D’Angelo, Antonio

doi:10.1111/jvim.15541

Cited by 11 publications

(8 citation statements)

References 19 publications

(40 reference statements)

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“…Different routes of administration could elicit different pharmacokinetic and pharmacodynamic responses of the same drug mixture. A decreased uptake of drugs is already known for benzodiazepine in dogs for IR; as suggested by [ 11 , 17 ], similar clinical effects occur with a range dose of 0.5–2 mg kg −1 in IR and 0.2–0.3 mg kg −1 in IV administration of diazepam. This consideration would seem valid for midazolam: IV and IR at the same posology present lower bioavailability in the second case [ 18 ].…”

Section: Discussionmentioning

confidence: 67%

Comparison of Certain Intrarectal versus Intramuscular Pharmacodynamic Effects of Ketamine, Dexmedetomidine and Midazolam in Cats

Paolini

Vignoli

Falerno

et al. 2022

Veterinary Sciences

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The aim of this clinical trial was to evaluate the impacts of administration via the intrarectal route (IR) in cats on their heart and respiratory rates, blood pressure, body temperature, and sedation quality compared to the intramuscular route (IM). The intramuscular group (IMG) received 0.003 mg kg−1 dexmedetomidine, 2 mg kg−1 ketamine, and 0.2 mg kg−1 midazolam while the intrarectal group (IRG) protocol was 0.003 mg kg−1 dexmedetomidine, 4 mg kg−1 ketamine, and 0.4 mg kg−1 midazolam. Cardiorespiratory values, temperature, and sedation score were measured 2 min after administration and then every 5 min up to the 40th minute. Cats belonging to IRG reacted less strongly to the drug, as opposed to those receiving intramuscular administration (2/10 in IRG vs. 8/10 in IMG). Average time between drug administration and standing position was 44.9 ± 5.79 in IRG and 57 ± 9.88 min in IMG. In IRG, maintenance of SpO₂ values is > 95% at each time point. Median and range peak of sedation {7 (5)} in IMG occurs at 20th, 25th, and 30th minutes post drug administration while was lower in IRG. Cardiorespiratory values were slightly lower in IMG than in IRG, but always constant in both treatments. Temperature did not differ between groups. At this dosage, although sedation score was higher in IMG, intrarectal route could be efficacious for performing minimally invasive clinical and diagnostic procedures in cats.

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Section: Discussionmentioning

confidence: 67%

Comparison of Certain Intrarectal versus Intramuscular Pharmacodynamic Effects of Ketamine, Dexmedetomidine and Midazolam in Cats

Paolini

Vignoli

Falerno

et al. 2022

Veterinary Sciences

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“…After the exclusion of duplicates, 87 (SE) and 28 (CS) studies remained and entered stage 2 screening. Of these, 38 clinical studies 2,3,37‐40,43‐74 (SE; dogs, n = 36; cats, n = 5) and 12 clinical studies 37,40,48,49,57,64,75‐80 (CS; dogs, n = 12; cats, n = 0) as well as 37 pharmacokinetic studies 49,57,65,81‐114 (dogs, n = 33; cats, n = 4) fulfilled stage 2 criteria and were selected for review. Some clinical studies included a mixed populations of dogs and cats.…”

Section: Results and Recommendationsmentioning

confidence: 99%

“…Pulse treatment has been recommended instead of long‐term continuous treatment, because it might prevent the development of tolerance associated with the drug's chronic use 77 . In the out‐of‐hospital setting, PO levetiracetam can be used as a first‐choice; R administration also can be used in dogs, especially when PO administration is not possible 49,76,77,101 . In dogs that are receiving chronic phenobarbital treatment, a higher dose of levetiracetam may be needed 77 .…”

Section: Specific Guidelines and Recommendations For The Treatment Of...mentioning

confidence: 99%

ACVIM Consensus Statement on the management of status epilepticus and cluster seizures in dogs and cats

Charalambous,

Muñana,

Patterson

et al. 2023

Veterinary Internal Medicne

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BackgroundSeizure emergencies (ie, status epilepticus [SE] and cluster seizures [CS]), are common challenging disorders with complex pathophysiology, rapidly progressive drug‐resistant and self‐sustaining character, and high morbidity and mortality. Current treatment approaches are characterized by considerable variations, but official guidelines are lacking.ObjectivesTo establish evidence‐based guidelines and an agreement among board‐certified specialists for the appropriate management of SE and CS in dogs and cats.AnimalsNone.Materials and MethodsA panel of 5 specialists was formed to assess and summarize evidence in the peer‐reviewed literature with the aim to establish consensus clinical recommendations. Evidence from veterinary pharmacokinetic studies, basic research, and human medicine also was used to support the panel's recommendations, especially for the interventions where veterinary clinical evidence was lacking.ResultsThe majority of the evidence was on the first‐line management (ie, benzodiazepines and their various administration routes) in both species. Overall, there was less evidence available on the management of emergency seizure disorders in cats in contrast to dogs. Most recommendations made by the panel were supported by a combination of a moderate level of veterinary clinical evidence and pharmacokinetic data as well as studies in humans and basic research studies.Conclusions and Clinical RelevanceSuccessful management of seizure emergencies should include an early, rapid, and stage‐based treatment approach consisting of interventions with moderate to preferably high ACVIM recommendations; management of complications and underlying causes related to seizure emergencies should accompany antiseizure medications.

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“…"Given the small number of patients admitted with SE (status epilepticus) in both groups, statistical analysis was performed taking into consideration only patients affected by CS (cluster seizures)." (119) "The possible confounding effects of the intraoperative administration of hydromorphone on recovery were evaluated. Twelve dogs in group P and 10 dogs in group KD did not receive hydromorphone at any time during the anesthetic period.…”

Section: Ancillary Analysesmentioning

confidence: 99%

The standards of reporting trials in pets (PetSORT): Explanation and elaboration

et al. 2023

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Well-designed randomized controlled trials (RCTs) provide the best evidence of the primary research designs for evaluating the effectiveness of interventions. However, if RCTs are incompletely reported, the methodological rigor with which they were conducted cannot be reliably evaluated and it may not be possible to replicate the intervention. Missing information also may limit the reader's ability to evaluate the external validity of a trial. Reporting guidelines are available for clinical trials in human healthcare (CONSORT), livestock populations (REFLECT), and preclinical experimental research involving animals (ARRIVE 2.0). The PetSORT guidelines complement these existing guidelines, providing recommendations for reporting controlled trials in pet dogs and cats. The rationale and scientific background are explained for each of the 25 items in the PetSORT reporting recommendations checklist, with examples from well-reported trials.

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Open‐label clinical trial of rectally administered levetiracetam as supplemental treatment in dogs with cluster seizures

Cited by 11 publications

References 19 publications

Comparison of Certain Intrarectal versus Intramuscular Pharmacodynamic Effects of Ketamine, Dexmedetomidine and Midazolam in Cats

Comparison of Certain Intrarectal versus Intramuscular Pharmacodynamic Effects of Ketamine, Dexmedetomidine and Midazolam in Cats

ACVIM Consensus Statement on the management of status epilepticus and cluster seizures in dogs and cats

The standards of reporting trials in pets (PetSORT): Explanation and elaboration

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