Lack of association of first and second-line medication dosing and progression to refractory status epilepticus in children

pSERG

doi:10.1016/j.seizure.2024.10.017

Lack of association of first and second-line medication dosing and progression to refractory status epilepticus in children

pSERG

Pediatrics

Research output: Contribution to journal › Article › peer-review

Abstract

Purpose: Evaluate the relationship between first and second-line medication dosing and progression to refractory status epilepticus (RSE) in children. Methods: This is a retrospective analysis of prospectively collected data from September 2014 to February 2020 of children with status epilepticus (SE) who received at least two antiseizure medications (ASMs). We evaluated the risk of developing RSE after receiving a low total benzodiazepine dose (lower than 100 % of the minimum recommended dose for each benzodiazepine dose administered within 10 min) and a low first non-benzodiazepine ASM dose (lower than 100 % of the minimum recommended dose of non-benzodiazepine ASM given as the first single-dose) using a logistic regression model, adjusting for confounders such as time to ASMs. The proportion of patients receiving low first non-benzodiazepine ASM doses was calculated and a logistic regression model was used to evaluate risk factors for low dosing of the first non-benzodiazepine ASM. Results: Among 320 children, 170 (53.1 %) developed RSE, and 150 (46.9 %) responded to the first non-benzodiazepine ASM dose (non-RSE). One hundred thirty-seven (42.8 %) received a low total benzodiazepine dose, and 128 (40 %) received a low first non-benzodiazepine ASM dose. The odds of developing RSE were not higher after a low total benzodiazepine dose (OR=0.76, 95 %CI 0.47–1.23, p = 0.27) or low first non-benzodiazepine ASM dose (OR=0.85, 95 %CI 0.42–1.71, p = 0.65). Receiving a low first non-benzodiazepine ASM dose was independently associated with having received a low total benzodiazepine dose (OR=1.65, 95 %CI 1.01–2.70, p = 0.04). Conclusion: For most patients, dosing variability in first and second-line medications for SE was not the sole clinical feature predicting progression to RSE in this cohort of benzodiazepine-resistant patients. Identification of additional modifiable clinical biomarkers that predict progression to RSE is needed. Though lower ASM doses did not predict RSE in this model, the administration of ASMs at doses likely to prevent RSE remains crucial in SE treatment.

Original language	English (US)
Pages (from-to)	133-141
Number of pages	9
Journal	Seizure
Volume	123
DOIs	https://doi.org/10.1016/j.seizure.2024.10.017
State	Published - Dec 2024

Funding

This study and consortium were funded by the Epilepsy Foundation of America (EF-213583, Targeted Initiative for Health Outcomes), the American Epilepsy Society/Epilepsy Foundation of America Infrastructure Award, and by the Pediatric Epilepsy Research Foundation, and the Epilepsy Research Fund. Study funding: This study and our Consortium were supported by the Epilepsy Foundation of America (EF- 213583, Targeted Initiative for Health Outcomes), the American Epilepsy Society / Epilepsy Foundation of America Infrastructure Award, the Pediatric Epilepsy Research Foundation, and the Epilepsy Research Fund.

Keywords

All epilepsy/seizures
Antiepileptic drugs
Outcome research
Pediatric
Status epilepticus

ASJC Scopus subject areas

Neurology
Clinical Neurology

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10.1016/j.seizure.2024.10.017

Cite this

@article{60ab32402a3041d3a00144e846b2fe57,

title = "Lack of association of first and second-line medication dosing and progression to refractory status epilepticus in children",

abstract = "Purpose: Evaluate the relationship between first and second-line medication dosing and progression to refractory status epilepticus (RSE) in children. Methods: This is a retrospective analysis of prospectively collected data from September 2014 to February 2020 of children with status epilepticus (SE) who received at least two antiseizure medications (ASMs). We evaluated the risk of developing RSE after receiving a low total benzodiazepine dose (lower than 100 % of the minimum recommended dose for each benzodiazepine dose administered within 10 min) and a low first non-benzodiazepine ASM dose (lower than 100 % of the minimum recommended dose of non-benzodiazepine ASM given as the first single-dose) using a logistic regression model, adjusting for confounders such as time to ASMs. The proportion of patients receiving low first non-benzodiazepine ASM doses was calculated and a logistic regression model was used to evaluate risk factors for low dosing of the first non-benzodiazepine ASM. Results: Among 320 children, 170 (53.1 %) developed RSE, and 150 (46.9 %) responded to the first non-benzodiazepine ASM dose (non-RSE). One hundred thirty-seven (42.8 %) received a low total benzodiazepine dose, and 128 (40 %) received a low first non-benzodiazepine ASM dose. The odds of developing RSE were not higher after a low total benzodiazepine dose (OR=0.76, 95 %CI 0.47–1.23, p = 0.27) or low first non-benzodiazepine ASM dose (OR=0.85, 95 %CI 0.42–1.71, p = 0.65). Receiving a low first non-benzodiazepine ASM dose was independently associated with having received a low total benzodiazepine dose (OR=1.65, 95 %CI 1.01–2.70, p = 0.04). Conclusion: For most patients, dosing variability in first and second-line medications for SE was not the sole clinical feature predicting progression to RSE in this cohort of benzodiazepine-resistant patients. Identification of additional modifiable clinical biomarkers that predict progression to RSE is needed. Though lower ASM doses did not predict RSE in this model, the administration of ASMs at doses likely to prevent RSE remains crucial in SE treatment.",

keywords = "All epilepsy/seizures, Antiepileptic drugs, Outcome research, Pediatric, Status epilepticus",

author = "pSERG and {Barcia Aguilar}, Cristina and Marta Amengual-Gual and Brenton, {J. Nicholas} and Chapman, {Kevin E.} and Justice Clark and Gaillard, {William D.} and Goldstein, {Joshua L.} and Goodkin, {Howard P.} and Robert Kahoud and Lai, {Yi Chen} and Mikati, {Mohamad A.} and Morgan, {Lindsey A.} and Payne, {Eric T.} and Press, {Craig A.} and Latania Reece and Sands, {Tristan T.} and Kumar Sannagowdara and Theodore Sheehan and Shellhaas, {Ren{\'e}e A.} and Tasker, {Robert C.} and Wainwright, {Mark S.} and Bo Zhang and Tobias Loddenkemper",

note = "Publisher Copyright: {\textcopyright} 2024",

year = "2024",

month = dec,

doi = "10.1016/j.seizure.2024.10.017",

language = "English (US)",

volume = "123",

pages = "133--141",

journal = "Seizure",

issn = "1059-1311",

publisher = "W.B. Saunders Ltd",

}

TY - JOUR

T1 - Lack of association of first and second-line medication dosing and progression to refractory status epilepticus in children

AU - pSERG

AU - Barcia Aguilar, Cristina

AU - Amengual-Gual, Marta

AU - Brenton, J. Nicholas

AU - Chapman, Kevin E.

AU - Clark, Justice

AU - Gaillard, William D.

AU - Goldstein, Joshua L.

AU - Goodkin, Howard P.

AU - Kahoud, Robert

AU - Lai, Yi Chen

AU - Mikati, Mohamad A.

AU - Morgan, Lindsey A.

AU - Payne, Eric T.

AU - Press, Craig A.

AU - Reece, Latania

AU - Sands, Tristan T.

AU - Sannagowdara, Kumar

AU - Sheehan, Theodore

AU - Shellhaas, Renée A.

AU - Tasker, Robert C.

AU - Wainwright, Mark S.

AU - Zhang, Bo

AU - Loddenkemper, Tobias

PY - 2024/12

Y1 - 2024/12

N2 - Purpose: Evaluate the relationship between first and second-line medication dosing and progression to refractory status epilepticus (RSE) in children. Methods: This is a retrospective analysis of prospectively collected data from September 2014 to February 2020 of children with status epilepticus (SE) who received at least two antiseizure medications (ASMs). We evaluated the risk of developing RSE after receiving a low total benzodiazepine dose (lower than 100 % of the minimum recommended dose for each benzodiazepine dose administered within 10 min) and a low first non-benzodiazepine ASM dose (lower than 100 % of the minimum recommended dose of non-benzodiazepine ASM given as the first single-dose) using a logistic regression model, adjusting for confounders such as time to ASMs. The proportion of patients receiving low first non-benzodiazepine ASM doses was calculated and a logistic regression model was used to evaluate risk factors for low dosing of the first non-benzodiazepine ASM. Results: Among 320 children, 170 (53.1 %) developed RSE, and 150 (46.9 %) responded to the first non-benzodiazepine ASM dose (non-RSE). One hundred thirty-seven (42.8 %) received a low total benzodiazepine dose, and 128 (40 %) received a low first non-benzodiazepine ASM dose. The odds of developing RSE were not higher after a low total benzodiazepine dose (OR=0.76, 95 %CI 0.47–1.23, p = 0.27) or low first non-benzodiazepine ASM dose (OR=0.85, 95 %CI 0.42–1.71, p = 0.65). Receiving a low first non-benzodiazepine ASM dose was independently associated with having received a low total benzodiazepine dose (OR=1.65, 95 %CI 1.01–2.70, p = 0.04). Conclusion: For most patients, dosing variability in first and second-line medications for SE was not the sole clinical feature predicting progression to RSE in this cohort of benzodiazepine-resistant patients. Identification of additional modifiable clinical biomarkers that predict progression to RSE is needed. Though lower ASM doses did not predict RSE in this model, the administration of ASMs at doses likely to prevent RSE remains crucial in SE treatment.

AB - Purpose: Evaluate the relationship between first and second-line medication dosing and progression to refractory status epilepticus (RSE) in children. Methods: This is a retrospective analysis of prospectively collected data from September 2014 to February 2020 of children with status epilepticus (SE) who received at least two antiseizure medications (ASMs). We evaluated the risk of developing RSE after receiving a low total benzodiazepine dose (lower than 100 % of the minimum recommended dose for each benzodiazepine dose administered within 10 min) and a low first non-benzodiazepine ASM dose (lower than 100 % of the minimum recommended dose of non-benzodiazepine ASM given as the first single-dose) using a logistic regression model, adjusting for confounders such as time to ASMs. The proportion of patients receiving low first non-benzodiazepine ASM doses was calculated and a logistic regression model was used to evaluate risk factors for low dosing of the first non-benzodiazepine ASM. Results: Among 320 children, 170 (53.1 %) developed RSE, and 150 (46.9 %) responded to the first non-benzodiazepine ASM dose (non-RSE). One hundred thirty-seven (42.8 %) received a low total benzodiazepine dose, and 128 (40 %) received a low first non-benzodiazepine ASM dose. The odds of developing RSE were not higher after a low total benzodiazepine dose (OR=0.76, 95 %CI 0.47–1.23, p = 0.27) or low first non-benzodiazepine ASM dose (OR=0.85, 95 %CI 0.42–1.71, p = 0.65). Receiving a low first non-benzodiazepine ASM dose was independently associated with having received a low total benzodiazepine dose (OR=1.65, 95 %CI 1.01–2.70, p = 0.04). Conclusion: For most patients, dosing variability in first and second-line medications for SE was not the sole clinical feature predicting progression to RSE in this cohort of benzodiazepine-resistant patients. Identification of additional modifiable clinical biomarkers that predict progression to RSE is needed. Though lower ASM doses did not predict RSE in this model, the administration of ASMs at doses likely to prevent RSE remains crucial in SE treatment.

KW - All epilepsy/seizures

KW - Antiepileptic drugs

KW - Outcome research

KW - Pediatric

KW - Status epilepticus

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UR - http://www.scopus.com/inward/citedby.url?scp=85209076507&partnerID=8YFLogxK

U2 - 10.1016/j.seizure.2024.10.017

DO - 10.1016/j.seizure.2024.10.017

M3 - Article

C2 - 39550933

AN - SCOPUS:85209076507

SN - 1059-1311

VL - 123

SP - 133

EP - 141

JO - Seizure

JF - Seizure

ER -

Lack of association of first and second-line medication dosing and progression to refractory status epilepticus in children

Abstract

Funding

Keywords

ASJC Scopus subject areas

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