Emergency (****); * (*): *-* This open-access article distributed under the terms of the Creative Commons Attribution NonCommercial 3.0 License (CC BY-NC 3.0). Copyright © 2015 Shahid Beheshti University of Medical Sciences. All rights reserved. Downloaded from: www.jemerg.com 159 Emergency (2015); 3 (4): 159-161 BRIEF REPERT Prevalence of Tramadol Consumption in First Seizure Patients; a One-Year Cross-sectional Study Payman Asadi, Vahid Monsef Kasmaei, Seyyed Zia Ziabari, Behzad Zohrevandi*, Aslan Moadab Manesh Road Trauma Research Center, Guilan University of Medical Sciences, Rasht, Iran. *Corresponding Author: Behzad Zohrevandi; Road trauma Research Center, Guilan University of Medical Sciences, Rasht, Iran. Tel: 09188523847. Fax: +981313238373; Email: bzohrevandi@yahoo.com Received: April 2015; Accepted: May 2016 Abstract Introduction: Previous studies have shown that there is a probability of seizure even with therapeutic doses of tramadol. Yet, no accurate data exist regarding this problem in Iran. Therefore, the present study aimed to evaluate the prevalence of tramadol consumption in patients with first seizure referred to the emergency department (ED). Methods: In the present retrospective one-year cross-sectional study, all patients who were referred to the ED of Poursina Hospital, Rasht, Iran, with the complaint of first seizure were evaluated. Demographic data and data re- garding history of tramadol consumption, duration, total dose, last dose, and time passed from the last dose of consumption were recorded and analyzed regarding the study questions using SPSS 20. Results: 383 (68.9%) out of the 556 patients referred to the ED, were experiencing their first seizure (mean age 26.43 ± 6.48 years; 70.5% male). 84 (21.9%) patients had recently used tramadol. History of seizure in the family of tramadol consumers was significantly lower (3.6% compared to 11%; p = 0.036). Mean total tramadol consumption dose in the last 24 hours was 140.17 ± 73.53 mg (range: 50-300 mg). Duration of tramadol consumption was less than 10 days in 84.5% (df: 2; χ2 = 96.1; p < 0.001). In addition, 62 (73.8%) patients had seizure within 6 hours of consumption (df: 3; χ2 = 29.5; p < 0.001). Conclusion: Results of the present study showed that 21.9% of the patients with first seizure had a history of tramadol consumption. Seizure following tramadol consumption is more prevalent in the initial 10 days and within 6 hours of consumption. In addition, it seems that lower doses of tramadol may also induce seizure. Key words: Seizures; tramadol; prevalence; epidemiology Cite this article as: Asadi P, Monsef Kasmaei V, Ziabari SZ, Zohrevandi B, Moadab Manesh A. Prevalence of tramadol consumption in first seizure patients; a one-year cross-sectional study. Emergency. 2015;3(4):159-61. Introduction: ramadol is an opioid used for treating moderate to severe pain. It has been legally used for pain man- agement since 1980 in some countries, and has been approved by food and drug administration of Iran since 2003. This drug is addictive and may be abused by the youth. Nausea, vomiting, central nervous system de- pression, tachycardia, cardiorespiratory arrest, and sei- zure are among the side effects of tramadol poisoning. However, there are reports that indicate the probability of seizure induction even with therapeutic doses of this drug (1-5). Tramadol abuse is increasing in Iran, (2, 6) and seizure is possible among abusers. Therefore, the present study aimed to evaluate the prevalence of tra- madol abuse in patients with first seizure, who were re- ferred to the emergency department (ED). Methods: In the present retrospective cross-sectional one-year study, all first seizure patients referred to the ED of Poursina Hospital, Rasht, Iran, during 2012 were evalu- ated. For each patient, data regarding age, sex, history of seizure in family, recent history of tramadol consump- tion, duration (days), total dose, last dose, and time passed from the last dose of consumption were recorded using a checklist. Data were then analyzed using SPSS 20.0. Quantitative data were reported as mean ± SD and qualitative ones as frequency and percentage. The groups with and without recent tramadol consumption were compared using independent t-test for quantitative variables and chi square or Fisher’s exact test for quali- tative ones. In addition, multinomial logistic regression test was used to evaluate distribution of the patients in groups regarding age, sex, duration of consumption, con- sumed dose in the last 24 hours, and time passed from the last dose of tramadol consumption. In all analyses, p < 0.05 was considered as significance level. This study T This open-access article distributed under the terms of the Creative Commons Attribution NonCommercial 3.0 License (CC BY-NC 3.0). Copyright © 2015 Shahid Beheshti University of Medical Sciences. All rights reserved. Downloaded from: www.jemerg.com Asadi et al 160 was approved by the Ethics Committee of Guilan Univer- sity of Medical Sciences. The researchers adhered to the principles of Helsinki declaration. Results: 383 (68.9%) out of the 556 patients who were referred to the ED with chief complaint of seizure throughout the course of the study, were experiencing their first seizure. Mean age of first seizure patients was 26.43 ± 6.48 years (range: 16-55 years; 70.5% male). 84 (21.9%) patients out of the 383 first seizures had re- cent history of tramadol consumption. 69 (82.1%) of tramadol consumers and 201 (67.2%) of other patients were male (p = 0.005). 48.8% of the tramadol consum- ing patients and 59.9% of other patients were 20 -30 years old (p = 0.016). History of seizure in the famil y of tramadol consumers was significantly lower (3.6% compared to 11%; p = 0.036). Table 1 shows baseline characteristics of the tramadol consumers. Mean total tramadol consumption dose in the last 24 hours was 140.17 ± 73.53 mg (range: 50-300 mg). Duration of con- sumption was less than 10 days in 84.5% of the pa- tients, 11-20 days in 10.7%, and more than 20 days in 4.8%. Incidence of seizure following ingestion was higher in patients who had recently started consump- tion (df: 2; χ2 = 96.1; p < 0.001). Yet, no correlation was detected between tramadol dosage and seizure inci- dence (df: 3; χ2 = 1.2; p = 0.1). Seizure had occurred within 6 hours of consumption in 62 (73.8%) patients (df: 3; χ2 = 29.5; p < 0.001). Discussion: Findings of the present study showed that 68.9% of the patients referred to Poursina Hospital, Rasht, Iran, were experiencing their first seizure, 21.9% of which had re- cent history of tramadol consumption. Seizure following tramadol consumption was more prevalent in the initial 10 days and within 6 hours of consumption. Previous studies show that about 86% of neurologic side effects manifest within 6 hours of consumption (7, 8). The pre- sent study showed that 73.8% of seizures due to tra- madol consumption also happened in this time. Based on the existing standards, to prevent side effects such as sei- zure, daily dose of tramadol should not exceed 400 mg (1, 2, 9). In this cross-section, mean total tramadol con- sumption dose in 24 hours was 140.17 ± 73.53 mg. In a study by Shadnia et al. (2), this dose was 1650 mg while, in a study by Pedramfar et al. (5), total dose in the 12 hours pre-seizure was 363.2 ± 303.1 mg (50 -1500). Mean consumption dose in the participants of this study was significantly lower than the mentioned studies. This may be due to the patients not revealing their real con- sumption dose, genetic differences in the studied popu- lations, different pharmaceutical companies making the drugs and other unknown reasons. Therefore, we should note that tramadol might also be able to induce seizure in lower doses. One of the limitations of this study was being retrospective, which led to limited access to some Table 1: Baseline characteristics of tramadol consuming patients Characteristics Number (%) P value Sex Male 69 (82.1) ref Female 15 (17.9) <0.001 Age (Year) < 20 19 (22.7) 0.006 20-30 41 (48.8) ref 31-40 18 (21.4) 0.004 > 40 6 (7.1) <0.001 Consumption duration (Day) < 10 71 (84.5) ref 11-20 9 (10.7) <0.001 > 20 4 (4.8) <0.001 Dose in the last 24 hours (mg) 50 16 (19.0) ref 50-100 27 (32.1) 0.1 100-200 29 (34.5) 0.06 > 200 12 (14.3) 0.45 Time passed since the last dose (Hour) < 3 hours 32 (38.1) ref 3-6 hours 30 (35.7) 0.8 6-12 hours 18 (21.4) 0.049 > 12 hours 4 (4.8) <0.001 This open-access article distributed under the terms of the Creative Commons Attribution NonCommercial 3.0 License (CC BY-NC 3.0). Copyright © 2015 Shahid Beheshti University of Medical Sciences. All rights reserved. Downloaded from: www.jemerg.com 161 Emergency (2015); 3 (4): 159-161 of the required data. Moreover, serum tramadol level was not evaluated and therefore its correlation with sei- zure incidence could not be determined. Conclusion: Results of the present study showed that 21.9% of the patients with first seizure had a history of tramadol con- sumption. Seizure following tramadol consumption is more prevalent in the initial 10 days and within 6 hours of consumption. Although the maximum recommended therapeutic dose of tramadol is 400 mg/day, mean con- sumption dose among the participants of this study was 140.17 ± 53.73 mg. Therefore, we might be able to con- clude that lower doses of tramadol may also induce sei- zure. Conflict of interest: None Funding support: None Authors’ contributions: All authors passed four criteria for authorship contribu- tion based on recommendations of the International Committee of Medical Journal Editors. References: 1. Mehrpour M. Intravenous Tramadol-Induced Seizure: Two Case Reports. Iran J Pharmacol Therapeut. 2005;4(2):146-7. 2. Shadnia S, Soltaninejad K, Heydari K, Sasanian G, Abdollahi M. Tramadol intoxication: a review of 114 cases. Hum Exp Toxicol. 2008;27:201–5. 3. Derakhshanfar H, Kalantari Meibodi M, Kariman H, Arhamidolatabadi A, Safari S. Substance Abuse among Drivers of Motor Vehicle Collisions. Trauma Mon. 2012;2012(01, Apr):236-8. 4. Tashakori A, Afshari R. Tramadol overdose as a cause of serotonin syndrome: a case series. Clin Toxicol (Phila). 2010;48(4):337-41. 5. Pedramfar P, Borhani Haghighi A. Tramadol Induced Seizure: Report of 106 Patients. Iran Red Crescent Med J. 2010;12(1):49-51. 6. Hassanian Moghaddam H, Pajoumand A. A oneyear epidemiological study of acute poisoning among adults and adolescents admitted to loghman Hospital, Tehran between 2005 and 2006. Pajouhandeh. 2007;12(57):169-76. [Persian]. 7. Jovanovic-Cupic V, Martinovic Z, Nešic N. Seizures associated with intoxication and abuse of tramadol. Clin Toxicol. 2006;44(2):143-6. 8. Marquardt KA, Alsop JA, Albertson TE. Tramadol exposures reported to statewide poison control system. Ann Pharmacother. 2005;39(6):1039-44. 9. Baratloo A, Rouhipour A, Forouzanfar M, Rahmati F, Hashemi B. Hypokalemia-Induced Abnormal Movements: Case Report. Trauma Mon. 2013;18(3):141-5. Introduction: Methods: Results: Discussion: Conclusion: Conflict of interest: Funding support: Authors’ contributions: References: