Your search keyword '"Brent, Jeffrey"' showing total 27 results

1. The role of QRS complex prolongation in predicting severe toxicity in single-xenobiotic overdose.

Author

Simon, Mark, Kaplan, Sabrina, Muschler, Karen, Hoyte, Christopher, and Brent, Jeffrey

Subjects

SODIUM channels, ARRHYTHMIA, DRUG overdose, PROGNOSIS, TRICYCLIC antidepressants, ACIDOSIS

Abstract

The QRS complex duration is commonly used to prognosticate severity, predict outcomes, and indicate treatment in overdose. However, literature to support this practice is mixed in tricyclic antidepressant overdoses and absent in non-tricyclic antidepressant overdoses. Our objective was to assess the validity of QRS complex duration as a prognostic marker in overdose. This was a secondary analysis of cases reported to the Toxicology Investigators Consortium between January 1, 2010, and December 31, 2022. Cases were assessed to determine the six xenobiotics most associated with QRS complex prolongation. All cases involving these six xenobiotics, regardless of QRS complex duration, constituted the study cohort. Inclusion criteria were cases of patients older than 12 years old with single-xenobiotic exposures. Clinical outcomes evaluated were seizure, ventricular dysrhythmia, metabolic acidosis, and death. Of 94,939 total cases, diphenhydramine, amitriptyline, bupropion, quetiapine, nortriptyline, and cocaine were most associated with QRS complex prolongation. Inclusion criteria were met by 4,655 cases of exposure to these xenobiotics. QRS complex prolongation was associated with increased odds ratio of seizure in all included xenobiotics, of ventricular dysrhythmia in all included xenobiotics except nortriptyline, and of metabolic acidosis or death in all included xenobiotics except nortriptyline and quetiapine. A normal QRS complex duration had a negative predictive value of greater than or equal to 93.0 percent of developing metabolic acidosis and 98.0 percent of developing a ventricular dysrhythmia or death from the xenobiotics studied. This study demonstrates that patients with QRS complex prolongation from all six xenobiotics studied had an increased prevalence and odds of developing severe outcomes. Furthermore, patients who did not develop QRS complex prolongation were unlikely to develop a ventricular dysrhythmia, metabolic acidosis, or death. These findings were noted in six xenobiotics that mechanistically can cause QRS complex prolongation through sodium channel or gap junction inhibition. Identification of patients at risk for severe outcomes after overdose can be aided by measuring the QRS complex duration. If prospectively validated, these outcomes have implications on risk stratification, disposition level of care, and appropriateness of treatments. [ABSTRACT FROM AUTHOR]

Published

2024

2. Lipid emulsion therapy during management of the critically-ill poisoned patient: a prospective cohort study.

Author

Levine, Michael, Brent, Jeffrey, Wiegand, Timothy, Maguire, Bryan, Cohen, Neta, Vaerrier, David, Beuhler, Michael, Leikin, Jerrold B., Ganetsky, Michael, Stellpflug, Samuel, Ruha, Anne-Michelle, Carey, Jennifer, Geib, Ann-Jeannette, Cao, Dazhe James, Kleinschmidt, Kurt, Vohra, Rais, Riley, Brad D., Moore, Phillip, Schwarz, Evan, and Neavyn, Mark

Subjects

*SYSTOLIC blood pressure, *INTRAVENOUS fat emulsions, *EMULSIONS, *COHORT analysis, *LONGITUDINAL method, *LIPIDS

Abstract

Despite conflicting data, intravenous lipid emulsion has emerged as a potential antidote. The "lipid sink" theory suggests that following intravenous administration of lipid, lipophilic drugs are sequestered in the vascular compartment, thereby reducing their tissue concentrations. This study sought to determine if survival is associated with the intoxicant's degree of lipophilicity. We reviewed all cases in the Toxicology Investigators Consortium's lipid sub-registry between May 2012 through December 2018. Information collected included demographics, exposure circumstances, clinical course, management, disposition, and outcome. The primary outcome was survival after lipid emulsion therapy. Survival was stratified by the log of the intoxicant's octanol-water partition coefficient. We also assessed the association between intoxicant lipophilicity and an increase in systolic blood pressure after lipid emulsion administration. We identified 134 patients, including 81 (60.4%) females. The median age was 40 years (interquartile range 21-75). One hundred and eight (80.6%) patients survived, including 45 (33.6%) with cardiac arrest during their intoxication. Eighty-two (61.2%) were hypotensive, and 98 (73.1%) received mechanical ventilation. There was no relationship between survival and the log of the partition coefficient of the intoxicant on linear analysis (P = 0.89) or polynomial model (P = 0.10). Systolic blood pressure increased in both groups. The median (interquartile range) systolic blood pressure before lipid administration was 68 (60-78) mmHg for those intoxicants with a log partition coefficient < 3.6 compared with 89 (76-104) mmHg after lipid administration. Among those drugs with a log partition coefficient > 3.6, the median (interquartile range) was 69 (60-84) mmHg before lipid and 89 (80-96) mmHg after lipid administration. Most patients in this cohort survived. Lipophilicity was not correlated with survival or the observed changes in blood pressure. The study did not address the efficacy of lipid emulsion. [ABSTRACT FROM AUTHOR]

Published

2023

3. Severe outcomes following pediatric cannabis intoxication: a prospective cohort study of an international toxicology surveillance registry.

Author

Cohen, Neta, Mathew, Mathew, Brent, Jeffrey, Wax, Paul, Davis, Adrienne L., Obilom, Cherie, Burns, Michele M., Canning, Joshua, Baumgartner, Kevin, Koons, Andrew L., Wiegand, Timothy J., Judge, Bryan, Hoyte, Christopher, Chenoweth, James A., Froberg, Blake, Farrar, Henry, Carey, Jennifer L., Hendrickson, Robert G., Hodgman, Michael, and Caravati, E. Martin

Subjects

COHORT analysis, LOGISTIC regression analysis, CANNABIS edibles, LONGITUDINAL method, CHILD patients

Abstract

An increasing number of jurisdictions have legalized recreational cannabis for adult use. The subsequent availability and marketing of recreational cannabis has led to a parallel increase in rates and severity of pediatric cannabis intoxications. We explored predictors of severe outcomes in pediatric patients who presented to the emergency department with cannabis intoxication. In this prospective cohort study, we collected data on all pediatric patients (<18 years) who presented with cannabis intoxication from August 2017 through June 2020 to participating sites in the Toxicology Investigators Consortium. In cases that involved polysubstance exposure, patients were included if cannabis was a significant contributing agent. The primary outcome was a composite severe outcome endpoint, defined as an intensive care unit admission or in-hospital death. Covariates included relevant sociodemographic and exposure characteristics. One hundred and thirty-eight pediatric patients (54% males, median age 14.0 years, interquartile range 3.7–16.0) presented to a participating emergency department with cannabis intoxication. Fifty-two patients (38%) were admitted to an intensive care unit, including one patient who died. In the multivariable logistic regression analysis, polysubstance ingestion (adjusted odds ratio = 16.3; 95% confidence interval: 4.6–58.3; P < 0.001)) and cannabis edibles ingestion (adjusted odds ratio = 5.5; 95% confidence interval: 1.9–15.9; P = 0.001) were strong independent predictors of severe outcome. In an age-stratified regression analysis, in children older than >10 years, only polysubstance abuse remained an independent predictor for the severe outcome (adjusted odds ratio 37.1; 95% confidence interval: 6.2–221.2; P < 0.001). As all children 10 years and younger ingested edibles, a dedicated multivariable analysis could not be performed (unadjusted odds ratio 3.3; 95% confidence interval: 1.6–6.7). Severe outcomes occurred for different reasons and were largely associated with the patient's age. Young children, all of whom were exposed to edibles, were at higher risk of severe outcomes. Teenagers with severe outcomes were frequently involved in polysubstance exposure, while psychosocial factors may have played a role. [ABSTRACT FROM AUTHOR]

Published

2023

4. Opioid overdoses involving xylazine in emergency department patients: a multicenter study.

Author

Love, Jennifer S., Levine, Michael, Aldy, Kim, Brent, Jeffrey, Krotulski, Alex J., Logan, Barry K., Vargas-Torres, Carmen, Walton, Sara E., Amaducci, Alexandra, Calello, Diane, Hendrickson, Robert, Hughes, Adrienne, Kurt, Anita, Judge, Bryan, Pizon, Anthony, Schwarz, Evan, Shulman, Joshua, Wiegan, Timothy, Wax, Paul, and Manini, Alex F.

Subjects

DRUG overdose, XYLAZINE, HOSPITAL emergency services, ADRENERGIC agonists, TIME-of-flight spectroscopy, EMERGENCY management

Abstract

Illicit opioids, consisting largely of fentanyl, novel synthetic opioids, and adulterants, are the primary cause of drug overdose fatality in the United States. Xylazine, an alpha-2 adrenergic agonist and veterinary tranquilizer, is being increasingly detected among decedents following illicit opioid overdose. Clinical outcomes in non-fatal overdose involving xylazine are unexplored. Therefore, among emergency department patients with illicit opioid overdose, we evaluated clinical outcome differences for patients with and without xylazine exposures. This multicenter, prospective cohort study enrolled adult patients with opioid overdose who presented to one of nine United States emergency departments between 21 September 2020, and 17 August 2021. Patients with opioid overdose were screened and included if they tested positive for an illicit opioid (heroin, fentanyl, fentanyl analog, or novel synthetic opioid) or xylazine. Patient serum was analyzed via liquid chromatography quadrupole time-of-flight mass spectroscopy to detect current illicit opioids, novel synthetic opioids, xylazine and adulterants. Overdose severity surrogate outcomes were: (a) cardiac arrest requiring cardiopulmonary resuscitation (primary); and (b) coma within 4 h of arrival (secondary). Three hundred and twenty-one patients met inclusion criteria: 90 tested positive for xylazine and 231 were negative. The primary outcome occurred in 37 patients, and the secondary outcome occurred in 111 patients. Using multivariable regression analysis, patients positive for xylazine had significantly lower adjusted odds of cardiac arrest (adjusted OR 0.30, 95% CI 0.10–0.92) and coma (adjusted OR 0.52, 95% CI 0.29–0.94). In this large multicenter cohort, cardiac arrest and coma in emergency department patients with illicit opioid overdose were significantly less severe in those testing positive for xylazine. [ABSTRACT FROM AUTHOR]

Published

2023

5. Rates and types of urine drug screen false negative results compared with confirmatory toxicology testing in major trauma patients.

Author

Weiss, Stephanie T., Veach, Laura J., McGill, William, and Brent, Jeffrey

Subjects

DRUG use testing, TOXICITY testing, CAFFEINE, DRUG abuse, LIQUID chromatography-mass spectrometry, OLDER patients

Abstract

Trauma centers are required to screen patients for alcohol use, and if necessary, intervene and refer to treatment (SBIRT). Similar screening for illicit drug use is recommended but not required. Urine drug screening (UDS) underestimates problematic substance use. This study aimed to estimate the types and rates of UDS false negatives (FN) compared to comprehensive testing by liquid chromatography-mass spectrometry (LC-MS) in trauma patients. We performed a prospective cohort study of deidentified urine samples from adult trauma and burn activation patients. Both UDS and LC-MS comprehensive testing of >200 analytes were performed by a reference laboratory on all samples. Iatrogenic medications were excluded from the FN count. Crosstab analyses were conducted for UDS versus LC-MS outcomes to establish FN types and rates. We dichotomized the results by creating an "intentionality" variable (intentional injuries by self/others versus accidental injuries). A series of crosstabs with odds ratios considered intentionality by substance class and demographics. Statistically significant variables by Chi-Square were assessed by logistic regression. Psychoactive FN were detected in 56/100 urine samples analyzed; the most frequent included anticonvulsants (primarily gabapentin, N = 13), opioid agonists (N = 12), antihistamines (primarily diphenhydramine, N = 10), and phenethylamines (primarily bupropion, N = 5). Nonpsychoactive FN were detected in 70/100 samples; the most common were nicotine (N = 33), caffeine (N = 23), acetaminophen (N = 22), and antidepressants (N = 12). Of substance classes included in the UDS and also tested by LC-MS, FN occurred for opiates (3%), amphetamines (5%) and opioids (25%). Polypharmacy was associated with fall injuries in elderly patients. Cocaine (p = 0.015) and cannabinoids (p = 0.002) were significantly associated with intentionality. Our results indicate that FN for potentially important psychoactive and nonpsychoactive substances are common when toxicologic testing is limited to routine UDS in trauma patients. We recommend expanding SBIRT in this patient population to include misuse of tobacco products, prescription analgesics, and over-the-counter antihistamines. [ABSTRACT FROM AUTHOR]

Published

2022

6. Ivermectin associated adverse events in the treatment and prevention of COVID-19 reported to the FACT pharmacovigilance project.

Author

Farah, Rita, Kazzi, Ziad, Brent, Jeffrey, Burkhart, Keith, Wax, Paul, and Aldy, Kim

Subjects

COVID-19 treatment, IVERMECTIN, VETERINARY hospitals, ACADEMIC medical centers, COVID-19, MEDICAL prescriptions

Abstract

In August 2021, the Centers for Disease Control and Prevention (CDC) released a health alert following the rapid increase in ivermectin prescriptions and reports of severe illness associated with use of products containing ivermectin for the prevention or treatment of COVID-19 infections. The United States Food and Drug Administration (FDA) and the CDC have explicitly discouraged the use of ivermectin in the prevention or treatment of COVID-19 outside of clinical trials. The study aims to describe the adverse events (AEs) related to ivermectin use for the prevention or treatment of COVID-19. This is a prospective case series of adverse events related to therapeutics used in the prevention or treatment of COVID-19 submitted to the FDA ACMT COVID-19 ToxIC (FACT) Pharmacovigilance Project sub-registry between October 2020 and December 2021. This is an ongoing toxico-surveillance system at 15 major academic medical centers in 12 states. Data collected included sociodemographics, exposure related information including dose, frequency, route, duration, and reason for taking ivermectin as well as a clinical description of the adverse event and the outcome. A total of 40 patients who developed AEs following ivermectin use were reported to FACT over 15 months. Self-medication with veterinary formulations were reported in 18/40 patients Thirty-three patients presented to emergency departments and nineteen patients were admitted to the hospital. Patients reported using ivermectin for prevention (24/40), treatment of symptoms (19/40), and for treatment of documented COVID-19 (8/40). Neurological toxicity was the most frequent finding. Fifteen patients had minor symptoms while 25 developed severe toxicity. Ivermectin use for the attempted treatment of COVID-19 has potential adverse health effects primarily related to neurological function. This is especially true when patients are self-treating with this medication and when they are using formulations intended for non-human use. [ABSTRACT FROM AUTHOR]

Published

2022

7. The serum glycolate concentration: its prognostic value and its correlation to surrogate markers in ethylene glycol exposures.

Author

Roberts, Darren M., Hoffman, Robert S., Brent, Jeffrey, Lavergne, Valéry, Hovda, Knut Erik, Porter, William H., McMartin, Kenneth E., and Ghannoum, Marc

Subjects

ETHYLENE glycol, BIOMARKERS, PROGNOSIS, ACUTE kidney failure, RECEIVER operating characteristic curves

Abstract

Ethylene glycol poisoning manifests as metabolic acidemia, acute kidney injury and death. The diagnosis and treatment depend on history and biochemical tests. Glycolate is a key toxic metabolite that impacts prognosis, but assay results are not widely available in a clinically useful timeframe. We quantitated the impact of serum glycolate concentration for prognostication and evaluated whether more readily available biochemical tests are acceptable surrogates for the glycolate concentration. The objectives of this study are to 1) assess the prognostic value of the initial glycolate concentration on the occurrence of AKI or mortality in patients with ethylene glycol exposure (prognostic study); 2) identify surrogate markers that correlate best with glycolate concentrations (surrogate study). A systematic review of the literature was performed using Medline/PubMed, EMBASE, Cochrane library, conference proceedings and reference lists. Human studies reporting measured glycolate concentrations were eligible. Glycolate concentrations were related to categorical clinical outcomes (acute kidney injury, mortality), and correlated with continuous surrogate biochemical measurements (anion gap, base excess, bicarbonate concentration and pH). Receiver operating characteristic curves were constructed to calculate the positive predictive values and the negative predictive values of the threshold glycolate concentrations that predict acute kidney injury and mortality. Further, glycolate concentrations corresponding to 100% negative predictive value for mortality and 95% negative predictive value for acute kidney injury were determined. Of 1,531 articles identified, 655 were potentially eligible and 32 were included, reflecting 137 cases from 133 patients for the prognostic study and 154 cases from 150 patients for the surrogate study. The median glycolate concentration was 11.2 mmol/L (85.1 mg/dL, range 0–38.0 mmol/L, 0–288.8 mg/dL), 93% of patients were treated with antidotes, 80% received extracorporeal treatments, 49% developed acute kidney injury and 13% died. The glycolate concentration best predicting acute kidney injury was 12.9 mmol/L (98.0 mg/dL, sensitivity 78.5%, specificity 88.1%, positive predictive value 86.4%, negative predictive value 80.9%). The glycolate concentration threshold for a 95% negative predictive value for acute kidney injury was 6.6 mmol/L (50.2 mg/dL, sensitivity 96.9%, specificity 62.7%). The glycolate concentration best predicting mortality was 19.6 mmol/L (149.0 mg/dL, sensitivity 61.1%, specificity 81.4%, positive predictive value 33.3%, negative predictive value 93.2%). The glycolate concentration threshold for a 100% negative predictive value for mortality was 8.3 mmol/L (63.1 mg/dL, sensitivity 100.0%, specificity 35.6%). The glycolate concentration correlated best with the anion gap (R2 = 0.73), followed by bicarbonate (R2 = 0.57), pH (R2 = 0.50) and then base excess (R2 = 0.25), while there was no correlation between the glycolate and ethylene glycol concentration (R2 = 0.00). These data can assist clinicians in planning treatments such as extracorporeal treatments and prognostication. Potentially, they may also provide some reassurance regarding when extracorporeal treatments can be delayed while awaiting the results of further testing in patients in whom ethylene glycol poisoning is suspected but not yet confirmed. This systematic review demonstrates that the glycolate concentration predicts mortality (unlikely if <8 mmol/L [61 mg/dL]). The anion gap is a reasonable surrogate measurement for glycolate concentration in the context of ethylene glycol poisoning. The findings are mainly based on published retrospective data which have various limitations. Further prospective validation studies are of interest. [ABSTRACT FROM AUTHOR]

Published

2022

8. Predictors of severe outcome following opioid intoxication in children.

Author

Cohen, Neta, Mathew, Mathew, Davis, Adrienne, Brent, Jeffrey, Wax, Paul, Schuh, Suzanne, Freedman, Stephen B., Froberg, Blake, Schwarz, Evan, Canning, Joshua, Tortora, Laura, Hoyte, Christopher, Koons, Andrew L., Burns, Michele M., McFalls, Joshua, Wiegand, Timothy J., Hendrickson, Robert G., Judge, Bryan, Quang, Lawrence S., and Hodgman, Michael

Subjects

CHILDREN'S hospitals, INTENSIVE care units, OPIOIDS, OPIOID epidemic, LOGISTIC regression analysis, MEDICAL consultation, POISONS

Abstract

While the opioid crisis has claimed the lives of nearly 500,000 in the U.S. over the past two decades, and pediatric cases of opioid intoxications are increasing, only sparse data exist regarding risk factors for severe outcome in children following an opioid intoxication. We explore predictors of severe outcome (i.e., intensive care unit [ICU] admission or in-hospital death) in children who presented to the Emergency Department with an opioid intoxication. In this prospective cohort study we collected data on all children (0–18 years) who presented with an opioid intoxication to the 50 medical centers in the US and two international centers affiliated with the Toxicology Investigators Consortium (ToxIC) of the American College of Medical Toxicology, from August 2017 through June 2020, and who received a bedside consultation by a medical toxicologist. We collected relevant demographic, clinical, management, disposition, and outcome data, and we conducted a multivariable logistic regression analysis to explore predictors of severe outcome. The primary outcome was a composite severe outcome endpoint, defined as ICU admission or in-hospital death. Covariates included sociodemographic, exposure and clinical characteristics. Of the 165 (87 females, 52.7%) children with an opioid intoxication, 89 (53.9%) were admitted to ICU or died during hospitalization, and 76 did not meet these criteria. Seventy-four (44.8%) children were exposed to opioids prescribed to family members. Fentanyl exposure (adjusted OR [aOR] = 3.6, 95% CI: 1.0–11.6; p = 0.03) and age ≥10 years (aOR = 2.5, 95% CI: 1.2–4.8; p = 0.01) were independent predictors of severe outcome. Children with an opioid toxicity that have been exposed to fentanyl and those aged ≥10 years had 3.6 and 2.5 higher odds of ICU admission or death, respectively, than those without these characteristics. Prevention efforts should target these risk factors to mitigate poor outcomes in children with an opioid intoxication. [ABSTRACT FROM AUTHOR]

Published

2022

9. Failure of chelator-provoked urine testing results to predict heavy metal toxicity in a prospective cohort of patients referred for medical toxicology evaluation.

Author

Weiss, Stephanie T., Campleman, Sharan, Wax, Paul, McGill, William, and Brent, Jeffrey

Subjects

URINALYSIS, POISONING, MEDICAL personnel, TOXICOLOGY, CHRONIC toxicity testing, MEDICAL societies, HEAVY metal toxicology, CHELATING agents

Abstract

Provoked urine testing (PUT), involving chelating agent administration prior to measuring urine metal excretion levels, is used by some alternative health care practitioners to diagnose patients with heavy metal poisoning. Multiple medical societies have advised against this practice due to its presumed unreliability, expense, and lack of validation. However, no prospective study of the predictive value of PUT for heavy metal poisoning has been undertaken. This study utilized the Toxicology Consortium's prospective case registry to evaluate the reliability of PUT for diagnosing heavy metal poisoning. Inclusion criteria were toxicology clinic patients with PUT results who were subsequently evaluated by a board-certified medical toxicologist and had a determination made regarding whether their signs and symptoms were likely related or unrelated to toxicologic exposures. The primary outcome was the positive predictive value of PUT for heavy metal toxicity as diagnosed by the evaluating medical toxicologist. Patients presenting to participating toxicology clinics without PUT served as a comparison group. 74 of 106 cases presenting with PUT results met inclusion criteria and were analyzed. 15 cases were determined by the examining toxicologist to be likely related to a toxicologic exposure. Only three cases were found to be related to heavy metal exposure, giving a positive predictive value of 4.3%. 20.2% of patients with PUT were found to have signs or symptoms related to any toxicologic exposure, compared to 14.3% of clinic patients without PUT. Demographics of toxicology clinic patients with and without PUT results were not significantly different except for age. Our results provide empiric support that PUT is an inaccurate predictor of a diagnosis of heavy metal poisoning by a board-certified medical toxicologist. Given the inability to properly interpret PUT results along with the increased cost burden and risk of false positives, PUT should not be performed. [ABSTRACT FROM AUTHOR]

Published

2022

10. Identification of a novel opioid, N-piperidinyl etonitazene (etonitazepipne), in patients with suspected opioid overdose.

Author

Calello, Diane P., Aldy, Kim, Jefri, Mohamed, Nguyen, Tuyet-Anh T., Krotulski, Alex, Logan, Barry, Brent, Jeffrey, Wax, Paul, Walton, Sara, and Manini, Alex F.

Subjects

HEROIN, DRUG overdose, DRUGS of abuse, OPIOIDS, INTENSIVE care units, PHENACETIN

Abstract

Novel opioids in the illicit drug supply, such as the "nitazene" group of synthetic opioids, present an ongoing public health problem due to high potency and respiratory depressant effects. We describe three patients in whom N-piperidinyl etonitazene, a compound not previously reported in human exposure, was detected after suspected opioid overdose. Other substances that these patients tested for included fentanyl, cocaine, levamisole, phenacetin, benzoylecgonine, para-fluorofentanyl, presumptive heroin (tested as 6-monoacetylmorphine (6-MAM), morphine, and codeine), and tramadol. This is a case series of patients with acute opioid overdose enrolled in an ongoing multicenter prospective cohort study. Data collected included reported substance use, clinical course, naloxone dose and response, outcome, and analytes detected in biological samples. Between October 6, 2020 and October 31, 2021, 1006 patients were screened and 412 met inclusion criteria. Of these, three patients (age 33–55) tested positive for N-piperidinyl etonitazene at one site in New Jersey over a period of three days in July 2021. Two patients reported the use of cocaine; one reported the use of heroin and alprazolam. All three patients received naloxone with improvement in their mental status (2 milligrams (mg) intranasally (IN); 8 mg IN; 0.08 mg intravenous (IV)). Two of three received subsequent doses for recurrence of opioid toxicity (0.4–0.6 mg IV). One patient was diagnosed with pneumonia and admitted to the intensive care unit, one was discharged from the Emergency Department (ED), and one used additional drug while in the ED and required admission for a naloxone infusion. None developed organ damage or sequelae. These cases represent a local outbreak of a novel "nitazene" opioid. Public health toxicosurveillance should incorporate routine testing of this emerging class of synthetic compounds in the illicit drug supply. [ABSTRACT FROM AUTHOR]

Published

2022

11. Fatalities in poisoned patients managed by medical toxicologists.

Author

Friedman, Nir, Shoshani-Levy, Mirit, Brent, Jeffrey, Wax, Paul, Campleman, Sharan L., and Finkelstein, Yaron

Subjects

OPIOID analgesics, ANTIPYRETICS, TOXICOLOGISTS, MEDICAL care, CENTRAL nervous system, SELF-poisoning

Abstract

Background: Poisoning is a leading cause of injury-related death in the United States. The Toxicology Investigators Consortium (ToxIC) Case Registry, established by the American College of Medical Toxicology, prospectively captures patients who were directly cared for and managed at the bedside by medical toxicology services. We sought to describe exposure cases who presented to Emergency Departments (EDs) across ToxIC sites, received direct bedside care by medical toxicologists; however, the intoxication resulted in fatality. Methods: We identified all cases in the ToxIC Case Registry that resulted in fatality after hospital presentation over the 6-year study period. We collected data on patient demographics and clinical information including age group, sex, circumstances of exposure, route of exposure, substances involved, presenting signs and symptoms and management prior to death. Results: Of 44,567 recorded cases in the registry over the study period, 268 (0.6%) fatalities met the inclusion criteria and comprise the study cohort. There was no sex predominance (138 females; 51.5%) and 27 (10.1%) were pediatric fatalities. In 195 (72.7%) patients, exposure was intentional. In 175 (65.3%) patients, fatality was associated with exposure to pharmaceuticals. The leading substances resulting in death were non-opioid analgesics, followed by opioids (72% prescription opioids), cardiovascular medications, sedatives, antipsychotics, antidepressants, and sympathomimetics. At time of consult, the central nervous system was the most common system affected in both fatal and non-fatal cases. Compared with non-fatal ToxIC cases (n = 44,299), fatal cases involved significantly less children (27.7% vs. 10.1%, respectively; p <.001), and were managed more aggressively (e.g., mechanical ventilation 8.3% vs. 69.8%, p <.001). Both non-opioid analgesics (25.3% vs. 14.7%; p <.001) and opioids (17.8% vs. 7.5%; p <.001) were significantly more likely to be ingested in fatal compared with non-fatal cases, although analgesics, opioids, and non-opioids, were the most common agents implicated in both groups. Conclusions: Most ToxIC registry exposures resulting in death involve intentional exposure, without sex predominance. One in 10 fatalities involved a child. Analgesics, non-opioids, and opioids are the most commonly implicated agents in both fatal and non-fatal intoxications, which highlights the centrality of these agents as major sources of both morbidity and mortality. [ABSTRACT FROM AUTHOR]

Published

2020

12. Response to Ok S-H, Wiedmer SK, Sohn J-T. Comment on "Lipid emulsion therapy during management of the critically-ill poisoned patient: a prospective cohort study".

Author

Levine, Michael, Beuhler, Michael, Brent, Jeffrey, and Finkelstein, Yaron

Subjects

EMULSIONS, INTRAVENOUS fat emulsions, SYSTOLIC blood pressure, COHORT analysis, LONGITUDINAL method, BLOOD pressure, LIPIDS

Abstract

This letter is a response to concerns raised by Ok and colleagues regarding the use of the octanol/water partition coefficient (Log P) in a previous manuscript. The authors respectfully disagree with the suggestion that Log D is a more reasonable descriptor than Log P. They argue that Log D changes depending on pH, which is not continuously measured in clinical practice and therefore impractical to use. The authors analyzed the data using both Log P and Log D and found almost identical findings, indicating that substance lipophilicity was not associated with patient survival. They also noted that the improvement in systolic blood pressure after the administration of intravenous lipid emulsion was independent of substance lipophilicity. However, due to the multiple interventions performed simultaneously in clinical practice, it is difficult to draw conclusions on the causal and temporal associations between lipid emulsion and blood pressure. The authors disclose no potential conflict of interest. [Extracted from the article]

Published

2023

13. Consensus statements on the approach to patients in a methanol poisoning outbreak.

Author

Hassanian-Moghaddam, Hossein, Zamani, Nasim, Roberts, Darren M., Brent, Jeffrey, McMartin, Kenneth, Aaron, Cynthia, Eddleston, Michael, Dargan, Paul I., Olson, Kent, Nelson, Lewis, Bhalla, Ashish, Hantson, Philippe, Jacobsen, Dag, Megarbane, Bruno, Balali-Mood, Mahdi, Buckley, Nicholas A., Zakharov, Sergey, Paasma, Raido, Jarwani, Bhavesh, and Mirafzal, Amirhossein

Subjects

ANTIDOTES, METHANOL, ALCOHOLIC beverage manufacturing, POISONING, OPEN-ended questions

Abstract

Background: Methanol poisoning is an important cause of mortality and morbidity worldwide. Although it often occurs as smaller sporadic events, epidemic outbreaks are not uncommon due to the illicit manufacture and sale of alcoholic beverages. Objective: We aimed to define methanol poisoning outbreak (MPO), outline an approach to triaging an MPO, and define criteria for prioritizing antidotes, extracorporeal elimination treatments (i.e., dialysis), and indications for transferring patients in the context of an MPO. Methods: We convened a group of experts from across the world to explore geographical, socio-cultural and clinical considerations in the management of an MPO. The experts answered specific open-ended questions based on themes aligned to the goals of this project. This project used a modified Delphi process. The discussion continued until there was condensation of themes. Results: We defined MPO as a sudden increase in the number of cases of methanol poisoning during a short period of time above what is normally expected in the population in that specific geographic area. Prompt initiation of an antidote is necessary in MPOs. Scarce hemodialysis resources require triage to identify patients most likely to benefit from this treatment. The sickest patients should not be transferred unless the time for transfer is very short. Transporting extracorporeal treatment equipment and antidotes may be more efficient. Conclusion: We have developed consensus statements on the response to a methanol poisoning outbreak. These can be used in any country and will be most effective when they are discussed by health authorities and clinicians prior to an outbreak. [ABSTRACT FROM AUTHOR]

Published

2019

14. Poisoning with malicious or criminal intent: characteristics and outcome of patients presenting for emergency care.

Author

Gauthey, Magali, Capua, Maya, Brent, Jeffrey, and Finkelstein, Yaron

Subjects

POISONING, CRIMINAL intent, EMERGENCY medicine, TOXICOLOGY, SYMPATHOMIMETIC agents, OPIOIDS

Abstract

Background: Poisoning is the leading cause of injury-related death in the USA. Poisoning with malicious or criminal intent is uncommon, and poorly characterized. Objectives: To explore substances, patients' demographics, clinical presentation, management and outcome in victims of malicious poisoning in the USA. Methods: Using the 47 participating sites of the Toxicology Investigators Consortium (ToxIC) Registry, a North American research consortium, we conducted an observational study of a prospectively collected cohort. We identified all patients exposed to malicious poisoning who had received medical toxicology consultation between January 2014 and June 2017. Clinical and demographic data were collected including age, sex, agents of exposure, clinical manifestations, treatment, disposition and outcome. Results: We identified 60 patients who presented to the emergency department with malicious poisoning, of whom 21 (35%) were children. Among 21 children, 17 (81%) were younger than 2 years. There was no sex dominance among patients. The main substances involved in pediatric patients were sympathomimetics (35%) and opioids (19%). In adults, a more varied panel of offending substances was used, with no specific dominant toxidrome. Children received more treatment interventions compared to adults (overall treatment 81% versus 46% [p = 0.0132]; mechanical ventilation: 29% versus 5% [p = 0.0176], respectively). Three (5%) patients died (two children, one adult). Conclusions: Poisonings with malicious intent are uncommon; they are disproportionally directed towards infants, frequently resulting in severe injury and carry relatively high mortality. [ABSTRACT FROM AUTHOR]

Published

2019

15. Loperamide misuse to avoid opioid withdrawal and to achieve a euphoric effect: high doses and high risk.

Author

Lee, Vincent R., Vera, Ariel, Alexander, Andreia, Ruck, Bruce, Nelson, Lewis S., Wax, Paul, Campleman, Sharan, Brent, Jeffrey, and Calello, Diane P.

Subjects

LOPERAMIDE, DRUG overdose, OPIOIDS, ELECTROCARDIOGRAPHY, CARDIOTOXICITY, DRUG dosage

Abstract

Introduction: Loperamide is a readily accessible nonprescription medication that is increasingly being used surreptitiously as an opioid substitute to alleviate the symptoms of acute opioid withdrawal. The objective of this study was to determine the clinical characteristics of patients with loperamide misuse and toxicity. Methods: The ToxIC registry, a nationwide, prospectively collected cohort of patients evaluated by medical toxicologists was searched from November 2011-December 2016 for patients with loperamide exposure. Each record was reviewed to determine the circumstances, dose, clinical presentations, treatment, and outcomes associated with loperamide use. Results: Twenty-six cases were identified, and both the absolute number and relative proportion of overall cases in the ToxIC registry increased annually. The median age was 27 and 54% were male. Of cases with known intent (n = 18), 12(67%) were misuse/abuse, 3(17%) were self-harm/suicide, and 3(17%) were pediatric exploratory ingestions. Circumstances for misuse included taking higher doses than labeled (n =7), avoiding withdrawal (n = 6), and gaining a pleasurable sensation (n =4). The dose was reported in nine cases and ranged from 4 mg to 400 mg. In patients seeking to avoid withdrawal doses were 160-400 mg/day; the most common reported dose was 200 mg. Reported ECG abnormalities included 10 cases of prolonged QTc (>500 ms), which consisted of misuse/abuse (n =6) and self-harm (n =1) exposures; six prolonged QRS (>120 ms); two first degree AV block; seven ventricular dysrhythmias, five of which were single-agent exposures. All but one ECG demonstrated prolonged QTc with a range of 566-749 ms. All patients with dysrhythmias in which dose were reported ingested ≥200 mg. Conclusions: The majority of patients had loperamide toxicity due to misuse/abuse, in-line with national trends. In patients avoiding withdrawal, doses >100 mg were observed. When taken in large doses (>200 mg), loperamide may cause significant cardiovascular effects, including QTc-prolongation and ventricular dysrhythmias. [ABSTRACT FROM AUTHOR]

Published

2019

16. Acute adverse events associated with the administration of Crotalidae polyvalent immune Fab antivenom within the North American Snakebite Registry.

Author

On Behalf of the ToxIC North American Snakebite Registry Group, Kleinschmidt, Kurt, Wax, Paul, Ruha, Anne-Michelle, Campleman, Sharan, and Brent, Jeffrey

Subjects

PIT vipers, MULTIVALENT molecules, IMMUNOLOGIC diseases, ANTIVENINS, SNAKEBITES

Abstract

Background: Crotalidae Polyvalent Immune Fab (Fab Antivenom) is the primary Viperid antivenom used in the United States since 2000. Adverse event data associated with its use are limited. The purpose of this study is to describe the prevalence of acute adverse events associated with the use of Fab antivenom. Methods: The American College of Medical Toxicology's Toxicology Investigators Consortium maintains a prospective case registry of poisoned and envenomated patients managed by medical toxicologists at the bedside. This registry includes the North American Snakebite sub-registry. We performed a review of 438 cases entered into the Snakebite sub-registry. Results: A total of 373 (85.2%) received at least one vial of Fab Antivenom. Forty percent were children. Adverse events occurred in 10 patients (2.7%) of whom six were adults. Rash was the most common adverse event. More severe adverse events (hypotension, bronchospasm, and/or angioedema) occurred in four (1.1%) patients. Prophylaxis was administered prior to Fab antivenom in 4.0%. Eight patients received various treatments for their adverse events. Neither the initial number of Fab antivenom vials, atopic history, nor prior envenomation correlated with the prevalence of adverse events. Discussion: This prevalence of adverse events was lower than in previous studies and in a meta-analysis of 11 studies. The types of adverse events and treatments used are consistent with those in previous reports. There were no prior reports of prophylaxis use with which to compare. Conclusion: The prevalence of Fab antivenom adverse events in the North American Snakebite Registry was 2.7%. [ABSTRACT FROM AUTHOR]

Published

2018

17. The authors reply – predictors of severe outcome following opioid intoxication in children.

Author

Cohen, Neta, Aldy, Kim, Brent, Jeffrey, Wax, Paul, and Finkelstein, Yaron

Subjects

OPIOIDS, ABANDONED children, POISONS, FENTANYL, URBAN hospitals, OPIOID analgesics, MEDICAL consultation

Abstract

Lastly, if the frontline physicians were comfortable managing an intoxicated child with naloxone and other measures, or if they felt that a phone consult by the regional poison information center is sufficient, a medical toxicology consultation at the bedside may not be requested, and the child will not be eligible or captured in the dedicated registry. Notably, in our series only half manifested classic opioid toxidrome, and the other half manifested a mixed clinical picture, reflecting a complex multi-drug exposure, which may have driven the medical toxicology consultation request [[2]]. The authors reply - predictors of severe outcome following opioid intoxication in children. [Extracted from the article]

Published

2022

18. Water-based solutions are the best decontaminating fluids for dermal corrosive exposures: A mini review*.

Author

Brent, Jeffrey

Subjects

*SKIN infections, *CORROSION & anti-corrosives, *SOLUTION (Chemistry), *DECONTAMINATION (From gases, chemicals, etc.), *POLLUTION, *HYDROFLUORIC acid

Abstract

Aim. The intention is to assess whether the fundamental principle ('the solution to pollution is dilution') should be the guide for the initial medical management of corrosive dermal exposures. Methods. The US National Library of Medicine Pubmed database was searched utilizing all combinations of the search terms 'decontamination', 'corrosive', and 'dermal'. A separate search was done specifically related to hydrofluoric acid. These searches found 69 relevant papers. Results. Only four controlled clinical studies comparing early and intensive water decontamination with no or less dilution treatment have been published on human corrosive dermal exposures. Although the authors' conclusion in the first study of 273 patients was that those that had more intensive water irrigation tended to have less time to skin grafting and shorter periods of hospitalization, the results were not statistically significant. In the second study of 51 patients, those who had 'adequate' decontamination (immediate dilution or neutralization therapy) had shortened length of stay (7.2 vs. 16.2 days), lower mortality (9.5% vs. 21%), and fewer skin grafts (19% vs. 36%) despite having slightly greater burn surface area (19.7% vs. 17.2%). However, no statistical analysis was provided. The third and fourth studies were conducted in the same center. In the third study of 35 patients, those who had 'immediate' water lavage (done within 10 min of exposure and continued for at least 15 min) had significantly fewer burns that progressed to full thickness (12.5% vs. 63%; p < 0.01) and significantly shorter mean hospital stays (7.7 days vs. 20.5 days; p < 0.01) than those who did not, despite the mean total burn surface area being twice as large in the adequate water decontamination group (12% vs. 6%; p < 0.05). In the fourth study of 83 patients (35 of whom had been reported in the previous study), those who had copious water lavage within 3 min of injury were less likely to progress to full thickness burns (13.5% vs. 60.8%; p < 0.01), had fewer delayed complications (5.4% vs. 30.4%; p < 0.01) and shorter lengths of stay (6.2 vs. 22 days; p < 0.01), compared with those who did not. In a further study, water was compared to the proprietary agent Diphoterine® in a controlled prospective cohort study of 180 dermal alkali exposures. The Diphoterine® first group was decontaminated significantly faster than the water first group (median times to irrigation 1 vs. 5 min; p < 0.001). No analysis adjusted for time to decontamination was provided, so the study demonstrated that only those individuals who decontaminated early did better than those who decontaminated later. Conclusions. The data support water as the best decontaminating solution. It has been shown to be efficacious in clinical trials, is widely available, and inexpensive. [ABSTRACT FROM AUTHOR]

Published

2013

19. Dilemmas about the toxicological consequences of metal-on-metal hip prostheses - What we do and do not know, and what we should do?

Author

Brent, Jeffrey and Devlin, John J.

Subjects

*ARTIFICIAL hip joints, *MEDICAL periodicals, *TOXICOLOGY of chromium, *METALS in medicine, *MEDICAL research

Abstract

The author reflects his views on debate regarding the toxicological consequences of metal-on-metal hip prostheses (MOM-HPs). He mentions that various publications of potential adverse systemic events associated with MOM-HPs are anecdotal and fail to explain the relation of exposure of cobalt and chromium with the effects observed in a patient. He cites a study which elucidates the level of concern about patients with MOM-HP-related elevated blood or serum ion concentrations.

Published

2013

20. Fomepizole for the treatment of pediatric ethylene and diethylene glycol, butoxyethanol, and methanol poisonings.

Author

Brent, Jeffrey

Subjects

*FOMEPIZOLE, *POISONING, *ETHYLENE glycol, *METHANOL, *DIETHYLENE glycol, *BUTOXYETHANOL, *ACIDOSIS, *DRUG therapy, *THERAPEUTICS

Abstract

Introduction. The use and clinical efficacy of the alcohol dehydrogenase inhibitor fomepizole is well established for the treatment of ethylene glycol and methanol poisonings in adults. Methods. A computerized search of the U.S. National Academy of medicine and EMBase databases was undertaken to identify published cases of patients treated with fomepizole. This search strategy identified 14 published cases related to the topic of this review: 10 due to ethylene glycol poisoning, 1 due to diethylene glycol poisoning, 1 due to butoxyethanol ingestion, and 2 due to methanol poisoning. The median age of these cases was 5.5 years old. Fomepizole in glycol and glycol ether poisoning. For the 10 ethylene glycol poisoned patients, the median recorded values of their arterial pH was 7.27 (range 7.03-7.38), serum bicarbonate concentration was 13 mEq/L (range 2-25), and ethylene glycol concentration was 2,140 mg/L (range 130-3,840). Eight of these patients were not hemodialyzed. The eight patients who were not hemodialyzed had ethylene glycol concentrations as high as 3,500 mg/L and serum bicarbonate concentrations as low as 4 mEq/L. All 10 patients had resolution of their metabolic acidosis and recovered without sequelae. The half-times of ethylene glycol elimination ranged from 9 to 15 h during fomepizole therapy, which is faster than the 19.7 h reported in adults. The two patients who ingested diethylene glycol or butoxyethanol all recovered without sequelae. The patient who ingested the butoxyethanol had a serum bicarbonate concentration of 13 mEq/L and was not hemodialyzed. Fomepizole in methanol poisoning. One of the two children who ingested methanol was hemodialyzed. Both cases had a similar degree of severity. Does fomepizole obviate the need for hemodialysis? Based on the experience reviewed herein it appears that, as in adults, hemodialysis may not be necessary in most cases of pediatric ethylene glycol poisoning if treated with fomepizole. Fomepizole pharmacokinetics. Plasma fomepizole concentrations were measured in three cases and were found to be therapeutic with apparent Michaelis-Menton kinetics, having a zero-order elimination rate of 0.6-1 mg/L/h at higher concentrations and a first-order elimination with an apparent elimination half-time of 3.9 h at lower concentrations. Fomepizole regimen. Most cases used the current U.S.-approved regimen. Adverse effects of fomepizole. The one adverse effect reported during fomepizole therapy was transient nystagmus in a 6-year-old with a serum ethylene glycol concentration of 130 mg/L and a serum bicarbonate concentration of 2 mEq/L; it is likely that ethylene glycol itself was the cause. Comparison of fomepizole with ethanol therapy. Two cases were originally treated with ethanol but switched to fomepizole because of adverse effects. In both cases, the adverse reactions to ethanol resolved once fomepizole treatment was initiated. Conclusions. The limited data available suggest that fomepizole, using the same dosage regimen as that used for adults, is efficacious and well tolerated in pediatric patients. In many cases of pediatric ethylene glycol poisoning treated with fomepizole, hemodialysis may not be necessary despite high concentrations and the presence of metabolic acidosis. [ABSTRACT FROM AUTHOR]

Published

2010

21. 2005 Louis Roche Lecture, Professional Societies and Evidence-Based Clinical Toxicology Delivered at the XXV International Congress of the European Association of Poisons Centres and Clinical Toxicologists Berlin, Germany.

Author

Brent, Jeffrey

Subjects

*CLINICAL toxicology, *CLINICAL medicine

Abstract

The article presents a speech by Jeffrey Brent, University of Colorado toxicology professor, delivered at the 25th International Congress of the European Association of Poisons Centres and Clinical Toxicologists in 2005. He discusses the contributions of Louis Roche to clinical toxicology. He emphasizes the importance of widespread access to both preventive and therapeutic care.

Published

2005

22. Initiation of a medical toxicology consult service at a tertiary care children's hospital.

Author

Wang, George Sam, Monte, Andrew, Hatten, Benjamin, Brent, Jeffrey, Buchanan, Jennie, and Heard, Kennon J.

Subjects

TOXICOLOGY, TERTIARY care, CHILDREN'S health, MEDICAL care, HOSPITAL medical staff

Abstract

Currently, only 10% of board-certified medical toxicologists are pediatricians. Yet over half of poison center calls involve children < 6 years, poisoning continues to be a common pediatric diagnosis and bedside toxicology consultation is not common at children's hospitals. In collaboration with executive staff from Department of Pediatrics and Emergency Medicine, regional poison center, and our toxicology fellowship, we established a toxicology consulting service at our tertiary-care children's hospital. There were 139 consultations, and the service generated 13 consultations in the first month; median of 11 consultations per month thereafter (range 8–16). The service increased pediatric cases seen by the fellowship program from 30 to 94. The transition to a consult service required a culture change. Historically, call center advice was the mainstay of consulting practice and the medical staff was not accustomed to the availability of bedside medical toxicology consultations. However, after promotion of the service and full attending and fellowship coverage, consultations increased. In collaboration with toxicologists from different departments, a consultation service can be rapidly established. The service filled a clinical need that was disproportionately utilized for high acuity patients, immediately utilized by the medical staff and provided a robust pediatric population for the toxicology fellowship. [ABSTRACT FROM PUBLISHER]

Published

2015

23. Aluminum phosphide intoxication mimicking ischemic heart disease led to unjustified treatment with streptokinase.

Author

Soltaninejad, Kambiz, Shadnia, Shahin, Ziyapour, Behrad, and Brent, Jeffrey

Subjects

LETTERS to the editor, ALUMINUM phosphide

Abstract

A letter to the editor about aluminum phosphide poisoning is presented.

Published

2009

24. Dermal decontamination for corrosive exposures.

Author

Brent, Jeffrey

Subjects

*CHEMICAL burns, *ALKALIES, *THERAPEUTICS

Abstract

A letter to the editor is presented in response to the article "Diphoterine for alkali chemical splashes to the skin at alumina refineries" by A.M. Donoghue published in a 2010 issue.

Published

2014

25. A Review of: “Medical Toxicology”.

Author

Brent, Jeffrey

Subjects

*TOXICOLOGY, *NONFICTION

Abstract

Reviews the book "Medical Toxicology," 3rd edition, edited by Richard C. Dart et al.

Published

2006

26. A Review of: “Uneasy Alchemy: Citizens and Experts in Louisiana's Chemical Corridor Disputes.”.

Author

Brent, Jeffrey

Subjects

*ALCHEMY, *NONFICTION

Abstract

Reviews the book "Uneasy Alchemy: Citizens and Experts in Louisiana's Chemical Corridor Disputes," by Barbara L. Allen.

Published

2006

27. A Review of: “Greenberg's Text Atlas of Emergency Medicine”.

Author

Brent, Jeffrey

Subjects

*EMERGENCY medicine, *NONFICTION

Abstract

Reviews the book "Greenberg's Text Atlas of Emergency Medicine," by Michael I. Greenberg.

Published

2005