228 results on '"Hoegberg, Lotte"'
Search Results
2. Contributors
- Author
-
Barbuto, Alexander F., primary, Bateman, D. Nicholas, additional, Bebarta, Vikhyat S., additional, Bentur, Yedidia, additional, Boyer, Edward W., additional, Brent, Jeffrey, additional, Brown, Mary Jean, additional, Burns, Michele M., additional, Dawson, Andrew, additional, Deng, Jou-Fang, additional, Descamps, Anne-Marie, additional, Desel, Herbert, additional, Dufol, Ana Ferrer, additional, Erickson, Timothy B., additional, Garnier, Robert, additional, Gaviola, Gabriel C., additional, Goldfarb, Yu. S., additional, Goldman, Rose, additional, Haines, John, additional, Hauptman, Marissa, additional, Hoegberg, Lotte C.G., additional, Howland, Mary Ann, additional, Jian, Xiangdong, additional, Kunzler, Nathan, additional, Kupferschmidt, Hugo, additional, Locatelli, Carlo Alessandro, additional, Maddry, Joseph K., additional, Makalinao, Irma Reyes, additional, McMartin, Kenneth E., additional, Mégarbane, Bruno, additional, Ng, Patrick C., additional, Nguyen, Nguyen Trung, additional, Ostapenko, Yu. N., additional, Panganiban, Lynn Crisanta del Rosario, additional, Pelclova, Daniela, additional, Perelman, Ronald O., additional, Proudfoot, Alex, additional, Rague, John, additional, van Riel, Antoinette, additional, Roh, Hyung-Keun, additional, Sriapha, Charuwan, additional, Stürer, Andreas, additional, Tempowski, Joanna, additional, Toomey, David, additional, Vandijck, Dominique, additional, de Vries, Irma, additional, Wananukul, Winai, additional, Whyte, Ian, additional, Woolf, Alan D., additional, Wright, Nicole, additional, Xarau, Santiago Nogué, additional, Yang, Chen-Chang, additional, and Zeng, Mei, additional
- Published
- 2022
- Full Text
- View/download PDF
3. Amitriptyline accumulation in tissues after coated activated charcoal hemoperfusion—a randomized controlled animal poisoning model
- Author
-
Jansen, Tejs, Hoegberg, Lotte C. G., Eriksen, Thomas, Dalhoff, Kim P., Belhage, Bo, and Johansen, Sys S.
- Published
- 2019
- Full Text
- View/download PDF
4. Adverse effects from selected antidotes commonly used in poisonings
- Author
-
Hoegberg, Lotte C.G. and Boegevig, Soeren
- Published
- 2021
- Full Text
- View/download PDF
5. Extracorporeal Treatment for Salicylate Poisoning: Systematic Review and Recommendations From the EXTRIP Workgroup
- Author
-
Anseeuw, Kurt, Bhalla, Ashish, Burdmann, Emmanuel A., Calello, Diane P., Dargan, Paul I., Decker, Brian S., Goldfarb, David S., Galvo, Tais, Hoegberg, Lotte C., Laliberté, Martin, Li, Yi, Liu, Kathleen D., MacLaren, Robert, Mactier, Robert, Mégarbane, Bruno, Mowry, James B., Phan, Véronique, Roberts, Darren M., Wiegand, Timothy J., Winchester, James F., Yates, Christopher, Juurlink, David N., Gosselin, Sophie, Kielstein, Jan T., Ghannoum, Marc, Lavergne, Valéry, Nolin, Thomas D., and Hoffman, Robert S.
- Published
- 2015
- Full Text
- View/download PDF
6. Tsujikawa and Lipid Emulsion
- Author
-
Wang, Josh J., Villeneuve, Eric, Gosselin, Sophie, Smolinske, Susan C., Hoegberg, Lotte C. G., and Hoffman, Robert S.
- Published
- 2018
- Full Text
- View/download PDF
7. Extracorporeal treatments for isoniazid poisoning: Systematic review and recommendations from the EXTRIP workgroup
- Author
-
Mowry, James, Shepherd, Greene, Hoffman, Robert, Lavergne, Valery, Gosselin, Sophie, Nolin, Thomas, Vijayan, Anitha, Kielstein, Jan, Roberts, Darren, Ghannoum, Marc, Alhatali, Badria, Anseeuw, Kurt, Bird, Steven, Berling, Ingrid, Bouchard, Josée, Bunchman, Timothy, Calello, Diane, Chin, Paul, Doi, Kent, Galvao, Tais, Goldfarb, David, Hassanian, Hossein, Hoegberg, Lotte, Kallab, Siba, Kebede, Sofia, Lewington, Andrew, Li, Yi, Macedo, Etienne, Maclaren, Rob, Mégarbane, Bruno, Ostermann, Marlies, Peng, Ai, Roy, Jean‐philippe, Walsh, Steven, Wong, Anselm, Wood, David, Yates, Christopher, Service de Réanimation Médicale et Toxicologique [Hôpital Lariboisière], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpital Lariboisière-Fernand-Widal [APHP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Optimisation thérapeutique en Neuropsychopharmacologie (OPTeN (UMR_S_1144 / U1144)), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris Cité (UPCité), Extracorporeal Treatments in Poisoning workgroup: Badria Alhatali, Kurt Anseeuw, Steven Bird, Ingrid Berling, Josée Bouchard, Timothy E Bunchman, Diane P Calello, Paul K Chin, Kent Doi, Tais Galvao, David S Goldfarb, Hossein Hassanian, Lotte C Hoegberg, Siba Kallab, Sofia Kebede, Andrew Lewington, Yi Li, Etienne M Macedo, Rob MacLaren, Bruno Megarbane, Marlies E Ostermann, Ai Peng, Jean-Philippe Roy, Steven J Walsh, Anselm Wong, David M Wood, Christopher Yates, and Mégarbane, Bruno
- Subjects
0301 basic medicine ,medicine.medical_specialty ,medicine.medical_treatment ,030106 microbiology ,030204 cardiovascular system & hematology ,[SDV.MHEP.PSR]Life Sciences [q-bio]/Human health and pathology/Pulmonology and respiratory tract ,Extracorporeal ,03 medical and health sciences ,0302 clinical medicine ,[SDV.MHEP.CSC]Life Sciences [q-bio]/Human health and pathology/Cardiology and cardiovascular system ,Renal Dialysis ,[SDV.MHEP.MI]Life Sciences [q-bio]/Human health and pathology/Infectious diseases ,Internal medicine ,Isoniazid ,medicine ,Animals ,Humans ,Pharmacology (medical) ,Dosing ,Dialysis ,[SDV.MHEP.ME] Life Sciences [q-bio]/Human health and pathology/Emerging diseases ,[SDV.MHEP.ME]Life Sciences [q-bio]/Human health and pathology/Emerging diseases ,business.industry ,Poisoning ,Pyridoxine ,[SDV.MHEP.CSC] Life Sciences [q-bio]/Human health and pathology/Cardiology and cardiovascular system ,[SDV.TOX] Life Sciences [q-bio]/Toxicology ,Systematic review ,[SDV.TOX]Life Sciences [q-bio]/Toxicology ,Practice Guidelines as Topic ,Cohort ,[SDV.MHEP.MI] Life Sciences [q-bio]/Human health and pathology/Infectious diseases ,[SDV.MHEP.PSR] Life Sciences [q-bio]/Human health and pathology/Pulmonology and respiratory tract ,Hemodialysis ,business ,medicine.drug - Abstract
Isoniazid toxicity from self-poisoning or dosing errors remains common in regions of the world where tuberculosis is prevalent. Although the treatment of isoniazid poisoning is centered on supportive care and pyridoxine administration, extracorporeal treatments (ECTRs), such as hemodialysis, have been advocated to enhance elimination of isoniazid. No systematic reviews or evidence-based recommendations currently exist on the benefit of ECTRs for isoniazid poisoning. The Extracorporeal Treatments in Poisoning (EXTRIP) workgroup systematically collected and rated the available evidence on the effect of and indications for ECTRs in cases of isoniazid poisoning. We conducted a systematic review of the literature, screened studies, extracted data on study characteristics, outcomes, and measurement characteristics, summarized findings, and formulated recommendations following published EXTRIP methods. Forty-three studies (two animal studies, 34 patient reports or patient series, and seven pharmacokinetic studies) met inclusion criteria. Toxicokinetic or pharmacokinetic analysis was available for 60 patients, most treated with hemodialysis (n = 38). The workgroup assessed isoniazid as "Moderately Dialyzable" by hemodialysis for patients with normal kidney function (quality of evidence = C) and "Dialyzable" by hemodialysis for patients with impaired kidney function (quality of evidence = A). Clinical data for ECTR in isoniazid poisoning were available for 40 patients. Mortality of the cohort was 12.5%. Historical controls who received modern standard care including appropriately dosed pyridoxine generally had excellent outcomes. No benefit could be extrapolated from ECTR, although there was evidence of added costs and harms related to the double lumen catheter insertion, the extracorporeal procedure itself, and the extracorporeal removal of pyridoxine. The EXTRIP workgroup suggests against performing ECTR in addition to standard care (weak recommendation, very low quality of evidence) in patients with isoniazid poisoning. If standard dose pyridoxine cannot be administered, we suggest performing ECTR only in patients with seizures refractory to GABAA receptor agonists (weak recommendation, very low quality of evidence).
- Published
- 2021
8. Lipid resuscitation in acute poisoning: after a decade of publications, what have we really learned?
- Author
-
Hoegberg, Lotte C.G. and Gosselin, Sophie
- Published
- 2017
- Full Text
- View/download PDF
9. Oesophageal Obstruction from a Pharmacobezoar Resulting in Death
- Author
-
Mortensen, Katrine Elisabeth, Munkholm, Julie, Dalhoff, Kim Peder, and Hoegberg, Lotte Christine Groth
- Published
- 2017
- Full Text
- View/download PDF
10. Measurement of lumefantrine and its metabolite in plasma by high performance liquid chromatography with ultraviolet detection
- Author
-
Khalil, Insaf F., Abildrup, Ulla, Alifrangis, Lene H., Maiga, Deogratius, Alifrangis, Michael, Hoegberg, Lotte, Vestergaard, Lasse S., Persson, Ola Per-Eric, Nyagonde, Nyagonde, Lemnge, Martha M., Theander, Thor G., and Bygbjerg, Ib C.
- Published
- 2011
- Full Text
- View/download PDF
11. Extracorporeal Treatment for Gabapentin and Pregabalin Poisoning: Systematic Review and Recommendations From the EXTRIP Workgroup
- Author
-
Bouchard, Josée, primary, Yates, Christopher, additional, Calello, Diane P., additional, Gosselin, Sophie, additional, Roberts, Darren M., additional, Lavergne, Valéry, additional, Hoffman, Robert S., additional, Ostermann, Marlies, additional, Peng, Ai, additional, Ghannoum, Marc, additional, Alhatali, Badria, additional, Anseeuw, Kurt, additional, Bird, Steven, additional, Berling, Ingrid, additional, Bunchman, Timothy E., additional, Chin, Paul K., additional, Doi, Kent, additional, Galvao, Tais, additional, Goldfarb, David S., additional, Hassanian, Hossein, additional, Hoegberg, Lotte C.G., additional, Kallab, Siba, additional, Kebede, Sofia, additional, Kielstein, Jan T., additional, Lewington, Andrew, additional, Macedo, Etienne M., additional, MacLaren, Rob, additional, Megarbane, Bruno, additional, Mowry, James B., additional, Nolin, Thomas D., additional, Roy, Jean-Philippe, additional, Vijayan, Anitha, additional, Walsh, Steven J., additional, Wong, Anselm, additional, and Wood, David M., additional
- Published
- 2022
- Full Text
- View/download PDF
12. Practice Trends in the Use of Extracorporeal Treatments for Poisoning in Four Countries
- Author
-
Ghannoum, Marc, Lavergne, Valery, Gosselin, Sophie, Mowry, James B., Hoegberg, Lotte C. G., Yarema, Mark, Thompson, Margaret, Murphy, Nancy, Thompson, John, Purssell, Roy, and Hoffman, Robert S.
- Published
- 2016
- Full Text
- View/download PDF
13. Recommendations from the EXTRIP workgroup on extracorporeal treatment for baclofen poisoning
- Author
-
Alhatali, Badria, Anseeuw, Kurt, Bird, Steven, Bouchard, Josée, Bunchman, Timothy E., Calello, Diane P., Chin, Paul K., Goldfarb, David S., Hassanian-Moghaddam, Hossein, Hoegberg, Lotte C., Kallab, Siba, Kebede, Sofia, Kielstein, Jan T., King, Joshua D., Li, Yi, Macedo, Etienne M., MacLaren, Rob, Megarbane, Bruno, Mowry, James B., Ostermann, Marlies E., Peng, Ai, Roy, Jean-Philippe, Shepherd, Greene, Vijayan, Anitha, Walsh, Steven J., Wong, Anselm, Wood, David M., Yates, Christopher, Ghannoum, Marc, Berling, Ingrid, Lavergne, Valéry, Roberts, Darren M., Galvao, Tais, Hoffman, Robert S., Nolin, Thomas D., Lewington, Andrew, Doi, Kent, and Gosselin, Sophie
- Published
- 2021
- Full Text
- View/download PDF
14. Recommendations from the EXTRIP workgroup on extracorporeal treatment for baclofen poisoning
- Author
-
Ghannoum, Marc, primary, Berling, Ingrid, additional, Lavergne, Valéry, additional, Roberts, Darren M., additional, Galvao, Tais, additional, Hoffman, Robert S., additional, Nolin, Thomas D., additional, Lewington, Andrew, additional, Doi, Kent, additional, Gosselin, Sophie, additional, Alhatali, Badria, additional, Anseeuw, Kurt, additional, Bird, Steven, additional, Bouchard, Josée, additional, Bunchman, Timothy E., additional, Calello, Diane P., additional, Chin, Paul K., additional, Goldfarb, David S., additional, Hassanian-Moghaddam, Hossein, additional, Hoegberg, Lotte C., additional, Kallab, Siba, additional, Kebede, Sofia, additional, Kielstein, Jan T., additional, King, Joshua D., additional, Li, Yi, additional, Macedo, Etienne M., additional, MacLaren, Rob, additional, Megarbane, Bruno, additional, Mowry, James B., additional, Ostermann, Marlies E., additional, Peng, Ai, additional, Roy, Jean-Philippe, additional, Shepherd, Greene, additional, Vijayan, Anitha, additional, Walsh, Steven J., additional, Wong, Anselm, additional, Wood, David M., additional, and Yates, Christopher, additional
- Published
- 2021
- Full Text
- View/download PDF
15. Systematic review on the use of activated charcoal for gastrointestinal decontamination following acute oral overdose
- Author
-
Hoegberg, Lotte C. G., primary, Shepherd, Greene, additional, Wood, David M., additional, Johnson, Jami, additional, Hoffman, Robert S., additional, Caravati, E. Martin, additional, Chan, Wui Ling, additional, Smith, Silas W., additional, Olson, Kent R., additional, and Gosselin, Sophie, additional
- Published
- 2021
- Full Text
- View/download PDF
16. A Nationwide Register-Based Survey of Baclofen Toxicity
- Author
-
Kiel, Louise Bendix, Hoegberg, Lotte Christine Groth, Jansen, Tejs, Petersen, John Asger, and Dalhoff, Kim Peder
- Published
- 2015
- Full Text
- View/download PDF
17. Systematic review on the use of activated charcoal for gastrointestinal decontamination following acute oral overdose
- Author
-
Hoegberg, Lotte C. G., Shepherd, Greene, Wood, David M., Johnson, Jami, Hoffman, Robert S., Caravati, E. Martin, Chan, Wui Ling, Smith, Silas W., Olson, Kent R., and Gosselin, Sophie
- Abstract
The use of activated charcoal in poisoning remains both a pillar of modern toxicology and a source of debate. Following the publication of the joint position statements on the use of single-dose and multiple-dose activated charcoal by the American Academy of Clinical Toxicology and the European Association of Poison Centres and Clinical Toxicologists, the routine use of activated charcoal declined. Over subsequent years, many new pharmaceuticals became available in modified or alternative-release formulations and additional data on gastric emptying time in poisoning was published, challenging previous assumptions about absorption kinetics. The American Academy of Clinical Toxicology, the European Association of Poison Centres and Clinical Toxicologists and the Asia Pacific Association of Medical Toxicology founded the Clinical Toxicology Recommendations Collaborative to create a framework for evidence-based recommendations for the management of poisoned patients. The activated charcoal workgroup of the Clinical Toxicology Recommendations Collaborative was tasked with reviewing systematically the evidence pertaining to the use of activated charcoal in poisoning in order to update the previous recommendations. The main objective was: Does oral activated charcoal given to adults or children prevent toxicity or improve clinical outcome and survival of poisoned patients compared to those who do not receive charcoal? Secondary objectives were to evaluate pharmacokinetic outcomes, the role of cathartics, and adverse events to charcoal administration. This systematic review summarizes the available evidence on the efficacy of activated charcoal. A medical librarian created a systematic search strategy for Medline (Ovid), subsequently translated for Embase (via Ovid), CINAHL (via EBSCO), BIOSIS Previews (via Ovid), Web of Science, Scopus, and the Cochrane Library/DARE. All databases were searched from inception to December 31, 2019. There were no language limitations. One author screened all citations identified in the search based on predefined inclusion/exclusion criteria. Excluded citations were confirmed by an additional author and remaining articles were obtained in full text and evaluated by at least two authors for inclusion. All authors cross-referenced full-text articles to identify articles missed in the searches. Data from included articles were extracted by the authors on a standardized spreadsheet and two authors used the GRADE methodology to independently assess the quality and risk of bias of each included study. From 22,950 titles originally identified, the final data set consisted of 296 human studies, 118 animal studies, and 145 in vitro studies. Also included were 71 human and two animal studies that reported adverse events. The quality was judged to have a Low or Very Low GRADE in 469 (83%) of the studies. Ninety studies were judged to be of Moderate or High GRADE. The higher GRADE studies reported on the following drugs: paracetamol (acetaminophen), phenobarbital, carbamazepine, cardiac glycosides (digoxin and oleander), ethanol, iron, salicylates, theophylline, tricyclic antidepressants, and valproate. Data on newer pharmaceuticals not reviewed in the previous American Academy of Clinical Toxicology/European Association of Poison Centres and Clinical Toxicologists statements such as quetiapine, olanzapine, citalopram, and Factor Xa inhibitors were included. No studies on the optimal dosing for either single-dose or multiple-dose activated charcoal were found. In the reviewed clinical data, the time of administration of the first dose of charcoal was beyond one hour in 97% (n = 1006 individuals), beyond two hours in 36% (n = 491 individuals), and beyond 12 h in 4% (n = 43 individuals) whereas the timing of the first dose in controlled studies was within one hour of ingestion in 48% (n = 2359 individuals) and beyond two hours in 36% (n = 484) of individuals. This systematic review found heterogenous data. The higher GRADE data was focused on a few select poisonings, while studies that addressed patients with unknown and or mixed ingestions were hampered by low rates of clinically meaningful toxicity or death. Despite these limitations, they reported a benefit of activated charcoal beyond one hour in many clinical scenarios.
- Published
- 2021
- Full Text
- View/download PDF
18. Extracorporeal treatment for calcium channel blocker poisoning: systematic review and recommendations from the EXTRIP workgroup
- Author
-
Wong, Anselm, Hoffman, Robert S., Walsh, Steven J., Roberts, Darren M., Gosselin, Sophie, Bunchman, Timothy E., Kebede, Sofia, Lavergne, Valery, Ghannoum, Marc, Badria Alhatali, Anseeuw, Kurt, Berling, Ingrid, Bouchard, Josee, Bird, Steven, Chin, Paul, Doi, Kent, Tais Galvao, Goldfarb, David, Hassanian, Hossein, Hoegberg, Lotte, Siba Kallab, Kielstein, Jan, Li, Yi, Macedo, Etienne, MacLaren, Rob, Megarbane, Bruno, Mowry, Jim, Nolin, Thomas D., Osterman, Marlies, Peng, Ai, Jean-Philippe Roy, Vijayan, Anitha, Wood, David, and Yates, Christopher
- Abstract
Calcium channel blockers (CCBs) are commonly used to treat conditions such as arterial hypertension and supraventricular dysrhythmias. Poisoning from these drugs can lead to severe morbidity and mortality. We aimed to determine the utility of extracorporeal treatments (ECTRs) in the management of CCB poisoning. We conducted systematic reviews of the literature, screened studies, extracted data, summarized findings, and formulated recommendations following published EXTRIP methods. A total of 83 publications (6 in vitro and 1 animal experiments, 55 case reports or case series, 19 pharmacokinetic studies, 1 cohort study and 1 systematic review) met inclusion criteria regarding the effect of ECTR. Toxicokinetic or pharmacokinetic data were available on 210 patients (including 32 for amlodipine, 20 for diltiazem, and 52 for verapamil). Regardless of the ECTR used, amlodipine, bepridil, diltiazem, felodipine, isradipine, mibefradil, nifedipine, nisoldipine, and verapamil were considered not dialyzable, with variable levels of evidence, while no dialyzability grading was possible for nicardipine and nitrendipine. Data were available for clinical analysis on 78 CCB poisoned patients (including 32 patients for amlodipine, 16 for diltiazem, and 23 for verapamil). Standard care (including high dose insulin euglycemic therapy) was not systematically administered. Clinical data did not suggest an improvement in outcomes with ECTR. Consequently, the EXTRIP workgroup recommends against using ECTR in addition to standard care for patients severely poisoned with either amlodipine, diltiazem or verapamil (strong recommendations, very low quality of the evidence (1D)). There were insufficient clinical data to draft recommendation for other CCBs, although the workgroup acknowledged the low dialyzability from, and lack of biological plausibility for, ECTR. Both dialyzability and clinical data do not support a clinical benefit from ECTRs for CCB poisoning. The EXTRIP workgroup recommends against using extracorporeal methods to enhance the elimination of amlodipine, diltiazem, and verapamil in patients with severe poisoning.
- Published
- 2021
- Full Text
- View/download PDF
19. Extracorporeal treatment for poisoning to beta-adrenergic antagonists: systematic review and recommendations from the EXTRIP workgroup
- Author
-
Bouchard, Josée, Shepherd, Greene, Hoffman, Robert, Gosselin, Sophie, Roberts, Darren, Li, Yi, Nolin, Thomas, Lavergne, Valéry, Ghannoum, Marc, Alhatali, Badria, Anseeuw, Kurt, Bird, Steven, Berling, Ingrid, Bunchman, Timothy, Calello, Diane, Chin, Paul, Doi, Kent, Galvao, Tais, Goldfarb, David, Hassanian-Moghaddam, Hossein, Hoegberg, Lotte Cg, Kallab, Siba, Kebede, Sofia, Kielstein, Jan, Lewington, Andrew, Macedo, Etienne, Maclaren, Rob, Mégarbane, Bruno, Mowry, James, Ostermann, Marlies, Peng, Ai, Roy, Jean-Philippe, Vijayan, Anitha, Walsh, Steven, Wong, Anselm, Wood, David, Yates, Christopher, Mégarbane, Bruno, Service de Réanimation Médicale et Toxicologique [Hôpital Lariboisière], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpital Lariboisière-Fernand-Widal [APHP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Optimisation thérapeutique en Neuropsychopharmacologie (OPTeN (UMR_S_1144 / U1144)), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris Cité (UPCité), and EXTRIP workgroup
- Subjects
Consensus ,Adrenergic beta-Antagonists ,Overdose ,030232 urology & nephrology ,Intoxication ,Critical Care and Intensive Care Medicine ,[SDV.MHEP.PSR]Life Sciences [q-bio]/Human health and pathology/Pulmonology and respiratory tract ,03 medical and health sciences ,Beta-blockers ,Extracorporeal Membrane Oxygenation ,0302 clinical medicine ,[SDV.MHEP.CSC]Life Sciences [q-bio]/Human health and pathology/Cardiology and cardiovascular system ,Nadolol ,[SDV.MHEP.MI]Life Sciences [q-bio]/Human health and pathology/Infectious diseases ,medicine ,Humans ,030212 general & internal medicine ,Labetalol ,ECLS ,Practolol ,[SDV.MHEP.ME] Life Sciences [q-bio]/Human health and pathology/Emerging diseases ,[SDV.MHEP.ME]Life Sciences [q-bio]/Human health and pathology/Emerging diseases ,Beta-adrenergic blocking agent ,RC86-88.9 ,business.industry ,Research ,Sotalol ,Medical emergencies. Critical care. Intensive care. First aid ,Atenolol ,Acebutolol ,[SDV.MHEP.CSC] Life Sciences [q-bio]/Human health and pathology/Cardiology and cardiovascular system ,Hemoperfusion ,[SDV.TOX] Life Sciences [q-bio]/Toxicology ,Bisoprolol ,Anesthesia ,Hemodialysis ,[SDV.TOX]Life Sciences [q-bio]/Toxicology ,[SDV.MHEP.MI] Life Sciences [q-bio]/Human health and pathology/Infectious diseases ,[SDV.MHEP.PSR] Life Sciences [q-bio]/Human health and pathology/Pulmonology and respiratory tract ,Drug Overdose ,business ,medicine.drug - Abstract
Backgroundβ-adrenergic antagonists (BAAs) are used to treat cardiovascular disease such as ischemic heart disease, congestive heart failure, dysrhythmias, and hypertension. Poisoning from BAAs can lead to severe morbidity and mortality. We aimed to determine the utility of extracorporeal treatments (ECTRs) in BAAs poisoning.MethodsWe conducted systematic reviews of the literature, screened studies, extracted data, and summarized findings following published EXTRIP methods.ResultsA total of 76 studies (4 in vitro and 2 animal experiments, 1 pharmacokinetic simulation study, 37 pharmacokinetic studies on patients with end-stage kidney disease, and 32 case reports or case series) met inclusion criteria. Toxicokinetic or pharmacokinetic data were available on 334 patients (including 73 for atenolol, 54 for propranolol, and 17 for sotalol). For intermittent hemodialysis, atenolol, nadolol, practolol, and sotalol were assessed as dialyzable; acebutolol, bisoprolol, and metipranolol were assessed as moderately dialyzable; metoprolol and talinolol were considered slightly dialyzable; and betaxolol, carvedilol, labetalol, mepindolol, propranolol, and timolol were considered not dialyzable. Data were available for clinical analysis on 37 BAA poisoned patients (including 9 patients for atenolol, 9 for propranolol, and 9 for sotalol), and no reliable comparison between the ECTR cohort and historical controls treated with standard care alone could be performed. The EXTRIP workgroup recommends against using ECTR for patients severely poisoned with propranolol (strong recommendation, very low quality evidence). The workgroup offered no recommendation for ECTR in patients severely poisoned with atenolol or sotalol because of apparent balance of risks and benefits, except for impaired kidney function in which ECTR is suggested (weak recommendation, very low quality of evidence). Indications for ECTR in patients with impaired kidney function include refractory bradycardia and hypotension for atenolol or sotalol poisoning, and recurrent torsade de pointes for sotalol. Although other BAAs were considered dialyzable, clinical data were too limited to develop recommendations.ConclusionsBAAs have different properties affecting their removal by ECTR. The EXTRIP workgroup assessed propranolol as non-dialyzable. Atenolol and sotalol were assessed as dialyzable in patients with kidney impairment, and the workgroup suggests ECTR in patients severely poisoned with these drugs when aforementioned indications are present.
- Published
- 2021
20. The impact of the first wave of COVID-19 on Poison Centre (PC) activities in 4 European countries: a pilot study
- Author
-
NVIC, Brain, Other research (not in main researchprogram), NVIC bedrijfsvoering, Hondebrink, Laura, Faber, Katrin, Zammit, Mark, Hoegberg, Lotte C. G., Lonati, Davide, NVIC, Brain, Other research (not in main researchprogram), NVIC bedrijfsvoering, Hondebrink, Laura, Faber, Katrin, Zammit, Mark, Hoegberg, Lotte C. G., and Lonati, Davide
- Published
- 2021
21. Guidelines for Reporting Case Studies on Extracorporeal Treatments in Poisonings: Methodology
- Author
-
Lavergne, Valéry, Ouellet, Georges, Bouchard, Josée, Galvao, Tais, Kielstein, Jan T., Roberts, Darren M., Kanji, Salmaan, Mowry, James B., Calello, Diane P., Hoffman, Robert S., Gosselin, Sophie, Nolin, Thomas D., Goldfarb, David S., Burdmann, Emmanuel A., Dargan, Paul I., Decker, Brian Scott, Hoegberg, Lotte C., Maclaren, Robert, Megarbane, Bruno, Sowinski, Kevin M., Yates, Christopher, Mactier, Robert, Wiegand, Timothy, and Ghannoum, Marc
- Published
- 2014
- Full Text
- View/download PDF
22. A severe and prolonged case of Amanita phalloides poisoning
- Author
-
Huusom, Anja J., Mette, Anne, Clausen, R., Laessoe, Thomas, Hoegberg, Lotte C. G., Huusom, Anja J., Mette, Anne, Clausen, R., Laessoe, Thomas, and Hoegberg, Lotte C. G.
- Published
- 2020
23. A Computerised Sampling Strategy for Therapeutic Drug Monitoring of Lithium Provides Precise Estimates and Significantly Reduces Dose-Finding Time
- Author
-
Hoegberg, Lotte Christine Groth, Jürgens, Gesche, Zederkof, Vivian Wederking, Holgersson, Bettina, Andersson, John Erik, Dalhoff, Kim Peder, Larsen, Ejnar Bundgaard, and Angelo, Helle Riis
- Published
- 2012
- Full Text
- View/download PDF
24. Comment on Antidotal use of lipid emulsion – the pendulum swings
- Author
-
Hoffman, Robert S., primary, Gosselin, Sophie, additional, Villeneuve, Eric, additional, Hayes, Bryan D., additional, Hoegberg, Lotte C. G., additional, and Smolinske, Susan C., additional
- Published
- 2020
- Full Text
- View/download PDF
25. Dose-Dependent Adsorptive Capacity of Activated Charcoal for Gastrointestinal Decontamination of a Simulated Paracetamol Overdose in Human Volunteers
- Author
-
Gude, Anne-Bolette Jill, Hoegberg, Lotte Christine Groth, Angelo, Helle Riis, and Christensen, Hanne Rolighed
- Published
- 2010
- Full Text
- View/download PDF
26. Combined paracetamol and amitriptyline adsorption to activated charcoal
- Author
-
Hoegberg, Lotte Christine Groth, Groenlykke, Thor Buch, Abildtrup, Ulla, and Angelo, Helle Riis
- Subjects
Acetaminophen -- Dosage and administration ,Acetaminophen -- Health aspects ,Amitriptyline -- Dosage and administration ,Amitriptyline -- Health aspects ,Carbon, Activated -- Research ,Carbon, Activated -- Health aspects ,Adsorption -- Research ,Adsorption -- Physiological aspects ,Drugs -- Health aspects ,Drugs -- Research ,Drugs -- Care and treatment ,Environmental issues ,Health ,Pharmaceuticals and cosmetics industries - Published
- 2010
27. Potential pharmacobezoar formation of large size extended-release tablets and their dissolution - an in vitro study
- Author
-
Hoegberg, Lotte Christine Groth, Refsgaard, Frank, Pedersen, Steen Hauge, Personne, Mark, Ullah, Shahid, Panagiotidis, Georgios, Petersen, Tonny Studsgaard, Annas, Anita, Hoegberg, Lotte Christine Groth, Refsgaard, Frank, Pedersen, Steen Hauge, Personne, Mark, Ullah, Shahid, Panagiotidis, Georgios, Petersen, Tonny Studsgaard, and Annas, Anita
- Published
- 2019
28. Comparison of the adsorption capacities of an activated-charcoal--yogurt mixture versus activated-charcoal--water slurry in vivo and in vitro
- Author
-
Hoegberg, Lotte Christine Groth, Christophersen, Anne-Bolette, Christensen, Hanne Rolighed, and Angelo, Helle Riis
- Subjects
Charcoal -- Health aspects ,Charcoal -- Research ,Yogurt -- Research ,Yogurt -- Usage ,Environmental issues ,Health ,Pharmaceuticals and cosmetics industries - Abstract
Background. An activated charcoal-yogurt mixture was evaluated in vivo to determine the effect on the gastrointestinal absorption of paracetamol, as compared to activated-charcoal-water slurry. The potential advantage of the activated-charcoal-yogurt mixture is a better palatability and general acceptance by the patients without loss of efficacy. In addition, paracetamol adsorption studies were carried out in vitro to calculate the maximum adsorption capacity of paracetamol to activated-charcoal-yogurt mixture. Methods. In vivo: A randomized crossover study on 15 adult volunteers, using paracetamol 50 mg/kg as a simulated overdose. Each study day volunteers were given a standard meal 1 h before paracetamol, then 50 g activated charcoal 1 h later in either of two preparations: standard water slurry or mixed with 400 mL yogurt. Paracetamol serum concentrations were measured using HPLC. The areas under the concentration-time curve (AUC) of the two preparations were compared and used to estimate the efficacy of each preparation. The palatability of both preparations was evaluated using a visual-analogue scale where the volunteers were asked to evaluate the appearance, smell, flavor, texture, ability to swallow, and overall impression of the mixtures. The time spent to consume the activated charcoal was also registered. In vitro: Activated charcoal, simulated gastric (pH 1.2) or intestinal (pH 7.2) fluid, and paracetamol were mixed with yogurt followed by 1 h incubation. The maximum adsorption capacity of paracetamol to activated charcoal was calculated using Langmuir's adsorption isotherm. Paracetamol concentration was analyzed using HPLC. Results. In vivo there was no significant difference (p>0.05) in the AUC of paracetamol between the two activated-charcoal preparations. Geometric mean values and 95% CI for the AUCs were (in mg/l x min): 6307 (4932-8065) for the activated charcoal-water slurry and 6525 (5111-8330) for the activated charcoal-yogurt mixture. The palatability study showed significant difference (p Keywords Absorption reduction; Activated charcoal; Adsorption; Gastric decontamination; Intoxication; Paracetamol; Poisoning; Yogurt, INTRODUCTION Activated charcoal has long been known to be effective in reducing the gastrointestinal absorption of many drugs, making it a potentially useful agent in the management of acute poisonings [...]
- Published
- 2005
29. The Effect of Food and Ice Cream on the Adsorption Capacity of Paracetamol to High Surface Activated Charcoal: In vitro Studies
- Author
-
Hoegberg, Lotte Christine Groth, Angelo, Helle Riis, Christophersen, Anne Bolette, and Christensen, Hanne Rolighed
- Published
- 2003
30. Effect of ethanol and pH on the adsorption of acetaminophen (paracetamol) to high surface activated charcoal, in vitro studies. (Article)
- Author
-
Hoegberg, Lotte Christine Groth, Angelo, Helle R., Christophersen, A. Bolette, and Christensen, Hanne R.
- Subjects
Carbon, Activated -- Usage ,Poisoning -- Care and treatment ,Acetaminophen -- Adverse and side effects ,Antidotes -- Physiological aspects ,Environmental issues ,Health ,Pharmaceuticals and cosmetics industries - Abstract
Background: Paracetamol (acetaminophen) intoxication often in combination with ethanol, is seen commonly in overdose cases. Doses of several grams might be close to the maximum adsorption capacity of the standard treatment dose (50g) of activated charcoal. The aim of this study was to determine the maximum adsorption capacity for paracetamol for two types of high surface-activated charcoal [Carbomix[R] and Norit Ready-To-Use (not yet registered trademark in Denmark) both from Norit Cosmara, Amersfoort, The Netherlands] in simulated in vivo environments: At pH 1.2 (gastric environment), at pH 7.2 (intestinal environment), and with and without 10% ethanol. Methods: Activated charcoal, at both gastric or intestinal pHs, and paracetamol were mixed, resulting in activated charcoal--paracetamol ratios from 10:1 to 1:1. In trials with ethanol some of the gastric or intestinal fluid was replaced with an equivalent volume of ethanol, resulting in an ethanol concentration of 10% v/v. After incubation, the concentration of unabsorbed paracetamol was analyzed by high-performance liquid chromatography. The maximum adsorption capacity of paracetamol to activated charcoal was calculated as mg paracetamol adsorbed/g activated charcoal, using Langmuir's isotherm. Results: Carbomix [95% confidence limits are shown in square brackets]: 623.7 [612.8;634.5] mg paracetamol adsorbed/g activated charcoal (pH 1.2), 626.2 [611.6;640.9] mg paracetamol adsorbed/g activated charcoal (pH 7.2); Norit Ready-To-Use: 693.6 [676.8; 710.5] mg paracetamol adsorbed/g activated charcoal (pH 1.2), 722.6 [687.4;757.9] mg paracetamol adsorbed/g activated charcoal (pH 7.2). For experiments with ethanol (10% v/v) the results with Carbomix were 465.7 [449.2;482.2] mg paracetamol adsorbed/g activated charcoal (pH 1.2), 498.6 [481.8;515.6] mg paracetamol adsorbed/g activated charcoal (pH 7.2); with Norit Ready-To-Use: 617.2 [606.6;627.7] mg paracetamol adsorbed/g activated charcoal (pH 1.2), 640.6 [624.9;656.4] mg paracetamol adsorbed/g activated charcoal (pH 7.2). Conclusion: Under conditions simulating immediate treatment with charcoal, a standard dose of 50 g of either of the two tested activated charcoals adsorbed a sufficient amount of paracetamol to be beneficial in the treatment of the majority of overdoses of this drug. For both types of activated charcoal, with or without ethanol, there was no significant difference in the adsorption of paracetamol at pH 1.2 and 7.2. Norit Ready-To-Use had a larger maximum adsorption capacity than Carbomix, and was not as sensitive as Carbomix to environmental changes (pH and ethanol). The presence of 10% ethanol lowered the adsorption capacity of the two tested activated charcoal preparations by an amount that might be clinically relevant in cases of intoxications by high-gram doses., INTRODUCTION When using activated charcoal (AC) as gastrointestinal (GI) decontamination in cases of drug poisoning, information concerning its maximum adsorption capacity of AC for the particular drug ingested theoretically permits [...]
- Published
- 2002
31. Electrocardiographic study in Ghanaian children with uncomplicated malaria, treated with artesunate-amodiaquine or artemether-lumefantrine
- Author
-
Adjei George O, Oduro-Boatey Collins, Rodrigues Onike P, Hoegberg Lotte C, Alifrangis Michael, Kurtzhals Jorgen A, and Goka Bamenla Q
- Subjects
Malaria ,Combination therapy ,Cardiotoxicity ,Children ,Ghana ,Arctic medicine. Tropical medicine ,RC955-962 ,Infectious and parasitic diseases ,RC109-216 - Abstract
Abstract Background Several anti-malarial drugs are associated with adverse cardiovascular effects. These effects may be exacerbated when different anti-malarials are used in combination. There has been no report yet on the potential cardiac effects of the combination artesunate-amodiaquine. Methods Electrocardiographic (ECG) intervals in Ghanaian children with uncomplicated malaria treated with artesunate-amodiaquine (n=47), were compared with that of children treated with artemether-lumefantrine (n=30). The ECG measurements were repeated one, two, three, seven and 28 days after treatment. The ECG intervals of artesunate-amodiaquine treated subjects were correlated with plasma concentrations of desethylamodiaquine (DEAQ), the main metabolite of amodiaquine. Results The mean ECG intervals were similar in both groups before treatment. After treatment (day 3), ECG intervals changed significantly from baseline in all subjects, but there were no differences between the two treatment groups. A significantly higher proportion of children treated with artesunate-amodiaquine developed sinus bradycardia compared with artemether-lumefantrine treated subjects (7/47 vs 0/30; χ2 p=0.03). Subjects who developed bradycardia were significantly older, and had higher DEAQ concentrations than those who did not develop bradycardia. The proportion of subjects with QTc interval prolongations did not differ significantly between the groups, and no relationship between prolonged QTc intervals and DEAQ levels were observed. No clinically significant rhythm disturbances were observed in any of the subjects. Conclusion Artesunate-amodiaquine treatment resulted in a higher incidence of sinus bradycardia than artemether-lumefantrine treatment in children with uncomplicated malaria, but no clinically significant rhythm disturbances were induced by combining artesunate with amodiaquine. These findings, although reassuring, may imply that non-amodiaquine based artemisinin combination therapy may be preferable for malaria treatment in patients who are otherwise at risk of cardiac effects.
- Published
- 2012
- Full Text
- View/download PDF
32. Population Pharmacokinetics of the Antimalarial Amodiaquine: a Pooled Analysis To Optimize Dosing
- Author
-
Ali, Ali Mohamed, Penny, Melissa, Smith, Thomas, Workman, Lesley, Sasi, Philip, Adjei, George O, Aweeka, Francesca, Kiechel, Jean-René, Jullien, Vincent, Rijken, Marcus, Mcgready, Rose, Mwesigwa, Julia, Kristensen, Kim, Stepniewska, Kasia, Tarning, Joel, Barnes, Karen, Denti, Paolo, Massougbodji, Achille, Gansané, Adama, Adeothy, Adicat, Aubouy, Agnès, Ouedraogo, Alphonse, Annerberg, Anna, Bruneel, Arnaud, Phyo, Aung Pyae, Win, Aye Kyi, Benakis, A., Goka, Bamenla, Gourmel, Bernard, Ogutu, Bernhards, Schramm, Birgit, McGee, Bryan, Morgan, Caroline, Obonyo, Charles, Mazinda, Charles, Parzy, D., Ashley, Elizabeth, Baudin, Elisabeth, Juma, Elizabeth, Comte, Eric, Ouedraogo, Esperance, Nosten, François, Sugnaux, F., Cottrell, Gilles, Dorsey, Grant, Carn, Gwenaelle, Kossou, Hortense, Amedome, Hyacinthe, Kalyango, Joan, Faucher, Jean-François, Jones, Joel, Simpson, Julie, Doritchamou, Justin, Kurtzhals, J., Pinoges, Loretxu, Hoegberg, Lotte, BERTAUX, L., Malaika, L. Tshilolo Muepu, Bergstrand, Martin, Alifrangis, Michael, Branger, Michel, Cot, Michel, Cammas, Mireille, Kamya, Moses, Day, Nicholas, White, Nicholas, Taudon, N., Rodrigues, Onike, Chotsiri, Palang, Valeh, Parastou, Houzé, Pascal, Deloron, Philippe, Guérin, Philippe, Rosenthal, Philip, Hsi, Poe, German, Polina, Singhasivanon, Pratap, Smith, Richard, Lwango, R., Sirima, Sodiomon, Parikh, Sunil, Alegre, S. Sese, Clark, Tamara, Sundaygar, Timothy, Drysdale, Troy, Taylor, Walter, Sinou, V., Zolia, Yah, Swiss Tropical and Public Health Institute [Basel], University of Basel (Unibas), Ifakara Health Institute, University of Cape Town, Muhimbili University of Health and Allied Sciences, University of Ghana, University of California, Drugs for Neglected Diseases Initiative, Service de Pharmacologie, Hôpital Européen George Pompidou, Université Paris Descartes, Paris, France, Hôpital Européen Georges Pompidou [APHP] (HEGP), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpitaux Universitaires Paris Ouest - Hôpitaux Universitaires Île de France Ouest (HUPO)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Hôpitaux Universitaires Paris Ouest - Hôpitaux Universitaires Île de France Ouest (HUPO), Mahidol University [Bangkok], University of Oxford [Oxford], London School of Hygiene & Tropical Medicine [Fajara, The Gambia], University of Antwerp (UA), Development DMPK-PKPD, Novo Nordisk, Copenhagen, Denmark, Univ Copenhagen, Fac Hlth & Med Sci, Novo Nordisk Fdn, Dis Syst Biol,Ctr Prot Res, Copenhagen, Denmark, and Partenaires INRAE-Partenaires INRAE
- Subjects
pediatrics ,dose optimization ,malaria ,[SDV.SP]Life Sciences [q-bio]/Pharmaceutical sciences ,NONMEM - Abstract
International audience; Amodiaquine plus artesunate is the recommended antimalarial treatment in many countries where malaria is endemic. However, pediatric doses are largely based on a linear extrapolation from adult doses. We pooled data from previously published studies on the pharmacokinetics of amodiaquine, to optimize the dose across all age groups. Adults and children with uncomplicated malaria received daily weight-based doses of amodiaquine or artesunate-amodiaquine over 3 days. Plasma concentration-time profiles for both the parent drug and the metabolite were characterized using nonlinear mixed-effects modeling. Amodiaquine pharmacokinetics were adequately described by a two-compartment disposition model, with first-order elimination leading to the formation of desethylamodiaquine, which was best described by a three-compartment disposition model. Body size and age were the main covariates affecting amodiaquine clearance. After adjusting for the effect of weight, clearance rates for amodiaquine and desethylamodiaquine reached 50% of adult maturation at 2.8 months (95% confidence interval [CI], 1.5 to 3.7 months) and 3.9 months (95% CI, 2.6 to 5.3 months) after birth, assuming that the baby was born at term. Bioavailability was 22.4% (95% CI, 15.6 to 31.9%) lower at the start of treatment than during convalescence, which suggests a malaria disease effect. Neither the drug formulation nor the hemoglobin concentration had an effect on any pharmacokinetic parameters. Results from simulations showed that current manufacturer dosing recommendations resulted in low desethylamodiaquine exposure in patients weighing 8 kg, 15 to 17 kg, 33 to 35 kg, and >62 kg compared to that in a typical 50-kg patient. We propose possible optimized dosing regimens to achieve similar drug exposures among all age groups, which require further validation.
- Published
- 2018
33. Pediatric vitamin D poisoning: diagnostic and treatment algorithm update
- Author
-
Hoegberg, Lotte C. G., Boegevig, Soeren, Anders, Schou J., Christesen, Henrik T., Kamperis, Konstantinos, Vojdeman, Fie J., Molgaard, Christian, Brot, Christine, and Schmidt, Ida M.
- Published
- 2018
34. Development of ELISA-based methods to measure the anti-malarial drug chloroquine in plasma and in pharmaceutical formulations
- Author
-
Ronn Anita, Bygbjerg Ib C, Recke Camilla, Hoegberg Lotte C, Alifrangis Michael, Khalil Insaf F, and Koch Claus
- Subjects
Arctic medicine. Tropical medicine ,RC955-962 ,Infectious and parasitic diseases ,RC109-216 - Abstract
Abstract Background In Central and South America and Eastern and Southern Africa, Plasmodium vivax infections accounts for 71-81% and 5% of malaria cases, respectively. In these areas, chloroquine (CQ) remains the treatment of choice for P. vivax malaria. In addition, CQ has recently proven to be an effective HIV-1 therapeutic agent. There is a dire need to continue monitoring quality of CQ as there is a major influx of substandard and fake formulations into malaria-endemic countries. The use of fake/substandard drugs will result in sub-therapeutic levels endangering the patient and possibly select for parasite resistance. The aim of this study was to develop an inexpensive, simple antibody-based ELISA to measure CQ concentrations in tablets and in plasma. Methods A monoclonal antibody (MAb) that reacts with the N-side chain of the CQ molecule was prepared by use of a CQ analogue. A specific and reliable ELISA for detection of CQ was developed. The developed assay was validated by measuring CQ in tablets sold in Denmark, India and Sudan. Furthermore, kinetics of CQ concentrations in plasma of four volunteers, who ingested two tablets of Malarex® containing, 250 mg CQ base, were measured before drug intake, three hours later and thereafter at days 1, 3, 7, 14, 21 and 28. The same plasma samples were simultaneously measured by high performance liquid chromatography (HPLC). Results The ELISA proved an easy-to-handle and very sensitive tool for the detection of CQ with a lower limit of detection at 3.9 ng/ml. ELISA levels of CQ in plasma showed high agreement with the levels obtained by HPLC (r = 0.98). The specificity in the negative control group was 100%. Conclusion The developed ELISA can be used for quality screening of CQ in pharmaceutical formulations and for drug monitoring in malaria and in other infectious diseases, such as HIV, where CQ proved to be an effective therapeutic agent. The methodology has been exploited to develop monoclonal antibodies for the drugs used in artemisinin-based combination therapy (ACT).
- Published
- 2011
- Full Text
- View/download PDF
35. Amodiaquine-artesunate vs artemether-lumefantrine for uncomplicated malaria in Ghanaian children: a randomized efficacy and safety trial with one year follow-up
- Author
-
Hoegberg Lotte CG, Alifrangis Michael, Rodrigues Onike P, Kurtzhals Jorgen AL, Adjei George O, Kitcher Emmanuel D, Badoe Ebenezer V, Lamptey Roberta, and Goka Bamenla Q
- Subjects
Arctic medicine. Tropical medicine ,RC955-962 ,Infectious and parasitic diseases ,RC109-216 - Abstract
Abstract Background Artesunate-amodiaquine (AS+AQ) and artemether-lumefantrine (AM-L) are efficacious artemisinin combination therapy (ACT) regimens that have been widely adopted in sub-Saharan Africa. However, there is little information on the efficacy of these regimens on subsequent episodes beyond 28 days, or on the safety of repeated treatments. Methods Children aged six months to 14 years with uncomplicated malaria were randomly assigned to treatment with AS+AQ (n = 116), or AM-L (n = 111). Recruited subjects were followed-up, initially for 28 days, and then monthly for up to one year. All subsequent attacks of uncomplicated malaria after 28 days were treated with the same regimen as at randomization. Investigations aimed at determining efficacy and side effects were conducted. Results Adequate clinical and parasitological response in subjects with evaluable end-points were, 97.1% (100/103) and 98.2% (107/109) on day 14, and 94.2% (97/103) and 95.3% (102/107) on day 28 in the AM-L and AS+AQ groups, respectively. Similar results were obtained after PCR correction. The incidence of malaria attacks in the year following recruitment was similar between the two treatment groups (p = 0.93). There was a high incidence of potentially AQ-resistant parasites in the study area. The incidence of adverse events, such as pruritus, fatigue and neutropaenia were similar in the two treatment groups. No patient showed signs of hearing impairment, and no abnormal neurological signs were observed during one year of follow-up. Other adverse events were mild in intensity and overlapped with known malaria symptomatology. No adverse event exacerbation was observed in any of the subjects who received multiple treatment courses with these ACT regimens during one year follow-up. Conclusion AS+AQ and AM-L were efficacious for treatment of children with uncomplicated malaria in Ghana and drug-related adverse events were rare in treated subjects during one year of follow-up. The high prevalence of potentially AQ resistant parasites raises questions about the utility of AQ as a partner drug for ACT in Ghana. The efficacy of AS+AQ in Ghana requires, therefore, continuous monitoring and evaluation. Trial registration NCT 00406146 http://www.clinicaltrials.gov
- Published
- 2008
- Full Text
- View/download PDF
36. Availability of Paracetamol Sold Over the Counter in Europe:A Descriptive Cross-Sectional International Survey of Pack Size Restriction
- Author
-
Morthorst, Britt Reuter, Erlangsen, Annette, Nordentoft, Merete, Hawton, Keith, Hoegberg, Lotte Christine Groth, Dalhoff, Kim Peder, Morthorst, Britt Reuter, Erlangsen, Annette, Nordentoft, Merete, Hawton, Keith, Hoegberg, Lotte Christine Groth, and Dalhoff, Kim Peder
- Abstract
Due to the risk of hepatotoxicity when excessive amounts of paracetamol are consumed, Poisons Information Centers (PICs) frequently receive paracetamol-related enquiries. This study examined how widely pack size restrictions of paracetamol sold over the counter have been implemented in Europe and also availability of paracetamol through non-pharmacy outlets and their possible associations with frequency of poisoning enquiries. A cross-sectional European multi-centre questionnaire study was performed using a questionnaire to identify the extent and nature of paracetamol pack size restrictions, non-pharmacy outlet sales and the frequency of paracetamol-related enquiries to PICs. In total, 21 European countries participated. All PICs provided telephone hotline services. In 14 (67%) countries, pack size restrictions had been implemented in pharmacies (range: 8–30 g). No significant difference (median difference 0.7%, p-value = 0.36) was found when comparing median frequencies of paracetamol-related enquiries in countries with pack size restriction to countries without restrictions. A significantly lower median frequency of paracetamol-related enquiries was found in countries without non-pharmacy outlet sales compared to those with such sales (median difference 2.2%, p = 0.02). Pack size restrictions on pharmacy sales of paracetamol have been implemented in two-thirds of examined countries. There was no difference in the proportion of paracetamol-related enquiries to PICs among countries with and without pack size restrictions. However, a lower rate of paracetamol-related enquiries was noted in countries where paracetamol was not available in non-pharmacy outlets.
- Published
- 2018
37. Advanced electrocardiogram (ECG) analysis in the amitriptyline-poisoned pig treated with coated activated charcoal hemoperfusion (CAC-HP)
- Author
-
Jansen, Tejs, Hoegberg, Lotte C. G., Eriksen, Thomas, Haarmark, Christian, Dalhoff, Kim P., Belhage, Bo, Jansen, Tejs, Hoegberg, Lotte C. G., Eriksen, Thomas, Haarmark, Christian, Dalhoff, Kim P., and Belhage, Bo
- Published
- 2018
38. Amitriptyline accumulation in tissues after coated activated charcoal hemoperfusion:a randomized controlled animal poisoning model
- Author
-
Jansen, Tejs, Hoegberg, Lotte C. G., Eriksen, Thomas, Dalhoff, Kim P., Belhage, Bo, Johansen, Sys S., Jansen, Tejs, Hoegberg, Lotte C. G., Eriksen, Thomas, Dalhoff, Kim P., Belhage, Bo, and Johansen, Sys S.
- Published
- 2018
39. Advanced Electrocardiogram Analysis in the Amitriptyline-poisoned Pig Treated with Activated Charcoal Haemoperfusion
- Author
-
Jansen, Tejs, Hoegberg, Lotte C.G., Eriksen, Thomas, Haarmark, Christian, Dalhoff, Kim, Belhage, Bo, Jansen, Tejs, Hoegberg, Lotte C.G., Eriksen, Thomas, Haarmark, Christian, Dalhoff, Kim, and Belhage, Bo
- Abstract
Coated activated charcoal haemoperfusion (CAC-HP) does not reduce the plasma concentration in amitriptyline (AT)-poisoned pigs. The aim of this non-blinded, randomized, controlled animal trial was to determine if CAC-HP reduces the pathological ECG changes caused by AT poisoning. Fourteen female Danish Landrace pigs (mean weight 27.7 kg, range 20-35 kg (CAC-HP) and 24.4 kg, range 18-30 kg (control group, CG), n = 7 in each group) were included. After randomization, the pigs were anaesthetized and intravenously poisoned with AT. The intervention group underwent 4 hr of CAC-HP plus standard care (oral activated charcoal). Intervention was compared to standard care alone. From each pig, a 12-lead ECG and haemodynamic variables were obtained at baseline, at full AT loading dose, before and during CAC-HP. Baseline ECG variables (RR, PR, QRS, QTc, QTp, QTe, TpTe and TpTe/QT) for lead II, v2 and v5 were not significantly different (F = 0.035-0.297, p-values 0.421-0.919). Differences within groups over time and between groups were tested by anova repeated measures. For all variables, the time-plus-group level of significance revealed a p-value > 0.05. Severe cardiovascular arrhythmias occurred in both groups with 3 in the CAC-HP group versus 1 incident with premature death in the CG. The attenuating effect of CAC-HP to orally instilled activated charcoal alone on AT-induced ECG alterations did not differ significantly. We conclude that the use of modern CAC-HP as an adjunctive treatment modality in AT-poisoned pigs is inadequate.
- Published
- 2018
40. Recreational drug use at a major music festival:trend analysis of anonymised pooled urine
- Author
-
Hoegberg, Lotte, Christiansen, Cecilie, Søe, Jesper Langager, Telving, Rasmus, Andreasen, Mette Findal, Stærk, Dan, Christrup, Lona Louring, Kongstad, Kenneth Thermann, Hoegberg, Lotte, Christiansen, Cecilie, Søe, Jesper Langager, Telving, Rasmus, Andreasen, Mette Findal, Stærk, Dan, Christrup, Lona Louring, and Kongstad, Kenneth Thermann
- Published
- 2018
41. Potential pharmacobezoar formation of large size extended-release tablets and their dissolution – an in vitro study
- Author
-
Hoegberg, Lotte Christine Groth, primary, Refsgaard, Frank, additional, Pedersen, Steen Hauge, additional, Personne, Mark, additional, Ullah, Shahid, additional, Panagiotidis, Georgios, additional, Petersen, Tonny Studsgaard, additional, and Annas, Anita, additional
- Published
- 2018
- Full Text
- View/download PDF
42. Utilization of lipid emulsion therapy in fatal overdose cases: an observational study
- Author
-
Smolinske, Susan, primary, Hoffman, Robert S., additional, Villeneuve, Eric, additional, Hoegberg, Lotte C. G., additional, and Gosselin, Sophie, additional
- Published
- 2018
- Full Text
- View/download PDF
43. Extracorporeal blood purification for treating acute paraquat poisoning
- Author
-
Lavergne, Valery, primary, Gosselin, Sophie, additional, Ghannoum, Marc, additional, Hoegberg, Lotte C, additional, and Roberts, Darren M, additional
- Published
- 2018
- Full Text
- View/download PDF
44. Availability of Paracetamol Sold Over the Counter in Europe: A Descriptive Cross‐Sectional International Survey of Pack Size Restriction
- Author
-
Morthorst, Britt Reuter, primary, Erlangsen, Annette, additional, Nordentoft, Merete, additional, Hawton, Keith, additional, Hoegberg, Lotte Christine Groth, additional, and Dalhoff, Kim Peder, additional
- Published
- 2018
- Full Text
- View/download PDF
45. Advanced Electrocardiogram Analysis in the Amitriptyline-poisoned Pig Treated with Activated Charcoal Haemoperfusion
- Author
-
Jansen, Tejs, primary, Hoegberg, Lotte C. G., additional, Eriksen, Thomas, additional, Haarmark, Christian, additional, Dalhoff, Kim, additional, and Belhage, Bo, additional
- Published
- 2017
- Full Text
- View/download PDF
46. Activated Charcoal Hemoperfusion in the Treatment of Experimental Amitriptyline Poisoning in Pigs - The Effect on Amitriptyline Plasma Concentration and Hemodynamic Parameters
- Author
-
Jansen, Tejs, Petersen, Henrik, Malskaer, Cecilie M, Gabel-Jensen, Charlotte, Dalhoff, Kim, Eriksen, Thomas, Belhage, Bo, Hoegberg, Lotte C G, Jansen, Tejs, Petersen, Henrik, Malskaer, Cecilie M, Gabel-Jensen, Charlotte, Dalhoff, Kim, Eriksen, Thomas, Belhage, Bo, and Hoegberg, Lotte C G
- Abstract
Coated activated charcoal hemoperfusion (CAC-HP) is a well-known treatment modality. Case reports have revealed conflicting results about the efficacy of CAC-HP in the treatment of amitriptyline (AT) poisoning, and no randomised clinical trials have been identified in the literature. This study aimed at quantifying the efficacy of modern CAC-HP as an adjunctive treatment of AT intoxication compared to standard care alone. Fourteen female Danish landrace pigs were randomized to either standard care or standard care plus 4 hr of CAC-HP. The pigs were anaesthetized and vital parameters were continuously recorded. Amitriptyline infusion (7.5 mg/kg) was completed in 20 min. Thirty minutes following AT infusion, activated charcoal was instilled orally in both groups. In the intervention group, CAC-HP was initiated 60 min. after AT infusion. Blood and urine samples were collected as were vital parameters at specific time intervals. The protocol was approved by the Danish Experimental Animal Expectorate and complied with the NIH guide for care and use of laboratory animals. Data were managed according to the ARRIVE guidelines. No statistical significant differences between intervention and control group were found when analysing for differences in AT levels in plasma at any time point. Furthermore, significant differences between the control and intervention group in regard to vital parameters could not be found either. In our animal model, the addition of CAC-HP did not improve the clearance of AT compared to standard treatment alone. We hypothesize that the effect of modern CAC-HP as a treatment modality in AT poisoned human patients may be inadequate. This article is protected by copyright. All rights reserved.
- Published
- 2017
47. Recreational drug use at a major music festival: trend analysis of anonymised pooled urine
- Author
-
Hoegberg, Lotte Christine Groth, primary, Christiansen, Cecilie, additional, Soe, Jesper, additional, Telving, Rasmus, additional, Andreasen, Mette Findal, additional, Staerk, Dan, additional, Christrup, Lona Louring, additional, and Kongstad, Kenneth Thermann, additional
- Published
- 2017
- Full Text
- View/download PDF
48. Letter in response to “Lipid emulsion improves survival in animal models of local anesthetic toxicity: a meta-analysis”
- Author
-
Hoegberg, Lotte C. G., primary, Hoffman, Robert S., additional, Hayes, Bryan D., additional, Lavergne, Valéry, additional, and Gosselin, Sophie, additional
- Published
- 2017
- Full Text
- View/download PDF
49. Activated Charcoal Haemoperfusion in the Treatment of Experimental Amitriptyline Poisoning in Pigs - The Effect on Amitriptyline Plasma Concentration and Haemodynamic Parameters
- Author
-
Jansen, Tejs, primary, Petersen, Henrik, additional, Malskaer, Cecilie M., additional, Gabel-Jensen, Charlotte, additional, Dalhoff, Kim, additional, Eriksen, Thomas, additional, Belhage, Bo, additional, and Hoegberg, Lotte C. G., additional
- Published
- 2017
- Full Text
- View/download PDF
50. Utilization of lipid emulsion therapy in fatal overdose cases: an observational study.
- Author
-
Smolinske, Susan, Hoffman, Robert S., Villeneuve, Eric, Hoegberg, Lotte C. G., and Gosselin, Sophie
- Subjects
DRUG overdose ,INTRAVENOUS fat emulsions ,POISONING ,EMULSIONS (Pharmacy) ,META-analysis - Abstract
Objective: Although anecdotal reports suggest that intravenous lipid emulsion (ILE) therapy is effective in a large variety of overdoses, the few controlled human trials published to date yielded disappointing results. Because of potential publication biases, there are few reports concerning the failure of ILE. The primary aim of this study was to identify fatal poisoning cases in the American Association of Poison Control Centers (AAPCC) National Poison Data System (NPDS) in which ILE was administered. Methods: We obtained an approved release of data from NPDS for years 2010-2015 in which the words "lipid," "ILE," or "fat" appeared in the narrative. Duplicate cases were excluded as were cases in which ILE was not clearly given. Case data were extracted by one author using a predetermined tool, and the information was confirmed by a second author. The timing of ILE administration was characterized into one of four categories: cardiac arrest, first line, last resort, or part of multiple therapies given simultaneously. Response to ILE and adverse events was recorded. Results: Of the 826 cases retrieved from NPDS, 459 met final inclusion criteria. Over 50% of included cases involved either a calcium channel blocker or a beta-adrenergic antagonist. Of note, less than 25% of cases involved a substance for which the Lipid Emulsion Working Group found evidence to support its use. Most often, ILE was given along with multiple therapies (277 cases) or as a last resort (137 cases). In 127 cases, ILE was given during cardiac arrest. ILE was used as first line therapy in 34 cases. Response rates were reported as follows: no response (45%), unknown response (38%), transient/minimal response (7%), ROSC (7%), and immediate worsening (3%). Possible adverse reactions included: ARDS in 39 patients, lipemia causing a delay in laboratory evaluation in three cases, lipemia causing failure of a CRRT filter in two cases, worsening or new onset seizure in two cases, asystole immediately after administration in two cases, and fat embolism in one case. Conclusion: Within the Association of Poison Control Centers (AAPCC) National Poison Data System (NPDS), hundreds of cases exist in which ILE therapy was given and death occurred. In many of these cases, ILE was given prior to cardiovascular collapse. Although there is some suggestion of transient improvement in a small subset of cases, adverse effects are also reported. When taken in totality, the number of published cases of failed lipid emulsion therapy outnumbers the published instances of ILE success. Given all the uncertainty generated by case reports, the evaluation of the role and efficacy of ILE therapy in non-local anesthetic poisoning needs robust controlled clinical trials. [ABSTRACT FROM AUTHOR]
- Published
- 2019
- Full Text
- View/download PDF
Catalog
Discovery Service for Jio Institute Digital Library
For full access to our library's resources, please sign in.