8 results on '"Sikma, M.A."'
Search Results
2. P03-14 Acute intoxications with metoprolol, atenolol and propranolol in obese and non-obese patients: a PBPK-PD modelling study
- Author
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Mattijsen, H.P., primary, Sikma, M.A., additional, Wijnands-Kleukers, A.P., additional, Lange, D.W.D., additional, and Hunault, C.C., additional
- Published
- 2022
- Full Text
- View/download PDF
3. The Effect of Renal Replacement Therapy in a Patient with Mercaptopurine Toxicity: Time to Revise Guidelines
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Quaedvlieg, H.J.L., Polderman, F.N., Borkent, M., Jonge, De H.J.M., Annema, P.A., Derijks, L.J.J., Sikma, M.A., and Bethlehem, C.
- Abstract
Introduction: Mercaptopurine, a thiopurine, is used in various disorders of immune regulation, such as autoimmune hepatitis. Thiopurine metabolism is complex with risk for overdosing, especially when metabolism is impaired by liver dysfunction. Hepatotoxicity may be due to mercaptopurine overdose and is often reversible after prompt cessation of the drug. Case Presentation: Treatment of thiopurine toxicity is mainly supportive and literature on enhanced elimination by renal replacement therapy is ambiguous. Conclusion: In this case of thiopurine toxicity, a patient with autoimmune hepatitis presents with abdominal pain, nausea, vomiting, and diarrhea. We show in this case report that renal replacement therapy had no effect on total body clearance of mercaptopurine.
- Published
- 2023
- Full Text
- View/download PDF
4. Irreversible Encephalopathy After Treatment With High-Dose Intravenous Metronidazole
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Groothoff, M.V.R., Hofmeijer, J., Sikma, M.A., Meulenbelt, J., Risk Assessment of Toxic and Immunomodulatory Agents, Dep IRAS, and University of Groningen
- Subjects
Adult ,fatal outcome ,Encephalopathy ,Drug Administration Schedule ,Diagnosis, Differential ,Anti-Infective Agents ,Levofloxacin ,Metronidazole ,adverse effect ,medicine ,Humans ,Pharmacology (medical) ,Adverse effect ,Omeprazole ,LEVOFLOXACIN ,Pharmacology ,Coma ,Brain Diseases ,biology ,Dose-Response Relationship, Drug ,business.industry ,Electroencephalography ,Osteomyelitis ,medicine.disease ,biology.organism_classification ,encephalopathy ,Magnetic Resonance Imaging ,BACLOFEN ,Discontinuation ,poisoning ,INTOXICATION ,Anesthesia ,Pyrosis ,Injections, Intravenous ,Female ,medicine.symptom ,business ,medicine.drug ,neurotoxic - Abstract
Background: Encephalopathy associated with metronidazole is rare and, in most cases, reversible following discontinuation. Objective: We describe a case of fatal encephalopathy after treatment with high-dose intravenous metronidazole and the potential causes of the irreversibility. Case summary: A 38-year-old white woman (weight, 45 kg) received metronidazole among other medications to treat osteomyelitis for 74 days after surgery to correct a spinal neuroarthropathy. An initial dose of 500 mg IV QID was administered. After 6 weeks, the patient was discharged and the dose was changed to 1500 mg IV administered once dally (over 90 minutes) by a visiting nurse. Other treatments included teicoplanin 400 mg once dally and trimethoprim-sulfamethoxazole 480 mg BID for the infection, baclofen 25 mg TID for pain associated with a congenital spinal cord lesion with paraplegia, and omeprazole 20 mg once daily for pyrosis. Tell weeks after the start of metronidazole, the patient developed somnolence and dysarthria, changing to encephalopathy with coma on admission 2 weeks later. Despite discontinuation of all medication, including metronidazole, 2 days after admission, the patient's condition appeared to be irreversible. After 8 weeks, her coma was considered permanent, mechanical ventilation was discontinued, and she died. Evaluating all medicines administered, metronidazole, with a Naranjo adverse drug reaction score of 5 (probable), was the most plausible cause of the encephalopathy. The other medicines, including baclofen, had a negative score of -3 to -2 (doubtful). All tests on infections, metabolic disorders, or interactions between medications were negative. Conclusion: This patient had a fatal encephalopathy, probably associated with long-standing exposure to high plasma concentration peaks of metronidazole, due to a once-dally dose of 1500 ing IV over several weeks. (Clin Ther. 2010;32:60-64) (C) 2010 Excerpta Medica Inc.
- Published
- 2010
- Full Text
- View/download PDF
5. Extracorporeal membrane oxygenation in the treatment of poisoned patients
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de Lange, D.W., Sikma, M.A., and Meulenbelt, J.
- Subjects
Circulatory shock ,Poisoning ,Intoxication ,Journal Article ,ARDS ,Review ,ECMO ,ECLS ,Toxicology - Abstract
CONTEXT : Although extracorporeal membrane oxygenation (ECMO) was used in many patients following its introduction in 1972, most hospitals had abandoned this experimental treatment for adult patients. Recently, improvements in the ECMO circuitry rendered it more biocompatible. The surprisingly low mortality in patients with severe acute respiratory distress syndrome who were treated with ECMO in the influenza A/H1N1 pandemic of 2009 resurrected interest in ECMO in many intensive care units around the world. OBJECTIVES: This article reviews the different techniques of ECMO, the indications, contraindications and complications of its use, its role in poisoned patients and the ethics of its use. METHODS: We searched Pubmed, Toxnet, Cochrane database and Embase from 1966 to September 2012 using the search terms (''extracorporeal membrane oxygenation'', 'extracorporeal life support', 'ECMO', 'ECLS', 'assist-device', and 'intox*' or 'poison*'). These searches identified 242 papers of which 116 described ECMO in conditions other than intoxications or were reviews. In total 46 publications selected for this manuscript were case reports or case series involving poisoned patients. ECMO TECHNIQUES: Two types of ECMO are used: veno-venous ECMO (VV-ECMO) or veno-arterial ECMO (VA-ECMO). VV-ECMO is used for patients with severe ARDS to secure adequate oxygenation of the organs while protecting the lungs from harmful ventilation pressures or prolonged inspiratory fraction of oxygen. VA-ECMO can be used whenever the patient remains in shock despite adequate fluid resuscitation and is refractory to administration of inotropes and vasopressors. INDICATIONS: The organ support that can be applied with ECMO makes it especially useful in patients with severe poisoning as the clinical impact of the intoxication is often temporary; ECMO can be used as a 'bridge to recovery'. CONTRAINDICATIONS: Absolute contraindications are uncontrolled coagulopathy and severe intracranial bleeding, which precludes the use of anticoagulation therapy. Relative contraindications to ECMO include advanced age, severe irreversible brain injury, untreatable metastatic cancer, severe organ dysfunction (some suggest a Sequential Organ Failure Assessment (SOFA) score > 15), and high pressure positive pressure ventilation for more than 7 days. COMPLICATIONS: The most common complication of ECMO is either bleeding at the cannulation site (in VV-ECMO) or bleeding at the surgical entry site (in VA-ECMO). Overall bleeding complications currently occur in 10-36% patients, and intracranial haemorrhage is seen in up to 6% of patients. ECMO should be reserved, therefore, for the most severely ill poisoned patients with a high risk of death. ECMO in poisoned patients. There are no randomised trials of ECMO in poisoned patients with refractory shock or who have ARDS caused by an intoxication. VV-ECMO can be considered in patients with type l and ll respiratory failure. In patients with life-threatening haemodynamic instability, VA-ECMO can be considered when shock persists despite volume administration, inotropes and vasoconstrictors, and (sometimes) intra-aortic balloon counterpulsation. Typical examples include poisoning due to calcium channel antagonists, beta-blockers, tricyclic antidepressants, chloroquine and colchicine. ETHICS OF ECMO USE: It is only ethical to use such a costly intervention (£19,252 and US$ 31,000 per quality-adjusted life year) if the treatment has a real purpose such as a 'bridge to recovery', a 'bridge to transplant', or a 'bridge to permanent assist device' (in the case of persistent cardiac failure). CONCLUSIONS: In the last decade, ECMO equipment has improved considerably, rendering it more biocompatible, and it has been used more frequently as an assist device for patients needing oxygenation as well as circulatory support. ECMO is considered a good salvage therapy for patients who are severely poisoned with ARDS or refractory circulatory shock.
- Published
- 2013
6. Extracorporeal membrane oxygenation in the treatment of poisoned patients
- Author
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Other research (not in main researchprogram), Intensive Care Centrum, Spoedeisende Hulp, NVIC, de Lange, D.W., Sikma, M.A., Meulenbelt, J., Other research (not in main researchprogram), Intensive Care Centrum, Spoedeisende Hulp, NVIC, de Lange, D.W., Sikma, M.A., and Meulenbelt, J.
- Published
- 2013
7. Irreversible encephalopathy after treatment with high-dose intravenous metronidazole.
- Author
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Risk Assessment of Toxic and Immunomodulatory Agents, Dep IRAS, Groothoff, M.V.R., Hofmeijer, J., Sikma, M.A., Meulenbelt, J., Risk Assessment of Toxic and Immunomodulatory Agents, Dep IRAS, Groothoff, M.V.R., Hofmeijer, J., Sikma, M.A., and Meulenbelt, J.
- Published
- 2010
8. A breakthrough in cryosurgery.
- Author
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Sikma, M.A., Coenen, J., Kloosterziel, C., Hasselt, B.A., Ruers, T.J.M., Sikma, M.A., Coenen, J., Kloosterziel, C., Hasselt, B.A., and Ruers, T.J.M.
- Abstract
Item does not contain fulltext, Liver cryosurgery is one of the treatment options for unresectable liver metastases. Indications for the use of this treatment instead of classic surgery are bilobar disease, location of the tumor at an irresectable anatomic site, and comorbid conditions of the patient. Possible complications of cryosurgery are hemorrhage, coagulopathy, pneumonia, pleural effusion, abdominal abscess, and bile fistula. We describe a patient in whom a hepatobronchial fistula developed after cryosurgery. The patient had cryosurgery because of an unresectable liver metastasis in a Dukes' C rectal carcinoma. More details are given in the case report. To our knowledge, a hepatobronchial fistula as a complication of cryosurgery has never been reported. It therefore should be added to the list of possible cryosurgery complications.
- Published
- 2002
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