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2. Lidocaine as treatment for neonatal seizures: Evaluation of previously developed population pharmacokinetic models and dosing regimen

Author

Favie, LMA, Huitema, ADR, Broek, MPB, Rademaker, CMA, de Haan, TR, van Straaten, HL, Simons, SHP (Sinno), Rijken, M, Nuytemans, D, Egberts, TC, Groenendaal, F, Brouwer, MJ, Tollenaer, SM, Jebbink-Akkerman, L, Dudink, J, de Jonge, RCJ, Bos, AA, Pediatrics, Neonatology, AGEM - Digestive immunity, AGEM - Endocrinology, metabolism and nutrition, and Amsterdam Reproduction & Development (AR&D)

Subjects
Lidocaine, medicine.medical_treatment, Population, 030226 pharmacology & pharmacy, neonatology, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Hypothermia, Induced, Seizures, medicine, Humans, Pharmacology (medical), 030212 general & internal medicine, Adverse effect, education, pharmacometrics, mass spectrometry, Pharmacology, education.field_of_study, Epilepsy, business.industry, Infant, Newborn, Original Articles, Hypothermia, Pharmacometrics, Confidence interval, Anticonvulsant, Anesthesia, modelling and simulation, Anticonvulsants, Original Article, clinical pharmacology, medicine.symptom, business, drug utilization, medicine.drug
Abstract

Aims: Lidocaine is used to treat neonatal seizures refractory to other anticonvulsants. It is effective, but also associated with cardiac toxicity. Previous studies have reported on the pharmacokinetics of lidocaine in preterm and term neonates and proposed a dosing regimen for effective and safe lidocaine use. The objective of this study was to evaluate the previously developed pharmacokinetic models and dosing regimen. As a secondary objective, lidocaine effectiveness and safety were assessed. Methods: Data from preterm neonates and (near-)term neonates with and without therapeutic hypothermia receiving lidocaine were included. Pharmacokinetic analyses were performed using non-linear mixed effects modelling. Simulations were performed to evaluate the proposed dosing regimen. Lidocaine was considered effective if no additional anticonvulsant was required and safe if no cardiac adverse events occurred. Results: Data were available for 159 neonates; 50 (31.4%) preterm and 109 term neonates, of whom 49 (30.8%) were treated with therapeutic hypothermia. Lidocaine clearance increased with postmenstrual age by 0.69%/day (95% confidence interval 0.54–0.84%). During therapeutic hypothermia (33.5°C), lidocaine clearance was reduced by 21.8% (7.26%/°C, 95% confidence interval 1.63–11.2%) compared to normothermia (36.5°C). Simulations demonstrated that the proposed dosing regimen leads to adequate average lidocaine plasma concentrations. Effectiveness and safety were assessed in 92 neonates. Overall effectiveness was 53.3% (49/92) and 56.5% (13/23) for neonates receiving the proposed dosing regimen. No cardiac toxicity was observed. Conclusion: Lidocaine pharmacokinetics was adequately described across the entire neonatal age range. With the proposed dosing regimen, lidocaine can provide effective and safe treatment for neonatal seizures.

Published
2020

3. Phenobarbital, Midazolam Pharmacokinetics, Effectiveness, and Drug-Drug Interaction in Asphyxiated Neonates Undergoing Therapeutic Hypothermia

Author

Favie, LMA, Groenendaal, F, Broek, MPB, Rademaker, CMA, de Haan, TR, van Straaten, HL, Dijk, PH, van Heijst, A, Simons, SHP (Sinno), Dijkman, KP, Rijken, M, Zonnenberg, IA, Cools, F, Zecic, A, v.d. Lee, JH, Nuytemans, D, van Bel, F, Egberts, TC, Huitema, ADR, Brouwer, MJ, Tollenaer, SM, Jebbink-Akkerman, L, Liem, D, Steiner, K, Dudink, J, de Jonge, RCJ, Bos, Annelies, Sonnaert, M, Camfferman, FA, Favie, LMA, Groenendaal, F, Broek, MPB, Rademaker, CMA, de Haan, TR, van Straaten, HL, Dijk, PH, van Heijst, A, Simons, SHP (Sinno), Dijkman, KP, Rijken, M, Zonnenberg, IA, Cools, F, Zecic, A, v.d. Lee, JH, Nuytemans, D, van Bel, F, Egberts, TC, Huitema, ADR, Brouwer, MJ, Tollenaer, SM, Jebbink-Akkerman, L, Liem, D, Steiner, K, Dudink, J, de Jonge, RCJ, Bos, Annelies, Sonnaert, M, and Camfferman, FA

Published
2019

4. Pharmacokinetics of morphine in encephalopathic neonates treated with therapeutic hypothermia

Author

Favie, LMA, Groenendaal, F, van den Broek, MPH, Rademaker, CMA, de Haan, TR, van Straaten, HLM (Henrica / Henriette), Dijk, PH, van Heijst, A, Dudink, J, Dijkman, KP, Rijken, M, Zonnenberg, IA, Cools, F, Zecic, A, v.d. Lee, JH, Nuytemans, D, van Bel, F, Egberts, TCG (Toine), Huitema, ADR, Brouwer, MJ, Tollenaer, SM, Jebbink-Akkerman, L, Liem, D, Steiner, K, Simons, SHP (Sinno), de Jonge, RCJ, Bos, AA (Annelies), Sonnaert, M, Camfferman, FA, Favie, LMA, Groenendaal, F, van den Broek, MPH, Rademaker, CMA, de Haan, TR, van Straaten, HLM (Henrica / Henriette), Dijk, PH, van Heijst, A, Dudink, J, Dijkman, KP, Rijken, M, Zonnenberg, IA, Cools, F, Zecic, A, v.d. Lee, JH, Nuytemans, D, van Bel, F, Egberts, TCG (Toine), Huitema, ADR, Brouwer, MJ, Tollenaer, SM, Jebbink-Akkerman, L, Liem, D, Steiner, K, Simons, SHP (Sinno), de Jonge, RCJ, Bos, AA (Annelies), Sonnaert, M, and Camfferman, FA

Published
2019

6. Pharmacokinetics and pharmacodynamics of medication in asphyciated newborns during controlled hypothermia. The PharmaCool multicenter study

Author

de Haan, TR, Bijleveld, YA, v.d. Lee, JH, Groenendaal, F, van den Broek, MPH, Rademaker, CMA, van Straaten, HLM (Henrica / Henriette), van Weissenbruch, MM, Vermeulen, JR, Dijk, PH, Dudink, J, Rijken, M, van Heijst, A, Dijkman, KP, Gavilanes, D, Kaam, AH, Offringa, M (Martin), Mathot, RAA, de Haan, TR, Bijleveld, YA, v.d. Lee, JH, Groenendaal, F, van den Broek, MPH, Rademaker, CMA, van Straaten, HLM (Henrica / Henriette), van Weissenbruch, MM, Vermeulen, JR, Dijk, PH, Dudink, J, Rijken, M, van Heijst, A, Dijkman, KP, Gavilanes, D, Kaam, AH, Offringa, M (Martin), and Mathot, RAA

Published
2012

7. Early postnatal allopurinol does not improve short term outcome after severe birth asphyxia.

Author

Benders MJN, Bos AF, Rademaker CMA, Rijken M, Torrance HL, Groenendaal F, and van Bel F

Abstract

OBJECTIVE: To investigate whether postnatal allopurinol would reduce free radical induced reperfusion/reoxygenation injury of the brain in severely asphyxiated neonates. METHOD: In an interim analysis of a randomised, double blind, placebo controlled study, 32 severely asphyxiated infants were given allopurinol or a vehicle within four hours of birth. RESULTS: The analysis showed an unaltered (high) mortality and morbidity in the infants treated with allopurinol. CONCLUSION: Allopurinol treatment started postnatally was too late to reduce the early reperfusion induced free radical surge. Allopurinol administration to the fetus with (imminent) hypoxia via the mother during labour may be more effective in reducing free radical induced post-asphyxial brain damage. [ABSTRACT FROM AUTHOR]

Published
2006

8. The efficacy of the entire-vial dosing of emicizumab: Real-world evidence on plasma concentrations, bleeds, and drug waste.

Author

Donners AAMT, van der Zwet K, Rademaker CMA, Egberts TCG, Schutgens REG, and Fischer K

Abstract

Background: Prophylaxis with emicizumab provides effective bleeding protection in persons with hemophilia A (PwHA) but pressures healthcare budgets. The body weight-adjusted dosing at 7-, 14-, or 28-day intervals, according to the label, often mismatches the vial content. Entire-vial dosing resulted in therapeutic concentrations according to pharmacokinetic simulations and was introduced to avoid waste., Objectives: The objective of this study was to evaluate the efficacy of entire-vial dosing of emicizumab by investigating real-world evidence of plasma concentrations, bleeds, and drug waste., Methods: This is a single-center, observational study with PwHA receiving emicizumab in mg/kg doses according to label but dosing interval extrapolated to the nearest vial size. Patient characteristics and bleeds were compared 1 year before starting emicizumab and during emicizumab until January 2022. Concentrations were assessed at weeks 4, 12, and annually. The mean (95% CI) annualized bleed rates were compared by using negative binomial regression. Drug waste between label-based dosing and entire-vial dosing was compared., Results: A total of 112 individuals (94% severe phenotype and 9% positive FVIII inhibitors) were followed for a median of 56 weeks (interquartile range [IQR] 52-68) before and 51 weeks (IQR 29-75) after starting emicizumab. The median emicizumab dose was 5.9 (IQR 5.5-6.2) mg/kg/4 wk with median concentrations of 63 (IQR 51-80) μg/mL. The annualized bleed rate of treated bleeds before emicizumab was 3.6 (95% CI 2.9-4.4) and was 0.8 (95% CI 0.6-1.1) during emicizumab ( P  < .001). Drug waste was reduced by 9%., Conclusion: The entire-vial dosing of emicizumab is an attractive treatment option for PwHA leading to therapeutic plasma concentrations, good bleeding control, and drug waste avoidance., (© 2023 The Author(s).)

Published
2023
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9. Association Between the Magnitude of Intravenous Busulfan Exposure and Development of Hepatic Veno-Occlusive Disease in Children and Young Adults Undergoing Myeloablative Allogeneic Hematopoietic Cell Transplantation.

Author

Bognàr T, Bartelink IH, Egberts TCG, Rademaker CMA, Versluys AB, Slatter MA, Kletzel M, Nath CE, Cuvelier GDE, Savic RM, Dvorak C, Long-Boyle JR, Cowan MJ, Bittencourt H, Bredius RGM, Güngör T, Shaw PJ, Ansari M, Hassan M, Krajinovic M, Hempel G, Marktel S, Chiesa R, Théoret Y, Lund T, Orchard PJ, Wynn RF, Boelens JJ, and Lalmohamed A

Subjects
Administration, Intravenous, Busulfan adverse effects, Child, Humans, Transplantation Conditioning adverse effects, Young Adult, Hematopoietic Stem Cell Transplantation, Hepatic Veno-Occlusive Disease epidemiology
Abstract

Intravenous busulfan is widely used as part of myeloablative conditioning regimens in children and young adults undergoing allogeneic hematopoietic cell transplantation (HCT). Hepatic veno-occlusive disease/sinusoidal obstruction syndrome (VOD/SOS) is a serious clinical problem observed with busulfan-based conditioning HCT. The development of VOD/SOS may be associated with busulfan exposure. Getting more insight into the association between busulfan exposure and the development of VOD/SOS enables further optimization of dosing and treatment strategies. The objective of this study was to assess the association between the magnitude of busulfan exposure and the occurrence of VOD/SOS in children and young adults undergoing myeloablative conditioning with a busulfan-containing regimen before allogeneic HCT. In this observational study we included all patients who underwent allogeneic HCT with intravenous busulfan as part of the conditioning regimen at 15 pediatric transplantation centers between 2000 and 2015. The endpoint was the development of VOD/SOS. The magnitude of busulfan exposure was estimated using nonlinear mixed effect modeling and expressed as the maximal concentration (Cmax; day 1 and day 1 to 4 Cmax), cumulative area under the curve (AUC; day 1, highest 1-day AUC in 4 days, and 4-day cumulative AUC), cumulative time above a concentration of 300 µg/L, and clearance on day 1. A total of 88 out of 697 patients (12.6%) developed VOD/SOS. The number of alkylators in the conditioning regimen was a strong effect modifier; therefore we stratified the regression analysis for the number of alkylators. For patients receiving only busulfan as one alkylator (36.3%, n = 253), cumulative busulfan exposure (>78 mg × h/L) was associated with increased VOD/SOS risk (12.6% versus 4.7%; odds ratio [OR] = 2.95, 95% confidence interval [CI] 1.13 to 7.66). For individuals receiving busulfan with one or two additional alkylators (63.7%, n = 444), cumulative busulfan exposure (≤78 and >78 mg × h/L) did not further increase the risk of VOD/SOS (15.4% versus 15.2%; OR = 1.03, 95% CI 0.61 to 1.75). The effect of the magnitude of busulfan exposure on VOD/SOS risk in children and young adults undergoing HCT is dependent on the number of alkylators. In patients receiving busulfan as the only alkylator, higher cumulative busulfan exposure increased the risk of VOD/SOS, whereas in those receiving multiple alkylators, the magnitude of busulfan exposure did not further increase this risk., (Copyright © 2022 The American Society for Transplantation and Cellular Therapy. All rights reserved.)

Published
2022
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11. Pharmacokinetics and short-term safety of the selective NOS inhibitor 2-iminobiotin in asphyxiated neonates treated with therapeutic hypothermia.

Author

Favié LMA, Peeters-Scholte CMPCD, Bakker A, Tjabbes H, Egberts TCG, van Bel F, Rademaker CMA, Vis P, and Groenendaal F

Subjects
Asphyxia Neonatorum diagnosis, Asphyxia Neonatorum enzymology, Biotin administration & dosage, Biotin adverse effects, Biotin pharmacokinetics, Drug Administration Schedule, Enzyme Inhibitors administration & dosage, Enzyme Inhibitors adverse effects, Female, Humans, Hypoxia-Ischemia, Brain diagnosis, Hypoxia-Ischemia, Brain enzymology, Infant, Newborn, Infusions, Intravenous, Male, Netherlands, Nitric Oxide Synthase metabolism, Prospective Studies, Treatment Outcome, Asphyxia Neonatorum therapy, Biotin analogs & derivatives, Enzyme Inhibitors pharmacokinetics, Hypothermia, Induced adverse effects, Hypoxia-Ischemia, Brain prevention & control, Nitric Oxide Synthase antagonists & inhibitors
Abstract

Background: Neonatal encephalopathy following perinatal asphyxia is a leading cause for neonatal death and disability, despite treatment with therapeutic hypothermia. 2-Iminobiotin is a promising neuroprotective agent additional to therapeutic hypothermia to improve the outcome of these neonates., Methods: In an open-label study, pharmacokinetics and short-term safety of 2-iminobiotin were investigated in neonates treated with therapeutic hypothermia. Group A (n = 6) received four doses of 0.16 mg/kg intravenously q6h. Blood sampling for pharmacokinetic analysis and monitoring of vital signs for short-term safety analysis were performed. Data from group A was used to determine the dose for group B, aiming at an AUC 0-48 h of 4800 ng*h/mL., Results: Exposure in group A was higher than targeted (median AUC 0-48 h 9522 ng*h/mL); subsequently, group B (n = 6) received eight doses of 0.08 mg/kg q6h (median AUC 0-48 h 4465 ng*h/mL). No changes in vital signs were observed and no adverse events related to 2-iminobiotin occurred., Conclusion: This study indicates that 2-iminobiotin is well tolerated and not associated with any adverse events in neonates treated with therapeutic hypothermia after perinatal asphyxia. Target exposure was achieved with eight doses of 0.08 mg/kg q6h. Optimal duration of therapy for clinical efficacy needs to be determined in future clinical trials.

Published
2020
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12. Lidocaine as treatment for neonatal seizures: Evaluation of previously developed population pharmacokinetic models and dosing regimen.

Author

Favié LMA, Huitema ADR, van den Broek MPH, Rademaker CMA, de Haan TR, van Straaten HLM, Simons SHP, Rijken M, Nuytemans DHGM, Egberts TCG, and Groenendaal F

Subjects
Anticonvulsants therapeutic use, Humans, Infant, Newborn, Lidocaine therapeutic use, Seizures drug therapy, Epilepsy drug therapy, Hypothermia, Induced
Abstract

Aims: Lidocaine is used to treat neonatal seizures refractory to other anticonvulsants. It is effective, but also associated with cardiac toxicity. Previous studies have reported on the pharmacokinetics of lidocaine in preterm and term neonates and proposed a dosing regimen for effective and safe lidocaine use. The objective of this study was to evaluate the previously developed pharmacokinetic models and dosing regimen. As a secondary objective, lidocaine effectiveness and safety were assessed., Methods: Data from preterm neonates and (near-)term neonates with and without therapeutic hypothermia receiving lidocaine were included. Pharmacokinetic analyses were performed using non-linear mixed effects modelling. Simulations were performed to evaluate the proposed dosing regimen. Lidocaine was considered effective if no additional anticonvulsant was required and safe if no cardiac adverse events occurred., Results: Data were available for 159 neonates; 50 (31.4%) preterm and 109 term neonates, of whom 49 (30.8%) were treated with therapeutic hypothermia. Lidocaine clearance increased with postmenstrual age by 0.69%/day (95% confidence interval 0.54-0.84%). During therapeutic hypothermia (33.5°C), lidocaine clearance was reduced by 21.8% (7.26%/°C, 95% confidence interval 1.63-11.2%) compared to normothermia (36.5°C). Simulations demonstrated that the proposed dosing regimen leads to adequate average lidocaine plasma concentrations. Effectiveness and safety were assessed in 92 neonates. Overall effectiveness was 53.3% (49/92) and 56.5% (13/23) for neonates receiving the proposed dosing regimen. No cardiac toxicity was observed., Conclusion: Lidocaine pharmacokinetics was adequately described across the entire neonatal age range. With the proposed dosing regimen, lidocaine can provide effective and safe treatment for neonatal seizures., (© 2019 The Authors. British Journal of Clinical Pharmacology published by John Wiley & Sons Ltd on behalf of British Pharmacological Society.)

Published
2020
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13. Pharmacokinetics of morphine in encephalopathic neonates treated with therapeutic hypothermia.

Author

Favié LMA, Groenendaal F, van den Broek MPH, Rademaker CMA, de Haan TR, van Straaten HLM, Dijk PH, van Heijst A, Dudink J, Dijkman KP, Rijken M, Zonnenberg IA, Cools F, Zecic A, van der Lee JH, Nuytemans DHGM, van Bel F, Egberts TCG, and Huitema ADR

Subjects
Female, Humans, Infant, Newborn, Male, Prospective Studies, Asphyxia Neonatorum blood, Asphyxia Neonatorum therapy, Brain Diseases blood, Brain Diseases therapy, Hypothermia, Induced, Morphine administration & dosage, Morphine pharmacokinetics
Abstract

Objective: Morphine is a commonly used drug in encephalopathic neonates treated with therapeutic hypothermia after perinatal asphyxia. Pharmacokinetics and optimal dosing of morphine in this population are largely unknown. The objective of this study was to describe pharmacokinetics of morphine and its metabolites morphine-3-glucuronide and morphine-6-glucuronide in encephalopathic neonates treated with therapeutic hypothermia and to develop pharmacokinetics based dosing guidelines for this population., Study Design: Term and near-term encephalopathic neonates treated with therapeutic hypothermia and receiving morphine were included in two multicenter cohort studies between 2008-2010 (SHIVER) and 2010-2014 (PharmaCool). Data were collected during hypothermia and rewarming, including blood samples for quantification of morphine and its metabolites. Parental informed consent was obtained for all participants., Results: 244 patients (GA mean (sd) 39.8 (1.6) weeks, BW mean (sd) 3,428 (613) g, male 61.5%) were included. Morphine clearance was reduced under hypothermia (33.5°C) by 6.89%/°C (95% CI 5.37%/°C- 8.41%/°C, p<0.001) and metabolite clearance by 4.91%/°C (95% CI 3.53%/°C- 6.22%/°C, p<0.001) compared to normothermia (36.5°C). Simulations showed that a loading dose of 50 μg/kg followed by continuous infusion of 5 μg/kg/h resulted in morphine plasma concentrations in the desired range (between 10 and 40 μg/L) during hypothermia., Conclusions: Clearance of morphine and its metabolites in neonates is affected by therapeutic hypothermia. The regimen suggested by the simulations will be sufficient in the majority of patients. However, due to the large interpatient variability a higher dose might be necessary in individual patients to achieve the desired effect., Trial Registration: www.trialregister.nl NTR2529., Competing Interests: The authors have declared that no competing interests exist.

Published
2019
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14. Nitric Oxide Synthase Inhibition as a Neuroprotective Strategy Following Hypoxic-Ischemic Encephalopathy: Evidence From Animal Studies.

Author

Favié LMA, Cox AR, van den Hoogen A, Nijboer CHA, Peeters-Scholte CMPCD, van Bel F, Egberts TCG, Rademaker CMA, and Groenendaal F

Abstract

Background: Hypoxic-ischemic encephalopathy following perinatal asphyxia is a leading cause of neonatal death and disability worldwide. Treatment with therapeutic hypothermia reduced adverse outcomes from 60 to 45%. Additional strategies are urgently needed to further improve the outcome for these neonates. Inhibition of nitric oxide synthase (NOS) is a potential neuroprotective target. This article reviews the evidence of neuroprotection by nitric oxide (NO) synthesis inhibition in animal models., Methods: Literature search using the EMBASE, Medline, Cochrane, and PubMed databases. Studies comparing NOS inhibition to placebo, with neuroprotective outcome measures, in relevant animal models were included. Methodologic quality of the included studies was assessed., Results: 26 studies were included using non-selective or selective NOS inhibition in rat, piglet, sheep, or rabbit animal models. A large variety in outcome measures was reported. Outcome measures were grouped as histological, biological, or neurobehavioral. Both non-selective and selective inhibitors show neuroprotective properties in one or more outcome measures. Methodologic quality was either low or moderate for all studies., Conclusion: Inhibition of NO synthesis is a promising strategy for additional neuroprotection. In humans, intervention can only take place after the onset of the hypoxic-ischemic event. Therefore, combined inhibition of neuronal and inducible NOS seems the most likely candidate for human clinical trials. Future studies should determine its safety and effectiveness in neonates, as well as a potential sex-specific neuroprotective effect. Researchers should strive to improve methodologic quality of animal intervention studies by using a systematic approach in conducting and reporting of these studies.

Published
2018
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15. Long-Term Melatonin Therapy for Adolescents and Young Adults with Chronic Sleep Onset Insomnia and Late Melatonin Onset: Evaluation of Sleep Quality, Chronotype, and Lifestyle Factors Compared to Age-Related Randomly Selected Population Cohorts.

Author

Zwart TC, Smits MG, Egberts TCG, Rademaker CMA, and van Geijlswijk IM

Abstract

The extent of continuance of melatonin therapy initiated in pre-pubertal children with chronic sleep onset insomnia (CSOI) was investigated in young adult life. Sleep timing, sleep quality, adverse events, reasons for cessation of therapy, and patient characteristics with regard to therapy regimen, chronotype and lifestyle factors possibly influencing sleeping behavior were assessed. With an online survey using questionnaires (Pittsburgh Sleep Quality Index, Insomnia Severity Index, Morningness-Eveningness Questionnaire, and Munich Chronotype Questionnaire), outcomes were measured and compared with age-related controls. These controls were extracted from published epidemiological research programs applying the same questionnaires. At the moment of the survey, melatonin was still continued by 27.3% of the patients, with a mean treatment duration of 10.8 years. The overall average treatment duration was 7.1 years. Sleep quality of both discontinued and persistent melatonin users did not deviate from controls. Sleep timing and chronotype scores indicated evening type preference in all responders. Adverse events were scarce but the perceived timing of pubertal development suggested a tendency towards delayed puberty in former and current users of melatonin. This study may underestimate the number of children that are able to stop using melatonin due to the response rate (47.8%) and appeal for continuing users. Sleep timing parameters were based on self-reported estimates. Control populations were predominantly students and were of varying nationalities. The statistical power of this study is low due to the limited sample size. Melatonin therapy sustained for 7.1 years does not result in substantial deviations of sleep quality as compared to controls and appears to be safe. The evening type preference suggests a causal relation with CSOI. This study shows that ten years after initiation of treatment with melatonin for CSOI, approximately 75% of the patients will have normal sleep quality without medication., Competing Interests: The authors declare no conflict of interest.

Published
2018
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