The ontogeny of P-glycoprotein in the developing human blood–brain barrier: implication for opioid toxicity in neonates

Lam, Jessica; Baello, Stephanie; Iqbal, Majid; Kelly, Lauren; Shannon, Patrick; Chitayat, David; Matthews, Stephen G.; Koren, Gideon

doi:10.1038/pr.2015.119

Cited by 74 publications

(72 citation statements)

References 34 publications

(50 reference statements)

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“…Nevertheless, in one pediatric study (n = 70, including 46 infants), seizures occurred in four infants aged #4 months (Slatter et al, 2011). In such young children, organization of the neurovascular unit and expression of ABCB1 in the brain capillary endothelium is expected to be diminished in relation to those above 1 year of age, similar to when comparing the JR to the YAR used in our study (Gazzin et al, 2008;Ose et al, 2008;Saunders et al, 2012;Semple et al, 2013;Ghersi-Egea, 2013, 2015;Lam et al, 2015). One may hypothesize that the seizure appearance in those youngest patients could be related, at least in part, from the higher brain penetration of TREO and/or S,S-EBDM.…”

Section: Penetration Of Treosulfan and Its Monoepoxide Into Cnssupporting

confidence: 67%

Penetration of Treosulfan and its Active Monoepoxide Transformation Product into Central Nervous System of Juvenile and Young Adult Rats

et al. 2015

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Treosulfan (TREO) is currently investigated as an alternative treatment of busulfan in conditioning before hematopoietic stem cell transplantation. The knowledge of the blood-brain barrier penetration of the drug is still scarce. In this paper, penetration of TREO and its active monoepoxide (S,S-EBDM) and diepoxide (S,S-DEB) into the CNS was studied in juvenile (JR) and young adult rats (YAR) for the first time. CD rats of both sexes (n = 96) received an intravenous dose of TREO 500 mg/kg b.wt. Concentrations of TREO, S,S-EBDM, and S,S-DEB in rat plasma, brain, and cerebrospinal fluid (CSF, in YAR only) were determined by validated bioanalytical methods. Pharmacokinetic calculations were performed in WinNonlin using a noncompartmental analysis and statistical evaluation was done in Statistica software. In male JR, female JR, male YAR, and female YAR, the brain/plasma area under the curve (AUC) ratio for unbound TREO was 0.14, 0.17, 0.10, and 0.07 and for unbound S,S-EBDM, it was 0.52, 0.48, 0.28, and 0.22, respectively. The CSF/plasma AUC ratio in male and female YAR was 0.12 and 0.11 for TREO and 0.66 and 0.64 for S,S-EBDM, respectively. Elimination rate constants of TREO and S,S-EBDM in all the matrices were sex-independent with a tendency to be lower in the JR. No quantifiable levels of S,S-DEB were found in the studied samples. TREO and S,S-EBDM demonstrated poor and sex-independent penetration into CNS. However, the brain exposure was greater in juvenile rats, so very young children might potentially be more susceptible to high-dose TREO-related CNS exposure than young adults.

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Section: Penetration Of Treosulfan and Its Monoepoxide Into Cnssupporting

confidence: 67%

Penetration of Treosulfan and its Active Monoepoxide Transformation Product into Central Nervous System of Juvenile and Young Adult Rats

et al. 2015

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“…This was explained by a deficiency in p-glycoprotein 47. These effects have not been shown in humans; studies exploring p-glycoprotein levels in the developing human brain suggest the protein is present from an early gestation and levels increase with postnatal age, reaching adult levels by 3–6 months of age 48. Recent studies have also challenged the long-standing belief that the blood–brain barrier is ‘immature’, ‘leaky’ or ‘incomplete’ in newborns and young infants; these studies indicate that there is significant functional capacity early in brain development 49–51…”

Section: Commentarymentioning

confidence: 99%

Question 1: Is it safe to use ivermectin in children less than five years of age and weighing less than 15 kg?

Wilkins

Steer²,

Cranswick³

et al. 2018

Arch Dis Child

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“…P-gp expression at birth is quite low and reaches adult levels only after 6 months. This plays a large role in the susceptibility to central nervous effects from opioids [30] and possibly also for other P-gp substrates such as ivermectin. No controlled trials of ivermectin pharmacokinetics and safety have been performed in neonates and infants.…”

Section: Essential Pharmacologymentioning

confidence: 99%

Ivermectin to reduce malaria transmission I. Pharmacokinetic and pharmacodynamic considerations regarding efficacy and safety

Chaccour

Hammann

Rabinovich

2017

Malar J

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Ivermectin is an endectocide that has been used broadly in single dose community campaigns for the control of onchocerciasis and lymphatic filariasis for more than 30 years. There is now interest in the potential use of ivermectin regimens to reduce malaria transmission, envisaged as community-wide campaigns tailored to transmission patterns and as complement of the local vector control programme. The development of new ivermectin regimens or other novel endectocides will require integrated development of the drug in the context of traditional entomological tools and endpoints. This document examines the main pharmacokinetic and pharmacodynamic parameters of the medicine and their potential influence on its vector control efficacy and safety at population level. This information could be valuable for trial design and clinical development into regulatory and policy pathways.Electronic supplementary materialThe online version of this article (doi:10.1186/s12936-017-1801-4) contains supplementary material, which is available to authorized users.

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The ontogeny of P-glycoprotein in the developing human blood–brain barrier: implication for opioid toxicity in neonates

Cited by 74 publications

References 34 publications

Penetration of Treosulfan and its Active Monoepoxide Transformation Product into Central Nervous System of Juvenile and Young Adult Rats

Penetration of Treosulfan and its Active Monoepoxide Transformation Product into Central Nervous System of Juvenile and Young Adult Rats

Question 1: Is it safe to use ivermectin in children less than five years of age and weighing less than 15 kg?

Ivermectin to reduce malaria transmission I. Pharmacokinetic and pharmacodynamic considerations regarding efficacy and safety

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