Literature DB >> 18810398

High absolute bioavailability of methylene blue given as an aqueous oral formulation.

Ingeborg Walter-Sack1, Jens Rengelshausen, Heike Oberwittler, Juergen Burhenne, Olaf Mueller, Peter Meissner, Gerd Mikus.   

Abstract

PURPOSE: Methylene blue (MB) has recently been reevaluated for malaria treatment. With the aim of excluding treatment failures due to low bioavailability, we have investigated the absolute bioavailability of MB given as an aqueous oral formulation and its interaction with chloroquine (CQ).
METHODS: A phase I study in 16 healthy individuals was performed as a monocenter prospective open randomized intra-individual cross-over comparison of MB single doses [50 mg intravenous (i.v.), 500 mg orally, separated by a 1-week wash-out]. After a second week, the group was split for a randomized parallel group comparison of CQ 750 mg administered orally alone or combined with 500 mg MB orally.
RESULTS: Mean MB plasma area under the substrate concentration-time curve (AUC 0-infinity) was 7,639 +/- 3,384 ng/mL*h and 51,171 +/- 17,147 ng/mL*h after i.v. and oral administration, respectively (dosage 1:10), and 76,897 +/- 46,037 ng/mL*h after MB combined with CQ. The absolute bioavailability was 72.3 +/- 23.9%. Co-administration with CQ significantly increased MB plasma concentrations (p <or= 0.016); CQ kinetics remained unaffected.
CONCLUSION: The absolute bioavailability of MB is high. Co-administration of MB and CQ increases plasma, but not whole blood MB concentrations.

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Year:  2008        PMID: 18810398     DOI: 10.1007/s00228-008-0563-x

Source DB:  PubMed          Journal:  Eur J Clin Pharmacol        ISSN: 0031-6970            Impact factor:   2.953


  27 in total

1.  Pharmacokinetics and organ distribution of intravenous and oral methylene blue.

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Journal:  Eur J Clin Pharmacol       Date:  2000-06       Impact factor: 2.953

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Review 5.  Clinical pharmacokinetics and metabolism of chloroquine. Focus on recent advancements.

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6.  The single dose kinetics of chloroquine and its major metabolite desethylchloroquine in healthy subjects.

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8.  Quantification of cationic anti-malaria agent methylene blue in different human biological matrices using cation exchange chromatography coupled to tandem mass spectrometry.

Authors:  Jürgen Burhenne; Klaus-Dieter Riedel; Jens Rengelshausen; Peter Meissner; Olaf Müller; Gerd Mikus; Walter E Haefeli; Ingeborg Walter-Sack
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Review 9.  Methylene blue in the treatment and prevention of ifosfamide-induced encephalopathy: report of 12 cases and a review of the literature.

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  38 in total

1.  Quantitative assessment of Plasmodium falciparum sexual development reveals potent transmission-blocking activity by methylene blue.

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3.  Methylene blue modulates β-secretase, reverses cerebral amyloidosis, and improves cognition in transgenic mice.

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4.  Methylene blue inhibits the asexual development of vivax malaria parasites from a region of increasing chloroquine resistance.

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5.  Multimodal Randomized Functional MR Imaging of the Effects of Methylene Blue in the Human Brain.

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6.  Methylene blue modulates huntingtin aggregation intermediates and is protective in Huntington's disease models.

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7.  Methylene blue upregulates Nrf2/ARE genes and prevents tau-related neurotoxicity.

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9.  A severe case of vasoplegic shock following metformin overdose successfully treated with methylene blue as a last line therapy.

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10.  Phenothiazine-mediated rescue of cognition in tau transgenic mice requires neuroprotection and reduced soluble tau burden.

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Journal:  Mol Neurodegener       Date:  2010-11-01       Impact factor: 14.195

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