Jyoti Paliwal scite author profile

US FDA released guidelines for bioanalytical method validation in 2001 and it became the basis for guidelines such as ANVISA and EMA. Even though there is a general agreement between these guidelines in terms of evaluation of validation parameters, significant diversity exists with respect to methodology employed. Present review compares and summarizes the regulatory guidelines issued by US FDA, ANVISA and EMA for bioanalytical method validation. This review also discusses evaluation of certain validation parameters such as matrix effect, incurred sample reanalysis, various stability aspects, effect of anticoagulant counter ions, specificity in the presence of concomitant medications, and identification of pharmacokinetic repeats wherein specific guidance and general consensus amongst scientific community does not exist.

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Arterolane, a New Synthetic Trioxolane for Treatment of UncomplicatedPlasmodium falciparumMalaria: A Phase II, Multicenter, Randomized, Dose‐Finding Clinical Trial

Valecha

Looareesuwan

Mårtensson

et al. 2010

CLIN INFECT DIS

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Pharmacokinetics and Pharmacodynamics of Endoperoxide Antimalarials

Gautam¹,

Ahmed²,

Batra³

et al. 2009

CDM

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There are several clinically useful endoperoxides, mainly artemisinin derivatives available in market for the treatment of malaria. These are highly potent drugs, with fastest parasite reduction ratio, broadest parasite stage specificity and effectiveness against all species of plasmodium in human. Endoperoxides are crystalline compounds having poor aqueous solubility. Several theories have been proposed for their mechanism of action, but the understanding is still incomplete. The major limitation of this class of compounds is the short half-life, requiring frequent administration, leading to noncompliance and recrudescence. Therefore, WHO recommends their use in combination with long acting antimalarial drugs (Artemisinin based combination therapy, ACT) to manage drug resistance, recrudescence, and non compliance. Endoperoxide compounds bind selectively to malaria-infected red blood cells and moderately to human plasma proteins. Artemisinin derivatives are converted primarily to the bioactive metabolite dihydroartemisinin after parenteral, oral or rectal administration. The rate of conversion is lowest for artelinic acid and highest for the water-soluble artesunate. Such conversion occurs largely in the liver by CYP enzymes. Oral bioavailability in animals ranges between 19 to 35%. Based on their liphophilicity, they tend to cross the blood-brain barrier, causing neurotoxicity in animal models. Efforts have been made to understand and develop pharmacokinetic-pharmacodynamic (PK-PD) correlation and identify PK-PD indices of endoperoxides. In the absence of the above, the selection of doses in ACTs has been empirical. There are several reports on clinical pharmacokinetic interactions of endoperoxides and their long acting partner drugs but as on date no clinically significant interaction has been reported. This review is an update on physicochemical, pharmacokinetic and pharmacodynamic properties of the endoperoxide antimalarials.

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Arterolane Maleate Plus Piperaquine Phosphate for Treatment of Uncomplicated Plasmodium falciparum Malaria: A Comparative, Multicenter, Randomized Clinical Trial

Valecha

Krudsood

Tangpukdee

et al. 2012

Clinical Infectious Diseases

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Novel molecular targets for antimalarial chemotherapy

Jana¹,

Paliwal²

2007

International Journal of Antimicrobial Agents

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Jyoti Paliwal

International Guidelines for Bioanalytical Method Validation: A Comparison and Discussion on Current Scenario

Arterolane, a New Synthetic Trioxolane for Treatment of UncomplicatedPlasmodium falciparumMalaria: A Phase II, Multicenter, Randomized, Dose‐Finding Clinical Trial

Pharmacokinetics and Pharmacodynamics of Endoperoxide Antimalarials

Arterolane Maleate Plus Piperaquine Phosphate for Treatment of Uncomplicated Plasmodium falciparum Malaria: A Comparative, Multicenter, Randomized Clinical Trial

Novel molecular targets for antimalarial chemotherapy

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