M.S. Weeks scite author profile

M.S. Weeks

5Publications

57Citation Statements Received

87Citation Statements Given

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Affiliations

University College London, Siga Technologies (United States)

Publications

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Comparison of the Safety and Pharmacokinetics of ST-246® after IV Infusion or Oral Administration in Mice, Rabbits and Monkeys

et al. 2011

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BackgroundST-246® is an antiviral, orally bioavailable small molecule in clinical development for treatment of orthopoxvirus infections. An intravenous (IV) formulation may be required for some hospitalized patients who are unable to take oral medication. An IV formulation has been evaluated in three species previously used in evaluation of both efficacy and toxicology of the oral formulation.Methodology/Principal FindingsThe pharmacokinetics of ST-246 after IV infusions in mice, rabbits and nonhuman primates (NHP) were compared to those obtained after oral administration. Ten minute IV infusions of ST-246 at doses of 3, 10, 30, and 75 mg/kg in mice produced peak plasma concentrations ranging from 16.9 to 238 µg/mL. Elimination appeared predominately first-order and exposure dose-proportional up to 30 mg/kg. Short IV infusions (5 to 15 minutes) in rabbits resulted in rapid distribution followed by slower elimination. Intravenous infusions in NHP were conducted at doses of 1 to 30 mg/kg. The length of single infusions in NHP ranged from 4 to 6 hours. The pharmacokinetics and tolerability for the two highest doses were evaluated when administered as two equivalent 4 hour infusions initiated 12 hours apart. Terminal elimination half-lives in all species for oral and IV infusions were similar. Dose-limiting central nervous system effects were identified in all three species and appeared related to high Cmax plasma concentrations. These effects were eliminated using slower IV infusions.Conclusions/SignificancePharmacokinetic profiles after IV infusion compared to those observed after oral administration demonstrated the necessity of longer IV infusions to (1) mimic the plasma exposure observed after oral administration and (2) avoid Cmax associated toxicity. Shorter infusions at higher doses in NHP resulted in decreased clearance, suggesting saturated distribution or elimination. Elimination half-lives in all species were similar between oral and IV administration. The administration of ST-246 was well tolerated as a slow IV infusion.

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Methylome analysis identifies a Wilms tumor epigenetic biomarker detectable in blood

et al. 2014

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Background: Wilms tumor is the most common pediatric renal malignancy and there is a clinical need for a molecular biomarker to assess treatment response and predict relapse. The known mutated genes in this tumor type show low mutation frequencies, whereas aberrant methylation at 11p15 is by far the most common aberration. We therefore analyzed the epigenome, rather than the genome, to identify ubiquitous tumor-specific biomarkers.

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Excretion of disodium Bis-2-mercaptoethanesulphonate (dimesna) in the urine of volunteers after oral dosing

Shaw

Weeks

1987

European Journal of Cancer and Clinical Oncology

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Excretion of sodium 2-mercaptoethanesulphonate (MESNA) in the urine of volunteers after oral dosing

Shaw

Weeks

1985

European Journal of Cancer and Clinical Oncology

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A Proposed Mechanism for Isophosphamide-induced Kidney Toxicity

1985

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M.S. Weeks

Comparison of the Safety and Pharmacokinetics of ST-246® after IV Infusion or Oral Administration in Mice, Rabbits and Monkeys

Methylome analysis identifies a Wilms tumor epigenetic biomarker detectable in blood

Excretion of disodium Bis-2-mercaptoethanesulphonate (dimesna) in the urine of volunteers after oral dosing

Excretion of sodium 2-mercaptoethanesulphonate (MESNA) in the urine of volunteers after oral dosing

A Proposed Mechanism for Isophosphamide-induced Kidney Toxicity

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