Evaluation of a <scp>DTPA</scp> Prodrug, <scp>C2E5</scp> as an Orally Bioavailable Radionuclide Decorporation Agent

Sadgrove, Matthew P.; Leed, Marina G.D.; Shapariya, Shraddha; Madhura, Dora B.; Jay, Michael

doi:10.1002/ddr.21019

Cited by 14 publications

(11 citation statements)

References 21 publications

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“…The five added ester moieties greatly increase the lipophilicity of DTPA, which is measured by increased CLogP. (CLogP of -2.7 for DTPA in contrast to ClogP of 4.7 to C2E5) Studies in rats confirmed that C2E5 shows enhanced oral bioavailability compared to DTPA, with extensive but incomplete metabolism 7 and can elicit effective radionuclide decorporation following oral 8 and transdermal delivery 9 . Together, these findings suggest that this prodrug may be a useful and effective alternative treatment to DTPA.…”

Section: Introductionmentioning

confidence: 99%

Interspecies Differences in the Metabolism of a Multiester Prodrug by Carboxylesterases

Pacyniak

Leed

et al. 2016

Journal of Pharmaceutical Sciences

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The penta-ethyl ester prodrug of the chelating agent diethylene triamine pentaacetic acid (DTPA) referred to as C2E5, is being developed as an orally bioavailable radionuclide decorporation agent. The predicted human efficacy obtained in these experimental animals is confounded by interspecies variations of metabolism. Therefore, in the present study, carboxylesterase-mediated metabolism of [14C]-C2E5 was compared in the S9 intestinal and hepatic fractions of human, dog and rat and their respective plasma. Intestinal hydrolysis of C2E5, resulting in the formation of the tetraethyl ester of DTPA (C2E4), was only detected in human and rat. The primary metabolite in human and dog hepatic fractions was C2E4 whereas the predominant species identified in rat hepatic fractions was the triethyl ester (C2E3). Hepatic hydrolysis of C2E5 causes the formation of C2E4 in human, dog and rat and C2E3 in rat only. Minimal C2E5 hydrolysis was observed in human and dog plasma whereas in rat plasma C2E5 converted to C2E3 rapidly, followed by slower further metabolism. Both recombinant CES1 and CES2 play roles in C2E5 metabolism. Together, these data suggest that dogs may be the most appropriate species for predicting human C2E5 metabolism whereas rats might be useful for clarifying the potential toxicity of C2E5 metabolites.

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Section: Introductionmentioning

confidence: 99%

Interspecies Differences in the Metabolism of a Multiester Prodrug by Carboxylesterases

Pacyniak

Leed

et al. 2016

Journal of Pharmaceutical Sciences

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“…The enzymes responsible for the metabolism of 33 to DTPA are the carboxylesterases (CESs), which could sequentially cleave the five ester moieties to form the metabolites and DTPA. 35,36 3 Oxidative stress-activated prochelators…”

Section: Accepted Manuscriptmentioning

confidence: 99%

Prochelator strategies for site-selective activation of metal chelators

Oliveri

Vecchio

2016

Journal of Inorganic Biochemistry

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“…Alternatively, in our lab we have focused on the development of DTPA pro-drugs (Sueda et al, 2012), (Sadgrove et al, 2012). The penta-ethyl ester of DTPA, although highly absorbed, is limited by its toxicity and the potential to form up to ten metabolites, thus complicating its regulatory approval.…”

Section: Introductionmentioning

confidence: 99%

Species-Dependent Chelation of 241Am by DTPA Di-Ethyl Ester

et al. 2015

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Diethylenetriaminepentaacetic acid (DTPA) is an FDA approved chelating agent for enhancing the elimination of transuranic elements such as americium from the body. Early access to therapy minimizes deposition of these radionuclides in tissues such as the bone. Due to its poor oral bioavailability, DTPA is administered as an IV injection, delaying access. Therefore a diethyl-ester analog of DTPA, named C2E2, was synthesized as a means to increase oral absorption. As a hexadentate ligand, it was hypothesized that C2E2 was capable of binding americium directly. Therefore, the protonation constants and americium stability constant for C2E2 were determined by potentiometric titration and a solvent extraction method, respectively. C2E2 was shown to bind americium with a log K of 19.6. The concentrations of C2E2, its metabolite C2E1, and DTPA required to achieve effective binding in rat, beagle, and human plasma were studied in vitro. Dose response curves for each ligand were established and the 50% maximal effective concentrations were determined for each species. As expected, higher concentrations of C2E2 were required to achieve the same degree of binding as DTPA. The results indicated that chelation in beagle plasma is more representative of the human response than rats. Finally, the pharmacokinetics of C2E2 were investigated in beagles and the data was fit to a two-compartment model with elimination from the central compartment, along with first-order absorption. Based on the in vitro data, a 100 mg kg−1 dose of C2E2 can be expected to have an effective duration of action of 3.8 hours in beagles.

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Evaluation of a DTPA Prodrug, C2E5 as an Orally Bioavailable Radionuclide Decorporation Agent

Cited by 14 publications

References 21 publications

Interspecies Differences in the Metabolism of a Multiester Prodrug by Carboxylesterases

Interspecies Differences in the Metabolism of a Multiester Prodrug by Carboxylesterases

Prochelator strategies for site-selective activation of metal chelators

Species-Dependent Chelation of 241Am by DTPA Di-Ethyl Ester

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