Your search keyword '"Schmidt, Keith T."' showing total 4 results

1. Population pharmacokinetic analysis of nanoparticle-bound and free camptothecin after administration of NLG207 in adults with advanced solid tumors.

Author

Schmidt, Keith T., Huitema, Alwin D. R., Dorlo, Thomas P. C., Peer, Cody J., Cordes, Lisa M., Sciuto, Linda, Wroblewski, Susan, Pommier, Yves, Madan, Ravi A., Thomas, Anish, and Figg, William D.

Subjects

*CAMPTOTHECIN, *DNA topoisomerase I, *PHARMACOKINETICS, *BODY weight, *CLINICAL trials, *PACLITAXEL

Abstract

Purpose: NLG207 (formerly CRLX101) is a nanoparticle–drug conjugate (NDC) of the potent topoisomerase I inhibitor, camptothecin (CPT). The present study sought to characterize the complex pharmacokinetics (PK) of NLG207 and better describe CPT release from nanoparticles using a population PK (popPK) model. Methods: From 27 patients enrolled on two phase II clinical trials (NCT02769962 and NCT03531827), dense sampling was performed up to 48 h post-administration of NLG207 during cycle one and six of treatment; samples were also collected at ~ 360 h post-dose. Conjugated and free CPT concentrations were quantified from each sample, resulting in 477 observations to build a popPK model using non-linear mixed-effects modeling. Results: The PK of NLG207 was characterized by combining two linear two-compartment models with first-order kinetics each to describe nanoparticle-bound (conjugated) and free CPT. Allometric scaling based on body weight provided the best body-size descriptor for all PK parameters. The typical volumes of distribution of the conjugated CPT central and free CPT central compartments were 3.16 L (BSV CV%; 18.1%) and 21.1 L (CV%; 79.8%), respectively. CPT release from the nanoparticle formulation was characterized via an initial rapid clearance of 5.71 L/h (CV%; 62.6%), which decreased via first-order decay (estimated half-life of 0.307 h) to the steady-state value of 0.0988 L/h (CV%; 33.5%) by ~ 4 h after end of infusion. Renal clearance of free CPT was 0.874 L/h (CV%; 42.2%). Conclusion: The popPK model confirmed nanoparticle behavior of conjugated CPT and mechanistically characterized CPT release from NLG207. The current analysis provides a strong foundation for future study as a potential predictive tool in ongoing NLG207 clinical trials. [ABSTRACT FROM AUTHOR]

Published

2020

2. A population pharmacokinetic analysis of the oral CYP17 lyase and androgen receptor inhibitor seviteronel in patients with advanced/metastatic castration-resistant prostate cancer or breast cancer.

Author

Peer, Cody J., Schmidt, Keith T., Kindrick, Jessica D., Eisner, Joel R., Brown, Victoria V., Baskin-Bey, Edwina, Madan, Ravi, and Figg, William D.

Subjects

*CASTRATION-resistant prostate cancer, *ANDROGEN receptors, *ANDROGEN drugs, *BREAST cancer, *PHARMACOKINETICS, *PROSTATE cancer

Abstract

Purpose: Seviteronel is an orally-administered selective cytochrome P450c17a 17,20-lyase and androgen receptor inhibitor with anti-tumor activity in vitro and in vivo, and clinical activity in men with advanced castration-resistant prostate cancer (CRPC) and men and women with advanced breast cancer. The purpose of this study was to assess the pharmacokinetics (PK) of seviteronel across the aforementioned populations.Methods: This report describes the PK of seviteronel (50-750 mg, QD or BID) using noncompartmental and population approaches from 243 patients with advanced breast or prostate cancer pooled across 4 clinical studies. First dose and steady-state PK were examined, as well as covariates including prandial status, sex and concomitant dexamethasone.Results: Seviteronel PK can be characterized by transit absorption and a bi-phasic first-order elimination while accounting for covariance between random effects. Prandial status did not significantly affect any parameters to a clinically-relevant extent. Both sex and body weight were significant covariates on clearance, explaining 37% of the interindividual variability on that parameter. There were no significant effects from the race or the presence of a corticosteroid (either dexamethasone or prednisone).Conclusions: Seviteronel demonstrates linear PK over the dose range of 50-750 mg given either BID or QD in men with advanced CRPC or men and women with breast cancer. The disposition of seviteronel following oral administration is well described by this population PK model and can be used for accurate simulations for future studies with body weight and sex affecting clearance, but not to a clinically-meaningful degree requiring a change in the current dosing scheme. [ABSTRACT FROM AUTHOR]

Published

2019

3. Study to Compare Capsule and Liquid Formulations of Enzalutamide After Single‐Dose Administration Under Fasting Conditions in Prostate Cancer.

Author

Cordes, Lisa M., Schmidt, Keith T., Peer, Cody J., Chau, Cindy H., Redmond, Erica, Francis, Deneise, Karzai, Fatima, Madan, Ravi A., and Figg, William D.

Subjects

FASTING, PILOT projects, ANTIANDROGENS, DRUG tolerance, BLOOD plasma, PHARMACEUTICAL encapsulation, ORAL drug administration, ANTINEOPLASTIC agents, BLOOD collection, RANDOMIZED controlled trials, CANCER patients, BLIND experiment, QUESTIONNAIRES, STATISTICAL sampling, CROSSOVER trials, PROSTATE tumors

Abstract

Lessons Learned: Limited evidence suggests an acceptable pharmacokinetic profile when enzalutamide is administered via a liquid formulation extracted from the commercially available liquid‐filled soft‐gelatin capsules.Tolerability may limit use in clinical practice. Background: Enzalutamide is an established standard‐of‐care treatment for advanced prostate cancer with a commercially available formulation that may be inconvenient for some patients. We proposed a study to evaluate the bioequivalence of a liquid formulation to provide an alternative method of administration. Methods: This was a single‐dose, randomized, open‐label, two‐way crossover pilot bioequivalence study to compare two oral formulations of enzalutamide: four enzalutamide 40 mg liquid‐filled soft‐gelatin capsules (commercially available) administered whole versus enzalutamide 160 mg liquid (extracted from capsules) administered via oral syringe. To assess bioequivalence, patients were randomized to receive a single dose of one formulation, then cross over to receive the alternative formulation following a 42‐day washout period; serial plasma samples were collected over the course of 24 hours, followed by collections at 3, 8, and 42 days after the dose for both formulations. Bioequivalence of the formulations was assessed via comparisons of area under the plasma concentration–time curve (AUC) calculations per U.S. Food and Drug Administration (FDA) guidance. The study also assessed the safety and tolerability of the formulations. Results: The study failed to meet proposed accrual, with only one patient enrolled, thus limiting the bioequivalence evaluation. Based on the data from a single patient, the drug exposure (measured by AUC) of enzalutamide and N‐desmethyl enzalutamide (primary active metabolite) for the liquid formulation was 112% and 117%, respectively, compared with the capsule formulation. Although both formulations appeared well tolerated with no adverse events reported, the tolerability assessment questionnaire revealed an unpleasant taste of the liquid formulation. Conclusion: Preliminary evidence suggests a similar pharmacokinetic profile when administering liquid extracted from enzalutamide soft‐gelatin capsules compared with intact capsules in patients with prostate cancer. [ABSTRACT FROM AUTHOR]

Published

2021

4. Measurement of NLG207 (formerly CRLX101) nanoparticle-bound and released camptothecin in human plasma.

Author

Schmidt, Keith T., Peer, Cody J., Huitema, Alwin D.R., Williams, Monique D., Wroblewski, Susan, Schellens, Jan H.M., Madan, Ravi A., and Figg, William D.

Subjects

*CAMPTOTHECIN, *DNA topoisomerase I, *FREEZE-thaw cycles, *SOLID phase extraction, *DRUG interactions, *PLASMA temperature, *PHARMACOKINETICS

Abstract

• NLG207 is a nanoparticle-drug conjugate of camptothecin (topoisomerase I inhibitor). • Analytical methods were developed to measure nanoparticle-bound & free camptothecin. • The pharmacokinetic assay to quantitate plasma concentrations was accurate & precise. • NLG207 samples were stable up to 24 h at 4 °C and following 4 freeze-thaw cycles. • Clinical utility was shown via quantitation of samples from NLG207-treated patients. Camptothecin (CPT), a potent inhibitor of topoisomerase I and HIF-1α, failed to demonstrate utility as an anti-cancer agent in early clinical trial investigations, primarily due to limited clinical activity and significant toxicity attributable to unfavorable physicochemical properties (e.g. low plasma solubility, pH-labile lactone ring). NLG207 (formerly CRLX101), a nanoparticle-drug conjugate (NDC) of CPT designed to optimize plasma pharmacokinetics and facilitate drug delivery to tumors, is included as part of combination treatment in two Phase II clinical trials ongoing at the National Cancer Institute (NCT02769962 and NCT03531827). To better understand the potential for drug-drug interactions and to correlate drug exposure to clinical outcomes and pharmacodynamic biomarkers, a robust analytical method was developed to measure CPT in human plasma. Two sample processing methods were developed to quantify both NDC-bound CPT and free CPT, primarily via alteration of pH conditions. A solid-phase extraction recovered >79 % of CPT prior to quantitative analysis by ultra HPLC-MS/MS. Dynamic calibration ranges of 10 to 10,000 ng/mL and 1 to 1000 ng/mL for total and free CPT, respectively were utilized to capture clinical ranges. NLG207 NDCs demonstrated significant rates of CPT release in human plasma at room temperature after 2 h but were shown to be stable at 4 °C for 24 h and through 4 freeze/thaw cycles. This assay was used to quantitate CPT plasma concentrations in clinical samples to confirm clinical utility following NLG207 treatment in subjects with advanced prostate cancer. [ABSTRACT FROM AUTHOR]

Published

2020