Your search keyword '"Buckeridge, Clare"' showing total 17 results

1. Danuglipron (PF-06882961) in type 2 diabetes: a randomized, placebo-controlled, multiple ascending-dose phase 1 trial

Author

Saxena, Aditi R., Gorman, Donal N., Esquejo, Ryan M., Bergman, Arthur, Chidsey, Kristin, Buckeridge, Clare, and Griffith, David A.

Subjects

Hypoglycemic agents -- Testing, Type 2 diabetes -- Drug therapy, Biological sciences, Health

Abstract

Agonism of the glucagon-like peptide-1 receptor (GLP-1R) results in glycemic lowering and body weight loss and is a therapeutic strategy to treat type 2 diabetes (T2D) and obesity. We developed danuglipron (PF-06882961), an oral small-molecule GLP-1R agonist and found it had comparable efficacy to injectable peptidic GLP-1R agonists in a humanized mouse model. We then completed a placebo-controlled, randomized, double-blind, multiple ascending-dose phase 1 study (NCT03538743), in which we enrolled 98 patients with T2D on background metformin and randomized them to receive multiple ascending doses of danuglipron or placebo for 28 d, across eight cohorts. The primary outcomes were assessment of adverse events (AEs), safety laboratory tests, vital signs and 12-lead electrocardiograms. Most AEs were mild, with nausea, dyspepsia and vomiting most commonly reported. There were no clinically meaningful AEs in laboratory values across groups. Heart rate generally increased with danuglipron treatment at day 28, but no heart-rate AEs were reported. Systolic blood pressure was slightly decreased and changes in diastolic blood pressure were similar with danuglipron treatment at day 28, compared with placebo. There were no clinically meaningful electrocardiogram findings. In this study in T2D, danuglipron was generally well tolerated, with a safety profile consistent with the mechanism of action of GLP-1R agonism. Results from a phase 1 study testing a new oral GLP-1 receptor agonist, danuglipron, in patients with type 2 diabetes demonstrate acceptable safety, tolerability and pharmacokinetic profiles of the drug, with exploratory analyses suggesting potential beneficial effects on glycemic control., Author(s): Aditi R. Saxena [sup.1] , Donal N. Gorman [sup.2] , Ryan M. Esquejo [sup.1] , Arthur Bergman [sup.1] , Kristin Chidsey [sup.1] , Clare Buckeridge [sup.1] , David A. [...]

Published

2021

2. Once‐daily oral small‐molecule glucagon‐like peptide‐1 receptor agonist lotiglipron (PF‐07081532) for type 2 diabetes and obesity: Two randomized, placebo‐controlled, multiple‐ascending‐dose Phase 1 studies.

Author

Buckeridge, Clare, Tsamandouras, Nikolaos, Carvajal‐Gonzalez, Santos, Brown, Lisa S., Hernandez‐Illas, Martha, and Saxena, Aditi R.

Subjects

*GLUCAGON-like peptide-1 receptor, *GLUCAGON-like peptide-1 agonists, *PEPTIDE receptors, *TYPE 2 diabetes, *WEIGHT loss, *COMPOSITE materials, *OBESITY

Abstract

Aim: To investigate the effects of lotiglipron (PF‐07081532), a once‐daily, oral small‐molecule glucagon‐like peptide‐1 receptor agonist, in participants with type 2 diabetes (T2D) and/or obesity. Materials and Methods: Two Phase 1 randomized, double‐blind, placebo‐controlled, multiple‐ascending‐dose studies were conducted to investigate the safety, tolerability, pharmacokinetics and pharmacodynamics of lotiglipron. Results: Across the studies, 74 participants with T2D were treated for 28 or 42 days, and 26 participants with obesity without diabetes were treated for 42 days, following randomization to placebo or lotiglipron (target doses 10–180 mg/day, with dose titration to higher target doses). Most adverse events were mild (89.6%), with nausea the most frequently reported in both studies. There were no clinically meaningful adverse trends noted in safety laboratory tests, vital signs, or electrocardiogram parameters. In participants with T2D, lotiglipron resulted in dose‐dependent reductions in mean daily glucose. The 180‐mg dose was associated with least squares mean decreases from baseline in glycated haemoglobin (−1.61% [90% confidence interval {CI} –2.08, −1.14] vs. −0.61% [−1.56, 0.34] for placebo) and body weight (−5.10 kg [90% CI –6.62, −3.58] vs. −2.06 kg [90% CI –4.47, 0.36] for placebo) after 42 days; a similar magnitude of weight loss was seen in participants with obesity. The observed pharmacokinetic profile supported once‐daily dosing. Conclusions: The profile of once‐daily lotiglipron with doses up to 180 mg, as observed in these two Phase 1 studies, indicated a safety and tolerability profile consistent with the mechanism of action, with dose‐dependent reductions in glycaemic indices (T2D) and body weight (both populations) after multiple doses. Clinicaltrials.gov identifier: NCT04305587, NCT05158244. [ABSTRACT FROM AUTHOR]

Published

2024

3. Supplementary Methods 1 from A Phase Ib First-In-Patient Study Assessing the Safety, Tolerability, Pharmacokinetics, and Pharmacodynamics of Ponsegromab in Participants with Cancer and Cachexia

Author

Crawford, Jeffrey, primary, Calle, Roberto A., primary, Collins, Susie M., primary, Weng, Yan, primary, Lubaczewski, Shannon L., primary, Buckeridge, Clare, primary, Wang, Ellen Q., primary, Harrington, Magdalena A., primary, Tarachandani, Anil, primary, Rossulek, Michelle I., primary, and Revkin, James H., primary

Published

2024

4. Supplementary Table S2 from A Phase Ib First-In-Patient Study Assessing the Safety, Tolerability, Pharmacokinetics, and Pharmacodynamics of Ponsegromab in Participants with Cancer and Cachexia

Author

Crawford, Jeffrey, primary, Calle, Roberto A., primary, Collins, Susie M., primary, Weng, Yan, primary, Lubaczewski, Shannon L., primary, Buckeridge, Clare, primary, Wang, Ellen Q., primary, Harrington, Magdalena A., primary, Tarachandani, Anil, primary, Rossulek, Michelle I., primary, and Revkin, James H., primary

Published

2024

5. Data from A Phase Ib First-In-Patient Study Assessing the Safety, Tolerability, Pharmacokinetics, and Pharmacodynamics of Ponsegromab in Participants with Cancer and Cachexia

Author

Crawford, Jeffrey, primary, Calle, Roberto A., primary, Collins, Susie M., primary, Weng, Yan, primary, Lubaczewski, Shannon L., primary, Buckeridge, Clare, primary, Wang, Ellen Q., primary, Harrington, Magdalena A., primary, Tarachandani, Anil, primary, Rossulek, Michelle I., primary, and Revkin, James H., primary

Published

2024

6. Supplementary Figure S4 from A Phase Ib First-In-Patient Study Assessing the Safety, Tolerability, Pharmacokinetics, and Pharmacodynamics of Ponsegromab in Participants with Cancer and Cachexia

Author

Crawford, Jeffrey, primary, Calle, Roberto A., primary, Collins, Susie M., primary, Weng, Yan, primary, Lubaczewski, Shannon L., primary, Buckeridge, Clare, primary, Wang, Ellen Q., primary, Harrington, Magdalena A., primary, Tarachandani, Anil, primary, Rossulek, Michelle I., primary, and Revkin, James H., primary

Published

2024

7. De novo lipogenesis is essential for platelet production in humans

Author

Kelly, Kenneth L., Reagan, William J., Sonnenberg, Gabriele E., Clasquin, Michelle, Hales, Katherine, Asano, Shoh, Amor, Paul A., Carvajal-Gonzalez, Santos, Shirai, Norimitsu, Matthews, Marcy D., Li, Kelvin W., Hellerstein, Marc K., Vera, Nicholas B., Ross, Trenton T., Cappon, Gregg, Bergman, Arthur, Buckeridge, Clare, Sun, Zhongyuan, Qejvanaj, Enida Ziso, Schmahai, Theodore, Beebe, David, Pfefferkorn, Jeffrey A., and Esler, William P.

Published

2020

8. A Phase Ib First-In-Patient Study Assessing the Safety, Tolerability, Pharmacokinetics, and Pharmacodynamics of Ponsegromab in Participants with Cancer and Cachexia

Author

Crawford, Jeffrey, primary, Calle, Roberto A., additional, Collins, Susie M., additional, Weng, Yan, additional, Lubaczewski, Shannon L., additional, Buckeridge, Clare, additional, Wang, Ellen Q., additional, Harrington, Magdalena A., additional, Tarachandani, Anil, additional, Rossulek, Michelle I., additional, and Revkin, James H., additional

Published

2023

9. Abstract CT108: First-in-patient study of the GDF-15 inhibitor ponsegromab in patients with cancer and cachexia: Safety, tolerability, and exploratory measures of efficacy

Author

Crawford, Jeffrey, primary, Calle, Roberto A., additional, Collins, Susie M., additional, Weng, Yan, additional, Lubaczewski, Shannon L., additional, Buckeridge, Clare, additional, Wang, Ellen Q., additional, Harrington, Magdalena A., additional, Tarachandani, Anil, additional, Rossulek, Michelle I., additional, and Revkin, James H., additional

Published

2023

10. A Small-Molecule Oral Agonist of the Human Glucagon-like Peptide-1 Receptor

Author

Griffith, David A., primary, Edmonds, David J., additional, Fortin, Jean-Philippe, additional, Kalgutkar, Amit S., additional, Kuzmiski, J. Brent, additional, Loria, Paula M., additional, Saxena, Aditi R., additional, Bagley, Scott W., additional, Buckeridge, Clare, additional, Curto, John M., additional, Derksen, David R., additional, Dias, João M., additional, Griffor, Matthew C., additional, Han, Seungil, additional, Jackson, V. Margaret, additional, Landis, Margaret S., additional, Lettiere, Daniel, additional, Limberakis, Chris, additional, Liu, Yuhang, additional, Mathiowetz, Alan M., additional, Patel, Jayesh C., additional, Piotrowski, David W., additional, Price, David A., additional, Ruggeri, Roger B., additional, and Tess, David A., additional

Published

2022

11. A small-molecule oral agonist of the human glucagon-like peptide-1 receptor

Author

Griffith, David A., primary, Edmonds, David J., additional, Fortin, Jean-Phillipe, additional, Kalgutkar, Amit S., additional, Kuzmiski, J. Brent, additional, Loria, Paula M., additional, Saxena, Aditi R., additional, Bagley, Scott W., additional, Buckeridge, Clare, additional, Curto, John M., additional, Derksen, David R., additional, Dias, João M., additional, Griffor, Matthew C., additional, Han, Seungil, additional, Jackson, V. Margaret, additional, Landis, Margaret S., additional, Lettiere, Daniel J., additional, Limberakis, Chris, additional, Liu, Yuhang, additional, Mathiowetz, Alan M., additional, Piotrowski, David W., additional, Price, David A., additional, Ruggeri, Roger B., additional, and Tess, David A., additional

Published

2020

12. 353-OR: Oral Small Molecule GLP-1R Agonist PF-06882961 Robustly Reduces Plasma Glucose and Body Weight after 28 Days in Adults with T2DM

Author

SAXENA, ADITI, primary, GORMAN, DONAL, additional, CHIDSEY, KRISTIN, additional, BUCKERIDGE, CLARE, additional, KIM, ALBERT M., additional, and BERGMAN, ARTHUR, additional

Published

2020

13. Human sebum requires de novo lipogenesis, which is increased in acne vulgaris and suppressed by acetyl-CoA carboxylase inhibition

Author

Esler, William P., primary, Tesz, Gregory J., additional, Hellerstein, Marc K., additional, Beysen, Carine, additional, Sivamani, Raja, additional, Turner, Scott M., additional, Watkins, Steven M., additional, Amor, Paul A., additional, Carvajal-Gonzalez, Santos, additional, Geoly, Frank J., additional, Biddle, Kathleen E., additional, Purkal, Julie J., additional, Fitch, Mark, additional, Buckeridge, Clare, additional, Silvia, Annette M., additional, Griffith, David A., additional, Gorgoglione, Matthew, additional, Hassoun, Lauren, additional, Bosanac, Suzana S., additional, Vera, Nicholas B., additional, Rolph, Timothy P., additional, Pfefferkorn, Jeffrey A., additional, and Sonnenberg, Gabriele E., additional

Published

2019

14. [O2–09–05]: SAFETY, TOLERABILITY, AND PHARMACOKINETIC AND PHARMACODYNAMIC EFFECTS OF PF‐06751979, A POTENT AND SELECTIVE ORAL BACE1 INHIBITOR: RESULTS FROM PHASE1 SINGLE AND MULTIPLE ASCENDING DOSE STUDIES IN HEALTHY YOUNG AND OLDER VOLUNTEERS

Author

Qiu, Ruolun, primary, Liu, Richann, additional, He, Ping, additional, Wills, Anne‐Marie, additional, Tankisheva, Ekaterina, additional, Alvey, Christine, additional, Buckeridge, Clare, additional, Bednar, Martin, additional, Alexander, Robert C., additional, and Chen, Danny, additional

Published

2017

15. PKNCA: Perform Pharmacokinetic Non-Compartmental Analysis

Author

Denney, Bill, primary and Buckeridge, Clare, additional

Published

2015

16. SAFETY, TOLERABILITY, AND PHARMACOKINETIC AND PHARMACODYNAMIC EFFECTS OF PF-06751979, A POTENT AND SELECTIVE ORAL BACE1 INHIBITOR: RESULTS FROM PHASE1 SINGLE AND MULTIPLE ASCENDING DOSE STUDIES IN HEALTHY YOUNG AND OLDER VOLUNTEERS

Author

Qiu, Ruolun, Liu, Richann, He, Ping, Wills, Anne-Marie, Tankisheva, Ekaterina, Alvey, Christine, Buckeridge, Clare, Bednar, Martin, Alexander, Robert C., and Chen, Danny

Published

2017

17. A Phase Ib First-In-Patient Study Assessing the Safety, Tolerability, Pharmacokinetics, and Pharmacodynamics of Ponsegromab in Participants with Cancer and Cachexia.

Author

Crawford J, Calle RA, Collins SM, Weng Y, Lubaczewski SL, Buckeridge C, Wang EQ, Harrington MA, Tarachandani A, Rossulek MI, and Revkin JH

Subjects

Adult, Humans, Growth Differentiation Factor 15 therapeutic use, Quality of Life, Antibodies, Monoclonal therapeutic use, Cachexia drug therapy, Cachexia etiology, Neoplasms complications, Neoplasms drug therapy

Abstract

Purpose: Cachexia is common in patients with advanced cancer and is associated with elevated serum growth differentiation factor 15 (GDF-15) concentrations. This first-in-patient (phase Ib), 24-week study assessed use of ponsegromab, a mAb against GDF-15, in adults with advanced cancer, cachexia, and elevated GDF-15 serum concentration., Patients and Methods: Participants (n = 10) received open-label ponsegromab subcutaneous 200 mg every 3 weeks for 12 weeks in addition to standard-of-care anticancer treatment. Ponsegromab safety, tolerability, and pharmacokinetics were assessed in addition to serum GDF-15 concentrations and exploratory measures of efficacy., Results: No treatment-related treatment-emergent adverse events, injection site reactions, or adverse trends in clinical laboratory tests, vital signs, or electrocardiogram parameters attributable to ponsegromab were identified. Median serum unbound GDF-15 concentration at baseline was 2.269 ng/mL. Following initiation of study treatment, median unbound GDF-15 concentrations were below the lower limit of quantification (0.0424 ng/mL) from day 1 (3 hours postdose) through week 15. Increases in body weight were observed at all time points during the treatment and follow-up periods. A least-squares mean (SE) increase of 4.63 (1.98) kg was observed at week 12, an increase of approximately 6.6% relative to baseline. Ponsegromab-mediated improvements in actigraphy-based assessments of physical activity and in quality of life, including appetite as assessed by Functional Assessment of Anorexia-Cachexia Therapy total and subscale scores, were also observed., Conclusions: Ponsegromab was well tolerated, suppressed serum GDF-15 concentrations, and demonstrated preliminary evidence of efficacy. These findings support the continued development of ponsegromab for the treatment of cachexia., (©2023 The Authors; Published by the American Association for Cancer Research.)

Published

2024