Your search keyword '"Goldsberry, Angela"' showing total 8 results

1. Safety, pharmacodynamics, and potential benefit of omaveloxolone in Friedreich ataxia.

Author

Lynch, David, Farmer, Jennifer, Hauser, Lauren, Blair, Ian, Wang, Qing, Mesaros, Clementina, Snyder, Nathaniel, Boesch, Sylvia, Chin, Melanie, Delatycki, Martin, Giunti, Paola, Goldsberry, Angela, Hoyle, Chad, McBride, Michael, Nachbauer, Wolfgang, OGrady, Megan, Perlman, Susan, Subramony, S, Wilmot, George, Zesiewicz, Theresa, and Meyer, Colin

Subjects

Adolescent, Adult, Dose-Response Relationship, Drug, Female, Friedreich Ataxia, Humans, Male, NF-E2-Related Factor 2, NF-kappa B, Treatment Outcome, Triterpenes, Young Adult

Abstract

OBJECTIVE: Previous studies have demonstrated that suppression of Nrf2 in Friedreich ataxia tissues contributes to excess oxidative stress, mitochondrial dysfunction, and reduced ATP production. Omaveloxolone, an Nrf2 activator and NF-kB suppressor, targets dysfunctional inflammatory, metabolic, and bioenergetic pathways. The dose-ranging portion of this Phase 2 study assessed the safety, pharmacodynamics, and potential benefit of omaveloxolone in Friedreich ataxia patients (NCT02255435). METHODS: Sixty-nine Friedreich ataxia patients were randomized 3:1 to either omaveloxolone or placebo administered once daily for 12 weeks. Patients were randomized in cohorts of eight patients, at dose levels of 2.5-300 mg/day. RESULTS: Omaveloxolone was well tolerated, and adverse events were generally mild. Optimal pharmacodynamic changes (noted by changes in ferritin and GGT) were observed at doses of 80 and 160 mg/day. No significant changes were observed in the primary outcome, peak work load in maximal exercise testing (0.9 ± 2.9 W, placebo corrected). At the 160 mg/day dose, omaveloxolone improved the secondary outcome of the mFARS by 3.8 points versus baseline (P = 0.0001) and by 2.3 points versus placebo (P = 0.06). Omaveloxolone produced greater improvements in mFARS in patients that did not have musculoskeletal foot deformity (pes cavus). In patients without this foot deformity, omaveloxolone improved mFARS by 6.0 points from baseline (P

Published

2019

2. Safety and efficacy of omaveloxolone in patients with mitochondrial myopathy: MOTOR trial

Author

Madsen, Karen L., Buch, Astrid E., Cohen, Bruce H., Falk, Marni J., Goldsberry, Angela, Goldstein, Amy, Karaa, Amel, Koenig, Mary K., Muraresku, Colleen C., Meyer, Colin, OʼGrady, Megan, Scaglia, Fernando, Shieh, Perry B., Vockley, Jerry, Zolkipli-Cunningham, Zarazuela, Haller, Ronald G., and Vissing, John

Published

2020

3. Clinical trial recommendations for potential Alport syndrome therapies

Author

Bonebrake, Lisa, Dunleavy, Marty, Kumnick, Phil, Lagas, Sharon, Parziale, Gina, Reed, Janine, Weinstock, André, Gear, Susie, Binaso, Kristen, Manuel, Raymond, Simon, James, Appel, Gerald, Blank, Melanie, Tang, Winson, Thompson, Aliza, Torra, Roser, Lieberman, Kenneth, Licht, Christoph, Dahan, Karin, Nozu, Kandai, Kai, Hirofumi, Ricardo, Sharon, Pariser, Anne, Feldman, David, Cook, Heather, Chin, Melanie, Goldsberry, Angela, Meyer, Colin, Melia, Lisa Anne, Komers, Radko, Markels, Michael, Mercer, Alex, Prunotto, Marco, Morgenstern, Bruce, Hariri, Ali, Modur, Vijay, Turner, Neil, Gross, Oliver, Lennon, Rachel, Fornoni, Alessia, Kashtan, Clifford, Rheault, Michelle, Baigent, Colin, DeSacco, Stephano, Perin, Laura, Barua, Moumita, Nakanishi, Koichi, Jarad, George, Miner, Jeffrey, Weinstock, B. André, Feldman, David L., Kashtan, Clifford E., Miner, Jeffrey H., Rheault, Michelle N., and Simon, James F.

Published

2020

4. Safety and efficacy of omaveloxolone in patients with mitochondrial myopathy:MOTOR trial

Author

Madsen, Karen L., Buch, Astrid E., Cohen, Bruce H., Falk, Marni J., Goldsberry, Angela, Goldstein, Amy, Karaa, Amel, Koenig, Mary K., Muraresku, Colleen C., Meyer, Colin, O'Grady, Megan, Scaglia, Fernando, Shieh, Perry B., Vockley, Jerry, Zolkipli-Cunningham, Zarazuela, Haller, Ronald G., Vissing, John, Madsen, Karen L., Buch, Astrid E., Cohen, Bruce H., Falk, Marni J., Goldsberry, Angela, Goldstein, Amy, Karaa, Amel, Koenig, Mary K., Muraresku, Colleen C., Meyer, Colin, O'Grady, Megan, Scaglia, Fernando, Shieh, Perry B., Vockley, Jerry, Zolkipli-Cunningham, Zarazuela, Haller, Ronald G., and Vissing, John

Abstract

OBJECTIVE: To investigate the safety and efficacy of escalating doses of the semi-synthetic triterpenoid omaveloxolone in patients with mitochondrial myopathy. METHODS: In cohorts of 8-13, 53 participants were randomized double-blind to 12 weeks of treatment with omaveloxolone 5, 10, 20, 40, 80, or 160 mg, or placebo. Outcome measures were change in peak cycling exercise workload (primary), in 6-minute walk test (6MWT) distance (secondary), and in submaximal exercise heart rate and plasma lactate (exploratory). RESULTS: No differences in peak workload or 6MWT were observed at week 12 with omaveloxolone treatment vs placebo for all omaveloxolone dose groups. In contrast, omaveloxolone 160 mg reduced heart rate at week 12 by 12.0 ± 4.6 bpm (SE) during submaximal exercise vs placebo, p = 0.01, and by 8.7 ± 3.5 bpm (SE) vs baseline, p = 0.02. Similarly, blood lactate was 1.4 ± 0.7 mM (SE) lower vs placebo, p = 0.04, and 1.6 ± 0.5 mM (SE) lower vs baseline at week 12, p = 0.003, with omaveloxolone 160 mg treatment. Adverse events were generally mild and infrequent. CONCLUSIONS: Omaveloxolone 160 mg was well-tolerated, and did not lead to change in the primary outcome measure, but improved exploratory endpoints lowering heart rate and lactate production during submaximal exercise, consistent with improved mitochondrial function and submaximal exercise tolerance. Therefore, omaveloxolone potentially benefits patients with mitochondrial myopathy, which encourages further investigations of omaveloxolone in this patient group. CLINICALTRIALSGOV IDENTIFIER: NCT02255422. CLASSIFICATION OF EVIDENCE: This study provides Class II evidence that, for patients with mitochondrial myopathy, omaveloxolone compared to placebo did not significantly change peak exercise workload.

Published

2020

5. Clinical trial recommendations for potential Alport syndrome therapies

Author

Weinstock, B. André, primary, Feldman, David L., additional, Fornoni, Alessia, additional, Gross, Oliver, additional, Kashtan, Clifford E., additional, Lagas, Sharon, additional, Lennon, Rachel, additional, Miner, Jeffrey H., additional, Rheault, Michelle N., additional, Simon, James F., additional, Bonebrake, Lisa, additional, Dunleavy, Marty, additional, Kumnick, Phil, additional, Parziale, Gina, additional, Reed, Janine, additional, Weinstock, André, additional, Gear, Susie, additional, Binaso, Kristen, additional, Manuel, Raymond, additional, Simon, James, additional, Appel, Gerald, additional, Blank, Melanie, additional, Tang, Winson, additional, Thompson, Aliza, additional, Torra, Roser, additional, Lieberman, Kenneth, additional, Licht, Christoph, additional, Dahan, Karin, additional, Nozu, Kandai, additional, Kai, Hirofumi, additional, Ricardo, Sharon, additional, Pariser, Anne, additional, Feldman, David, additional, Cook, Heather, additional, Chin, Melanie, additional, Goldsberry, Angela, additional, Meyer, Colin, additional, Melia, Lisa Anne, additional, Komers, Radko, additional, Markels, Michael, additional, Mercer, Alex, additional, Prunotto, Marco, additional, Morgenstern, Bruce, additional, Hariri, Ali, additional, Modur, Vijay, additional, Turner, Neil, additional, Kashtan, Clifford, additional, Rheault, Michelle, additional, Baigent, Colin, additional, DeSacco, Stephano, additional, Perin, Laura, additional, Barua, Moumita, additional, Nakanishi, Koichi, additional, Jarad, George, additional, and Miner, Jeffrey, additional

Published

2020

6. Safety, pharmacodynamics, and potential benefit of omaveloxolone in Friedreich ataxia

Author

Lynch, David R., primary, Farmer, Jennifer, additional, Hauser, Lauren, additional, Blair, Ian A., additional, Wang, Qing Qing, additional, Mesaros, Clementina, additional, Snyder, Nathaniel, additional, Boesch, Sylvia, additional, Chin, Melanie, additional, Delatycki, Martin B., additional, Giunti, Paola, additional, Goldsberry, Angela, additional, Hoyle, Chad, additional, McBride, Michael G., additional, Nachbauer, Wolfgang, additional, O'Grady, Megan, additional, Perlman, Susan, additional, Subramony, S. H., additional, Wilmot, George R., additional, Zesiewicz, Theresa, additional, and Meyer, Colin, additional

Published

2018

7. Topical application of RTA 408 lotion activates Nrf2 in human skin and is well-tolerated by healthy human volunteers

Author

Reisman, Scott A., primary, Goldsberry, Angela R., additional, Lee, Chun-Yue I., additional, O’Grady, Megan L., additional, Proksch, Joel W., additional, Ward, Keith W., additional, and Meyer, Colin J., additional

Published

2015

8. Topical application of RTA 408 lotion activates Nrf2 in human skin and is welltolerated by healthy human volunteers

Author

Reisman, Scott A., Goldsberry, Angela R., Lee, Chun-Yue I., O’Grady, Megan L., Proksch, Joel W., Ward, Keith W., and Meyer, Colin J.

Abstract

Background: Topical application of the synthetic triterpenoid RTA 408 to rodents elicits a potent dermal cytoprotective phenotype through activation of the transcription factor Nrf2. Therefore, studies were conducted to investigate if such cytoprotective properties translate to human dermal cells, and a topical lotion formulation was developed and evaluated clinically. Methods: In vitro, RTA 408 (3–1000 nM) was incubated with primary human keratinocytes for 16 h. Ex vivo, RTA 408 (0.03, 0.3, or 3 %) was applied to healthy human skin explants twice daily for 3 days. A Phase 1 healthy volunteer clinical study with RTA 408 Lotion (NCT02029716) consisted of 3 sequential parts. In Part A, RTA 408 Lotion (0.5 %, 1 %, and 3 %) and lotion vehicle were applied to individual 4-cm2 sites twice daily for 14 days. In Parts B and C, separate groups of subjects had 3 % RTA 408 Lotion applied twice daily to a 100-cm2 site for 14 days or a 500-cm2 site for 28 days. Results: RTA 408 was well-tolerated in both in vitro and ex vivo settings up to the highest concentrations tested. Further, RTA 408 significantly and dose-dependently induced a variety of Nrf2 target genes. Clinically, RTA 408 Lotion was also well-tolerated up to the highest concentration, largest surface area, and longest duration tested. Moreover, significant increases in expression of the prototypical Nrf2 target gene NQO1 were observed in skin biopsies, suggesting robust activation of the pharmacological target. Conclusions: Overall, these data suggest RTA 408 Lotion is well-tolerated, activates Nrf2 in human skin, and appears suitable for continued clinical development. [ABSTRACT FROM AUTHOR]

Published

2015