Pharmacologic activity and pharmacokinetics of metabolites of regorafenib in preclinical models
Abstract Regorafenib is an orally administered inhibitor of protein kinases involved in tumor angiogenesis, oncogenesis, and maintenance of the tumor microenvironment. Phase III studies showed that regorafenib has efficacy in patients with advanced gastrointestinal stromal tumors or treatment‐refrac...
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| Series: | Cancer Medicine |
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| Online Access: | https://doi.org/10.1002/cam4.883 |
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doaj-16c86fc82aff40a3b594ce21968b89fc2020-11-25T03:32:27ZengWileyCancer Medicine2045-76342016-11-015113176318510.1002/cam4.883Pharmacologic activity and pharmacokinetics of metabolites of regorafenib in preclinical modelsDieter Zopf0Iduna Fichtner1Ajay Bhargava2Wolfram Steinke3Karl‐Heinz Thierauch4Konstanze Diefenbach5Scott Wilhelm6Frank‐Thorsten Hafner7Michael Gerisch8Drug Discovery Bayer Pharma AG Müllerstraße 178 Berlin 13353 GermanyExperimental Pharmacology & Oncology GmbH Robert‐Rössle‐Str. 10 Berlin‐Buch 13125 GermanyShakti Bioresearch 1 Bradley Road, STE 401 Woodbridge Connecticut 06525Pharmacokinetic Imaging Consulting & Autoradiography Services Halverscheid 13, D‐58553 Halver GermanyDrug Discovery Bayer Pharma AG Müllerstraße 178 Berlin 13353 GermanyDrug Discovery Bayer Pharma AG Müllerstraße 178 Berlin 13353 GermanyBayer HealthCare Pharmaceuticals 100 Bayer Blvd Whippany New Jersey 07981Drug Discovery Bayer Pharma AG Müllerstraße 178 Berlin 13353 GermanyDrug Discovery Bayer Pharma AG Müllerstraße 178 Berlin 13353 GermanyAbstract Regorafenib is an orally administered inhibitor of protein kinases involved in tumor angiogenesis, oncogenesis, and maintenance of the tumor microenvironment. Phase III studies showed that regorafenib has efficacy in patients with advanced gastrointestinal stromal tumors or treatment‐refractory metastatic colorectal cancer. In clinical studies, steady‐state exposure to the M‐2 and M‐5 metabolites of regorafenib was similar to that of the parent drug; however, the contribution of these metabolites to the overall observed clinical activity of regorafenib cannot be investigated in clinical trials. Therefore, we assessed the pharmacokinetics and pharmacodynamics of regorafenib, M‐2, and M‐5 in vitro and in murine xenograft models. M‐2 and M‐5 showed similar kinase inhibition profiles and comparable potency to regorafenib in a competitive binding assay. Inhibition of key target kinases by all three compounds was confirmed in cell‐based assays. In murine xenograft models, oral regorafenib, M‐2, and M‐5 significantly inhibited tumor growth versus controls. Total peak plasma drug concentrations and exposure to M‐2 and M‐5 in mice after repeated oral dosing with regorafenib 10 mg/kg/day were comparable to those in humans. In vitro studies showed high binding of regorafenib, M‐2, and M‐5 to plasma proteins, with unbound fractions of ~0.6%, ~0.9%, and ~0.4%, respectively, in murine plasma and ~0.5%, ~0.2%, and ~0.05%, respectively, in human plasma. Estimated free plasma concentrations of regorafenib and M‐2, but not M‐5, exceeded the IC50 at human and murine VEGFR2, suggesting that regorafenib and M‐2 are the primary contributors to the pharmacologic activity of regorafenib in vivo.https://doi.org/10.1002/cam4.883Antitumor activitymetabolitemultikinase inhibitorpharmacologyregorafenib |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Dieter Zopf Iduna Fichtner Ajay Bhargava Wolfram Steinke Karl‐Heinz Thierauch Konstanze Diefenbach Scott Wilhelm Frank‐Thorsten Hafner Michael Gerisch |
| spellingShingle |
Dieter Zopf Iduna Fichtner Ajay Bhargava Wolfram Steinke Karl‐Heinz Thierauch Konstanze Diefenbach Scott Wilhelm Frank‐Thorsten Hafner Michael Gerisch Pharmacologic activity and pharmacokinetics of metabolites of regorafenib in preclinical models Cancer Medicine Antitumor activity metabolite multikinase inhibitor pharmacology regorafenib |
| author_facet |
Dieter Zopf Iduna Fichtner Ajay Bhargava Wolfram Steinke Karl‐Heinz Thierauch Konstanze Diefenbach Scott Wilhelm Frank‐Thorsten Hafner Michael Gerisch |
| author_sort |
Dieter Zopf |
| title |
Pharmacologic activity and pharmacokinetics of metabolites of regorafenib in preclinical models |
| title_short |
Pharmacologic activity and pharmacokinetics of metabolites of regorafenib in preclinical models |
| title_full |
Pharmacologic activity and pharmacokinetics of metabolites of regorafenib in preclinical models |
| title_fullStr |
Pharmacologic activity and pharmacokinetics of metabolites of regorafenib in preclinical models |
| title_full_unstemmed |
Pharmacologic activity and pharmacokinetics of metabolites of regorafenib in preclinical models |
| title_sort |
pharmacologic activity and pharmacokinetics of metabolites of regorafenib in preclinical models |
| publisher |
Wiley |
| series |
Cancer Medicine |
| issn |
2045-7634 |
| publishDate |
2016-11-01 |
| description |
Abstract Regorafenib is an orally administered inhibitor of protein kinases involved in tumor angiogenesis, oncogenesis, and maintenance of the tumor microenvironment. Phase III studies showed that regorafenib has efficacy in patients with advanced gastrointestinal stromal tumors or treatment‐refractory metastatic colorectal cancer. In clinical studies, steady‐state exposure to the M‐2 and M‐5 metabolites of regorafenib was similar to that of the parent drug; however, the contribution of these metabolites to the overall observed clinical activity of regorafenib cannot be investigated in clinical trials. Therefore, we assessed the pharmacokinetics and pharmacodynamics of regorafenib, M‐2, and M‐5 in vitro and in murine xenograft models. M‐2 and M‐5 showed similar kinase inhibition profiles and comparable potency to regorafenib in a competitive binding assay. Inhibition of key target kinases by all three compounds was confirmed in cell‐based assays. In murine xenograft models, oral regorafenib, M‐2, and M‐5 significantly inhibited tumor growth versus controls. Total peak plasma drug concentrations and exposure to M‐2 and M‐5 in mice after repeated oral dosing with regorafenib 10 mg/kg/day were comparable to those in humans. In vitro studies showed high binding of regorafenib, M‐2, and M‐5 to plasma proteins, with unbound fractions of ~0.6%, ~0.9%, and ~0.4%, respectively, in murine plasma and ~0.5%, ~0.2%, and ~0.05%, respectively, in human plasma. Estimated free plasma concentrations of regorafenib and M‐2, but not M‐5, exceeded the IC50 at human and murine VEGFR2, suggesting that regorafenib and M‐2 are the primary contributors to the pharmacologic activity of regorafenib in vivo. |
| topic |
Antitumor activity metabolite multikinase inhibitor pharmacology regorafenib |
| url |
https://doi.org/10.1002/cam4.883 |
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