A phase I pharmacodynamic trial of sequential sunitinib with bevacizumab in patients with renal cell carcinoma and other advanced solid malignancies

Justine Yang Bruce; Jill M. Kolesar; Hans Hammers; Mark N. Stein; Lakeesha Carmichael; Jens Eickhoff; Susan A. Johnston; Kimberly A. Binger; Jennifer L. Heideman; Scott B. Perlman; Robert Jeraj; Glenn Liu

doi:10.1007/s00280-013-2373-9

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A phase I pharmacodynamic trial of sequential sunitinib with bevacizumab in patients with renal cell carcinoma and other advanced solid malignancies

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A phase I pharmacodynamic trial of sequential sunitinib with bevacizumab in patients with renal cell carcinoma and other advanced solid malignancies

Justine Yang Bruce, Jill M. Kolesar, Hans Hammers, Mark N. Stein, Lakeesha Carmichael, Jens Eickhoff, Susan A. Johnston, Kimberly A. Binger, Jennifer L. Heideman, Scott B. Perlman, …

Cancer chemotherapy and pharmacology, Vol.73(3), pp.485-493

03/01/2014

DOI: 10.1007/s00280-013-2373-9

PMCID: PMC4200479

PMID: 24414551

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https://www.ncbi.nlm.nih.gov/pmc/articles/4200479View

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Abstract

Sunitinib treatment results in a compensatory increase in plasma VEGF levels. Acute withdrawal of sunitinib results in a proliferative withdrawal flare, primarily due to elevated VEGF levels. Concurrent sunitinib plus bevacizumab is poorly tolerated with high (37 %) incidence of microangiopathic hemolytic anemia (MAHA). We evaluated a sequential design administering bevacizumab during the sunitinib treatment break to suppress the sunitinib withdrawal flare. Patients with no prior VEGF treatment were enrolled in this study. All patients had target lesions amenable to serial FLT PET/CT imaging. Sunitinib 37.5 mg was given on days 1-28 every 6 weeks with bevacizumab 5 mg/kg on day 29. If safe and tolerable, sunitinib increased to 50 mg. FLT PET/CT scans would be obtained at baseline (D1), week 4, and week 6 to evaluate pharmacodynamics of the sequential combination. Sunitinib pharmacokinetics and total, free, and bound VEGF levels were obtained on each cycle at D1, pre-bevacizumab (D29), 4 h post-bevacizumab (D29H4), and day 42 (D42). Six patients enrolled in the safety cohort of sunitinib 37.5 mg plus bevacizumab (see Table). One patient experienced grade 1 MAHA, and after discussion with the Cancer Therapy Evaluation Program (CTEP), the trial was closed to further accrual. No imaging scans were obtained due to early closure. [GRAPHICS] Subclinical MAHA was seen despite using sequential sunitinib with low-dose bevacizumab, and this combination was not feasible for further development. As predicted, VEGF levels increased during sunitinib exposure followed by a rapid decline after bevacizumab. Due to the long half-life of bevacizumab, we expected VEGF ligand suppression through D42, but instead observed a complete rebound in total/free VEGF levels by D42. The increase in VEGF at D42 was unexpected based on sunitinib alone and contrary to the hypothesis that we would block VEGF flare with low-dose bevacizumab. VEGF ligand production may increase as a result of bevacizumab, implying a robust host compensatory mechanism to VEGF signaling pathway inhibition. A greater understanding of the compensatory mechanism would aid future sequencing strategies of new agents.

Life Sciences & Biomedicine

Oncology

Pharmacology & Pharmacy

Science & Technology

Details

Title: Subtitle: A phase I pharmacodynamic trial of sequential sunitinib with bevacizumab in patients with renal cell carcinoma and other advanced solid malignancies
Creators: Justine Yang Bruce - University of Wisconsin–Madison
Jill M. Kolesar - University of Wisconsin–Madison
Hans Hammers - Sidney Kimmel Comprehensive Cancer Center
Mark N. Stein - Cancer Institute of Florida
Lakeesha Carmichael - University of Wisconsin–Madison
Jens Eickhoff - University of Wisconsin–Madison
Susan A. Johnston - University of Wisconsin–Madison
Kimberly A. Binger - University of Wisconsin–Madison
Jennifer L. Heideman - University of Wisconsin–Madison
Scott B. Perlman - University of Wisconsin–Madison
Robert Jeraj - University of Wisconsin–Madison
Glenn Liu - University of Wisconsin–Madison
Resource Type: Journal article
Publication Details: Cancer chemotherapy and pharmacology, Vol.73(3), pp.485-493
DOI: 10.1007/s00280-013-2373-9
PMID: 24414551
PMCID: PMC4200479
NLM abbreviation: Cancer Chemother Pharmacol
ISSN: 0344-5704
eISSN: 1432-0843
Publisher: Springer Nature
Number of pages: 9
Grant note: GA4061YX / Pfizer P30CA014520 / NATIONAL CANCER INSTITUTE; United States Department of Health & Human Services; National Institutes of Health (NIH) - USA; NIH National Cancer Institute (NCI) UL1TR000427 / NATIONAL CENTER FOR ADVANCING TRANSLATIONAL SCIENCES; United States Department of Health & Human Services; National Institutes of Health (NIH) - USA; NIH National Center for Advancing Translational Sciences (NCATS) P30 CA014520 / NIH/NCI-UW Comprehensive Cancer Center; United States Department of Health & Human Services; National Institutes of Health (NIH) - USA; NIH National Cancer Institute (NCI) U01 CA062491 / NIH/NCI; United States Department of Health & Human Services; National Institutes of Health (NIH) - USA; NIH National Cancer Institute (NCI)
Language: English
Date published: 03/01/2014
Academic Unit: Pharmacy; Pharmaceutical Sciences and Experimental Therapeutics
Record Identifier: 9984695784802771

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