Abstract
Simple SummaryVascular-disrupting agents promise significant therapeutic efficacy against solid tumors by selectively damaging tumor-associated vasculature. Dynamic BLI and oxygen-enhanced multispectral optoacoustic tomography (OE-MSOT) were used to compare vascular shutdown following administration of KGP265. BLI signal and vascular oxygenation response (ΔsO2) to a gas breathing challenge were both significantly reduced within 2 h indicating vascular disruption, which continued over 24 h. Twice-weekly doses of KGP265 caused a significant growth delay in MDA-MB-231 human breast tumor xenografts and 4T1 syngeneic breast tumors growing orthotopically in mice.The selective disruption of tumor-associated vasculature represents an attractive therapeutic approach. We have undertaken the first in vivo evaluation of KGP265, a water-soluble prodrug of a benzosuberene-based tubulin-binding agent, and found promising vascular-disrupting activity in three distinct tumor types. Dose escalation in orthotopic MDA-MB-231-luc breast tumor xenografts in mice indicated that higher doses produced more effective vascular shutdown, as revealed by dynamic bioluminescence imaging (BLI). In syngeneic orthotopic 4T1-luc breast and RENCA-luc kidney tumors, dynamic BLI and oxygen enhanced multispectral optoacoustic tomography (OE-MSOT) were used to compare vascular shutdown following the administration of KGP265 (7.5 mg/kg). The BLI signal and vascular oxygenation response (ΔsO2) to a gas breathing challenge were both significantly reduced within 2 h, indicating vascular disruption, which continued over 24 h. A correlative histology confirmed increased necrosis and hemorrhage. Twice-weekly doses of KGP265 caused significant growth delay in both MDA-MB-231 and 4T1 breast tumors, with no obvious systemic toxicity. A combination with carboplatin produced significantly greater tumor growth delay than carboplatin alone, though significant carboplatin-associated toxicity was observed (whole-body weight loss). KGP265 was found to be effective at low concentrations, generating long-term vascular shutdown and tumor growth delay, thus providing strong rationale for further development, particularly in combination therapies.
Highlights
Solid tumor growth beyond about 1–3 mm in diameter depends extensively on angiogenesis initiating neovascularization for the supply of nutrients and oxygen [1]
Noting that BLI depends on the delivery of the substrate luciferin to the tumor, we have previously demonstrated the utility of dynamic bioluminescence imaging (BLI) to evaluate several vascular-disrupting agents (VDAs), including CA4P and analogs [5,40,42,43,44], and this approach has been used by others [45]
We have shown that the KGP265 prodrug (100 μM) was readily dephosphorylated (100%) in 24 h by alkaline phosphatase (1 unit) at pH 8.6 at a rate of 7.3 μM/min/unit enzyme activity to generate active KGP18, which functions as both a VDA and an antimitotic agent
Summary
Solid tumor growth beyond about 1–3 mm in diameter depends extensively on angiogenesis initiating neovascularization for the supply of nutrients and oxygen [1]. Tumor neovasculature is abnormal, in terms of both structure and function, and has been proposed as a specific target for chemotherapy [2,3,4,5]. Tumor endothelial cells undergo rapid proliferation, and blood vessels are ill-formed, leaky and generally lack pericyte coverage [6,7]. Two types of therapy have been proposed to target tumor-associated vasculature: antiangiogenic agents inhibit the development of blood vessels a priori [8], while vascular-disrupting agents (VDAs) target the existing neovasculature [4,5,9,10,11]. Colchicine and vinblastine cause microtubule destabilization, leading to vascular disruption, but at concentrations that are close to their maximum tolerated dose, mandating a need for modified agents [13,14]
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