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Open Access 01-12-2015 | Research

Pyruvate sensitizes pancreatic tumors to hypoxia-activated prodrug TH-302

Authors: Jonathan W Wojtkowiak, Heather C Cornnell, Shingo Matsumoto, Keita Saito, Yoichi Takakusagi, Prasanta Dutta, Munju Kim, Xiaomeng Zhang, Rafael Leos, Kate M Bailey, Gary Martinez, Mark C Lloyd, Craig Weber, James B Mitchell, Ronald M Lynch, Amanda F Baker, Robert A Gatenby, Katarzyna A Rejniak, Charles Hart, Murali C Krishna, Robert J Gillies

Published in: Cancer & Metabolism | Issue 1/2015

Abstract

Background

Hypoxic niches in solid tumors harbor therapy-resistant cells. Hypoxia-activated prodrugs (HAPs) have been designed to overcome this resistance and, to date, have begun to show clinical efficacy. However, clinical HAPs activity could be improved. In this study, we sought to identify non-pharmacological methods to acutely exacerbate tumor hypoxia to increase TH-302 activity in pancreatic ductal adenocarcinoma (PDAC) tumor models.

Results

Three human PDAC cell lines with varying sensitivity to TH-302 (Hs766t > MiaPaCa-2 > SU.86.86) were used to establish PDAC xenograft models. PDAC cells were metabolically profiled in vitro and in vivo using the Seahorse XF system and hyperpolarized ¹³C pyruvate MRI, respectively, in addition to quantitative immunohistochemistry. The effect of exogenous pyruvate on tumor oxygenation was determined using electroparamagnetic resonance (EPR) oxygen imaging. Hs766t and MiaPaCa-2 cells exhibited a glycolytic phenotype in comparison to TH-302 resistant line SU.86.86. Supporting this observation is a higher lactate/pyruvate ratio in Hs766t and MiaPaCa xenografts as observed during hyperpolarized pyruvate MRI studies in vivo. Coincidentally, response to exogenous pyruvate both in vitro (Seahorse oxygen consumption) and in vivo (EPR oxygen imaging) was greatest in Hs766t and MiaPaCa models, possibly due to a higher mitochondrial reserve capacity. Changes in oxygen consumption and in vivo hypoxic status to pyruvate were limited in the SU.86.86 model. Combination therapy of pyruvate plus TH-302 in vivo significantly decreased tumor growth and increased survival in the MiaPaCa model and improved survival in Hs766t tumors.

Conclusions

Using metabolic profiling, functional imaging, and computational modeling, we show improved TH-302 activity by transiently increasing tumor hypoxia metabolically with exogenous pyruvate. Additionally, this work identified a set of biomarkers that may be used clinically to predict which tumors will be most responsive to pyruvate + TH-302 combination therapy. The results of this study support the concept that acute increases in tumor hypoxia can be beneficial for improving the clinical efficacy of HAPs and can positively impact the future treatment of PDAC and other cancers.

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Title: Pyruvate sensitizes pancreatic tumors to hypoxia-activated prodrug TH-302
Authors: Jonathan W Wojtkowiak
Heather C Cornnell
Shingo Matsumoto
Keita Saito
Yoichi Takakusagi
Prasanta Dutta
Munju Kim
Xiaomeng Zhang
Rafael Leos
Kate M Bailey
Gary Martinez
Mark C Lloyd
Craig Weber
James B Mitchell
Ronald M Lynch
Amanda F Baker
Robert A Gatenby
Katarzyna A Rejniak
Charles Hart
Murali C Krishna
Robert J Gillies
Publication date: 01-12-2015
Publisher: BioMed Central
Published in: Cancer & Metabolism / Issue 1/2015
Electronic ISSN: 2049-3002
DOI: https://doi.org/10.1186/s40170-014-0026-z

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