Literature DB >> 17047054

Probing the intracellular redox status of tumors with magnetic resonance imaging and redox-sensitive contrast agents.

Fuminori Hyodo1, Ken-Ichiro Matsumoto, Atsuko Matsumoto, James B Mitchell, Murali C Krishna.   

Abstract

Nitroxide radicals are paramagnetic contrast agents, used in magnetic resonance imaging (MRI), that also exert antioxidant effects. Participating in cellular redox reactions, they lose their ability to provide contrast as a function of time after administration. In this study, the rate of contrast loss was correlated to the reducing power of the tissue or the "redox status." The preferential reduction of nitroxides in tumors compared with normal tissue was observed by MRI. The influence of the structure of the nitroxide on the reduction rate was investigated by MRI using two cell-permeable nitroxides, 4-hydroxy-2,2,6,6,-tetramethyl-1-piperidynyloxyl (Tempol) and 3-carbamoyl-2,2,5,5-tetramethylpyrrolidine-1-oxyl (3CP), and one cell-impermeable nitroxide, 3-carboxy-2,2,5,5,5-tetramethylpyrrolidine-1-oxyl (3CxP). Pharmacokinetic images of these nitroxides in normal tissue, tumor, kidney, and artery regions in mice were simultaneously obtained using MRI. The decay of Tempol and 3CP in tumor tissue was significantly faster than in normal tissue. No significant change in the total nitroxide (oxidized + reduced forms) was noted from tissue extracts, suggesting that the loss in contrast as a function of time is a result of intracellular bioreduction. However, in the case of 3CxP (membrane impermeable), there was no difference in the reduction rates between normal and tumor tissue. The time course of T(1) enhancement by 3CxP and the total amount of 3CxP (oxidized + reduced) in the femoral region showed similar pharmacokinetics. These results show that the differential bioreduction of cell-permeable nitroxides in tumor and normal tissue is supported by intracellular processes and the reduction rates are a means by which the intracellular redox status can be assessed noninvasively.

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Year:  2006        PMID: 17047054     DOI: 10.1158/0008-5472.CAN-06-0879

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  53 in total

1.  Brain redox imaging.

Authors:  Ken-ichiro Matsumoto; Fuminori Hyodo; Kazunori Anzai; Hideo Utsumi; James B Mitchell; Murali C Krishna
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2.  Effects of oxygen challenging to tissue redox and pO2 status.

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4.  Synthesis and reduction kinetics of sterically shielded pyrrolidine nitroxides.

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Journal:  Org Lett       Date:  2012-10-10       Impact factor: 6.005

5.  Redox-responsive branched-bottlebrush polymers for in vivo MRI and fluorescence imaging.

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Review 7.  Chemistry of MRI Contrast Agents: Current Challenges and New Frontiers.

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8.  Accelerated dynamic EPR imaging using fast acquisition and compressive recovery.

Authors:  Rizwan Ahmad; Alexandre Samouilov; Jay L Zweier
Journal:  J Magn Reson       Date:  2016-10-08       Impact factor: 2.229

9.  Brain redox imaging using blood-brain barrier-permeable nitroxide MRI contrast agent.

Authors:  Fuminori Hyodo; Kai-Hsiang Chuang; Artem G Goloshevsky; Agnieszka Sulima; Gary L Griffiths; James B Mitchell; Alan P Koretsky; Murali C Krishna
Journal:  J Cereb Blood Flow Metab       Date:  2008-02-13       Impact factor: 6.200

10.  Tumor Xenograft Response to Redox-Active Therapies Assessed by Magnetic Resonance Imaging Using a Thiol-Bearing DOTA Complex of Gadolinium.

Authors:  Gerald P Guntle; Bhumasamudram Jagadish; Eugene A Mash; Garth Powis; Robert T Dorr; Natarajan Raghunand
Journal:  Transl Oncol       Date:  2012-06-01       Impact factor: 4.243

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