Atm deletion with dual recombinase technology preferentially radiosensitizes tumor endothelium
Everett J. Moding, … , Shiva Das, David G. Kirsch
Everett J. Moding, … , Shiva Das, David G. Kirsch
Published July 18, 2014
Citation Information: J Clin Invest. 2014;124(8):3325-3338. https://doi.org/10.1172/JCI73932.
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Research Article

Atm deletion with dual recombinase technology preferentially radiosensitizes tumor endothelium

Abstract

Cells isolated from patients with ataxia telangiectasia are exquisitely sensitive to ionizing radiation. Kinase inhibitors of ATM, the gene mutated in ataxia telangiectasia, can sensitize tumor cells to radiation therapy, but concern that inhibiting ATM in normal tissues will also increase normal tissue toxicity from radiation has limited their clinical application. Endothelial cell damage can contribute to the development of long-term side effects after radiation therapy, but the role of endothelial cell death in tumor response to radiation therapy remains controversial. Here, we developed dual recombinase technology using both FlpO and Cre recombinases to generate primary sarcomas in mice with endothelial cell–specific deletion of Atm to determine whether loss of Atm in endothelial cells sensitizes tumors and normal tissues to radiation. Although deletion of Atm in proliferating tumor endothelial cells enhanced the response of sarcomas to radiation, Atm deletion in quiescent endothelial cells of the heart did not sensitize mice to radiation-induced myocardial necrosis. Blocking cell cycle progression reversed the effect of Atm loss on tumor endothelial cell radiosensitivity. These results indicate that endothelial cells must progress through the cell cycle in order to be radiosensitized by Atm deletion.

Authors

Everett J. Moding, Chang-Lung Lee, Katherine D. Castle, Patrick Oh, Lan Mao, Shan Zha, Hooney D. Min, Yan Ma, Shiva Das, David G. Kirsch

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Figure 5

Characterization of cardiac and respiratory function in VAtmfl/+ and VAtmfl/fl mice with and without whole-heart irradiation.

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Characterization of cardiac and respiratory function in VAtmfl/+ and VAt...
(A) Representative echocardiography recordings from VAtmfl/+ and VAtmfl/fl mice 6 weeks or 1 year after 12 Gy whole-heart irradiation and in unirradiated controls. (BD) Changes in fractional shortening (B), left ventricular mass (C), and left ventricular end-systolic dimension (LVDs) (D) in VAtmfl/+ and VAtmfl/fl mice 6 weeks and 1 year after 12 Gy whole-heart irradiation and in unirradiated controls (n = 6 mice per group). (E) Respiratory rate in VAtmfl/+ and VAtmfl/fl mice 1 year after 12 Gy whole-heart irradiation and in unirradiated controls (n = 5 per group). All data are mean ± SEM.