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HIF-1–Dependent Stromal Adaptation to Ischemia Mediates In Vivo Tumor Radiation Resistance

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TLDR
The results illustrate that tumor radioresistance is mediated by a capacity to compensate for stromal vascular disruption through HIF-1–dependent proangiogenic signaling and that clinically relevant vascular imaging techniques can spatially define mechanisms associated with tumor irradiation.
Abstract
Purpose: Hypoxia-inducible factor 1 (HIF-1) promotes cancer cell survival and tumor progression. The specific role played by HIF-1 and tumor–stromal interactions toward determining tumor resistance to radiation treatment remains undefined. We applied a multimodality preclinical imaging platform to mechanistically characterize tumor response to radiation, with a focus on HIF-1–dependent resistance pathways. Methods: C6 glioma and HN5 human squamous carcinoma cells were stably transfected with a dual HIF-1 signaling reporter construct (dxHRE-tk/eGFP-cmvRed2XPRT). Reporter cells were serially interrogated in vitro before and after irradiation as monolayer and multicellular spheroid cultures and as subcutaneous xenografts in nu/nu mice. Results: In vitro , single-dose irradiation of C6 and HN5 reporter cells modestly impacted HIF-1 signaling in normoxic monolayers and inhibited HIF-1 signaling in maturing spheroids. In contrast, irradiation of C6 or HN5 reporter xenografts with 8 Gy in vivo elicited marked upregulation of HIF-1 signaling and downstream proangiogenic signaling at 48 hours which preceded recovery of tumor growth. In situ ultrasound imaging and dynamic contrast-enhanced (DCE) MRI indicated that HIF-1 signaling followed acute disruption of stromal vascular function. High-resolution positron emission tomography and dual-contrast DCE-MRI of immobilized dorsal skin window tumors confirmed postradiotherapy HIF-1 signaling to spatiotemporally coincide with impaired stromal vascular function. Targeted disruption of HIF-1 signaling established this pathway to be a determinant of tumor radioresistance. Conclusions: Our results illustrate that tumor radioresistance is mediated by a capacity to compensate for stromal vascular disruption through HIF-1–dependent proangiogenic signaling and that clinically relevant vascular imaging techniques can spatially define mechanisms associated with tumor irradiation. Mol Cancer Res; 9(3); 259–70. ©2011 AACR .

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Radiobiology for the Radiologist

TL;DR: This text is a general introduction to radiation biology and a complete, self-contained course especially for residents in diagnostic radiology and nuclear medicine that follows the Syllabus in Radiation Biology of the RSNA.
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HIF Inhibitors: Status of Current Clinical Development

TL;DR: Clinical studies of the HIF inhibitors in patients with advanced/refractory cancers suggest benefit and warrant further studies ofThe Hif inhibitors either as a single agent or in combination with other therapeutic agents.
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The Role of Hypoxia Inducible Factor-1 in Hepatocellular Carcinoma

TL;DR: The mechanism by which Hif-1 is regulated and how HIF-1 mediates the biological effects of hypoxia in tissues are described, which could shed light on new therapeutic approaches for the treatment of HCC.
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Hypoxia-inducible factors as molecular targets for liver diseases

TL;DR: The evidence for HIF stabilization in liver disease is summarized, the mechanistic involvement of HIFs in disease development is discussed, and the potential of pharmacological HIF modifiers in the treatment of liver disease are explored.
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Understanding the role of cytokines in Glioblastoma Multiforme pathogenesis.

TL;DR: This review summarizes the current understanding of the functions of key cytokines on Glioblastoma Multiforme, and highlights potential therapeutic applications targeting these cytokines.
References
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Journal Article

Tumor oxygenation predicts for the likelihood of distant metastases in human soft tissue sarcoma.

TL;DR: The 18-month actuarial disease-free survival was 70% for patients with tumor median oxygen pressure (pO2) values of >10 mm Hg but only 35% for those with median pO2 values of <10mm Hg (P=0.01); potential mechanisms and implications for clinical trial design are discussed.
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Cellular adaptation to hypoxia: O2-sensing protein hydroxylases, hypoxia-inducible transcription factors, and O2-regulated gene expression

TL;DR: This review aims to summarize the current knowledge of oxygen‐regulated gene expression, which includes the finding that HIF‐1 regulates the expression of many more genes apart from erythropoietin, and the elucidation of the oxygen‐dependent mechanisms degrading the HIF a subunits.
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Radiation activates HIF-1 to regulate vascular radiosensitivity in tumors: role of reoxygenation, free radicals, and stress granules

TL;DR: Novel pathways contributing significantly to the understanding of HIF-1 regulation which may be major determinants of tumor radiosensitivity, potentially having high clinical relevance are described.
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Hypoxia-inducible factor-1alpha is a positive factor in solid tumor growth

TL;DR: The evidence from these experiments indicates that hypoxic response via Hif-1α is an important positive factor in solid tumor growth and that HIF-1 α affects tumor expansion in ways unrelated to its regulation of VEGF expression.
Journal ArticleDOI

Inhibition of vasculogenesis, but not angiogenesis, prevents the recurrence of glioblastoma after irradiation in mice

TL;DR: A novel approach is suggested for the treatment of GBM: in addition to radiotherapy, the vasculogenesis pathway needs to be blocked, and this can be accomplished using the clinically approved drug AMD3100, a small molecule inhibitor of SDF-1/CXCR4 interactions.
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