Cerenkov Luminescence Imaging (CLI) for cancer therapy monitoring.

In molecular imaging, positron emission tomography (PET) and optical imaging (OI) are two of the most important and thus most widely used modalities. PET is characterized by its excellent sensitivity and quantification ability while OI is notable for non-radiation, relative low cost, short scanning time, high throughput, and wide availability to basic researchers. However, both modalities have their shortcomings as well. PET suffers from poor spatial resolution and high cost, while OI is mostly limited to preclinical applications because of its limited tissue penetration along with prominent scattering optical signals through the thickness of living tissues. Recently a bridge between PET and OI has emerged with the discovery of Cerenkov Luminescence Imaging (CLI). CLI is a new imaging modality that harnesses Cerenkov Radiation (CR) to image radionuclides with OI instruments. Russian Nobel laureate Alekseyevich Cerenkov and his colleagues originally discovered CR in 1934. It is a form of electromagnetic radiation emitted when a charged particle travels at a superluminal speed in a dielectric medium. The charged particle, whether positron or electron, perturbs the electromagnetic field of the medium by displacing the electrons in its atoms. After passing of the disruption photons are emitted as the displaced electrons return to the ground state. For instance, one (18)F decay was estimated to produce an average of 3 photons in water. Since its emergence, CLI has been investigated for its use in a variety of preclinical applications including in vivo tumor imaging, reporter gene imaging, radiotracer development, multimodality imaging, among others. The most important reason why CLI has enjoyed much success so far is that this new technology takes advantage of the low cost and wide availability of OI to image radionuclides, which used to be imaged only by more expensive and less available nuclear imaging modalities such as PET. Here, we present the method of using CLI to monitor cancer drug therapy. Our group has recently investigated this new application and validated its feasibility by a proof-of-concept study. We demonstrated that CLI and PET exhibited excellent correlations across different tumor xenografts and imaging probes. This is consistent with the overarching principle of CR that CLI essentially visualizes the same radionuclides as PET. We selected Bevacizumab (Avastin; Genentech/Roche) as our therapeutic agent because it is a well-known angiogenesis inhibitor. Maturation of this technology in the near future can be envisioned to have a significant impact on preclinical drug development, screening, as well as therapy monitoring of patients receiving treatments.

[1]  Se-Il Park,et al.  Luminescence imaging using radionuclides: a potential application in molecular imaging. , 2011, Nuclear medicine and biology.

[2]  Erin Jackson,et al.  Cerenkov Radiation Energy Transfer (CRET) Imaging: A Novel Method for Optical Imaging of PET Isotopes in Biological Systems , 2010, PloS one.

[3]  H. Hochster Bevacizumab in combination with chemotherapy: first-line treatment of patients with metastatic colorectal cancer. , 2006, Seminars in oncology.

[4]  Zhen Cheng,et al.  Optical imaging of reporter gene expression using a positron-emission-tomography probe. , 2010, Journal of biomedical optics.

[5]  Lei Xing,et al.  Intraoperative Imaging of Tumors Using Cerenkov Luminescence Endoscopy: A Feasibility Experimental Study , 2012, The Journal of Nuclear Medicine.

[6]  Jan Grimm,et al.  Intraoperative Imaging of Positron Emission Tomographic Radiotracers Using Cerenkov Luminescence Emissions , 2011, Molecular imaging.

[7]  Zhen Cheng,et al.  Proof-of-Concept Study of Monitoring Cancer Drug Therapy with Cerenkov Luminescence Imaging , 2012, The Journal of Nuclear Medicine.

[8]  P. A. Čerenkov Visible radiation produced by electrons moving in a medium with velocities exceeding that of light , 1937 .

[9]  Xiaoyuan Chen,et al.  Positron emission tomography imaging of cancer biology: current status and future prospects. , 2011, Seminars in oncology.

[10]  Zhen Cheng,et al.  Harnessing the Power of Radionuclides for Optical Imaging: Cerenkov Luminescence Imaging , 2011, The Journal of Nuclear Medicine.

[11]  Sanjiv S. Gambhir,et al.  Molecular Optical Imaging with Radioactive Probes , 2010, PloS one.

[12]  Samuel Achilefu,et al.  Optical Imaging in Cancer Research: Basic Principles, Tumor Detection, and Therapeutic Monitoring , 2011, Medical Principles and Practice.

[13]  Riccardo Calandrino,et al.  In vivo 18F-FDG tumour uptake measurements in small animals using Cerenkov radiation , 2010, European Journal of Nuclear Medicine and Molecular Imaging.

[14]  Yeong Su Ha,et al.  Facile preparation of a hybrid nanoprobe for triple-modality optical/PET/MR imaging. , 2010, Small.

[15]  S R Cherry,et al.  Optical imaging of Cerenkov light generation from positron-emitting radiotracers , 2009, Physics in medicine and biology.

[16]  Jie Tian,et al.  Experimental Cerenkov luminescence tomography of the mouse model with SPECT imaging validation. , 2010, Optics express.