Abstract
Molecular imaging consists of non-invasive monitoring of spatial-temporal distribution of molecular or cellular processes, and may be used for early disease detection and real-time monitoring of therapeutic responses. Several strategies have been developed over the last two decades. Early attempts used monoclonal antibodies or antibody fragments and, although specific _targeting was achieved, these probes was largely unsuccessful. In the quest for better agents, labeled peptides were then used. Peptides are easier to synthesize, less likely to be immunogenic, and have rapid blood clearance, which results in adequate _target-to-background ratios in a short period of time.
This review discusses state-of-the-art cancer imaging by means of labeled peptides, the radionuclide, optical and nanoplatform-based imaging techniques which can provide functional information of the disease and track biochemical processes in vivo. The advantages and disadvantages of each technique are discussed. Lastly, the emphasis of this paper is on the new multimodal probes which can overcome individual limitations and exploit the individual strengths of the latest molecular imaging techniques.
Keywords: Cancer Imaging, In Vivo Molecular Imaging, Liposomes, MRI Imaging, Multimodal Probes, Multimodal _targeting, Nanoparticles, Nanotubes, Optical imaging, Photoacoustic imaging, Peptide Hormones, Peptide PET Imaging, Quantum Dots, Radionuclide Imaging, Raman Imaging, Tumor _targeting, SPECT Imaging
Anti-Cancer Agents in Medicinal Chemistry
Title:Optical and Multimodal Peptide-Based Probes for In Vivo Molecular Imaging
Volume: 12 Issue: 5
Author(s): Laura Melendez-Alafort, Pier Carlo Muzzio and Antonio Rosato
Affiliation:
Keywords: Cancer Imaging, In Vivo Molecular Imaging, Liposomes, MRI Imaging, Multimodal Probes, Multimodal _targeting, Nanoparticles, Nanotubes, Optical imaging, Photoacoustic imaging, Peptide Hormones, Peptide PET Imaging, Quantum Dots, Radionuclide Imaging, Raman Imaging, Tumor _targeting, SPECT Imaging
Abstract: Molecular imaging consists of non-invasive monitoring of spatial-temporal distribution of molecular or cellular processes, and may be used for early disease detection and real-time monitoring of therapeutic responses. Several strategies have been developed over the last two decades. Early attempts used monoclonal antibodies or antibody fragments and, although specific _targeting was achieved, these probes was largely unsuccessful. In the quest for better agents, labeled peptides were then used. Peptides are easier to synthesize, less likely to be immunogenic, and have rapid blood clearance, which results in adequate _target-to-background ratios in a short period of time.
This review discusses state-of-the-art cancer imaging by means of labeled peptides, the radionuclide, optical and nanoplatform-based imaging techniques which can provide functional information of the disease and track biochemical processes in vivo. The advantages and disadvantages of each technique are discussed. Lastly, the emphasis of this paper is on the new multimodal probes which can overcome individual limitations and exploit the individual strengths of the latest molecular imaging techniques.
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Cite this article as:
Melendez-Alafort Laura, Carlo Muzzio Pier and Rosato Antonio, Optical and Multimodal Peptide-Based Probes for In Vivo Molecular Imaging, Anti-Cancer Agents in Medicinal Chemistry 2012; 12 (5) . https://dx.doi.org/10.2174/187152012800617858
DOI https://dx.doi.org/10.2174/187152012800617858 |
Print ISSN 1871-5206 |
Publisher Name Bentham Science Publisher |
Online ISSN 1875-5992 |
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