Literature DB >> 25355699

Clinical translation of an ultrasmall inorganic optical-PET imaging nanoparticle probe.

Evan Phillips1, Oula Penate-Medina1, Pat B Zanzonico2, Richard D Carvajal3, Pauliah Mohan1, Yunpeng Ye1, John Humm2, Mithat Gönen4, Hovanes Kalaigian2, Heiko Schöder1, H William Strauss1, Steven M Larson1, Ulrich Wiesner5, Michelle S Bradbury6.   

Abstract

A first-in-human clinical trial of ultrasmall inorganic hybrid nanoparticles, "C dots" (Cornell dots), in patients with metastatic melanoma is described for the imaging of cancer. These renally excreted silica particles were labeled with (124)I for positron emission tomography (PET) imaging and modified with cRGDY peptides for molecular targeting. (124)I-cRGDY-PEG-C dot particles are inherently fluorescent, containing the dye, Cy5, so they may be used as hybrid PET-optical imaging agents for lesion detection, cancer staging, and treatment management in humans. However, the clinical translation of nanoparticle probes, including quantum dots, has not kept pace with the accelerated growth in minimally invasive surgical tools that rely on optical imaging agents. The safety, pharmacokinetics, clearance properties, and radiation dosimetry of (124)I-cRGDY-PEG-C dots were assessed by serial PET and computerized tomography after intravenous administration in patients. Metabolic profiles and laboratory tests of blood and urine specimens, obtained before and after particle injection, were monitored over a 2-week interval. Findings are consistent with a well-tolerated inorganic particle tracer exhibiting in vivo stability and distinct, reproducible pharmacokinetic signatures defined by renal excretion. No toxic or adverse events attributable to the particles were observed. Coupled with preferential uptake and localization of the probe at sites of disease, these first-in-human results suggest safe use of these particles in human cancer diagnostics.
Copyright © 2014, American Association for the Advancement of Science.

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Year:  2014        PMID: 25355699      PMCID: PMC4426391          DOI: 10.1126/scitranslmed.3009524

Source DB:  PubMed          Journal:  Sci Transl Med        ISSN: 1946-6234            Impact factor:   17.956


  39 in total

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