| Literature DB >> 26924502 |
Frederick O Cope1, Bonnie Abbruzzese2, James Sanders2, Wendy Metz2, Kristyn Sturms2, David Ralph2, Michael Blue2, Jane Zhang3, Paige Bracci3, Wiam Bshara4, Spencer Behr4, Toby Maurer4, Kenneth Williams5, Joshua Walker5, Allison Beverly6, Brooke Blay6, Anirudh Damughatla6, Mark Larsen6, Courtney Mountain6, Erin Neylon6, Kaeli Parcel6, Kapil Raghuraman6, Kevin Ricks6, Lucas Rose6, Akhilesh Sivakumar6, Nicholas Streck6, Bryan Wang6, Christopher Wasco6, Larry S Schlesinger, Abul Azad, Murugesan V S Rajaram, Wael Jarjour, Nicholas Young, Thomas Rosol, Amifred Williams6, Michael McGrath3.
Abstract
In considering the challenges of approaches to clinical imaging, we are faced with choices that sometimes are impacted by rather dogmatic notions about what is a better or worse technology to achieve the most useful diagnostic image for the patient. For example, is PET or SPECT most useful in imaging any particular disease dissemination? The dictatorial approach would be to choose PET, all other matters being equal. But is such a totalitarian attitude toward imaging selection still valid? In the face of new receptor targeted SPECT agents one must consider the remarkable specificity and sensitivity of these agents. (99m)Tc-Tilmanocept is one of the newest of these agents, now approved for guiding sentinel node biopsy (SLNB) in several solid tumors. Tilmanocept has a Kd of 3×10(-11)M, and it specificity for the CD206 receptor is unlike any other agent to date. This coupled with a number of facts, that specific disease-associated macrophages express this receptor (100 to 150 thousand receptors), that the receptor has multiple binding sites for tilmanocept (>2 sites per receptor) and that these receptors are recycled every 15 min to bind more tilmanocept (acting as intracellular "drug compilers" of tilmanocept into non-degraded vesicles), gives serious pause as to how we select our approaches to diagnostic imaging. Clinically, the size of SLNs varies greatly, some, anatomically, below the machine resolution of SPECT. Yet, with tilmanocept targeting, the SLNs are highly visible with macrophages stably accruing adequate (99m)Tc-tilmanocept counting statistics, as high target-to-background ratios can compensate for spatial resolution blurring. Importantly, it may be targeted imaging agents per se, again such as tilmanocept, which may significantly shrink any perceived chasm between the imaging technologies and anchor the diagnostic considerations in the targeting and specificity of the agent rather than any lingering dogma about the hardware as the basis for imaging approaches. Beyond the elements of imaging applications of these agents is their evolution to therapeutic agents as well, and even in the neo-logical realm of theranostics. Characteristics of agents such as tilmanocept that exploit the natural history of diseases with remarkably high specificity are the expectations for the future of patient- and disease-centered diagnosis and therapy.Entities:
Keywords: CD206; Imaging; Immunodiagnostic; Immunotherapy; Macrophage; Tilmanocept
Mesh:
Year: 2015 PMID: 26924502 PMCID: PMC4794336 DOI: 10.1016/j.nucmedbio.2015.11.007
Source DB: PubMed Journal: Nucl Med Biol ISSN: 0969-8051 Impact factor: 2.408