Development
of Tumor-Targeted Near Infrared Probes
for Fluorescence Guided Surgery
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Abstract
Complete surgical resection of malignant
disease is the only reliable
method to cure cancer. Unfortunately, quantitative tumor resection
is often limited by a surgeon’s ability to locate all malignant
disease and distinguish it from healthy tissue. Fluorescence-guided
surgery has emerged as a tool to aid surgeons in the identification
and removal of malignant lesions. While nontargeted fluorescent dyes
have been shown to passively accumulate in some tumors, the resulting
tumor-to-background ratios are often poor, and the boundaries between
malignant and healthy tissues can be difficult to define. To circumvent
these problems, our laboratory has developed high affinity tumor targeting
ligands that bind to receptors that are overexpressed on cancer cells
and deliver attached molecules selectively into these cells. In this
study, we explore the use of two tumor-specific targeting ligands
(i.e., folic acid that targets the folate receptor (FR) and DUPA that
targets prostate specific membrane antigen (PSMA)) to deliver near-infrared
(NIR) fluorescent dyes specifically to FR and PSMA expressing cancers,
thereby rendering only the malignant cells highly fluorescent. We
report here that all FR- and PSMA-targeted NIR probes examined bind
cultured cancer cells in the low nanomolar range. Moreover, upon intravenous
injection into tumor-bearing mice with metastatic disease, these same
ligand–NIR dye conjugates render receptor-expressing tumor
tissues fluorescent, enabling their facile resection with minimal
contamination from healthy tissues