Abstract
Raman spectroscopic imaging has shown great promise for improved cancer detection and localization with the use of tumor targeting surface enhanced Raman scattering (SERS) nanoparticles. With the ultrasensitive detection and multiplexing capabilities that SERS imaging has to offer, scientists have been investigating several clinical applications that could benefit from this unique imaging strategy. Recently, there has been a push to develop new image-guidance tools for surgical resection to help surgeons sensitively and specifically identify tumor margins in real time. We hypothesized that SERS nanoparticles (NPs) topically applied to breast cancer resection margins have the potential to provide real-time feedback on the presence of residual cancer in the resection margins during lumpectomy. Here, we explore the ability of SERS nanoparticles conjugated with a cluster of differentiation-47 (CD47) antibody to target breast cancer. CD47 is a cell surface receptor that has recently been shown to be overexpressed on several solid tumor types. The binding potential of our CD47-labeled SERS nanoparticles was assessed using fluorescence assisted cell sorting (FACS) on seven different human breast cancer cell lines, some of which were triple negative (negative expression of estrogen receptor (ER), progesterone receptor (PR), and human epidermal growth factor receptor-2 (HER2)). Xenograft mouse models were also used to assess the ability of our Raman imaging system to identify tumor from normal tissue. A ratiometric imaging strategy was used to quantify specific vs. nonspecific probe binding, resulting in improved tumor-to-background ratios. FACS analysis showed that CD47-labeled SERS nanoparticles bound to seven different breast cancer cell lines at levels 12-fold to 70-fold higher than isotype control-labeled nanoparticles (p < 0.01), suggesting that our CD47-targeted nanoparticles actively bind to CD47 on breast cancer cells. In a mouse xenograft model of human breast cancer, topical application of CD47-targeted nanoparticles to excised normal and cancer tissue revealed increased binding of CD47-targeted nanoparticles on tumor relative to normal adjacent tissue. The findings of this study support further investigation and suggest that SERS nanoparticles topically applied to breast cancer could guide more complete surgical resection during lumpectomy.
Highlights
Raman imaging of surface enhanced Raman scattering (SERS) nanoparticles (NPs) is an optical technique that offers unsurpassed sensitivity and multiplexing capabilities to the field of molecular imaging [1,2]
We evaluated seven different breast cancer cell lines with varying expression levels of estrogen, progesterone, and HER2 (Table 1)
DLD1 is known to overexpress cluster of differentiation-47 (CD47), so we used this cell line to serve as our positive control and our negative control was derived from the same DLD1 cell line that underwent a TALEN-mediated knockout of CD47
Summary
Raman imaging of surface enhanced Raman scattering (SERS) nanoparticles (NPs) is an optical technique that offers unsurpassed sensitivity (on the order of fM) and multiplexing capabilities to the field of molecular imaging [1,2]. Incorporating these unique characteristics into a new diagnostic tool that surgeons can use in the operating room (OR) has the potential to significantly impact their ability to successfully identify and remove the entire tumor while minimizing damage to healthy neighboring tissue and decreasing the chances of recurrence and the need for repeat surgery. In addition to the negative oncologic consequences, positive tumor margins may necessitate reoperation, thereby increasing associated patient morbidity and healthcare expenditure (e.g., imaging, anesthesia, pathology) [4,5,6]
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