RT Journal Article SR Electronic T1 An Approach to Breast Cancer Diagnosis via PET Imaging of Microcalcifications Using 18F-NaF JF Journal of Nuclear Medicine JO J Nucl Med FD Society of Nuclear Medicine SP 1138 OP 1143 DO 10.2967/jnumed.114.139170 VO 55 IS 7 A1 George H. Wilson III A1 John C. Gore A1 Thomas E. Yankeelov A1 Stephanie Barnes A1 Todd E. Peterson A1 Jarrod M. True A1 Sepideh Shokouhi A1 J. Oliver McIntyre A1 Melinda Sanders A1 Vandana Abramson A1 The-Quyen Ngyuen A1 Anita Mahadevan-Jansen A1 Mohammed N. Tantawy YR 2014 UL http://jnm.snmjournals.org/content/55/7/1138.abstract AB Current radiologic methods for diagnosing breast cancer detect specific morphologic features of solid tumors or any associated calcium deposits. These deposits originate from an early molecular microcalcification process of 2 types: type 1 is calcium oxylate and type II is carbonated calcium hydroxyapatite. Type I microcalcifications are associated mainly with benign tumors, whereas type II microcalcifications are produced internally by malignant cells. No current noninvasive in vivo techniques are available for detecting intratumoral microcalcifications. Such a technique would have a significant impact on breast cancer diagnosis and prognosis in preclinical and clinical settings. 18F-NaF PET has been used solely for bone imaging by targeting the bone hydroxyapatite. In this work, we provide preliminary evidence that 18F-NaF PET imaging can be used to detect breast cancer by targeting the hydroxyapatite lattice within the tumor microenvironment with high specificity and soft-tissue contrast-to-background ratio while delineating tumors from inflammation. Methods: Mice were injected with approximately 106 MDA-MB-231 cells subcutaneously and imaged with 18F-NaF PET/CT in a 120-min dynamic sequence when the tumors reached a size of 200–400 mm3. Regions of interest were drawn around the tumor, muscle, and bone. The concentrations of radiotracer within those regions of interest were compared with one another. For comparison to inflammation, rats with inflamed paws were subjected to 18F-NaF PET imaging. Results: Tumor uptake of 18F− was significantly higher (P < 0.05) than muscle uptake, with the tumor-to-muscle ratio being about 3.5. The presence of type II microcalcification in the MDA-MB-231 cell line was confirmed histologically using alizarin red S and von Kossa staining as well as Raman microspectroscopy. No uptake of 18F− was observed in the inflamed tissue of the rats. Lack of hydroxyapatite in the inflamed tissue was verified histologically. Conclusion: This study provides preliminary evidence suggesting that specific targeting with 18F− of hydroxyapatite within the tumor microenvironment may be able to distinguish between inflammation and cancer.