Cypate and Cypate-Glucosamine as Near-Infrared Fluorescent Probes for In Vivo Tumor Imaging.
Mona DoshiDaniel A NierenbergOrielyz Flores-FernandezPragney DemeEdilu BecerraAnnette R KhaledSampath ParthasarathyPublished in: Molecular pharmacology (2019)
Near-infrared (NIR) imaging is a promising technique for use as a noninvasive and sensitive diagnostic tool. Although the NIR fluorescently labeled glucose analog glucosamine (cypate-glucosamine) has applications in preclinical imaging, the transport pathways and fate of this probe in tissues remain unaddressed. Here, we have synthesized and characterized cypate and cypate-glucosamine conjugate (cy-2-glu), and investigated the probable transport pathways of these probes in vitro and in vivo. We compared uptake of the probes in the presence and absence of excess d-glucose, "saturated cypate" and palmitic acid in two normal-cancer cell line pairs: lung cancer (A549)-normal (MRC9) and prostate cancer (DU145)-normal (BPH). Breast cancer (MDA-MB-231) and liver cancer (HepG2) cell lines were also examined. Results support use of the glucose transport pathway by cy-2-glu and fatty acid transport pathway by cypate. Mass spectrometry data on the in vitro extracts revealed deamidation of cy-2-glu in prostate and liver cells, suggesting release of glucosamine. In vivo biodistribution studies in mice engrafted with breast tumors showed a distinct accumulation of cy-2-glu in liver and tumors, and to a lesser extent in kidneys and spleen. A negligible accumulation of cypate alone in tumors was observed. Analysis of urine extracts revealed renal excretion of the cy-2-glu probe in the form of free cypate, indicating deamidation of cy-2-glu in tissues. Thus, investigation of the metabolic pathways used by NIR probes such as cy-2-glu advances their use in the detection and monitoring of tumor progression in preclinical animal studies.
Keyphrases
- living cells
- fluorescence imaging
- fluorescent probe
- prostate cancer
- high resolution
- small molecule
- photodynamic therapy
- mass spectrometry
- single molecule
- gene expression
- fatty acid
- quantum dots
- induced apoptosis
- drug release
- computed tomography
- stem cells
- poor prognosis
- radical prostatectomy
- liquid chromatography
- drug delivery
- young adults
- electronic health record
- pet imaging
- big data
- cell death
- case control
- benign prostatic hyperplasia
- papillary thyroid
- cell therapy
- simultaneous determination
- endoplasmic reticulum stress
- tandem mass spectrometry
- childhood cancer