Your search keyword '"In vivo fluorescence"' showing total 2 results

1. The pH low insertion peptide pHLIP Variant 3 as a novel marker of acidic malignant lesions.

Author

Tapmeier, Thomas T., Moshnikova, Anna, Beech, John, Allen, Danny, Kinchesh, Paul, Smart, Sean, Harris, Adrian, McIntyre, Alan, Engelman, Donald M., Andreev, Oleg A., Reshetnyak, Yana K., and Muschel, Ruth J.

Subjects

*HYDROGEN-ion concentration, *ACIDITY, *HOMOGRAFTS, *CARBONIC anhydrase, *ACETAZOLAMIDE, TUMOR surgery, ANIMAL models of tumors

Abstract

Current strategies for early detection of breast and other cancers are limited in part because some lesions identified as potentially malignant do not develop into aggressive tumors. Acid pH has been suggested as a key characteristic of aggressive tumors that might distinguish aggressive lesions from more indolent pathology. We therefore investigated the novel class of molecules, pH low insertion peptides (pHLIPs), as markers of low pH in tumor allografts and of malignant lesions in a mouse model of spontaneous breast cancer, BALB/neu-T. pHLIP Variant 3 (Var3) conjugated with fluorescent Alexa546 was shown to insert into tumor spheroids in a sequence-specific manner. Its signal reflected pH in murine tumors. It was induced by carbonic anhydrase IX (CAIX) overexpression and inhibited by acetazolamide (AZA) administration. By using 31P magnetic resonance spectroscopy (MRS), we demonstrated that pHLIP Var3 was retained in tumors of pH equal to or less than 6.7 but not in tissues of higher pH. In BALB/neu-T mice at different stages of the disease, the fluorescent signal from pHLIP Var3 marked cancerous lesions with a very low false-positive rate. However, only ~60% of the smallest lesions retained a pHLIP Var3 signal, suggesting heterogeneity in pH. Taken together, these results show that pHLIP can identify regions of lower pH, allowing for its development as a theranostic tool for clinical applications. [ABSTRACT FROM AUTHOR]

Published

2015

2. Differential structured illumination microendoscopy for in vivo imaging of molecular contrast agents

Author

Preetha Ramalingam, Rebecca Richards-Kortum, Kathleen M. Schmeler, and Pelham Keahey

Subjects

Optical fiber, Materials science, genetic structures, Optical sectioning, Colon, media_common.quotation_subject, Contrast Media, 01 natural sciences, Epithelium, law.invention, 010309 optics, 03 medical and health sciences, 0302 clinical medicine, Optics, Imaging, Three-Dimensional, law, In vivo, 0103 physical sciences, In vivo fluorescence, Contrast (vision), Animals, A fibers, media_common, Multidisciplinary, business.industry, Endoscopy, Biological Sciences, Structured illumination, eye diseases, Microspheres, Mice, Inbred C57BL, 030220 oncology & carcinogenesis, Female, business, Preclinical imaging

Abstract

Fiber optic microendoscopy has shown promise for visualization of molecular contrast agents used to study disease in vivo. However, fiber optic microendoscopes have limited optical sectioning capability, and image contrast is limited by out-of-focus light generated in highly scattering tissue. Optical sectioning techniques have been used in microendoscopes to remove out-of-focus light but reduce imaging speed or rely on bulky optical elements that prevent in vivo imaging. Here, we present differential structured illumination microendoscopy (DSIMe), a fiber optic system that can perform structured illumination in real time for optical sectioning without any opto-mechanical components attached to the distal tip of the fiber bundle. We demonstrate the use of DSIMe during in vivo fluorescence imaging in patients undergoing surgery for cervical adenocarcinoma in situ. Images acquired using DSIMe show greater contrast than standard microendoscopy, improving the ability to detect cellular atypia associated with neoplasia.

Published

2016