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| public:ccsip:optical_biopsy 2010/11/24 00:06 | public:ccsip:optical_biopsy 2010/11/24 11:10 current | ||
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| - | ====== Optical Biopsy Theme ====== | + | ====== Optical Biopsy (Tissue level) Theme ====== |
| ===== Description of the Technology ===== | ===== Description of the Technology ===== | ||
| Line 5: | Line 5: | ||
| ==== Basic modalities ==== | ==== Basic modalities ==== | ||
| - | Point Spectroscopy | + | * Point Spectroscopy |
| - | Reflectance & Fluorescence | + | * Reflectance & Fluorescence |
| - | Spatially Resolved | + | * Raman |
| - | Polarized | + | * IR |
| - | Time Domain | + | * Spatially resolved, Time Domain, Polarized |
| - | Raman | + | |
| - | IR | + | |
| - | In Vivo Microscopic Imaging | + | |
| - | Confocal Reflectance & Fluorescence Microscopy | + | |
| - | Multi Photon Microscopy | + | |
| - | Optical Coherence Tomography | + | |
| ==== Current research in the group ==== | ==== Current research in the group ==== | ||
| - | Haisha Zheng: Raman, Reflectance and Fluorescence Spectroscopy (Skin, Lung, GI) | + | **UBC: Calum MacAulay, Haisha Zheng, Pierre Lane**: \\ |
| + | Raman, Reflectance and Fluorescence Spectroscopy, In vivo confocal microendscopy, multi-photon\\ | ||
| + | Anatomical Location: Skin, Lung, GI, Cervix\\ | ||
| - | Calum MacAulay: OCT, reflectance and fluorescence spectroscopy, In vivo confocal microendscopy (Lung, Oral, Cervix, GI) | + | **McMaster: Qiyin Fang, Joe Hayward, Tom Farrell, Mike Patterson**: \\ |
| + | Time-resolved fluorescence spectroscopy & imaging, Diffused Reflectance + TRF; \\ | ||
| + | Anatomical Location: Brain, GI, Lung\\ | ||
| + | |||
| + | **UCLA: Warren Grundfest, William H. Yong** \\ | ||
| + | |||
| + | **UC Irvine: ** | ||
| - | Pierre Lane: OCT, reflectance and fluorescence spectroscopy, In vivo confocal microendscopy (Lung, Cervix, Ovarian) | ||
| ===== Challenges ===== | ===== Challenges ===== | ||
| + | Sensitivity and Specificity | ||
| - | ==== Significant clinical prblems ==== | + | Identifying opportunities/indications needing/requiring immediate clinical action (see and treat methodology) since in the genomic age if a biopsy can be taken it will be for conventional pathology (current practice) and genetic/genomic analysis (future studies) |
| + | |||
| + | ==== Significant clinical problems ==== | ||
| + | Brain, Heart, etc (tissues for which biopsy entails significant clinical risk) | ||
| + | |||
| + | Screening settings in which low specificity of primary test could result in too frequent biopsy which induces costs or morbidity (Oral, Skin, etc) | ||
| ==== Key technology barriers ==== | ==== Key technology barriers ==== | ||
| Line 36: | Line 42: | ||
| ==== potential industrial partners ==== | ==== potential industrial partners ==== | ||
| + | |||
| + | ===== References ===== | ||
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