Article ID Journal Published Year Pages File Type
4217954 Academic Radiology 2014 8 Pages PDF
Abstract
Advances in genomics are enabling integration of various -omics to reveal the complexities underneath carcinogenesis. Multivariate signaling pathways are deregulated and evolve spatially and temporally depending on the tumor microenvironment. This finding shifts the focus of cancer research from “one disease-one target and drug” to “one disease-multiple pathway targets and combinational therapy” and imposes new challenges on the imaging community in terms of imaging targets, scales and information levels. In current clinical settings, most imaging modalities assess cancer risk through alternations in anatomy, function, metabolism, cellularity, or limited molecular events. Few clinical-translatable imaging modalities are capable of detecting aberrations in signaling pathways at the level of tissue biology. An exception to this is hyperpolarized 13C magnetic resonance spectroscopic imaging (HP 13C MRI), which is capable of imaging the molecular signatures of special metabolic enzymes using HP 13C-labeled substrates. HP 13C MRI can identify multiple metabolites including intermediates and products simultaneously to allow extraction of critical parameters such as flux alterations for multiple metabolic pathways. Meanwhile, recent progress in cancer metabolism research affirms that metabolic alterations are directly controlled by signaling pathways. Thus, in vivo assessment of aberrations occurring in signaling pathways becomes feasible through HP 13C imaging. This report briefly reviews the connections between signaling pathways and cancer metabolic phenotypes, the current status of HP 13C MRI in assessing signal pathways, and recent advances in HP 13C MRI techniques. Integrated with cancer genomics and animal models, HP 13C MRI may hold high promise in exploring important issues in cancer that are linked to functionality of signaling pathways. Examples include genomic-driven therapy, intratumoral heterogeneity, and drug resistances.
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