【摘 要】
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Many types of biocompatible nanomaterials have proven of low cytotoxicity and hold great promise for various applications in nanomedicine.Whereas they generally do not cause apparent organ toxicity or
【机 构】
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Key Laboratory of Food Safety Research, Institute for Nutritional Sciences, Shanghai Institutes for
【出 处】
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2016(第二届)毒性测试替代方法与转化毒理学(国际)学术研讨会暨有害结局路径(AOP)与风险评估培训会议
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Many types of biocompatible nanomaterials have proven of low cytotoxicity and hold great promise for various applications in nanomedicine.Whereas they generally do not cause apparent organ toxicity or tissue damage in adult animals, it is yet to determine their biological consequences in more general contexts.In this study, we investigate how silica nanoparticles (NPs) affect cellular activities and functions under several physiological or pathological conditions.Although silica Nps are generally regarded as "inert" nanocarriers and widely employed in biomedical studies, we find that they actively affect Wnt signaling in various types of cell lines, diminishing its anti-adipogenic effect in preadipocytes and pro-invasive effect in breast cancer cells, and more significantly, impair Wnt-regulated embryonic development in Zebrafish.We further demonstrate that intracellular silica NPs block Wnt signal transduction in a way resembling signaling molecules.Specifically, silica NPs target the Dvl protein, a key component of Wnt signaling cascade, for lysosomal degradation.As Wnt signaling play significant roles in embryonic development and adipogenesis, the observed physiological effects beyond toxicity imply potential risk of obesity, or developmental defects in somitogenesis and osteogenesis upon exposure to silica NPs.In addition, our work also establishes for the first time a molecular link between nanomaterials and the Wnt signaling pathway, and expands our understanding of biological effects induced by nanomaterials.
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