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測(cè)量應(yīng)用案例-20200710

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發(fā)布時(shí)間:2020-07-28
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文獻(xiàn)名: Metal–DrugProtein Assemblies: Gd3+ SelfEnhanced Magnetic Resonance Imaging, HighSensitive TumorTargeting Imaging and Efficient ChemoPhototherapy

 

作者 Jia Zhou, Tianliang Li, Yiran Zhang, Xiaoyu Xu, Chunlei Zhang, Yuehua Li, Daxiang Cui, Yingsheng Cheng

Department of Radiology, Shanghai Jiao Tong University Affiliated Sixth People's Hospital, 600 Yishan Road, Shanghai, 200233 China

 

摘要:Magnetic resonance imaging (MRI) contrast agents are broadly employed for better clinical trials in MR imaging. Magnevist solution (GdDTPA), a clinical MRI contrast agent, possesses inherent shortcomings like poor r1 relaxation, short halftime, nephrotoxicity, etc. To overcome these problems, GdDTPAgrafted protein assemblies (GdPABs) loading with anticancer drug cisplatin and photosentizer IR780 are constructed via chelation of Gd3+. GdPABs exhibit dual MR/fluorescence (FL) imagingguided chemo/photothermal therapy. Interestingly, GdPABs behave as aggregationenhanced magnetic resonance imaging with an extremely high r1 value of 26.391 s−1 mm−1, which is about 5.5fold larger than GdDTPA (4.8 s−1 mm−1). Consequently, better MRI performance is presented with the same concentration of Gd ions. When exposed to acidic tumor microenvironment and light irradiation, Gd‐PABs show significant drug release capacity. Good cell killing ability in vitro is also determined due to effective folatetargeting ability and high photoheat conversion. In vivo MR/FL imaging results reveal that GdPABs possess highsensitivity tumortargeting imaging and long tumor retention, which are attributed to the folatetargeting ability and small size effect. Combined chemo/photothermal therapy in vivo demonstrates that the tumor can be eventually ablated. Altogether, the GdPABs possess great potential for clinical imagingguided tumor therapy.

 

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