There is a rapid rise in cybercrime cases. There does not exist any effective forensic methods to deal with these eybercrime cases. Investigators are required to study the details of a large amount of tedious source i...There is a rapid rise in cybercrime cases. There does not exist any effective forensic methods to deal with these eybercrime cases. Investigators are required to study the details of a large amount of tedious source in order to understand the crime model and dig out the evidence. This requires a lot of effort and may result in human errors. In order to overcome these potential errors that may cause by the investigators, we propose a semi-automatic approach that integrates the user view (based on a high level study of the forensic investigator) and the system view (based on the automatic analysis of the source codes) to assist investigators in refining the scope of the investigation. The approach has been verified using a real cybercrime case and the method has been shown to be effective in assisting the investigators in refining the scope of investigation and understanding the crime model. The semi-automatic approach has improved the efficiency and reliability of the digital forensic analysis of cybercrime cases involving large volume of digital evidence from multiple sources.展开更多
diagnostic and therapeutic capability are highly needed for the treatment of hepatic cancer.Herein,we aimed to develop a novel mesoporous polydopamine(MPDA)-based theranostic agent for T1/T2 dual magnetic resonance im...diagnostic and therapeutic capability are highly needed for the treatment of hepatic cancer.Herein,we aimed to develop a novel mesoporous polydopamine(MPDA)-based theranostic agent for T1/T2 dual magnetic resonance imaging(MRI)-guided cancer chemo-photothermal therapy.Superparamagnetic iron oxide(SPIO)-loaded MPDA NPs(MPDA@SPIO)was firstly prepared,followed by modifying with a targeted molecule of sialic acid(SA)and chelating with Fe^(3+)(SA-MPDA@SPIO/Fe^(3+) NPs).After that,doxorubicin(DOX)-loaded SA-MPDA@SPIO/Fe^(3+) NPs(SA-MPDA@SPIO/DOX/Fe^(3+))was prepared for tumor theranostics.The prepared SAPEG-MPDA@SPIO/Fe^(3+) NPs were water-dispersible and biocompatible as evidenced by MTT assay.In vitro photothermal and relaxivity property suggested that the novel theranostic agent possessed excellent photothermal conversion capability and photostability,with relaxivity of being r1=4.29 mM1s1 and r2=105.53 mM1s1,respectively.SAPEG-MPDA@SPIO/Fe^(3+) NPs could effectively encapsulate the DOX,showing dual pH-and thermal-triggered drug release behavior.In vitro and in vivo studies revealed that SA-MPDA@SPIO/DOX/Fe^(3+) NPs could effectively target to the hepatic tumor tissue,which was possibly due to the specific interaction between SA and the overexpressed E-selectin.This behavior also endowed SA-MPDA@SPIO/DOX/Fe^(3+)NPs with a more precise T1-T2 dual mode contrast imaging effect than the one without SA modification.In addition,SAPEG-MPDA@SPIO/DOX/Fe^(3+) NPs displayed a superior therapeutic effect,which was due to its active targeting ability and combined effects of chemotherapy and photothermal therapy.These results demonstrated that SAPEG-MPDA@SPIO/DOX/Fe^(3+) NPs is an effective targeted nanoplatform for tumor theranostics,having potential value in the effective treatment of hepatic cancer.展开更多
文摘There is a rapid rise in cybercrime cases. There does not exist any effective forensic methods to deal with these eybercrime cases. Investigators are required to study the details of a large amount of tedious source in order to understand the crime model and dig out the evidence. This requires a lot of effort and may result in human errors. In order to overcome these potential errors that may cause by the investigators, we propose a semi-automatic approach that integrates the user view (based on a high level study of the forensic investigator) and the system view (based on the automatic analysis of the source codes) to assist investigators in refining the scope of the investigation. The approach has been verified using a real cybercrime case and the method has been shown to be effective in assisting the investigators in refining the scope of investigation and understanding the crime model. The semi-automatic approach has improved the efficiency and reliability of the digital forensic analysis of cybercrime cases involving large volume of digital evidence from multiple sources.
基金supported by Institute of Nanomaterials and Nanotechnology,Lishui Hospital of Zhejiang UniversityPostdoctoral Foundation of ZheJiang province+2 种基金National Key Research and Development projects intergovernmental cooperation in science and technology of China(2018YFE0126900)Zhejiang Provincial Natural Science Foundation(LY15H030010,LY20H180016,Q21H180011)The Key R&D Program of Lishui City(2019ZDYF17).
文摘diagnostic and therapeutic capability are highly needed for the treatment of hepatic cancer.Herein,we aimed to develop a novel mesoporous polydopamine(MPDA)-based theranostic agent for T1/T2 dual magnetic resonance imaging(MRI)-guided cancer chemo-photothermal therapy.Superparamagnetic iron oxide(SPIO)-loaded MPDA NPs(MPDA@SPIO)was firstly prepared,followed by modifying with a targeted molecule of sialic acid(SA)and chelating with Fe^(3+)(SA-MPDA@SPIO/Fe^(3+) NPs).After that,doxorubicin(DOX)-loaded SA-MPDA@SPIO/Fe^(3+) NPs(SA-MPDA@SPIO/DOX/Fe^(3+))was prepared for tumor theranostics.The prepared SAPEG-MPDA@SPIO/Fe^(3+) NPs were water-dispersible and biocompatible as evidenced by MTT assay.In vitro photothermal and relaxivity property suggested that the novel theranostic agent possessed excellent photothermal conversion capability and photostability,with relaxivity of being r1=4.29 mM1s1 and r2=105.53 mM1s1,respectively.SAPEG-MPDA@SPIO/Fe^(3+) NPs could effectively encapsulate the DOX,showing dual pH-and thermal-triggered drug release behavior.In vitro and in vivo studies revealed that SA-MPDA@SPIO/DOX/Fe^(3+) NPs could effectively target to the hepatic tumor tissue,which was possibly due to the specific interaction between SA and the overexpressed E-selectin.This behavior also endowed SA-MPDA@SPIO/DOX/Fe^(3+)NPs with a more precise T1-T2 dual mode contrast imaging effect than the one without SA modification.In addition,SAPEG-MPDA@SPIO/DOX/Fe^(3+) NPs displayed a superior therapeutic effect,which was due to its active targeting ability and combined effects of chemotherapy and photothermal therapy.These results demonstrated that SAPEG-MPDA@SPIO/DOX/Fe^(3+) NPs is an effective targeted nanoplatform for tumor theranostics,having potential value in the effective treatment of hepatic cancer.