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Dewi  Melissa R.  Laufersky  Geoffry  Nann  Thomas 《Mikrochimica acta》2015,182(13):2293-2298

Hetero-dimeric magnetic nanoparticles of the type Au-Fe3O4 have been synthesised from separately prepared, differently shaped (spheres and cubes), monodisperse nanoparticles. This synthesis was achieved by the following steps: (a) Mono-functionalising each type of nanoparticles with aldehyde functional groups through a solid support approach, where nanoparticle decorated silica nanoparticles were fabricated as an intermediate step; (b) Derivatising the functional faces with complementary functionalities (e.g. amines and carboxylic acids); (c) Dimerising the two types of particles via amide bond formation. The resulting hetero-dimers were characterised by high-resolution TEM, Fourier transform IR spectroscopy and other appropriate methods.

Nano-LEGO: Assembling two types of separately prepared nanoparticles into a hetero-dimer is the first step towards complex nano-architectures. This study shows a solid support approach to combine a gold and a magnetite nanocrystal.

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Hetero-dimeric magnetic nanoparticles of the type Au-Fe3O4 have been synthesised from separately prepared, differently shaped (spheres and cubes), monodisperse nanoparticles. This synthesis was achieved by the following steps: (a) Mono-functionalising each type of nanoparticles with aldehyde functional groups through a solid support approach, where nanoparticle decorated silica nanoparticles were fabricated as an intermediate step; (b) Derivatising the functional faces with complementary functionalities (e.g. amines and carboxylic acids); (c) Dimerising the two types of particles via amide bond formation. The resulting hetero-dimers were characterised by high-resolution TEM, Fourier transform IR spectroscopy and other appropriate methods.
Graphical Abstract Nano-LEGO: Assembling two types of separately prepared nanoparticles into a hetero-dimer is the first step towards complex nano-architectures. This study shows a solid support approach to combine a gold and a magnetite nanocrystal.
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Glycogen synthase kinase-3 α/β is involved in dysregulation of neuronal tau protein in Alzheimer's disease (AD). There is an unmet clinical need for a blood-brain barrier (BBB) permeable positron emission tomography (PET) probe for imaging of GSK-3α/β in the brain to understand the pathogenesis of AD. Herein, we synthesized two PET probes, [18F]F-CNBI and [18F]F-CNPIFE, and evaluated their BBB permeability and affinity towards GSK-3α/β. [19F]F-CNPIFE showed higher in-vitro binding towards GSK-3α/β (IC50=19.4±2.5 nM; n=3, for GSK-3α, IC50=19.4±3.8 nM; n=3, for GSK-3β) compared to [19F]F-CNBI (IC50=107.6±26.0 nM; n=4, for GSK-3α, IC50=105.3±18.2 nM; n=3, for GSK-3β). [18F]F-CNPIFE showed 9.5-fold higher brain uptake than [18F]F-CNBI, in normal FVB/NJ mice, which was increased by additional 1.5-fold on co-administration of [19F]F-CNPIFE with respect to [18F]F-CNBI. Overall, [18F]F-CNPIFE is a promising PET probe for GSK-3α/β imaging and warrants further evaluation in an AD mouse model.  相似文献   
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