A novel electrochemical <Superscript>99</Superscript>Mo/<Superscript>99m</Superscript>Tc generator

A novel electrochemical process to avail clinical grade ^99mTc from (n,γ)⁹⁹Mo has been demonstrated. The electrochemical parameters were optimized to maximize the ^99mTc yield with minimal ⁹⁹Mo contamination. ⁹⁹Mo/^99mTc generators containing up to 29.6 GBq (800 mCi) ⁹⁹Mo were developed and their performance were extensively evaluated for 10 days without changing the operating conditions. Very high radioactive concentration of ^99mTcO₄ ⁻ of acceptable quality, commensurate with hospital radiopharmacy requirements could be availed from the system with >90% yield. The compatibility of the product for the formulation of ^99mTc labeled radiopharmaceuticals such as ^99mTc-DMSA and ^99mTc-EC was found to be satisfactory in terms of high labeling yields. The proposed route represents an important step for enhancing the scope of accessing clinical grade ^99mTc from low specific activity (n, γ)⁹⁹Mo.     

Preparation of <Superscript>99m</Superscript>Tc-PQQ and preliminary biological evaluation for the NMDA receptor

Pyrroloquinoline quinone (PQQ), an essential nutrient, antioxidant, redox modulator and nerve growth factor found in a class of enzymes called quinoproteins, was labeled with ^99mTc by using stannous fluoride (SnF₂) method. Radiolabeling qualification, quality control and characterization of ^99mTc-PQQ and its biodistribution studies in mice were performed and discussed. Effects of pH values, temperature, time and reducing agents concentration on the radiolabeling yield were investigated. The quality control procedure of ^99mTc-PQQ was determined by thin layer chromatography (TLC), radio high-performance liquid chromatography (RHPLC) and paper electrophoresis methods. The average radiolabeling yield was 94 ± 1% under optimum conditions of 0.99 mg of PQQ, 30 μg of SnF₂, 0.5 mg of ethylenediaminetetraacetic acid disodium salt (EDTA-2Na) and 18.5 MBq of Na^99mTcO₄ at pH 6 and 25 °C with a response volume of 1 ± 0.1 mL. ^99mTc-PQQ was stable and anionic. Lipid–water partition coefficient of ^99mTc-PQQ was −1.49 ± 0.16. The pharmacokinetics parameters of ^99mTc-PQQ were t _1/2α = 18.16 min, t _1/2β = 100.45 min, K ₁₂ = 0.013 min⁻¹, K ₂₁ = 0.017 min⁻¹, K _e = 0.016 min⁻¹, AUC (area under the curve) = 1040.78 ID% g⁻¹ min and CL (plasma clearance) = 0.096 mL min⁻¹. The dual-exponential equation was Y = 10.88e^−0.038t  + 5.21e^−0.0069t . The biodistribution of ^99mTc-PQQ was studied in ICR (Institute for Cancer Research 7701 Burhelme Are., Fox Chase, Philadelphia, PA 1911 USA) mice. In vitro autoradiographic studies clearly showed that the ^99mTc-PQQ radioactivity accumulated predominantly in the hippocampus and cortex, which had a high density of N-methyl-d-aspartate Receptor (NMDAR). The enrichment can be blocked by NMDAR redox modulatory site antagonists-ebselen (EB) and ^99mTc-PQQ is therefore a promising candidate for the molecular imaging of NMDAR. To date, however, there have been no studies characterizing ^99mTc-PQQ.     

Adsorption behavior of <Superscript>99</Superscript>Tc on Fe,Fe<Subscript>2</Subscript>O<Subscript>3</Subscript> and Fe<Subscript>2</Subscript>O<Subscript>4</Subscript>

Summary The adsorption of ⁹⁹Tc on the adsorbers Fe, Fe₂O₃ and Fe₃O₄ was studied by batch experiments under aerobic and anoxic conditions. The effects of pH and CO₃^2- concentration of the simulated ground water on the adsorption ratios were also investigated, and the valences of Tc in solution after the adsorption equilibrium were studied by solvent extraction. The adsorption isotherms of TcO₄- on the adsorbers Fe, Fe₂O₃ and Fe₃O₄ were determined. Experimental results have shown that the adsorption ratio of Tc on Fe decreases with the increase of pH in the range of 5-12 and increases with the decrease of the CO₃^2- concentration in the range of 10^-8M-10^-2M. Under aerobic conditions, the adsorption ratios of ⁹⁹Tc on Fe₂O₃ and Fe₃O₄ were not influenced by pH and CO₃^2-concentration. When Fe was used as adsorbent, Tc existed mainly in the form of Tc(IV) after equilibrium and in the form of Tc(VII) when the adsorbent was Fe₂O₃ or Fe₃O₄ under aerobic conditions. The adsorption ratios of Tc on Fe, Fe₂O₃ and Fe₃O₄ decreased with the increase of pH in the range of 5-12 and increased with the decrease of the CO₃^2- concentration in the range of 10^-8M-10^-2M under anoxic conditions. Tc existed mainly in the form of Tc(IV) after equilibrium when Fe, Fe₂O₃ and Fe₃O₄ was the adsorbent under anoxic conditions. The adsorption isotherms of TcO_4- on the adsorbers Fe, Fe₂O₃ and Fe₃O₄ are fairly in agreement with the Freundlich’s equation under both aerobic and anoxic conditions.     

Biodistribution and toxicity assessment of radiolabeled and DMSA coated ferrite nanoparticles in mice

DMSA-coated Fe₃O₄ nanoparticles were synthesized by wet-chemical method. The chemical interaction between Fe₃O₄ and DMSA were investigated by FTIR. They were directly radiolabeled with ^99mTc radioisotope (Fe₃O₄@DMSA–^99mTc) at room temperature in the presence of stannous solution as a reducing agent. Magnetic and structure properties of Fe₃O₄@DMSA–^99mTc nanoparticles were investigated by AGFM, TEM, and XRD. Biodistribution and toxicity assessment of Fe₃O₄@DMSA–^99mTc were studied in mice by intravenous and intraperitoneally injections, respectively. Blood, kidney, and liver factors were measured 4 days post injection and at the mean-while tissue sections were prepared from their kidney and liver. The results indicate that, the Fe₃O₄@DMSA–^99mTc nanoparticles were passed through the membrane of different cells but do not create any disorder in the kidney and liver function even in high doses such as 300 mg/kg.     

Facile deposition of gold nanoparticles on core–shell Fe3O4@polydopamine as recyclable nanocatalyst

A simple and green method for the controllable synthesis of core–shell Fe₃O₄ polydopamine nanoparticles (Fe₃O₄@PDA NPs) with tunable shell thickness and their application as a recyclable nanocatalyst support is presented. Magnetite Fe₃O₄ NPs formed in a one-pot process by the hydrothermal approach with a diameter of ∼240 nm were coated with a polydopamine shell layer with a tunable thickness of 15–45 nm. The facile deposition of Au NPs atop Fe₃O₄@PDA NPs was achieved by utilizing PDA as both the reducing agent and the coupling agent. The satellite nanocatalysts exhibited high catalytic performance for the reduction of p-nitrophenol. Furthermore, the recovery and reuse of the catalyst was demonstrated 8 times without detectible loss in activity. The synergistic combination of unique features of PDA and magnetic nanoparticles establishes these core–shell NPs as a versatile platform for potential applications.     

Synthesis of nano‐sized magnetite mesoporous carbon for removal of Reactive Yellow dye from aqueous solutions

In this study, core‐shell structures of magnetite nanoparticles coated with CMK‐8 ordered mesoporous carbon (Fe₃O₄@SiO₂‐CMK‐8 NPs) have been successfully synthesized for the first time by carbonizing sucrose inside the pores of the Kit‐6 mesoporous silica. The nano‐sized mesoporous particles were characterized by X‐ray diffraction, Fourier transform‐infrared spectroscopy, scanning electron microscope, dynamic light scattering, vibrating‐sample magnetometer, Brunauer–Emmett–Teller (BET) and transmission electron microscopy instruments. The obtained nanocomposite was used for removal of Reactive Yellow 160 (RY 160) dye from aqueous samples. The N₂ adsorption–desorption method (at 77 K) confirmed the mesoporous structure of synthesized Fe₃O₄@SiO₂‐CMK‐8 NPs. Also, the surface area was calculated by the BET method and Langmuir plot as 276.84 m²/g and 352.32 m²/g, respectively. The surface area, volume and pore diameter of synthesized nanoparticles (NPs) were calculated from the pore size distribution curves using the Barrett–Joyner–Halenda formula (BJH). To obtain the optimum experimental variables, the effect of various experimental parameters on the dye removal efficiency was studied using Taguchi orthogonal array experimental design method. According to the experimental results, about 90.0% of RY 160 was removed from aqueous solutions at the adsorbent amount of 0.06 g, pH 3 and ionic strength = 0.05 m during 10 min. The pseudo‐second order kinetic model provided a very good fit for the RY 160 dye removal (R² = 0.999). The Langmuir, Freundlich, Temkin and Dubinin–Radushkevich models were applied to describe the equilibrium isotherms, and the Langmuir isotherm showed the best fit to data with the maximum adsorption capacity of 62.893 mg/g. Furthermore, the Fe₃O₄@SiO₂‐CMK‐8 NPs could be simply recovered by external magnet, and exhibited recyclability and reusability for a subsequent six runs.     

Synthesis of novel magnetic sulfur-doped Fe<Subscript>3</Subscript>O<Subscript>4</Subscript> nanoparticles for efficient removal of Pb(II)

In this work, we report the synthesis of magnetic sulfur-doped Fe₃O₄ nanoparticles (Fe₃O₄:S NPs) with a novel simple strategy, which includes low temperature multicomponent mixing and high temperature sintering. The prepared Fe₃O₄:S NPs exhibit a much better adsorption performance towards Pb(II) than bare Fe₃O₄ nanoparticles. FTIR, XPS, and XRD analyses suggested that the removal mechanisms of Pb(II) by Fe₃O₄:S NPs were associated with the process of precipitation (formation of PbS), hydrolysis, and surface adsorption. The kinetic studies showed that the adsorption data were described well by a pseudo second-order kinetic model, and the adsorption isotherms could be presented by Freundlich isotherm model. Moreover, the adsorption was not significantly affected by the coexisting ions, and the adsorbent could be easily separated from water by an external magnetic field after Pb(II) adsorption. Thus, Fe₃O₄:S NPs are supposed to be a good adsorbents for Pb(II) ions in environmental remediation.     

Synthesis,radiochemical and biological characteristics of <Superscript>99m</Superscript>Tc-8-hydroxy-7-substituted quinoline complex: a novel agent for infection imaging

2,2′-[(8-hydroxyquinolin-7-yl)methylazanediyl]diacetic acid (HQMADA) was synthesized via reaction of 8-hydroxyquinoline with iminodiacetic acid in presence of paraformaldehyde with a yield of 27%. The obtained compound was well characterized via different analytical techniques. Labeling of the synthesized compound with technetium-99m in pertechnetate form (^99mTcO₄ ⁻) in the presence of stannous chloride dihydrate was carried out via chelation reaction. The reaction parameters that affect the labeling yield such as HQMADA concentration, stannous chloride dihydrate concentration, pH of the reaction mixture, and reaction time were studied to optimize the labeling conditions. Maximum radiochemical yield of ^99mTc-HQMADA complex (91.9%) was obtained by using 1.5 mg HQMADA, 50 μg SnCl₂·2H₂O, pH 8 and 30 min reaction time. Biodistribution studies in mice were carried out in experimentally induced infection in the left thigh using E. coli. ^99mTc-HQMADA complex showed higher uptake (T/NT = 5.5 ± 0.3) in the infectious lesion than the commercially available ^99mTc-ciprofloxacin (T/NT = 3.8 ± 0.8). Biodistribution studies for ^99mTc-HQMADA complex in Albino mice bearing septic and aseptic inflammation models showed that ^99mTc-HQMADA complex able to differentiate between septic and aseptic inflammation.     

Pectin mediated green synthesis of Fe3O4/Pectin nanoparticles under ultrasound condition as an anti-human colorectal carcinoma bionanocomposite

This work described the one-pot synthesis of apple pectin encapsulated Fe₃O₄ nanoparticles (Fe₃O₄/Pectin NPs) which is prepared by co-precipitation of Fe(II/(III) ions in alkaline solution mediated by pectin under ultrasound condition. This process led to formation of magnetic nanoparticles within the network of pectin. Physicochemical characterization of the as-synthesized Fe₃O₄/Pectin NPs was carried out through electron microscopy (SEM and TEM), energy dispersive X-ray spectroscopy (EDX), vibrating sample magnetometer (VSM) and X-ray diffraction (XRD). The in vitro cytotoxic and anti-colorectal cancer effects of biologically synthesized Fe₃O₄/Pectin NPs against Ramos.2G6.4C10, HCT-8 [HRT-18], HCT 116, and HT-29 cancer cell lines were assessed. The anti-colorectal cancer properties of the Fe₃O₄/Pectin NPs could significantly remove Ramos.2G6.4C10, HCT-8 [HRT-18], HCT 116, and HT-29 cancer cell lines in a time and concentration-dependent manner by MTT assay. The IC₅₀ of the Fe₃O₄/Pectin NPs were 317, 337, 187, and 300 µg/mL against Ramos.2G6.4C10, HCT-8 [HRT-18], HCT 116, and HT-29 cancer cell lines. The antioxidant activity of Fe₃O₄/Pectin NPs was determined by DPPH method. The Fe₃O₄/Pectin NPs showed the high antioxidant activity according to the IC₅₀ value. It seems that the anti-human colorectal cancer effect of recent nanoparticles is due to their antioxidant effects.     

Magnetic nanoparticles (Fe<Subscript>3</Subscript>O<Subscript>4</Subscript> &amp; Co<Subscript>3</Subscript>O<Subscript>4</Subscript>) and their applications in urea biosensing

Nanobiotechnology has opened a new and exciting opportunities for exploring urea biosensor based on magnetic nanoparticles (NPs) mainly Fe₃O₄ and Co₃O₄. These NPs have been extensively exploited to develop biosensors with stability, selectivity, reproducibility and fast response time. This review gives an overview of the development of urea biosensor based on Fe₃O₄ and Co₃O₄ for in vitro diagnostic applications along with significant improvements over the last few decades. Additionally, effort has been made to elaborate properties of magnetic nanoparticles (MNPs) in biosensing aspects. It also gives details of recent developments in hybrid nanobiocomposite based urea biosensor.     

S-bridged complex of <Superscript>99m</Superscript>Tc with <Emphasis Type="Italic">fac</Emphasis>(S)-[Rh(aet)<Subscript>3</Subscript>]: Quality control,characterization and biodistribution studies in rats

fac(S)-[Rh(aet)₃] (aet = 2-aminoethanethiolate) is N₃S₃ metalloligand which can coordinate to transition metal ions to form S-bridge polynuclear complexes. The reaction was carried out between ^99mTcO₄Na and fac(S)-[Rh(aet)₃] in the presence of SnCl₂·2H₂O. A complex analogous to [Re{Rh(aet₃)}₂]³⁺ is formed.⁶ A simple method for radiolabeling of fac(S)-[Rh(aet)₃] with ^99mTc has been developed and radiolabeling efficiency was higher than 99%. Effect of SnCl₂·2H₂O concentration, electrophoresis, HPLC, UV-Visible absorption spectra and biodistribution studies in rats were performed. Higher uptake by kidneys showed rapid distributions of the labeled fac(S)-[Rh(aet)₃]. Liver uptake was significant, stomach, lungs and intestine uptake was high at 4 hours post injection time.     

Kinetics of adsorption of Saccharomyces cerevisiae mandelated dehydrogenase on magnetic Fe3O4–chitosan nanoparticles

The adsorption of Saccharomyces cerevisiae mandelated dehydrogenase (SCMD) protein on the surface-modified magnetic nanoparticles coated with chitosan was studied in a batch adsorption system. Functionalization of surface-modified magnetic particles was performed by the covalent binding of chitosan onto the surface of magnetic Fe₃O₄ nanoparticles. Characterization of these particles was carried out using FTIR spectra, transmission electron micrography (TEM), X-ray diffraction (XRD) and vibrating sample magnetometry (VSM). Magnetic measurement revealed that the magnetic Fe₃O₄–chitosan nanoparticles were superparamagnetic and the saturation magnetization was about 37.3 emu g⁻¹. The adsorption capacities and rates of SCMD protein onto the magnetic Fe₃O₄–chitosan nanoparticles were evaluated. The adsorption capacity was influenced by pH, and it reached a maximum value around pH 8.0. The adsorption capacity increased with the increase in temperature. The adsorption isothermal data could be well interpreted by the Freundlich isotherm model. The kinetic experimental data properly correlated with the first-order kinetic model, which indicated that the reaction is the adsorption control step. The apparent adsorption activation energy was 27.62 kJ mol⁻¹ and the first-order constant for SCMD protein was 0.01254 min⁻¹ at 293 K.     

Synthesis, biodistribution and evaluation of 99mTc-sitafloxacin kit: a novel infection imaging agent

Radiosynthesis of ^99mTc-sitafloxacin (^99mTc-STF) complex and its efficacy as a potential infection imaging agent was evaluated. Effect of sitafloxacin (STF) concentration, sodium pertechnetate (Na^99mTcO₄), stannous chloride dihydrate (SnCl₂·2H₂O), and pH on the % radiochemical purity yield (RCP) of ^99mTc-STF complex was studied. A stable ^99mTc-STF complex up to 120 min with maximum %RCP yield was observed by mixing 2 mg of STF with 3 mCi of Na^99mTcO₄ and 150 μL of SnCl₂·2H₂O (1 μg/μL in 0.01 N HCl) at a pH 5.5. Artificially infected rats with Staphylococcus aureus were used for studying the biodistribution behavior of the ^99mTc-STF complex. After 30 min of the intravenous (I.V.) administration of the ^99mTc-STF complex, 7.50 ± 0.10% was absorbed in the infected thigh of the rats and the uptake gradually increased to 18.50 ± 0.20% within 90 min. Rabbits with artificially induced infection were used for evaluating the scintigraphic accuracy. Higher uptake in the infected thigh was observed after 2 h of I.V. administration of the ^99mTc-STF complex. Target to non-target organ ratio of the % absorbed dose incase of infected/normal muscle was 6.82 ± 0.40, 17.11 ± 0.60, and 23.13 ± 1.00% at 30, 60 and 90 min of administration. Stable and higher %RCP, higher uptake in the infected thigh, and spectral studies, recommend the ^99mTc-STF for routine infection imaging.     

Synthesis and evaluation of a new bombesin analog labeled with <Superscript>99m</Superscript>Tc as a GRP receptor imaging agent

Tumors such as prostate, small cell lung cancer, breast, gastric and colon cancer are known to overexpress receptors to bombesin (BBN). In this study, a new bombesin analogue was labeled with ^99mTc via HYNIC and tricine/EDDA as coligands and investigated further. HYNIC-GABA-Bombesin (7–14) NH₂ was synthesized using a standard Fmoc strategy. Labeling with ^99mTc was performed at 100 °C for 10 min and radiochemical analysis involved ITLC and HPLC methods. The stability of radiopeptide was checked in the presence of humane serum at 37 °C up to 24 h. The receptor bound internalization and externalization rates were studied in GRP receptor expressing PC-3 cells. Biodistribution of radiopeptide was studied in nude mice bearing PC-3 tumor. Labeling yield of >98% was obtained corresponding to a specific activity of ~2.6 MBq/nmol. Peptide conjugate showed good stability in the presence of human serum. The radioligand showed high and specific internalization into PC-3 cells (14.63 ± 0.41% at 4 h). In biodistribution studies, a receptor-specific uptake was observed in GRP-receptor-positive organs so that after 4 h the uptakes in mouse tumor and pancreas were 1.31 ± 0.18 and 1.2 ± 0.13% ID/g, respectively.     

Quantification of <Superscript>241</Superscript>Pu in aerosols released from nuclear power plants

Two peptide ligands conjugated adenine, [9-N-(tritylmercapto acetyl diglycyl aminoethyl) adenine, Tr-MAG₂-Ade] and [9-N-(tritylmercapto acetyl triglycyl aminoethyl) adenine, Tr-MAG₃-Ade], are synthesized and labeled with ^99mTc by directly labeling method. The stability of ^99mTc-MAG₂-adenine and ^99mTc-MAG₃-adenine in vitro is measured. The uptake radios of tumor to muscle at 3h post-injection are 5.70 and 4.92, respectively. The biodistribution and scintigraphic imaging studies show that the two complexes have high localization in tumor and high contrasted tumor images can be obtained, which suggest their potential utility as tumor imaging agents. But the high radioactivity of abdomen could prevent the tumor imaging in this area.     

Preparation and biological evaluation of radiolabeled-folate embedded superparamagnetic nanoparticles in wild-type rats

In this study, superparamagnetic iron oxide nanoparticles (SPION) embedded by folic acid (SPION-folate) were prepared by a modified co-precipitation method. The structure, size, morphology, magnetic property and relaxivity of the SPION-folate were characterized systematically by means of XRD, VSM, HRSEM and TEM and the interaction between folate and iron oxide (Fe₃O₄) was characterized by FT-IR. The particle size was shown to be ≈5–10 nm. To ensure biocompatibility, the interaction of these SPION with mouse connective tissue cells (adhesive) was investigated using an MTT assay. Consequently, gallium-67 labeled nanoparticles ([⁶⁷Ga]-SPION-folate) were prepared using ⁶⁷Ga with a high labeling efficiency (over 96%, RTLC method) and they also showed an excellent stability at room temperature for at least 2 days and were evaluated for their biodistribution in normal rats up to 24 h compared with free Ga³⁺ cation and [⁶⁷Ga]-SPION biodistribution. The biodistribution of the tracer among 3 other folate tracers were compared, showing lower liver uptake and higher blood circulation after 24 h leading to better bioavailability. The bone:muscle, kidney:muscle, lung:muscle, stomach:muscle ratios were 9.3, 9.32, 7.6 and 5.83 respectively. The developed folate-containing nano-system can be an interesting folate receptor tracer, capable of better cell membrane permeability while possessing paramagnetic properties for thermotherapy.     

The interaction of <Superscript>99m</Superscript>Tc with pyrimidine compounds

The reaction of ^99mTc of different oxidation states (+7, +4) with 2-thiouracil and 5-nitrobarbituric acid have been studied at different temperatures, pH and concentrations. The reaction mixtures have been analyzed at different times using thin layer chromatography (TLC) and a radio detector to show the peaks at the plates. ^99mTc is obtained from the Mo generators with oxidation state (+7). The use of SnCl₂ as a reducing agent gave ^99mTc with oxidation state (+4). It is very difficult to separate the complexes formed from the reactions in very small concentration. The percentage of ^99mTc and its oxidation state involved in the complexes can be determined. The labeling efficiencies (percentage of complex) in the reaction of ^99mTc⁺⁷ with 5-nitro-barbituric-acid increases mostly at pH  10. Both oxidation states of ^99mTc(+7, +4) can be detected at pH’s 4 and 10, but at pH  4, the reduced form ^99mTCO₂, is more pronounced. At pH  7 no complexes were detected and most of ^99mTc remains as ^99mTCO₄ ⁻ . By increasing the ligand concentration, the labeling efficiencies of the complex increases. For the reaction of ^99mTc of oxidation states (+4, +7) with 2-thiouracil at different temperatures and analytical times it is concluded that several complexes with different R_f values were observed in equilibrium and most of these complexes were unstable.     

Magnetically recyclable nano copper/chitosan in O‐arylation of phenols with aryl halides

Interaction of chitosan (CS) with Fe₃O₄, followed by embedding Cu nanoparticles (NPs) on the magnetic surface through adsorption of Cu²⁺, and its reduction to Cu^o via NaBH₄, offers a reusable efficient catalyst (Fe₃O₄/CS‐Cu NPs) that is employed in cross‐coupling reactions of aryl halides with phenols, which affords the corresponding diaryl ethers, with good to excellent yields. The catalyst is completely recoverable from the reaction mixture by using an external magnet. It can be reused four times, without significant loss in its catalytic activity.     

Synthesis of Co/MFe2O4 (M=Fe, Mn) core/shell nanocomposite particles

Monodispersed cobalt nanoparticles (NPs) with controllable size (8–14 nm) have been synthesized using thermal decomposition of dicobaltoctacarbonyl in organic solvent. The as-synthesized high magnetic moment (125 emu/g) Co NPs are dispersible in various organic solvents, and can be easily transferred into aqueous phase by surface modification using phospholipids. However, the modified hydrophilic Co NPs are not stable as they are quickly oxidized, agglomerated in buffer. Co NPs are stabilized by coating the MFe₂O₄ (M=Fe, Mn) ferrite shell. Core/shell structured bimagnetic Co/MFe₂O₄ nanocomposites are prepared with tunable shell thickness (1–5 nm). The Co/MFe₂O₄ nanocomposites retain the high magnetic moment density from the Co core, while gaining chemical and magnetic stability from the ferrite shell. Compared to Co NPs, the nanocomposites show much enhanced stability in buffer solution at elevated temperatures, making them promising for biomedical applications.     

Perylene diimide‐modified magnetic γ‐Fe2O3/CeO2 nanoparticles as peroxidase mimics for highly sensitive colorimetric detection of Vitamin C

Perylene diimide‐modified magnetic γ‐Fe₂O₃/CeO₂ nanoparticles (γ‐Fe₂O₃/CeO₂‐PDI) were prepared and exhibited excellent peroxidase‐like activity. The samples were characterized by HR‐TEM, XRD, Raman, N₂ adsorption, magnetic strength and XPS. The obtained γ‐Fe₂O₃/CeO₂‐PDI had size of 10~20 nm with high specific surface area of 77 m²/g, and could be easily separated from the aqueous solution by using a magnet, which are in favor of its practical application. Due to the decoration of PDI, the γ‐Fe₂O₃/CeO₂‐PDI possessed more surface defects (Ce³⁺) and active oxygen species than that of γ‐Fe₂O₃/CeO₂, resulting in the outstanding catalytic performance. And the composite catalyst also showed highly sensitive and selectivity toward VC with a limit of detection of 0.45 μM. Based on the fluorescent results, a possible hydroxyl radical (?OH) catalytic mechanism was proposed. It is believed that the as‐prepared γ‐Fe₂O₃/CeO₂‐PDI nanoparticles are promising biosensors applied for biomedical and food analysis.