Targeting nano drug delivery system aiming at brain glioma and preparation methods and application thereof
A nano-drug delivery system and brain glioma technology, which is applied in the direction of anti-tumor drugs, drug combinations, non-active ingredients of polymer compounds, etc., can solve the problems of mutual interference of targeted molecules and complex construction methods
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Embodiment 1
[0031] Preparation of PEG-PLA nanoparticles (NP): Prepared by single milk method, accurately weigh 28mg MPEG-PLA, 2mgCOOH-PEG-PLA, dissolve in 1ml dichloromethane, add 5ml 0.6% sodium cholate, ice water bath Sonicate for 5 s, stop for 5 s, 20 times in total, remove dichloromethane by rotary steaming at 37°C for 15 min, centrifuge at 13500 rpm at 4°C for 50 min, discard the supernatant, disperse and precipitate with 0.5 mL deionized water to obtain nanoparticles.
[0032] Preparation of Peptide-PEG-PLA nanoparticles (PNP): Add carboxyl activation reagents NHS and EDC to the prepared deionized water-dispersed nanoparticles at 100mmol / L and 200mmol / L respectively, and after standing in the dark for 30min, use 100KD The ultrafiltration tube was ultrafiltered at 6000rpm for 20min three times. Before each ultrafiltration, the volume of the system was fixed to 4ml with deionized water, so as to completely remove the excess NHS and EDC of the activated carboxyl group. Collect nanoparti...
Embodiment 2
[0035] BCEC cells were divided into 5×10 4 The concentration of cells per well was inoculated in the Transwell cell culture pool, and the transmembrane electrical resistance (TEER) of monolayer BCECs was measured by Millcell-ERS, and the TEER value was selected to be greater than 200 Ω cm 2的 cell pool for experiments. Add 1ml paclitaxel carrier solution to each well, totally four groups: Taxol, NP-PTX, PNP-PTX and PNP-PTX+200μg / ml peptide-22 (PTX concentration is 10μg / ml), in 1h, 2h, At 4h, 8h, 12h, and 24h, 300 μl of samples were taken from the receiving pool and supplemented with an equal amount of fresh DMEM. The PTX content in the samples at different time points was analyzed by liquid chromatography. The results showed that the targeted functional molecules helped the nanoparticles cross the BBB, while Pre-incubation of the short peptide occupies the binding site of low-density lipoprotein, which can inhibit the transmembrane transport of PNP-PTX.
Embodiment 3
[0037] Near-infrared dye DiR labeled nanoparticles, normal mice were given 10 μg / kg dose of tail vein for 8 hours, and then the heart was perfused with 4% paraformaldehyde, and the brain was taken out, and the distribution of different nanoparticles in the brain tissue was observed by small animal live imaging. It shows that the distribution of nanoparticles modified by targeting functional molecules in the brain is significantly better than that of ordinary nanoparticles, suggesting that targeting functional molecules help nanoparticles cross the BBB into the brain parenchyma.
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