Preparation method and antitumor enhancement application of dual-targeting delivery chemotherapeutic drug nanosystem
A chemotherapeutic drug and dual-targeting technology, applied in the field of medicine, can solve the problems of fast metabolism in the body, short validity period, and large side effects, and achieve the effect of enhancing the enrichment ability.
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Embodiment 1
[0049] Embodiment 1: the preparation method of targeting nanogel
[0050] 1. Dissolve 0.84g of 25kPEI into 20ml of Milli-Qwater, and adjust the pH to 7 with hydrochloric acid;
[0051] 2. Accurately weigh 0.4746g of NIPAM crystals and 13.146mg of BIS crystals into the above solution;
[0052] 3. Transfer the above mixture to a 50ml ground-necked flask, and add 10ml Milli-Qwater;
[0053] 4. Immerse the bottom of the flask into a constant temperature magnetic stirrer containing silicone oil, and heat the silicone oil to 50°C while stirring;
[0054] 5. Inject high-purity nitrogen into the system and stir for 30 minutes;
[0055] After 6.30 minutes, heat the silicone oil to 80°C, and add 250 μl of 0.01M tert-butyl hydroperoxide (TBHP) to the system;
[0056] 7. At 80°C, maintain a nitrogen atmosphere and stir for another 2 hours;
[0057] After 8.2 hours, stop N 2 , pass into O 2 , stirred overnight;
[0058] 9. Collect the prepared microgel, purify the microgel with a fl...
Embodiment 2
[0061] Example 2: Identification of Targeted Nanogel Components
[0062] 1. Freeze-dry the microgel after dialysis (25KPEI content is 60%);
[0063] 2. Take an appropriate amount of microgel powder and dissolve it in D 2 O, 1 H-NMR test microgel components; NIPAM contains amide bonds (δ, 5.0-8.0), PEI contains amines (δ, 0.5-5.0), microgels obtained from synthesis 1 In the H-NMR spectrum, it can be found that there are proton absorption peaks of amide bonds and amine proton absorption peaks of PEI. It can be seen that we have successfully grafted PEI and PNIPAM to form nanogel copolymers.
Embodiment 3
[0064] Embodiment 3: the test of target nano microgel particle size
[0065] 1. Dilute the dialyzed microgel with an appropriate amount of Mi1li-Qwater;
[0066] 2. Take 1ml of microgel solution, after confirming that no air bubbles are generated in the measurement container, add it into the sample pool, and repeat the measurement 3 times for each sample. The measurement conditions are: 170 scattering angle, 25°C.
[0067] Experimental results such as figure 2 As shown, with the increase of the PEI content in the microgel carrier, from 0% to 70%, its particle size gradually decreased from 493±55nm to 255.2±30nm, this is because with the increase of the PEI content in the carrier, the microgel The closer the crossover of the gel, the more positive charge the microgel carries gradually, which is conducive to the stability of the system and the increase of the drug loading capacity.
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