Investigation of chitosan-g-PEG grafted nanoparticles as a half-life enhancer carrier for tissue plasminogen activator delivery

被引:2
作者
Khosravi, Arezoo [1 ]
Baharifar, Hadi [2 ]
Darvishi, Mohamad Hasan [3 ]
Karimi Zarchi, Ali Akbar [3 ]
机构
[1] Baqiyatallah Univ Med Sci, Atherosclerosis Res Ctr, Tehran, Iran
[2] Islamic Azad Univ, Sci & Res Branch, Dept Med Nanotechnol, Appl Biophoton Res Ctr, Tehran, Iran
[3] Baqiyatallah Univ Med Sci, Nanobiotechnol Res Ctr, Tehran, Iran
关键词
drug delivery systems; nanofabrication; drugs; nanomedicine; coagulation; biomedical materials; cellular biophysics; enzymes; biochemistry; toxicology; molecular biophysics; biological tissues; blood; nanoparticles; polymers; chitosan-g-PEG grafted nanoparticles; half-life enhancer carrier; tissue plasminogen activator delivery; tPA half-life; prolonged continuous infusion; enzyme dosage; polyethylene glycol; cytotoxicity; enzyme activity; encapsulated tPA; enzyme half-life; blood coagulation; time; 5; 0; min; PARTICLE-SIZE; IN-VITRO; POLY(ETHYLENE GLYCOL); VINCRISTINE SULFATE; CROSS-LINKING; CYTOTOXICITY; STREPTOKINASE; OPTIMIZATION; THROMBOLYSIS; ALBUMIN;
D O I
10.1049/iet-nbt.2019.0304
中图分类号
Q5 [生物化学];
学科分类号
071010 ; 081704 ;
摘要
Tissue plasminogen activator (tPA) a thrombolytic agent is commonly used for digesting the blood clot. tPA half-life is low (4-6 min) and its administration needs a prolonged continuous infusion. Improving tPA half-life could reduce enzyme dosage and enhance patient compliance. Nano-carries could be used as delivery systems for the protection of enzymes physically, enhancing half-life and increasing the stability of them. In this study, chitosan (CS) and polyethylene glycol (PEG) were used for the preparation of CS-g-PEG/tPA nanoparticles (NPs) via the ion gelation method. Particles' size and loading capacity were optimised by central composite design. Then, NPs cytotoxicity, release profile, enzyme activity and in vivo half-life and coagulation time were investigated. The results showed that NPs does not have significant cytotoxicity. Release study revealed that a burst effect happened in the first 5 min and resulted in releasing 30% of tPA. Loading tPA in NPs could decrease 25% of its activity but the half-life of it increases in comparison to free tPA in vivo. Also, blood coagulation time has significantly affected (p-value = 0.041) by encapsulated tPA in comparison to free tPA. So, CS-g-PEG/tPA could increase enzyme half-life during the time and could be used as a non-toxic candidate delivery system for tPA.
引用
收藏
页码:899 / 907
页数:9
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