target drug delivery system
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2021 ◽  
Vol 19 (1) ◽  
Author(s):  
Yan Lin ◽  
Yujie Wan ◽  
Xingjie Du ◽  
Jian Li ◽  
Jun Wei ◽  
...  

Abstract Background Spinal Cord injury (SCI) is a kind of severe traumatic disease. The inflammatory response is a significant feature after SCI. Tetramethylpyrazine (TMP), a perennial herb of umbelliferae, is an alkaloid extracted from ligustici. TMP can inhibit the production of nitric oxide and reduce the inflammatory response in peripheral tissues. It can be seen that the therapeutic effect of TMP on SCI is worthy of affirmation. TMP has defects such as short half-life and poor water-solubility. In addition, the commonly used dosage forms of TMP include tablets, dropping pills, injections, etc., and its tissue and organ targeting is still a difficult problem to solve. To improve the solubility and targeting of TMP, here, we developed a nanotechnology-based drug delivery system, TMP-loaded nanoparticles modified with HIV trans-activator of transcription (TAT-TMP-NPs). Results The nanoparticles prepared in this study has integrated structure. The hemolysis rate of each group is less than 5%, indicating that the target drug delivery system has good safety. The results of in vivo pharmacokinetic studies show that TAT-TMP-NPs improves the bioavailability of TMP. The quantitative results of drug distribution in vivo show that TAT-TMP-NPs is more distributed in spinal cord tissue and had higher tissue targeting ability compared with other treatment groups. Conclusions The target drug delivery system can overcome the defect of low solubility of TMP, achieve the targeting ability, and show the further clinical application prospect.


2020 ◽  
Vol 35 (1) ◽  
pp. 15-27 ◽  
Author(s):  
Taicheng Lu ◽  
Zhenzhen Nong ◽  
Liying Wei ◽  
Mei Wei ◽  
Guo Li ◽  
...  

In this study, a transferrin/folic acid double-targeting graphene oxide drug delivery system loaded with doxorubicin was designed. Graphene oxide was prepared by ultrasound improved Hummers method and was modified with Pluronic F68, folic acid, and transferrin to decrease its toxicity and to allow dual-targeting. The results show that the double target drug delivery system (TFGP*DOX) has good and controllable drug delivery performance with no toxicity. Moreover, TFGP*DOX has a better inhibitory effect on SMMC-7721 cells than does a single target drug delivery system (FGP*DOX). The results of drug release analysis and cell inhibition studies showed that TFGP*DOX has a good sustained release function that can reduce the drug release rate in blood circulation over time and improve the local drug concentration in or near a targeted tumor. Therefore, the drug loading system (TFGP*DOX) has potential application value in the treatment of hepatocellular carcinoma.


2009 ◽  
Vol 13 (12) ◽  
pp. 37-50

CSIRO and Circadian Collaborate in Oncology R&D. Successful Trials in Bone Marrow Regeneration Using Cord Blood. Pfizer China and BMP Sunstone Venture into Women's Healthcare Product. Novartis Acquires Zhejiang Tianyuan to Expand Human Vaccines Presence in China. Carbon Nanotechnology for Target Drug Delivery System Launched in India. Cipla Launches Antiflu to Combat Influenza. Tokyo CRO and Ecron Acunova in Alliance to Strengthen Global Network. World's First Oral Jelly for Alzheimer's Disease Treatment. Leading Japanese and Swedish Biotech Firms Seal Antibody Deal. Caduet® Combination Tablets Launched in Japan. Spectrum Teams Up with Korea's Handok on Apaziquone. Biologics, CEVEC Sign Agreement for Using Human CAP Technology. Chaperone Technologies and MerLion Pharmaceuticals in Antimicrobials Collaboration. Quintiles Expands Asia-Pacific Headquarters in Singapore. NCKU and ScinoPharm Taiwan Establish University-Industry Cooperation.


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