BAOJi 1,2 , SUNJiu 3,4 , ZHOUYongjie 1 , WUQiong 1 , WANGYujia 1 , LILi 1 , JIANGXin 5 , MALang 5 , XIEMingjun 3,4 , SHIYujun 1 , BUHong 1,2
  • 1. Laboratory of Pathology, West China Hospital, Sichuan University, Chengdu 610041, China;
  • 2. Department of Pathology, West China Hospital, Sichuan University, Chengdu 610041, China;
  • 3. Department of General Surgery, The First People's Hospital of Yibin, Yibin 644000, China;
  • 4. Department of Clinical Medicine, Luzhou Medical College, Luzhou 646000, China;
  • 5. College of Polymer Science and Engineering, Sichuan University, Chengdu, 610065, China;
BUHong, Email: hongbu@scu.edu.cn
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In order to enhance the anticoagulant properties of decellularized biological materials as scaffolds for tissue engineering research via heparinized process, the decellularized porcine liver scaffolds were respectively immobilized with heparin through layer-by-layer self-assembly technique (LBL), multi-point attachment (MPA) or end-point attachment (EPA). The effects of heparinization and anticoagulant ability were tested. The results showed that the three different scaffolds had different contents of heparin. All the three kinds of heparinized scaffolds gained better performance of anticoagulant than that of the control scaffold. The thrombin time (TT), prothrombin time (PT) and activated partial thromboplastin time (APTT) of EPA scaffold group were longest in all the groups, and all the three times exceeded the measurement limit of the instrument. In addition, EPA scaffolds group showed the shortest prepared time, the slowest speed for heparin release and the longest recalcification time among all the groups. The decellularized biological materials for tissue engineering acquire the best effect of anticoagulant ability in vitro via EPA heparinized technique.

Citation: BAOJi, SUNJiu, ZHOUYongjie, WUQiong, WANGYujia, LILi, JIANGXin, MALang, XIEMingjun, SHIYujun, BUHong. Anticoagulant Ability and Heparinization of Decellularized Biomaterial Scaffolds. Journal of Biomedical Engineering, 2015, 32(3): 594-598. doi: 10.7507/1001-5515.20150108 Copy

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