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Merck
CN
  • Polymeric nano-shielded islets with heparin-polyethylene glycol in a non-human primate model.

Polymeric nano-shielded islets with heparin-polyethylene glycol in a non-human primate model.

Biomaterials (2018-04-27)
Hyojun Park, Muhammad R Haque, Jae Berm Park, Kyo Won Lee, Sanghoon Lee, Yeongbeen Kwon, Han Sin Lee, Geun-Soo Kim, Du Yeon Shin, Sang-Man Jin, Jae Hyeon Kim, Hee Jung Kang, Youngro Byun, Sung Joo Kim
摘要

Intraportal pancreatic islet transplantation incurs huge cell losses during its early stages due to instant blood-mediated inflammatory reactions (IBMIRs), which may also drive regulation of the adaptive immune system. Therefore, a method that evades IBMIR will improve clinical islet transplantation. We used a layer-by-layer approach to shield non-human primate (NHP) islets with polyethylene glycol (nano-shielded islets, NSIs) and polyethylene glycol plus heparin (heparin nano-shielded islets; HNSIs). Islets ranging from 10,000 to 20,000 IEQ/kg body weight were transplanted into 19 cynomolgus monkeys (n = 4, control; n = 5, NSI; and n = 10, HNSI). The mean C-peptide positive graft survival times were 68.5, 64 and 108 days for the control, NSI and HNSI groups, respectively (P = 0.012). HNSI also reduced the factors responsible for IBMIR in vitro. Based on these data, HNSIs in conjunction with clinically established immunosuppressive drug regimens will result in superior outcomes compared to those achieved with the current protocol for clinical islet transplantation.

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Sigma-Aldrich
3,4-二羟苯基丙酸, 98%
Sigma-Aldrich
头孢唑啉 钠盐, 89.1-110.1%
Sigma-Aldrich
3-氨基丙硫醇盐酸盐 盐酸盐, technical grade
Sigma-Aldrich
3-马来酰亚胺基苯甲酸 N -羟基琥珀酰亚胺酯, crystalline