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Hepatic Immunosuppressive Effects of Systemically-Administered Novel Dextran-Methylprednisolone Prodrugs with Peptide Linkers in Rats

机译:大鼠肽接头的全身施用新型葡聚糖 - 甲基丙酮醇酮前药的肝免疫抑制作用

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摘要

The hepatic immunosuppressive activities of two novel dextran prodrugs of methylprednisolone (MP) containing one (DMP1) or five (DMP5) amino acids as linkers were studied in rats. At various times (0–2 weeks) after intravenous administration of single 5-mg/kg (MP equivalent) doses of each prodrug or MP succinate (MPS), livers were isolated and immunologically stimulated ex vivo with lipopolysaccharide. The concentrations of tumor necrosis factor (TNF)-α in the outlet perfusate were then quantitated to assess immune response. Additionally, the concentrations of DMP1, DMP5, and/or MP were measured in the liver. MPS, DMP5, or DMP1 injections caused a maximum of 48.9%, 63.5%, or 85.7% decrease in the TNF-α secretion into the perfusate, with the time above the 50% inhibitory effect being <5, <24, or 120 h, respectively. Additionally, the area under the effect-time curve for DMP1 was 11- or 4-fold higher than that after the administration of MPS or DMP5, respectively. Relatively high concentrations of DMP1 were present in the liver even at the last sampling time of two weeks. These data suggest that a single intravenous dose of DMP1 produces an intense and sustained immunosuppression in the liver for a relatively long time, which may be useful in liver transplantation.
机译:在大鼠中研究了两种新型的含有一个(DMP1)或五个(DMP5)氨基酸作为连接基的甲基强的松龙(MP)的右旋糖酐前药的肝免疫抑制活性。在静脉内以每种前药5 mg / kg(MP当量)剂量或MP琥珀酸酯(MPS)静脉给药后的不同时间(0–2周),分离肝脏并用脂多糖离体免疫刺激。然后对出口灌注液中肿瘤坏死因子(TNF)-α的浓度进行定量,以评估免疫反应。此外,还测量了肝脏中DMP1,DMP5和/或MP的浓度。注射MPS,DMP5或DMP1导致灌注液中TNF-α分泌最多减少48.9%,63.5%或85.7%,超过50%抑制作用的时间为<5,<24或120 h , 分别。此外,DMP1的作用时间曲线下面积分别比MPS或DMP5施用后高11倍或4倍。即使在两周的最后采样时间,肝脏中也存在相对较高浓度的DMP1。这些数据表明,单次静脉内给药的DMP1在相对较长的时间内会在肝脏中产生强烈而持续的免疫抑制作用,这可能在肝移植中有用。

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