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脂质体胞壁酰三肽磷脂酰乙醇胺(MTP-PE)可促进受辐照小鼠的造血恢复。

Liposomal muramyl tripeptide phosphatidylethanolamine (MTP-PE) promotes haemopoietic recovery in irradiated mouse.

作者信息

Fedorocko P

机构信息

Department of Cellular and Molecular Biology, Faculty of Sciences, P. J. Safárik University, Kosice, Slovak Republic.

出版信息

Int J Radiat Biol. 1994 Apr;65(4):465-75. doi: 10.1080/09553009414550541.

Abstract

Pretreatment of C57B1/6 mouse with the macrophage activator muramyl tripeptide phosphatidylethanolamine encapsulated in liposomes (MTP-PE/MLV) induced haemopoietic recovery in subsequently irradiated mouse. An optimal endoCFU-S survival was observed when 200 micrograms MTP-PE/MLV was administered i.p. 24 h before irradiation. MTP-PE/MLV did not affect the day 8 exogenous CFU-S survival in the bone marrow immediately after irradiation. However, 3, 6, 9 and 14 days after irradiation the number of day 8 CFU-S was almost 2 to 4-fold higher in the bone marrow of the MTP-PE/MLV injected mouse. Also, recovery of the GM-CFC pools in femoral bone marrow after irradiation proceeded at a faster rate in the MTP-PE/MLV-treated animal than in control groups. After a single i.p. injection of MTP-PE/MLV to the non-irradiated mouse, the number of CFU-S in bone marrow was not significantly different from controls, whereas the number of GM-CSC was significantly increased. In addition, the percentage of day 8 CFU-S and GM-CFC in S-phase of the cell cycle was significantly increased, as was colony-stimulating activity present in the serum of treated animals. Pretreatment with MTP-PE/MLV protected the C57Bl/6 mouse in a dose-dependent manner from the lethal effects of ionizing radiation. A single dose (100 or 200 micrograms) injected i.p. 24 h, or 100 micrograms MTP-PE/MLV injected i.v. 24 h before 9.5 Gy gamma-rays protected 47, 85 and 59% of C57B1/6 mouse, respectively. The dose reduction factor in the case when the MTP-PE/MLV (200 micrograms per mouse) was administered i.p. at that time was 1.17 (95% CL 1.13, 1.21). Combined administration of MTP-PE/MLV (24 h) and indomethacin (24 and 3 h) to mouse prior to irradiation exerted an additional radioprotective effect.

摘要

用包裹在脂质体中的巨噬细胞激活剂胞壁酰三肽磷脂酰乙醇胺(MTP - PE/MLV)对C57B1/6小鼠进行预处理,可使随后接受照射的小鼠造血功能恢复。在照射前24小时腹腔注射200微克MTP - PE/MLV时,观察到最佳的内源性脾集落形成单位(endoCFU - S)存活情况。MTP - PE/MLV对照射后即刻骨髓中第8天的外源性CFU - S存活没有影响。然而,照射后3、6、9和14天,注射MTP - PE/MLV小鼠骨髓中第8天CFU - S的数量几乎比对照组高2至4倍。此外,照射后,MTP - PE/MLV处理的动物股骨骨髓中粒细胞 - 巨噬细胞集落形成细胞(GM - CFC)池的恢复速度比对照组快。对未照射的小鼠单次腹腔注射MTP - PE/MLV后,骨髓中CFU - S的数量与对照组无显著差异,而粒细胞 - 巨噬细胞干细胞(GM - CSC)的数量显著增加。此外,细胞周期S期的第8天CFU - S和GM - CFC的百分比显著增加,处理动物血清中的集落刺激活性也增加。用MTP - PE/MLV预处理以剂量依赖的方式保护C57Bl/6小鼠免受电离辐射的致死效应。在9.5 Gy γ射线照射前24小时腹腔注射单剂量(100或200微克)或静脉注射100微克MTP - PE/MLV,分别保护了47%、85%和59%的C57B1/6小鼠。当时腹腔注射MTP - PE/MLV(每只小鼠200微克)的情况下,剂量降低因子为1.17(95%置信区间1.13,1.21)。在照射前对小鼠联合给予MTP - PE/MLV(24小时)和吲哚美辛(24小时和3小时)具有额外的辐射防护作用。

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