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Protected graft copolymer-formulated fibroblast growth factors mitigate the lethality of partial body irradiation injury

机译:受保护的接枝共聚物配制的成纤维细胞生长因子可减轻部分身体照射损伤的致死性

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摘要

We evaluated the mitigating effects of fibroblast growth factor 4 and 7 (FGF4 and FGF7, respectively) in comparison with long acting protected graft copolymer (PGC)-formulated FGF4 and 7 (PF4 and PF7, respectively) administered to C57BL/6J mice a day after exposure to LD50/30 (15.7 Gy) partial body irradiation (PBI) which targeted the gastrointestinal (GI) system. The PGC that we developed increased the bioavailability of FGF4 and FGF7 by 5- and 250-fold compared to without PGC, respectively, and also sustained a 24 hr presence in the blood after a single subcutaneous administration. The dose levels tested for mitigating effects on radiation injury were 3 mg/kg for the PF4 and PF7 and 1.5 mg each for their combination (PF4/7). Amifostine administered prior to PBI was used as a positive control. The PF4, PF7, or PF4/7 mitigated the radiation lethality in mice. The mitigating effect of PF4 and PF7 was similar to the positive control and PF7 was better than other mitigators tested. The plasma citrulline levels and hematology parameters were early markers of recovery and survival. GI permeability function appeared to be a late or full recovery indicator. The villus length and crypt number correlated with plasma citrulline level, indicating that it can act as a surrogate marker for these histology evaluations. The IL-18 concentrations in jejunum as early as day 4 and TPO levels in colon on day 10 following PBI showed statistically significant changes in irradiated versus non-irradiated mice which makes them potential biomarkers of radiation exposure. Other colon and jejunum cytokine levels are potentially useful but require larger numbers of samples than in the present study before their full utility can be realized.
机译:与每天向C57BL / 6J小鼠给药的长效受保护的接枝共聚物(PGC)配制的FGF4和7(分别为PF4和PF7)相比,我们评估了成纤维细胞生长因子4和7(分别为FGF4和FGF7)的缓解效果。在暴露于LD50 / 30(15.7 Gy)的局部胃肠道(PBI)之后,该辐射针对胃肠道(GI)系统。与不使用PGC时相比,我们开发的PGC分别将FGF4和FGF7的生物利用度提高了5倍和250倍,并且在单次皮下给药后在血液中也持续存在24小时。 PF4和PF7所测试的减轻辐射损伤的剂量水平为3 mg / kg,其组合(PF4 / 7)各自为1.5 mg。在PBI之前使用氨磷汀作为阳性对照。 PF4,PF7或PF4 / 7减轻了小鼠的辐射致死性。 PF4和PF7的缓解效果与阳性对照相似,并且PF7优于其他测试的缓解剂。血浆瓜氨酸水平和血液学参数是恢复和存活的早期标志。胃肠道通透性功能似乎是晚期或完全恢复的指标。绒毛长度和隐窝数目与血浆瓜氨酸水平相关,表明它可以作为这些组织学评估的替代标记。 PBI后第4天,空肠中的IL-18浓度和第10天结肠中的TPO水平在辐照小鼠和未辐照小鼠中显示出统计学上的显着变化,这使其成为潜在的辐射暴露生物标志物。其他结肠和空肠细胞因子水平可能是有用的,但在实现其全部效用之前,需要比本研究更多的样品。

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