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Ciprofloxacin Modulates Cytokine/Chemokine Profile in Serum Improves Bone Marrow Repopulation and Limits Apoptosis and Autophagy in Ileum after Whole Body Ionizing Irradiation Combined with Skin-Wound Trauma

机译:环丙沙星调节细胞因子/趋化因子谱血清改善骨髓再增殖和全身电离辐射组合后该限制细胞凋亡和自噬在回肠皮肤伤口创伤

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摘要

Radiation combined injury (CI) is a radiation injury (RI) combined with other types of injury, which generally leads to greater mortality than RI alone. A spectrum of specific, time-dependent pathophysiological changes is associated with CI. Of these changes, the massive release of pro-inflammatory cytokines, severe hematopoietic and gastrointestinal losses and bacterial sepsis are important treatment targets to improve survival. Ciprofloxacin (CIP) is known to have immunomodulatory effect besides the antimicrobial activity. The present study reports that CIP ameliorated pathophysiological changes unique to CI that later led to major mortality. B6D2F1/J mice received CI on day 0, by RI followed by wound trauma, and were treated with CIP (90 mg/kg p.o., q.d. within 2 h after CI through day 10). At day 10, CIP treatment not only significantly reduced pro-inflammatory cytokine and chemokine concentrations, including interleukin-6 (IL-6) and KC (i.e., IL-8 in human), but it also enhanced IL-3 production compared to vehicle-treated controls. Mice treated with CIP displayed a greater repopulation of bone marrow cells. CIP also limited CI-induced apoptosis and autophagy in ileal villi, systemic bacterial infection, and IgA production. CIP treatment led to LD0/10 compared to LD20/10 for vehicle-treated group after CI. Given the multiple beneficial activities of CIP shown in our experiments, CIP may prove to be a useful therapeutic drug for CI.
机译:放射综合损伤(CI)是放射损伤(RI)与其他类型的损伤相结合,通常比单独的RI导致更高的死亡率。一系列特定的,时间依赖性的病理生理变化与CI相关。在这些变化中,促炎性细胞因子的大量释放,严重的造血和胃肠道损失以及细菌性败血症是提高生存率的重要治疗目标。已知环丙沙星(CIP)除具有抗菌活性外,还具有免疫调节作用。本研究报告指出,CIP改善了CI独特的病理生理变化,后来导致重大死亡率。 B6D2F1 / J小鼠在第0天接受CI,随后是RI,然后是伤口创伤,并接受CIP治疗(90 mg / kg p.o.,每天一次,CI后2小时内,第10天)。在第10天,CIP治疗不仅显着降低了促炎性细胞因子和趋化因子的浓度,包括白介素6(IL-6)和KC(即人中的IL-8),而且与媒介物相比还提高了IL-3的产生。处理的对照。 CIP处理的小鼠显示出更多的骨髓细胞种群。 CIP还限制了CI引起的回肠绒毛,系统性细菌感染和IgA产生中的凋亡和自噬。 CI后,CIP处理导致载体治疗组的LD0 / 10与LD20 / 10相比。考虑到我们实验中显示的CIP的多种有益活性,CIP可能被证明是CI的有用治疗药物。

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