首页> 外文期刊>Nuclear Medicine Communications >Systemic and local release of inflammatory cytokines regulates hepatobiliary excretion of 99mTc-mebrofenin.
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Systemic and local release of inflammatory cytokines regulates hepatobiliary excretion of 99mTc-mebrofenin.

机译:炎性细胞因子的系统性和局部释放可调节99mTc-Mebrofenin的肝胆排泄。

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OBJECTIVES: Imaging agents capable of providing cell compartment-specific information will facilitate studies of pathophysiological mechanisms, natural history of diseases, and therapeutic development. To demonstrate the effects of liver injury on the disposal of the organic anion mebrofenin, we performed animal studies. METHODS: Acute liver injury was induced in Fischer 344 rats with 0.25-1 ml/kg single doses of carbon tetrachloride followed by studies of animals over 4 weeks. The liver injury was analyzed by blood tests and histological grading. Additional rats were treated with lipopolysaccharide, interleukin-6 or tumor necrosis factor-alpha to activate inflammatory events. Hepatic clearance of Tc-mebrofenin was studied with dynamic imaging and fractional retention after 60 min of peak hepatic mebrofenin activity was determined. RESULTS: In healthy rats, only 24+/-2% of peak mebrofenin activity was retained in the liver after 60 min. By contrast, 24 h after carbon tetrachloride, virtually all mebrofenin activity was retained in the liver (P<0.001). Three weeks were required for mebrofenin excretion to become normal after carbon tetrachloride administration. In this situation, we found that Kupffer cell activity was increased. In addition, the abnormality in mebrofenin excretion was reproduced by lipopolysaccharide, which activates Kupffer cells. Moreover, mebrofenin excretion was highly sensitive to interleukin-6 and/or tumor necrosis factor-alpha, which help mediate the Kupffer cell response. CONCLUSION: Hepatobiliary excretion of mebrofenin was affected rapidly and over an extended period by inflammatory cytokines released after liver injury. The remarkable sensitivity of mebrofenin excretion to cytokines suggests that Tc-mebrofenin imaging will be helpful for assessing cytokine-mediated liver inflammation.
机译:目的:能够提供细胞室特异性信息的显像剂将促进病理生理机制,疾病自然史和治疗发展的研究。为了证明肝脏损伤对有机阴离子美洛芬宁处理的影响,我们进行了动物研究。方法:采用0.25-1 ml / kg单剂量四氯化碳在Fischer 344大鼠中诱发急性肝损伤,然后进行为期4周的动物研究。通过血液检查和组织学分级分析肝损伤。另外的大鼠用脂多糖,白介素-6或肿瘤坏死因子-α治疗以激活炎症事件。用动态成像技术研究了Tc-Mebrofenin的肝清除率,并测定了60分钟后的峰值肝保卫素活性。结果:在健康大鼠中,60分钟后肝脏中仅保留了24%+/- 2%的甲苯芬净峰值活性。相比之下,四氯化碳处理24小时后,实际上所有的mebrofenin活性都保留在肝脏中(P <0.001)。服用四氯化碳后,需要三周的时间才能使美罗芬的排泄恢复正常。在这种情况下,我们发现库普弗细胞活性增加。此外,通过激活库普弗细胞的脂多糖可重现出甲苯芬净排泄异常。此外,美洛芬素的排泄对白介素6和/或肿瘤坏死因子α高度敏感,这有助于介导Kupffer细胞反应。结论:肝损伤后释放的炎性细胞因子对美洛芬宁的肝胆排泄迅速且长期有影响。美洛芬净排泄对细胞因子的显着敏感性表明,Tc-美芬净成像对评估细胞因子介导的肝脏炎症有帮助。

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