免疫系统在奈韦拉平诱导大鼠亚临床肝损伤模型中的作用。

Zanelle Bekker, Andrew Walubo, Jan B du Plessis
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引用次数: 12

摘要

本研究通过观察奈韦拉平(NVP-)诱导的亚临床肝损伤大鼠模型初始阶段免疫参数的变化,探讨免疫系统在NVP-诱导的亚临床肝损伤中的作用。急性期,两组大鼠各10只,分别腹腔注射细菌脂多糖(LPS)或生理盐水(S),再口服NVP,分别于6、24 h处死5只。在慢慢性阶段,两组15只大鼠每天接受NVP治疗,在第7、14和21天,每组5只大鼠分别给予LPS或S,然后再给予当天的NVP剂量,24小时后处死。NVP导致肝损伤长达7天,并在21天内逐渐增加IL-2和IFN-γ水平和淋巴细胞计数。nvp诱导的肝损伤表现为细胞凋亡和变性改变,LPS诱导的肝损伤表现为细胞肿胀、白细胞淤积和门静脉炎症。NVP和LPS联合使用可减轻NVP引起的肝损伤。综上所述,免疫系统参与了NVP的毒性作用,LPS的作用可能为开发抗NVP肝毒性的治疗策略提供线索。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The role of the immune system in nevirapine-induced subclinical liver injury of a rat model.

The role of the immune system in nevirapine-induced subclinical liver injury of a rat model.

The role of the immune system in nevirapine-induced subclinical liver injury of a rat model.

The role of the immune system in nevirapine-induced subclinical liver injury of a rat model.

In this study, the role of the immune system in nevirapine- (NVP-) induced subclinical liver injury was investigated by observing for changes of some immune parameters during the initial stages of NVP-induced hepatotoxicity in a rat model. In the acute phase, two test-groups of 10 Sprague-Dawley rats each were administered with bacterial lipopolysaccharide (LPS) or saline (S) intraperitoneally, followed by oral NVP, after which 5 rats from each group were sacrificed at 6 and 24 hours. For the chronic phase, two groups of 15 rats each received daily NVP, and on days 7, 14, and 21, five rats from each group were administered with either LPS or S, followed by that day's NVP dose, and were sacrificed 24 hours later. NVP caused liver injury up to seven days and progressively increased IL-2 and IFN-γ levels and lymphocyte count over the 21 days. NVP-induced liver injury was characterized by apoptosis and degeneration changes, while, for LPS, it was cell swelling, leukostasis, and portal inflammation. Coadministration of NVP and LPS attenuated NVP-induced liver injury. In conclusion, the immune system is involved in NVP toxicity, and the LPS effects may lay the clue to development of therapeutic strategies against NVP-induced hepatotoxicity.

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