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首页> 外文期刊>World Journal of Gastroenterology >Influence of Kupffer cells on hepatic signal transduction as demonstrated by second messengers and nuclear transcription factors
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Influence of Kupffer cells on hepatic signal transduction as demonstrated by second messengers and nuclear transcription factors

机译:第二信使和核转录因子证明库普弗细胞对肝信号转导的影响

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AIM: To understand the influence of Kupffer cell (KC) on signal transduction pathways in the liver. METHODS: To decrease selectively the number and function of KC, Kunming mice were ip injected with a single dose of gadolinium chloride (GdCl_3, 20 mg-kg~(-1)), the time-effect relationship assessment was performed after 1 d, 3 d and 6 d. sALT, sGST, liver glycogen content, phagocytic index, and expression of CD68 were assessed as the indexes of hepatotoxicity and functions of KC respectively, and morphology of KC was observed with transmission electron microscopy. Furthermore, cAMP, PGE_2 level, nitric oxide(NO) content, and mRNA expression of NFkappaBp65, Erk1, STAT1 were examined. RESULTS: GdCl_3 could selectively cause apoptosis of KC and obvious reduction of KC's activity, but no hepatotoxicity was observed. One day after KC blockade, NO, PGE_2, cAMP contents in the liver were reduced 21.0%, 6.94-fold, 8.3%, respectively, and mRNA expression of NFkappaBp65 was decreased 3.0-fold. The change tendency of NO, PGE_2, and cAMP contents and mRNA expression of NFkappaBp65 were concomitant with recovery of the functions of KC. The contents of NO, PEG2, cAMP were increased when the functions of KC was recovered. However, all of the changes could not return to the normal level except NO content after 6 d Gdcl_3 treatment. No obvious changes were found in STAT1 and Erk1 mRNA expression in the present study. CONCLUSION: Hepatic NO, PGE2, cAMP level and mRNA expression of NFkappaBp65 are closely related with the status of KC. It suggests that KC may play an important role in the cell to cell signal transduction in the liver.
机译:目的:了解库普弗细胞(KC)对肝脏信号转导通路的影响。方法:为选择性降低KC的数量和功能,昆明小鼠腹腔注射单剂量氯化g(GdCl_3,20 mg-kg〜(-1)),在1 d后进行时效关系评估, 3天和6天。分别以sALT,sGST,肝糖原含量,吞噬指数和CD68的表达作为肝毒性指标和KC功能,并用透射电镜观察KC的形态。此外,还检测了cAMP,PGE_2水平,一氧化氮(NO)含量以及NFkappaBp65,Erk1,STAT1的mRNA表达。结果:GdCl_3可以选择性地引起KC凋亡,并明显降低KC活性,但未观察到肝毒性。 KC阻断后一天,肝脏中的NO,PGE_2和cAMP含量分别降低了21.0%,6.94倍和8.3%,NFkappaBp65的mRNA表达降低了3.0倍。 NO,PGE_2,cAMP含量和NFkappaBp65 mRNA表达的变化趋势与KC功能的恢复有关。恢复KC功能后,NO,PEG2,cAMP的含量增加。但是,除6 d Gdcl_3处理后的NO含量外,所有变化都无法恢复到正常水平。在本研究中,STAT1和Erk1 mRNA表达未发现明显变化。结论:NFkappaBp65的肝NO,PGE2,cAMP水平和mRNA表达与KC状态密切相关。这表明KC可能在肝细胞间信号转导中起重要作用。

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