肝实质细胞抑制细菌增殖作用及机制研究  

作　　者：马娓 舒俊傑 陈地友 王丽[1] 杨霞 高强国[1] MA Wei;SHU Junjie;CHEN Diyou;WANG Li;YANG Xia;GAO Qiangguo(Department of Cell Biology,College of Basic Medical Sciences,Army Medical University(Third Military Medical University),Chongqing,400038;Department of Wound Infection and Drug,Army Medical Center of PLA,Chongqing,400042,China;Department of Radiology,Army Medical Center of PLA,Chongqing,400042,China;Department of Military Traffic Injury Prevention and Treatment,Army Medical Center of PLA,Chongqing,400042,China)

机构地区：[1]陆军军医大学(第三军医大学)基础医学院细胞生物学教研室,重庆400038 [2]陆军特色医学中心野战外科研究部战伤感染与特需药品研究室,重庆400042 [3]陆军特色医学中心放射科,重庆400042 [4]陆军特色医学中心野战外科研究部军事交通伤防治研究室,重庆400042

出　　处：《陆军军医大学学报》2023年第21期2206-2213,共8页Journal of Army Medical University

基　　金：国家自然科学基金面上项目(81772717,82172134)。

摘　　要：目的探讨肝细胞通过直接吞噬和抗菌蛋白介导抑制细菌增殖的作用及其机制。方法利用正常小鼠FL83B肝细胞系建立大肠杆菌感染模型,以小鼠Kupffer细胞系为对照,观察肝细胞对大肠杆菌的增殖影响;建立细菌-细胞和(或)细胞上清共培养体系,通过Kupffer/FL83B细胞及其6、12、24 h的上清与大肠杆菌的共培养,检测大肠杆菌的致死情况,明确肝细胞直接抑菌效应;通过吞噬功能检测肝细胞的吞噬能力,qRT-PCR、Western blot检测相关基因的表达。结果将大肠杆菌与细胞共孵育,发现FL83B细胞与Kupffer细胞类似,可直接抑制大肠杆菌的增殖(P<0.05),且肝细胞自身保持高存活率;通过吞噬功能检测,明确了FL83B细胞可直接吞噬细菌颗粒;与对照组相比,感染后肝细胞内吞噬相关基因Fcgr1、Marco、Cdc42、RhoB mRNA上调,抗原递呈相关基因β2M mRNA上调,NF-κB、MAPK、STAT3通路活化,且介导抗菌作用的相关蛋白iNOS、NOX2、RhoB表达上调(P<0.05)。结论小鼠FL83B肝细胞可直接通过吞噬作用和抗菌相关蛋白介导抑制细菌增殖。Objective To explore the role and mechanism of hepatocytes in inhibiting bacterial proliferation by phagocytizing bacteria directly and mediating the expression of antibacterial proteins indirectly.Methods Cellular model of Escherichia coli(E.coli)infection was established in normal murine hepatocyte line FL83B and mouse Kupffer cells to determine the effects of the cells on the proliferation of bacteria.After the bacteria were co-cultured with Kupffer/FL83B cells and the 6-,12-,and 24-hour supernatants,respectively,the lethality of E.coli was determined for the direct bacteriostatic effect of the hepatocytes.The phagocytizing ability of FL83B cells were measured with phagocytosis reagent kit.qRT-PCR and Western blotting were employed to detect the expression of related molecules at mRNA and protein levels.Results When the hepatocyte were incubated with E.coli,FL83B cells,as Kupffer cells,could directly inhibit the proliferation of the bacteria(P<0.05)and maintained a high survival rate at same time.Phagocytic function test showed that FL83B cells could directly phagocytize bacterial particles.Compared with the FL83B cells without E.coli infection,the mRNA levels of phagocytosis-related genes Fcgr1,Marco,Cdc42,and RhoB were increased,that of antigen presentation related geneβ2M was also upregulated,the NF-κB,MAPK,and STAT3 signaling pathways were activated,and the protein levels of antibacterial-related proteins iNOS,NOX2,and RhoB were also enhanced in the cells after infection(all P<0.05).Conclusion Mouse FL83B hepatocytes possess the ability to inhibit bacteria through direct phagocytosis and indirect upregulation of antibacterial-related proteins.

关 键 词：肝细胞 细菌感染 吞噬作用 

分 类 号：R322.47[医药卫生—人体解剖和组织胚胎学] R329.28[医药卫生—基础医学] R378