Thrombospondin-1 expression correlates with angiogenesis in experimental cirrhosis

AIM:To investigate the significance of Thrombospondin-1 (TSP-1) expression and its relationship with angiogenesis during experimental fibrosis. METHODS:Cirrhosis was induced in male Wistar rats by intraperitoneal administration of diethyl nitrosamine (DEN). The serial sections from liver tissues were stained with anti-CD34 and anti-TSP-1 antibodies before being quantitated by light microscopy. RESULTS:Our results showed that of TSP-1 expression gradually increases according to the severity of fibrosis (GroupⅠvs group Ⅱ, Group Ⅲ and Group Ⅳ;Group Ⅱ vs group Ⅲ and group Ⅳ;group Ⅲ vs group Ⅳ, P < 0.05). Moreover, TSP-1 expression was found to be correlated with angiogenesis (P < 0.05). CONCLUSION:The correlative evidence of the link between TSP-1 and fibrosis or angiogenesis provided by this study suggests that besides its role as a strong promoter of transforming growth factor-β1 (TGF-β1), TSP-1 might have an additional role in liver fibrogenesis by stimulating angiogenesis and this protein could be a potential target to prevent fibrogenesis in chronic inflammatory diseases of the liver.

Modifi cation of sleep architecture in an animal model of experimental cirrhosis

AIM： To analyze the polygraphic sleep patterns during cirrhosis progression in a rat model by repeated CCh administration. METHODS： Male Wistar rats received three weekly injections of CCl4 for 11 wk, and were analyzed before and during the induction of cirrhosis. Rats were im- planted with electrodes to record their sleep patterns. Polygraph recordings were made weekly over 11 wk for 8 h, during the light period. After a basal recording, rats received three weekly injections of CCl4. Histological confirmation of cirrhosis was performed after 11 wk. RESULTS： The results showed a progressive decrease in total wake time that reached statistical significance from the second week of treatment. In addition, there was an increase in total time of slow wave sleep （SWS）Ⅱ and rapid eye movement sleep （REM sleep） in most of the 11 wk. SWS I showed no significant variations. During the final weeks, a significant increase in REM sleep frequency was also observed. Histological analyses of the livers showed unequivocal signs of cirrhosis. CONCLUSION： These data suggest that hepatic failure produced by CCh administration is capable of modifying the sleep pattern even after only a few doses.

DYNAMIC CHANGES OF ITO CELLS IN EXPERIMENTAL LIVER CIRRHOSIS OF RAT

That Ho cells in rat liver express desmin was confirmed by immunohistochemical technique. Consequently, changes of desmin-positive cells, lysozyme-positive cells and fibronectin were further studied in experimental cirrhosis of rat. It was found that desmln- positive cells, with the transitional feature between Ito cells and myofibroblasts or fibrobiasts under electron microscope, increased in number and expression of desmin in the necrotic areas as well as in the cellular fibrous septa, but decreased in number in the fibrous septa except those areas closed to the edges of the septa. These results suggested that Ito cells, myofibroblasts and fibroblasts might belong to the same cellular system and play an important role in the pathogenesis of cirrhosis. Meanwhile, it was also noted that changes of both fibronectin and lysozymepositive cells were correlated with those of desmin-positive cells. These provide evidence in vivo that flbronectin and Kupffer cells might exert certain effects on the migration and proliferation of Ito cells in liver cirrhosis.

Immunohistochemical study on expression of epidermal growth factor receptor at hepatocyte nuclei in experimental rat liver cirrhosis

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Regulating effect of Chinese herbal medicine on the peritoneal lymphatic stomata in enhancing ascites absorption of experimental hepatofibrotic mice

AIM: To observe the regulatory effect of Chinese herbal medicine on peritoneal lymphatic stomata and its significance in treating ascites in liver fibrosis model mice. METHODS: Two Chinese herbal composite prescriptions were used separately to treat the carbon tetrachloride-induced mouse model of liver fibrosis. The histo-pathologic changes of the liver sections (HE and VG stainings) were observed. The peritoneal lymphatic stomata was detected by scanning electron microscopy and computer image processing. The changes of urinary volume and sodium ion concentration were measured. RESULTS: In the model group, lots of fibrous tissue formed in liver and extended into the hepatic lobules to separate them incompletely. In the treated and prevention groups, the histo-pathologic changes of liver was rather milder, only showed much less fibrous tissue proliferation in the hepatic lobules. The peritoneal lymphatic stomata enlarged with increased density in the experimental groups (diameter: PA, 3.07 +/- 0.69 microm; PB, 2.82 +/- 0.37 microm; TA, 3.25 +/- 0.82 microm and TB, 2.82 +/- 0.56 microm; density: PA, 7.11 +/- 1.90 stomata.1000 microm(-2); PB, 8.76 +/- 1.45 stomata.1000 microm(-2); TA, 6.55 +/- 1.44 stomata.1000 microm(-2)and TB, 8.76+/-1.79 stomata.1000 microm(-2)), as compared with the model group (diameter: 2.00+/-0.52 microm density: 4.45+/-1.05 stomata.1000 microm(-2)). After treatment, the urinary volume and sodium ion excretion increased in the experimental groups (PA, 231.28+/-41.09 mmol.L(-1); PB, 171.69 +/- 27.48 mmol.L(-1) and TA, 231.44 +/- 34.12 mmol.L(-1)), which were significantly different with those in the model group (129.33 +/- 36.75 mmol.L(-1)). CONCLUSION: Chinese herbal medicine has marked effects in alleviating liver fibrosis, regulating peritoneal lymphatic stomata, improving the drainage of ascites from peritoneal cavity and causing increase of urinary volume and sodium ion excretion to reduce the water and sodium retention, and thus have favorable therapeutic effect in treating ascites.

Bone disorders in experimentally induced liver disease in growing rats

AIM： To investigate the change of bone parameters in a new model of experimentally induced liver cirrhosis and hepatocellular carcinoma （HCC） in growing rats. METHODS： Fischer-344 rats （n = 55） were used. Carbon tetrachloride （CCh）, phenobarbital （PB）, and a single diethylnitrosamine （DEN） injection were used. Animals were killed at wk 8 and 16. Bone mineral content, femoral length, cortical index （quotient of cortical thickness and whole diameter） and ultimate bending load （Fmax） of the femora were determined. The results in animals treated with DEN＋PB＋CCh （DPC, n = 21） were com- pared to those in untreated animals （UNT, n = 14） and in control group treated only with DEN＋PB （DP, n = 20）. RESULTS： Fatty liver and cirrhosis developed in each DPC-treated rat at wk 8 and HCC was presented at wk 16. No skeletal changes were found in this group at wk 8, but each parameter was lower （P〈0.05 for each） at wk 16 in comparison to the control group. Neither fatty liver nor cirrhosis was observed in DP-treated animals at any time point. Femoral length and Fmax values were higher （P〈0.05 for both） in DP-treated animals at wk 8 compared to the UNT controls. However, no difference was found at wk 16. CONCLUSION： Experimental liver cirrhosis and HCC are accompanied with inhibited skeletal growth, reduced bone mass, and decreased mechanical resistance in growing rats. Our results are in concordance withthe data of other studies using different animal models. A novel finding is the transiently accelerated skeletal growth and bone strength after a 8-wk long phenobarbital treatment following diethylnitrosamine injection.

马齿苋多糖抗CCl4诱导的小鼠慢性肝纤维化作用

目的:研究马齿苋多糖(Purslane polysaccharide,POP)对小鼠慢性肝纤维化的逆转作用。方法:采用四氯化碳(CCl4)诱导的小鼠肝纤维化模型,分别灌胃给予不同剂量的POP(25、50、100 mg·kg^(-1))、2.5 mg·kg^(-1)的联苯双酯或等体积的生理盐水治疗6周。HE染色观察肝组织形态,电镜观察肝细胞结构变化,定量PCR(qPCR)方法检测肝组织中胶原蛋白(Collagen)Ⅰ和Ⅲ、α-平滑肌动蛋白(Alpha smooth muscle actin,α-SMA)、转化生长因子β1(Transforming growth factor,TGF-β1)、Smad4的mRNA表达,ELISA方法检测透明质酸(Hyaluronic acid,HA)、层黏连蛋LN(Laminin,LN)和Ⅲ型前胶原-N(Procollagen typeⅢ-N,PⅢNP)等肝纤维化相关蛋白含量,Western blot方法检测α-SMA蛋白表达。结果:(1)模型组小鼠表现为肝组织脂肪变性,空泡,脉管区炎性细胞浸润,肝细胞变性坏死,纤维增生;不同剂量POP组肝组织炎症浸润不同程度改善,肝索排列规律;(2)模型组肝细胞结构不清,细胞核增大,常染色质数量异常增加,线粒体和内质网等细胞器代偿性增多,脊增多或断裂,有少许空泡;与模型组相比,POP给药组和联苯双酯组上述状态减轻;(3)模型组α-SMA、TGF-β1、Smad4、CollagenⅢ的mRNA表达增高,POP治疗组以上基因表达呈剂量依赖性下降;(4)模型组LN、HA、PⅢNP和α-SMA含量升高,POP治疗后以上相关蛋白随剂量表达下降。结论:POP可缓解CCl4诱导的小鼠肝纤维化,其机制可能与POP抑制TGF-β1/Smad信号通路,进而下调胶原蛋白的表达有关。

人脐带间充质干细胞经不同移植途径治疗肝硬化大鼠模型的效果比较

目的探讨人脐带间充质干细胞(hUC-MSC)制剂(冷冻细胞制剂和新鲜细胞制剂)通过两种给药途径(门静脉/尾静脉)移植对肝硬化模型大鼠的治疗效果。方法70只SPF级健康雄性SD大鼠随机分为正常组(n=13,予以普通自来水及普通鼠粮喂养)和肝硬化模型组(n=57,给予CCl4/橄榄油溶液混合液,皮下多点注射造模)。第8周观察两组大鼠的生长状况,取正常组及肝硬化模型组小鼠各3只行组织病理学检查,明确肝硬化形成。选取50只肝硬化模型组大鼠按随机数字表法分为模型组、门静脉(新鲜细胞制剂)组、门静脉(冷冻细胞制剂)组、尾静脉(新鲜细胞制剂)组、尾静脉(冷冻细胞制剂)组,每组10只。分别取新鲜或冷冻hUC-MSC制剂通过门静脉或尾静脉途径移植。给药4周后,比较各组大鼠肝功能指标、肝纤维化程度变化。计量资料两组间比较采用成组t检验;多组间比较采用单因素方差分析,进一步两两比较采用LSD-t检验。结果造模第8周时,肝硬化模型组大鼠肝脏形成多个大小不等的假小叶,符合肝硬化诊断标准,ALT、AST、TBil、ALP水平相较于正常组均明显升高(P值均<0.001),肝硬化大鼠造模成功。第12周时5组大鼠ALT、AST、TBil、ALP水平比较差异均有统计学意义(F值分别为232.00、177.10、112.30、121.70,P值均<0.001)。进一步两两比较结果显示,模型组ALT、AST、TBil、ALP水平均显著高于正常组(P值均<0.01);门静脉(新鲜细胞制剂)组、门静脉(冷冻细胞制剂)组、尾静脉(新鲜细胞制剂)组、尾静脉(冷冻细胞制剂)组ALT、AST、TBil、ALP水平均显著低于模型组(P值均<0.01)。结论hUC-MSC移植4周可改善肝硬化模型大鼠肝功能和肝纤维化程度,细胞制剂的不同、给药途径的不同对治疗结果无明显影响。

益肝煎剂对实验性肝纤维化大鼠Ⅰ,Ⅲ型胶原蛋白表达的影响

目的探讨益肝煎剂对实验性肝纤维化大鼠肝脏Ⅰ、Ⅲ型胶原蛋白表达的影响。方法采用400 mL·L^(-1)四氯化碳(CCl_4)sc制备大鼠实验性肝纤维化模型,将80只(雌雄各半)Wistar大鼠随机分成正常对照组(A组)、模型对照组(B组)、秋水仙碱组(C组)和益肝煎剂组(D组)各20只,后两组于造模的同时开始给药,观察10wk。采用苦味酸-天狼星红(Picric acid-Sirius red)染色显示Ⅰ,Ⅲ型胶原,偏振光显微镜下区分Ⅰ,Ⅲ型胶原。用半定量评分方法判断细胞变性程度和纤维化程度。结果益肝煎剂组大鼠肝组织的脂肪变性程度较模型组明显减轻,脂肪变性积分分别为2.00±1.36和3.17±0.75(P<0.01);Ⅰ,Ⅲ型胶原蛋白含量明显少于模型组,纤维化程度积分分别为1.32±0.57和2.33±0.82(P<0.01)。结论益肝煎剂对大鼠实验性肝纤维化的形成有明显抑制作用。

虫草菌丝提取物对DMN诱导肝纤维化大鼠肝窦内皮细胞通透性影响

目的：研究二甲基亚硝胺(DMN)诱导大鼠肝纤维化模型肝窦内皮细胞(SECs)通透性变化模式,以及虫草菌丝提取物(CME)对SECs通透性的影响,以阐明其抗肝纤维化的作用机制。方法：采用DMN 10μg·kg^(-1)腹腔注射,每周3次,连续4wk的方法制作大鼠肝纤维化模型。按10mg·kg^(-1)·d^(-1)剂量给予CME干预和治疗模型大鼠,qd,连续2wk和4wk。透射电镜观察肝组织超微结构。免疫组织化学染色法观察肝窦壁CD31和小窝蛋白1(Car-1)表达。结果：正常肝窦壁SECs有许多窗孔,CD31和Cav-1呈现弱阳性染色。给予DMN刺激后,模型组大鼠肝窦壁SECs窗孔数量逐渐减少,CD31和Cav-1阳性染色细胞逐渐增多,至4wk末时到达峰值；停止DMN刺激后,模型对照组大鼠肝窦壁SECs窗孔数量逐渐增多,CD31和Car-1阳性染色细胞逐渐减少。经2wk和4wk处理后,与模型组和模型对照组比较,CME预防组和治疗组大鼠肝窦壁SECs窗孔数量显著增多,CD31和Cav-1阳性染色细胞逐渐显著减少。结论：在DMN诱导大鼠肝纤维化形成过程中,SECs表型发生变化,其通透性模式由以窗孔运送为主转变为以小窝运送为主,使通透性减少。CME能够改善SECs通透性,这可能是其抗肝纤维化作用机制之一。

螺内酯对肝纤维化大鼠Ⅰ/Ⅲ型胶原蛋白表达的影响

目的探讨螺内酯对实验性大鼠肝纤维化Ⅰ/Ⅲ型胶原蛋白表达的影响,初步揭示螺内酯对大鼠肝纤维化的预防作用及可能的机制.方法雄性 SD 大鼠81只,随机分为正常对照组(10只)、肝纤维化模型对照组(45只)及螺内酯组(26只).采用复合因素造模,螺内酯从造模开始每日1mL 100mg·kg^(-1)灌胃,共7wk.免疫组化染色及图像分析检测Ⅰ/Ⅲ型胶原含量.结果螺内酯组与肝纤维化组胶原面积比Ⅰ型胶原分别为:2.84±0.86,5.41±2.08,Ⅲ型胶原分别为:2.95±0.82,5.35±2.30.螺内酯组Ⅰ/Ⅲ型胶原增生程度明显降低(P<0.01).结论螺内酯可使肝组织Ⅰ/Ⅲ型胶原沉积明显减轻,提示螺内酯可明显预防肝纤维化的形成,ALD 在肝纤维化的发病中有一定意义.

苦参碱对实验大鼠肝纤维化的影响

目的 :研究苦参碱对实验大鼠肝纤维化的防治作用 ,并探讨其可能的机制。方法 :应用四氯化碳诱导大鼠实验性肝纤维化 ,以苦参碱防治。观察3,6 ,12wk时溶剂对照组、四氯化碳组、苦参碱组血清丙氨酸转氨酶 (ALT)、透明质酸 (HA)、肝组织羟脯氨酸 (HyP)含量以及肝脏病理变化。结果 :苦参碱能显著减轻实验大鼠肝细胞变性、坏死及纤维组织的形成 ,同时能降低不同实验阶段血清ALT(P <0 .0 1) ,HA(P <0 .0 1)以及肝组织中HyP含量 (P <0 .0 5)。结论 :苦参碱有保护肝细胞 ,减轻肝细胞坏死 ,防治四氯化碳诱发的肝纤维化的作用。

经典退黄三方抗二甲基亚硝胺诱导的大鼠肝纤维化的方证比较研究

目的:通过观察经典退黄三方茵陈蒿汤、茵陈五苓散和栀子柏皮汤对二甲基亚硝胺(dimeth-ylnitrosamine,DMN)诱导的大鼠肝纤维化模型的效应,探讨该模型的病机。方法:48只大鼠按体质量分层随机分为正常对照组、模型组、茵陈蒿汤组、茵陈五苓散组和栀子柏皮汤组,采用DMN腹腔注射4周的方法诱导大鼠肝纤维化模型。从造模第3周开始,各药物组在继续造模的同时予以相应的药物干预,正常对照组和模型组给以等量生理盐水。4周末结束实验,杀鼠取材,观察各组大鼠一般情况、肝组织病理学、羟脯氨酸(hydroxyproline,Hyp)含量及肝功能变化。结果:与正常对照组相比,模型组大鼠出现显著的肝损伤和肝纤维化,肝组织Hyp含量显著升高(P<0.01),肝功能显著异常(P<0.01)。与模型组比较,茵陈蒿汤可显著改善肝功能(P<0.05或P<0.01),显著改善肝组织病理改变,降低肝组织Hyp含量及肝脏胶原增生程度(P<0.01);茵陈五苓散可显著降低血清总胆红素含量(P<0.01),对肝组织病理影响不明显;而栀子柏皮汤显著改变肝脏病理,并对肝组织Hyp含量有降低作用。结论:茵陈蒿汤对DMN诱导的大鼠肝纤维化的治疗效果优于茵陈五苓散和栀子柏皮汤;DMN诱导的大鼠肝纤维化模型在其形成期的病机以"湿(瘀)热内蕴"为主,且湿(瘀)热并重,与茵陈蒿汤方证高度相关。

高脂饮食致大鼠非酒精性脂肪性肝炎肝纤维化模型的建立

目的建立并研究高脂肪饮食导致大鼠非酒精性脂肪性肝炎(NASH)肝纤维化的动物模型。方法雄性SD大鼠60只,随机分成正常对照组30只和模型组30只,分别给予普通饲料与高脂饲料,于第4、8、12周末将正常对照组与模型组随机处死10只。分别检测血清学指标,取肝组织做HE染色及Masson染色,应用图像分析法对Masson染色进行纤维化面积定量分析。结果两组大鼠体重均增加,8周时肝指数明显升高,血清胆固醇及总甘油三酯8周开始与正常对照组比较差异具有统计学意义。转氨酶不同时间点均有升高,8、12周时与正常对照组比较差异具有统计学意义。高脂饮食4周末,HE染色可见肝小叶结构完整,汇管区见少量炎症细胞浸润,无病理性纤维化发生。8周末,达到脂肪肝的诊断标准,开始出现肝纤维化趋势。造模12周,大鼠肝组织脂肪变程度达重度,纤维化面积增大。结论经改良配方后,成功建立了大鼠NASH肝纤维化模型。

中药软肝缩脾丸对肝纤维化大鼠TIMP-1/2蛋白表达的影响

目的探索肝纤维化发生的分子机制,尤其是TIMP-1,TIMP-2的作用。方法采用免疫组化和原位杂交的方法分别测定5组肝纤维化大鼠不同治疗前后TIMP-1,TIMP-2的基因调节和蛋白表达。结果 CCl_4模型组TIMP-1,TIMP-2 mRNA及蛋白水平明显高于治疗组。正常组大鼠肝组织无一例阳性。结论 TIMP-1,TIMP-2与肝纤维化形成密切相关,软肝缩脾丸对TIMP-1,TIMP-2的基因和蛋白表达有一定的抑制作用。

虫草菌丝提取物对大鼠脂肪性肝炎与肝纤维化的影响

目的探讨虫草菌丝提取物对大鼠脂肪性肝炎与盱纤维化的作用。方法Wistar雄性大鼠,随机分为3 wk和6 wk的正常组、模型组和虫草菌丝组。造模后3 wk和6 wk分别观察肝组织脂肪变性、炎症与胶原沉积;分析血清ALT、AST水平与TBil、Alb、TG、TC含量;肝组织TG、MDA、GSH含量与SOD、γ-GT活性、羟脯氯酸(Hyp)含量及肝组织α-SMA表达。结果3 wk、6 wk模型大鼠血清ALT、AST、γ-GT活性与TBil含量均升高(P<0.05),Alb、TG含量下降(P<0.01),肝组织Hyp、TG、MDA含量明显增加(P<0.01),α-SMA表达增加。3 wk虫草菌丝组改善模型大鼠肝组织脂肪变性与炎症;降低血清TBil含量,提高血清Alb含量;降低肝组织TG、MDA含量(P<0.01),提高肝组织GSH含量与SOD活性(P<0.05)。6 wk虫草菌丝组减轻模型大鼠肝纤维化;降低血清ALT、AST水平(P<0.05);降低肝组织TG、MDA含量和γ-GT活性(P<0.05),提高SOD活性。虫草菌丝3 wk和6 wk组均明显减少α-SMA表达(P<0.05),且6 wk作用较3 wk更为明显。结论虫草菌丝提取物显著改善大鼠脂肪性肝炎、抑制脂肪性肝纤维化,其作用机制与抗肝脂质过氧化、抑制肝星状细胞活化有关。

MR弥散加权成像在兔肝纤维化模型中的初步实验研究

目的探讨MR弥散加权成像(MR-DWI)检测早期肝纤维化及定量肝纤维化程度的能力。方法对以CCl4诱导产生的肝纤维化模型兔和对照兔行MR常规扫描及DWI检查,以病理学肝纤维化分期为基础将其划分为无肝纤维化组(S0)、轻中度纤维化组(S1～S2)和重度纤维化/肝硬化组(S3～S4) ,在b取300、600、1000 s/ mm2时,比较各组DWI图像信号强度(SI)、表观弥散系数(ADC)和指数表观弥散系数(EADC)的变化情况。结果在b取300、600 s/ mm2时,无肝纤维化组、轻中度纤维化组和重度纤维化/肝硬化组的SI与EADC值依次升高,ADC值依次降低,差异存在统计学意义(P<0 .01) ;在b取1000 s/ mm2时,仅SI值随肝纤维化组别升高而升高(P<0 .01)。b取300 s/ mm2时,ADC与EADC值三组间两两比较差异均有统计学意义(P<0 .01)。结论初步实验研究表明,肝纤维化时肝内水分子弥散受限,且随肝纤维化程度增高,水分子弥散能力逐渐减低。在选择合适b值的情况下,MR-DWI可成为检测早期肝纤维化及定量肝纤维化程度的有效手段。

磁共振氢质子波谱在兔肝纤维化模型中的应用

目的通过动物模型评价氢质子磁共振波谱(1H-MRS)在肝纤维化诊断中的应用价值。方法对以四氯化碳诱导产生的肝纤维化模型兔和对照组兔行1H-MRS检查,获得肝脏主要含氢代谢物的波峰下面积,包括脂质(lipid)、胆碱(Cho)、糖原/葡萄糖复合物(Glyu),同时计算代谢物与脂质的波峰下面积比值(Cho/lipid、Glyu/lipid)。以病理学肝纤维化分期为基础将兔划分为无纤维化组(S0)、轻中度纤维化组(S1～S2)和重度纤维化/肝硬化组(S3～S4),比较不同组间1H-MRS参数变化情况,同时观察透射电镜下肝脏超微结构的变化。结果Cho、Glyu和lipid在轻中度纤维化组降低,在重度纤维化/肝硬化组升高;Cho/lipid和Glyu/lipid随肝纤维化的加重而升高。重度纤维化/肝硬化组与另两组Cho/lipid比较,差异有统计学意义(P均<0.05),其余指标在纤维化各组间差异无统计学意义。肝组织超微结构改变在轻中度纤维化时以肝细胞损伤为主,在重度纤维化/肝硬化时肝细胞损伤与细胞外纤维基质沉积并重。结论肝纤维化时肝细胞损伤引起代谢物减少,细胞外基质沉积阻碍代谢物排出,1H-MRS变化是对肝组织超微结构改变的综合反映。Cho/lipid是检测重度纤维化/肝硬化的有效指标。

肝硬化大鼠模型的建立及其稳定性

目的:探讨肝硬化动物模型(CM)的建立及其稳定性。方法:80只Wistar大鼠,雌雄各半。分别采用复合因素法、四氯化碳(CCl4)加乙醇法及玉米面、胆固醇加乙醇法建立大鼠肝硬化的模型(假小叶形成为判定CM成功的唯一标准)。复合因素法:40只大鼠,饲料为80%的玉米面、20%的动物油、0.5%胆固醇,饮料仅为15%的酒精,首次皮下注射40%CCl4-橄榄油溶液5 mL.kg-1(以下浓度相同),以后每3 d皮下注射CCl43 mL.kg-1。第6周末随机处死6只大鼠做肝脏病理,均符合肝硬化诊断标准。将余下存活的26只(逃逸2只、死亡6只)随机分为两组,每组13只均正常饲养,其中一组每7 d皮下注射3 mL.kg-1CCl4,观察第7、8周末的病理变化。CCl4加乙醇法:20只大鼠,以正常饲料喂养,余条件同复合因素法前6周。玉米面、胆固醇加乙醇法:20只大鼠,不用CCl4,余条件同复合因素法前6周。结果:复合因素法6周末处死6只大鼠均形成CM,成模后正常饲养,2周后假小叶均消失,而继续应用CCl42周后,大鼠假小叶基本存在。其余2种方法大鼠均未见典型肝硬化改变。结论:采用复合因素法建立的CM形成率高,成模后CCl4的应用能够保持CM的相对稳定。

肝纤维化磁共振灌注成像的初步实验研究

目的:探讨大鼠化学性肝纤维化的MR灌注加权成像(PWI)表现,评价PWI对肝纤维化的诊断价值。方法:皮下注射CCl4建立大鼠肝纤维化模型(50只)和对照组(10只)进行MR-PWI扫描。按肝纤维化病理分期进行分组,采用方差分析比较各组间门静脉和肝实质灌注曲线的峰值时间、信号最大上升斜率和最大下降斜率的变化,分析各灌注参数与肝纤维化程度的相关性。结果:模型组38只和对照组10只共48只大鼠完成MR检查。病理分期S0(n=13)、S1(n=5)、S2(n=9)、S3(n=13)、S4(n=8)。S0期门静脉和肝实质的峰值时间[(15.03±1.05)s和(25.93±1.70)s],S1~S4期肝纤维化组的峰值时间逐渐递增[均值(26.29±3.52)s和(41.92±5.76)s],S0期与S2~S4期差异有统计学意义(P<0.05,<0.001,<0.001)。S0期门静脉和肝实质的最大上升斜率、最大下降斜率[门静脉(420.46±27.26)1/s和(193.50±16.76)1/s,肝实质(140.10±16.73)1/s和(121.00±15.16)1/s],S1~S4期肝纤维化组的最大上升、下降斜率逐渐递减[门静脉均值(292.61±40.02)1/s和(139.73±13.22)1/s,肝实质均值(76.70±9.55)1/s和(97.56±15.73)1/s],S0~S2期与S3、S4期差异有统计学意义(P<0.05)。峰值时间与肝纤维化分期呈显著正相关(P<0.01),最大上升斜率、门静脉的最大下降斜率与肝纤维化分期呈显著负相关(P<0.01)。结论:MR-PWI可以检测大鼠肝纤维化改变,可对中重度(S2~S4期)肝纤维化进行早期诊断。